| Literature DB >> 11950998 |
Jan de Boer1, Jaan Olle Andressoo, Jan de Wit, Jan Huijmans, Rudolph B Beems, Harry van Steeg, Geert Weeda, Gijsbertus T J van der Horst, Wibeke van Leeuwen, Axel P N Themmen, Morteza Meradji, Jan H J Hoeijmakers.
Abstract
One of the factors postulated to drive the aging process is the accumulation of DNA damage. Here, we provide strong support for this hypothesis by describing studies of mice with a mutation in XPD, a gene encoding a DNA helicase that functions in both repair and transcription and that is mutated in the human disorder trichothiodystrophy (TTD). TTD mice were found to exhibit many symptoms of premature aging, including osteoporosis and kyphosis, osteosclerosis, early greying, cachexia, infertility, and reduced life-span. TTD mice carrying an additional mutation in XPA, which enhances the DNA repair defect, showed a greatly accelerated aging phenotype, which correlated with an increased cellular sensitivity to oxidative DNA damage. We hypothesize that aging in TTD mice is caused by unrepaired DNA damage that compromises transcription, leading to functional inactivation of critical genes and enhanced apoptosis.Entities:
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Year: 2002 PMID: 11950998 DOI: 10.1126/science.1070174
Source DB: PubMed Journal: Science ISSN: 0036-8075 Impact factor: 47.728