Literature DB >> 35758641

Phosphoregulation of DSB-1 mediates control of meiotic double-strand break activity.

Heyun Guo1, Ericca L Stamper2,3,4,5, Aya Sato-Carlton1, Masa A Shimazoe1,6, Xuan Li1, Liangyu Zhang2,3,4,5, Lewis Stevens7, K C Jacky Tam1, Abby F Dernburg2,3,4,5, Peter M Carlton1,8,9.   

Abstract

In the first meiotic cell division, proper segregation of chromosomes in most organisms depends on chiasmata, exchanges of continuity between homologous chromosomes that originate from the repair of programmed double-strand breaks (DSBs) catalyzed by the Spo11 endonuclease. Since DSBs can lead to irreparable damage in germ cells, while chromosomes lacking DSBs also lack chiasmata, the number of DSBs must be carefully regulated to be neither too high nor too low. Here, we show that in Caenorhabditis elegans, meiotic DSB levels are controlled by the phosphoregulation of DSB-1, a homolog of the yeast Spo11 cofactor Rec114, by the opposing activities of PP4PPH-4.1 phosphatase and ATRATL-1 kinase. Increased DSB-1 phosphorylation in pph-4.1 mutants correlates with reduction in DSB formation, while prevention of DSB-1 phosphorylation drastically increases the number of meiotic DSBs both in pph-4.1 mutants and in the wild-type background. C. elegans and its close relatives also possess a diverged paralog of DSB-1, called DSB-2, and loss of dsb-2 is known to reduce DSB formation in oocytes with increasing age. We show that the proportion of the phosphorylated, and thus inactivated, form of DSB-1 increases with age and upon loss of DSB-2, while non-phosphorylatable DSB-1 rescues the age-dependent decrease in DSBs in dsb-2 mutants. These results suggest that DSB-2 evolved in part to compensate for the inactivation of DSB-1 through phosphorylation, to maintain levels of DSBs in older animals. Our work shows that PP4PPH-4.1, ATRATL-1, and DSB-2 act in concert with DSB-1 to promote optimal DSB levels throughout the reproductive lifespan.
© 2022, Guo et al.

Entities:  

Keywords:  ATR; C. elegans; PP4; cell biology; double-strand breaks; genetics; genomics; meiosis; phosphoregulation

Mesh:

Substances:

Year:  2022        PMID: 35758641      PMCID: PMC9278955          DOI: 10.7554/eLife.77956

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.713


  94 in total

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Journal:  Nature       Date:  2003-01-16       Impact factor: 49.962

6.  HTP-3 links DSB formation with homolog pairing and crossing over during C. elegans meiosis.

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7.  Polo-like kinase-dependent phosphorylation of the synaptonemal complex protein SYP-4 regulates double-strand break formation through a negative feedback loop.

Authors:  Saravanapriah Nadarajan; Talley J Lambert; Elisabeth Altendorfer; Jinmin Gao; Michael D Blower; Jennifer C Waters; Monica P Colaiácovo
Journal:  Elife       Date:  2017-03-27       Impact factor: 8.140

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Journal:  Nucleic Acids Res       Date:  2012-11-29       Impact factor: 16.971

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