Meiotic DNA exchanges inC. elegansare promoted by proximity to the synaptonemal complex

Author:

Almanzar David E1,Gordon Spencer G1,Bristow Chloe1,Hamrick Antonia1,von Diezmann Lexy1,Liu Hanwenheng1ORCID,Rog Ofer1ORCID

Affiliation:

1. School of Biological Sciences and Center for Cell and Genome Sciences, University of Utah

Abstract

During meiosis, programmed double-strand DNA breaks are repaired to form exchanges between the parental chromosomes called crossovers. Chromosomes lacking a crossover fail to segregate accurately into the gametes, leading to aneuploidy. In addition to engaging the homolog, crossover formation requires the promotion of exchanges, rather than non-exchanges, as repair products. However, the mechanism underlying this meiosis-specific preference is not fully understood. Here, we study the regulation of meiotic sister chromatid exchanges inCaenorhabditis elegansby direct visualization. We find that a conserved chromosomal interface that promotes exchanges between the parental chromosomes, the synaptonemal complex, can also promote exchanges between the sister chromatids. In both cases, exchanges depend on the recruitment of the same set of pro-exchange factors to repair sites. Surprisingly, although the synaptonemal complex usually assembles between the two DNA molecules undergoing an exchange, its activity does not rely on a specific chromosome conformation. This suggests that the synaptonemal complex regulates exchanges—both crossovers and sister exchanges—by establishing a nuclear domain conducive to nearby recruitment of exchange-promoting factors.

Publisher

Life Science Alliance, LLC

Subject

Health, Toxicology and Mutagenesis,Plant Science,Biochemistry, Genetics and Molecular Biology (miscellaneous),Ecology

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