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人补体第一成分抑制剂C1:cDNA克隆的特性及基因在11号染色体上的定位

Human inhibitor of the first component of complement, C1: characterization of cDNA clones and localization of the gene to chromosome 11.

作者信息

Davis A E, Whitehead A S, Harrison R A, Dauphinais A, Bruns G A, Cicardi M, Rosen F S

出版信息

Proc Natl Acad Sci U S A. 1986 May;83(10):3161-5. doi: 10.1073/pnas.83.10.3161.

Abstract

C1 inhibitor is a heavily glycosylated plasma protein that regulates the activity of the first component of complement (C1) by inactivation of the serine protease subcomponents, C1r and C1s. C1 inhibitor cDNA clones have been isolated, and one of these (pC1INH1, 950 base pairs) has been partially sequenced. Sequence analysis demonstrates that the C1 inhibitor is a member of the serpin "superfamily" of protease inhibitors. In the region sequenced, C1 inhibitor has 22% identity with antithrombin III, 26% with alpha 1-antitrypsin and alpha 1-antichymotrypsin, and 18% with human angiotensinogen. C1 inhibitor has a larger amino-terminal extension than do the other plasma protease inhibitors. In addition, inspection of residues that are invariant among the other protease inhibitors shows that C1 inhibitor differs at 14 of 41 of these positions. Thus, it appears that C1 inhibitor diverged from the group relatively early in evolution, although probably after the divergence of angiotensinogen. Southern blot analysis of BamHI-digested DNA from normal individuals and from rodent-human somatic cell hybrid cell lines (that contain a limited but varied human chromosome complement) was used to localize the human C1 inhibitor gene to chromosome 11.

摘要

C1抑制剂是一种高度糖基化的血浆蛋白,它通过使丝氨酸蛋白酶亚成分C1r和C1s失活来调节补体第一成分(C1)的活性。已分离出C1抑制剂的cDNA克隆,其中之一(pC1INH1,950个碱基对)已进行了部分测序。序列分析表明,C1抑制剂是蛋白酶抑制剂丝氨酸蛋白酶抑制剂“超家族”的成员。在测序区域,C1抑制剂与抗凝血酶III有22%的同源性,与α1-抗胰蛋白酶和α1-抗糜蛋白酶有26%的同源性,与人类血管紧张素原18%的同源性。C1抑制剂的氨基末端延伸比其他血浆蛋白酶抑制剂更大。此外,检查其他蛋白酶抑制剂中不变的残基表明,C1抑制剂在这些位置的41个中有14个不同。因此,尽管可能在血管紧张素原分化之后,但C1抑制剂似乎在进化过程中相对较早地从该组中分化出来。对来自正常个体和啮齿动物-人类体细胞杂交细胞系(含有有限但多样的人类染色体组)的经BamHI消化的DNA进行Southern印迹分析,用于将人类C1抑制剂基因定位到11号染色体上。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ea0a/323472/5233ef31b594/pnas00314-0122-a.jpg

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