JPS5953264B2 - Method for producing novel α-aminooxycarboxylic acid hydrazide derivative - Google Patents
Method for producing novel α-aminooxycarboxylic acid hydrazide derivativeInfo
- Publication number
- JPS5953264B2 JPS5953264B2 JP57052368A JP5236882A JPS5953264B2 JP S5953264 B2 JPS5953264 B2 JP S5953264B2 JP 57052368 A JP57052368 A JP 57052368A JP 5236882 A JP5236882 A JP 5236882A JP S5953264 B2 JPS5953264 B2 JP S5953264B2
- Authority
- JP
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- Prior art keywords
- formula
- group
- acid
- melting point
- elemental analysis
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
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Classifications
-
- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07C—ACYCLIC OR CARBOCYCLIC COMPOUNDS
- C07C243/00—Compounds containing chains of nitrogen atoms singly-bound to each other, e.g. hydrazines, triazanes
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P31/00—Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
- A61P31/04—Antibacterial agents
-
- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61P—SPECIFIC THERAPEUTIC ACTIVITY OF CHEMICAL COMPOUNDS OR MEDICINAL PREPARATIONS
- A61P31/00—Antiinfectives, i.e. antibiotics, antiseptics, chemotherapeutics
- A61P31/04—Antibacterial agents
- A61P31/06—Antibacterial agents for tuberculosis
-
- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D307/00—Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom
- C07D307/02—Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom not condensed with other rings
- C07D307/34—Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members
- C07D307/56—Heterocyclic compounds containing five-membered rings having one oxygen atom as the only ring hetero atom not condensed with other rings having two or three double bonds between ring members or between ring members and non-ring members with hetero atoms or with carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals, directly attached to ring carbon atoms
- C07D307/70—Nitro radicals
- C07D307/71—Nitro radicals attached in position 5
- C07D307/72—Nitro radicals attached in position 5 with hydrocarbon radicals, substituted by nitrogen-containing radicals, attached in position 2
- C07D307/73—Nitro radicals attached in position 5 with hydrocarbon radicals, substituted by nitrogen-containing radicals, attached in position 2 by amino or imino, or substituted amino or imino radicals
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- Chemical & Material Sciences (AREA)
- Organic Chemistry (AREA)
- Health & Medical Sciences (AREA)
- Pharmacology & Pharmacy (AREA)
- Animal Behavior & Ethology (AREA)
- Chemical Kinetics & Catalysis (AREA)
- General Chemical & Material Sciences (AREA)
- Medicinal Chemistry (AREA)
- Nuclear Medicine, Radiotherapy & Molecular Imaging (AREA)
- Communicable Diseases (AREA)
- Veterinary Medicine (AREA)
- Life Sciences & Earth Sciences (AREA)
- Oncology (AREA)
- General Health & Medical Sciences (AREA)
- Public Health (AREA)
- Pulmonology (AREA)
- Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
- Plural Heterocyclic Compounds (AREA)
- Pyridine Compounds (AREA)
- Hydrogenated Pyridines (AREA)
- Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)
- Furan Compounds (AREA)
Description
【発明の詳細な説明】
本発明は新規置換α−アミノオキシ カルボン酸ヒドラ
ジド誘導体の製造方法に関する。DETAILED DESCRIPTION OF THE INVENTION The present invention relates to a method for producing novel substituted α-aminooxycarboxylic acid hydrazide derivatives.
本発明により製造される新規化合物は次式(I)の化合
物及びその酸付加塩である。The novel compounds produced by the present invention are compounds of the following formula (I) and acid addition salts thereof.
X二N−O−CH−Co−NH−NHZ(I)(式中、
Xはシクロペンチリデン基あるいは炭素数1〜5個のア
ルキル、フェニル、ハロフエニル、ヒドロキシフェニル
、ニトロフェニル、アミノフェニル、フリル及びニトロ
フリル基から選んだ少なくとも1個の置換基を有するメ
チレン基を表わし;Rは水素、ベンジル基又は随意にメ
チルチオ置換基を有する炭素数1〜5個のアルキル基を
表わし;Zはピリジンカルボン酸から誘導されたアシル
基を表わす。X2N-O-CH-Co-NH-NHZ(I) (in the formula,
X represents a cyclopentylidene group or a methylene group having at least one substituent selected from alkyl having 1 to 5 carbon atoms, phenyl, halophenyl, hydroxyphenyl, nitrophenyl, aminophenyl, furyl and nitrofuryl; R represents hydrogen, a benzyl group or an alkyl group having 1 to 5 carbon atoms optionally having a methylthio substituent; Z represents an acyl group derived from pyridinecarboxylic acid.
)本発明により製造される新規化合物は塩基性であり、
酸付加塩を形成し、従つて式()の化合物の酸付加塩の
製造法も本発明の範囲内に包含される。) The new compound produced by the present invention is basic;
Acid addition salts are formed and therefore processes for preparing acid addition salts of compounds of formula () are also encompassed within the scope of this invention.
式(1)の新規化合物は価値ある薬学的性質を有し、主
として抗結核剤として使用できる。The new compounds of formula (1) have valuable pharmaceutical properties and can be used primarily as antituberculous agents.
英国特許第1323170号明細書には、遊離又はアシ
ル置換アミノ基を有するある種の抗結核活性のα−アミ
ノオキシ カルボン酸ヒドラジドが記載されている。GB 1323170 describes certain anti-tuberculous active α-aminooxycarboxylic acid hydrazides having free or acyl substituted amino groups.
α−アミノオキシ カルボン酸とカルボニル化合物との
反応は以前から分析の目的で利用されてきた(J.Bl
Ol.Chem.リ』,539(1936)参照)。The reaction between α-aminooxycarboxylic acids and carbonyl compounds has long been used for analytical purposes (J.Bl.
Ol. Chem. 539 (1936)).
かかる反応で生成されるある種のシツフ塩基は植物生長
調整活性を有し(J.Am.Chem−SOc・立』,
718(1947)参照)、またあるものはビタミンK
と同様の作用する(英国特許第621934号明細書参
照)。J.Med.Chem.l,824(1964)
にはα−アミノオキシ酢酸及びα−アミノオキシ酢酸エ
チルのある種のアルドキシム及びケトキシムについて記
載されている。Certain Schiff bases produced in such reactions have plant growth regulating activity (J. Am. Chem-SOc.
718 (1947)), and some contain vitamin K.
(see British Patent No. 621,934). J. Med. Chem. l, 824 (1964)
describes certain aldoximes and ketoximes of α-aminooxyacetic acid and ethyl α-aminooxyacetate.
ある種のα−アミノオキシ カルボン酸から形成される
シツフ塩基は半合成ペニシリン誘導体の研究と関連して
ActaChemicaScandinavica9l
9ツ317(1965)に言ウ裁されている。しかしな
がら、これらの文献にはこれらのオキシム及びシツフ塩
基の生物学的作用については何ら言及されていない。H
elveticaChimicaActa′46p76
6(1963)には、ある種のアミノオキシカルボン酸
誘導体、特にシツフ塩基の誘導体の制菌活性を調べた結
果、種々の微生物に及ぼされる制菌活性は遊離のアミノ
オキシ基の存在に基因するものであると記述されている
。Schiff bases formed from certain α-aminooxycarboxylic acids have been studied at ActaChemica Scandinavica9l in connection with the study of semisynthetic penicillin derivatives.
It was judged in 9th 317 (1965). However, these documents do not mention anything about the biological effects of these oximes and Schiff bases. H
elveticaChimicaActa'46p76
6 (1963), as a result of investigating the bacteriostatic activity of certain aminooxycarboxylic acid derivatives, particularly derivatives of Schiff bases, it was found that the bacteriostatic activity exerted on various microorganisms is due to the presence of free aminooxy groups. It is described as something.
PrOgressinMedicinalChemis
try2i斗1348(1967)には種々のニトロフ
ルフリリデン鱒導体の制?作用について述べられている
が、それらの抗結核作用については何ら言及されていな
い。PrOgressinMedicinalChemis
Try2i Dou 1348 (1967) includes various nitrofurfurylidene conductor systems. effects are mentioned, but no mention is made of their antituberculous effects.
式(I)においてXがモノ置換メチレン基である場合、
その置換基はメチル、エチル、n−プロピル、イソプロ
ピル、n−ブチル、イソブチル又はペンチル基の如きア
ルキル基、随意にハロゲン、ヒドロキシ、ニトロ又はア
ミノ置換基を有するフエニル基あるいはフルフリル又は
ニトロフルフリル基であり得る。When X is a monosubstituted methylene group in formula (I),
The substituents are alkyl groups such as methyl, ethyl, n-propyl, isopropyl, n-butyl, isobutyl or pentyl groups, phenyl groups or furfuryl or nitrofurfuryl groups optionally with halogen, hydroxy, nitro or amino substituents. could be.
Xがジ置換メチレン基の場合にはこれらの置換基を2個
有する。Rは水素又はベンジル基あるいは随意にメチル
チオ置換基を有するエチル、プロピル、ブチル又はペン
チル基の如き炭素数1〜5個のアルキル基である。When X is a di-substituted methylene group, it has two of these substituents. R is hydrogen or an alkyl group of 1 to 5 carbon atoms such as benzyl group or ethyl, propyl, butyl or pentyl group optionally with a methylthio substituent.
Rが水素以外の基である式(1)の化合物は不整炭素原
子を含むので出発原料に応じて純枠な光学活性異性体又
はラセミ体の形で製造できる。ラセミ化合物はそれ自体
既知の方法で、例えば一対のジアステレオマ一塩の形成
により分割できる。前述の如く、zはピリジンカルボン
酸から誘導されるアシル基、例えばイソニコチノイル基
である。Since the compound of formula (1) in which R is a group other than hydrogen contains an asymmetric carbon atom, it can be produced in the form of a pure optically active isomer or a racemate depending on the starting material. Racemates can be resolved in a manner known per se, for example by forming a pair of diastereomeric monosalts. As mentioned above, z is an acyl group derived from pyridinecarboxylic acid, such as an isonicotinoyl group.
本発明によれば、式(1)の化合物は、式(I[):(
式中、X及びRは前記の意義を有し、wは水素、炭素数
1〜5個のアルキル基あるいは1個又は2個以上のハロ
ゲン又はニトロ置換基を有するフエニル基である)のシ
ツフ塩基を式():H2N−NHZ(111)(式中、
zはピリジンカルボン酸から誘導されるアシル基である
)のヒドラジン誘導体と反応させ、ついで所望ならば、
得られた塩基を常法によりその酸付加塩に転化するかあ
るいは得られた塩を常法によりその遊離塩基又は別の塩
に転化することによつて製造される。According to the invention, the compound of formula (1) is a compound of formula (I[):(
In the formula, X and R have the above-mentioned meanings, and w is hydrogen, an alkyl group having 1 to 5 carbon atoms, or a phenyl group having one or more halogen or nitro substituents). The formula (): H2N-NHZ (111) (in the formula,
z is an acyl group derived from pyridine carboxylic acid) and then, if desired,
They are prepared by converting the resulting base into its acid addition salt using conventional methods, or by converting the resulting salt into its free base or another salt using conventional methods.
式()の化合物において、置換基R′は水素、メチル、
エチル、プロピル、ブチル又はペンチルあるいは置換フ
エニル、例えばp−ニトロフエニル、トリクロロフエニ
ル、トリフルオロフエニル、ペンタクロロフエニル又は
ペンタフルオロフエニル基を表わす。In the compound of formula (), the substituent R' is hydrogen, methyl,
It represents ethyl, propyl, butyl or pentyl or substituted phenyl, such as p-nitrophenyl, trichlorophenyl, trifluorophenyl, pentachlorophenyl or pentafluorophenyl groups.
本発明により製造される化合物はすべて新規であるが、
出発物質は一部は公知であり、新規の出発物質は例えば
パンカリ一特許第160181号明細書に記載されるよ
うにあるいは後記の実施例で示されるように既知の方法
によつて製造できる。Although all the compounds produced by the present invention are new,
Some of the starting materials are known, and new starting materials can be prepared by known methods, for example as described in Pankali Patent No. 160,181 or as shown in the examples below.
本発明方法の好ましい実施態様においては、式()の活
性化エステル、好ましくはペンタクロロフエニルエステ
ル、即ちR′がエステル形成基、好ましくはペンタクロ
ロフエニル基である化合物又は式(Uf)のR′が水素
である酸のN,N′−ジシクロヘキシルカルボジイミド
を置換ヒドラジド、好ましくはイソニコチン酸ヒドラジ
ドと室温で有機溶剤、好ましくはジメチルホルムアミド
の存在下で反応させる。In a preferred embodiment of the process of the invention, activated esters of the formula (), preferably pentachlorophenyl esters, i.e. compounds in which R' is an ester-forming group, preferably a pentachlorophenyl group, or R' of the formula (Uf) are used. N,N'-dicyclohexylcarbodiimide, an acid in which is hydrogen, is reacted with a substituted hydrazide, preferably isonicotinic acid hydrazide, at room temperature in the presence of an organic solvent, preferably dimethylformamide.
反応混合物は1〜72時間、好ましくは16時間放置せ
しめ、ついで副生成物(例えばペンタクロロフエノール
又はN,N/−ジシタロヘキシル尿素)をろ過又は抽出
により除去し、混合物を蒸発させ、所要ならば生成物を
抽出又は晶出により精製する。本発明により製造される
化合物は優れた抗結核活性を有し、特にヒドラジン基上
にイソニコチノイル置換基を有する化合物が有効である
。The reaction mixture is allowed to stand for 1 to 72 hours, preferably 16 hours, then by-products (e.g. pentachlorophenol or N,N/-disitalohexyl urea) are removed by filtration or extraction and the mixture is evaporated to remove the product if necessary. The product is purified by extraction or crystallization. The compounds produced according to the present invention have excellent antituberculous activity, and compounds having an isonicotinoyl substituent on the hydrazine group are particularly effective.
5−ニトロフルフリリデン基を有する化合物はその顕著
なる抗結核活性の他に、ミコバクテリウム属の微生物の
耐性菌に対して有効であるという利点を有する。In addition to their remarkable antituberculous activity, compounds having a 5-nitrofurfurylidene group have the advantage of being effective against resistant microorganisms of the genus Mycobacterium.
本発明者の知る限りでは本発明により製造される化合物
は抗結核活性を有する最初の5−ニトロフルフリリデ7
誘導体である。本発明による新規化合物の試験管内試験
をアルブミン2.5(Fbを含む栄養培地上で行つた。To the best of the inventor's knowledge, the compounds prepared according to the present invention are the first 5-nitrofurfurylide 7 compounds with antituberculous activity.
It is a derivative. In vitro tests of the new compounds according to the invention were carried out on a nutrient medium containing albumin 2.5 (Fb).
供試化合物を含む培地に新鮮なバクテリア培養液0.0
1巧を接種し、37℃で3週間培養させた。ついで阻止
濃度を測定した。試験に用いたバクテリア菌はミコバク
テリウム ツベルクロシスH3,Rv(M.t.H3,
Rv)、イソニコチノイル ヒドラジド(INH)に耐
性のミコバクテリウム ツベルクロシス(M.t.)、
ストレプトマイシン(Strp.)に耐性のミコバクテ
リウム ツベルクロシス(M.t.)及びミコバクテリ
ウム カンサシイ(Kansasii)(M.t.)で
ある。得られた試験結果を第1表に示す。Add 0.0 of a fresh bacterial culture to the medium containing the test compound.
1 Takumi was inoculated and cultured at 37°C for 3 weeks. The inhibitory concentration was then measured. The bacteria used in the test were Mycobacterium tuberculosis H3, Rv (M.t.H3,
Rv), Mycobacterium tuberculosis (M.t.) resistant to isonicotinoyl hydrazide (INH),
Mycobacterium tuberculosis (M.t.) and Mycobacterium Kansasii (M.t.) resistant to streptomycin (Strp.). The test results obtained are shown in Table 1.
本発明により製造される化合牧は経口及び/又は非経口
投与用薬剤の形、例えば錠剤、被覆錠剤、注入性製剤、
坐薬等の形で治療に使用できる。The compounds produced according to the invention can be prepared in the form of pharmaceuticals for oral and/or parenteral administration, such as tablets, coated tablets, injectable preparations,
It can be used for treatment in the form of suppositories.
活性化合物の1日の投与量は哺乳動物の治療には約2〜
801!If/Kfl好ましくは10〜50111/Q
であることができ、この量は分割方式で又は遅効性方式
で添加できる。生成物の純度は薄層クロマトグラフイ一
により測定した。The daily dosage of active compound for the treatment of mammals is about 2 to
801! If/Kfl preferably 10-50111/Q
The amount can be added in portions or in a slow-release manner. Product purity was determined by thin layer chromatography.
実施例で示されるRf値は溶離剤としてn−ヘキサン、
氷酢酸及びクロロホルムの1:1:8混合物を用いてシ
リカゲル0G″(Stahl)上で測定したものである
。化合物の融点はDr.TOttOli型装置を用いて
測定した。得られた化合物の構造は場合により1.R.
,N.M.R.及び質量スペクトル分析によつて確認し
た。光学活性体の比施光度はオブトン(0pt0n)施
光計を用いて測定した。次に本発明を実施例により更に
説明する。The Rf values shown in the examples are based on n-hexane as the eluent,
Measured on silica gel 0G'' (Stahl) using a 1:1:8 mixture of glacial acetic acid and chloroform. The melting point of the compound was determined using a Dr. TOttOli type apparatus. In some cases 1.R.
,N. M. R. and confirmed by mass spectrometry. The specific optical density of the optically active substance was measured using an Obton (0pt0n) spectrophotometer. Next, the present invention will be further explained by examples.
実施例 1
N−(N″−5−ニトロフルフリリデン)−D−α−ア
ミノオキシブチリル一N′−イソニコチノイルーヒドラ
ジンD−α−アミノオキシ酪酸塩酸塩3.10g(0.
020モル)を水7.0d中に溶解し、この溶液に酢酸
ナトリウム1.649(0.020モル)を添加した。Example 1 N-(N″-5-nitrofurfurylidene)-D-α-aminooxybutyryl-N′-isonicotinoylhydrazine D-α-aminooxybutyric acid hydrochloride 3.10 g (0.
020 mol) was dissolved in 7.0 d of water and 1.649 (0.020 mol) of sodium acetate was added to this solution.
この混合物にメタノール10.071Lt中の5−ニト
ロフルフロール2.849(0.020モル)の溶液を
攪拌下に室温で滴加した。反応混合物を室温で16時間
放置し、ついで水23.0dを添加した。析出した生成
物を戸別し、乾燥し、酢酸エチルから再結晶してD−α
−N−(5−ニトロフルフリリデン)−アミノオキシ酪
酸2.129(88%)を得た。融点:117〜118
℃(酢酸エチルから再結晶後),Rf=0.77,〔α
〕智=+34″(c=1,1エタノール中)。元素分析
:
計算値(C,HlOO6N2):
C,44.7% H,4.l% N,ll.6%実測値
:C,44.8% H,4.O% N,ll.6%D−
α−N−(5−ニトロフルフリリデン)−アミノオキシ
酪酸1.09(0.00412モル)、イソニコチン酸
ヒドラジド0.559(0.004モル)、N,マージ
シクロヘキシル カルボジイミド 0.859(0.0
0412モル)及び無水ジメチルホルムアミド10.0
mtの混合物を室温で16時間攪拌した。A solution of 2.849 (0.020 mol) of 5-nitrofurfurol in 10.071 Lt of methanol was added dropwise to this mixture at room temperature while stirring. The reaction mixture was left at room temperature for 16 hours, then 23.0 d of water was added. The precipitated product was separated, dried, and recrystallized from ethyl acetate to obtain D-α.
2.129 (88%) of -N-(5-nitrofurfurylidene)-aminooxybutyric acid was obtained. Melting point: 117-118
°C (after recrystallization from ethyl acetate), Rf = 0.77, [α
] Chi=+34″ (c=1,1 in ethanol). Elemental analysis: Calculated value (C, HlOO6N2): C, 44.7% H, 4.1% N, ll.6% Actual value: C, 44 .8% H, 4.O% N, 1.6% D-
α-N-(5-nitrofurfurylidene)-aminooxybutyric acid 1.09 (0.00412 mol), isonicotinic acid hydrazide 0.559 (0.004 mol), N,merized cyclohexyl carbodiimide 0.859 (0. 0
0412 mol) and anhydrous dimethylformamide 10.0
The mt mixture was stirred at room temperature for 16 hours.
析出したN,N′−ジシクロヘキシル尿素をP別し、P
液を減圧下で蒸発乾固した。残渣を1Nf1Lrit1
5d中溶解し、この溶液を酢酸エチル3X5dで抽出し
た。水相を固体炭酸水素ナトリウムでPH=7まで中和
し、析出物をP別し、水洗いし、エタノール509bと
水との混合物から再結晶して標題化合物0.96f1(
69(Fb)を得た。融点:164〜1660C,Rf
=0.15,〔α〕M=+1324(c=1、エタノー
ル中)。元素分析:計算値(Cl5H,lO6N,):
C,49.2% H,4.3% N,2O.O%実測値
:C,49.3% H,4.4(!) N,l9.9(
Fb実施例 2N−(N″−5−ニトロフルフリリデン
)−Dα−アミノオキシ−r−メチルーメルカブトーブ
チリル一N′−イソニコチノイルーヒドラジン標題化合
物を適当な出発物質を用いて実施例1と同様に製造した
。The precipitated N,N'-dicyclohexyl urea was separated from P and P
The liquid was evaporated to dryness under reduced pressure. The residue is 1Nf1Lrit1
The solution was extracted with 3×5 d of ethyl acetate. The aqueous phase was neutralized with solid sodium bicarbonate to pH=7, the precipitate was separated from P, washed with water, and recrystallized from a mixture of ethanol 509b and water to yield the title compound 0.96f1 (
69 (Fb) was obtained. Melting point: 164-1660C, Rf
=0.15, [α]M=+1324 (c=1, in ethanol). Elemental analysis: Calculated values (Cl5H, 1O6N,): C, 49.2% H, 4.3% N, 2O. O% actual value: C, 49.3% H, 4.4 (!) N, l9.9 (
Fb Example 2N-(N″-5-nitrofurfurylidene)-Dα-aminooxy-r-methyl-mercabutobutyryl-N′-isonicotinoylhydrazine Example 2 Preparation of the title compound using appropriate starting materials It was manufactured in the same manner as 1.
収率70%:融点130〜135℃(酢酸エチルから再
結晶後):Rf=0.17:〔α〕M=+89結(c=
1、エタノール中)。元素分析:
計算値(Cl6H,,O5N,S):
C,47.2% H,4.2(FbN,l7.2%実測
値:C,47.2% H,4.3% N,l7.l%出
発物質としてのD−α−N−(5−ニトロフルフリリデ
ン)−アミノオキシ−r−メチルメルカプト酪酸を実施
例1と同様に製造し、この化合物をより良好な取扱い適
性を確保するためにそのシンクロヘキシルアンモニウム
塩に転化した。Yield 70%: Melting point 130-135°C (after recrystallization from ethyl acetate): Rf = 0.17: [α] M = +89 (c =
1 in ethanol). Elemental analysis: Calculated value (Cl6H,,O5N,S): C, 47.2% H, 4.2 (FbN, l7.2% Actual value: C, 47.2% H, 4.3% N, l7 D-α-N-(5-nitrofurfurylidene)-aminooxy-r-methylmercaptobutyric acid as starting material is prepared analogously to Example 1 to ensure better handling suitability of this compound. It was converted into its synchhexylammonium salt for the purpose.
得られた塩は使用前にそれ自体既知の方法により酸の形
に遊離させる。生成物の融点:158〜159℃。元素
分析:
計算値(C22H3,O,N,S):
C,56.3(FbH,7.5% N,9.O(Fb実
測値:C,56.3% H,7.4% N,9.l(F
b実施例 3N−(N′5−5−ニトロフルフリリデン
)−D一α−アミノオキシ−β−フエニループロピオニ
ル一N′−イソニコチノイルーヒ下ラジン塩酸塩D−α
−アミノオキシ−β−フエニループロピオン酸塩酸塩2
.179(0.010モル)と5−ニトロフルフロール
1.429(0.010モル)とを実施例1の前半と同
様にして反応させてD−α一N−(5−ニトロフルフリ
リデン)−アミノオキシ−β−フエニループロピオン酸
2.75f1(919b)を得た。The salts obtained are liberated into the acid form by methods known per se before use. Melting point of product: 158-159°C. Elemental analysis: Calculated values (C22H3, O, N, S): C, 56.3 (FbH, 7.5% N, 9.O (Fb actual values: C, 56.3% H, 7.4% N) ,9.l(F
b Example 3N-(N'5-5-nitrofurfurylidene)-D-α-aminooxy-β-phenylpropionyl-N'-isonicotinoyl-Razine hydrochloride D-α
-Aminooxy-β-phenylpropionate hydrochloride 2
.. 179 (0.010 mol) and 5-nitrofurfurol 1.429 (0.010 mol) were reacted in the same manner as in the first half of Example 1 to obtain D-α-N-(5-nitrofurfurylidene)- Aminooxy-β-phenylpropionic acid 2.75f1 (919b) was obtained.
融点:156〜158℃:Rf=0.52:〔α〕智=
−86(c=0.6,エタノール中)。元素分析:
言十j家イ直( Cl4Hl2O6N2):C,55.
2% H,4.O% N,9.2%実測値:C,55.
2% H,4.l% N,9.l%D−α−N−(5−
ニトロフルフリリデン)アミノオキシ一β−フエニルー
プロピオン酸1.0f1(0.0046モル)、ペンタ
クロロフエノール1.229(0.0046モル)及び
N,N′−ジシクロヘキシルカルボジイミド0.95f
i・(0.0046モル)をジオキサン10.0d中に
撹拌下室温で溶解した。Melting point: 156-158°C: Rf = 0.52: [α] Wisdom =
-86 (c=0.6, in ethanol). Elemental analysis: Cl4Hl2O6N2: C, 55.
2% H, 4. O% N, 9.2% Actual value: C, 55.
2% H, 4. 1% N,9. l%D-α-N-(5-
Nitrofurfurylidene) aminooxy-β-phenylpropionic acid 1.0f1 (0.0046 mol), pentachlorophenol 1.229 (0.0046 mol) and N,N'-dicyclohexylcarbodiimide 0.95f
i. (0.0046 mol) was dissolved in 10.0 d of dioxane at room temperature with stirring.
この反応混合物を室温で16時間放置し、析出したN,
N′−ジシクロヘキシル尿素を戸別し、淵液を減圧下で
蒸発乾固した。残渣をエタノールと水との8:2混合物
から再結晶してD−α−N−(5−ニトロフルフリリデ
ン)−アミノオキシ−β−フエニループロピオン酸ペン
タクロロフエニルエステル2.129(83%)を得ム
融点:164〜165℃:Rf=0.77:〔α席=+
134〜(c=1、エタノール中)。元素分析:
計算値(C2OH,lO,N2Cl,):C,43.5
O!) H,2.O% Ce,32.O%実御値:C,
43.6% H,2.l% Cl,3l.9%D−α−
N−(5−ニトロフルフリリデン)−アミノオキシ−β
−フエニループロピオン酸ペンタクロロフエニル エス
テル1.0f1(0.0018モル)及びイソニコチン
酸ヒドラジド0.25f!(0.0018モル)を無水
ジメチルホルムアミド10.0TILI中に溶解し、こ
の溶液を室温で6時間撹拌した。This reaction mixture was left at room temperature for 16 hours, and the precipitated N,
N'-dicyclohexylurea was separated and the bottom liquid was evaporated to dryness under reduced pressure. The residue was recrystallized from an 8:2 mixture of ethanol and water to give D-α-N-(5-nitrofurfurylidene)-aminooxy-β-phenyl-propionic acid pentachlorophenyl ester 2.129 (83%). Melting point: 164-165℃: Rf = 0.77: [α seat = +
134~(c=1 in ethanol). Elemental analysis: Calculated value (C2OH, lO, N2Cl,): C, 43.5
O! ) H, 2. O% Ce, 32. O% actual value: C,
43.6% H, 2. 1% Cl, 3l. 9%D-α-
N-(5-nitrofurfurylidene)-aminooxy-β
-Phenyl-propionate pentachlorophenyl ester 1.0f1 (0.0018 mol) and isonicotinic acid hydrazide 0.25f! (0.0018 mol) was dissolved in 10.0 TILI of anhydrous dimethylformamide and the solution was stirred at room temperature for 6 hours.
ついで反応混合物を減圧下で蒸発乾固した。残渣を酢酸
エチル101LI,中に溶解し、1M炭酸水素ナトリウ
ム溶液3X5m1、ついで水2X5dで洗浄した。有機
相を硫酸ナトリウムで乾燥し、溶剤を減圧留去した。残
渣を0.5Nエーテル性塩酸207n1で処理し、析出
した塩を戸別し、熱エタノール中に溶解し、冷却後ジエ
チル エーテルを加えた溶液から沈澱させた。かくして
N−(N′5−5−ニトロフルフリリデシ)一D−α−
アミノオキシ−β−フエニループロピオニルーマーイソ
ニコチノイルーヒドラジ7塩酸塩0.64g(81%)
を得た。The reaction mixture was then evaporated to dryness under reduced pressure. The residue was dissolved in 101 LI of ethyl acetate and washed with 3.times.5 ml of 1M sodium bicarbonate solution and then 2.times.5 ml of water. The organic phase was dried over sodium sulfate and the solvent was distilled off under reduced pressure. The residue was treated with 207 nl of 0.5N ethereal hydrochloric acid, and the precipitated salt was separated, dissolved in hot ethanol and, after cooling, precipitated from the solution with diethyl ether. Thus, N-(N'5-5-nitrofurfurylidecy)-D-α-
Aminooxy-β-phenylpropionyl lumer isonicotinoyl hydrazi heptahydrochloride 0.64g (81%)
I got it.
融点:75〜76℃;Rf=0.08:〔α〕=+86
:(c=1、工タノール中)。元素分析:
計算値(C,。Melting point: 75-76°C; Rf = 0.08: [α] = +86
: (c=1, in ethanol). Elemental analysis: Calculated values (C,.
H,8N,CO:C,52.3% H,3.9% Ce
,7.7%実測値:C,52.2(FbH,4.O%
Cl,7.7%実施例1〜3と同様にして適当な出発物
質から下記の化合物を製造した。H, 8N, CO:C, 52.3% H, 3.9% Ce
, 7.7% Actual value: C, 52.2 (FbH, 4.O%
Cl, 7.7% The following compounds were prepared from the appropriate starting materials in a similar manner to Examples 1-3.
実施例 4
N−(N″−m−ニトローベンザル)−アミノオキシア
セチル−N′−イソニコチノイルーヒドラジン融点:1
58〜160℃(エタノールから再結晶後)元素分析:
計算値(COH,,O,N,):
C,52.59bH,3.8% N,2O.4%実二1
・゛ ゛C,52.5!FbH,3,9(!)N,2
O.5%実施例 5N−(N2−1−メチル−p−アミ
ノーベンザル)−アミノオキシアセチル−N′−イソニ
コチノイルーヒドラジン融点:175〜177℃(エタ
ノールから再結晶後)
C元素分析:計算値(ClIHl?0,N
.):
゛コCt5&フ% H,5.29hN,2l.4%実棚
値; ゛7C,58.▼% H:12%N,2
l.2% ;実施例 6N−(N″−p−ヒドロキシー
ベンザル)−アミノオキシアセチル−N′−イソニコチ
ノイルーヒドラジンし゜融点:203〜204℃(エタ
ノールから再結 FM)元素分析:
計算値(ClHiO,Sl):
C,57.4% H・,4J・1fbN,17.89i
実測値:C,57.5% H,4.6% N,l7.8
%実施例 7N−(N″−0−クロローベンザル)−ア
ミノオキシアセチル−N′−イソニコチノイルーヒドラ
ジン融点:147〜149℃(エタノールから再結晶後
)元素分析:
計算値(Cl6H,3O,N4Cl):
C,54.l% H,3.9% C2,lO.7%実測
値:C,54.O% H,4.O% Ce,・10.7
%実施例 8N−(N′5−シクロペンチリデン)−ア
ミノオキシアセチル−N′−イソニコチノイルーヒドラ
ジン融点:160〜161℃(水から再結晶後)元素分
析:計算値(C,,Hl6O,N4):
C,56.5% H,5.8% N,2O.3%実測値
:C,56.5% H,5.8% N,2O.l%実施
例 9N−(N′5−フルフリリデン)−アミノオキシ
アセチル−N′−イソニコチノイルービドラジン融点:
123〜125℃(水から再結晶後)元素分析:計算値
(C,,H,,O4N4):
C,54.l% H,4.2% N,l9.4%実測値
:C,54.2% H,4.3lfbN,l9.4%実
施例 10N−(N″−1−メチルーベンザル)−アミ
ノオキシアセチル−W−イソニコチノイjソレーヒドラ
ジン融点:160〜162℃(エタノールから再結晶後
)元素分析:
計算値(C,,H,。Example 4 N-(N″-m-nitrobenzal)-aminooxyacetyl-N′-isonicotinoylhydrazine Melting point: 1
58-160°C (after recrystallization from ethanol) Elemental analysis: Calculated values (COH,,O,N,): C, 52.59bH, 3.8% N, 2O. 4% real 21
・゛ ゛C, 52.5! FbH,3,9(!)N,2
O. 5% Example 5N-(N2-1-methyl-p-aminobenzal)-aminooxyacetyl-N'-isonicotinoylhydrazine Melting point: 175-177°C (after recrystallization from ethanol)
C elemental analysis: Calculated value (ClIHl?0,N
.. ): ゛CoCt5&F%H, 5.29hN, 2l. 4% actual shelf value; ゛7C, 58. ▼%H:12%N,2
l. 2%; Example 6 N-(N″-p-hydroxybenzal)-aminooxyacetyl-N′-isonicotinoylhydrazine Melting point: 203-204°C (reconsolidated from ethanol FM) Elemental analysis: Calculated value (ClHiO, Sl): C, 57.4% H, 4J, 1fbN, 17.89i
Actual value: C, 57.5% H, 4.6% N, l7.8
% Example 7 N-(N″-0-chlorobenzal)-aminooxyacetyl-N′-isonicotinoylhydrazine Melting point: 147-149°C (after recrystallization from ethanol) Elemental analysis: Calculated value (Cl6H,3O,N4Cl ): C, 54.1% H, 3.9% C2, 1O.7% Actual value: C, 54.0% H, 4.0% Ce, ・10.7
% Example 8 N-(N'5-cyclopentylidene)-aminooxyacetyl-N'-isonicotinoylhydrazine Melting point: 160-161°C (after recrystallization from water) Elemental analysis: Calculated value (C,, Hl6O , N4): C, 56.5% H, 5.8% N, 2O. 3% actual value: C, 56.5% H, 5.8% N, 2O. 1% Example 9 N-(N'5-furfurylidene)-aminooxyacetyl-N'-isonicotinoyl-hydrazine Melting point:
123-125°C (after recrystallization from water) Elemental analysis: Calculated value (C,,H,,O4N4): C, 54. 1% H, 4.2% N, 19.4% Actual value: C, 54.2% H, 4.3lfbN, 19.4% Example 10 N-(N″-1-methyl-benzal)-aminooxy Acetyl-W-Isonicotinoidj Solehydrazine Melting point: 160-162°C (after recrystallization from ethanol) Elemental analysis: Calculated value (C,,H,.
O,N,):C,6l.5% H,5.l% N,l8
.O%実測値:C,6l.4% H,5.3% N,l
8.2実施例 11
N−(N″−シクロペンチリデン)−D−α−アミノオ
キシ−β−フエニループロピオニル一N′ーイソニコチ
ノイルーヒドラジン融点:191〜194℃(水性エタ
ノールから再結晶後),〔α〕R=71性(C=1,エ
タノール中)。O, N, ): C, 6l. 5% H,5. 1% N, 18
.. O% actual value: C, 6l. 4% H, 5.3% N, l
8.2 Example 11 N-(N″-cyclopentylidene)-D-α-aminooxy-β-phenylpropionyl-N′-isonicotinoylhydrazine Melting point: 191-194°C (recrystallized from aqueous ethanol) after), [α]R=71 (C=1, in ethanol).
元素分析:
計算値(C2OH2,O3N4):
C,65.6% H,6.l% N,l5.3%実側値
:
C,65.5CfbH,6、2% N,l5.3%実施
例 12
N−(N7′−m−ニトローベンザル)−D−α−アミ
ノオキシ−β−フエニループロピオニルー一N′−イソ
ニコチノイルーヒドラジン塩酸塩融点:76〜78チc
,〔α〕M=+72酸(c=1、エタノール中)。Elemental analysis: Calculated values (C2OH2, O3N4): C, 65.6% H, 6. 1% N, 15.3% Actual value: C, 65.5CfbH, 6, 2% N, 15.3% Example 12 N-(N7'-m-nitrobenzal)-D-α-aminooxy-β -Phenyl-propionyl-N'-isonicotinoyl-hydrazine hydrochloride Melting point: 76-78 c
, [α]M=+72 acid (c=1, in ethanol).
元素分析:
計算値(C22H,OO,N,ce):
C,56.3% H,4.3% C2,7.59)実測
値:
C,56.39l) H,゛4.4% Cl,7.4%
実施例 13
N−(N″−5−ニトロフルフリリデン)−アミノオキ
シアセチル−N′−イソニコチノイルーヒドラジン融点
:168〜170℃(水から再結晶化後)<元素分析:
計算値(Cl3HllO,N,):C,46.9% H
,3.39bN,2l.O%実測値:
C,46.8% H,3,3% N,2l.O9b実施
例 14
N−(N′5−イソプロピリデン)−アミノオキシアセ
チル−N′−イソニコチノイルーヒドラジン融点:13
5〜136℃0
元素分析:
計算値(C,lH,4O,N4):
C,52.8% H,5.6(FbN,22.4%実測
値:
C,52.7% H,5.7% N,22.4%この化
合物0.509を氷酢酸中の臭化水素の36%溶液2.
0W11中に溶解し、形成された塩を無水ジエチルエー
テル10,0dを加えて沈澱させてその臭化水素酸塩0
,639(96%)を得た。Elemental analysis: Calculated value (C22H, OO, N, ce): C, 56.3% H, 4.3% C2, 7.59) Actual value: C, 56.39l) H, 4.4% Cl ,7.4%
Example 13 N-(N″-5-nitrofurfurylidene)-aminooxyacetyl-N′-isonicotinoylhydrazine Melting point: 168-170°C (after recrystallization from water) <Elemental analysis:
Calculated value (Cl3HllO, N,): C, 46.9% H
, 3.39bN, 2l. O% actual value: C, 46.8% H, 3.3% N, 2l. O9b Example 14 N-(N'5-isopropylidene)-aminooxyacetyl-N'-isonicotinoylhydrazine Melting point: 13
5-136°C 0 Elemental analysis: Calculated value (C, lH, 4O, N4): C, 52.8% H, 5.6 (FbN, 22.4% Actual value: C, 52.7% H, 5 .7% N, 22.4% This compound was dissolved in a 36% solution of hydrogen bromide in glacial acetic acid.
0W11 and the salt formed was precipitated by adding 10.0d of anhydrous diethyl ether to obtain its hydrobromide salt.
,639 (96%).
融点:152℃,Rf=0.07。Melting point: 152°C, Rf=0.07.
元素分析:
計算値(Cl,Hl,O3N4Br):
C,39.9Ol) H,4.5% Br,24.89
b実測値:
C,39.8% H,4.6% Br,24.9%。Elemental analysis: Calculated values (Cl, Hl, O3N4Br): C, 39.9Ol) H, 4.5% Br, 24.89
b Actual values: C, 39.8% H, 4.6% Br, 24.9%.
Claims (1)
びRは後記の意義を有し:R′は水素、炭素数1〜5個
のアルキル基あるいは1個又は2個以上のハロゲン又は
ニトロ置換基を有するフェニル基である)のシッフ塩基
を式(III):H_2N−NHZ(III)(式中、Zはピ
リジンカルボン酸から誘導されるアシル基である)のヒ
ドラジン誘導体と反応させ、ついで所望ならば、得られ
た塩基を常法によりその酸付加塩に転化するかあるいは
得られた塩を常法によりその遊離塩基又は別の塩に転化
することからなる式( I ):▲数式、化学式、表等が
あります▼( I )(式中、Xはシクロペンチリデン基
あるいは炭素数1〜5個のアルキル、フェニル、ハロフ
エニル、ヒドロキシフェニル、ニトロフェニル、アミノ
フェニル、フリル及びニトロフリル基から選んだ少なく
とも1個の置換基を有するメチレン基を表わし;Rは水
素、ベンジル基又は随意にメチルチオ置換基を有する炭
素数1〜5個のアルキル基を表わし;Zはピリジンカル
ボン酸から誘導されたアシル基を表わす)の化合物又は
その酸付加塩の製造法。[Claims] 1 General formula (II): ▲ Numerical formulas, chemical formulas, tables, etc. ▼ (II) (In the formula, X and R have the meanings below: R' is hydrogen, carbon number 1- 5 alkyl groups or a phenyl group having one or more halogen or nitro substituents) with the formula (III): H_2N-NHZ(III) (wherein Z is from pyridinecarboxylic acid) the hydrazine derivative (which is the acyl group to be derived) and then, if desired, the resulting base is converted into its acid addition salt by conventional methods or the resulting salt is converted into its free base or another salt by conventional methods. Formula (I): ▲ There are mathematical formulas, chemical formulas, tables, etc. ▼ (I) (wherein, Represents a methylene group having at least one substituent selected from hydroxyphenyl, nitrophenyl, aminophenyl, furyl and nitrofuryl; R is hydrogen, a benzyl group, or a carbon number of 1 to 5, optionally having a methylthio substituent represents an alkyl group; Z represents an acyl group derived from pyridinecarboxylic acid) or an acid addition salt thereof.
Applications Claiming Priority (2)
Application Number | Priority Date | Filing Date | Title |
---|---|---|---|
HU530 | 1973-11-29 | ||
HURI530A HU167365B (en) | 1973-11-29 | 1973-11-29 |
Publications (2)
Publication Number | Publication Date |
---|---|
JPS57192365A JPS57192365A (en) | 1982-11-26 |
JPS5953264B2 true JPS5953264B2 (en) | 1984-12-24 |
Family
ID=11000941
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Application Number | Title | Priority Date | Filing Date |
---|---|---|---|
JP49136382A Expired JPS5951537B2 (en) | 1973-11-29 | 1974-11-29 | Method for producing novel α-aminooxycarboxylic acid hydrazide derivative |
JP57052368A Expired JPS5953264B2 (en) | 1973-11-29 | 1982-04-01 | Method for producing novel α-aminooxycarboxylic acid hydrazide derivative |
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Application Number | Title | Priority Date | Filing Date |
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---|---|
JP (2) | JPS5951537B2 (en) |
AT (1) | AT340920B (en) |
BE (1) | BE822767A (en) |
CA (1) | CA1018171A (en) |
CH (2) | CH612926A5 (en) |
CS (1) | CS199568B2 (en) |
DD (1) | DD118874A5 (en) |
DE (1) | DE2455353C3 (en) |
FR (1) | FR2252845B1 (en) |
GB (1) | GB1446980A (en) |
HU (1) | HU167365B (en) |
NL (1) | NL7415589A (en) |
SU (2) | SU574146A3 (en) |
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ATE52765T1 (en) * | 1984-10-18 | 1990-06-15 | Shell Int Research | ALPHA AMINOOXY C4 ALKANOIC ACIDS AND ESTERS. |
JPH0317434Y2 (en) * | 1986-03-11 | 1991-04-12 | ||
US5002605A (en) * | 1988-12-21 | 1991-03-26 | Ici Americas Inc. | Alkylidine aminooxyamide compounds useful in controlling undesirable vegetation |
EA011074B1 (en) | 2004-03-30 | 2008-12-30 | Дзе Риджентс Оф Дзе Юниверсити Оф Калифорния | Hydrazide-containing cftr inhibitor compounds and uses thereof |
AU2007336897A1 (en) | 2006-12-22 | 2008-07-03 | The Regents Of The University Of California | Macromolecular conjugates of cystic fibrosis transmembrane conductance regulator protein inhibitors and uses thereof |
CN101668732A (en) | 2007-04-02 | 2010-03-10 | 同一世界健康研究院 | CFTR inhibitor compound and uses thereof |
ES2422603T3 (en) | 2007-05-31 | 2013-09-12 | Shionogi & Co | Oxyimino compounds and the use of these |
JP5380435B2 (en) * | 2007-05-31 | 2014-01-08 | ユーロ−セルティーク ソシエテ アノニム | Amide compounds and uses thereof |
US8207205B2 (en) | 2008-04-21 | 2012-06-26 | Institute For Oneworld Health | Compounds, compositions and methods comprising oxadiazole derivatives |
US8236838B2 (en) | 2008-04-21 | 2012-08-07 | Institute For Oneworld Health | Compounds, compositions and methods comprising isoxazole derivatives |
US8518934B2 (en) | 2008-06-11 | 2013-08-27 | Shonogi & Co., Ltd. | Oxycarbamoyl compounds and the use thereof |
US8343976B2 (en) | 2009-04-20 | 2013-01-01 | Institute For Oneworld Health | Compounds, compositions and methods comprising pyrazole derivatives |
CN102276593B (en) * | 2011-07-01 | 2013-10-30 | 华东师范大学 | Heterocyclic ketene hydrazone compound and preparation method as well as tubercle bacillus resistant application |
WO2014201446A2 (en) * | 2013-06-14 | 2014-12-18 | Hellmich Mark | Use of hydrogen sulfide synthesis inhibitors for the therapy of colorectal cancers |
-
1973
- 1973-11-29 HU HURI530A patent/HU167365B/hu unknown
-
1974
- 1974-11-20 GB GB5027274A patent/GB1446980A/en not_active Expired
- 1974-11-21 CH CH1549474A patent/CH612926A5/en not_active IP Right Cessation
- 1974-11-21 CH CH1154777A patent/CH614954A5/en not_active IP Right Cessation
- 1974-11-22 DE DE2455353A patent/DE2455353C3/en not_active Expired
- 1974-11-25 AT AT940574A patent/AT340920B/en not_active IP Right Cessation
- 1974-11-26 CS CS748076A patent/CS199568B2/en unknown
- 1974-11-27 DD DD182612A patent/DD118874A5/xx unknown
- 1974-11-28 SU SU7402082854A patent/SU574146A3/en active
- 1974-11-29 FR FR7439299A patent/FR2252845B1/fr not_active Expired
- 1974-11-29 BE BE150997A patent/BE822767A/en not_active IP Right Cessation
- 1974-11-29 NL NL7415589A patent/NL7415589A/en not_active Application Discontinuation
- 1974-11-29 CA CA214,911A patent/CA1018171A/en not_active Expired
- 1974-11-29 JP JP49136382A patent/JPS5951537B2/en not_active Expired
-
1976
- 1976-06-21 SU SU762373709A patent/SU608472A3/en active
-
1982
- 1982-04-01 JP JP57052368A patent/JPS5953264B2/en not_active Expired
Also Published As
Publication number | Publication date |
---|---|
CS199568B2 (en) | 1980-07-31 |
DD118874A5 (en) | 1976-03-20 |
CH614954A5 (en) | 1979-12-28 |
GB1446980A (en) | 1976-08-18 |
NL7415589A (en) | 1975-06-02 |
SU608472A3 (en) | 1978-05-25 |
DE2455353B2 (en) | 1978-12-07 |
FR2252845B1 (en) | 1978-07-21 |
AT340920B (en) | 1978-01-10 |
FR2252845A1 (en) | 1975-06-27 |
SU574146A3 (en) | 1977-09-25 |
CH612926A5 (en) | 1979-08-31 |
JPS5951537B2 (en) | 1984-12-14 |
BE822767A (en) | 1975-03-14 |
ATA940574A (en) | 1977-05-15 |
DE2455353C3 (en) | 1979-08-09 |
HU167365B (en) | 1975-09-27 |
CA1018171A (en) | 1977-09-27 |
JPS5084523A (en) | 1975-07-08 |
JPS57192365A (en) | 1982-11-26 |
DE2455353A1 (en) | 1975-06-05 |
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