Different mutator phenotypes in
            <i>Mlh1</i>
            - versus
            <i>Pms2</i>
            -deficient mice

Yao, Xiang; Buermeyer, Andrew B.; Narayanan, Latha; Tran, Doan Duy Hai; Baker, Sean M.; Prolla, Tomas A.; Glazer, Peter M.; Liskay, R. Michael; Arnheim, Norman

doi:10.1073/pnas.96.12.6850

Cited by 120 publications

(91 citation statements)

References 37 publications

(46 reference statements)

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“…This study revealed a signi®cant di erence between the expansion and contraction mutations within these repeats, which resulted in elevated frameshift mutant frequencies in Mlh1 7/7 mice (Yao et al, 1999). With the lacI reporter system, however, we did not ®nd a similar di erence in expansions and contractions.…”

Section: Discussioncontrasting

confidence: 54%

“…The discordant tumor spectrum of the Mlh1 7/7 and Pms2 7/7 mice has suggested a di erential role for these two proteins in tumor formation, likely as a result of di erences in genomic instability. In keeping with this, Yao et al (1999) recently demonstrated that mice de®cient in Mlh1 exhibited a greater degree of instability at repetitive sequences than did mice lacking Pms2.…”

Section: Introductionmentioning

confidence: 65%

“…Recently, a study of microsatellite instabilities and frameshift mutations in mono-and dinucleotide repeats was carried out in Mlh1 7/7 and Pms2 7/7 mice (Yao et al, 1999). This study revealed a signi®cant di erence between the expansion and contraction mutations within these repeats, which resulted in elevated frameshift mutant frequencies in Mlh1 7/7 mice (Yao et al, 1999).…”

Section: Discussionmentioning

confidence: 96%

“…Mutant frequencies and mutation spectra depend not only on the speci®c reporter genes employed, but also such variables as sequence context, DNA methylation, chromosomal location and transcriptional activity (Dogliotti, 1996). The lacI gene, for example, lacks long mononucleotide repeats such as those present within the supF reporter gene or microsatellite sequences used by Yao et al (1999). Indeed, as lacI gene mononucleotide repeats are generally 56 nucleotides in length, it is possible that di erences in the ratio of expansions-to-contractions in Mlh1 7/7 and Pms2 7/7 mice are not possible to observe with the lacI reporter system.…”

Section: Discussionmentioning

confidence: 99%

See 3 more Smart Citations

Elevated mutant frequencies and increased C : G→T : A transitions in Mlh1−/− versus Pms2−/− murine small intestinal epithelial cells

et al. 2001

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Section: Discussioncontrasting

confidence: 54%

Section: Introductionmentioning

confidence: 65%

Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

See 2 more Smart Citations

Elevated mutant frequencies and increased C : G→T : A transitions in Mlh1−/− versus Pms2−/− murine small intestinal epithelial cells

et al. 2001

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“…Another set of related experiments studies microsatellite mutations in vivo but in organisms whose mismatch repair system has been knocked out. For an example in mice see [55] and in yeast see [36]. There are many more microsatellite mutations in individuals with deficient mismatch repair systems, and this is informative for studying microsatellite models, but in addition to the rate the pattern of mutations also appears to be different in these individuals.…”

Section: Experiments and Analysismentioning

confidence: 99%

Models of Microsatellite Evolution

Calabrese

Sainudiin

Statistical Methods in Molecular Evolution

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Human DNA repair genes

Ronen

Glickman

2001

Environ and Mol Mutagen

142

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DNA repair systems are essential for the maintenance of genome integrity. Consequently, the disregulation of repair genes can be expected to be associated with significant, detrimental health effects, which can include an increased prevalence of birth defects, an enhancement of cancer risk, and an accelerated rate of aging. Although original insights into DNA repair and the genes responsible were largely derived from studies in bacteria and yeast, well over 125 genes directly involved in DNA repair have now been identified in humans, and their cDNA sequence established. These genes function in a diverse set of pathways that involve the recognition and removal of DNA lesions, tolerance to DNA damage, and protection from errors of incorporation made during DNA replication or DNA repair. Additional genes indirectly affect DNA repair, by regulating the cell cycle, ostensibly to provide an opportunity for repair or to direct the cell to apoptosis. For about 70 of the DNA repair genes listed in Table I, both the genomic DNA sequence and the cDNA sequence and chromosomal location have been elucidated. In 45 cases single-nucleotide polymorphisms have been identified and, in some cases, genetic variants have been associated with specific disorders. With the accelerating rate of gene discovery, the number of identified DNA repair genes and sequence variants is quickly rising. This report tabulates the current status of what is known about these genes. The report is limited to genes whose function is directly related to DNA repair.

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Different mutator phenotypes in Mlh1 - versus Pms2 -deficient mice

Cited by 120 publications

References 37 publications

Elevated mutant frequencies and increased C : G→T : A transitions in Mlh1−/− versus Pms2−/− murine small intestinal epithelial cells

Elevated mutant frequencies and increased C : G→T : A transitions in Mlh1−/− versus Pms2−/− murine small intestinal epithelial cells

Models of Microsatellite Evolution

Human DNA repair genes

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