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本文引用的文献

1
Identifying the genomic determinants of aging and longevity in human population studies: progress and challenges.在人类群体研究中鉴定衰老和长寿的基因组决定因素:进展与挑战。
Bioessays. 2013 Apr;35(4):386-96. doi: 10.1002/bies.201200148. Epub 2013 Feb 19.
2
Genetic investigation of FOXO3A requires special attention due to sequence homology with FOXO3B.由于 FOXO3A 与 FOXO3B 具有序列同源性,因此对其进行遗传研究需要特别注意。
Eur J Hum Genet. 2013 Feb;21(2):240-2. doi: 10.1038/ejhg.2012.83. Epub 2012 May 16.
3
FOXO3 gene variants and human aging: coding variants may not be key players.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。
J Gerontol A Biol Sci Med Sci. 2012 Nov;67(11):1132-9. doi: 10.1093/gerona/gls067. Epub 2012 Mar 28.
4
A genome-wide association study confirms APOE as the major gene influencing survival in long-lived individuals.一项全基因组关联研究证实 APOE 是影响长寿个体生存的主要基因。
Mech Ageing Dev. 2011 Jun-Jul;132(6-7):324-30. doi: 10.1016/j.mad.2011.06.008. Epub 2011 Jun 29.
5
Genetic variability of the forkhead box O3 and prostate cancer risk in the European Prospective Investigation on Cancer.FOXO3 基因多态性与欧洲癌症前瞻性调查中的前列腺癌风险。
Oncol Rep. 2011 Oct;26(4):979-86. doi: 10.3892/or.2011.1359. Epub 2011 Jun 24.
6
Genome-wide association study identifies a single major locus contributing to survival into old age; the APOE locus revisited.全基因组关联研究确定了一个单一的主要基因座,有助于延长寿命进入老年;重新研究 APOE 基因座。
Aging Cell. 2011 Aug;10(4):686-98. doi: 10.1111/j.1474-9726.2011.00705.x. Epub 2011 May 6.
7
Heritability analysis of life span in a semi-isolated population followed across four centuries reveals the presence of pleiotropy between life span and reproduction.对跨越四个世纪的半隔离种群寿命进行遗传分析,揭示了寿命与繁殖之间存在多效性。
J Gerontol A Biol Sci Med Sci. 2011 Jan;66(1):26-37. doi: 10.1093/gerona/glq163. Epub 2010 Sep 24.
8
Genetic variation in insulin/IGF-1 signaling pathways and longevity.胰岛素/IGF-1 信号通路的遗传变异与长寿。
Ageing Res Rev. 2011 Apr;10(2):201-4. doi: 10.1016/j.arr.2010.09.002. Epub 2010 Sep 22.
9
Replication of an association of variation in the FOXO3A gene with human longevity using both case-control and longitudinal data.利用病例对照和纵向数据复制 FOXO3A 基因变异与人类长寿之间的关联。
Aging Cell. 2010 Dec;9(6):1010-7. doi: 10.1111/j.1474-9726.2010.00627.x. Epub 2010 Oct 21.
10
FOXO3 encodes a carcinogen-activated transcription factor frequently deleted in early-stage lung adenocarcinoma.FOXO3 编码一种致癌物激活的转录因子,该转录因子在早期肺腺癌中经常缺失。
Cancer Res. 2010 Aug 1;70(15):6205-15. doi: 10.1158/0008-5472.CAN-09-4008. Epub 2010 Jul 14.

对吸烟因素进行调整并不会改变FOXO3A基因与长寿之间的关联。

Adjustment for smoking does not alter the FOXO3A association with longevity.

作者信息

Däumer Carolin, Flachsbart Friederike, Caliebe Amke, Schreiber Stefan, Nebel Almut, Krawczak Michael

机构信息

Institute of Medical Informatics and Statistics, Christian-Albrechts University, Brunswiker Straße 10, 24105, Kiel, Germany.

出版信息

Age (Dordr). 2014 Apr;36(2):911-21. doi: 10.1007/s11357-013-9578-z. Epub 2013 Sep 7.

DOI:10.1007/s11357-013-9578-z
PMID:24014251
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4039245/
Abstract

Human longevity is a multifactorial phenotype influenced by both genetic and environmental factors. Despite its heritability of 25-32 %, the genetic background of longevity is as yet largely unexplained. Apart from APOE status, variation in the FOXO3A gene is the only confirmed genetic contributor to survival into old age. On the other hand, FOXO3A activity is known to be downregulated in various cancers, and the gene was recently identified as a novel deletion hotspot in human lung adenocarcinoma. In view of the strong association between smoking and lung cancer, we set out to explore whether smoking modifies the known association between FOXO3A variation and longevity. To this end, we conducted a case-control study in two different populations, drawing upon extensive collections of old-aged individuals and younger controls available to us (1,613 German centenarians/nonagenarians and 1,104 controls; 1,088 Danish nonagenarians and 736 controls). In the German sample, 21 single nucleotide polymorphisms (SNPs) from the FOXO3A gene region were genotyped, whereas 15 FOXO3A SNPs were analyzed in the Danish sample. Eight SNPs were typed in both populations. Logistic regression analysis revealed that adjustment for smoking does not systematically alter the association between FOXO3A variation and longevity in neither population. Our analysis therefore suggests that the said association is not largely due to the confounding effects of lung cancer.

摘要

人类长寿是一种受遗传和环境因素影响的多因素表型。尽管其遗传率为25%-32%,但长寿的遗传背景在很大程度上仍未得到解释。除了载脂蛋白E(APOE)状态外,叉头框蛋白O3A(FOXO3A)基因的变异是唯一已证实的与活到老年有关的遗传因素。另一方面,已知FOXO3A活性在各种癌症中下调,并且该基因最近被确定为人类肺腺癌中的一个新的缺失热点。鉴于吸烟与肺癌之间的密切关联,我们着手探讨吸烟是否会改变FOXO3A变异与长寿之间已知的关联。为此,我们在两个不同人群中进行了一项病例对照研究,利用了我们可获得的大量老年个体和年轻对照样本(1613名德国百岁老人/九旬老人和1104名对照;1088名丹麦九旬老人和736名对照)。在德国样本中,对FOXO3A基因区域的21个单核苷酸多态性(SNP)进行了基因分型,而在丹麦样本中分析了15个FOXO3A SNP。在两个人群中都对8个SNP进行了分型。逻辑回归分析显示,对吸烟进行校正后,两个人群中FOXO3A变异与长寿之间的关联均未发生系统性改变。因此,我们的分析表明,上述关联很大程度上并非由于肺癌的混杂效应。