1. Repositório Aberto da Universidade do Porto
  2. I3S - Instituto de Investigação e Inovação em Saúde
  3. I3S - Artigo em Revista Científica Internacional
Please use this identifier to cite or link to this item: https://hdl.handle.net/10216/127072
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dc.creatorMarteil, G-
dc.creatorGuerrero, A-
dc.creatorVieira, AF-
dc.creatorAlmeida, B-
dc.creatorMachado, P-
dc.creatorMendonça, S-
dc.creatorMesquita, M-
dc.creatorVillarreal, B-
dc.creatorFonseca, I-
dc.creatorFrancia, M-
dc.creatorDores, K-
dc.creatorMartins, N-
dc.creatorJana, S-
dc.creatorTranfield, E-
dc.creatorBarbosa-Morais, N-
dc.creatorParedes, J-
dc.creatorPellman, D-
dc.creatorGodinho, S-
dc.creatorBettencourt-Dias, M-
dc.date.accessioned2020-05-13T10:50:46Z-
dc.date.available2020-05-13T10:50:46Z-
dc.date.issued2018-
dc.identifier.issn2041-1723-
dc.identifier.urihttps://hdl.handle.net/10216/127072-
dc.description.abstractCentrosomes are the major microtubule organising centres of animal cells. Deregulation in their number occurs in cancer and was shown to trigger tumorigenesis in mice. However, the incidence, consequence and origins of this abnormality are poorly understood. Here, we screened the NCI-60 panel of human cancer cell lines to systematically analyse centriole number and structure. Our screen shows that centriole amplification is widespread in cancer cell lines and highly prevalent in aggressive breast carcinomas. Moreover, we identify another recurrent feature of cancer cells: centriole size deregulation. Further experiments demonstrate that severe centriole over-elongation can promote amplification through both centriole fragmentation and ectopic procentriole formation. Furthermore, we show that overly long centrioles form over-active centrosomes that nucleate more microtubules, a known cause of invasiveness, and perturb chromosome segregation. Our screen establishes centriole amplification and size deregulation as recurrent features of cancer cells and identifies novel causes and consequences of those abnormalities.-
dc.description.sponsorshipWe thank the Cancer and Centrosome Consortium of the Harvard Medical School Portugal Program, the Harvard Medical School Portugal Program members and directors, and all members of M.B-D. lab for fruitful discussions. We are thankful to Jadranka Loncarek and Joana Vaz for help with experiments and critical reading of the manuscript. We are also grateful to Rita Fior, Sérgio Dias and Filipe Leal for critical reading of the manuscript. We are deeply grateful to all the people that provided us with the cell lines. G.M. and A.G. were funded by the FCT-Harvard Medical School Program Portugal grant (HMSP-CT/SAU-ICT/0075/2009) and individual FCT post-doctoral fellowships (SFRH/BPD/98439/2013 and SFRH/BPD/82420/2011, respectively). The M.BD. laboratory is supported by IGC, an EMBO installation grant, ERC grant ERC-2010- StG-261344, FCT grants (FCT Investigator to M.B-D., POCI-01-0145-FEDER-016390 and PTDC/BIM-ONC/6858/2014) and a FCT-Harvard Medical School Program Portugal grant (HMSP-CT/SAU-ICT/0075/2009).-
dc.language.isoeng-
dc.publisherNature-
dc.relationinfo:eu-repo/grantAgreement/FCT/3599-PPCDT/110408/PT-
dc.relationinfo:eu-repo/grantAgreement/FCT/SFRH/SFRH%2FBPD%2F82420%2F2011/PT-
dc.relationinfo:eu-repo/grantAgreement/FCT/SFRH/SFRH%2FBPD%2F98439%2F2013/PT-
dc.relation.ispartofNature Communications, vol.9(1):1258-
dc.rightsopenAccess-
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/-
dc.subject.meshAutomation-
dc.subject.meshBreast Neoplasms / metabolismo-
dc.subject.meshCell Cycle / physiology-
dc.subject.meshCell Cycle Proteins / metabolismo-
dc.subject.meshCell Line, Tumor-
dc.subject.meshCentrioles / metabolismo-
dc.subject.meshCentrosome / metabolismo-
dc.subject.meshChromosomes / ultrastructure-
dc.subject.meshHumans-
dc.subject.meshMicroscopy, Electron, Transmission-
dc.subject.meshMicrotubule-Associated Proteins / metabolismo-
dc.subject.meshMicrotubules / metabolismo-
dc.subject.meshMitosis-
dc.subject.meshNeoplasms / genetics-
dc.subject.meshNeoplasms / metabolismo-
dc.subject.meshPloidies-
dc.subject.meshTumor Suppressor Protein p53 / metabolism-
dc.titleOver-elongation of centrioles in cancer promotes centriole amplification and chromosome missegregation-
dc.typeArtigo em Revista Científica Internacional-
dc.contributor.uportoInstituto de Investigação e Inovação em Saúde-
dc.identifier.doi10.1038/s41467-018-03641-x-
dc.relation.publisherversionhttps://www.nature.com/articles/s41467-018-03641-x-
Appears in Collections:I3S - Artigo em Revista Científica Internacional

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