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α5(IV)胶原蛋白的分子克隆及该基因在含有奥尔波特综合征基因座的X染色体区域的定位。

Molecular cloning of alpha 5(IV) collagen and assignment of the gene to the region of the X chromosome containing the Alport syndrome locus.

作者信息

Myers J C, Jones T A, Pohjolainen E R, Kadri A S, Goddard A D, Sheer D, Solomon E, Pihlajaniemi T

机构信息

Department of Biochemistry and Biophysics, University of Pennsylvania School of Medicine, Philadelphia 19104-6059.

出版信息

Am J Hum Genet. 1990 Jun;46(6):1024-33.

Abstract

Type IV collagen is a major structural component of basement membranes. Four constituent polypeptides have been described and characterized to different degrees. Whereas the primary structure of the alpha 1(IV) and alpha 2(IV) chains has been completely established, only short protein sequences have been reported for the recently recognized alpha 3(IV) and alpha 4(IV) subunits. We have isolated overlapping human cDNA clones whose derived amino acid sequence is highly homologous to the alpha 1(IV) and alpha 2(IV) chains. However, these clones code for neither alpha 3(IV) nor alpha 4(IV), and thus this new polypeptide has been designated the alpha 5 chain of type IV collagen. To determine whether the gene encoding the alpha 5(IV) chain is syntenic with the contiguously arranged alpha 1(IV) and alpha 2(IV) genes at 13q34, the alpha 5(IV) cloned DNA was hybridized to genomic DNA from somatic cell hybrids and to metaphase chromosomes. The results demonstrated that the alpha 5(IV) collagen gene is located on the long arm of the X chromosome. Since 14 collagen genes have previously been assigned to nine autosomes, these data represent the first mapping of a collagen gene to the X chromosome. Most important, the alpha 5(IV) gene has been sublocalized to bands Xq22----q23, which are in the same region known to contain the locus for the X-linked form of Alport syndrome. It is therefore possible that this severe dominantly inherited nephritis, manifested by splitting of the glomerular basement membrane, could be caused by mutations in the alpha 5(IV) collagen gene.

摘要

IV型胶原是基底膜的主要结构成分。已描述了四种组成多肽,并对其进行了不同程度的表征。虽然α1(IV)和α2(IV)链的一级结构已完全确定,但对于最近发现的α3(IV)和α4(IV)亚基,仅报道了短的蛋白质序列。我们分离出了重叠的人cDNA克隆,其推导的氨基酸序列与α1(IV)和α2(IV)链高度同源。然而,这些克隆既不编码α3(IV)也不编码α4(IV),因此这种新的多肽被命名为IV型胶原的α5链。为了确定编码α5(IV)链的基因是否与位于13q34的相邻排列的α1(IV)和α2(IV)基因同线,将克隆的α5(IV)DNA与体细胞杂种的基因组DNA以及中期染色体进行杂交。结果表明,α5(IV)胶原基因位于X染色体的长臂上。由于先前已将14个胶原基因定位到9条常染色体上,这些数据代表了胶原基因首次定位到X染色体上。最重要的是,α5(IV)基因已被定位到Xq22----q23带,该区域与已知包含X连锁型Alport综合征基因座的区域相同。因此,这种以肾小球基底膜分裂为特征的严重显性遗传性肾炎可能是由α5(IV)胶原基因突变引起的。

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