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人血清淀粉样蛋白A。六种主要亚型与三个已发表基因序列的对应关系以及两个基因位点的证据。

Human serum amyloid A protein. The assignment of the six major isoforms to three published gene sequences and evidence for two genetic loci.

作者信息

Strachan A F, Brandt W F, Woo P, van der Westhuyzen D R, Coetzee G A, de Beer M C, Shephard E G, de Beer F C

机构信息

Department of Internal Medicine, University of Stellenbosch Medical School, Tygerberg, Republic of South Africa.

出版信息

J Biol Chem. 1989 Nov 5;264(31):18368-73.

PMID:2808379
Abstract

Serum amyloid A protein (apo-SAA) is an acute-phase reactant and an apolipoprotein of high density lipoproteins (HDL). Six major isoforms of apo-SAA occur in humans (pI 6.0, 6.4, 7.0, 7.4, 7.5, 8.0). In this report we have rationalized the phenotypic expression of apo-SAA isoforms with published apo-SAA structures predicted from apo-SAA cDNA's pA1 and pSAA82 and the genomic DNA SAAg9. The six apo-SAA isoforms fall into three pairs, pI 6.0/6.4, 7.0/7.5, and 7.4/8.0, which are products of cDNA pA1, cDNA pSAA82, and genomic DNA SAAg9, respectively. The second of each isoform pair (i.e. pI 6.4, 7.5, and 8.0) is the "primary" product: a 104-residue peptide with the NH2-terminal sequence Arg-Ser-Phe-Phe. Each primary product is processed either to a major 103-residue peptide with the NH2-terminal sequence Ser-Phe-Phe or processed to a minor 102-residue product which results from the loss of both an Arg and a Ser residue from the NH2 termini. These "secondary" products have the lower pI values of 6.0, 7.0, and 7.4, respectively. The isoelectric points of the SAAg9 products were confirmed by expression of SAAg9 in transfected mouse L-cells. Both the pI 8.0 and 7.4 isoforms were present in cellular extracts, suggesting that post-translational modification of apo-SAA may occur intracellularly. However, the greater relative abundance of the pI 7.4 isoform extracellularly suggests that the major conversion may occur after secretion. Whereas the gene corresponding to the pA1 cDNA sequence does not show allelic variation, the segregation characteristics of the pI 7.0/7.5 and 7.4/8.0 isoform pairs amongst individuals suggests that these isoforms are the products of genes (with sequences corresponding to pSAA82 and SAAg9, respectively) which are allelic variants at a single locus distinct from that for the pI 6.0/6.4 isoform pair.

摘要

血清淀粉样蛋白A(apo-SAA)是一种急性期反应物,也是高密度脂蛋白(HDL)的一种载脂蛋白。人类中存在六种主要的apo-SAA亚型(等电点分别为6.0、6.4、7.0、7.4、7.5、8.0)。在本报告中,我们根据从apo-SAA cDNA的pA1和pSAA82以及基因组DNA SAAg9预测的已发表的apo-SAA结构,对apo-SAA亚型的表型表达进行了合理化分析。六种apo-SAA亚型分为三对,即等电点6.0/6.4、7.0/7.5和7.4/8.0,它们分别是cDNA pA1、cDNA pSAA82和基因组DNA SAAg9的产物。每对等位基因中的第二个(即等电点6.4、7.5和8.0)是“主要”产物:一种含有104个氨基酸残基的肽,其氨基末端序列为精氨酸-丝氨酸-苯丙氨酸-苯丙氨酸。每个主要产物要么被加工成一种主要的含有103个氨基酸残基的肽,其氨基末端序列为丝氨酸-苯丙氨酸-苯丙氨酸,要么被加工成一种次要的含有102个氨基酸残基的产物,该产物是由于氨基末端的一个精氨酸和一个丝氨酸残基缺失而产生的。这些“次要”产物的等电点较低,分别为6.0、7.0和7.4。通过在转染的小鼠L细胞中表达SAAg9,证实了SAAg9产物的等电点。细胞提取物中同时存在等电点8.0和7.4的亚型,这表明apo-SAA的翻译后修饰可能发生在细胞内。然而,细胞外等电点7.4亚型的相对丰度更高,这表明主要的转化可能发生在分泌之后。虽然与pA1 cDNA序列对应的基因没有显示出等位基因变异,但个体中等电点7.0/7.5和7.4/8.0亚型对的分离特征表明,这些亚型是基因(其序列分别对应于pSAA82和SAAg9)的产物,这些基因是位于与等电点6.0/6.4亚型对不同的单一基因座上的等位基因变体。

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