Literature DB >> 29360988

CHEK1 coordinates DNA damage signaling and meiotic progression in the male germline of mice.

Hironori Abe1,2, Kris G Alavattam1,2, Yasuko Kato1,2, Diego H Castrillon3, Qishen Pang2,4, Paul R Andreassen2,4, Satoshi H Namekawa1,2.   

Abstract

The continuity of life depends on mechanisms in the germline that ensure the integrity of the genome. The DNA damage response/checkpoint kinases ATM and ATR are essential signaling factors in the germline. However, it remains unknown how a downstream transducer, Checkpoint Kinase 1 (CHEK1 or CHK1), mediates signaling in the male germline. Here, we show that CHEK1 has distinct functions in both the mitotic and meiotic phases of the male germline in mice. In the mitotic phase, CHEK1 is required for the resumption of prospermatogonia proliferation after birth and the maintenance of spermatogonia. In the meiotic phase, we uncovered two functions for CHEK1: one is the stage-specific attenuation of DNA damage signaling on autosomes, and the other is coordination of meiotic stage progression. On autosomes, the loss of CHEK1 delays the removal of DNA damage signaling that manifests as phosphorylation of histone variant H2AX at serine 139 (γH2AX). Importantly, CHEK1 does not have a direct function in meiotic sex chromosome inactivation (MSCI), an essential event in male meiosis, in which ATR is a key regulator. Thus, the functions of ATR and CHEK1 are uncoupled in MSCI, in contrast to their roles in DNA damage signaling in somatic cells. Our study reveals stage-specific functions for CHEK1 that ensure the integrity of the male germline.

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Year:  2018        PMID: 29360988      PMCID: PMC6185175          DOI: 10.1093/hmg/ddy022

Source DB:  PubMed          Journal:  Hum Mol Genet        ISSN: 0964-6906            Impact factor:   6.150


  57 in total

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Authors:  Ronit I Yarden; Sherly Pardo-Reoyo; Magda Sgagias; Kenneth H Cowan; Lawrence C Brody
Journal:  Nat Genet       Date:  2002-02-11       Impact factor: 38.330

2.  H2AX is required for chromatin remodeling and inactivation of sex chromosomes in male mouse meiosis.

Authors:  Oscar Fernandez-Capetillo; Shantha K Mahadevaiah; Arkady Celeste; Peter J Romanienko; R Daniel Camerini-Otero; William M Bonner; Katia Manova; Paul Burgoyne; André Nussenzweig
Journal:  Dev Cell       Date:  2003-04       Impact factor: 12.270

Review 3.  DNA double strand break repair, chromosome synapsis and transcriptional silencing in meiosis.

Authors:  Akiko Inagaki; Sam Schoenmakers; Willy M Baarends
Journal:  Epigenetics       Date:  2010-05-16       Impact factor: 4.528

Review 4.  Mechanisms of germ line genome instability.

Authors:  Seoyoung Kim; Shaun E Peterson; Maria Jasin; Scott Keeney
Journal:  Semin Cell Dev Biol       Date:  2016-02-12       Impact factor: 7.727

5.  Rapid PIKK-dependent release of Chk1 from chromatin promotes the DNA-damage checkpoint response.

Authors:  Veronique A J Smits; Philip M Reaper; Stephen P Jackson
Journal:  Curr Biol       Date:  2005-12-15       Impact factor: 10.834

Review 6.  Gonocytes, from the fifties to the present: is there a reason to change the name?

Authors:  Martine Culty
Journal:  Biol Reprod       Date:  2013-08-29       Impact factor: 4.285

Review 7.  Control of Meiotic Crossovers: From Double-Strand Break Formation to Designation.

Authors:  Stephen Gray; Paula E Cohen
Journal:  Annu Rev Genet       Date:  2016-09-14       Impact factor: 16.830

8.  MDC1 directs chromosome-wide silencing of the sex chromosomes in male germ cells.

Authors:  Yosuke Ichijima; Misako Ichijima; Zhenkun Lou; André Nussenzweig; R Daniel Camerini-Otero; Junjie Chen; Paul R Andreassen; Satoshi H Namekawa
Journal:  Genes Dev       Date:  2011-05-01       Impact factor: 11.361

9.  Chk1 is haploinsufficient for multiple functions critical to tumor suppression.

Authors:  Michael H Lam; Qinghua Liu; Stephen J Elledge; Jeffrey M Rosen
Journal:  Cancer Cell       Date:  2004-07       Impact factor: 31.743

10.  Stem cell defects in ATM-deficient undifferentiated spermatogonia through DNA damage-induced cell-cycle arrest.

Authors:  Keiyo Takubo; Masako Ohmura; Masaki Azuma; Go Nagamatsu; Wakako Yamada; Fumio Arai; Atsushi Hirao; Toshio Suda
Journal:  Cell Stem Cell       Date:  2008-02-07       Impact factor: 24.633

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1.  Oocyte Elimination Through DNA Damage Signaling from CHK1/CHK2 to p53 and p63.

Authors:  Vera D Rinaldi; Jordana C Bloom; John C Schimenti
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2.  The Initiation of Meiotic Sex Chromosome Inactivation Sequesters DNA Damage Signaling from Autosomes in Mouse Spermatogenesis.

Authors:  Hironori Abe; Kris G Alavattam; Yueh-Chiang Hu; Qishen Pang; Paul R Andreassen; Rashmi S Hegde; Satoshi H Namekawa
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3.  Dual functions for the ssDNA-binding protein RPA in meiotic recombination.

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5.  YTHDC2 is essential for pachytene progression and prevents aberrant microtubule-driven telomere clustering in male meiosis.

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Journal:  Cell Rep       Date:  2021-12-14       Impact factor: 9.423

6.  Hub Genes and Key Pathways of Intervertebral Disc Degeneration: Bioinformatics Analysis and Validation.

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Journal:  Biomed Res Int       Date:  2021-09-10       Impact factor: 3.411

7.  Multiple 9-1-1 complexes promote homolog synapsis, DSB repair, and ATR signaling during mammalian meiosis.

Authors:  Catalina Pereira; Gerardo A Arroyo-Martinez; Matthew Z Guo; Michael S Downey; Emma R Kelly; Kathryn J Grive; Shantha K Mahadevaiah; Jennie R Sims; Vitor M Faca; Charlton Tsai; Carl J Schiltz; Niek Wit; Heinz Jacobs; Nathan L Clark; Raimundo Freire; James Turner; Amy M Lyndaker; Miguel A Brieno-Enriquez; Paula E Cohen; Marcus B Smolka; Robert S Weiss
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8.  Genetic insights into biological mechanisms governing human ovarian ageing.

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9.  SKP1 drives the prophase I to metaphase I transition during male meiosis.

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10.  The DNA damage response is required for oocyte cyst breakdown and follicle formation in mice.

Authors:  Ana Martínez-Marchal; Yan Huang; Maria Teresa Guillot-Ferriols; Mònica Ferrer-Roda; Anna Guixé; Montserrat Garcia-Caldés; Ignasi Roig
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  10 in total

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