Genetic Contribution to Aging: Deleterious and Helpful Genes Define Life Expectancy

doi:10.1196/annals.1356.003

For the best understanding of aging, we must consider a geneticpool in which genes with negative effects (deleterious genesthat shorten the life span) interact with genes with positiveeffects (helpful genes that promote longevity) in a constantepistatic relationship that results in a modulation of the finalexpression under particular environmental influences. Examplesof deleterious genes affecting aging (predisposition to early-lifepathology and disease) are those that confer risk for developingvascular disease in the heart, brain, or peripheral vessels(APOE, ACE, MTFHR, and mutation at factor II and factor V genes),a gene associated with sporadic late-onset Alzheimer's disease(APOE E4), a polymorphism (COLIA1 Sp1) associated with an increasedfracture risk, and several genetic polymorphisms involved inhormonal metabolism that affect adverse reactions to estrogenreplacement in postmenopausal women. In summary, the processof aging can be regarded as a multifactorial trait that resultsfrom an interaction between stochastic events and sets of epistaticalleles that have pleiotropic age-dependent effects. Lackingthose alleles that predispose to disease and having the longevity-enablinggenes (those beneficial genetic variants that confer diseaseresistance) are probably both important to such a remarkablesurvival advantage.

				I. Irminger-Finger Science of Cancer and Aging J. Clin. Oncol., May 10, 2007; 25(14): 1844 - 1851. [Abstract] [Full Text] [PDF]