Longevity and the genetic determination of collagen glycoxidation kinetics in mammalian senescence

  1. D R Sell,
  2. M A Lane,
  3. W A Johnson,
  4. E J Masoro,
  5. O B Mock,
  6. K M Reiser,
  7. J F Fogarty,
  8. R G Cutler,
  9. D K Ingram,
  10. G S Roth, and
  11. V M Monnier
  1. Institute of Pathology, Case Western Reserve University, Cleveland, OH 44106, USA.

Abstract

A fundamental question in the basic biology of aging is whether there is a universal aging process. If indeed such a process exists, one would expect that it develops at a higher rate in short- versus long-lived species. We have quantitated pentosidine, a marker of glycoxidative stress in skin collagen from eight mammalian species as a function of age. A curvilinear increase was modeled for all species, and the rate of increase correlated inversely with maximum life-span. Dietary restriction, a potent intervention associated with increased life-span, markedly inhibited glycoxidation rate in the rodent. On the assumption that collagen turnover rate is primarily influenced by the crosslinking due to glycoxidation, these results suggest that there is a progressive age-related deterioration of the process that controls the collagen glycoxidation rate. Thus, the ability to withstand damage due to glycoxidation and the Maillard reaction may be under genetic control.

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  1. PNAS January 9, 1996 vol. 93 no. 1 485-490
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