叉头框转录因子 3(FOXO3)基因变异与人类衰老:编码变异可能不是关键因素。
FOXO3 gene variants and human aging: coding variants may not be key players.
机构信息
Honolulu Heart Program, Kuakini Medical Center, Honolulu Hawaii, USA.
出版信息
J Gerontol A Biol Sci Med Sci. 2012 Nov;67(11):1132-9. doi: 10.1093/gerona/gls067. Epub 2012 Mar 28.
Abstract
FOXO3 is generally recognized as a "master" gene in aging since its association with longevity has been replicated in multiple organisms and human populations. A group of single nucleotide polymorphisms in linkage disequilibrium with a coding region has been associated with human longevity, but the actual functional variant is unidentified. Therefore, we sequenced the coding region in our long-lived Japanese American population in order to enhance resources for fine mapping this region. We demonstrate that of 38 published variants, 6 are misalignments with homologous nonallelic sequences from FOXO3B (ZNF286B), a pseudogene on a different chromosome; 2 are attributable to ZNF286B only, and the remaining 30 were unconfirmed, indicating that they are very rare and not likely involved in longevity. Furthermore, we identified a novel, unique, nonsynonymous coding variant in exon 3 (Gly566Ala; rs138174682) that is prevalent in multiple ethnic groups but appeared too rare for major longevity effects in our study populations.
摘要
FOXO3 通常被认为是衰老过程中的“主”基因,因为它与长寿的关联在多种生物和人类群体中得到了复制。一组与编码区域连锁不平衡的单核苷酸多态性与人类长寿有关,但实际的功能变体尚未确定。因此,我们对我们的长寿日本裔美国人进行了 FOXO3 编码区的测序,以增强对该区域精细作图的资源。我们证明,在 38 个已发表的变体中,有 6 个与 FOXO3B(ZNF286B)同源非等位序列不匹配,而 ZNF286B 是位于不同染色体上的假基因;有 2 个仅归因于 ZNF286B,其余 30 个未得到确认,表明它们非常罕见,不太可能与长寿有关。此外,我们在第 3 外显子中鉴定出一个独特的非同义编码变异(Gly566Ala;rs138174682),该变异在多个族群中普遍存在,但在我们的研究人群中,这种变异太罕见,不太可能对长寿有主要影响。
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