Literature DB >> 27729423

Maternal MEMI Promotes Female Meiosis II in Response to Fertilization in Caenorhabditis elegans.

Maryam Ataeian1, Justus Tegha-Dunghu1, Donna G Curtis1, Ellen M E Sykes1, Ashkan Nozohourmehrabad1, Megha Bajaj1, Karen Cheung1, Martin Srayko2.   

Abstract

In most animals, female meiosis completes only after fertilization. Sperm entry has been implicated in providing a signal for the initiation of the final meiotic processes; however, a maternal component required for this process has not been previously identified. We report the characterization of a novel family of three highly similar paralogs (memi-1, memi-2, memi-3) that encode oocyte-specific proteins. A hyper-morphic mutation memi-1(sb41) results in failure to exit female meiosis II properly; however, loss of all three paralogs results in a "skipped meiosis II" phenotype. Mutations that prevent fertilization, such as fer-1(hc1), also cause a skipped meiosis II phenotype, suggesting that the MEMI proteins represent a maternal component of a postfertilization signal that specifies the meiosis II program. MEMI proteins are degraded before mitosis and sensitive to ZYG-11, a substrate-specific adapter for cullin-based ubiquitin ligase activity, and the memi-1(sb41) mutation results in inappropriate persistence of the MEMI-1 protein into mitosis. Using an RNAi screen for suppressors of memi-1(sb41), we identified a sperm-specific PP1 phosphatase, GSP-3/4, as a putative sperm component of the MEMI pathway. We also found that MEMI and GSP-3/4 proteins can physically interact via co-immunoprecipitation. These results suggest that sperm-specific PP1 and maternal MEMI proteins act in the same pathway after fertilization to facilitate proper meiosis II and the transition into embryonic mitosis.
Copyright © 2016 by the Genetics Society of America.

Entities:  

Keywords:  Caenorhabditis elegans; PP1 phosphatase; female meiosis; fertilization; mitosis

Mesh:

Substances:

Year:  2016        PMID: 27729423      PMCID: PMC5161279          DOI: 10.1534/genetics.116.192997

Source DB:  PubMed          Journal:  Genetics        ISSN: 0016-6731            Impact factor:   4.562


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