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Literature DB >> 33406239

A pathway for error-free non-homologous end joining of resected meiotic double-strand breaks.

Talia Hatkevich¹, Danny E Miller², Carolyn A Turcotte¹, Margaret C Miller³, Jeff Sekelsky^1,3,4.

Abstract

Programmed DNA double-strand breaks (DSBs) made during meiosis are repaired by recombination with the homologous chromosome to generate, at selected sites, reciprocal crossovers that are critical for the proper separation of homologs in the first meiotic division. Backup repair processes can compensate when the normal meiotic recombination processes are non-functional. We describe a novel backup repair mechanism that occurs when the homologous chromosome is not available in Drosophila melanogaster meiosis. In the presence of a previously described mutation (Mcm5A7) that disrupts chromosome pairing, DSB repair is initiated by homologous recombination but is completed by non-homologous end joining (NHEJ). Remarkably, this process yields precise repair products. Our results provide support for a recombination intermediate recently proposed in mouse meiosis, in which an oligonucleotide bound to the Spo11 protein that catalyzes DSB formation remains bound after resection. We propose that this oligonucleotide functions as a primer for fill-in synthesis to allow scarless repair by NHEJ. We argue that this is a conserved repair mechanism that is likely to be invoked to overcome occasional challenges in normal meiosis.

Entities: Chemical Disease Gene Species

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Year: 2021 PMID： 33406239 PMCID： PMC7826270 DOI： 10.1093/nar/gkaa1205

Source DB: PubMed Journal: Nucleic Acids Res ISSN： 0305-1048 Impact factor: 16.971

67 in total

1. The TopoVIB-Like protein family is required for meiotic DNA double-strand break formation.

Authors: T Robert; A Nore; C Brun; C Maffre; B Crimi; H-M Bourbon; B de Massy
Journal: Science Date: 2016-02-26 Impact factor: 47.728

Review 2. Meiotic versus mitotic recombination: two different routes for double-strand break repair: the different functions of meiotic versus mitotic DSB repair are reflected in different pathway usage and different outcomes.

Authors: Sabrina L Andersen; Jeff Sekelsky
Journal: Bioessays Date: 2010-10-21 Impact factor: 4.345

3. Relationship of DNA double-strand breaks to synapsis in Drosophila.

Authors: Janet K Jang; Dalia E Sherizen; Rajal Bhagat; Elizabeth A Manheim; Kim S McKim
Journal: J Cell Sci Date: 2003-06-10 Impact factor: 5.285

4. Partner choice during meiosis is regulated by Hop1-promoted dimerization of Mek1.

Authors: Hengyao Niu; Lihong Wan; Bridget Baumgartner; Dana Schaefer; Josef Loidl; Nancy M Hollingsworth
Journal: Mol Biol Cell Date: 2005-10-12 Impact factor: 4.138

5. A genetic analysis of the Drosophila mcm5 gene defines a domain specifically required for meiotic recombination.

Authors: Cathleen M Lake; Kathy Teeter; Scott L Page; Rachel Nielsen; R Scott Hawley
Journal: Genetics Date: 2007-06-11 Impact factor: 4.562

6. The Spartan ortholog maternal haploid is required for paternal chromosome integrity in the Drosophila zygote.

Authors: Laetitia Delabaere; Guillermo A Orsi; Laure Sapey-Triomphe; Béatrice Horard; Pierre Couble; Benjamin Loppin
Journal: Curr Biol Date: 2014-09-18 Impact factor: 10.834

7. A Whole-Chromosome Analysis of Meiotic Recombination in Drosophila melanogaster.

Authors: Danny E Miller; Satomi Takeo; Kavyasree Nandanan; Ariel Paulson; Madelaine M Gogol; Aaron C Noll; Anoja G Perera; Kendra N Walton; William D Gilliland; Hua Li; Karen K Staehling; Justin P Blumenstiel; R Scott Hawley
Journal: G3 (Bethesda) Date: 2012-02-01 Impact factor: 3.154

A pathway for error-free non-homologous end joining of resected meiotic double-strand breaks.

1. The TopoVIB-Like protein family is required for meiotic DNA double-strand break formation.

Review 2. Meiotic versus mitotic recombination: two different routes for double-strand break repair: the different functions of meiotic versus mitotic DSB repair are reflected in different pathway usage and different outcomes.

3. Relationship of DNA double-strand breaks to synapsis in Drosophila.

4. Partner choice during meiosis is regulated by Hop1-promoted dimerization of Mek1.

5. A genetic analysis of the Drosophila mcm5 gene defines a domain specifically required for meiotic recombination.

6. The Spartan ortholog maternal haploid is required for paternal chromosome integrity in the Drosophila zygote.

7. A Whole-Chromosome Analysis of Meiotic Recombination in Drosophila melanogaster.

8. REC, Drosophila MCM8, drives formation of meiotic crossovers.

9. Haploid meiosis in Arabidopsis: double-strand breaks are formed and repaired but without synapsis and crossovers.

10. SPRTN is a mammalian DNA-binding metalloprotease that resolves DNA-protein crosslinks.

1. De novo deletions and duplications at recombination hotspots in mouse germlines.

2. The proteome of developing barley anthers during meiotic prophase I.