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与血小板结合的牛血管性血友病因子片段的特性分析

Characterization of a fragment of bovine von Willebrand factor that binds to platelets.

作者信息

Mascelli M A, Edgington T S, Kirby E P

出版信息

Biochemistry. 1986 Oct 7;25(20):6325-35. doi: 10.1021/bi00368a074.

Abstract

Bovine von Willebrand factor was digested with human plasmin in order to isolate and characterize a fragment that can bind to human platelets. A terminal plasmin digest of bovine von Willebrand factor is composed of five fragments, ranging in relative molecular weight (Mr) from 250,000 to 35,000. The major fragment has a Mr of 250,000 and consists of four disulfide-linked polypeptide chains with Mr from 69,000 to 35,000. The Mr 69,000 and 49,000 polypeptides possess carbohydrate moieties, as indicated by their reaction with periodate-Schiff reagent. Gel filtration studies suggest that, at physiological ionic strength, four of the Mr 250,000 fragments associate into a limited noncovalent oligomer. Monoclonal antibodies were prepared against native von Willebrand factor and used to characterize the distribution of epitopes on native vWF and the Mr 250,000 major fragment. Two of the monoclonal antibodies that recognize the major fragment (2 and H-9) inhibit platelet agglutination. The Mr 250,000 fragment binds to human platelets, and the binding is inhibited by monoclonal antibodies 2 and H-9. The Mr 250,000 fragment does not agglutinate platelets, consistent with a requirement for high molecular weight oligomers of von Willebrand factor for platelet agglutination. The Mr 250,000 fragment can compete with intact, bovine von Willebrand factor for binding to human platelets. However, its affinity is one-tenth that of intact von Willebrand factor.

摘要

用人类纤溶酶消化牛血管性血友病因子,以分离和鉴定一种能与人类血小板结合的片段。牛血管性血友病因子的终末纤溶酶消化产物由五个片段组成,相对分子量(Mr)在250,000至35,000之间。主要片段的Mr为250,000,由四条二硫键连接的多肽链组成,Mr从69,000至35,000。Mr为69,000和49,000的多肽具有碳水化合物部分,这可通过它们与高碘酸-希夫试剂的反应表明。凝胶过滤研究表明,在生理离子强度下,四个Mr为250,000的片段缔合成一种有限的非共价寡聚物。制备了针对天然血管性血友病因子的单克隆抗体,并用于鉴定天然vWF和Mr为250,000的主要片段上抗原决定簇的分布。识别主要片段的两种单克隆抗体(2和H-9)可抑制血小板凝集。Mr为250,000的片段与人类血小板结合,且这种结合可被单克隆抗体2和H-9抑制。Mr为250,000的片段不会使血小板凝集,这与血管性血友病因子的高分子量寡聚物对血小板凝集的需求一致。Mr为250,000的片段可与完整的牛血管性血友病因子竞争与人类血小板的结合。然而,其亲和力是完整血管性血友病因子的十分之一。

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