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The ssDNA-binding protein MEIOB acts as a dosage-sensitive regulator of meiotic recombination.


ABSTRACT: Meiotic recombination enables reciprocal exchange of genetic information between parental chromosomes and is essential for fertility. MEIOB, a meiosis-specific ssDNA-binding protein, regulates early meiotic recombination. Here we report that the human infertility-associated missense mutation (N64I) in MEIOB causes protein degradation and reduced crossover formation in mouse testes. Although the MEIOB N64I substitution is associated with human infertility, the point mutant mice are fertile despite meiotic defects. Meiob mutagenesis identifies serine 67 as a critical residue for MEIOB. Biochemically, these two mutations (N64I and S67 deletion) cause self-aggregation of MEIOB and sharply reduced protein half-life. Molecular genetic analyses of both point mutants reveal an important role for MEIOB in crossover formation in late meiotic recombination. Furthermore, we find that the MEIOB protein levels directly correlate with the severity of meiotic defects. Our results demonstrate that MEIOB regulates meiotic recombination in a dosage-dependent manner.

SUBMITTER: Guo R 

PROVIDER: S-EPMC7708077 | biostudies-literature | 2020 Nov

REPOSITORIES: biostudies-literature

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The ssDNA-binding protein MEIOB acts as a dosage-sensitive regulator of meiotic recombination.

Guo Rui R   Xu Yang Y   Leu N Adrian NA   Zhang Lei L   Fuchs Serge Y SY   Ye Lan L   Wang P Jeremy PJ  

Nucleic acids research 20201201 21


Meiotic recombination enables reciprocal exchange of genetic information between parental chromosomes and is essential for fertility. MEIOB, a meiosis-specific ssDNA-binding protein, regulates early meiotic recombination. Here we report that the human infertility-associated missense mutation (N64I) in MEIOB causes protein degradation and reduced crossover formation in mouse testes. Although the MEIOB N64I substitution is associated with human infertility, the point mutant mice are fertile despit  ...[more]

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