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人类载脂蛋白-J/簇集蛋白基因的多态性:种族差异及在阿尔茨海默病中的分布

Polymorphisms in the human apolipoprotein-J/clusterin gene: ethnic variation and distribution in Alzheimer's disease.

作者信息

Tycko B, Feng L, Nguyen L, Francis A, Hays A, Chung W Y, Tang M X, Stern Y, Sahota A, Hendrie H, Mayeux R

机构信息

Gertrude H. Sergievsky Center, Columbia University, New York, NY 10032, USA.

出版信息

Hum Genet. 1996 Oct;98(4):430-6. doi: 10.1007/s004390050234.

Abstract

Apolipoprotein-J/clusterin (APOJ/CLI) shares many biological properties with apolipoprotein-E (APOE) including, but not limited to, avid binding with beta-amyloid peptide. Thus, APOJ/CLI warrants scrutiny as a candidate Alzheimer's disease (AD) susceptibility gene. We identified seven nucleotide sequence polymorphisms in APOJ/ CLI, two of which, in exon 7, after the predicted amino acid sequence. The JVIIB variant is an asparagine-to-histidine substitution, which deletes a glycosylation signal at amino acid 317; the JVIIC variant is an aspartate-to-asparagine substitution, which forms a new glycosylation signal at position 328. Both of these coding variants, as well as two neutral polymorphisms in exon 2, were more frequent in African-Americans than Hispanics and were rare in Caucasians. However, no individual coding or noncoding variant was consistently associated with AD. At the population level, APOJ/CLI polymorphisms are frequent among persons of African descent, but probably do not alter susceptibility to AD.

摘要

载脂蛋白-J/簇集素(APOJ/CLI)与载脂蛋白-E(APOE)具有许多生物学特性,包括但不限于与β淀粉样肽的紧密结合。因此,APOJ/CLI作为阿尔茨海默病(AD)易感基因值得深入研究。我们在APOJ/CLI中鉴定出7个核苷酸序列多态性,其中两个位于外显子7,在预测的氨基酸序列之后。JVIIB变体是天冬酰胺到组氨酸的替换,它删除了氨基酸317处的一个糖基化信号;JVIIC变体是天冬氨酸到天冬酰胺的替换,它在位置328处形成了一个新的糖基化信号。这两个编码变体以及外显子2中的两个中性多态性在非裔美国人中比西班牙裔更常见,在白种人中则很少见。然而,没有单个编码或非编码变体与AD始终相关。在人群水平上,APOJ/CLI多态性在非洲裔人群中很常见,但可能不会改变对AD的易感性。

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