| Literature DB >> 32845237 |
Natalia Felipe-Medina1, Sandrine Caburet2,3, Fernando Sánchez-Sáez1, Yazmine B Condezo1, Dirk G de Rooij4, Laura Gómez-H1, Rodrigo Garcia-Valiente1, Anne Laure Todeschini2,3, Paloma Duque1, Manuel Adolfo Sánchez-Martin5,6, Stavit A Shalev7,8, Elena Llano1,9, Reiner A Veitia2,3,10, Alberto M Pendás1.
Abstract
Primary Ovarian Insufficiency (POI) is a major cause of infertility, but its etiology remains poorly understood. Using whole-exome sequencing in a family with three cases of POI, we identified the candidate missense variant S167L in HSF2BP, an essential meiotic gene. Functional analysis of the HSF2BP-S167L variant in mouse showed that it behaves as a hypomorphic allele compared to a new loss-of-function (knock-out) mouse model. Hsf2bpS167L/S167L females show reduced fertility with smaller litter sizes. To obtain mechanistic insights, we identified C19ORF57/BRME1 as a strong interactor and stabilizer of HSF2BP and showed that the BRME1/HSF2BP protein complex co-immunoprecipitates with BRCA2, RAD51, RPA and PALB2. Meiocytes bearing the HSF2BP-S167L variant showed a strongly decreased staining of both HSF2BP and BRME1 at the recombination nodules and a reduced number of the foci formed by the recombinases RAD51/DMC1, thus leading to a lower frequency of crossovers. Our results provide insights into the molecular mechanism of HSF2BP-S167L in human ovarian insufficiency and sub(in)fertility.Entities:
Keywords: cell biology; fertility; human genetics; meiosis; meiotic recombination; mouse; reproduction
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Year: 2020 PMID: 32845237 PMCID: PMC7498267 DOI: 10.7554/eLife.56996
Source DB: PubMed Journal: Elife ISSN: 2050-084X Impact factor: 8.140