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TW202423987A - Anti-ccr8 antibody and application thereof - Google Patents

Anti-ccr8 antibody and application thereof Download PDF

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TW202423987A
TW202423987A TW112147381A TW112147381A TW202423987A TW 202423987 A TW202423987 A TW 202423987A TW 112147381 A TW112147381 A TW 112147381A TW 112147381 A TW112147381 A TW 112147381A TW 202423987 A TW202423987 A TW 202423987A
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seq
amino acid
acid sequence
antibody
variable region
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TW112147381A
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郭建
霍永庭
蘆迪
肖亮
張軼博
歐穎燁
羅穎
張喆
李永鋒
耿夢圓
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大陸商廣東菲鵬製藥股份有限公司
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Publication of TW202423987A publication Critical patent/TW202423987A/en

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Abstract

The present disclosure relates to the technical field of biotechnology, and provides an anti-human CCR8 antibody and application thereof. The anti-human CCR8 antibody provided in the present disclosure includes a heavy chain complementary determining region and a light chain complementary determining region. The anti-CCR8 antibody can specifically bind to human CCR8 antigen and can be used to treat tumors.

Description

抗CCR8抗體及其應用Anti-CCR8 antibodies and their applications

[優先權聲明][Priority Claim]

本申請請求2022年12月07日向中國國家知識產權局提交的專利申請號為202211578659.6,發明名稱為「抗CCR8抗體及其應用」的中國專利申請的優先權和權益,並且通過參照將其全文併入本申請。This application claims the priority and benefits of the Chinese patent application numbered 202211578659.6, filed with the National Intellectual Property Administration of China on December 7, 2022, entitled "Anti-CCR8 Antibodies and Their Applications", and the entire text of which is incorporated into this application by reference.

本公開涉及生物技術領域,具體地,涉及一種抗CCR8抗體及其應用。The present disclosure relates to the field of biotechnology, and specifically, to an anti-CCR8 antibody and its application.

隨著人們對腫瘤免疫微環境認識的不斷提高,Treg(regulatory T cell)細胞對抑制機體抗腫瘤免疫應答的作用被越來越重視。As people's understanding of the tumor immune microenvironment continues to improve, the role of Treg (regulatory T cell) cells in inhibiting the body's anti-tumor immune response has become increasingly important.

趨化因子受體8(Chemokine receptor 8,CCR8)為七跨膜G蛋白偶聯受體,屬於趨化因子受體CC亞家族。近年來的一些研究證明,在多種小鼠腫瘤模型及人腫瘤組織中僅腫瘤組織浸潤的Treg細胞廣泛高表現CCR8,而在外周血中的Treg細胞及其他PBMC(Peripheral Blood Mononuclear Cell)均不表現CCR8,CCR8已被視為腫瘤浸潤Treg的表面標記。標靶CCR8是一種很有前景的癌症免疫治療方法。但CCR8為七次跨膜的GPCR(G protein-coupled receptor)受體,胞外端非常短且不連續,相較於一般單次跨膜的蛋白而言,製備抗體的難度更大。Chemokine receptor 8 (CCR8) is a seven-transmembrane G protein-coupled receptor that belongs to the CC subfamily of chemokine receptors. Some studies in recent years have shown that in various mouse tumor models and human tumor tissues, only tumor tissue-infiltrating Treg cells widely and highly express CCR8, while Treg cells in peripheral blood and other PBMCs (Peripheral Blood Mononuclear Cells) do not express CCR8. CCR8 has been regarded as a surface marker of tumor-infiltrating Treg. Targeting CCR8 is a promising cancer immunotherapy method. However, CCR8 is a seven-transmembrane GPCR (G protein-coupled receptor) receptor with a very short and discontinuous extracellular end. Compared with general single-transmembrane proteins, it is more difficult to prepare antibodies.

本公開開發一種抗CCR8抗體。在一些實施方案中,其可增強機體抗腫瘤免疫反應,提高腫瘤患者生存率。The present invention discloses an anti-CCR8 antibody. In some embodiments, the anti-CCR8 antibody can enhance the body's anti-tumor immune response and improve the survival rate of tumor patients.

在一些實施方案中,本公開公開一種抗人CCR8抗體,所述抗體包含重鏈可變區和輕鏈可變區,所述重鏈可變區包括SEQ ID No.1、3、5、7、9或11中的HCDR1、HCDR2和HCDR3,和/或所述抗體的輕鏈可變區包括SEQ ID No.2、4、6、8、10或12中的LCDR1、LCDR2和LCDR3。In some embodiments, the present disclosure discloses an anti-human CCR8 antibody, which comprises a heavy chain variable region and a light chain variable region, wherein the heavy chain variable region includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.1, 3, 5, 7, 9 or 11, and/or the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.2, 4, 6, 8, 10 or 12.

在一些實施方案中,其中, A.所述抗體的重鏈可變區包括SEQ ID No.1中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.2中的LCDR1、LCDR2和LCDR3; B.所述抗體的重鏈可變區包括SEQ ID No.3中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.4中的LCDR1、LCDR2和LCDR3; C.所述抗體的重鏈可變區包括SEQ ID No.5中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.6中的LCDR1、LCDR2和LCDR3; D.所述抗體的重鏈可變區包括SEQ ID No.7中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.8中的LCDR1、LCDR2和LCDR3; E.所述抗體的重鏈可變區包括SEQ ID No.9中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.10中的LCDR1、LCDR2和LCDR3;或者 F.所述抗體的重鏈可變區包括SEQ ID No.11中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.12中的LCDR1、LCDR2和LCDR3。 In some embodiments, wherein, A. the heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.1, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.2; B. the heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.3, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.4; C. the heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.5, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.6; D. the heavy chain variable region of the antibody includes SEQ ID E. The heavy chain variable region of the antibody comprises HCDR1, HCDR2 and HCDR3 in SEQ ID No.7, and the light chain variable region of the antibody comprises LCDR1, LCDR2 and LCDR3 in SEQ ID No.8; E. The heavy chain variable region of the antibody comprises HCDR1, HCDR2 and HCDR3 in SEQ ID No.9, and the light chain variable region of the antibody comprises LCDR1, LCDR2 and LCDR3 in SEQ ID No.10; or F. The heavy chain variable region of the antibody comprises HCDR1, HCDR2 and HCDR3 in SEQ ID No.11, and the light chain variable region of the antibody comprises LCDR1, LCDR2 and LCDR3 in SEQ ID No.12.

在一些實施方案中,前述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3由IMGT編號系統定義,或由Kabat編號系統定義,或由Chothia 編號系統定義,或由Contact編號系統定義,或由AbM編號系統定義;在一些實施方案中,前述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3根據 Kabat編號系統定義。在一些實施方案中,前述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3根據 IMGT編號系統定義。In some embodiments, the aforementioned HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined by the IMGT numbering system, or by the Kabat numbering system, or by the Chothia numbering system, or by the Contact numbering system, or by the AbM numbering system; in some embodiments, the aforementioned HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined according to the Kabat numbering system. In some embodiments, the aforementioned HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined according to the IMGT numbering system.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,其中, a.重鏈可變區的HCDR1包含SEQ ID NO.13的氨基酸序列,HCDR2包含SEQ ID NO.14的氨基酸序列,和HCDR3包含SEQ ID NO.15的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.17的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列; b.重鏈可變區的HCDR1包含SEQ ID NO.19的氨基酸序列,HCDR2包含SEQ ID NO.20的氨基酸序列,和HCDR3包含SEQ ID NO.21的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.17的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列; c.重鏈可變區的HCDR1包含SEQ ID NO.22的氨基酸序列,HCDR2包含SEQ ID NO.23的氨基酸序列,和HCDR3包含SEQ ID NO.24的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.25的氨基酸序列,LCDR2包含SEQ ID NO.26的氨基酸序列,和LCDR3包含SEQ ID NO.27的氨基酸序列; d.重鏈可變區的HCDR1包含SEQ ID NO.13的氨基酸序列,HCDR2包含SEQ ID NO.28的氨基酸序列,和HCDR3包含SEQ ID NO.29的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.30的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列; e.重鏈可變區的HCDR1包含SEQ ID NO.31的氨基酸序列,HCDR2包含SEQ ID NO.32的氨基酸序列,和HCDR3包含SEQ ID NO.33的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.34的氨基酸序列,LCDR2包含SEQ ID NO.35的氨基酸序列,和LCDR3包含SEQ ID NO.36的氨基酸序列;或 f.重鏈可變區的HCDR1包含SEQ ID NO.13的氨基酸序列,HCDR2包含SEQ ID NO.37的氨基酸序列,和HCDR3包含SEQ ID NO.38的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.17的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列。 In some embodiments, the anti-human CCR8 antibody as described in any of the above items, wherein, a. HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, HCDR2 comprises the amino acid sequence of SEQ ID NO.14, and HCDR3 comprises the amino acid sequence of SEQ ID NO.15; and LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18; b. HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.19, HCDR2 comprises the amino acid sequence of SEQ ID NO.20, and HCDR3 comprises the amino acid sequence of SEQ ID NO.21; and LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18; c. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.22, HCDR2 comprises the amino acid sequence of SEQ ID NO.23, and HCDR3 comprises the amino acid sequence of SEQ ID NO.24; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.25, LCDR2 comprises the amino acid sequence of SEQ ID NO.26, and LCDR3 comprises the amino acid sequence of SEQ ID NO.27; d. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, HCDR2 comprises the amino acid sequence of SEQ ID NO.28, and HCDR3 comprises the amino acid sequence of SEQ ID NO.29; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.30, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18; e. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.31, HCDR2 comprises the amino acid sequence of SEQ ID NO. ID NO.32, and HCDR3 comprises the amino acid sequence of SEQ ID NO.33; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.34, LCDR2 comprises the amino acid sequence of SEQ ID NO.35, and LCDR3 comprises the amino acid sequence of SEQ ID NO.36; or f. the HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, HCDR2 comprises the amino acid sequence of SEQ ID NO.37, and HCDR3 comprises the amino acid sequence of SEQ ID NO.38; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,其包含分別如SEQ ID NO.13、SEQ ID NO.14和SEQ ID NO.15所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.16、SEQ ID NO.17和SEQ ID NO.18所示的LCDR1、LCDR2和LCDR3;或者所述抗人CCR8抗體包含分別如SEQ ID NO.19、SEQ ID NO.20和SEQ ID NO.21所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.16、SEQ ID NO.17和SEQ ID NO.18所示的LCDR1、LCDR2和LCDR3;或者所述抗人CCR8抗體包含分別如SEQ ID NO.22、SEQ ID NO.23和SEQ ID NO.24所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.25、SEQ ID NO.26和SEQ ID NO.27所示的LCDR1、LCDR2和LCDR3。In some embodiments, the anti-human CCR8 antibody as described in any of the above items comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.13, SEQ ID NO.14 and SEQ ID NO.15, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.17 and SEQ ID NO.18, respectively; or the anti-human CCR8 antibody comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.19, SEQ ID NO.20 and SEQ ID NO.21, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.17 and SEQ ID NO.18, respectively; or the anti-human CCR8 antibody comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.22, SEQ ID NO.23 and SEQ ID NO.24, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.25, SEQ ID NO.26 and SEQ ID NO. LCDR1, LCDR2 and LCDR3 shown in NO.27.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,所述抗體為鼠源抗體,嵌合抗體或人源化抗體。In some embodiments, the anti-human CCR8 antibody as described in any of the above items is a murine antibody, a chimeric antibody or a humanized antibody.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,其中,所述抗體的重鏈可變區包括與SEQ ID No.1、3、5、7、9或11具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列,和/或輕鏈可變區包括與SEQ ID No.2、4、6、8、10或12具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列。In some embodiments, the anti-human CCR8 antibody as described in any of the above items, wherein the heavy chain variable region of the antibody comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity with SEQ ID No.1, 3, 5, 7, 9 or 11, and/or the light chain variable region comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity with SEQ ID No.2, 4, 6, 8, 10 or 12.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,其中,所述抗體的重鏈可變區包括與SEQ ID No.1、3、5、7、9或11具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列,並且輕鏈可變區包括與SEQ ID No.2、4、6、8、10或12具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列。In some embodiments, the anti-human CCR8 antibody as described in any of the above items, wherein the heavy chain variable region of the antibody comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity with SEQ ID No.1, 3, 5, 7, 9 or 11, and the light chain variable region comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity with SEQ ID No.2, 4, 6, 8, 10 or 12.

在一些實施方案中,本公開提供一種抗人CCR8抗體,其中,所述抗體的重鏈可變區包括與SEQ ID No.1、3、5、7、9或11具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列,和/或輕鏈可變區包括與SEQ ID No.2、4、6、8、10或12具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列。In some embodiments, the present disclosure provides an anti-human CCR8 antibody, wherein the heavy chain variable region of the antibody comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity to SEQ ID No. 1, 3, 5, 7, 9 or 11, and/or the light chain variable region comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity to SEQ ID No. 2, 4, 6, 8, 10 or 12.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,其中,所述抗體的重鏈可變區包括與SEQ ID No.1、3、5、7、9或11具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列,並且輕鏈可變區包括與SEQ ID No.2、4、6、8、10或12具有至少90%(例如90%、91%、92%、93%、94%、95%、96%、97%、98%或99%)序列同一性的氨基酸序列。In some embodiments, the anti-human CCR8 antibody as described in any of the above items, wherein the heavy chain variable region of the antibody comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity with SEQ ID No.1, 3, 5, 7, 9 or 11, and the light chain variable region comprises an amino acid sequence having at least 90% (e.g., 90%, 91%, 92%, 93%, 94%, 95%, 96%, 97%, 98% or 99%) sequence identity with SEQ ID No.2, 4, 6, 8, 10 or 12.

在一些實施方案中,如上任一項所述的抗人CCR8抗體, (i)所述重鏈可變區包含SEQ ID NO.1的氨基酸序列,和所述輕鏈可變區包含SEQ ID NO.2的氨基酸序列; (ii)所述重鏈可變區包含SEQ ID NO.3的氨基酸序列,和所述輕鏈可變區包含SEQ ID NO.4的氨基酸序列; (iii)所述重鏈可變區包含SEQ ID NO.5的氨基酸序列,和所述輕鏈可變區包含SEQ ID NO.6的氨基酸序列; (iv)所述重鏈可變區包含SEQ ID NO.7的氨基酸序列,和所述輕鏈可變區包含SEQ ID NO.8的氨基酸序列; (v)所述重鏈可變區包含SEQ ID NO.9的氨基酸序列,和所述輕鏈可變區包含SEQ ID NO.10的氨基酸序列; (vi)所述重鏈可變區包含SEQ ID NO.11的氨基酸序列,和所述輕鏈可變區包含SEQ ID NO.12的氨基酸序列。 In some embodiments, the anti-human CCR8 antibody as described in any of the above items, (i) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.1, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.2; (ii) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.3, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.4; (iii) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.5, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.6; (iv) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.7, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.8; (v) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.9, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.10; (vi) the heavy chain variable region comprises SEQ The amino acid sequence of SEQ ID NO.11, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.12.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,所述抗體還包含恒定區;在一些實施方案中,所述抗體的重鏈恒定區選自IgG1、IgG2、IgG3和IgG4的重鏈恒定區,所述輕鏈恒定區選自κ或λ鏈恒定區;在一些實施方案中,所述恒定區的種屬來源為鼠或人;在一些實施方案中,所述重鏈恒定區為鼠IgG2a恒定區、鼠IgG1恒定區、人IgG1恒定區;在一些實施方案中,重鏈恒定區為人IgG1(DLE)或人IgG1(DE)恒定區;和/或輕鏈恒定區為鼠κ恒定區或人κ恒定區。In some embodiments, the anti-human CCR8 antibody as described in any of the above items further comprises a constant region; in some embodiments, the heavy chain constant region of the antibody is selected from the heavy chain constant regions of IgG1, IgG2, IgG3 and IgG4, and the light chain constant region is selected from the κ or λ chain constant region; in some embodiments, the species origin of the constant region is mouse or human; in some embodiments, the heavy chain constant region is mouse IgG2a constant region, mouse IgG1 constant region, human IgG1 constant region; in some embodiments, the heavy chain constant region is human IgG1 (DLE) or human IgG1 (DE) constant region; and/or the light chain constant region is mouse κ constant region or human κ constant region.

在一些實施方案中,所述重鏈恒定區包括SEQ ID NO.39、41或42的氨基酸序列,輕鏈恒定區包括SEQ ID NO.40或43的氨基酸序列。In some embodiments, the heavy chain constant region comprises the amino acid sequence of SEQ ID NO.39, 41 or 42, and the light chain constant region comprises the amino acid sequence of SEQ ID NO.40 or 43.

在一些實施方案中,所述抗人CCR8抗體重鏈包含SEQ ID NO.44的氨基酸序列,輕鏈包括SEQ ID NO.45的氨基酸序列;或者所述抗人CCR8抗體重鏈包含SEQ ID NO.46的氨基酸序列,輕鏈包括SEQ ID NO.47的氨基酸序列;或者所述抗人CCR8抗體重鏈包含SEQ ID NO.48的氨基酸序列,輕鏈包括SEQ ID NO.49的氨基酸序列。In some embodiments, the anti-human CCR8 antibody heavy chain comprises the amino acid sequence of SEQ ID NO.44, and the light chain comprises the amino acid sequence of SEQ ID NO.45; or the anti-human CCR8 antibody heavy chain comprises the amino acid sequence of SEQ ID NO.46, and the light chain comprises the amino acid sequence of SEQ ID NO.47; or the anti-human CCR8 antibody heavy chain comprises the amino acid sequence of SEQ ID NO.48, and the light chain comprises the amino acid sequence of SEQ ID NO.49.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,所述抗體為全長抗體或為選自F(ab’)2、Fab’-SH、Fab’、Fab、scFab、dsFv、(dsFv)2、Fv和scFv中的任意一種抗原結合片段。In some embodiments, the anti-human CCR8 antibody as described in any of the above items is a full-length antibody or any antigen-binding fragment selected from F(ab')2, Fab'-SH, Fab', Fab, scFab, dsFv, (dsFv)2, Fv and scFv.

在一些實施方案中,發明公開與前面任一項所述的抗人CCR8抗體競爭性結合人CCR8的抗體,或與前面任一項所述的抗人CCR8抗體結合相同表位的抗體。In some embodiments, the invention discloses an antibody that competitively binds to human CCR8 with any of the anti-human CCR8 antibodies described above, or an antibody that binds to the same epitope as any of the anti-human CCR8 antibodies described above.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,其中所述抗人CCR8抗體具有以下特性中的至少一種: A. 所述抗人CCR8抗體能與人CCR8特異性結合;在一些實施方案中,所述抗人CCR8抗體能以≤5nM(例如,≤4.50 nM、≤3.00 nM、≤2.00 nM、≤1.00 nM、≤0.9nM、≤0.8nM、≤0.7nM、≤0.6nM、≤0.5nM、≤0.4nM、≤0.3nM、≤0.2nM、≤0.1nM、≤0.09nM、≤0.08nM或更小)的EC50值(Concentration for 50% of Maximal Effect)與表現人CCR8的Raji細胞結合,其中,所述EC50值通過流式細胞分析法測定;在一些實施方案中,所述EC50值通過本申請實施例2的方法測定; B. 所述抗人CCR8抗體具有抑制腫瘤生長功能; 在一些實施方案中,所述抗人CCR8抗體腫瘤抑制率大於或等於30%(例如,大於30%、40%、45%、50%、60%、70%、80%、90%或更大);在一些實施方案中,所述抗人CCR8抗體腫瘤抑制率通過本公開實施例5方法測定; C. 所述抗人CCR8抗體具有ADCC(Antibody-dependent cellular cytotoxicity)活性;在一些實施方案中,所述抗人CCR8抗體ADCC活性通過本公開實施例4的方法測定。 In some embodiments, the anti-human CCR8 antibody as described in any of the above items, wherein the anti-human CCR8 antibody has at least one of the following properties: A. The anti-human CCR8 antibody can specifically bind to human CCR8; In some embodiments, the anti-human CCR8 antibody can bind to human CCR8 with an EC50 value (Concentration for 50% of Maximal Effect) binds to Raji cells expressing human CCR8, wherein the EC50 value is determined by flow cytometry; in some embodiments, the EC50 value is determined by the method of Example 2 of this application; B. The anti-human CCR8 antibody has the function of inhibiting tumor growth; in some embodiments, the anti-human CCR8 antibody tumor inhibition rate is greater than or equal to 30% (for example, greater than 30%, 40%, 45%, 50%, 60%, 70%, 80%, 90% or greater); in some embodiments, the anti-human CCR8 antibody tumor inhibition rate is determined by the method of Example 5 of this disclosure; C. The anti-human CCR8 antibody has ADCC (Antibody-dependent cellular cytotoxicity) activity; in some embodiments, the anti-human CCR8 antibody ADCC activity is determined by the method of Example 4 of this disclosure.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,其中所述抗人CCR8抗體能與人CCR8特異性結合;在一些實施方案中,所述抗人CCR8抗體能以≤5nM(例如,≤4.50 nM、≤3.00 nM、≤2.00 nM、≤1.00 nM、≤0.9nM、≤0.8nM、≤0.7nM、≤0.6nM、≤0.5nM、≤0.4nM、≤0.3nM、≤0.2nM、≤0.1nM、≤0.09nM、≤0.08nM或更小)的EC50值與表現人CCR8的Raji細胞結合,其中,所述EC50值通過流式細胞分析法測定。In some embodiments, the anti-human CCR8 antibody as described in any of the above items, wherein the anti-human CCR8 antibody can specifically bind to human CCR8; in some embodiments, the anti-human CCR8 antibody can bind to Raji cells expressing human CCR8 with an EC50 value of ≤5nM (e.g., ≤4.50 nM, ≤3.00 nM, ≤2.00 nM, ≤1.00 nM, ≤0.9nM, ≤0.8nM, ≤0.7nM, ≤0.6nM, ≤0.5nM, ≤0.4nM, ≤0.3nM, ≤0.2nM, ≤0.1nM, ≤0.09nM, ≤0.08nM or less), wherein the EC50 value is determined by flow cytometry.

在一些實施方案中,所述EC50值通過本申請實施例2的方法測定。In some embodiments, the EC50 value is determined by the method of Example 2 of this application.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,具有抑制腫瘤生長功能。In some embodiments, the anti-human CCR8 antibody described in any of the above items has the function of inhibiting tumor growth.

在一些實施方案中,所述抗人CCR8抗體腫瘤抑制率大於或等於30%(例如,大於30%、40%、45%、50%、60%、70%、80%、90%或更大)。In some embodiments, the anti-human CCR8 antibody tumor inhibition rate is greater than or equal to 30% (e.g., greater than 30%, 40%, 45%, 50%, 60%, 70%, 80%, 90% or more).

在一些實施方案中,所述抗人CCR8抗體腫瘤抑制率通過本公開實施例5方法測定。In some embodiments, the anti-human CCR8 antibody tumor inhibition rate is determined by the method of Example 5 of the present disclosure.

在一些實施方案中,如上任一項所述的抗人CCR8抗體,具有ADCC活性。In some embodiments, the anti-human CCR8 antibody described in any of the above items has ADCC activity.

在一些實施方案中,所述抗人CCR8抗體ADCC活性通過本公開實施例4的方法測定。In some embodiments, the anti-human CCR8 antibody ADCC activity is determined by the method of Example 4 of the present disclosure.

本公開還提供一種多特異性抗體,所述多特異性抗體包含前面任一項所示的抗人CCR8抗體。The present disclosure also provides a multispecific antibody, which comprises the anti-human CCR8 antibody described in any of the above items.

在一些實施方案中,所述抗體為雙特異性抗體。In some embodiments, the antibody is a bispecific antibody.

本公開還提供一種抗體偶聯物,所述抗體偶聯物包括前面任一項所述的抗人CCR8抗體。The present disclosure also provides an antibody conjugate, which comprises the anti-human CCR8 antibody described in any of the above items.

在一些實施方案中,所述抗體偶聯物還包括與所述抗體偶聯的治療劑或顯像劑。In some embodiments, the antibody conjugate further comprises a therapeutic agent or an imaging agent conjugated to the antibody.

在一些實施方案中,所述抗體偶聯物還包括與所述抗體偶聯的生物素或生物素衍生物。In some embodiments, the antibody conjugate further comprises biotin or a biotin derivative conjugated to the antibody.

在一些實施方案中,所述抗體偶聯物還包括與所述抗體偶聯的固相載體。In some embodiments, the antibody conjugate further comprises a solid phase carrier coupled to the antibody.

在一些實施方案中,所述抗體偶聯物還包括與所述抗體偶聯的標記物。In some embodiments, the antibody conjugate further comprises a label conjugated to the antibody.

在一些實施方案中,所述標記物選自螢光染料、酶、放射性同位素、化學發光試劑和納米顆粒類標記物中的至少一種。In some embodiments, the label is selected from at least one of fluorescent dyes, enzymes, radioisotopes, chemiluminescent reagents and nanoparticle labels.

在一些實施方案中,所述標記物為膠體金。In some embodiments, the label is colloidal gold.

本公開還提供一種嵌合抗原受體(CAR),所述嵌合抗原受體包括抗原結合結構域,所述抗原結合結構域包括前面任一項所述的抗人CCR8抗體。The present disclosure also provides a chimeric antigen receptor (CAR), wherein the chimeric antigen receptor comprises an antigen binding domain, and the antigen binding domain comprises the anti-human CCR8 antibody described in any of the above items.

本公開還提供一種CAR-免疫細胞,所述CAR-免疫細胞表現前面所述的嵌合抗原受體。The present disclosure also provides a CAR-immune cell, which expresses the chimeric antigen receptor described above.

本公開還提供一種分離的核酸,其編碼前面任一項所述的抗人CCR8抗體。The present disclosure also provides an isolated nucleic acid encoding the anti-human CCR8 antibody described in any of the above items.

本公開還提供一種細胞,其含前述的核酸。The present disclosure also provides a cell comprising the aforementioned nucleic acid.

本公開還提供一種藥物組合物,其包含:前面任一項所述的抗人CCR8抗體、多特異性抗體、抗體偶聯物、細胞或核酸。The present disclosure also provides a pharmaceutical composition comprising: the anti-human CCR8 antibody, multispecific antibody, antibody conjugate, cell or nucleic acid described in any one of the above items.

在一些實施方案中,所述藥物組合物還包含一種或多種藥學上可接受的載體、稀釋劑或賦形劑。In some embodiments, the pharmaceutical composition further comprises one or more pharmaceutically acceptable carriers, diluents, or excipients.

本公開還提供前面任一項所述的抗人CCR8抗體、多特異性抗體、抗體偶聯物、細胞、核酸或藥物組合物在製備具有以下至少一種用途的產品中的應用:診斷人CCR8表現異常的相關疾病、治療人CCR8表現異常的相關疾病或檢測人CCR8的表現。The present disclosure also provides the use of any of the above-mentioned anti-human CCR8 antibodies, multispecific antibodies, antibody conjugates, cells, nucleic acids or drug compositions in the preparation of products having at least one of the following uses: diagnosing diseases related to abnormal human CCR8 expression, treating diseases related to abnormal human CCR8 expression or detecting human CCR8 expression.

在一些實施方案中,所述人CCR8表現異常的相關疾病為腫瘤。所述人CCR8表現異常的腫瘤優選為乳腺癌、卵巢癌、腎癌、胰腺癌、膀胱癌、胃癌、宮頸癌、結腸癌、肉瘤、肝癌或肺癌。In some embodiments, the disease related to abnormal human CCR8 expression is a tumor. The tumor with abnormal human CCR8 expression is preferably breast cancer, ovarian cancer, kidney cancer, pancreatic cancer, bladder cancer, gastric cancer, cervical cancer, colon cancer, sarcoma, liver cancer or lung cancer.

在一些實施方案中,本公開提供一種治療疾病的方法,所述方法包括向有需要的受試者施用治療有效量的前面任一項所述的抗人CCR8抗體、多特異性抗體、抗體偶聯物、細胞、核酸或藥物組合物的步驟。In some embodiments, the present disclosure provides a method for treating a disease, comprising the step of administering to a subject in need thereof a therapeutically effective amount of any of the above anti-human CCR8 antibodies, multispecific antibodies, antibody conjugates, cells, nucleic acids or drug compositions.

在一些實施方案中,所述疾病為人CCR8表現異常的相關疾病。In some embodiments, the disease is a disease related to abnormal expression of human CCR8.

在一些實施方案中,所述疾病為腫瘤。所述人CCR8表現異常的腫瘤優選為乳腺癌、卵巢癌、腎癌、胰腺癌、膀胱癌、胃癌、宮頸癌、結腸癌、肉瘤、肝癌或肺癌。In some embodiments, the disease is a tumor. The tumor in which human CCR8 expresses abnormally is preferably breast cancer, ovarian cancer, kidney cancer, pancreatic cancer, bladder cancer, gastric cancer, cervical cancer, colon cancer, sarcoma, liver cancer or lung cancer.

在另一個方面,本公開還提供用作藥物的前述任一項所述的抗人CCR8抗體、多特異性抗體、抗體偶聯物、細胞、核酸或藥物組合物。In another aspect, the present disclosure also provides any of the aforementioned anti-human CCR8 antibodies, multispecific antibodies, antibody conjugates, cells, nucleic acids or drug compositions for use as a drug.

在一些實施方案中,藥物用於治療疾病。在一些實施方案中,所述疾病為人CCR8表現異常的相關疾病。在一些實施方案中,所述人CCR8表現異常的相關疾病為腫瘤。所述人CCR8表現異常的腫瘤優選為乳腺癌、卵巢癌、腎癌、胰腺癌、膀胱癌、胃癌、宮頸癌、結腸癌、肉瘤、肝癌或肺癌。In some embodiments, the drug is used to treat a disease. In some embodiments, the disease is a disease related to abnormal human CCR8 expression. In some embodiments, the disease related to abnormal human CCR8 expression is a tumor. The tumor with abnormal human CCR8 expression is preferably breast cancer, ovarian cancer, kidney cancer, pancreatic cancer, bladder cancer, gastric cancer, cervical cancer, colon cancer, sarcoma, liver cancer or lung cancer.

在一些實施方案中,前面任一項所述的治療,進一步包括向受試者施用另外的治療藥物。In some embodiments, the treatment described in any of the above items further comprises administering an additional therapeutic drug to the subject.

在一些實施方案中,所述另外的治療藥物為化療劑,例如鉑絡合物、紫杉烷、培美曲塞、吉西他濱、氟尿嘧啶、伊立替康、依託泊苷或多柔比星等。In some embodiments, the additional therapeutic agent is a chemotherapy agent, such as a platinum complex, a taxane, pemetrexed, gemcitabine, fluorouracil, irinotecan, etanercept, or doxorubicin.

本公開還提供一種檢測或測定人CCR8的方法,所述方法包括使用如前任一項所述抗人CCR8抗體或抗體偶聯物檢測或測定人CCR8的步驟。The present disclosure also provides a method for detecting or measuring human CCR8, which comprises the step of detecting or measuring human CCR8 using the anti-human CCR8 antibody or antibody conjugate as described in any of the preceding items.

本公開還提供一種試劑盒,其包含如前任一項所述的抗人CCR8抗體或抗體偶聯物;在一些實施方案中,所述試劑盒用於檢測或測定人CCR8。The present disclosure also provides a kit comprising the anti-human CCR8 antibody or antibody conjugate as described in any of the preceding items; in some embodiments, the kit is used to detect or measure human CCR8.

本公開還提供了一種製備如前任一項所述的抗人CCR8抗體的方法,其包括培養如前任一項所述的細胞,然後分離和純化獲得抗人CCR8抗體的步驟。The present disclosure also provides a method for preparing the anti-human CCR8 antibody as described in any of the preceding items, which comprises the steps of culturing the cells as described in any of the preceding items, and then isolating and purifying the anti-human CCR8 antibody.

本公開公開的抗人CCR8抗體能夠特異性結合人CCR8;在一些實施方案中,所述抗體在體外和體內均具有顯著的抗腫瘤作用;在一些實施方案中,還具有很好的ADCC活性。The anti-human CCR8 antibody disclosed in the present disclosure can specifically bind to human CCR8; in some embodiments, the antibody has significant anti-tumor effects both in vitro and in vivo; in some embodiments, it also has good ADCC activity.

為使本公開實施例的目的、技術方案和優點更加清楚,下面對本公開實施例中的技術方案進行清楚、完整地描述,但是描述和實施例不應被解釋為限制本公開的範圍。實施例中未注明具體條件者,按照常規條件或製造商建議的條件進行。所用試劑或儀器未注明生產廠商者,均為可以通過市售購買獲得的常規產品。除非另外定義,本文所用的全部技術術語和科學術語具有與本公開所屬領域的普通技術人員通常所理解的相同含義。In order to make the purpose, technical scheme and advantages of the disclosed embodiments clearer, the technical scheme in the disclosed embodiments is described clearly and completely below, but the description and embodiments should not be interpreted as limiting the scope of the disclosure. If no specific conditions are specified in the embodiments, the conventional conditions or the conditions recommended by the manufacturer are followed. If the manufacturer of the reagents or instruments used is not specified, they are all conventional products that can be purchased commercially. Unless otherwise defined, all technical terms and scientific terms used herein have the same meanings as those commonly understood by ordinary technicians in the field to which the disclosure belongs.

本公開中,所用的單數形式「一個」、「一種」和「所述」包括複數指代,除非上下文清楚表明並非如此。另外,術語「第一」、「第二」僅用於描述目的,而不能理解為指示或暗示相對重要性或者隱含指明所指示的技術特徵的數量。術語「多個」的含義是至少兩個,例如2個、3個等,除非另有明確具體的限定。In this disclosure, the singular forms "a", "an", and "the" include plural references unless the context clearly indicates otherwise. In addition, the terms "first", "second", and "first" are used for descriptive purposes only and should not be understood as indicating or implying relative importance or implicitly indicating the quantity of the indicated technical features. The term "plurality" means at least two, such as 2, 3, etc., unless otherwise clearly and specifically limited.

本公開所用氨基酸三字母代碼和單字母代碼如J. biol. chem,243,p3558(1968)中所述。The three-letter and one-letter codes for amino acids used in this disclosure are as described in J. biol. chem, 243, p3558 (1968).

術語「氨基酸」是指天然存在的氨基酸和合成的氨基酸,以及以與天然存在的氨基酸類似的方式起作用的氨基酸類似物或氨基酸模擬物。天然存在的氨基酸是由遺傳密碼編碼的那些氨基酸,以及後來修飾的那些氨基酸,例如羥脯氨酸、γ-羧基谷氨酸和O-磷酸絲氨酸;常見的天然氨基酸包括丙氨酸(Ala;A)、精氨酸(Arg;R)、天冬醯胺(Asn;N)、天冬氨酸(Asp;D)、半胱氨酸(Cys;C);谷氨酸(Glu;E)、穀氨醯胺(Gln;Q)、甘氨酸(Gly;G);組氨酸(His;H)、異亮氨酸(Ile;I)、亮氨酸(Leu;L)、賴氨酸(Lys;K)、甲硫氨酸(Met;M)、苯丙氨酸(Phe;F)、脯氨酸(Pro;P)、絲胺酸(Ser;S)、蘇氨酸(Thr;T)、色氨酸(Trp;W)、酪氨酸(Tyr;Y)和纈氨酸(Val;V)。氨基酸類似物是指與天然存在的氨基酸具有相同基本化學結構(即與氫、羧基、氨基和R基團結合的α碳)的化合物,例如高絲氨酸、正亮氨酸、甲硫氨酸亞碸、甲硫氨酸甲基鋶。此類類似物具有修飾的R基團(例如,正亮氨酸)或修飾的肽骨架,但保留與天然存在的氨基酸相同的基本化學結構。氨基酸模擬物是指具有與氨基酸的一般化學結構不同的結構,但是以與天然存在的氨基酸類似的方式起作用的化學化合物。The term "amino acid" refers to naturally occurring amino acids and synthetic amino acids, as well as amino acid analogs or amino acid mimetics that function in a manner similar to the naturally occurring amino acids. Naturally occurring amino acids are those encoded by the genetic code, as well as those that are later modified, such as hydroxyproline, γ-carboxyglutamate, and O-phosphoserine; common natural amino acids include alanine (Ala; A), arginine (Arg; R), asparagine (Asn; N), aspartic acid (Asp; D), cysteine (Cys; C); glutamate (Glu; E), glutamine (Gln; Q), glycine (Gly; G); histidine (His; H), isoleucine (Ile; I), leucine (Leu; L), lysine (Lys; K), methionine (Met; M), phenylalanine (Phe; F), proline (Pro; P), serine (Ser; S), threonine (Thr; T), tryptophan (Trp; W), tyrosine (Tyr; Y), and valine (Val; V). Amino acid analogs are compounds that have the same basic chemical structure (i.e., alpha carbon bound to hydrogen, carboxyl, amino, and R groups) as naturally occurring amino acids, such as homoserine, norleucine, methionine sulfonate, and methionine methyl sulfonate. Such analogs have modified R groups (e.g., norleucine) or modified peptide backbones, but retain the same basic chemical structure as naturally occurring amino acids. Amino acid mimetics are chemical compounds that have a structure that is different from the general chemical structure of an amino acid, but function in a manner similar to a naturally occurring amino acid.

在本公開中,術語「抗體」在最廣義上使用,該術語涵蓋各種抗體結構,包括但不限於單克隆抗體、多克隆抗體、多特異性抗體(例如雙特異性抗體、三特異性抗體、四特異性抗體等)、鼠源抗體、嵌合抗體、人源化抗體、全長抗體或其抗原結合片段(或稱抗原結合部分),只要它們展示出所期望的抗原結合活性。In the present disclosure, the term "antibody" is used in the broadest sense, and the term covers various antibody structures, including but not limited to monoclonal antibodies, polyclonal antibodies, multispecific antibodies (e.g., bispecific antibodies, trispecific antibodies, tetraspecific antibodies, etc.), murine antibodies, chimeric antibodies, humanized antibodies, full-length antibodies or antigen-binding fragments thereof (or antigen-binding portions), as long as they exhibit the desired antigen-binding activity.

「天然抗體」指天然存在的免疫球蛋白分子。例如,天然IgG抗體是約150,000道爾頓的異四聚糖蛋白,由兩條相同輕鏈和兩條相同重鏈構成。從N至C端,每條重鏈具有一個重鏈可變區(VH,又稱作可變重域),接著是重鏈恒定區,天然IgG重鏈恒定區通常包括三個恒定域(CH1、CH2和CH3)。類似地,從N至C端,每條輕鏈具有一個輕鏈可變區(VL,又稱作可變輕域),接著是一個輕鏈恒定區(CL,也稱輕鏈恒定域)。"Native antibodies" refer to naturally occurring immunoglobulin molecules. For example, natural IgG antibodies are heterotetrameric glycoproteins of approximately 150,000 daltons, composed of two identical light chains and two identical heavy chains. From N to C terminus, each heavy chain has a heavy chain variable region (VH, also called a variable heavy domain), followed by a heavy chain constant region, and the natural IgG heavy chain constant region usually includes three constant domains (CH1, CH2, and CH3). Similarly, from N to C terminus, each light chain has a light chain variable region (VL, also called a variable light domain), followed by a light chain constant region (CL, also called a light chain constant domain).

術語「全長抗體」或「完整抗體」指包含與天然抗體結構基本類似的結構的抗體,或重鏈包含Fc區的抗體。The term "full-length antibody" or "intact antibody" refers to an antibody that comprises a structure substantially similar to a native antibody structure, or an antibody whose rechain comprises an Fc region.

術語抗體「可變區」或「可變域」指抗體重鏈或輕鏈中涉及抗體結合抗原的域。本文中,抗體重鏈可變區(VH)和輕鏈可變區(VL)各包含四個保守的框架區(FR)和三個互補決定區(CDR)。術語「互補決定區」或「CDR」指可變區內主要促成與抗原特異性結合的區域;「框架」或「FR」是指可變區中除CDR殘基之外的可變結構域殘基。VH包含3個CDR區:HCDR1(重鏈互補決定區1)、HCDR2(重鏈互補決定區2)和HCDR3(重鏈互補決定區3);VL包含3個CDR區:LCDR1(輕鏈互補決定區1)、LCDR2(輕鏈互補決定區2)和LCDR3(輕鏈互補決定區3)。每個VH和VL由從氨基末端(也稱N末端)排到羧基末端(也稱C末端)按以下順序排列的3個CDR和4個FR構成:FR1-CDR1-FR2-CDR2-FR3-CDR3-FR4。在本公開具體實施方式中,CDRs是指所述抗體的重鏈和輕鏈中2個以上CDR。可以通過各種公知方案來確定CDR的氨基酸序列邊界,例如:「Kabat」編號規則(參見Kabat等(1991),「Sequences of Proteins of Immunological Interest」,第5版,Public Health Service,National Institutes of Health,Bethesda,MD)、「Chothia」編號規則、「ABM」編號規則、「contact」編號規則(參見Martin, ACR. Protein Sequence and Structure Analysis of Antibody Variable Domains[J]. 2001)和ImMunoGenTics(IMGT)編號規則(Lefranc, M.P.等,Dev. Comp. Immunol., 27,55-77(2003))等;各種編號系統之間的對應關係是本領域技術人員熟知的。The term antibody "variable region" or "variable domain" refers to the domain of the antibody heavy chain or light chain involved in the antibody binding to the antigen. Herein, the antibody heavy chain variable region (VH) and light chain variable region (VL) each contain four conserved framework regions (FR) and three complementary determining regions (CDR). The term "complementary determining region" or "CDR" refers to the region in the variable region that mainly contributes to the specific binding to the antigen; "framework" or "FR" refers to the variable domain residues in the variable region excluding the CDR residues. VH contains 3 CDR regions: HCDR1 (heavy chain complementation determining region 1), HCDR2 (heavy chain complementation determining region 2) and HCDR3 (heavy chain complementation determining region 3); VL contains 3 CDR regions: LCDR1 (light chain complementation determining region 1), LCDR2 (light chain complementation determining region 2) and LCDR3 (light chain complementation determining region 3). Each VH and VL is composed of 3 CDRs and 4 FRs arranged in the following order from the amino terminus (also called the N terminus) to the carboxyl terminus (also called the C terminus): FR1-CDR1-FR2-CDR2-FR3-CDR3-FR4. In the specific embodiments of the present disclosure, CDRs refer to more than 2 CDRs in the heavy chain and light chain of the antibody. The amino acid sequence boundaries of CDRs can be determined by various well-known schemes, for example: the "Kabat" numbering rule (see Kabat et al. (1991), "Sequences of Proteins of Immunological Interest", 5th edition, Public Health Service, National Institutes of Health, Bethesda, MD), the "Chothia" numbering rule, the "ABM" numbering rule, the "contact" numbering rule (see Martin, ACR. Protein Sequence and Structure Analysis of Antibody Variable Domains [J]. 2001) and the ImMunoGenTics (IMGT) numbering rule (Lefranc, M.P. et al., Dev. Comp. Immunol., 27, 55-77 (2003)), etc.; the correspondence between various numbering systems is well known to those skilled in the art.

在一些實施方案中,本公開抗人CCR8抗體,其包含重鏈可變區和輕鏈可變區, 所述重鏈可變區包括SEQ ID No.1、3、5、7、9或11中的HCDR1、HCDR2和HCDR3,和/或所述抗體的輕鏈可變區包括SEQ ID No.2、4、6、8、10或12中的LCDR1、LCDR2和LCDR3。In some embodiments, the present invention discloses an anti-human CCR8 antibody, which comprises a heavy chain variable region and a light chain variable region, wherein the heavy chain variable region includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.1, 3, 5, 7, 9 or 11, and/or the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.2, 4, 6, 8, 10 or 12.

在一些實施方案中,本公開抗人CCR8抗體,其包含重鏈可變區和輕鏈可變區, 所述重鏈可變區包括SEQ ID No.1、3、5、7、9或11中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.2、4、6、8、10或12中的LCDR1、LCDR2和LCDR3。In some embodiments, the present invention discloses an anti-human CCR8 antibody, which comprises a heavy chain variable region and a light chain variable region, wherein the heavy chain variable region includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.1, 3, 5, 7, 9 or 11, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.2, 4, 6, 8, 10 or 12.

在一些實施方案中,本公開抗人CCR8抗體,其中, A.所述抗體的重鏈可變區包括SEQ ID No.1中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.2中的LCDR1、LCDR2和LCDR3; B.所述抗體的重鏈可變區包括SEQ ID No.3中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.4中的LCDR1、LCDR2和LCDR3; C.所述抗體的重鏈可變區包括SEQ ID No.5中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.6中的LCDR1、LCDR2和LCDR3; D.所述抗體的重鏈可變區包括SEQ ID No.7中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.8中的LCDR1、LCDR2和LCDR3; E.所述抗體的重鏈可變區包括SEQ ID No.9中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.10中的LCDR1、LCDR2和LCDR3; 或者F.所述抗體的重鏈可變區包括SEQ ID No.11中的HCDR1、HCDR2和HCDR3,並且所述抗體的輕鏈可變區包括SEQ ID No.12中的LCDR1、LCDR2和LCDR3。 In some embodiments, the present disclosure discloses an anti-human CCR8 antibody, wherein: A. the heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.1, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.2; B. the heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.3, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.4; C. the heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.5, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.6; D. the heavy chain variable region of the antibody includes SEQ ID No.7, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.8; E. The heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.9, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.10; or F. The heavy chain variable region of the antibody includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.11, and the light chain variable region of the antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.12.

在一些實施方案中,前述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3由IMGT編號系統定義,或由Kabat編號系統定義,或由Chothia 編號系統定義,或由Contact編號系統定義,或由AbM編號系統定義。In some embodiments, the aforementioned HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined by the IMGT numbering system, or by the Kabat numbering system, or by the Chothia numbering system, or by the Contact numbering system, or by the AbM numbering system.

在一些實施方案中,本公開抗人CCR8抗體,所述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3根據 Kabat編號系統定義。In some embodiments, the anti-human CCR8 antibodies disclosed herein, the HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined according to the Kabat numbering system.

在一些實施方案中,本公開抗人CCR8抗體,所述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3根據 IMGT編號系統定義。In some embodiments, the present disclosure discloses an anti-human CCR8 antibody, wherein the HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined according to the IMGT numbering system.

在一些實施方案中,本公開所述的抗人CCR8抗體,其中, a.重鏈可變區的HCDR1包含SEQ ID NO.13的氨基酸序列,HCDR2包含SEQ ID NO.14的氨基酸序列,和HCDR3包含SEQ ID NO.15的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.17的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列; b. 重鏈可變區的HCDR1包含SEQ ID NO.19的氨基酸序列,HCDR2包含SEQ ID NO.20的氨基酸序列,和HCDR3包含SEQ ID NO.21的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.17的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列; c. 重鏈可變區的HCDR1包含SEQ ID NO.22的氨基酸序列,HCDR2包含SEQ ID NO.23的氨基酸序列,和HCDR3包含SEQ ID NO.24的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.25的氨基酸序列,LCDR2包含SEQ ID NO.26的氨基酸序列,和LCDR3包含SEQ ID NO.27的氨基酸序列; d.重鏈可變區的HCDR1包含SEQ ID NO.13的氨基酸序列,HCDR2包含SEQ ID NO.28的氨基酸序列,和HCDR3包含SEQ ID NO.29的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.30的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列; e.重鏈可變區的HCDR1包含SEQ ID NO.31的氨基酸序列,HCDR2包含SEQ ID NO.32的氨基酸序列,和HCDR3包含SEQ ID NO.33的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.34的氨基酸序列,LCDR2包含SEQ ID NO.35的氨基酸序列,和LCDR3包含SEQ ID NO.36的氨基酸序列; 或f.重鏈可變區的HCDR1包含SEQ ID NO.13的氨基酸序列,HCDR2包含SEQ ID NO.37的氨基酸序列,和HCDR3包含SEQ ID NO.38的氨基酸序列;並且所述輕鏈可變區的LCDR1包含SEQ ID NO.16的氨基酸序列,LCDR2包含SEQ ID NO.17的氨基酸序列,和LCDR3包含SEQ ID NO.18的氨基酸序列。 In some embodiments, the anti-human CCR8 antibody disclosed herein, wherein: a. HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, HCDR2 comprises the amino acid sequence of SEQ ID NO.14, and HCDR3 comprises the amino acid sequence of SEQ ID NO.15; and LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18; b. HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.19, HCDR2 comprises the amino acid sequence of SEQ ID NO.20, and HCDR3 comprises the amino acid sequence of SEQ ID NO.21; and LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18; c. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.22, HCDR2 comprises the amino acid sequence of SEQ ID NO.23, and HCDR3 comprises the amino acid sequence of SEQ ID NO.24; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.25, LCDR2 comprises the amino acid sequence of SEQ ID NO.26, and LCDR3 comprises the amino acid sequence of SEQ ID NO.27; d. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, HCDR2 comprises the amino acid sequence of SEQ ID NO.28, and HCDR3 comprises the amino acid sequence of SEQ ID NO.29; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.30, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18; e. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.31, HCDR2 comprises the amino acid sequence of SEQ ID NO.32, and HCDR3 comprises the amino acid sequence of SEQ ID NO.33; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.34, LCDR2 comprises the amino acid sequence of SEQ ID NO.35, and LCDR3 comprises the amino acid sequence of SEQ ID NO.36; or f. the HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, HCDR2 comprises the amino acid sequence of SEQ ID NO.37, and HCDR3 comprises the amino acid sequence of SEQ ID NO.38; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and LCDR3 comprises the amino acid sequence of SEQ ID NO.18.

在一些實施方案中,本公開所述的抗人CCR8抗體,其包含分別如SEQ ID NO.13、SEQ ID NO.14和SEQ ID NO.15所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.16、SEQ ID NO.17和SEQ ID NO.18所示的LCDR1、LCDR2和LCDR3;或者所述抗人CCR8抗體包含分別如SEQ ID NO.19、SEQ ID NO.20和SEQ ID NO.21所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.16、SEQ ID NO.17和SEQ ID NO.18所示的LCDR1、LCDR2和LCDR3;或者所述抗人CCR8抗體包含分別如SEQ ID NO.22、SEQ ID NO.23和SEQ ID NO.24所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.25、SEQ ID NO.26和SEQ ID NO.27所示的LCDR1、LCDR2和LCDR3;或者所述抗人CCR8抗體包含分別如SEQ ID NO.13、SEQ ID NO.28和SEQ ID NO.29所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.16、SEQ ID NO.30和SEQ ID NO.18所示的LCDR1、LCDR2和LCDR3;或者所述抗人CCR8抗體包含分別如SEQ ID NO.30、SEQ ID NO.31和SEQ ID NO.32所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.33、SEQ ID NO.34和SEQ ID NO.35所示的LCDR1、LCDR2和LCDR3;或者所述抗人CCR8抗體包含分別如SEQ ID NO.13、SEQ ID NO.36和SEQ ID NO.37所示的HCDR1、HCDR2和HCDR3,以及分別如SEQ ID NO.16、SEQ ID NO.17和SEQ ID NO.18所示的LCDR1、LCDR2和LCDR3。In some embodiments, the anti-human CCR8 antibody described in the present disclosure comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.13, SEQ ID NO.14 and SEQ ID NO.15, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.17 and SEQ ID NO.18, respectively; or the anti-human CCR8 antibody comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.19, SEQ ID NO.20 and SEQ ID NO.21, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.17 and SEQ ID NO.18, respectively; or the anti-human CCR8 antibody comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.22, SEQ ID NO.23 and SEQ ID NO.24, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.25, SEQ ID NO.26 and SEQ ID NO. NO.27; or the anti-human CCR8 antibody comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.13, SEQ ID NO.28 and SEQ ID NO.29, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.30 and SEQ ID NO.18, respectively; or the anti-human CCR8 antibody comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.30, SEQ ID NO.31 and SEQ ID NO.32, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.33, SEQ ID NO.34 and SEQ ID NO.35, respectively; or the anti-human CCR8 antibody comprises HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.13, SEQ ID NO.36 and SEQ ID NO.37, respectively, and LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.31 and SEQ ID NO.32, respectively. LCDR1, LCDR2 and LCDR3 shown in NO.17 and SEQ ID NO.18.

術語「抗原結合片段」或「抗原結合域」指不同於完整抗體的分子,其包含完整抗體的部分,所述部分能夠與完整抗體所結合的抗原特異性結合。抗原結合片段的實例包括但不限於Fv(由VH和VL組成)、Fab(由一條輕鏈和一條重鏈的恒定區1(CH1)及重鏈可變區組成)、Fab'( 由Fab區和鉸鏈區組成)、Fab'-SH(Fab'片段的鉸鏈區的半胱氨酸殘基攜帶游離硫醇基團)、(Fab')2(二聚化Fab')、scFv(單鏈抗體分子,由輕鏈可變區與重鏈可變區直接相連或通過連接子連接)、scFab(單鏈Fab)、dsFv(二硫鍵穩定化的Fv片段)、(dsFv)2(二聚化dsFv),以及由抗體片段形成的多特異性抗體。The term "antigen-binding fragment" or "antigen-binding domain" refers to a molecule other than an intact antibody that comprises a portion of an intact antibody that is capable of specifically binding to the antigen to which the intact antibody binds. Examples of antigen-binding fragments include, but are not limited to, Fv (composed of VH and VL), Fab (composed of one light chain and one heavy chain constant region 1 (CH1) and a heavy chain variable region), Fab' (composed of a Fab region and a hinge region), Fab'-SH (the cysteine residue in the hinge region of the Fab' fragment carries a free thiol group), (Fab')2 (dimeric Fab'), scFv (single-chain antibody molecule, in which a light chain variable region is directly linked to a heavy chain variable region or is linked via a linker), scFab (single-chain Fab), dsFv (disulfide-stabilized Fv fragment), (dsFv)2 (dimeric dsFv), and multispecific antibodies formed from antibody fragments.

術語「Fc區」用於定義抗體重鏈的C末端區域,包括天然Fc區和改造的Fc區。在一些實施方式中,用於本文所述抗體的Fc區包括人IgG1、IgG2(IgG2a、IgG2b)、IgG3和IgG4的Fc區。在一些實施方式中,Fc區為包含DLE突變的人IgG1(也即人IgG1的Fc進行S239D/A330L/I332E突變,序列如SEQ ID No.42所示)。在一些實施方式中,Fc區為包含DE突變的人IgG1(也即人IgG1的Fc進行S239D/ I332E突變)。在一些實施方式中,Fc區的邊界還可以變化,例如缺失Fc區的C末端賴氨酸(根據EU編號系統的殘基447)或缺失Fc區的C末端甘氨酸和賴氨酸(根據EU編號系統的殘基446和447)。除非另有說明,Fc區的編號規則為EU編號系統,又稱作EU索引。The term "Fc region" is used to define the C-terminal region of the antibody rechain, including native Fc regions and modified Fc regions. In some embodiments, the Fc region used in the antibodies described herein includes the Fc region of human IgG1, IgG2 (IgG2a, IgG2b), IgG3 and IgG4. In some embodiments, the Fc region is a human IgG1 comprising a DLE mutation (i.e., the Fc of human IgG1 undergoes S239D/A330L/I332E mutations, and the sequence is shown in SEQ ID No. 42). In some embodiments, the Fc region is a human IgG1 comprising a DE mutation (i.e., the Fc of human IgG1 undergoes S239D/I332E mutations). In some embodiments, the boundaries of the Fc region may also be altered, such as by deleting the C-terminal lysine of the Fc region (residue 447 according to the EU numbering system) or deleting the C-terminal glycine and lysine of the Fc region (residues 446 and 447 according to the EU numbering system). Unless otherwise indicated, the numbering convention for the Fc region is the EU numbering system, also known as the EU index.

術語「嵌合」抗體指抗體中的重鏈和/或輕鏈的一部分源自一種物種,而重鏈和/或輕鏈的其它部分源自另外一種物種。The term "chimeric" antibody refers to an antibody in which a portion of the heavy chain and/or light chain is derived from one species, while the other portion of the heavy chain and/or light chain is derived from another species.

術語「人源化」抗體是保留非人抗體的反應性,同時在人中具有較低免疫原性的抗體。例如,可以通過保留非人CDR區,其餘部分用人源抗體對應物(即,恒定區以及可變區的框架區部分)替換來實現。The term "humanized" antibody is an antibody that retains the reactivity of a non-human antibody while having reduced immunogenicity in humans. For example, this can be achieved by retaining the non-human CDR regions and replacing the rest with human antibody counterparts (i.e., the constant region and the framework region portion of the variable region).

術語「人抗體」、「人源抗體」、「全人抗體」、「完全人抗體」可以互換使用,意指可變區及恒定區是人序列的抗體。The terms "human antibody", "humanized antibody", "fully human antibody" and "completely human antibody" are used interchangeably to refer to antibodies whose variable and constant regions are human sequences.

術語「親和力」是指分子(例如,抗體)的單個結合部位與其結合配體(例如,抗原)之間非共價相互作用的總體的強度。除非另外指明,如本文所用,結合「親和力」是指內部結合親和力,其反映出結合對(例如,抗體與抗原)的成員之間1:1相互作用。分子X對其配體Y的親和力通常可以由解離常數(KD)表示。親和力可以通過本領域已知的常規方法測量。術語「kassoc」或「ka」指特定抗體-抗原相互作用的締合速率,術語「kdis」或「kd」指特定抗體-抗原相互作用的解離速率。術語「KD」指解離常數,其獲得自kd與ka的比率(即kd/ka)並且表示為摩爾濃度(M)。可以使用本領域公知的方法測定抗體的KD值。例如,使用生物傳感系統例如系統測量表面等離子體共振(例如Biacore),或通過溶液平衡滴定法(SET)測量溶液中的親和力。The term "affinity" refers to the overall strength of non-covalent interactions between a single binding site of a molecule (e.g., an antibody) and its binding ligand (e.g., an antigen). Unless otherwise indicated, as used herein, binding "affinity" refers to internal binding affinity, which reflects a 1:1 interaction between members of a binding pair (e.g., an antibody and an antigen). The affinity of a molecule X to its ligand Y can generally be represented by a dissociation constant (KD). Affinity can be measured by conventional methods known in the art. The term "kassoc" or "ka" refers to the association rate of a specific antibody-antigen interaction, and the term "kdis" or "kd" refers to the dissociation rate of a specific antibody-antigen interaction. The term "KD" refers to a dissociation constant, which is obtained from the ratio of kd to ka (i.e., kd/ka) and is expressed as molar concentration (M). The KD value of an antibody can be determined using methods known in the art, for example, using a biosensor system such as a system measuring surface plasmon resonance (e.g., Biacore), or by measuring affinity in solution by solution equilibrium titration (SET).

術語「效應子功能」指那些可歸於抗體Fc區(天然序列Fc區或氨基酸序列突變的Fc區)的生物學活性。抗體效應子功能的例子包括但不限於:C1q結合和補體依賴性細胞毒性、Fc受體結合、抗體依賴性細胞介導的細胞毒性(ADCC)、吞噬作用、細胞表面受體(例如B細胞受體)下調;和B細胞活化。The term "effector function" refers to those biological activities attributable to an antibody Fc region (either a native sequence Fc region or an Fc region with amino acid sequence mutations). Examples of antibody effector functions include, but are not limited to: C1q binding and complement-dependent cytotoxicity, Fc receptor binding, antibody-dependent cell-mediated cytotoxicity (ADCC), phagocytosis, downregulation of cell surface receptors (e.g., B cell receptors); and B cell activation.

術語「單克隆抗體」指基本上均質的抗體的群,即在該群中包含的抗體分子的氨基酸序列是相同的,除了可能少量存在的天然突變以外。相比之下,多克隆抗體製劑通常包含在其可變結構域具有不同氨基酸序列的多種不同抗體,其通常特異性針對不同表位。「單克隆」表示從基本上均質的抗體群體獲得的抗體的特徵,並且不應解釋為要求通過任何特定方法來生產抗體。在一些實施方式中,本公開提供的抗體是單克隆抗體。The term "monoclonal antibody" refers to a population of substantially homogeneous antibodies, i.e., the amino acid sequences of the antibody molecules contained in the population are identical, except for possible natural mutations that may be present in small amounts. In contrast, a polyclonal antibody preparation typically contains a plurality of different antibodies having different amino acid sequences in their variable domains, which are typically specific for different epitopes. "Monoclonal" refers to the characteristic of an antibody obtained from a substantially homogeneous population of antibodies, and should not be interpreted as requiring the production of an antibody by any particular method. In some embodiments, the antibodies provided by the present disclosure are monoclonal antibodies.

術語「抗原」是指能夠由抗原結合蛋白(例如抗體)選擇性結合劑結合的分子。抗原可具有一個或多個能夠與不同的抗原結合蛋白(例如抗體)相互作用的表位。The term "antigen" refers to a molecule that can be selectively bound by an antigen binding protein (e.g., an antibody). An antigen may have one or more epitopes that can interact with different antigen binding proteins (e.g., antibodies).

術語「表位」指能夠與抗體特異性結合的抗原上的區域(area或region)。表位可以由連續氨基酸串(線性表位)形成或包含非連續氨基酸(構象表位),例如因抗原的折疊(即通過蛋白質性質的抗原的三級折疊)而變成空間接近。構象表位和線性表位的差別在於:在變性溶劑的存在下,抗體對構象表位的結合喪失。構象表位包含處於獨特空間構象的至少3,至少4,至少5,至少6,至少7,或8-10個氨基酸。篩選結合特定表位的抗體(即那些結合相同表位的)可以使用本領域例行方法來進行,例如丙氨酸掃描,肽印跡,肽切割分析,表位切除,表位提取,抗原的化學修飾(見Prot. Sci. 9(2000)487-496),和交叉阻斷。The term "epitope" refers to an area or region on an antigen that is capable of specific binding to an antibody. An epitope may be formed by a string of consecutive amino acids (linear epitope) or comprise non-consecutive amino acids (conformational epitope), for example brought into spatial proximity by folding of the antigen (i.e., by tertiary folding of proteinaceous antigens). Conformational epitopes differ from linear epitopes in that antibody binding to a conformational epitope is lost in the presence of a denaturing solvent. A conformational epitope comprises at least 3, at least 4, at least 5, at least 6, at least 7, or 8-10 amino acids in a unique spatial conformation. Screening for antibodies that bind to a specific epitope (i.e., those that bind to the same epitope) can be performed using routine methods in the art, such as alanine scanning, peptide blotting, peptide cleavage analysis, epitope excision, epitope extraction, chemical modification of the antigen (see Prot. Sci. 9 (2000) 487-496), and cross-blocking.

與參照抗體結合相同表位的抗體或與參照抗體競爭結合的抗體意指在競爭測定法中,將參照抗體對其抗原的結合阻斷50%或更多的抗體,或其對抗原的結合被參照抗體阻斷50%或更多的抗體。例如,為了測定待測抗體是否與參照抗體結合相同表位,在飽和條件下容許參照抗體結合抗原,然後在去除過量的參照抗體後,評估待測抗體結合抗原的能力;如果該待測抗體能夠在參照抗體的飽和結合之後結合抗原,那麼可以得出結論,該待測抗體與參照抗體結合不同表位;而如果該待測抗體在參照抗體的飽和結合之後不能夠結合抗原,那麼該待測抗體可結合與參照抗體結合相同的表位。為了確認待測抗體是否結合相同表位,可以使用常規實驗(例如,肽突變和使用ELISA、RIA、表面等離子共振、流式細胞術或本領域可獲得的任何其它定量或定性抗體結合測定的結合分析)檢測。在一些實施方案中,如在競爭性結合測定中所測量的(參見例如,Junghans等,Cancer Res.50 (1990) 1495-1502),如果一個過量(例如1倍、5倍、10倍、20倍或100倍的量)的抗體將另一個抗體與抗原的結合抑制至少50%、至少75%、至少90%或甚至99%或更多,則認為兩個抗體結合相同或重疊的表位。An antibody that binds to the same epitope as a reference antibody or an antibody that competes for binding with a reference antibody means an antibody that blocks the binding of the reference antibody to its antigen by 50% or more in a competition assay, or an antibody whose binding to the antigen is blocked by the reference antibody by 50% or more. For example, to determine whether the test antibody binds to the same epitope as the reference antibody, the reference antibody is allowed to bind to the antigen under saturated conditions, and then after removing excess reference antibody, the ability of the test antibody to bind to the antigen is assessed; if the test antibody is able to bind to the antigen after saturated binding of the reference antibody, then it can be concluded that the test antibody binds to a different epitope than the reference antibody; and if the test antibody is unable to bind to the antigen after saturated binding of the reference antibody, then the test antibody can bind to the same epitope as the reference antibody. To confirm whether the test antibody binds to the same epitope, conventional experiments (e.g., peptide mutations and binding analysis using ELISA, RIA, surface plasmon resonance, flow cytometry, or any other quantitative or qualitative antibody binding assay available in the art) can be used. In some embodiments, two antibodies are considered to bind to the same or overlapping epitope if an excess (e.g., a 1-fold, 5-fold, 10-fold, 20-fold, or 100-fold amount) of one antibody inhibits binding of the other antibody to the antigen by at least 50%, at least 75%, at least 90%, or even 99% or more, as measured in a competitive binding assay (see, e.g., Junghans et al., Cancer Res. 50 (1990) 1495-1502).

術語「能夠特異性結合」、「特異性結合」或「結合」是指相比其他抗原或表位,抗體能夠以更高的親和力結合至某個抗原或該抗原內的表位。通常地,抗體以約100nM或更小(例如約10nM、1nM、0.1nM、0.01nM或更小)的平衡解離常數(KD)結合抗原或抗原內的表位。在一些實施方式中,抗體與抗原結合的KD為該抗體結合至非特異性抗原(例如BSA、酪蛋白)的KD的10%或更低(例如1%)。可使用已知的方法來測量KD,包括但不限於Biacore測定法、Octet方法、微量熱泳法、HPLC‑MS方法和流式細胞螢光分選技術;例如通過BIACORE®表面等離子體共振測定法所測量的。The term "capable of specific binding", "specific binding" or "binding" means that the antibody is able to bind to an antigen or an epitope within the antigen with a higher affinity than other antigens or epitopes. Typically, the antibody binds to the antigen or an epitope within the antigen with an equilibrium dissociation constant (KD) of about 100 nM or less (e.g., about 10 nM, 1 nM, 0.1 nM, 0.01 nM or less). In some embodiments, the KD of the antibody binding to the antigen is 10% or less (e.g., 1%) of the KD of the antibody binding to a non-specific antigen (e.g., BSA, casein). KD can be measured using known methods, including but not limited to Biacore assays, Octet methods, microthermophoresis, HPLC-MS methods, and flow cytometry fluorescence sorting techniques; for example, as measured by BIACORE® surface plasmon resonance assays.

本公開提供的抗人CCR8抗體與人CCR8的結合也可以用「半最大有效濃度」(EC50)值表示,一般EC50越小親和力越好,表示更低的濃度下即可以與抗原結合。可以通過本領域已知的結合檢測法,例如直接或間接結合檢測法(例如酶聯免疫吸附檢測法(ELISA)、流式細胞螢光分選技術和其他結合檢測法)來測定EC50值。The binding of the anti-human CCR8 antibody provided in the present disclosure to human CCR8 can also be expressed by the "half-maximal effective concentration" (EC50) value. Generally, the smaller the EC50, the better the affinity, indicating that it can bind to the antigen at a lower concentration. The EC50 value can be determined by binding assays known in the art, such as direct or indirect binding assays (e.g., enzyme-linked immunosorbent assay (ELISA), flow cytometry and other binding assays).

術語「抗體依賴性細胞的細胞毒性」、「抗體依賴性細胞介導的細胞毒性」或「ADCC」是誘導細胞死亡的機制,該機制依賴于抗體包被靶細胞與具有裂解活性的效應細胞(諸如自然殺傷細胞(NK)、單核細胞、巨噬細胞和中性粒細胞)經由效應細胞上表現的Fcγ受體(FcγR)發生的相互作用。例如,NK細胞表現FcγRIIIa,而單核細胞表現FcγRI、FcγRII和FcγRIIIa。本文提供的抗體的ADCC活性可使用體外測定,使用表現抗原的細胞作為靶細胞和NK細胞作為效應細胞進行評定。根據從裂解的細胞中釋放的標記物(例如放射性底物、螢光染料或天然胞內蛋白)來檢測細胞裂解。The term "antibody-dependent cellular cytotoxicity", "antibody-dependent cell-mediated cytotoxicity" or "ADCC" is a mechanism of inducing cell death that relies on the interaction of antibody-coated target cells with lytic effector cells (such as natural killer (NK) cells, monocytes, macrophages and neutrophils) via Fcγ receptors (FcγRs) expressed on the effector cells. For example, NK cells express FcγRIIIa, while monocytes express FcγRI, FcγRII and FcγRIIIa. The ADCC activity of the antibodies provided herein can be assessed using an in vitro assay using cells expressing the antigen as target cells and NK cells as effector cells. Cell lysis is detected based on the release of a marker (e.g., a radioactive substrate, a fluorescent dye, or a native intracellular protein) from the lysed cells.

術語「抗體依賴性細胞吞噬作用」(ADCP)是指通過吞噬細胞(諸如巨噬細胞或樹突狀細胞)的內化作用消除抗體包被的靶細胞的機制。The term "antibody-dependent cellular phagocytosis" (ADCP) refers to the mechanism by which antibody-coated target cells are eliminated by internalization by phagocytic cells such as macrophages or dendritic cells.

術語「補體依賴性細胞毒性」或「CDC」是指誘導細胞死亡的機制,其中靶結合抗體的Fc效應域結合並激活補體成分C1q,C1q繼而激活補體級聯,從而導致靶細胞死亡。補體的激活也可導致補體成分沉積在靶細胞表面上,這些補體成分通過結合白細胞上的補體受體(例如,CR3)來促進CDC。The term "complement-dependent cytotoxicity" or "CDC" refers to a mechanism of cell death induction in which the Fc effector domain of a target-binding antibody binds and activates the complement component C1q, which in turn activates the complement cascade, leading to target cell death. Complement activation can also result in the deposition of complement components on the surface of target cells, which promote CDC by binding to complement receptors (e.g., CR3) on leukocytes.

本文中「CAR」為嵌合抗原受體,是人工改造受體,例如其是能夠將識別腫瘤細胞表面抗原或病毒抗原的特異性分子(如抗體)錨定在免疫細胞(如T細胞)上,使免疫細胞識別腫瘤抗原或病毒抗原並殺死腫瘤細胞或病毒的受體。表現CAR的T細胞稱為CAR-T(或CART)。通常,嵌合抗原受體依次包含胞外結構域、跨膜區域和胞內信號結構域。可採用本領域已知的用於構建CAR的跨膜區域和胞內信號結構域來構建本公開的嵌合抗原受體。腫瘤細胞表面的抗原(受體)與嵌合抗原受體的抗體(配體)結合時,通過鉸鏈區和跨膜區將信號傳遞至胞內,胞內信號域再將信號轉化為活化信號,激活效應細胞,效應細胞通過分泌穿孔素或者產生細胞因子殺傷腫瘤細胞,同時效應細胞本身也發生擴增,進一步擴大免疫殺傷作用。胞外結構域可包含抗原結合結構域(也稱特異性結合抗原的抗體部分),抗原結合結構域可以是特異性結合抗原的單鏈可變片段(single-chain variable fragment,scFv)。單鏈可變片段可作為CAR的胞外結構域,該結構域決定CAR-免疫細胞的特異性。鉸鏈區是連接單鏈抗體單位和跨膜結構域的CAR細胞外結構區,它通常維持效應細胞中穩健的CAR表現和活性所需的穩定性,大多數CAR的鉸鏈區由IgG的鉸鏈或CD8α/CD28胞外區衍變而來。鉸鏈區的類型和長度對CAR的功能活動有重要影響。跨膜結構域將CAR的細胞外結構域與細胞內信號轉導結構域連接。常用的跨膜結構域來源於CD4,CD8α,CD28和CD3ζ。跨膜結構域的選擇影響CAR結構在細胞功能上的活化程度。胞內結構域由共刺激結構域和信號轉導結構域構成。在可選的實施方式中,所述CAR為嵌合抗原受體,其主要成分還可以包括跨膜結構域和胞內結構域。在可選的實施方式中,所述CAR還可以包括共刺激分子。「共刺激分子」是指存在於抗原提呈細胞表面,能與Th細胞上的共刺激分子受體結合,產生協同刺激信號的分子。T淋巴細胞的增殖不僅需要抗原的結合,還需要接受共刺激分子信號。共刺激信號傳遞給T細胞主要是通過表現在抗原呈遞細胞表面的共刺激分子CD80、CD86與T細胞表面的CD28分子結合。B細胞接受共刺激信號可以通過一般的病原體成分例如LPS,或者通過補體成分,或者通過激活了的抗原特異性的Th細胞表面的CD40L。可採用本領域已知的用於構建CAR的共刺激分子,包括但不限於CD27、CD28、4-1BB、OX40、ICOS、B7-H3和/或它們的任何組合。"CAR" herein is a chimeric antigen receptor, which is an artificially modified receptor, for example, it is a receptor that can anchor specific molecules (such as antibodies) that recognize tumor cell surface antigens or viral antigens on immune cells (such as T cells), allowing immune cells to recognize tumor antigens or viral antigens and kill tumor cells or viruses. T cells expressing CAR are called CAR-T (or CART). Generally, chimeric antigen receptors contain an extracellular domain, a transmembrane region, and an intracellular signaling domain in sequence. The transmembrane region and intracellular signaling domain known in the art for constructing CAR can be used to construct the chimeric antigen receptor disclosed herein. When the antigen (receptor) on the surface of the tumor cell binds to the antibody (ligand) of the chimeric antigen receptor, the signal is transmitted to the cell through the hinge region and the transmembrane region. The intracellular signal domain then converts the signal into an activation signal to activate the effector cells. The effector cells kill the tumor cells by secreting perforins or producing cytokines. At the same time, the effector cells themselves also expand, further expanding the immune killing effect. The extracellular domain can contain an antigen binding domain (also called the antibody part that specifically binds to the antigen), and the antigen binding domain can be a single-chain variable fragment (scFv) that specifically binds to the antigen. The single-chain variable fragment can serve as the extracellular domain of CAR, which determines the specificity of CAR-immune cells. The hinge region is the extracellular domain of CAR that connects the single-chain antibody unit and the transmembrane domain. It usually maintains the stability required for robust CAR expression and activity in effector cells. The hinge region of most CARs is derived from the hinge of IgG or the extracellular region of CD8α/CD28. The type and length of the hinge region have an important influence on the functional activity of CAR. The transmembrane domain connects the extracellular domain of CAR to the intracellular signal transduction domain. Commonly used transmembrane domains are derived from CD4, CD8α, CD28 and CD3ζ. The choice of transmembrane domain affects the degree of activation of the CAR structure in cell function. The intracellular domain is composed of a co-stimulatory domain and a signal transduction domain. In an optional embodiment, the CAR is a chimeric antigen receptor, and its main components may also include a transmembrane domain and an intracellular domain. In an optional embodiment, the CAR may also include a co-stimulatory molecule. "Co-stimulatory molecules" refer to molecules that exist on the surface of antigen-presenting cells and can bind to co-stimulatory molecule receptors on Th cells to produce synergistic stimulation signals. The proliferation of T lymphocytes requires not only the binding of antigens, but also the acceptance of co-stimulatory molecule signals. The co-stimulatory signal is transmitted to T cells mainly through the binding of co-stimulatory molecules CD80 and CD86 expressed on the surface of antigen-presenting cells to CD28 molecules on the surface of T cells. B cells can receive costimulatory signals through general pathogen components such as LPS, or through complement components, or through CD40L on the surface of activated antigen-specific Th cells. Costimulatory molecules known in the art for constructing CARs can be used, including but not limited to CD27, CD28, 4-1BB, OX40, ICOS, B7-H3 and/or any combination thereof.

術語「CAR-免疫細胞」是指表現CAR的免疫細胞或CAR修飾的免疫細胞,其中,免疫細胞包括但不限於T細胞、自然殺傷(NK細胞)、巨噬細胞(M細胞)、Treg細胞。The term "CAR-immune cell" refers to an immune cell expressing CAR or a CAR-modified immune cell, wherein the immune cell includes but is not limited to T cells, natural killer (NK cells), macrophages (M cells), and Treg cells.

術語「核酸」在本文中可與術語「多核苷酸」互換使用,並且是指呈單鏈或雙鏈形式的脫氧核糖核苷酸或核糖核苷酸及其聚合物。所述術語涵蓋含有已知核苷酸類似物或修飾的骨架殘基或連接的核酸,所述核酸是合成的、天然存在的和非天然存在的,具有與參考核酸相似的結合特性,並且以類似於參考核苷酸的方式代謝。此類類似物的實例包括但不限於硫代磷酸酯、氨基磷酸酯、甲基膦酸酯、手性-甲基膦酸酯、2-O-甲基核糖核苷酸、肽-核酸(PNA)。「分離的」核酸指已經與其天然環境的組分分開的核酸分子。分離的核酸包括在下述細胞中含有的核酸分子,所述細胞通常含有該核酸分子,但該核酸分子存在於染色體外或存在於不同於其天然染色體位置的染色體位置處。編碼多肽或融合蛋白的分離的核酸指編碼多肽或融合蛋白的一個或更多個核酸分子,包括在單一載體或分開的載體中的這樣的一個或更多個核酸分子,和存在於宿主細胞中一個或更多個位置的這樣的一個或更多個核酸分子。除非另有說明,否則特定的核酸序列還隱含地涵蓋其保守修飾的變體(例如,簡並密碼子取代)和互補序列以及明確指明的序列。具體地,如下詳述,簡並密碼子取代可以通過產生如下序列而獲得,在這些序列中,一個或多個所選的(或全部)密碼子的第三位被混合堿基和/或脫氧肌苷殘基取代。The term "nucleic acid" is used interchangeably with the term "polynucleotide" herein and refers to deoxyribonucleotides or ribonucleotides and polymers thereof in single-stranded or double-stranded form. The term encompasses nucleic acids containing backbone residues or linkages of known nucleotide analogs or modifications, which are synthetic, naturally occurring, and non-naturally occurring, have similar binding properties as reference nucleic acids, and are metabolized in a manner similar to reference nucleotides. Examples of such analogs include, but are not limited to, phosphorothioates, phosphoramidates, methylphosphonates, chiral-methylphosphonates, 2-O-methyl ribonucleotides, peptide-nucleic acids (PNAs). An "isolated" nucleic acid refers to a nucleic acid molecule that has been separated from components of its natural environment. An isolated nucleic acid includes a nucleic acid molecule contained in a cell that normally contains the nucleic acid molecule, but the nucleic acid molecule is present extrachromosomally or at a chromosomal location that is different from its natural chromosomal location. An isolated nucleic acid encoding a polypeptide or fusion protein refers to one or more nucleic acid molecules encoding a polypeptide or fusion protein, including such one or more nucleic acid molecules in a single vector or separate vectors, and such one or more nucleic acid molecules present in one or more positions in a host cell. Unless otherwise specified, a specific nucleic acid sequence also implicitly encompasses conservatively modified variants thereof (e.g., degenerate codon substitutions) and complementary sequences as well as explicitly specified sequences. Specifically, as described in detail below, degenerate codon substitutions can be obtained by generating sequences in which the third position of one or more selected (or all) codons is substituted with mixed alkali and/or deoxyinosine residues.

術語「多肽」和「蛋白質」在本文中可互換使用,指氨基酸殘基的聚合物。該術語適用於氨基酸聚合物,其中一個或多個氨基酸殘基是相應天然存在的氨基酸的人工化學模擬物,以及適用于天然存在的氨基酸聚合物和非天然存在的氨基酸聚合物。The terms "polypeptide" and "protein" are used interchangeably herein to refer to a polymer of amino acid residues. The term applies to amino acid polymers in which one or more amino acid residues are artificial chemical mimics of the corresponding naturally occurring amino acids, as well as to naturally occurring amino acid polymers and non-naturally occurring amino acid polymers.

術語序列「同一性」指,當對兩條序列進行最佳比對時(必要時引入間隙,以獲取最大序列同一性百分比,且不將任何保守性取代視為序列同一性的一部分),兩條序列的氨基酸/核酸在等價位置相同的程度(百分比)。為測定序列同一性百分比,比對可以通過本領域技術已知的技術來實現,例如使用公開可得到的計算機軟件,諸如BLAST、BLAST-2、ALIGN、ALIGN-2或Megalign(DNASTAR)軟件。本領域技術人員可確定適用於測量比對的參數,包括在所比較的序列全長上達成最大比對所需的任何算法。The term sequence "identity" refers to the degree (percentage) to which the amino acids/nucleic acids of the two sequences are identical at equivalent positions when the two sequences are optimally aligned (introducing gaps, if necessary, to obtain the maximum sequence identity percentage, and not considering any conservative substitutions as part of the sequence identity). To determine the percentage of sequence identity, alignment can be achieved by techniques known to those skilled in the art, for example, using publicly available computer software such as BLAST, BLAST-2, ALIGN, ALIGN-2 or Megalign (DNASTAR) software. Those skilled in the art can determine the parameters suitable for measuring alignment, including any algorithm required to achieve maximum alignment over the entire length of the compared sequences.

本公開中,「抗體偶聯物」包括抗人CCR8抗體與治療劑或顯像劑偶聯而成的偶聯物。在可選的實施方式中,所述抗體偶聯物由抗人CCR8抗體與治療劑通過連接子偶聯而成;在可選的實施方式中,所述治療劑為細胞毒劑;在可選的實施方式中,所述治療劑可選自毒素、化療劑、抗生素、放射性同位素和核溶酶。In the present disclosure, "antibody conjugates" include conjugates formed by coupling anti-human CCR8 antibodies to therapeutic agents or imaging agents. In an optional embodiment, the antibody conjugate is formed by coupling anti-human CCR8 antibodies to therapeutic agents via a linker; in an optional embodiment, the therapeutic agent is a cytotoxic agent; in an optional embodiment, the therapeutic agent can be selected from toxins, chemotherapeutic agents, antibiotics, radioactive isotopes and nucleolytic enzymes.

本公開中,「細胞毒劑」是指抑制或防止細胞的功能和/或引起細胞死亡或破壞的物質;「毒素」指能夠對細胞的生長或增殖產生有害效果的物質(例如美登素類、卡利奇黴素、紫杉烷類、長春新堿、秋水仙堿、澳瑞他汀等)。「化療劑」指可用於治療癌症的化學化合物。In this disclosure, "cytotoxic agent" refers to a substance that inhibits or prevents the function of cells and/or causes cell death or destruction; "toxin" refers to a substance that can have a harmful effect on the growth or proliferation of cells (such as maytansine, calicheamicin, taxanes, vincristine, colchicine, auristatin, etc.). "Chemotherapeutic agent" refers to a chemical compound that can be used to treat cancer.

在可選的實施方式中,本公開所述抗體偶聯物還包括與所述抗體偶聯的生物素或生物素衍生物。In an alternative embodiment, the antibody conjugate disclosed herein further comprises biotin or a biotin derivative conjugated to the antibody.

在可選的實施方式中,所述抗體偶聯物還包括與所述抗體偶聯的標記物。In an alternative embodiment, the antibody conjugate further comprises a label conjugated to the antibody.

在可選的實施方式中,上述標記物是指具有能夠被肉眼直接觀察或被儀器檢測或探測到的特性例如發光、顯色、放射性等特性的一類物質,通過該特性可以實現對相應目標物的定性或定量檢測。In an optional embodiment, the above-mentioned marker refers to a type of substance having properties that can be directly observed by the naked eye or detected or detected by an instrument, such as luminescence, color development, radioactivity, etc., through which qualitative or quantitative detection of the corresponding target object can be achieved.

在可選的實施方式中,所述標記物選自螢光染料、酶、放射性同位素、化學發光試劑和納米顆粒類標記物中的至少一種。在實際的使用過程中,本領域技術人員可以根據檢測條件或實際需要選擇其它合適的標記物,無論使用何種標記物,均屬本公開的保護範圍。In an optional embodiment, the marker is selected from at least one of fluorescent dyes, enzymes, radioactive isotopes, chemiluminescent reagents and nanoparticle markers. In actual use, those skilled in the art can select other suitable markers according to detection conditions or actual needs. No matter what marker is used, it belongs to the protection scope of this disclosure.

在可選的實施方式中,所述螢光染料包括但不限於螢光素類染料及其衍生物(例如包括但不限於異硫氰酸螢光素(FITC)羥基光素(FAM)、四氯光素(TET)等或其類似物)、羅丹明類染料及其衍生物(例如包括但不限於紅色羅丹明(RBITC)、四甲基羅丹明(TAMRA)、羅丹明B(TRITC)等或其類似物)、Cy系列染料及其衍生物(例如包括但不限於Cy2、Cy3、Cy3B、Cy3.5、Cy5、Cy5.5、Cy3等或其類似物)、Alexa系列染料及其衍生物(例如包括但不限於AlexaFluor350、405、430、488、532、546、555、568、594、610、33、647、680、700、750等或其類似物)和蛋白類染料及其衍生物(例如包括但不限於藻紅蛋白(PE)、藻藍蛋白(PC)、別藻藍蛋白(APC)、多甲藻黃素-葉綠素蛋白(preCP)等)。In an optional embodiment, the fluorescent dye includes but is not limited to fluorescein dyes and their derivatives (for example, including but not limited to fluorescein isothiocyanate (FITC), hydroxyfluorescein (FAM), tetrachlorofluorescein (TET), etc. or their analogs), rhodamine dyes and their derivatives (for example, including but not limited to red rhodamine (RBITC), tetramethylrhodamine (TAMRA), rhodamine B (TRITC), etc. or their analogs), Cy series dyes and their derivatives (for example, including but not limited to Cy2, Cy3, Cy3B, Cy3.5, Cy3.7, Cy3.8, Cy3.9, Cy3.10, Cy3.11, Cy3.12, Cy3.13, Cy3.14, Cy3.15, Cy3.16, Cy3.17, Cy3.18, Cy3.19, Cy3.20, Cy3.21, Cy3.22, Cy3.23, Cy3.24, Cy3.25, Cy3.26, Cy3.27, Cy3.28, Cy3.29, Cy3.30, Cy3.31, Cy3.32, Cy3.33, Cy3.34, Cy3.35, Cy3.36, Cy3.37, Cy3.38, Cy3.39, Cy3.3A, Cy3.3A, Cy3.3A, Cy3.3B ... y5, Cy5.5, Cy3, etc. or their analogs), Alexa series dyes and their derivatives (for example, including but not limited to AlexaFluor350, 405, 430, 488, 532, 546, 555, 568, 594, 610, 33, 647, 680, 700, 750, etc. or their analogs) and protein dyes and their derivatives (for example, including but not limited to phycoerythrin (PE), phycocyanin (PC), allophycocyanin (APC), peridinin-chlorophyll protein (preCP), etc.).

在可選的實施方式中,所述酶包括但不限於辣根過氧化物酶、鹼性磷酸酶、β-半乳糖苷酶、葡萄糖氧化酶、碳酸酐酶、乙醯膽鹼酯酶以及6-磷酸葡萄糖脫氧酶。在可選的實施方式中,所述放射性同位素包括但不限於 212Bi、 131I、 111In、 90Y、 186Re、 211At、 125I、 188Re、 153Sm、 213Bi、 32P、 94mTc、 99mTc、 203Pb、 67Ga、 68Ga、 43Sc、 47Sc、 110mIn、 97Ru、 62Cu、 64Cu、 67Cu、 68Cu、 86Y、 88Y、 121Sn、 161Tb、 166Ho、 105Rh、 177Lu、 172Lu和 18F。 In an alternative embodiment, the enzyme includes but is not limited to horseradish peroxidase, alkaline phosphatase, β-galactosidase, glucose oxidase, carbonic anhydrase, acetylcholinesterase and 6-phosphoglucose deoxidase. In an alternative embodiment, the radioactive isotope includes but is not limited to 212 Bi, 13 1I, 111 In, 90 Y, 186 Re, 211 At, 125 I, 188 Re, 153 Sm, 213 Bi, 32 P, 94 mTc, 99 mTc, 203 Pb, 67 Ga, 68 Ga, 43 Sc, 47 Sc, 110 mIn, 97 Ru, 62 Cu, 64 Cu, 67 Cu, 68 Cu, 86 Y, 88 Y, 121 Sn, 161 Tb, 166 Ho, 105 Rh, 177 Lu, 172 Lu and 18 F.

在可選的實施方式中,所述化學發光試劑包括但不限於魯米諾及其衍生物、光澤精、甲殼動物螢光素及其衍生物、聯吡啶釕及其衍生物、吖啶酯及其衍生物、二氧環乙烷及其衍生物、洛粉堿及其衍生物和過氧草酸鹽及其衍生物。在可選的實施方式中,所述納米顆粒類標記物包括但不限於納米顆粒、膠體、有機納米顆粒、磁性納米顆粒、量子點納米顆粒和稀土絡合物納米顆粒。In an optional embodiment, the chemiluminescent reagent includes but is not limited to luminol and its derivatives, luminol, crustacean fluorescein and its derivatives, bipyridine ruthenium and its derivatives, acridinium ester and its derivatives, dioxane and its derivatives, lophanol and its derivatives, and peroxyoxalate and its derivatives. In an optional embodiment, the nanoparticle marker includes but is not limited to nanoparticles, colloids, organic nanoparticles, magnetic nanoparticles, quantum dot nanoparticles, and rare earth complex nanoparticles.

在可選的實施方式中,所述膠體包括但不限於膠體金屬、膠體硒、分散型染料、染料標記的微球和乳膠。在可選的實施方式中,所述膠體金屬包括但不限於膠體金或膠體銀。在可選的實施方式中,所述膠體金屬為膠體金。In an optional embodiment, the colloid includes but is not limited to colloidal metal, colloidal selenium, disperse dye, dye-labeled microspheres and latex. In an optional embodiment, the colloidal metal includes but is not limited to colloidal gold or colloidal silver. In an optional embodiment, the colloidal metal is colloidal gold.

在可選的實施方式中,所述抗體偶聯物還可包括與所述抗體偶聯的固相載體。抗體偶聯物中,所述抗體偶聯至固相載體。在可選的實施方式中,所述固相載體選自微球、板和膜。在可選的實施方式中,所述固相包括但不限於磁性微球、塑料微球、塑膠微粒、微孔板、玻璃、毛細管、尼龍和硝酸纖維素膜。在可選的實施方式中,所述固相載體為硝酸纖維素膜。In an alternative embodiment, the antibody conjugate may further include a solid phase carrier coupled to the antibody. In the antibody conjugate, the antibody is coupled to a solid phase carrier. In an alternative embodiment, the solid phase carrier is selected from microspheres, plates and membranes. In an alternative embodiment, the solid phase includes but is not limited to magnetic microspheres, plastic microspheres, plastic particles, microporous plates, glass, capillaries, nylon and cellulose nitrate membranes. In an alternative embodiment, the solid phase carrier is a cellulose nitrate membrane.

術語「連接子」、「Linker」或「接頭」指連接兩個多肽片段的連接單元,通常具有一定的柔性,接頭的使用不會使蛋白質結構域原有的功能喪失。連接子可以是肽連接子,其包含一個或多個氨基酸,典型的約1-30個、2-24個或3-15個氨基酸。在一些實施方案中,所述連接子為選自(GxS)y連接子,其中,x選自1-5的整數,y選自0-6的整數,在一些實施方案中,所述連接子為選自(GxS)y連接子,其中,x選自1-5的整數,y選自1-6的整數。The term "linker", "linker" or "connector" refers to a connecting unit that connects two polypeptide fragments, which usually has a certain degree of flexibility, and the use of the linker will not cause the original function of the protein domain to be lost. The linker can be a peptide linker, which contains one or more amino acids, typically about 1-30, 2-24 or 3-15 amino acids. In some embodiments, the linker is selected from (GxS)y linkers, wherein x is selected from integers of 1-5 and y is selected from integers of 0-6. In some embodiments, the linker is selected from (GxS)y linkers, wherein x is selected from integers of 1-5 and y is selected from integers of 1-6.

另一方面,本公開實施例還提供了一種檢測CCR8的方法,其包括:將如前任一項所述的抗體或如前任一項所述的抗體偶聯物或如前任一項所述的試劑或試劑盒與待檢測樣品混合,使所述抗體與待測樣本中的CCR8接觸,形成免疫複合物。在優選的實施方式中,所述免疫複合物還包括第二抗體,所述第二抗體與所述抗體結合。在優選的實施方式中,所述免疫複合物還包括第二抗體,所述第二抗體與CCR8結合。On the other hand, the disclosed embodiments also provide a method for detecting CCR8, comprising: mixing the antibody as described in any of the preceding items, or the antibody conjugate as described in any of the preceding items, or the reagent or reagent kit as described in any of the preceding items with a sample to be tested, so that the antibody contacts CCR8 in the sample to be tested to form an immune complex. In a preferred embodiment, the immune complex further comprises a second antibody, and the second antibody binds to the antibody. In a preferred embodiment, the immune complex further comprises a second antibody, and the second antibody binds to CCR8.

另一方面,本公開實施例還提供了一種製備如前任一項所述的抗體的方法,其包括:培養如前任一項所述的細胞步驟。還包括純化回收抗體的步驟。On the other hand, the disclosed embodiments also provide a method for preparing the antibody as described in any of the preceding items, comprising: culturing the cells as described in any of the preceding items, and further comprising a step of purifying and recovering the antibody.

在本公開公開了抗體的氨基酸序列的基礎上,本領域技術人員可以採用基因工程技術或其他技術(化學合成、重組表現)製備得到該抗體,例如從能夠重組表現如上任一項所述的抗體的重組細胞的培養產物中分離純化得到該抗體,這對本領域技術人員來說是容易實現的,基於此,無論採用何種技術製備本公開的抗體,其均屬本公開的保護範圍。Based on the amino acid sequence of the antibody disclosed in the present disclosure, a person skilled in the art can prepare the antibody using genetic engineering technology or other technology (chemical synthesis, recombinant expression), for example, the antibody can be separated and purified from the culture product of recombinant cells that can recombinantly express the antibody as described in any of the above items. This is easy to achieve for a person skilled in the art. Based on this, no matter what technology is used to prepare the antibody disclosed in the present disclosure, it is within the scope of protection of the present disclosure.

術語「載體」意指能夠轉運與其連接的另一多核苷酸的多核苷酸分子。一種類型的載體是「質粒」,其是指環狀雙鏈DNA環,其中可以連接附加的DNA區段。另一種類型的載體是病毒載體,例如腺相關病毒載體(AAV或AAV2),其中另外的DNA區段可以連接到病毒基因組中。某些載體能夠在引入它們的宿主細胞中自主複製(例如,具有細菌複製起點的細菌載體和附加型哺乳動物載體)。其他載體(例如,非附加型哺乳動物載體)可以在引入宿主細胞中後整合到宿主細胞的基因組中,從而與宿主基因組一起複製。術語「表達載體」或「表達構建體」是指可對宿主細胞進行轉化,且含有指導和/或控制(連同宿主細胞一起)與其可操作地連接的一個或多個異源編碼區的表達的核酸序列的載體。表達構建體可以包括但不限於影響或控制轉錄、翻譯且在存在內含子時影響與其可操作地連接的編碼區的RNA剪接的序列。The term "vector" means a polynucleotide molecule capable of transporting another polynucleotide to which it is linked. One type of vector is a "plasmid," which refers to a circular double-stranded DNA loop into which additional DNA segments can be ligated. Another type of vector is a viral vector, such as an adeno-associated viral vector (AAV or AAV2), in which additional DNA segments can be ligated into the viral genome. Certain vectors are capable of autonomous replication in a host cell into which they are introduced (e.g., bacterial vectors with a bacterial origin of replication and episomal mammalian vectors). Other vectors (e.g., non-episomal mammalian vectors) can be integrated into the host cell's genome upon introduction into the host cell, thereby replicating along with the host genome. The term "expression vector" or "expression construct" refers to a vector that can transform a host cell and contains a nucleic acid sequence that directs and/or controls (together with the host cell) the expression of one or more heterologous coding regions operably linked thereto. The expression construct may include, but is not limited to, sequences that affect or control transcription, translation, and, when introns are present, RNA splicing of the coding region operably linked thereto.

術語「宿主細胞」、「宿主細胞系」和「宿主細胞培養物」可互換使用,並且指已經導入外源核酸的細胞,包括此類細胞的後代。宿主細胞包括「轉化體」和「經轉化的細胞」,其包括原代的經轉化的細胞及自其衍生的後代,而不考慮傳代的次數。後代在核酸內容物上可以與親本細胞不完全相同,而是可以含有突變。本文中包括具有與在初始轉化細胞中篩選或選擇的相同功能或生物學活性的突變體後代。宿主細胞包括原核和真核宿主細胞,其中真核宿主細胞包括但不限於哺乳動物細胞、昆蟲細胞系植物細胞和真菌細胞。哺乳動物宿主細胞包括人、小鼠、大鼠、犬、猴、豬、山羊、牛、馬和倉鼠細胞,包括但不限於中國倉鼠卵巢(CHO)細胞、NSO、SP2細胞、HeLa細胞、幼倉鼠腎(BHK)細胞、猴腎細胞(COS)、人肝細胞癌細胞(例如,Hep G2)、A549細胞、3T3細胞和HEK-293細胞。真菌細胞包括酵母和絲狀真菌細胞,包括例如巴氏畢赤酵母(Pichiapastoris)、芬蘭畢赤酵母(Pichia finlandica)、海藻畢赤酵母(Pichia trehalophila)、科克拉馬畢赤酵母(Pichia koclamae)、膜狀畢赤酵母(Pichia membranaefaciens)、小畢赤酵母(Pichia minuta)(Ogataea minuta、Pichia lindneri)、仙人掌畢赤酵母(Pichiaopuntiae)、耐熱畢赤酵母(Pichia thermotolerans)、柳畢赤酵母(Pichia salictaria)、Pichia guercuum、皮傑普畢赤酵母(Pichia pijperi)、具柄畢赤酵母(Pichia stiptis)、甲醇畢赤酵母(Pichia methanolica)、畢赤酵母屬、釀酒酵母(Saccharomycescerevisiae)、釀酒酵母屬、多形漢遜酵母(Hansenula polymorpha)、克魯維酵母屬、乳酸克魯維酵母(Kluyveromyces lactis)、白色念珠菌(Candida albicans)、構巢麯黴(Aspergillus nidulans)、黑麯黴(Aspergillus niger)、米麯黴(Aspergillus oryzae)、裡氏木黴(Trichoderma reesei)、勒克氏菌(Chrysosporium lucknowense)、鐮刀菌屬(Fusarium sp.)、禾穀鐮刀菌(Fusarium gramineum)、菜鐮刀菌(Fusarium venenatum)、小立碗蘚(Physcomitrella patens)和粗糙脈孢菌(Neurospora crassa)。畢赤酵母屬、任何釀酒酵母屬、多形漢遜酵母(Hansenula polymorpha)、任何克魯維酵母屬、白色念珠菌(Candida albicans)、任何麯黴屬、裡氏木黴(Trichoderma reesei)、勒克黴菌(Chrysosporium lucknowense)、任何鐮刀菌屬、解脂耶氏酵母(Yarrowia lipolytica)和粗糙脈孢菌(Neurospora crassa)。The terms "host cell," "host cell line," and "host cell culture" are used interchangeably and refer to cells into which exogenous nucleic acid has been introduced, including the progeny of such cells. Host cells include "transformants" and "transformed cells," which include the primary transformed cell and progeny derived therefrom, without regard to the number of passages. Progeny may not be completely identical to the parent cell in nucleic acid content, but may contain mutations. Mutant progeny having the same function or biological activity as screened or selected in the initial transformed cell are included herein. Host cells include prokaryotic and eukaryotic host cells, wherein eukaryotic host cells include, but are not limited to, mammalian cells, insect cell lines, plant cells, and fungal cells. Mammalian host cells include human, mouse, rat, dog, monkey, pig, goat, cow, horse, and hamster cells, including but not limited to Chinese hamster ovary (CHO) cells, NSO, SP2 cells, HeLa cells, baby hamster kidney (BHK) cells, monkey kidney cells (COS), human hepatocellular carcinoma cells (e.g., Hep G2), A549 cells, 3T3 cells, and HEK-293 cells. Fungal cells include yeast and filamentous fungal cells, including, for example, Pichia pastorii, Pichia finlandica, Pichia trehalophila, Pichia koclamae, Pichia membranaefaciens, Pichia minuta (Ogataea minuta, Pichia lindneri), Pichia cactus (Pichia thermotolerans), Pichia salictaria, Pichia guercuum, Pichia pijperi, Pichia stiptis, Pichia methanolica, Pichia spp. methanolica), Bisaccharomyces spp., Saccharomyces cerevisiae, Saccharomyces spp., Hansenula polymorpha, Kluyveromyces spp., Kluyveromyces lactis, Candida albicans, Aspergillus nidulans, Aspergillus niger, Aspergillus oryzae, Trichoderma reesei, Chrysosporium lucknowense, Fusarium sp., Fusarium gramineum, Fusarium venenatum, Physcomitrella patens, and Neurospora crassa. Bifidobacterium, any brewer's yeast, Hansenula polymorpha, any Kluyveromyces, Candida albicans, any Aspergillus, Trichoderma reesei, Chrysosporium lucknowense, any Scyphozoite, Yarrowia lipolytica, and Neurospora crassa.

如在本申請中所使用的,「細胞」、「細胞系」和「細胞培養物」可以互換使用,並且所有這樣的名稱均包括子代。詞語「轉化體」和「轉化的細胞」包括原代受試者細胞和來源於其的培養物,而與傳代的次數無關。還應理解的是,由於有意或無意的突變,使得並非所有子代均具有完全相同的DNA內容物。包括與篩選出其的原始轉化細胞具有相同功能或生物活性的突變子代。As used in this application, "cell", "cell line" and "cell culture" are used interchangeably, and all such designations include progeny. The terms "transformants" and "transformed cells" include the primary subject cell and cultures derived therefrom, regardless of the number of passages. It is also understood that not all progeny have exactly the same DNA content, due to intentional or unintentional mutations. Mutant progeny that have the same function or biological activity as the original transformed cell from which they were selected are included.

術語「藥物組合物」表示含有一種或多種本文所述的抗體等活性成分與其他化學組分的混合物,所述其他組分例如生理學/可藥用的載體和賦形劑。The term "pharmaceutical composition" refers to a mixture containing one or more active ingredients such as the antibodies described herein and other chemical components, such as physiologically/pharmaceutically acceptable carriers and excipients.

術語「藥學上可接受的載體」 指藥學配製劑中與活性成分不同的,且對受試者無毒的成分。藥學可接受載劑包括但不限於緩衝劑、賦形劑、穩定劑或防腐劑。The term "pharmaceutically acceptable carrier" refers to a component in a pharmaceutical formulation that is different from the active ingredient and is non-toxic to the subject. Pharmaceutically acceptable carriers include but are not limited to buffers, excipients, stabilizers or preservatives.

術語「受試者」或「個體」包括人類和非人類動物。非人動物包括所有脊椎動物(例如哺乳動物和非哺乳動物)例如非人靈長類(例如,食蟹猴)、綿羊、狗、牛、雞、兩棲動物和爬行動物。除非指出時,否則所述術語「患者」或「受試者」在本文中可互換地使用。如本文所使用的,術語「食蟹猴(cyno)」或「食蟹猴(cynomolgus)」是指食蟹猴(Macaca fascicularis)。在某些實施方案中,個體或受試者是人。The term "subject" or "individual" includes humans and non-human animals. Non-human animals include all vertebrates (e.g., mammals and non-mammals) such as non-human primates (e.g., cynomolgus monkeys), sheep, dogs, cows, chickens, amphibians, and reptiles. Unless otherwise indicated, the terms "patient" or "subject" are used interchangeably herein. As used herein, the term "cynomolgus" or "cynomolgus" refers to cynomolgus monkeys (Macaca fascicularis). In certain embodiments, the individual or subject is a human.

「施用」或「給予」,當其應用於動物、人、實驗受試者、細胞、組織、器官或生物流體時,是指外源性藥物、治療劑、診斷劑或組合物與動物、人、受試者、細胞、組織、器官或生物流體的接觸。"Administer" or "administer," as applied to animals, humans, experimental subjects, cells, tissues, organs or biological fluids, means the contact of an exogenous drug, therapeutic agent, diagnostic agent or composition with an animal, human, subject, cell, tissue, organ or biological fluid.

術語「樣本」是指從受試者分離的類似流體、細胞、或組織的採集物,以及存在於受試者體內的流體、細胞或組織。示例性樣本為生物流體,諸如血液、血清和漿膜液、血漿、淋巴液、尿液、唾液、囊液、淚液、排泄物、痰、分泌組織和器官的粘膜分泌物、陰道分泌物、腹水、胸膜、心包、腹膜、腹腔和其它體腔的流體、由支氣管灌洗液收集的流體、滑液、與受試者或生物來源接觸的液體溶液,例如細胞和器官培養基(包括細胞或器官條件培養基)、灌洗液等,組織活檢樣本、細針穿刺、手術切除的組織、器官培養物或細胞培養物。The term "sample" refers to a collection of fluids, cells, or tissues isolated from a subject, as well as fluids, cells, or tissues present in a subject. Exemplary samples are biological fluids such as blood, serum and serous fluids, plasma, lymph, urine, saliva, cystic fluid, tears, feces, sputum, mucosal secretions of secretory tissues and organs, vaginal secretions, ascites, pleura, pericardium, peritoneum, fluids of the abdominal cavity and other body cavities, fluids collected by bronchial lavage, synovial fluid, liquid solutions in contact with a subject or biological source, such as cell and organ culture media (including cell or organ conditioned media), lavage fluids, etc., tissue biopsy specimens, fine needle aspirations, surgically removed tissues, organ cultures or cell cultures.

「治療(treatment或treat)」指試圖改變所治療個體的天然過程的臨床干預,並且可以為了預防或者在臨床病理學的過程期間實施。治療的期望效果包括但不限於預防疾病的發生或再發生,減輕症狀,減輕/減少疾病的任何直接或間接病理後果,預防轉移,降低疾病進展速率,改善或減輕疾病狀態,和消退或改善的預後。在一些實施方案中,使用本公開的抗體來延遲疾病的形成或減緩疾病的進展。"Treatment" refers to clinical intervention that attempts to alter the natural course of the individual being treated, and can be performed for prevention or during the course of clinical pathology. Desired effects of treatment include, but are not limited to, preventing the occurrence or recurrence of a disease, alleviating symptoms, alleviating/reducing any direct or indirect pathological consequences of a disease, preventing metastasis, reducing the rate of disease progression, ameliorating or reducing the disease state, and regression or improved prognosis. In some embodiments, the antibodies disclosed herein are used to delay the development of a disease or slow the progression of a disease.

「有效量」一般是足以降低症狀的嚴重程度及/或頻率、消除這些症狀及/或潛在病因、預防症狀及/或其潛在病因出現及/或改良或改善由疾病狀態引起或與其相關的損傷(例如肺病)的量。在一些實施例中,有效量是治療有效量或預防有效量。「治療有效量」是足以治療疾病狀態或症狀、尤其與該疾病狀態相關的狀態或症狀,或者以其他方式預防、阻礙、延遲或逆轉該疾病狀態或以任何方式與該疾病相關的任何其他不理想症狀的進展的量。「預防有效量」是當給予受試者時將具有預定預防效應,例如預防或延遲該疾病狀態的發作(或復發),或者降低該疾病狀態或相關症狀的發作(或復發)可能性的量。完全治療或預防效未必在給予一個劑量之後便發生,可能在給予一系列劑量之後發生。因而,治療或預防有效量可以一次或多次給予的方式給予。「治療有效量」和「預防有效量」可取決於多種因素變化:諸如個體的疾病狀態、年齡、性別和體重,以及治療劑或治療劑組合在個體中引發期望的應答的能力。有效治療劑或治療劑組合的示例性指標包括例如患者改善的健康狀況。An "effective amount" is generally an amount sufficient to reduce the severity and/or frequency of symptoms, eliminate these symptoms and/or potential causes, prevent the occurrence of symptoms and/or their potential causes, and/or ameliorate or improve damage caused by or associated with a disease state (e.g., lung disease). In some embodiments, an effective amount is a therapeutically effective amount or a prophylactically effective amount. A "therapeutically effective amount" is an amount sufficient to treat a disease state or symptom, particularly a state or symptom associated with the disease state, or otherwise prevent, hinder, delay, or reverse the progression of the disease state or any other undesirable symptom associated with the disease in any way. A "prophylactically effective amount" is an amount that, when administered to a subject, will have a predetermined prophylactic effect, such as preventing or delaying the onset (or recurrence) of the disease state, or reducing the likelihood of onset (or recurrence) of the disease state or related symptoms. A complete therapeutic or prophylactic effect may not occur after administration of one dose, but may occur after administration of a series of doses. Thus, a therapeutically or prophylactically effective amount may be administered in one or more administrations. "Therapeutically effective amount" and "prophylactically effective amount" may vary depending on a variety of factors: such as the individual's disease state, age, sex, and weight, and the ability of the therapeutic agent or combination of therapeutic agents to elicit the desired response in the individual. Exemplary indicators of an effective therapeutic agent or combination of therapeutic agents include, for example, improved health status of the patient.

為使本公開實施例的目的、技術方案和優點更加清楚,下面將對本公開實施例中的技術方案進行清楚、完整地描述。實施例中未注明具體條件者,按照常規條件或製造商建議的條件進行。所用試劑或儀器未注明生產廠商者,均為可以通過市售購買獲得的常規產品。In order to make the purpose, technical solution and advantages of the disclosed embodiment clearer, the technical solution in the disclosed embodiment is described clearly and completely below. If no specific conditions are specified in the embodiment, the experiment is carried out according to conventional conditions or conditions recommended by the manufacturer. If the manufacturer of the reagents or instruments used is not specified, they are all conventional products that can be purchased commercially.

除非另有定義,否則本文使用的所有技術和科學術語具有與本公開內容所屬領域的普通技術人員通常理解的含義相同的含義。儘管與本文描述的那些方法和材料類似或等同的任何方法和材料都可用于本文的製劑或單位劑量的實踐或測試,但現在描述一些方法和材料。除非另有說明,否則本文採用或考慮的技術是標準方法。材料、方法和實例僅是說明性而非限制性的。Unless otherwise defined, all technical and scientific terms used herein have the same meaning as those commonly understood by those skilled in the art to which this disclosure belongs. Although any methods and materials similar or equivalent to those described herein can be used in the practice or testing of the formulations or unit doses herein, some methods and materials are now described. Unless otherwise specified, the techniques used or considered herein are standard methods. The materials, methods, and examples are illustrative only and not limiting.

除非另外指明,否則實踐本公開將採用細胞生物學、分子生物學(包含重組技術)、微生物學、生物化學和免疫學的常規技術,所述常規技術在本領域技術人員的能力範圍內。文獻中充分解釋了這種技術,如《分子克隆:實驗室手冊(Molecular Cloning:A Laboratory Manual)》,第二版(Sambrook等人,1989);《寡核苷酸合成(Oligonucleotide Synthesis)》(M.J.Gait編,1984);《動物細胞培養(Animal Cell Culture)》(R.I.Freshney編,1987);《酶學方法(Methods in Enzymology)》(學術出版社有限公司(Academic Press,Inc.);《實驗免疫學手冊(Handbook of Experimental Immunology)》(D.M.Weir和C.C.Blackwell編);《哺乳動物細胞用基因轉移載體(Gene Transfer Vectors for Mammalian Cells)》(J.M.Miller和M.P.Calos編,1987);《當代分子生物學方法(Current Protocols in Molecular Biology)》(F.M.Ausubel等人編,1987);《PCR:聚合酶鏈反應(PCR:The Polymerase Chain Reaction)》(Mullis等人編,1994);以及《當代免疫學方法(Current Protocols in Immunology)》(J.E.Coligan等人編,1991),所述文獻中的每個文獻均通過引用明確併入本文中。Unless otherwise indicated, the practice of this disclosure will employ conventional techniques of cell biology, molecular biology (including recombinant techniques), microbiology, biochemistry, and immunology, which are within the capabilities of a skilled artisan. The technique is fully explained in the literature, such as Molecular Cloning: A Laboratory Manual, 2nd edition (Sambrook et al., 1989); Oligonucleotide Synthesis (M.J. Gait, ed., 1984); Animal Cell Culture (R.I. Freshney, ed., 1987); Methods in Enzymology (Academic Press, Inc.); Handbook of Experimental Immunology (D.M. Weir and C.C. Blackwell, eds.); Gene Transfer Vectors for Mammalian Cells (J.M. Miller and M.P. Calos, eds., 1987); and Current Protocols in Molecular Biology (Ed., 1996). Biology" (F. M. Ausubel et al., eds., 1987); PCR: The Polymerase Chain Reaction (Mullis et al., eds., 1994); and Current Protocols in Immunology (J. E. Coligan et al., eds., 1991), each of which is expressly incorporated herein by reference.

以下結合實施例對本公開的特徵和性能作進一步的詳細描述。The features and performance of the present invention are further described in detail below in conjunction with the embodiments.

實施例Embodiment 1.1. anti- CCR8CCR8 雜交瘤Hybridoma 抗體製備Antibody preparation

採用Balb/c小鼠,用過表現人CCR8的CHO(中國倉鼠卵巢細胞)細胞(CHO-hCCR8)及人CCR8的N端1-35位氨基酸與小鼠Fc的融合蛋白(CCR8N-term-mFc)作為免疫原,進行多次免疫。每一到兩周進行一次,共6-10次。在第四次免疫後,對小鼠進行眼眶取血,通過ELISA及流式細胞術檢測抗人CCR8抗體的血清效價。將小鼠血清倍比稀釋後與Raji細胞系(人BURKITT'S淋巴瘤細胞)及過表現人CCR8的Raji細胞系(Raji-hCCR8)共同培育,並通過PE標記的山羊抗小鼠Fc抗體(Biolegend)進行染色,通過流式細胞術檢測血清效價。同時,將CCR8N-term-hFc蛋白(人CCR8的N端1-35位氨基酸與人Fc的融合蛋白)包被至96孔盤中,加入倍比稀釋的血清培育,隨後加入HRP標記的山羊抗小鼠Fc抗體(Sigma),通過ELISA檢測血清效價。根據流式細胞術及ELISA的結果確定效價最高的小鼠,對小鼠進行安樂死,收集脾細胞,與SP20細胞系進行融合。Balb/c mice were used, and CHO (Chinese hamster ovary cells) cells expressing human CCR8 (CHO-hCCR8) and a fusion protein of the N-terminal 1-35 amino acids of human CCR8 and mouse Fc (CCR8N-term-mFc) were used as immunogens for multiple immunizations. This was done once every one to two weeks, for a total of 6-10 times. After the fourth immunization, the mice were bled from the eye sockets, and the serum titer of anti-human CCR8 antibodies was detected by ELISA and flow cytometry. The mouse serum was diluted in multiples and co-cultured with Raji cell lines (human BURKITT'S lymphoma cells) and Raji cell lines expressing human CCR8 (Raji-hCCR8), and stained with PE-labeled goat anti-mouse Fc antibodies (Biolegend), and the serum titer was detected by flow cytometry. At the same time, CCR8N-term-hFc protein (a fusion protein of the N-terminal 1-35 amino acids of human CCR8 and human Fc) was coated into a 96-well plate, and the serum was incubated with multiple dilutions, followed by the addition of HRP-labeled goat anti-mouse Fc antibody (Sigma), and the serum titer was tested by ELISA. The mice with the highest titer were determined based on the results of flow cytometry and ELISA, and the mice were euthanized, spleen cells were collected, and fused with the SP20 cell line.

挑選出與Raji-hCCR8結合活性強、且不與Raji細胞系結合的上清的單克隆細胞用以擴大培養。一周後收集上清,對上清中的抗體進行純化。Monoclonal cells with strong binding activity to Raji-hCCR8 and no binding to Raji cell line were selected for expansion culture. After one week, the supernatant was collected and the antibodies in the supernatant were purified.

實施例Embodiment 2.2. anti- CCR8CCR8 抗體的結合活性篩選Antibody Binding Activity Screening

對Raji-hCCR8和Raji細胞進行計數,調整密度至2E6/ml,加入100μL/孔細胞懸液至96孔盤中,400×g離心5分鐘,棄上清。配置濃度為200nM的雜交瘤純化抗體,並進行3倍梯度稀釋。用100μL稀釋好的雜交瘤純化抗體重懸細胞,4℃孵育30分鐘。用PBS洗滌2次後,加入100μL按1:500稀釋的PE標記的山羊抗小鼠Fc抗體重懸細胞,4℃培育30分鐘。用PBS洗滌1次後,加入100μL/孔PBS重懸細胞,通過流式細胞術分析PE螢光強度。Count Raji-hCCR8 and Raji cells, adjust the density to 2E6/ml, add 100μL/well cell suspension to a 96-well plate, centrifuge at 400×g for 5 minutes, and discard the supernatant. Prepare hybridoma-purified antibodies at a concentration of 200nM and perform a 3-fold gradient dilution. Resuspend the cells with 100μL of diluted hybridoma-purified antibodies and incubate at 4℃ for 30 minutes. After washing twice with PBS, add 100μL of PE-labeled goat anti-mouse Fc antibodies diluted 1:500 and resuspend the cells, and incubate at 4℃ for 30 minutes. After washing once with PBS, 100 μL/well PBS was added to resuspend the cells, and the PE fluorescence intensity was analyzed by flow cytometry.

抗CCR8抗體與Raji-hCCR8的結合檢測結果如圖1所示,實驗結果表明,F022-7、F022-59、F022-63、F022-66、F022-68、F022-75這6個雜交瘤純化抗體展現出了與Raji-hCCR8較強的結合活性。The binding test results of anti-CCR8 antibodies to Raji-hCCR8 are shown in Figure 1. The experimental results show that the six hybridoma-purified antibodies F022-7, F022-59, F022-63, F022-66, F022-68, and F022-75 exhibited strong binding activity to Raji-hCCR8.

實施例Embodiment 3.3. 重組的抗Recombinant Antibodies CCR8CCR8 抗體的製備Antibody preparation

調取F022-7、F022-59、F022-63、F022-66、F022-68、F022-75雜交瘤純化抗體的序列,測序結果證明所有雜交瘤純化抗體的輕鏈恒定區均為鼠κ型(如SEQ ID No.40所示),F022-7、F022-63和F022-75的重鏈恒定區為mIgG2a型(如SEQ ID No.41所示),F022-59、F022-66和F022-68的重鏈恒定區為mIgG1型(如SEQ ID No.39所示)。將雜交瘤純化抗體的重鏈恒定區替換為小鼠mIgG2a,其它序列不變,並克隆至pCDNA3.4A表現質體中,將質體轉染至EXPI293細胞系中,7天後收取上清,經protein A純化後得到重組抗體,重組抗體分別命名為F022-7-mIgG2a,F022-59-mIgG2a,F022-63-mIgG2a,F022-66-mIgG2a,F022-68-mIgG2a,F022-75-mIgG2a,例如重組抗體「F022-59-mIgG2a」表示雜交瘤純化抗體「F022-59」的重鏈恒定區被「mIgG2a」替換後形成的抗體,其它依此類推。將雜交瘤純化抗體的重鏈恒定區替換為人hIgG1Fc(DLE)(也即人IgG1的Fc進行S239D/A330L/I332E突變,序列如SEQ ID No.42所示),同時輕鏈恒定區替換為人κ輕鏈恒定區(如SEQ ID No.43所示),其它序列不變,並克隆至pCDNA3.4A表現質體中,將質體轉染至EXPI293細胞系中,7天後收取上清,經protein A純化後得到重組抗體,重組抗體分別命名為F022-7-hIgG1(DLE),F022-59-hIgG1(DLE),F022-63-hIgG1(DLE),F022-66-hIgG1(DLE),F022-68-hIgG1(DLE),F022-75-hIgG1(DLE),例如重組抗體「F022-59-hIgG1(DLE)」表示雜交瘤純化抗體「F022-59」的重鏈恒定區被人hIgG1(DLE)且輕鏈恒定區被人κ輕鏈恒定區替換後形成的抗體,其它依此類推。抗體的可變區序列見表1,CDRs序列見表2。The sequences of F022-7, F022-59, F022-63, F022-66, F022-68, and F022-75 hybridoma-purified antibodies were retrieved, and the sequencing results showed that the light chain constant regions of all hybridoma-purified antibodies were of mouse κ type (as shown in SEQ ID No.40), the heavy chain constant regions of F022-7, F022-63, and F022-75 were of mIgG2a type (as shown in SEQ ID No.41), and the heavy chain constant regions of F022-59, F022-66, and F022-68 were of mIgG1 type (as shown in SEQ ID No.39). The heavy chain constant region of the hybridoma purified antibody was replaced with mouse mIgG2a, and other sequences remained unchanged. The antibody was cloned into pCDNA3.4A expression plasmid, and the plasmid was transfected into EXPI293 cell line. After 7 days, the supernatant was collected and purified with protein A to obtain recombinant antibodies. The recombinant antibodies were named F022-7-mIgG2a, F022-59-mIgG2a, F022-63-mIgG2a, F022-66-mIgG2a, F022-68-mIgG2a, and F022-75-mIgG2a. For example, the recombinant antibody "F022-59-mIgG2a" means that the heavy chain constant region of the hybridoma purified antibody "F022-59" was replaced with "mIgG2a", and the others are similar. The heavy chain constant region of the hybridoma purified antibody was replaced with human hIgG1Fc (DLE) (i.e., human IgG1 Fc was mutated with S239D/A330L/I332E, the sequence is shown in SEQ ID No.42), and the light chain constant region was replaced with human κ light chain constant region (as shown in SEQ ID No.43), and the other sequences were kept unchanged. ... of the hybridoma purified antibody was replaced with human κ light chain constant region (as shown in SEQ ID No.43), and the other sequences were kept unchanged. The heavy chain constant region of the hybridoma purified antibody was replaced with human hIgG1Fc (DLE), and the light chain constant region of the hybridoma purified antibody was replaced with human hIgG1Fc (DLE), and the light chain constant region of the hybridoma purified antibody was replaced with human hIgG1Fc (DLE After purification, recombinant antibodies were obtained. The recombinant antibodies were named F022-7-hIgG1 (DLE), F022-59-hIgG1 (DLE), F022-63-hIgG1 (DLE), F022-66-hIgG1 (DLE), F022-68-hIgG1 (DLE), and F022-75-hIgG1 (DLE). For example, the recombinant antibody "F022-59-hIgG1 (DLE)" means that the heavy chain constant region of the hybridoma purified antibody "F022-59" is replaced by human hIgG1 (DLE) and the light chain constant region is replaced by human κ light chain constant region, and the others are similar. The variable region sequences of the antibodies are shown in Table 1, and the CDRs sequences are shown in Table 2.

表1. 抗CCR8抗體可變區序列表 抗體 VH VL F022-7 EVQLVESGGGLVQPKGSLKLSCAASGFTFNTYAMNWVRQAPGKGLEWVARVRSKSNFYATYYADSVKDRFTISRDDSQNMLSLQMNNLKTEDTAIYYCVRGKDAKGIYAMDFWGQGTSVTVSS (SEQ ID No.1) DIVMTQAAPSVVVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPRLLIYRMSNLASGVPDRFSGSGSGTAFTLRISRVEAEDVGVYYCMQHLEYPFTFGGGTILEIK (SEQ ID No.2) F022-59 EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSS (SEQ ID No.3) DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELK (SEQ ID No.4) F022-63 EVQLVESGGGLVQPKGSLKLSCAASGFTFNPYAMNWVRQAPGKGLEWVARIRSKSNNYATYYADSVKDRFTISRDDSQSMLYLQMNNLKTEDTAMYYCVRQWVRRDYAMDYWGQGTSVTVSS (SEQ ID No.5) DVVMTQSPLSLPVSLGDQASISCRSSQSLVHSNGNTYLHWYLQKPGQSPKLLIYKVSNRFSGVPDRFSGSGSGTDFTLKISRVEAEDLGVYFCSQSTHVPFTFGSGTKLEIK (SEQ ID No.6) F022-66 EVQLVESGGGLVQPKGSLKLSCAASGFSFNTYAMNWVRQAPGKGLEWVGRIRTKSNSYATYYADSVKDRFTISRDDSESMVYLQMNNLKTEDGAMYYCVRGGWGYRNFVYFDVWGTGTTVTVSS (SEQ ID No.7) DIVMTQDAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRTSNLASGVPDRFSGSGSGTAFTLRISRVEAEDVGVYYCMQHLEYPFTFGGGTKLEIK (SEQ ID No.8) F022-68 EVQLVESGGGLVQPKGSLKLSCAASGFSFNIYAMNWVRQAPGKGLEWVARIRSKSNKYATFYADSVKDRFTISRDDSESKLYLHMNNLKTEDTAMYYCVRHKRGLNYGMDYWGQGTSVTVSS (SEQ ID No.9) DIVLTQSPVSLVVSLGQRATISCRASKSVSTSGYSYMHWYQQKPGQAPKLLIYLASNLESGVPARFSGSGSGTDFTLNIHPVEEEDAATYYCQHSRELPWTFGGGTKLEIK (SEQ ID No.10) F022-75 AVQFVETGGGLVQPRGSLKLSCAASGFTFNTYAMNWVRQAPGKGLEWVARIRSKSNNYATYFADSVRDRFTISRDDSQSILYLQMNNLKTEDTAMYYCVRGGERRGDYAMDYWGQGTSVTVSS (SEQ ID No.11) DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTAFTLRISRVEAEDVGVYYCMQHLEYPFTFGSGTKLEMK (SEQ ID No.12) Table 1. Anti-CCR8 antibody variable region sequence list antibody VH V L F022-7 EVQLVESGGGLVQPKGSLKLSCAASGFTFNTYAMNWVRQAPGKGLEWVARVRSKSNFYATYYADSVKDRFTISRDDSQNMLSLQMNNLKTEDTAIYYCVRGKDAKGIYAMDFWGQGTSVTVSS (SEQ ID No. 1) DIVMTQAAPSVVVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPRLLIYRMSNLASGVPDRFSGSGSGTAFTLRISRVEAEDVGVYYCMQHLEYPFTFGGGTILEIK (SEQ ID No. 2) F022-59 EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSS (SEQ ID No. 3) DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELK (SEQ ID No. 4) F022-63 EVQLVESGGGLVQPKGSLKLSCAASGFTFNPYAMNWVRQAPGKGLEWVARIRSKSNNYATYYADSVKDRFTISRDDSQSMLYLQMNNLKTEDTAMYYCVRQWVRRDYAMDYWGQGTSVTVSS (SEQ ID No. 5) DVVMTQSPLSLPVSLGDQASISCRSSQSLVHSNGNTYLHWYLQKPGQSPKLLIYKVSNRFSGVPDRFSGSGSGTDFTLKISRVEAEDLGVYFCSQSTHVPFTFGSGTKLEIK (SEQ ID No. 6) F022-66 EVQLVESGGGLVQPKGSLKLSCAASGFSFNTYAMNWVRQAPGKGLEWVGRIRTKSNSYATYYADSVKDRFTISRDDSESMVYLQMNNLKTEDGAMYYCVRGGWGYRNFVYFDVWGTGTTVTVSS (SEQ ID No. 7) DIVMTQDAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRTSNLASGVPDRFSGSGSGTAFTLRISRVEAEDVGVYYCMQHLEYPFTFGGGTKLEIK (SEQ ID No. 8) F022-68 EVQLVESGGGLVQPKGSLKLSCAASGFSFNIYAMNWVRQAPGKGLEWVARIRSKSNKYATFYADSVKDRFTISRDDSESKLYLHMNNLKTEDTAMYYCVRHKRGLNYGMDYWGQGTSVTVSS (SEQ ID No. 9) DIVLTQSPVSLVVSLGQRATISCRASKSVSTSGYSYMHWYQQKPGQAPKLLIYLASNLESGVPARFSGSGSGTDFTLNIHPVEEEDAATYYCQHSRELPWTFGGGTKLEIK (SEQ ID No.10) F022-75 AVQFVETGGGLVQPRGSLKLSCAASGFTFNTYAMNWVRQAPGKGLEWVARIRSKSNNYATYFADSVRDRFTISRDDSQSILYLQMNNLKTEDTAMYYCVRGGERRGDYAMDYWGQGTSVTVSS (SEQ ID No. 11) DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTAFTLRISRVEAEDVGVYYCMQHLEYPFTFGSGTKLEMK (SEQ ID No. 12)

表2.抗CCR8抗體CDRs序列表 抗體 重鏈CDR 輕鏈CDR F022-7 HCDR1 TYAMN (SEQ ID No.13) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RVRSKSNFYATYYADSVKD (SEQ ID No.14) LCDR2 RMSNLAS (SEQ ID No.17) HCDR3 GKDAKGIYAMDF (SEQ ID No.15) LCDR3 MQHLEYPFT (SEQ ID No.18) F022-59 HCDR1 TNAMN (SEQ ID No.19) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RIRTKSNNYATYYADSVKD (SEQ ID No.20) LCDR2 RMSNLAS (SEQ ID No.17) HCDR3 GGYGYDVRSGMEY (SEQ ID No.21) LCDR3 MQHLEYPFT (SEQ ID No.18) F022-63 HCDR1 PYAMN (SEQ ID No.22) LCDR1 RSSQSLVHSNGNTYLH (SEQ ID No.25) HCDR2 RIRSKSNNYATYYADSVKD (SEQ ID No.23) LCDR2 KVSNRFS (SEQ ID No.26) HCDR3 QWVRRDYAMDY (SEQ ID No.24) LCDR3 SQSTHVPFT (SEQ ID No.27) F022-67 HCDR1 TYAMN (SEQ ID No.13) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RIRTKSNSYATYYADSVKD (SEQ ID No.28) LCDR2 RTSNLAS (SEQ ID No.30) HCDR3 GGWGYRNFVYFDV (SEQ ID No.29) LCDR3 MQHLEYPFT (SEQ ID No.18) F022-68 HCDR1 IYAMN (SEQ ID No.31) LCDR1 RASKSVSTSGYSYMH (SEQ ID No.34) HCDR2 RIRSKSNKYATFYADSVKD (SEQ ID No.32) LCDR2 LASNLES (SEQ ID No.35) HCDR3 HKRGLNYGMDY (SEQ ID No.33) LCDR3 QHSRELPWT (SEQ ID No.36) F022-75 HCDR1 TYAMN (SEQ ID No.13) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RIRSKSNNYATYFADSVRD (SEQ ID No.37) LCDR2 RMSNLAS (SEQ ID No.17) HCDR3 GGERRGDYAMDY (SEQ ID No.38) LCDR3 MQHLEYPFT (SEQ ID No.18) 備註:上述表2所述抗體的HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3是根據Kabat編碼系統確認。 Table 2. Anti-CCR8 antibody CDRs sequence list antibody Rechain CDR Light Chain CDR F022-7 HCDR1 TYAMN (SEQ ID No. 13) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RVRSKSNFYATYYADSVKD (SEQ ID No.14) LCDR2 RMSNLAS (SEQ ID No.17) HCDR3 GKDAKGIYAMDF (SEQ ID No.15) LCDR3 MQHLEYPFT (SEQ ID No.18) F022-59 HCDR1 TNAMN (SEQ ID No.19) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RIRTKSNNYATYYADSVKD (SEQ ID No.20) LCDR2 RMSNLAS (SEQ ID No.17) HCDR3 GGYGYDVRSGMEY (SEQ ID No.21) LCDR3 MQHLEYPFT (SEQ ID No.18) F022-63 HCDR1 PYAMN (SEQ ID No. 22) LCDR1 RSSQSLVHSNGNTYLH (SEQ ID No.25) HCDR2 RIRSKSNNYATYYADSVKD (SEQ ID No.23) LCDR2 KVSNRFS (SEQ ID No. 26) HCDR3 QWVRRDYAMDY (SEQ ID No.24) LCDR3 SQSTHVPFT (SEQ ID No. 27) F022-67 HCDR1 TYAMN (SEQ ID No. 13) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RIRTKSNSYATYYADSVKD (SEQ ID No.28) LCDR2 RTSNLAS (SEQ ID No.30) HCDR3 GGWGYRNFVYFDV (SEQ ID No.29) LCDR3 MQHLEYPFT (SEQ ID No.18) F022-68 HCDR1 IYAMN (SEQ ID No.31) LCDR1 RASKSVSTSGYSYMH (SEQ ID No.34) HCDR2 RIRSKSNKYATFYADSVKD (SEQ ID No.32) LCDR2 LASNLES (SEQ ID No.35) HCDR3 HKRGLNYGMDY (SEQ ID No.33) LCDR3 QHSRELPWT (SEQ ID No. 36) F022-75 HCDR1 TYAMN (SEQ ID No.13) LCDR1 RSSKSLLHSNGNTYLY (SEQ ID No.16) HCDR2 RIRSKSNNYATYFADSVRD (SEQ ID No.37) LCDR2 RMSNLAS (SEQ ID No.17) HCDR3 GGERRGDYAMDY (SEQ ID No.38) LCDR3 MQHLEYPFT (SEQ ID No.18) Note: HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 of the antibodies described in Table 2 above were identified according to the Kabat coding system.

鼠mIgG1重鏈恒定區的氨基酸序列(SEQ ID No.39): AKTTPPSVYPLAPGSAAQTNSMVTLGCLVKGYFPEPVTVTWNSGSLSSGVHTFPAVLQSDLYTLSSSVTVPSSTWPSQTVTCNVAHPASSTKVDKKIVPRDCGCKPCICTVPEVSSVFIFPPKPKDVLTITLTPKVTCVVVDISKDDPEVQFSWFVDDVEVHTAQTKPREEQFNSTFRSVSELPIMHQDWLNGKEFKCRVNSAAFPAPIEKTISKTKGRPKAPQVYTIPPPKEQMAKDKVSLTCMITNFFPEDITVEWQWNGQPAENYKNTQPIMDTDGSYFVYSKLNVQKSNWEAGNTFTCSVLHEGLHNHHTEKSLSHSPGK Amino acid sequence of mouse mIgG1 heavy chain constant region (SEQ ID No. 39): AKTTPPSVYPLAPGSAAQTNSMVTLGCLVKGYFPEPVTWNSGSLSSGVHTFPAVLQSDLYTLSSSVTVPSSTWPSQTVTCNVAHPASSTKVDKKIVPRDCGCKPCICTVPEVSSVFIFPPKPKDVLTITLTPKVTCVVVDISKDDPEVQFSWFVDDVEVHTAQ TKPREEQFNSTFRSVSELPIMHQDWLNGKEFKCRVNSAAFPAPIEKTISKTKGRPKAPQVYTIPPPKEQMAKDKVSLTCMITNFFPEDITVEWQWNGQPAENYKNTQPIMDTDGSYFVYSKLNVQKSNWEAGNTFTCSVLHEGLHNHHTEKSLSHSPGK

鼠κ輕鏈恒定區的氨基酸序列(SEQ ID No.40): RADAAPTVSIFPPSSEQLTSGGASVVCFLNNFYPKDINVKWKIDGSERQNGVLNSWTDQDSKDSTYSMSSTLTLTKDEYERHNSYTCEATHKTSTSPIVKSFNRNEC The amino acid sequence of the mouse kappa light chain constant region (SEQ ID No. 40): RADAAPTVSIFPPSSEQLTSGGASVVCFLNNFYPKDINVKWKIDGSERQNGVLNSWTDQDSKDSTYSMSSTLTLTKDEYERHNSYTCEATHKTSTSPIVKSFNRNEC

鼠mIgG2a重鏈恒定區的氨基酸序列(SEQ ID No.41): AKTTAPSVYPLAPVCGDTTGSSVTLGCLVKGYFPEPVTLTWNSGSLSSGVHTFPAVLQSDLYTLSSSVTVTSSTWPSQSITCNVAHPASSTKVDKKIEPRGPTIKPCPPCKCPAPNLLGGPSVFIFPPKIKDVLMISLSPIVTCVVVDVSEDDPDVQISWFVNNVEVHTAQTQTHREDYNSTLRVVSALPIQHQDWMSGKEFKCKVNNKDLPAPIERTISKPKGSVRAPQVYVLPPPEEEMTKKQVTLTCMVTDFMPEDIYVEWTNNGKTELNYKNTEPVLDSDGSYFMYSKLRVEKKNWVERNSYSCSVVHEGLHNHHTTKSFSRTPGK Amino acid sequence of mouse mIgG2a heavy chain constant region (SEQ ID No. 41): AKTTAPSVYPLAPVCGDTTGSSVTLGCLVKGYFPEPVTLTWNSGSLSSGVHTFPAVLQSDLYTLSSSVTVTSSTWPSQSITCNVAHPASSTKVDKKIEPRGPTIKPCPPCKCPAPNLLGGPSVFIFPPKIKDVLMISLSPIVTCVVVDVSEDDPDVQISWFVNNV EVHTAQTQTHREDYNSTLRVVSALPIQHQDWMSGKEFKCKVNNKDLPAPIERTISKPKGSVRAPQVYVLPPPEEEMTKKQVTLTCMVTDFMPEDIYVEWTNNGKTELNYKNTEPVLDSDGSYFMYSKLRVEKKNWVERNSYSCSVVHEGLHNHHTTKSFSRTPGK

人hIgG1(DLE)抗體重鏈恒定區序列(SEQ ID No.42): ASTKGPSVFPLAPSSKSTSGGTAALGCLVKDYFPEPVTVSWNSGALTSGVHTFPAVLQSSGLYSLSSVVTVPSSSLGTQTYICNVNHKPSNTKVDKRVEPKSCDKTHTCPPCPAPELLGGPDVFLFPPKPKDTLMISRTPEVTCVVVDVSHEDPEVKFNWYVDGVEVHNAKTKPREEQYNSTYRVVSVLTVLHQDWLNGKEYKCKVSNKALPLPEEKTISKAKGQPREPQVYTLPPSREEMTKNQVSLTCLVKGFYPSDIAVEWESNGQPENNYKTTPPVLDSDGSFFLYSKLTVDKSRWQQGNVFSCSVMHEALHNHYTQKSLSLSPGK Human hIgG1 (DLE) antibody heavy chain constant region sequence (SEQ ID No. 42): ASTKGPSVFPLAPSSKSTSGGTAALGCLVKDYFPEPVTVSWNSGALTSGVHTFPAVLQSSGLYSLSSVVTVPSSSLGTQTYICNVNHKPSNTKVDKRVEPKSCDKTHTCPPCPAPELLGGPDVFLFPPKPKDTLMISRTPEVTCVVVDVSHEDPEVKFNWYVDGV EVHNAKTKPREEQYNSTYRVVSVLTVLHQDWLNGKEYKCKVSNKALPLPEEKTISKAKGQPREPQVYTLPPSREEMTKNQVSLTCLVKGFYPSDIAVEWESNGQPENNYKTTPPVLDSDGSFFLYSKLTVDKSRWQQGNVFSCSVMHEALHNHYTQKSLSLSPGK

人κ輕鏈恒定區序列(SEQ ID No.43): RTVAAPSVFIFPPSDEQLKSGTASVVCLLNNFYPREAKVQWKVDNALQSGNSQESVTEQDSKDSTYSLSSTLTLSKADYEKHKVYACEVTHQGLSSPVTKSFNRGEC Human kappa light chain constant region sequence (SEQ ID No. 43): RTVAAPSVFIFPPSDEQLKSGTASVVCLLNNFYPREAKVQWKVDNALQSGNSQESVTEQDSKDSTYSLSSTLTLSKADYEKHKVYACEVTHQGLSSPVTKSFNRGEC

示例性地,F022-59、F022-59-mIgG2a、F022-59-hIgG1(DLE)的全長序列如下:Exemplarily, the full-length sequences of F022-59, F022-59-mIgG2a, and F022-59-hIgG1 (DLE) are as follows:

F022-59重鏈可變區的氨基酸序列(SEQ ID No.44): EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSSAKTTPPSVYPLAPGSAAQTNSMVTLGCLVKGYFPEPVTVTWNSGSLSSGVHTFPAVLQSDLYTLSSSVTVPSSTWPSQTVTCNVAHPASSTKVDKKIVPRDCGCKPCICTVPEVSSVFIFPPKPKDVLTITLTPKVTCVVVDISKDDPEVQFSWFVDDVEVHTAQTKPREEQFNSTFRSVSELPIMHQDWLNGKEFKCRVNSAAFPAPIEKTISKTKGRPKAPQVYTIPPPKEQMAKDKVSLTCMITNFFPEDITVEWQWNGQPAENYKNTQPIMDTDGSYFVYSKLNVQKSNWEAGNTFTCSVLHEGLHNHHTEKSLSHSPGK Amino acid sequence of F022-59 heavy chain variable region (SEQ ID No. 44): EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSSAKTTPPSVYPLAPGSAAQTNSMVTLGCLVKGYFPEPVTVTWTW NSGSLSSGVHTFPAVLQSDLYTLSSSVTVPSSTWPSQTVTCNVAHPASSTKVDKKIVPR DCGCKPCICTVPEVSSVFIFPPKPKDVLTITLTPKVTCVVVDISKDDPEVQFSWFVDDVEVHTAQTKPREEQFNSTFRSSVSELPIMHQDWLNGKEFKCRVNSAAFPAPIEKTISKTKGRPKAPQVYTIPPPKEQMAKDKVSLTCMITNFFPEDITVEWQWNGQPAENYKNTQPIMDTDGSYFVYSKLNVQKSNWEAGNTFT CSVLHEGLHNHHTEKSLSHSPGK

F022-59輕鏈可變區的氨基酸序列(SEQ ID No.45): DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELK RADAAPTVSIFPPSSEQLTSGGASVVCFLNNFYPKDINVKWKIDGSERQNGVLNSWTDQDSKDSTYSMSSTLTLTKDEYERHNSYTCEATHKTSTSPIVKSFNRNEC The amino acid sequence of the variable region of the light chain of F022-59 (SEQ ID No. 45): DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELK RADAAPTVSIFPPSSEQLTSGGASVVCFLNNFYPKDINVKWKIDGSERQNGVLNSWTDQDSKDSTYSMSSTLTLTKDEYERHNSYTCEATHKTSTSPIVKSFNRNEC

F022-59-mIgG2a重鏈可變區的氨基酸序列(SEQ ID No.46): EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSSAKTTAPSVYPLAPVCGDTTGSSVTLGCLVKGYFPEPVTLTWNSGSLSSGVHTFPAVLQSDLYTLSSSVTVTSSTWPSQSITCNVAHPASSTKVDKKIEPRGPTIKPCPPCKCPAPNLLGGPSVFIFPPKIKDVLMISLSPIVTCVVVDVSEDDPDVQISWFVNNVEVHTAQTQTHREDYNSTLRVVSALPIQHQDWMSGKEFKCKVNNKDLPAPIERTISKPKGSVRAPQVYVLPPPEEEMTKKQVTLTCMVTDFMPEDIYVEWTNNGKTELNYKNTEPVLDSDGSYFMYSKLRVEKKNWVERNSYSCSVVHEGLHNHHTTKSFSRTPGK Amino acid sequence of F022-59-mIgG2a heavy chain variable region (SEQ ID No. 46): EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSSAKTTAPSVYPLAPVCGDTTGSSVTLGCLVK GYFPEPVTLTWNSGLSSGVHTFPAVLQSDLYTLSSSVTVTSSTWPSQSITCNVAHPASSTKVDKKIEPRGPT IKPCPPCKCPAPNLLGGPSVFIFPPPKIKDVLMISLSPIVTCVVVDVSEDDPDVQISWFVNNVEVHTAQTQTHREDYNSTLRVVSALPIQHQDWMSGKEFKCKVNNKDLPAPIERTISKPKGSVRAPQVYVLPPPEEEMTKKQVTLTCMVTDFMPEDIYVEWTNNGKTELNYKNTEPVLDSDGSYFMYSKLRVEKKNWVERNS YSCSVVHEGLHNHHTTKSFSRTPGK

F022-59-mIgG2a輕鏈可變區的氨基酸序列(SEQ ID No.47): DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELK The amino acid sequence of the variable region of the light chain of F022-59-mIgG2a (SEQ ID No. 47): DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELK

F022-59-hIgG1(DLE)重鏈可變區的氨基酸序列(SEQ ID No.48): EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSSASTKGPSVFPLAPSSKSTSGGTAALGCLVKDYFPEPVTVSWNSGALTSGVHTFPAVLQSSGLYSLSSVVTVPSSSLGTQTYICNVNHKPSNTKVDKRVEPKSCDKTHTCPPCPAPELLGGPDVFLFPPKPKDTLMISRTPEVTCVVVDVSHEDPEVKFNWYVDGVEVHNAKTKPREEQYNSTYRVVSVLTVLHQDWLNGKEYKCKVSNKALPLPEEKTISKAKGQPREPQVYTLPPSREEMTKNQVSLTCLVKGFYPSDIAVEWESNGQPENNYKTTPPVLDSDGSFFLYSKLTVDKSRWQQGNVFSCSVMHEALHNHYTQKSLSLSPGK Amino acid sequence of F022-59-hIgG1 (DLE) heavy chain variable region (SEQ ID No. 48): EVQLVETGGGLVQPKGSLKLSCAASGFTFNTNAMNWVRQAPGKGLEWVARIRTKSNNYATYYADSVKDRFTISRDDSRSLLYLQMNTLKTEDSAMYYCVRGGYGYDVRSGMEYWGQGTSVTVSSASTKGPSVFPLAPSSKSTSGGTAALGCLV KDYFPEPVTVSWNSGALTSGVHTFPAVLQSSGLYSLSSVVTVPSSSLGTQTYICNVNHKPSNTKVDKRVEPKSC DKTHTCPPCPAPELLGGPDVFLFPPKPKDTLMISRTPEVTCVVVDVSHEDPEVKFNWYVDGVEVHNAKTKPREEQYNSTYRVVSVLTVLHQDWLNGKEYKCKVSNKALPLPEEKTISKAKGQPREPQVYTLPPSREEMTKNQVSLTCLVKGFYPSDIAVEWESNGQPENNYKTTPPVLDSDGSFFLYSKLTVDKSRW QQGNVFSCSVMHEALHNHYTQKSLSLSPGK

F022-59-hIgG1(DLE)輕鏈可變區的氨基酸序列(SEQ ID No.49): DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELKRTVAAPSVFIFPPSDEQLKSGTASVVCLLNNFYPREAKVQWKVDNALQSGNSQESVTEQDSKDSTYSLSSTLTLSKADYEKHKVYACEVTHQGLSSPVTKSFNRGEC Amino acid sequence of F022-59-hIgG1 (DLE) light chain variable region (SEQ ID No. 49): DIVMTQAAPSVPVTPGESVSISCRSSKSLLHSNGNTYLYWFLQRPGQSPQLLIYRMSNLASGVPDRFSGSGSGTVFTLRISRVEAEDVGVYYCMQHLEYPFTFGAGTKLELKRTVAAPSVFIFPPSDEQLKSGTASVVCLLNNFYPREAKVQW KVDNALQSGNSQESVTEQDSKDSTYSLSSTLTLSKADYEKHKVYACEVTHQGLSSPVTKSFNRGEC

另外,陽性對照抗體4A19-mIgG2a(WO2021194942A1專利中的4A19抗體可變區連接mIgG2a恒定區獲得)的氨基酸序列如下:In addition, the amino acid sequence of the positive control antibody 4A19-mIgG2a (obtained by connecting the variable region of the 4A19 antibody in the WO2021194942A1 patent to the mIgG2a constant region) is as follows:

4A19-mIgG2a重鏈的氨基酸序列(SEQ ID No.50): QVQLVQSGAEVKKPGASVKVSCKASGYTFTDSEMHWVRQATGQGLEWMGAIQPETGGTAYNQKFKARVTMTRDTSISTAYMELSSLRSEDTAVYYCARRRRNFDYWGQGTLVTVSSAKTTAPSVYPLAPVCGDTTGSSVTLGCLVKGYFPEPVTLTWNSGSLSSGVHTFPAVLQSDLYTLSSSVTVTSSTWPSQSITCNVAHPASSTKVDKKIEPRGPTIKPCPPCKCPAPNLLGGPSVFIFPPKIKDVLMISLSPIVTCVVVDVSEDDPDVQISWFVNNVEVHTAQTQTHREDYNSTLRVVSALPIQHQDWMSGKEFKCKVNNKDLPAPIERTISKPKGSVRAPQVYVLPPPEEEMTKKQVTLTCMVTDFMPEDIYVEWTNNGKTELNYKNTEPVLDSDGSYFMYSKLRVEKKNWVERNSYSCSVVHEGLHNHHTTKSFSRTPGK Amino acid sequence of 4A19-mIgG2a heavy chain (SEQ ID No. 50): QVQLVQSGAEVKKPGASVKVSCKASGYTFTDSEMHWVRQATGQGLEWMGAIQPETGGTAYNQKFKARVTMTRDTSISTAYMELSSLRSEDTAVYYCARRRRNFDYWGQGTLVTVSSAKTTAPSVYPLAPVCGDTTGSSVTLGCLVKGYFPEPVTLTWN SGSLSSGVHTFPAVLQSDLYTLSSSVTVTSSTWPSQSITCNVAHPASSTKVDKKIEPRGPTIKPC PPCKCPAPNLLGGPSVFIFPPKIKDVLMISLSPIVTCVVVDVSEDDPDVQISWFVNNVEVHTAQTQTHREDYNSTLRVVSALPIQHQDWMSGKEFKCKVNNKDLPAPIERTISKPKGSVRAPQVYVLPPPEEEMTKKQVTLTCMVTDFMPEDIYVEWTNNGKTELNYKNTEPVLDSDGSYFMYSKLRVEKKNWVERNSYSCSV VHEGLHNHHTTKSFSRTPGK

4A19-mIgG2a輕鏈的氨基酸序列(SEQ ID No.51): DIVMTQTPLSLSVTPGQPASISCRSSQSLFHSSGNTYLHWYLQKPGQPPQLLIYKVSNRFSGVPDRFSGSGSGTDFTLKISRVEAEDVGVYYCSQSTHVPFTFGQGTKLEIKRADAAPTVSIFPPSSEQLTSGGASVVCFLNNFYPKDINVKWKIDGSERQNGVLNSWTDQDSKDSTYSMSSTLTLTKDEYERHNSYTCEATHKTSTSPIVKSFNRNEC Amino acid sequence of 4A19-mIgG2a light chain (SEQ ID No. 51): DIVMTQTPLSLSVTPGQPASISCRSSQSLFHSSGNTYLHWYLQKPGQPPQLLIYKVSNRFSGVPDRFSGSGTDFTLKISRVEAEDVGVYYCSQSTHVPFTFGQGTKLEIKRADAAPTVSIFPPSSEQLTSGGASVVCFLNNFYPKDINVKW KIDGSERQNGVLNSWTDQDSKDSTYSMSSTLTLTKDEYERHNSYTCEATHKTSTSPIVKSFNRNEC

實施例Embodiment 4.4. anti- CCR8CCR8 抗體體外活性分析Antibody in vitro activity analysis

利用Lymphoprep(Axis-Shield)按照說明書的操作步驟分離外周血單個核細胞(PBMC)。利用EasySep Human CD4+CD127lowCD25+Regulatory T Cell Isolation Kit(Stem Cell)按照說明書的操作步驟分離PBMC中的Treg。分離好的Treg與Dynabeads Human T-Activator CD3/CD28(Gibco)按照1:1的比例混合,用完全培養基(90%X-VIVO 15+10%FBS+500IU/ml IL-2,X-VIVO 15:Lonza,FBS:Gibco,IL-2:四環生物)培養5到8天,活化擴增Treg細胞。分別通過流式細胞術檢測重組抗體與Raji-hCCR8、Treg(活化後),Raji,PBMC和Raji-hCCR4(Raji細胞過表現人CCR4)的結合活性。實驗方法同上述實施例2,mIgG2a亞型抗體使用PE標記的抗小鼠Fc二抗(Biolegend)檢測,hIgG1(DLE)亞型抗體使用Alexa Fluor 647標記的抗人Fab二抗(Jackson)檢測。實驗結果如圖2-6所示,重組抗體均展現出了與Raji-hCCR8(圖2)和Treg(圖3)的較強的結合活性。同時,重組抗體均不與Raji(圖4), PBMC(圖5)及Raji-hCCR4(圖6)結合,這說明本公開的抗CCR8抗體具有較好的特異性。Peripheral blood mononuclear cells (PBMCs) were isolated using Lymphoprep (Axis-Shield) according to the instructions. Tregs were isolated from PBMCs using EasySep Human CD4+CD127lowCD25+Regulatory T Cell Isolation Kit (Stem Cell) according to the instructions. The isolated Tregs were mixed with Dynabeads Human T-Activator CD3/CD28 (Gibco) at a ratio of 1:1 and cultured in complete medium (90% X-VIVO 15+10% FBS+500IU/ml IL-2, X-VIVO 15: Lonza, FBS: Gibco, IL-2: Tetracycline) for 5 to 8 days to activate and expand Treg cells. The binding activity of the recombinant antibodies to Raji-hCCR8, Treg (after activation), Raji, PBMC and Raji-hCCR4 (Raji cells overexpressing human CCR4) was detected by flow cytometry. The experimental method was the same as that in Example 2 above. The mIgG2a subtype antibody was detected using a PE-labeled anti-mouse Fc secondary antibody (Biolegend), and the hIgG1 (DLE) subtype antibody was detected using an Alexa Fluor 647-labeled anti-human Fab secondary antibody (Jackson). The experimental results are shown in Figures 2-6. The recombinant antibodies all showed strong binding activity to Raji-hCCR8 (Figure 2) and Treg (Figure 3). Meanwhile, the recombinant antibodies did not bind to Raji ( FIG. 4 ), PBMC ( FIG. 5 ) and Raji-hCCR4 ( FIG. 6 ), which indicates that the anti-CCR8 antibody disclosed in the present invention has good specificity.

另外,在NK-92細胞中通過表現hCD16分子(NK-92-hCD16)用以檢測抗體介導的ADCC功能。用CFSE對Jurkat-hCCR8細胞(Jurkat,人外周血白血病T細胞系,ATCC)進行染色。按2E4/孔的密度將Jurkat-hCCR8細胞加入96孔盤中。按1E5/孔的密度將NK-92-hCD16細胞加入96孔盤中,隨後加入抗具有hIgG1 Fc(DLE)的抗CCR8抗體,37度培育6小時。取出96孔盤加入PI染色,通過流式細胞術檢測CSFE及PI螢光,計算PI、CFSE雙陽性的細胞在CFSE陽性細胞群中的比例,即為細胞殺傷率。實驗結果如圖7所示,所有重組抗體均展示出優秀的ADCC活性。In addition, antibody-mediated ADCC function was detected by expressing hCD16 molecules (NK-92-hCD16) in NK-92 cells. Jurkat-hCCR8 cells (Jurkat, human peripheral blood leukemia T cell line, ATCC) were stained with CFSE. Jurkat-hCCR8 cells were added to a 96-well plate at a density of 2E4/well. NK-92-hCD16 cells were added to a 96-well plate at a density of 1E5/well, followed by the addition of anti-CCR8 antibody with hIgG1 Fc (DLE) and incubation at 37 degrees for 6 hours. The 96-well plate was taken out and PI was added for staining. CSFE and PI fluorescence were detected by flow cytometry. The ratio of PI and CFSE double-positive cells in the CFSE-positive cell population was calculated, which was the cell killing rate. The experimental results are shown in Figure 7. All recombinant antibodies showed excellent ADCC activity.

實施例Embodiment 5.5. anti- CCR8CCR8 抗體體內活性分析Antibody in vivo activity analysis

為驗證抗CCR8抗體的體內藥效,在hCCR8敲入小鼠(B-hCCR8,百奧塞圖)中皮下注射MC38細胞(3E5/隻),建立腫瘤模型。在腫瘤接種第7天,將F022-7-mIgG2a,F022-59-mIgG2a,F022-75-mIgG2a抗體進行靜脈注射給藥,同時以同型無關靶點抗體作為陰性對照,以4A19-mIgG2a為陽性對照。給藥劑量為10mg/kg,一周給藥2次,共給藥6次。每週測量兩次小鼠腫瘤體積,按照腫瘤體積=腫瘤長徑×腫瘤短徑×腫瘤短徑/2計算。腫瘤接種34天後,計算小鼠腫瘤抑制率,抑制率按公式計算:[1-(治療組給藥後瘤體積-治療組給藥前瘤體積) / (對照組給藥後瘤體積 -對照組給藥前瘤體積)]×100%。實驗結果見表3及附圖8所示,重組抗體在體內均有顯著的抗腫瘤作用。To verify the in vivo efficacy of anti-CCR8 antibodies, MC38 cells (3E5/mouse) were subcutaneously injected into hCCR8 knock-in mice (B-hCCR8, Biocytogen) to establish a tumor model. On the 7th day after tumor inoculation, F022-7-mIgG2a, F022-59-mIgG2a, and F022-75-mIgG2a antibodies were intravenously injected, and isotype-independent target antibodies were used as negative controls, and 4A19-mIgG2a was used as a positive control. The dosage was 10 mg/kg, and the drug was administered twice a week for a total of 6 times. The tumor volume of mice was measured twice a week and calculated according to tumor volume = tumor long diameter × tumor short diameter × tumor short diameter/2. 34 days after tumor inoculation, the tumor inhibition rate of mice was calculated according to the formula: [1-(tumor volume of the treatment group after drug administration - tumor volume of the treatment group before drug administration) / (tumor volume of the control group after drug administration - tumor volume of the control group before drug administration)] × 100%. The experimental results are shown in Table 3 and Figure 8. The recombinant antibodies have significant anti-tumor effects in vivo.

表3. 抗CCR8抗體抑制腫瘤生長實驗結果表 組別 腫瘤平均體積(mm 3 腫瘤生長抑制(TGI, %) Isotype-mIgG2a 3353.71 / F022-7-mIgG2a 1610.05 53.32 F022-59-mIgG2a 1242.16 64.6 F022-75-mIgG2a 1803.5 47.42 4A19-mIgG2a 2534.92 25.07 Table 3. Results of the anti-CCR8 antibody inhibition of tumor growth experiment Group Average tumor volume (mm 3 ) Tumor growth inhibition (TGI, %) Isotype-mIgG2a 3353.71 / F022-7-mIgG2a 1610.05 53.32 F022-59-mIgG2a 1242.16 64.6 F022-75-mIgG2a 1803.5 47.42 4A19-mIgG2a 2534.92 25.07

以上所述僅為本公開的優選實施例而已,並不用於限制本公開,對於本領域的技術人員來說,本公開可以有各種更改和變化。凡在本公開的精神和原則之內,所作的任何修改、等同替換、改進等,均應包含在本公開的保護範圍之內。The above is only a preferred embodiment of the disclosure and is not intended to limit the disclosure. For those skilled in the art, the disclosure may be subject to various modifications and changes. Any modification, equivalent replacement, improvement, etc. made within the spirit and principles of the disclosure shall be included in the protection scope of the disclosure.

without

為了更清楚地說明本發明實施例的技術方案,下面將對實施例中所需要使用的附圖作簡單地介紹,應當理解,以下附圖僅示出了本發明的某些實施例,因此不應被看作是對範圍的限定,對於本領域普通技術人員來講,在不付出創造性勞動的前提下,還可以根據這些附圖獲得其他相關的附圖。 圖1為雜交瘤純化抗體與Raji-hCCR8的結合檢測結果圖。 圖2為重組抗體與Raji-hCCR8的結合檢測結果圖。 圖3為重組抗體與Treg的結合檢測結果圖。 圖4為重組抗體與Raji的結合檢測結果圖。 圖5為重組抗體與PBMC的結合檢測結果圖。 圖6為重組抗體與Raji-hCCR4的結合檢測結果圖。 圖7為重組抗體ADCC活性實驗結果圖。 圖8抗CCR8抗體抑制腫瘤生長實驗結果圖。 In order to more clearly illustrate the technical solutions of the embodiments of the present invention, the following will briefly introduce the figures required for use in the embodiments. It should be understood that the following figures only show certain embodiments of the present invention and should not be regarded as limiting the scope. For ordinary technicians in this field, other relevant figures can be obtained based on these figures without creative work. Figure 1 is a diagram showing the binding test results of hybridoma purified antibodies and Raji-hCCR8. Figure 2 is a diagram showing the binding test results of recombinant antibodies and Raji-hCCR8. Figure 3 is a diagram showing the binding test results of recombinant antibodies and Treg. Figure 4 is a diagram showing the binding test results of recombinant antibodies and Raji. Figure 5 is a diagram showing the binding test results of recombinant antibodies and PBMC. Figure 6 is a graph showing the binding test results of the recombinant antibody and Raji-hCCR4. Figure 7 is a graph showing the ADCC activity test results of the recombinant antibody. Figure 8 is a graph showing the results of the anti-CCR8 antibody inhibition of tumor growth test results.

TW202423987A_112147381_SEQL.xmlTW202423987A_112147381_SEQL.xml

Claims (16)

一種抗人CCR8抗體,所述抗人CCR8抗體包含重鏈可變區和輕鏈可變區,所述重鏈可變區包括SEQ ID No.3、1、5、7、9或11中的HCDR1、HCDR2和HCDR3,和/或所述抗人CCR8抗體的輕鏈可變區包括SEQ ID No.4、2、6、8、10或12中的LCDR1、LCDR2和LCDR3。An anti-human CCR8 antibody, comprising a heavy chain variable region and a light chain variable region, wherein the heavy chain variable region includes HCDR1, HCDR2 and HCDR3 in SEQ ID No.3, 1, 5, 7, 9 or 11, and/or the light chain variable region of the anti-human CCR8 antibody includes LCDR1, LCDR2 and LCDR3 in SEQ ID No.4, 2, 6, 8, 10 or 12. 如請求項1所述的抗人CCR8抗體,其中 所述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3由IMGT編號系統定義,或由Kabat編號系統定義,或由Chothia 編號系統定義,或由Contact編號系統定義,或由AbM編號系統定義; 可選地, A. 所述抗人CCR8抗體的所述重鏈可變區包括所述SEQ ID No.3中的所述HCDR1、HCDR2和HCDR3,並且所述抗人CCR8抗體的所述輕鏈可變區包括所述SEQ ID No.4中的所述LCDR1、LCDR2和LCDR3; B. 所述抗人CCR8抗體的所述重鏈可變區包括所述SEQ ID No.1中的所述HCDR1、HCDR2和HCDR3,並且所述抗人CCR8抗體的所述輕鏈可變區包括所述SEQ ID No.2中的所述LCDR1、LCDR2和LCDR3; C. 所述抗人CCR8抗體的所述重鏈可變區包括所述SEQ ID No.5中的所述HCDR1、HCDR2和HCDR3,並且所述抗人CCR8抗體的所述輕鏈可變區包括所述SEQ ID No.6中的所述LCDR1、LCDR2和LCDR3; D. 所述抗人CCR8抗體的所述重鏈可變區包括所述SEQ ID No.7中的所述HCDR1、HCDR2和HCDR3,並且所述抗人CCR8抗體的所述輕鏈可變區包括所述SEQ ID No.8中所述的LCDR1、LCDR2和LCDR3; E. 所述抗人CCR8抗體的所述重鏈可變區包括所述SEQ ID No.9中的所述HCDR1、HCDR2和HCDR3,並且所述抗人CCR8抗體的所述輕鏈可變區包括所述SEQ ID No.10中的所述LCDR1、LCDR2和LCDR3;或者 F. 所述抗人CCR8抗體的所述重鏈可變區包括所述SEQ ID No.11中的所述HCDR1、HCDR2和HCDR3,並且所述抗人CCR8抗體的所述輕鏈可變區包括所述SEQ ID No.12中的所述LCDR1、LCDR2和LCDR3; 可選地,所述HCDR1、HCDR2、HCDR3、LCDR1、LCDR2和LCDR3由IMGT編號系統定義; 可選地,所述的抗人CCR8抗體,其中, a. 所述重鏈可變區的所述HCDR1包含SEQ ID NO.19的氨基酸序列,所述HCDR2包含SEQ ID NO.20的氨基酸序列,和所述HCDR3包含SEQ ID NO.21的氨基酸序列;並且所述輕鏈可變區的所述LCDR1包含SEQ ID NO.16的氨基酸序列,所述LCDR2包含SEQ ID NO.17的氨基酸序列,和所述LCDR3包含SEQ ID NO.18的氨基酸序列; b. 所述重鏈可變區的所述HCDR1包含SEQ ID NO.13的氨基酸序列,所述HCDR2包含SEQ ID NO.14的氨基酸序列,和所述HCDR3包含SEQ ID NO.15的氨基酸序列;並且所述輕鏈可變區的所述LCDR1包含所述SEQ ID NO.16的氨基酸序列,所述LCDR2包含所述SEQ ID NO.17的所述氨基酸序列,和所述LCDR3包含所述SEQ ID NO.18的氨基酸序列; c. 所述重鏈可變區的所述HCDR1包含SEQ ID NO.22的氨基酸序列,所述HCDR2包含SEQ ID NO.23的氨基酸序列,和所述HCDR3包含SEQ ID NO.24的氨基酸序列;並且所述輕鏈可變區的所述LCDR1包含SEQ ID NO.25的氨基酸序列,所述LCDR2包含SEQ ID NO.26的氨基酸序列,和所述LCDR3包含SEQ ID NO.27的氨基酸序列; d. 所述重鏈可變區的所述HCDR1包含所述SEQ ID NO.13的氨基酸序列,所述HCDR2包含SEQ ID NO.28的氨基酸序列,和所述HCDR3包含SEQ ID NO.29的氨基酸序列;並且所述輕鏈可變區的所述LCDR1包含所述SEQ ID NO.16的氨基酸序列,所述LCDR2包含SEQ ID NO.30的氨基酸序列,和所述LCDR3包含所述SEQ ID NO.18的氨基酸序列; e. 所述重鏈可變區的所述HCDR1包含SEQ ID NO.31的氨基酸序列,所述HCDR2包含SEQ ID NO.32的氨基酸序列,和所述HCDR3包含SEQ ID NO.33的氨基酸序列;並且所述輕鏈可變區的所述LCDR1包含SEQ ID NO.34的氨基酸序列,所述LCDR2包含SEQ ID NO.35的氨基酸序列,和所述LCDR3包含SEQ ID NO.36的氨基酸序列;或 f. 所述重鏈可變區的所述HCDR1包含所述SEQ ID NO.13的所述氨基酸序列,所述HCDR2包含SEQ ID NO.37的氨基酸序列,和所述HCDR3包含SEQ ID NO.38的氨基酸序列;並且所述輕鏈可變區的所述LCDR1包含所述SEQ ID NO.16的所述氨基酸序列,所述LCDR2包含所述SEQ ID NO.17的所述氨基酸序列,和所述LCDR3包含所述SEQ ID NO.18的所述氨基酸序列; 可選地, A. 所述抗人CCR8抗體包含分別如所述SEQ ID NO.19、所述SEQ ID NO.20和所述SEQ ID NO.21所示的所述HCDR1、所述HCDR2和所述HCDR3,以及分別如所述SEQ ID NO.16、所述SEQ ID NO.17和所述SEQ ID NO.18所示的所述LCDR1、所述LCDR2和所述LCDR3; B. 所述抗人CCR8抗體包含分別所述如SEQ ID NO.13、所述SEQ ID NO.14和所述SEQ ID NO.15所示的所述HCDR1、所述HCDR2和所述HCDR3,以及分別如所述SEQ ID NO.16、所述SEQ ID NO.17和所述SEQ ID NO.18所示的所述LCDR1、所述LCDR2和所述LCDR3;或者 C.所述抗人CCR8抗體包含分別如所述SEQ ID NO.22、所述SEQ ID NO.23和所述SEQ ID NO.24所示的所述HCDR1、所述HCDR2和所述HCDR3,以及分別如所述SEQ ID NO.25、所述SEQ ID NO.26和所述SEQ ID NO.27所示的所述LCDR1、所述LCDR2和所述LCDR3。 An anti-human CCR8 antibody as described in claim 1, wherein the HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined by the IMGT numbering system, or by the Kabat numbering system, or by the Chothia numbering system, or by the Contact numbering system, or by the AbM numbering system; Optionally, A. the heavy chain variable region of the anti-human CCR8 antibody includes the HCDR1, HCDR2 and HCDR3 in the SEQ ID No.3, and the light chain variable region of the anti-human CCR8 antibody includes the LCDR1, LCDR2 and LCDR3 in the SEQ ID No.4; B. the heavy chain variable region of the anti-human CCR8 antibody includes the SEQ ID No.1, and the light chain variable region of the anti-human CCR8 antibody includes the LCDR1, LCDR2 and LCDR3 in SEQ ID No.2; C. The heavy chain variable region of the anti-human CCR8 antibody includes the HCDR1, HCDR2 and HCDR3 in SEQ ID No.5, and the light chain variable region of the anti-human CCR8 antibody includes the LCDR1, LCDR2 and LCDR3 in SEQ ID No.6; D. The heavy chain variable region of the anti-human CCR8 antibody includes the HCDR1, HCDR2 and HCDR3 in SEQ ID No.7, and the light chain variable region of the anti-human CCR8 antibody includes the LCDR1, LCDR2 and LCDR3 in SEQ ID No.8; E. The heavy chain variable region of the anti-human CCR8 antibody includes the SEQ ID No.9, and the light chain variable region of the anti-human CCR8 antibody includes the LCDR1, LCDR2 and LCDR3 in SEQ ID No.10; or F. The heavy chain variable region of the anti-human CCR8 antibody includes the HCDR1, HCDR2 and HCDR3 in SEQ ID No.11, and the light chain variable region of the anti-human CCR8 antibody includes the LCDR1, LCDR2 and LCDR3 in SEQ ID No.12; Optionally, the HCDR1, HCDR2, HCDR3, LCDR1, LCDR2 and LCDR3 are defined by the IMGT numbering system; Optionally, the anti-human CCR8 antibody, wherein, a. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.19, and the HCDR2 comprises the amino acid sequence of SEQ ID NO.20, and the HCDR3 comprises the amino acid sequence of SEQ ID NO.21; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, the LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and the LCDR3 comprises the amino acid sequence of SEQ ID NO.18; b. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, the HCDR2 comprises the amino acid sequence of SEQ ID NO.14, and the HCDR3 comprises the amino acid sequence of SEQ ID NO.15; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, the LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and the LCDR3 comprises the amino acid sequence of SEQ ID NO.18; c. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.22, the HCDR2 comprises the amino acid sequence of SEQ ID NO. NO.23, and the HCDR3 comprises the amino acid sequence of SEQ ID NO.24; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.25, the LCDR2 comprises the amino acid sequence of SEQ ID NO.26, and the LCDR3 comprises the amino acid sequence of SEQ ID NO.27; d. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, the HCDR2 comprises the amino acid sequence of SEQ ID NO.28, and the HCDR3 comprises the amino acid sequence of SEQ ID NO.29; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, the LCDR2 comprises the amino acid sequence of SEQ ID NO.30, and the LCDR3 comprises the amino acid sequence of SEQ ID NO.18; e. The HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.31, the HCDR2 comprises the amino acid sequence of SEQ ID NO. NO.32, and the HCDR3 comprises the amino acid sequence of SEQ ID NO.33; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.34, the LCDR2 comprises the amino acid sequence of SEQ ID NO.35, and the LCDR3 comprises the amino acid sequence of SEQ ID NO.36; or f. the HCDR1 of the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.13, the HCDR2 comprises the amino acid sequence of SEQ ID NO.37, and the HCDR3 comprises the amino acid sequence of SEQ ID NO.38; and the LCDR1 of the light chain variable region comprises the amino acid sequence of SEQ ID NO.16, the LCDR2 comprises the amino acid sequence of SEQ ID NO.17, and the LCDR3 comprises the amino acid sequence of SEQ ID NO.18; Optionally, A. the anti-human CCR8 antibody comprises SEQ ID NO.19, SEQ ID NO.20 and SEQ ID NO.21, and the LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.17 and SEQ ID NO.18, respectively; B. The anti-human CCR8 antibody comprises the HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.13, SEQ ID NO.14 and SEQ ID NO.15, and the LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.16, SEQ ID NO.17 and SEQ ID NO.18, respectively; or C. The anti-human CCR8 antibody comprises the HCDR1, HCDR2 and HCDR3 as shown in SEQ ID NO.22, SEQ ID NO.23 and SEQ ID NO.24, and the LCDR1, LCDR2 and LCDR3 as shown in SEQ ID NO.25, SEQ ID NO.26 and SEQ ID NO. The LCDR1, LCDR2 and LCDR3 shown in NO.27. 如請求項1-2中任一項之所述的抗人CCR8抗體,其中所述抗人CCR8抗體為鼠源抗體,嵌合抗體或人源化抗體。The anti-human CCR8 antibody as described in any one of claims 1-2, wherein the anti-human CCR8 antibody is a murine antibody, a chimeric antibody or a humanized antibody. 一種抗人CCR8抗體,其中,所述抗人CCR8抗體的重鏈可變區包括與SEQ ID No.3、1、5、7、9或11具有至少90%序列同一性的氨基酸序列,和/或輕鏈可變區包括與SEQ ID No.4、2、6、8、10或12具有至少90%序列同一性的氨基酸序列; 可選地, (i)所述重鏈可變區包含SEQ ID NO.3的氨基酸序列,和所述輕鏈可變區包含所述SEQ ID NO.4的氨基酸序列; (ii)所述重鏈可變區包含所述SEQ ID NO.1的氨基酸序列,和所述輕鏈可變區包含所述SEQ ID NO.2的氨基酸序列; (iii)所述重鏈可變區包含所述SEQ ID NO.5的氨基酸序列,和所述輕鏈可變區包含所述SEQ ID NO.6的氨基酸序列; (iv)所述重鏈可變區包含所述SEQ ID NO.7的氨基酸序列,和所述輕鏈可變區包含所述SEQ ID NO.8的氨基酸序列; (v)所述重鏈可變區包含所述SEQ ID NO.9的氨基酸序列,和所述輕鏈可變區包含所述SEQ ID NO.10的氨基酸序列;或 (vi)所述重鏈可變區包含所述SEQ ID NO.11的氨基酸序列,和所述輕鏈可變區包含所述SEQ ID NO.12的氨基酸序列。 An anti-human CCR8 antibody, wherein the heavy chain variable region of the anti-human CCR8 antibody comprises an amino acid sequence having at least 90% sequence identity with SEQ ID No.3, 1, 5, 7, 9 or 11, and/or the light chain variable region comprises an amino acid sequence having at least 90% sequence identity with SEQ ID No.4, 2, 6, 8, 10 or 12; Optionally, (i) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.3, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.4; (ii) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.1, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.2; (iii) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.5, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.6; (iv) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.7, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.8; (v) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.9, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.10; or (vi) the heavy chain variable region comprises the amino acid sequence of SEQ ID NO.11, and the light chain variable region comprises the amino acid sequence of SEQ ID NO.12. 如請求項1-4中任一項之所述的抗人CCR8抗體,所述抗人CCR8抗體還包含恒定區; 可選地,所述抗人CCR8抗體的重鏈恒定區選自IgG1、IgG2、IgG3和IgG4的重鏈恒定區,輕鏈恒定區選自κ或λ鏈恒定區; 可選地,所述恒定區的種屬來源為鼠或人; 可選地,所述重鏈恒定區為鼠IgG2a恒定區、鼠IgG1恒定區或人IgG1恒定區,和/或所述輕鏈恒定區為鼠κ恒定區或人κ恒定區; 可選地,所述重鏈恒定區為人IgG1(DE)或人IgG1(DLE)恒定區; 可選地,所述重鏈恒定區包括SEQ ID NO.39、41或42的氨基酸序列,所述輕鏈恒定區包括SEQ ID NO.40或43的氨基酸序列; 可選地,所述抗人CCR8抗體重鏈包含SEQ ID NO.46的氨基酸序列,所述抗人CCR8抗體輕鏈包括SEQ ID NO.47的氨基酸序列;或者 所述抗人CCR8抗體重鏈包含SEQ ID NO.44的氨基酸序列,所述抗人CCR8抗體輕鏈包括SEQ ID NO.45的氨基酸序列;或者 所述抗人CCR8抗體重鏈包含SEQ ID NO.48的氨基酸序列,所述抗人CCR8抗體輕鏈包括SEQ ID NO.49的氨基酸序列。 The anti-human CCR8 antibody as described in any one of claims 1-4, wherein the anti-human CCR8 antibody further comprises a constant region; Optionally, the heavy chain constant region of the anti-human CCR8 antibody is selected from the heavy chain constant regions of IgG1, IgG2, IgG3 and IgG4, and the light chain constant region is selected from the κ or λ chain constant region; Optionally, the species of the constant region is mouse or human; Optionally, the heavy chain constant region is a mouse IgG2a constant region, a mouse IgG1 constant region or a human IgG1 constant region, and/or the light chain constant region is a mouse κ constant region or a human κ constant region; Optionally, the heavy chain constant region is a human IgG1 (DE) or a human IgG1 (DLE) constant region; Optionally, the heavy chain constant region comprises the amino acid sequence of SEQ ID NO.39, 41 or 42, and the light chain constant region comprises the amino acid sequence of SEQ ID NO. NO.40 or 43; Optionally, the anti-human CCR8 antibody heavy chain comprises the amino acid sequence of SEQ ID NO.46, and the anti-human CCR8 antibody light chain comprises the amino acid sequence of SEQ ID NO.47; or The anti-human CCR8 antibody heavy chain comprises the amino acid sequence of SEQ ID NO.44, and the anti-human CCR8 antibody light chain comprises the amino acid sequence of SEQ ID NO.45; or The anti-human CCR8 antibody heavy chain comprises the amino acid sequence of SEQ ID NO.48, and the anti-human CCR8 antibody light chain comprises the amino acid sequence of SEQ ID NO.49. 如請求項1-4中任一項之所述的抗人CCR8抗體,所述抗人CCR8抗體為全長抗體或為選自F(ab’)2、Fab’-SH、Fab’、Fab、scFab 、dsFv、(dsFv)2、Fv和scFv中的任意一種抗原結合片段。The anti-human CCR8 antibody as described in any one of claims 1 to 4, wherein the anti-human CCR8 antibody is a full-length antibody or any antigen-binding fragment selected from F(ab’)2, Fab’-SH, Fab’, Fab, scFab, dsFv, (dsFv)2, Fv and scFv. 一種與如請求項1-6中任一項之所述的抗人CCR8抗體競爭性結合人CCR8的抗體,或一種與如請求項1-6中任一項之所述的抗人CCR8抗體結合相同表位的抗體。An antibody that competitively binds to human CCR8 as the anti-human CCR8 antibody as described in any one of claims 1 to 6, or an antibody that binds to the same epitope as the anti-human CCR8 antibody as described in any one of claims 1 to 6. 如請求項1-7中任一項之所述的抗人CCR8抗體,其中所述抗人CCR8抗體具有以下特性中的至少一種: A. 能與人CCR8特異性結合;可選地,其能以≤5nM的EC50值與表現人CCR8的Raji細胞結合,其中,所述EC50值通過流式細胞分析法測定; B. 具有抑制腫瘤生長功能; C. 具有ADCC(Antibody-dependent cellular cytotoxicity)活性。 An anti-human CCR8 antibody as described in any one of claims 1-7, wherein the anti-human CCR8 antibody has at least one of the following properties: A. It can specifically bind to human CCR8; optionally, it can bind to Raji cells expressing human CCR8 with an EC50 value of ≤5nM, wherein the EC50 value is determined by flow cytometry; B. It has the function of inhibiting tumor growth; C. It has ADCC (Antibody-dependent cellular cytotoxicity) activity. 一種多特異性抗體,所述多特異性抗體包含如請求項1-8中任一項之所述的抗人CCR8抗體。A multispecific antibody, comprising the anti-human CCR8 antibody as described in any one of claims 1-8. 一種抗體偶聯物,所述抗體偶聯物包括如請求項1-8中任一項之所述的抗人CCR8抗體。An antibody conjugate, comprising the anti-human CCR8 antibody as described in any one of claims 1 to 8. 一種嵌合抗原受體(CAR),所述嵌合抗原受體包括抗原結合結構域,所述抗原結合結構域包括如請求項1-8中任一項之所述的抗人CCR8抗體。A chimeric antigen receptor (CAR), comprising an antigen binding domain, wherein the antigen binding domain comprises the anti-human CCR8 antibody as described in any one of claims 1-8. 一種CAR-免疫細胞,所述CAR-免疫細胞表現如請求項11所述的嵌合抗原受體。A CAR-immune cell, wherein the CAR-immune cell expresses the chimeric antigen receptor as described in claim 11. 一種分離的核酸,其編碼如請求項1-8中任一項之所述的抗人CCR8抗體。An isolated nucleic acid encoding the anti-human CCR8 antibody as described in any one of claims 1-8. 一種細胞,其含有如請求項13所述的核酸。A cell comprising the nucleic acid of claim 13. 一種藥物組合物,其包含如請求項1-8中任一項之所述的抗人CCR8抗體、如請求項9所述的多特異性抗體、如請求項10所述的抗體偶聯物、如請求項12所述的CAR-免疫細胞的或如請求項13所述的核酸;可選地,其還包含一種或多種藥學上可接受的載體、稀釋劑或賦形劑。A drug composition comprising an anti-human CCR8 antibody as described in any one of claims 1-8, a multispecific antibody as described in claim 9, an antibody conjugate as described in claim 10, a CAR-immune cell as described in claim 12, or a nucleic acid as described in claim 13; optionally, it also comprises one or more pharmaceutically acceptable carriers, diluents or excipients. 如請求項1-8中任一項之所述的抗人CCR8抗體、如請求項9所述的多特異性抗體、如請求項10所述的抗體偶聯物、如請求項12所述的CAR-免疫細胞的、如請求項13所述的核酸或如請求項15所述的藥物組合物,在製備具有以下至少一種用途的產品中的應用:診斷人CCR8表現異常的相關疾病、治療所述人CCR8表現異常的相關疾病或檢測人CCR8的表現;可選地,所述人CCR8表現異常的相關疾病為腫瘤;可選地,所述腫瘤為乳腺癌、卵巢癌、腎癌、胰腺癌、膀胱癌、胃癌、宮頸癌、結腸癌、肉瘤、肝癌或肺癌。Use of the anti-human CCR8 antibody as described in any one of claims 1-8, the multispecific antibody as described in claim 9, the antibody conjugate as described in claim 10, the CAR-immune cell as described in claim 12, the nucleic acid as described in claim 13 or the drug composition as described in claim 15 in the preparation of a product having at least one of the following uses: diagnosing a disease related to abnormal expression of human CCR8, treating a disease related to abnormal expression of human CCR8 or detecting the expression of human CCR8; optionally, the disease related to abnormal expression of human CCR8 is a tumor; optionally, the tumor is breast cancer, ovarian cancer, kidney cancer, pancreatic cancer, bladder cancer, gastric cancer, cervical cancer, colon cancer, sarcoma, liver cancer or lung cancer.
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