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Mouse HORMAD1 and HORMAD2, two conserved meiotic chromosomal proteins, are depleted from synapsed chromosome axes with the help of TRIP13 AAA-ATPase

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dc.contributor.authorWojtasz, Lukasz
dc.contributor.authorDaniel, Katrin
dc.contributor.authorRoig, Ignasi
dc.contributor.authorBolcun-Filas, Ewelina
dc.contributor.authorXu, Huiling
dc.contributor.authorBoonsanay, Verawan
dc.contributor.authorEckmann, Christian R.
dc.contributor.authorCooke, Howard J.
dc.contributor.authorJasin, Maria
dc.contributor.authorKeeney, Scott
dc.contributor.authorMcKay, Michael J.
dc.contributor.authorToth, Attila
dc.date.accessioned2015-10-26T00:02:56Z
dc.date.available2015-10-26T00:02:56Z
dc.date.issued2009-10-23
dc.date.updated2015-12-08T10:47:20Z
dc.description.abstractMeiotic crossovers are produced when programmed double-strand breaks (DSBs) are repaired by recombination from homologous chromosomes (homologues). In a wide variety of organisms, meiotic HORMA-domain proteins are required to direct DSB repair towards homologues. This inter-homologue bias is required for efficient homology search, homologue alignment, and crossover formation. HORMA-domain proteins are also implicated in other processes related to crossover formation, including DSB formation, inhibition of promiscuous formation of the synaptonemal complex (SC), and the meiotic prophase checkpoint that monitors both DSB processing and SCs. We examined the behavior of two previously uncharacterized meiosis-specific mouse HORMA-domain proteins--HORMAD1 and HORMAD2--in wild-type mice and in mutants defective in DSB processing or SC formation. HORMADs are preferentially associated with unsynapsed chromosome axes throughout meiotic prophase. We observe a strong negative correlation between SC formation and presence of HORMADs on axes, and a positive correlation between the presumptive sites of high checkpoint-kinase ATR activity and hyper-accumulation of HORMADs on axes. HORMADs are not depleted from chromosomes in mutants that lack SCs. In contrast, DSB formation and DSB repair are not absolutely required for depletion of HORMADs from synapsed axes. A simple interpretation of these findings is that SC formation directly or indirectly promotes depletion of HORMADs from chromosome axes. We also find that TRIP13 protein is required for reciprocal distribution of HORMADs and the SYCP1/SC-component along chromosome axes. Similarities in mouse and budding yeast meiosis suggest that TRIP13/Pch2 proteins have a conserved role in establishing mutually exclusive HORMAD-rich and synapsed chromatin domains in both mouse and yeast. Taken together, our observations raise the possibility that involvement of meiotic HORMA-domain proteins in the regulation of homologue interactions is conserved in mammals.
dc.description.sponsorshipMeDDrive38 from the Medical Faculty of TU Dresden, Deutsche Forschungsgemeinschaft (grants: TO421/4-1 SPP1384 and TO421/3-1) and the Saechsisches Staatsministerium fuer Wissenschaft und Kunst supported LW, KD, VB, and AT; Grant HD40916 from the US National Institutes of Health supported IR, MJ, and SK; National Health and Medical Research Council of Australia (Project Grant no. 400310) supported MJM and HX; the Medical Research Council UK supported HJC and EBF; and the Max-Planck society supported CRE.en_AU
dc.format28 pages
dc.identifier.issn1553-7404en_AU
dc.identifier.urihttp://hdl.handle.net/1885/16074
dc.publisherPublic Library of Science
dc.relationhttp://purl.org/au-research/grants/nhmrc/400310
dc.rights© 2009 Wojtasz et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited
dc.sourcePLoS Genetics
dc.subjectadenosine triphosphatases
dc.subjectanimals
dc.subjectcell cycle proteins
dc.subjectchromosome pairing
dc.subjectdna breaks, double-stranded
dc.subjectfemale
dc.subjectmale
dc.subjectmice
dc.subjectmice, inbred c57bl
dc.subjectsynaptonemal complex
dc.subjectmeiosis
dc.titleMouse HORMAD1 and HORMAD2, two conserved meiotic chromosomal proteins, are depleted from synapsed chromosome axes with the help of TRIP13 AAA-ATPase
dc.typeJournal article
dcterms.dateAccepted2009-09-25
local.bibliographicCitation.issue10en_AU
local.bibliographicCitation.lastpage28
local.bibliographicCitation.startpagee1000702en_AU
local.contributor.affiliationWojtasz, Lukasz, Technical University of Dresden, Germanyen_AU
local.contributor.affiliationDaniel, Katrin, Technical University of Dresden, Germanyen_AU
local.contributor.affiliationRoig, Ignasi, Memorial Sloan-Kettering Cancer Center, United States of Americaen_AU
local.contributor.affiliationBolcun-Filas, Ewelina, Cornell University, United States of Americaen_AU
local.contributor.affiliationXu, Huiling, Peter MacCallum Cancer Centre, Australiaen_AU
local.contributor.affiliationBoonsanay, Verawan, Technical University of Dresden, Germanyen_AU
local.contributor.affiliationEckmann, Christian, Max Planck Institute, Germanyen_AU
local.contributor.affiliationCooke, Howard, Western General Hospital, Edinburgh, United Kingdomen_AU
local.contributor.affiliationJasin, Maria, Memorial Sloan-Kettering Cancer Center, United States of Americaen_AU
local.contributor.affiliationKeeney, Scott, Howard Hughes Medical Institute, United States of Americaen_AU
local.contributor.affiliationMcKay, Michael, College of Medicine, Biology and Environment, CMBE ANU Medical School, ANU Medical School, The Australian National Universityen_AU
local.contributor.affiliationToth, Attila, Technical University of Dresden, Germanyen_AU
local.contributor.authoruida276689en_AU
local.description.notesImported from ARIESen_AU
local.identifier.absfor111201en_AU
local.identifier.ariespublicationu4201517xPUB150en_AU
local.identifier.citationvolume5en_AU
local.identifier.doi10.1371/journal.pgen.1000702en_AU
local.identifier.essn1553-7404en_AU
local.identifier.scopusID2-s2.0-73449091167
local.publisher.urlhttps://www.plos.org/en_AU
local.type.statusPublished Versionen_AU

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