Concerted action of the MutLβ heterodimer and Mer3 helicase regulates the global extent of meiotic gene conversion

نویسندگان

  • Yann Duroc
  • Rajeev Kumar
  • Lepakshi Ranjha
  • Céline Adam
  • Raphaël Guérois
  • Khan Md Muntaz
  • Marie-Claude Marsolier-Kergoat
  • Florent Dingli
  • Raphaëlle Laureau
  • Damarys Loew
  • Bertrand Llorente
  • Jean-Baptiste Charbonnier
  • Petr Cejka
  • Valérie Borde
چکیده

Gene conversions resulting from meiotic recombination are critical in shaping genome diversification and evolution. How the extent of gene conversions is regulated is unknown. Here we show that the budding yeast mismatch repair related MutLβ complex, Mlh1-Mlh2, specifically interacts with the conserved meiotic Mer3 helicase, which recruits it to recombination hotspots, independently of mismatch recognition. This recruitment is essential to limit gene conversion tract lengths genome-wide, without affecting crossover formation. Contrary to expectations, Mer3 helicase activity, proposed to extend the displacement loop (D-loop) recombination intermediate, does not influence the length of gene conversion events, revealing non-catalytical roles of Mer3. In addition, both purified Mer3 and MutLβ preferentially recognize D-loops, providing a mechanism for limiting gene conversion in vivo. These findings show that MutLβ is an integral part of a new regulatory step of meiotic recombination, which has implications to prevent rapid allele fixation and hotspot erosion in populations.

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عنوان ژورنال:

دوره 6  شماره 

صفحات  -

تاریخ انتشار 2017