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Publication : Loss of MAX results in meiotic entry in mouse embryonic and germline stem cells.

First Author  Suzuki A Year  2016
Journal  Nat Commun Volume  7
Pages  11056 PubMed ID  27025988
Mgi Jnum  J:236826 Mgi Id  MGI:5807326
Doi  10.1038/ncomms11056 Citation  Suzuki A, et al. (2016) Loss of MAX results in meiotic entry in mouse embryonic and germline stem cells. Nat Commun 7:11056
abstractText  Meiosis is a unique process that allows the generation of reproductive cells. It remains largely unknown how meiosis is initiated in germ cells and why non-germline cells do not undergo meiosis. We previously demonstrated that knockdown of Max expression, a gene encoding a partner of MYC family proteins, strongly activates expression of germ cell-related genes in ESCs. Here we find that complete ablation of Max expression in ESCs results in profound cytological changes reminiscent of cells undergoing meiotic cell division. Furthermore, our analyses uncovers that Max expression is transiently attenuated in germ cells undergoing meiosis in vivo and its forced reduction induces meiosis-like cytological changes in cultured germline stem cells. Mechanistically, Max depletion alterations are, in part, due to impairment of the function of an atypical PRC1 complex (PRC1.6), in which MAX is one of the components. Our data highlight MAX as a new regulator of meiotic onset.
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