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Avidin

From Wikipedia, the free encyclopedia
Avidin family
Tetrameric structure of streptavidin with 2 bound biotins
Identifiers
SymbolAvidin
PfamPF01382
InterProIPR005468
PROSITEPDOC00499
CATH1slf
SCOP21slf / SCOPe / SUPFAM
Available protein structures:
Pfam  structures / ECOD  
PDBRCSB PDB; PDBe; PDBj
PDBsumstructure summary
Biotin - Avidin can bind up to four molecules of biotin simultaneously with a high degree of affinity and specificity

Avidin is a tetrameric biotin-binding protein produced in the oviducts of birds, reptiles and amphibians and deposited in the whites of their eggs. Dimeric members of the avidin family are also found in some bacteria.[1] In chicken egg white, avidin makes up approximately 0.05% of total protein (approximately 1800 μg per egg). The tetrameric protein contains four identical subunits (homotetramer), each of which can bind to biotin (Vitamin B7, vitamin H) with a high degree of affinity and specificity. The dissociation constant of the avidin-biotin complex is measured to be KD ≈ 10−15 M, making it one of the strongest known non-covalent bonds.[2]

In its tetrameric form, avidin is estimated to be 66–69 kDa in size.[3] 10% of the molecular weight is contributed by carbohydrate, composed of four to five mannose and three N-acetylglucosamine residues[4] The carbohydrate moieties of avidin contain at least three unique oligosaccharide structural types that are similar in structure and composition.[5]

Functional avidin is found in raw egg, but depending on the amount of heat it is exposed to during cooking, the quantity of molecules available for binding biotin can change. The natural function of avidin in eggs is not known, although it has been postulated to be made in the oviduct as a bacterial growth inhibitor, by binding biotin helpful for bacterial growth. As evidence for this, streptavidin, a related protein with equal biotin affinity and a very similar binding site, is made by certain strains of Streptomyces bacteria, and is thought to serve to inhibit the growth of competing bacteria, in the manner of an antibiotic.[6]

A non-glycosylated form of avidin has been isolated from commercially prepared product; however, it is not conclusive as to whether the non-glycosylated form occurs naturally or is a product of the manufacturing process.[7]

Discovery

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A raw egg yolk surrounded by the egg white. Avidin was first isolated from raw chicken egg white by Esmond Emerson Snell

Avidin was discovered by Esmond Emerson Snell (1914–2003). This discovery began with the observation that chicks on a diet of raw egg white were deficient in biotin, despite availability of the vitamin in their diet.[8] It was concluded that a component of the egg-white was sequestering biotin[8] which Snell verified in vitro using a yeast assay.[9] Snell later isolated the component of egg white responsible for biotin binding, and, in collaboration with Paul György, confirmed that the isolated egg protein was the cause of biotin deficiency or “egg white injury”.[10] At the time the protein had been tentatively named avidalbumin (literally, hungry albumin) by researchers at the University of Texas.[10] The name of the protein was later revised to "avidin" based on its affinity for biotin (avid + biotin).[11]

Applications

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Avidin
Identifiers
OrganismChicken
SymbolAVD
UniProtP02701
Search for
StructuresSwiss-model
DomainsInterPro
Unless otherwise specified, "avidin" the biomedical reagent is chicken avidin.

Research in the 1970s helped establish the avidin-biotin system as a powerful tool in biological sciences. Aware of the strength and specificity of the avidin-biotin complex, researchers began to exploit chicken avidin and streptavidin as probes and affinity matrices in numerous research projects.[12][13][14][15] Soon after, researchers Bayer and Wilchek developed new methods and reagents to biotinylate antibodies and other biomolecules,[16][17] allowing the transfer of the avidin-biotin system to a range of biotechnological applications. Today, avidin is used in a variety of applications ranging from research and diagnostics to medical devices and pharmaceuticals.

Avidin's affinity for biotin is exploited in wide-ranging biochemical assays, including western blot, ELISA, ELISPOT and pull-down assays. In some cases the use of biotinylated antibodies has allowed the replacement of radioiodine labeled antibodies in radioimmunoassay systems, to give an assay system which is not radioactive.[citation needed]

Avidin immobilized onto solid supports is also used as purification media to capture biotin-labelled protein or nucleic acid molecules. For example, cell surface proteins can be specifically labelled with membrane impermeable biotin reagent, then specifically captured using an avidin-based support.[citation needed]

Modified forms

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As a basically charged glycoprotein, avidin exhibits non-specific binding in some applications. Neutralite avidin, a deglycosylated avidin with modified arginines, exhibits a more neutral isoelectric point (pI) and is available as an alternative to native avidin, whenever problems of non-specific binding arise. Deglycosylated, neutral forms of chicken avidin are available through Sigma-Aldrich (Extravidin), Thermo Scientific (NeutrAvidin), Invitrogen (NeutrAvidin), and e-Proteins (NeutraLite).

Given the strength of the avidin-biotin bond, dissociation of the avidin-biotin complex requires extreme conditions that cause protein denaturation. The non-reversible nature of the avidin-biotin complex can limit avidin's application in affinity chromatography applications where release of the captured ligand is desirable. Researchers have created an avidin with reversible binding characteristics through nitration or iodination of the binding site tyrosine.[18] The modified avidin exhibits strong biotin binding characteristics at pH 4 and releases biotin at a pH of 10 or higher.[18] A monomeric form of avidin with a reduced affinity for biotin is also employed in many commercially available affinity resins. The monomeric avidin is created by treatment of immobilized native avidin with urea or guanidine HCl (6–8 M), giving it a lower dissociation KD ≈ 10−7M.[19] This allows elution from the avidin matrix to occur under milder, non-denaturing conditions, using low concentrations of biotin or low pH conditions. For a single high affinity biotin binding site without crosslinking, a monovalent version of avidin's distant relative, streptavidin, may be used.[20]

Blocking of biotin binding

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The thermal stability and biotin binding activity of avidin are of both practical and theoretical interest to researchers, as avidin's stability is unusually high and avidin is an antinutrient in human food.[21] A 1966 study published in Biochemical and Biophysical Research Communications found that the structure of avidin remains stable at temperatures below 70 °C (158 °F). Above 70 °C (158 °F), avidin's structure is rapidly disrupted and by 85 °C (185 °F), extensive loss of structure and loss of ability to bind biotin is found.[22] A 1991 assay for the Journal of Food Science detected substantial avidin activity in cooked egg white: "mean residual avidin activity in fried, poached and boiled (2 min) egg white was 33, 71 and 40% of the activity in raw egg white." The assay surmised that cooking times were not sufficient to adequately heat all cold spot areas within the egg white. Complete inactivation of avidin's biotin binding capacity required boiling for over 4 minutes.[23]

A 1992 study found that thermal inactivation of the biotin binding activity of avidin was described by D121 °C = 25 min and z = 33 °C. This study disagreed with prior assumptions "that the binding site of avidin is destroyed on heat denaturation".[21]

The biotin-binding properties of avidin were exploited during the development of idrabiotaparinux, a long-acting low molecular weight heparin used in the treatment of venous thrombosis. Due to the long-acting nature of idraparinux, concerns were made about the clinical management of bleeding complications. By adding a biotin moiety to the idraparinux molecule, idrabiotaparinux was formed; its anticoagulant activity in the setting of a bleeding event can be reversed through an intravenous infusion of avidin.[24]

See also

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References

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  1. ^ Helppolainen SH, Nurminen KP, Määttä JA, Halling KK, Slotte JP, Huhtala T, et al. (August 2007). "Rhizavidin from Rhizobium etli: the first natural dimer in the avidin protein family". The Biochemical Journal. 405 (3): 397–405. doi:10.1042/BJ20070076. PMC 2267316. PMID 17447892.
  2. ^ Green NM (December 1963). "Avidin. 1. The Use of (14-C)Biotin for Kinetic Studies and for Assay". The Biochemical Journal. 89 (3): 585–91. doi:10.1042/bj0890585. PMC 1202466. PMID 14101979.
  3. ^ Korpela J (1984). "Avidin, a high affinity biotin-binding protein, as a tool and subject of biological research". Medical Biology. 62 (1): 5–26. PMID 6379329.
  4. ^ Green NM (1975). Anfinsen CB, Edsall JT, Richards FM (eds.). "Avidin". Advances in Protein Chemistry. 29: 85–133. doi:10.1016/S0065-3233(08)60411-8. ISBN 978-0-12-034229-7. PMID 237414.
  5. ^ Bruch RC, White HB (October 1982). "Compositional and structural heterogeneity of avidin glycopeptides". Biochemistry. 21 (21): 5334–41. doi:10.1021/bi00264a033. PMID 6816268.
  6. ^ Hendrickson WA, Pähler A, Smith JL, Satow Y, Merritt EA, Phizackerley RP (April 1989). "Crystal structure of core streptavidin determined from multiwavelength anomalous diffraction of synchrotron radiation". Proceedings of the National Academy of Sciences of the United States of America. 86 (7): 2190–4. Bibcode:1989PNAS...86.2190H. doi:10.1073/pnas.86.7.2190. JSTOR 33443. PMC 286877. PMID 2928324.
  7. ^ Hiller Y, Gershoni JM, Bayer EA, Wilchek M (November 1987). "Biotin binding to avidin. Oligosaccharide side chain not required for ligand association". The Biochemical Journal. 248 (1): 167–71. doi:10.1042/bj2480167. PMC 1148514. PMID 3435435.
  8. ^ a b Eakin RE, McKinley WA, Williams RJ (September 1940). "Egg-White Injury in Chicks and ITS Relationship to a Deficiency of Vitamin H (Biotin)". Science. 92 (2384): 224–5. Bibcode:1940Sci....92..224E. doi:10.1126/science.92.2384.224. PMID 17743857.
  9. ^ Snell EE, Eakin RE, Williams RJ (1940). "A Quantitative Test for Biotin and Observations Regarding its Occurrence and Properties". Journal of the American Chemical Society. 62: 175–8. doi:10.1021/ja01858a052.
  10. ^ a b György P, Rose CS, Eakin RE, Snell EE, Williams RJ (May 1941). "Egg-White Injury as the Result of Nonabsorption or Inactivation of Biotin". Science. 93 (2420): 477–8. Bibcode:1941Sci....93..477G. doi:10.1126/science.93.2420.477. PMID 17757050.
  11. ^ Kresge N, Simoni RD, Hill RL (2004). "The Discovery of Avidin by Esmond E. Snell". The Journal of Biological Chemistry. 279 (41): e5–e6. doi:10.1016/S0021-9258(20)77095-X.
  12. ^ Hofmann K, Kiso Y (October 1976). "An approach to the targeted attachment of peptides and proteins to solid supports". Proceedings of the National Academy of Sciences of the United States of America. 73 (10): 3516–8. Bibcode:1976PNAS...73.3516H. doi:10.1073/pnas.73.10.3516. JSTOR 66631. PMC 431147. PMID 185617.
  13. ^ Bayer EA, Skutelsky E, Wynne D, Wilchek M (August 1976). "Preparation of ferritin-avidin conjugates by reductive alkylation for use in electron microscopic cytochemistry". The Journal of Histochemistry and Cytochemistry. 24 (8): 933–9. doi:10.1177/24.8.182877. PMID 182877.
  14. ^ Angerer L, Davidson N, Murphy W, Lynch D, Attardi G (September 1976). "An electron microscope study of the relative positions of the 4S and ribosomal RNA genes in HeLa cells mitochondrial DNA". Cell. 9 (1): 81–90. doi:10.1016/0092-8674(76)90054-4. PMID 975242. S2CID 54340885.
  15. ^ Heggeness MH, Ash JF (June 1977). "Use of the avidin-biotin complex for the localization of actin and myosin with fluorescence microscopy". The Journal of Cell Biology. 73 (3): 783–8. doi:10.1083/jcb.73.3.783. PMC 2111432. PMID 326797.
  16. ^ Bayer EA, Zalis MG, Wilchek M (September 1985). "3-(N-Maleimido-propionyl)biocytin: a versatile thiol-specific biotinylating reagent". Analytical Biochemistry. 149 (2): 529–36. doi:10.1016/0003-2697(85)90609-8. PMID 3935007.
  17. ^ Wilchek M, Ben-Hur H, Bayer EA (July 1986). "p-Diazobenzoyl biocytin--a new biotinylating reagent for the labeling of tyrosines and histidines in proteins". Biochemical and Biophysical Research Communications. 138 (2): 872–9. doi:10.1016/S0006-291X(86)80577-0. PMID 3741438.
  18. ^ a b Morag E, Bayer EA, Wilchek M (May 1996). "Reversibility of biotin-binding by selective modification of tyrosine in avidin". The Biochemical Journal. 316 (1): 193–9. doi:10.1042/bj3160193. PMC 1217322. PMID 8645205.
  19. ^ Kohanski RA, Lane MD (1990). Monovalent avidin affinity columns. Methods in Enzymology. Vol. 184. pp. 194–200. doi:10.1016/0076-6879(90)84274-K. ISBN 978-0-12-182085-5. PMID 2388570.
  20. ^ Howarth M, Chinnapen DJ, Gerrow K, Dorrestein PC, Grandy MR, Kelleher NL, et al. (April 2006). "A monovalent streptavidin with a single femtomolar biotin binding site". Nature Methods. 3 (4): 267–73. doi:10.1038/nmeth861. PMC 2576293. PMID 16554831.
  21. ^ a b Durance TD, Wong NS (1992). "Kinetics of thermal inactivation of avidin". Food Research International. 25 (2): 89–92. doi:10.1016/0963-9969(92)90148-X.
  22. ^ Pritchard AB, McCormick DB, Wright LD (1966). "Optical rotatory dispersion studies of the heat denaturation of avidin and the avidin-biotin complex". Biochemical and Biophysical Research Communications. 25 (5): 524–8. doi:10.1016/0006-291X(66)90623-1.
  23. ^ Durance TD (1991). "Residual Avid in Activity in Cooked Egg White Assayed with Improved Sensitivity". Journal of Food Science. 56 (3): 707–9. doi:10.1111/j.1365-2621.1991.tb05361.x.
  24. ^ Büller HR, Gallus AS, Pillion G, Prins MH, Raskob GE (January 2012). "Enoxaparin followed by once-weekly idrabiotaparinux versus enoxaparin plus warfarin for patients with acute symptomatic pulmonary embolism: a randomised, double-blind, double-dummy, non-inferiority trial". Lancet. 379 (9811): 123–9. doi:10.1016/S0140-6736(11)61505-5. PMID 22130488. S2CID 205964156.
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