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因子VIII/血管性血友病因子的复杂多聚体组成。

The complex multimeric composition of factor VIII/von Willebrand factor.

作者信息

Ruggeri Z M, Zimmerman T S

出版信息

Blood. 1981 Jun;57(6):1140-3.

PMID:6784794
Abstract

We have analyzed the multimeric structure of factor VIII/von Willebrand factor in plasma by sodium dodecyl sulfate electrophoresis using gels of varying porosity and a discontinuous buffer system. Factor VIII/von Willebrand factor bands were identified by reaction with 125I-labeled affinity-purified antibody and subsequent autoradiography. In 1% agarose gels, normal plasma displayed a series of sharply defined oligomers. However, increasing the agarose concentration to 2.0% or utilizing mixtures of 0.8% agarose--1.75% acrylamide revealed two bands of lesser intensity interposed between the major bands. When the acrylamide concentration in the gels was increased to 2.5%, bands with a faster mobility than IgM and fibronectin were now evident. Type IIA von Willebrand's disease showed not only an absence of the larger multimers but also a relative increase in several of the newly identified bands as compared to type IIB, type I, and normal. These studies suggest that factor VII/von Willebrand factor in IIA von Willebrand's disease is structurally different from that in other forms of the disorder. They also indicate that the multimeric composition of factor VII/von Willebrand factor is more complex than can be explained by simple linear polymerization of a single protomer.

摘要

我们通过使用不同孔隙率的凝胶和不连续缓冲系统的十二烷基硫酸钠电泳,分析了血浆中凝血因子VIII/血管性血友病因子的多聚体结构。通过与125I标记的亲和纯化抗体反应并随后进行放射自显影来鉴定凝血因子VIII/血管性血友病因子条带。在1%琼脂糖凝胶中,正常血浆显示出一系列清晰定义的寡聚体。然而,将琼脂糖浓度增加到2.0%或使用0.8%琼脂糖-1.75%丙烯酰胺的混合物时,在主要条带之间出现了两条强度较低的条带。当凝胶中的丙烯酰胺浓度增加到2.5%时,出现了迁移率比IgM和纤连蛋白更快的条带。IIA型血管性血友病不仅显示出较大多聚体的缺失,而且与IIB型、I型和正常情况相比,一些新鉴定的条带相对增加。这些研究表明,IIA型血管性血友病中的凝血因子VII/血管性血友病因子在结构上与该疾病的其他形式不同。它们还表明,凝血因子VII/血管性血友病因子的多聚体组成比单一原体的简单线性聚合所能解释的更为复杂。

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