Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.

Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.

Meiotic recombination safeguards proper segregation of homologous chromosomes into gametes, affects genetic variation within species, and contributes to meiotic chromosome recognition, pairing and synapsis. The Prdm9 gene has a dual role, it controls meiotic recombination by determining the genomic...

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Main Authors: Maria Balcova, Barbora Faltusova, Vaclav Gergelits, Tanmoy Bhattacharyya, Ondrej Mihola, Zdenek Trachtulec, Corinna Knopf, Vladana Fotopulosova, Irena Chvatalova, Sona Gregorova, Jiri Forejt
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2016-04-01
Series:PLoS Genetics
Online Access:http://europepmc.org/articles/PMC4841592?pdf=render
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spelling doaj-a71f05be23e34a5abf3ec431383f05a62020-11-24T21:32:38ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042016-04-01124e100590610.1371/journal.pgen.1005906Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.Maria BalcovaBarbora FaltusovaVaclav GergelitsTanmoy BhattacharyyaOndrej MiholaZdenek TrachtulecCorinna KnopfVladana FotopulosovaIrena ChvatalovaSona GregorovaJiri ForejtMeiotic recombination safeguards proper segregation of homologous chromosomes into gametes, affects genetic variation within species, and contributes to meiotic chromosome recognition, pairing and synapsis. The Prdm9 gene has a dual role, it controls meiotic recombination by determining the genomic position of crossover hotspots and, in infertile hybrids of house mouse subspecies Mus m. musculus (Mmm) and Mus m. domesticus (Mmd), it further functions as the major hybrid sterility gene. In the latter role Prdm9 interacts with the hybrid sterility X 2 (Hstx2) genomic locus on Chromosome X (Chr X) by a still unknown mechanism. Here we investigated the meiotic recombination rate at the genome-wide level and its possible relation to hybrid sterility. Using immunofluorescence microscopy we quantified the foci of MLH1 DNA mismatch repair protein, the cytological counterparts of reciprocal crossovers, in a panel of inter-subspecific chromosome substitution strains. Two autosomes, Chr 7 and Chr 11, significantly modified the meiotic recombination rate, yet the strongest modifier, designated meiotic recombination 1, Meir1, emerged in the 4.7 Mb Hstx2 genomic locus on Chr X. The male-limited transgressive effect of Meir1 on recombination rate parallels the male-limited transgressive role of Hstx2 in hybrid male sterility. Thus, both genetic factors, the Prdm9 gene and the Hstx2/Meir1 genomic locus, indicate a link between meiotic recombination and hybrid sterility. A strong female-specific modifier of meiotic recombination rate with the effect opposite to Meir1 was localized on Chr X, distally to Meir1. Mapping Meir1 to a narrow candidate interval on Chr X is an important first step towards positional cloning of the respective gene(s) responsible for variation in the global recombination rate between closely related mouse subspecies.http://europepmc.org/articles/PMC4841592?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Maria Balcova
Barbora Faltusova
Vaclav Gergelits
Tanmoy Bhattacharyya
Ondrej Mihola
Zdenek Trachtulec
Corinna Knopf
Vladana Fotopulosova
Irena Chvatalova
Sona Gregorova
Jiri Forejt
spellingShingle Maria Balcova
Barbora Faltusova
Vaclav Gergelits
Tanmoy Bhattacharyya
Ondrej Mihola
Zdenek Trachtulec
Corinna Knopf
Vladana Fotopulosova
Irena Chvatalova
Sona Gregorova
Jiri Forejt
Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.
PLoS Genetics
author_facet Maria Balcova
Barbora Faltusova
Vaclav Gergelits
Tanmoy Bhattacharyya
Ondrej Mihola
Zdenek Trachtulec
Corinna Knopf
Vladana Fotopulosova
Irena Chvatalova
Sona Gregorova
Jiri Forejt
author_sort Maria Balcova
title Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.
title_short Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.
title_full Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.
title_fullStr Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.
title_full_unstemmed Hybrid Sterility Locus on Chromosome X Controls Meiotic Recombination Rate in Mouse.
title_sort hybrid sterility locus on chromosome x controls meiotic recombination rate in mouse.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2016-04-01
description Meiotic recombination safeguards proper segregation of homologous chromosomes into gametes, affects genetic variation within species, and contributes to meiotic chromosome recognition, pairing and synapsis. The Prdm9 gene has a dual role, it controls meiotic recombination by determining the genomic position of crossover hotspots and, in infertile hybrids of house mouse subspecies Mus m. musculus (Mmm) and Mus m. domesticus (Mmd), it further functions as the major hybrid sterility gene. In the latter role Prdm9 interacts with the hybrid sterility X 2 (Hstx2) genomic locus on Chromosome X (Chr X) by a still unknown mechanism. Here we investigated the meiotic recombination rate at the genome-wide level and its possible relation to hybrid sterility. Using immunofluorescence microscopy we quantified the foci of MLH1 DNA mismatch repair protein, the cytological counterparts of reciprocal crossovers, in a panel of inter-subspecific chromosome substitution strains. Two autosomes, Chr 7 and Chr 11, significantly modified the meiotic recombination rate, yet the strongest modifier, designated meiotic recombination 1, Meir1, emerged in the 4.7 Mb Hstx2 genomic locus on Chr X. The male-limited transgressive effect of Meir1 on recombination rate parallels the male-limited transgressive role of Hstx2 in hybrid male sterility. Thus, both genetic factors, the Prdm9 gene and the Hstx2/Meir1 genomic locus, indicate a link between meiotic recombination and hybrid sterility. A strong female-specific modifier of meiotic recombination rate with the effect opposite to Meir1 was localized on Chr X, distally to Meir1. Mapping Meir1 to a narrow candidate interval on Chr X is an important first step towards positional cloning of the respective gene(s) responsible for variation in the global recombination rate between closely related mouse subspecies.
url http://europepmc.org/articles/PMC4841592?pdf=render
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