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人 XVIII 型胶原蛋白两种变体形式的完整一级结构及相应转录本表达的组织特异性差异

Complete primary structure of two variant forms of human type XVIII collagen and tissue-specific differences in the expression of the corresponding transcripts.

作者信息

Saarela J, Ylikärppä R, Rehn M, Purmonen S, Pihlajaniemi T

机构信息

Collagen Research Unit, University of Oulu, Finland.

出版信息

Matrix Biol. 1998 Jan;16(6):319-28. doi: 10.1016/s0945-053x(98)90003-8.

Abstract

We report on full-length human type XVIII collagen cDNAs that encode 1516- or 1336-residue alpha 1 (XVIII) chains. The two chains have different signal peptides and variant N-terminal non-collagenous NC1 domains of 493 (NC1-493) and 303 (NC1-303) amino acid residues, respectively, but share 301 residues of their NC1 domains, a 688-residue highly interrupted collagenous portion, and a 312-residue C-terminal non-collagenous portion. Alternative splicing affecting a 43-residue stretch at the junction of the NC1 domain and the beginning of the collagenous portion was identified. The amino acid sequences of the human and previously characterized mouse alpha 1 (XVIII) chains exhibit an overall identity of 79%. The highest homology between these chains was observed in their last 184 residues, corresponding to the proteolytic fragment endostatin, which is capable of inhibiting endothelial cell proliferation, angiogenesis and tumor growth (O'Reilly, et al., Cell 88: 277-285, 1997). Northern analysis of several adult and fetal tissues with a probe for the NC1-493 variant revealed marked amounts of the corresponding 6.2 and 5.0 kb mRNAs in liver, while other tissues contained only faint or undetectable signals. Hybridizations with a probe specific for the NC1-303 variant virtually lacked the liver signal but revealed clear 5.6 and 4.5 kb bands in heart, kidney, placenta, prostate, ovaries, skeletal muscle and small intestine, and faint signals in several other tissues. Thus mRNAs for the long variant occur prominently in liver, while those for the short variant appear to be the major ones in the other tissues analyzed.

摘要

我们报道了编码1516个或1336个残基的α1(XVIII)链的全长人XVIII型胶原蛋白cDNA。这两条链具有不同的信号肽以及分别为493个(NC1 - 493)和303个(NC1 - 303)氨基酸残基的可变N端非胶原蛋白NC1结构域,但它们的NC1结构域有301个相同残基、一个688个残基的高度间断的胶原部分以及一个312个残基的C端非胶原蛋白部分。已确定在NC1结构域与胶原部分起始处的交界处存在影响43个残基片段的可变剪接。人和先前已表征的小鼠α1(XVIII)链的氨基酸序列总体一致性为79%。这些链之间的最高同源性出现在其最后184个残基中,这部分对应于蛋白水解片段内皮抑素,它能够抑制内皮细胞增殖、血管生成和肿瘤生长(O'Reilly等人,《细胞》88: 277 - 285,1997)。用针对NC1 - 493变体的探针进行的几种成人和胎儿组织的Northern分析显示,肝脏中存在大量相应的6.2 kb和5.0 kb mRNA,而其他组织仅含有微弱或无法检测到的信号。用针对NC1 - 303变体的特异性探针杂交几乎没有肝脏信号,但在心脏、肾脏、胎盘、前列腺、卵巢、骨骼肌和小肠中显示出清晰的5.6 kb和4.5 kb条带,在其他几种组织中显示出微弱信号。因此,长变体的mRNA在肝脏中显著存在,而短变体的mRNA似乎是所分析的其他组织中的主要类型。

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