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肾小球基底膜。IV型胶原非胶原结构域(六聚体)二聚体亚基及Goodpasture抗原的鉴定。

Glomerular basement membrane. Identification of dimeric subunits of the noncollagenous domain (hexamer) of collagen IV and the Goodpasture antigen.

作者信息

Gunwar S, Ballester F, Kalluri R, Timoneda J, Chonko A M, Edwards S J, Noelken M E, Hudson B G

机构信息

Department of Biochemistry & Molecular Biology, University of Kansas Medical Center, Kansas City 66103.

出版信息

J Biol Chem. 1991 Aug 15;266(23):15318-24.

PMID:1869555
Abstract

The noncollagenous (NC1) domain hexamer of glomerular basement membrane (GBM) collagen is composed of a multiplicity of monomeric and dimeric subunits, and specific subunits are the targets for anti-GBM autoantibodies of patients with Goodpasture (GP) syndrome. The identity of GBM monomers has been established and the alpha 3(IV)NC1 monomer identified as the one that binds GP antibodies (Gunwar, S., Saus, J., Noelken, M. E., and Hudson, B. G. (1990) J. Biol. Chem. 265, 5466-5469). In the present study, the chain origin of 25 dimeric components and the identity of those that bound the anti-GBM antibodies from two GP patients were determined. This was accomplished by NH2-terminal sequence analysis and immunoblotting analysis of dimeric components that were resolved by two-dimensional electrophoresis in combination with high pressure liquid chromatography. The results revealed that (a) the components are mainly homodimers of the NC1 domains of alpha 1, alpha 2, alpha 3, alpha 4, and probably alpha 5 chains of collagen IV, reflecting a specificity of promoter-promoter association and (b) each homodimer had several size and charge isoforms. The GP antibodies bound exclusively to both alpha 3(IV)NC1 monomers and dimers and not to other basement membrane constituents. These findings provided new insights about the structure of GBM collagen and together with our previous findings firmly established the alpha 3(IV) chain as the target for the anti-GBM antibodies that mediate glomerulonephritis and pulmonary hemorrhage in patients with Goodpasture syndrome.

摘要

肾小球基底膜(GBM)胶原蛋白的非胶原蛋白(NC1)结构域六聚体由多种单体和二聚体亚基组成,特定亚基是Goodpasture(GP)综合征患者抗GBM自身抗体的靶标。GBM单体的身份已确定,α3(IV)NC1单体被确定为与GP抗体结合的单体(Gunwar,S.,Saus,J.,Noelken,M.E.和Hudson,B.G.(1990)J.Biol.Chem.265,5466 - 5469)。在本研究中,确定了25种二聚体成分的链起源以及来自两名GP患者的与抗GBM抗体结合的成分的身份。这是通过对二维电泳结合高压液相色谱分离的二聚体成分进行NH2末端序列分析和免疫印迹分析来完成的。结果显示:(a)这些成分主要是IV型胶原蛋白α1、α2、α3、α4以及可能的α5链的NC1结构域的同型二聚体,反映了启动子 - 启动子关联的特异性;(b)每个同型二聚体都有几种大小和电荷异构体。GP抗体仅与α3(IV)NC1单体和二聚体结合,而不与其他基底膜成分结合。这些发现为GBM胶原蛋白的结构提供了新的见解,并与我们之前的发现一起牢固地确立了α3(IV)链作为介导Goodpasture综合征患者肾小球肾炎和肺出血的抗GBM抗体的靶标。

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J Biol Chem. 1991 Aug 15;266(23):15318-24.
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