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doi:10.1534/genetics.105.047092
A more recent version of this article appeared on December 1, 2005.
REGULAR RESEARCH PAPERS |
Analysis of repeat-mediated deletions in the mitochondrial genome of Saccharomyces cerevisiae
Naina Phadnis 1, Rey A. Sia 2 and Elaine A. Sia 1*
1 University of Rochester
2 SUNY Brockport
* To whom correspondence should be addressed. E-mail: esia{at}mail.rochester.edu.
Submitted on June 20, 2005
Revised on August 15, 2005
Accepted on 26 August 2005
Mitochondrial DNA deletions and point mutations accumulate in an age-dependent manner in mammals. The mitochondrial genome in aging humans often displays a 4977 bp deletion flanked by short direct repeats. Additionally, direct repeats flank two-thirds of the reported mitochondrial DNA deletions. The mechanism by which these deletions arise is unknown, but direct repeat-mediated deletion involving polymerase slippage, homologous recombination and non-homologous end joining have been proposed. We have developed a genetic reporter to measure the rate at which direct-repeat-mediated deletions arise in the mitochondrial genome of Saccharomyces cerevisiae. Here we analyze the effect of repeat size and heterology between repeats on the rate of deletions. We find that the dependence on homology for repeat-mediated deletions is linear down to 33 bp. Heterology between repeats does not affect the deletion rate substantially. Analysis of recombination products suggests that the deletions are produced by at least two different pathways, one that generates only deletions and one that appears to generate both deletions and reciprocal products of recombination. We discuss how this reporter may be used to identify the proteins in yeast that have an impact on the generation of direct repeat-mediated deletions.
Key Words: DNA deletions, Direct repeats, Mitochondria, Recombination
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