AI Article Synopsis

  • - The study examines gene duplication in baker's yeast, focusing on the MLH family of DNA mismatch repair (MMR) proteins, specifically Pms1 and Mlh3, which have evolved to perform specialized functions despite their common ancestry.
  • - Pms1 is key for fixing errors during DNA replication, while Mlh3 resolves chromosome structures during meiosis, showing how duplicated genes can diverge significantly over time, maintaining only 19% similarity.
  • - Research suggests that certain regions of MLH proteins are crucial for their specific roles, and modifications in Mlh3 can compensate for the absence of Pms1, indicating that their ancestor likely performed both functions before specialization.

Article Abstract

Baker's yeast contains a large number of duplicated genes; some function redundantly, whereas others have more specialized roles. We used the MLH family of DNA mismatch repair (MMR) proteins as a model to better understand the steps that lead to gene specialization following a gene duplication event. We focused on two highly conserved yeast MLH proteins, Pms1 and Mlh3, with Pms1 having a major role in the repair of misincorporation events during DNA replication and Mlh3 acting to resolve recombination intermediates in meiosis to form crossovers. The baker's yeast Mlh3 and Pms1 proteins are significantly diverged (19% overall identity), suggesting that an extensive number of evolutionary steps, some major, others involving subtle refinements, took place to diversify the MLH proteins. Using phylogenetic and molecular approaches, we provide evidence that all three domains (N-terminal ATP binding, linker, C-terminal endonuclease/MLH interaction) in the MLH protein family are critical for conferring pathway specificity. Importantly, mlh3 alleles in the ATP binding and endonuclease domains improved MMR functions in strains lacking the Pms1 protein and did not disrupt Mlh3 meiotic functions. This ability for mlh3 alleles to complement the loss of Pms1 suggests that an ancestral Pms1/Mlh3 protein was capable of performing both MMR and crossover functions. Our strategy for analyzing MLH pathway specificity provides an approach to understand how paralogs have evolved to support distinct cellular processes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8495741PMC
http://dx.doi.org/10.1093/g3journal/jkab111DOI Listing

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