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Literature DB >> 22871458

Genotype×age interaction in human transcriptional ageing.

Jack W Kent¹, Harald H H Göring, Jac C Charlesworth, Eugene Drigalenko, Vincent P Diego, Joanne E Curran, Matthew P Johnson, Thomas D Dyer, Shelley A Cole, Jeremy B M Jowett, Michael C Mahaney, Anthony G Comuzzie, Laura Almasy, Eric K Moses, John Blangero, Sarah Williams-Blangero.

Abstract

Individual differences in biological ageing (i.e., the rate of physiological response to the passage of time) may be due in part to genotype-specific variation in gene action. However, the sources of heritable variation in human age-related gene expression profiles are largely unknown. We have profiled genome-wide expression in peripheral blood mononuclear cells from 1240 individuals in large families and found 4472 human autosomal transcripts, representing ~4349 genes, significantly correlated with age. We identified 623 transcripts that show genotype by age interaction in addition to a main effect of age, defining a large set of novel candidates for characterization of the mechanisms of differential biological ageing. We applied a novel SNP genotype × age interaction test to one of these candidates, the ubiquilin-like gene UBQLNL, and found evidence of joint cis-association and genotype by age interaction as well as trans-genotype by age interaction for UBQLNL expression. Both UBQLNL expression levels at recruitment and cis genotype are associated with longitudinal cancer risk in our study cohort.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Year: 2012 PMID： 22871458 PMCID： PMC3541784 DOI： 10.1016/j.mad.2012.07.005

Source DB: PubMed Journal: Mech Ageing Dev ISSN： 0047-6374 Impact factor: 5.432

36 in total

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