主要组织相容性位点的补体成分。

R R Porter
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引用次数: 33

摘要

补体成分的多态性,通过其抗原特异性或电泳迁移性的差异,以及对遗传缺陷的研究,已经使许多补体结构基因得以定位。在人类中,3个基因(C2、C4和因子B)被放置在6号染色体上的HLA-D和HLA-B之间,在小鼠中,C4被放置在17号染色体上的H2-I和H2-D之间。结构研究表明,这些构件具有特殊的特征。含有C3和C5转化酶蛋白水解活性位点的C2和因子B分别属于经典途径和替代途径,在结构和功能上相似。两者都是新型的丝氨酸蛋白酶。C4(和C3一样)含有一个对溶血活性至关重要的链内硫酯键。分子遗传学研究正在确定这些基因的相对位置和它们的精确结构,并应阐明它们与与这部分人类基因组缺陷相关的遗传疾病的关系。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The complement components of the major histocompatibility locus.
Polymorphism of complement components, recognized by differences in either their antigenic specificity or their electrophoretic mobility, together with studies of inherited deficiencies, has enabled many of their structural genes to be mapped. In humans, three genes (for C2, C4, and factor B) have been placed between HLA-D and HLA-B on chromosome 6 and in mice, C4 between H2-I and H2-D, chromosome 17. Structural studies show that these components have exceptional features. C2 and factor B which contain the proteolytic active site of the C3 and C5 convertases are of the classical and alternative pathway respectively and are similar in structure and function. Both are novel types of serine proteases. C4 (as C3) contains an intrachain thioester bond essential for hemolytic activity. Molecular genetic investigations are determining the relative positions of these genes, and their precise structure, and should clarify their relation to the inherited diseases which are associated with defects in this section of the human genome.
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