Rate volatility and asymmetric segregation diversify mutation burden in mutator cells

Abstract: Mutations that compromise mismatch repair (MMR) or DNA polymerase exonuclease 11domains produce mutator phenotypes capable of fueling cancer evolution. Tandem 12 defects in these pathways dramatically increase mutation rate. Here, we model how 13 mutator phenotypes expand genetic heterogeneity in budding yeast cells using a single-14 cell resolution approach that tallies all replication errors arising from individual 15divisions. The distribution of count data from cells lacking MMR and polymerase 16 proofread… Show more