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asymmetric strand segregation epigenetic costs of genetic fidelity不对称链隔离表观遗传基因富达的成本
Asymmetric Strand Segregation: Epigenetic Costs of
Genetic Fidelity?
Diane P. Genereux*
Department of Biology, University of Washington, Seattle, Washington, United States of America
Abstract
Asymmetric strand segregation has been proposed as a mechanism to minimize effective mutation rates in epithelial tissues.
Under asymmetric strand segregation, the double-stranded molecule that contains the oldest DNA strand is preferentially
targeted to the somatic stem cell after each round of DNA replication. This oldest DNA strand is expected to have fewer errors
than younger strands because some of the errors that arise on daughter strands during their synthesis fail to be repaired.
Empirical findings suggest the possibility of asymmetric strand segregation in a subset of mammalian cell lineages, indicating
that it may indeed function to increase genetic fidelity. However, the implications of asymmetric strand segregation for the
fidelity of epigenetic information remain unexplored. Here, I explore the impact of strand-segregation dynamics on epigenetic
fidelity using a mathematical-modelling approach that draws on the known molecular mechanisms of DNA methylation and
existing rate estimates from empirical methylation data. I find that, for a wide range of starting methylation densities,
asymmetric—but not symmetric—strand segregation leads to systematic increases in methylation levels if parent strands are
subject to de novo methylation events. I found that epigenetic fidelity can be compromised when enhanced genetic fidelity is
achieved through asymmetric strand segregation. Strand segregation dynamics could thus explain the increased DNA
methylation densities that are observed in structured cellular populations during aging and in disease.
Citation: Genereux DP (2009) Asymmetric Strand Segregation: Epigenetic Costs of Genetic Fidelity? PL
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