Two susceptibility loci identified for prostate cancer aggressiveness.

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dc.contributor.authorBerndt, S.I.
dc.contributor.authorWang, Z.
dc.contributor.authorYeager, M.
dc.contributor.authorAlavanja, M.C.
dc.contributor.authorAlbanes, D.
dc.contributor.authorAmundadottir, L.
dc.contributor.authorAndriole, G.
dc.contributor.authorBeane Freeman, L.
dc.contributor.authorCampa, D.
dc.contributor.authorCancel-Tassin, G.
dc.contributor.authorCanzian, F.
dc.contributor.authorCornu, J.-N.
dc.contributor.authorCussenot, O.
dc.contributor.authorDiver, W.R.
dc.contributor.authorGapstur, S.M.
dc.contributor.authorGrönberg, H.
dc.contributor.authorHaiman, C.A.
dc.contributor.authorHenderson, B.
dc.contributor.authorHutchinson, A.
dc.contributor.authorHunter, D.J.
dc.contributor.authorKey, T.J.
dc.contributor.authorKolb, S.
dc.contributor.authorKoutros, S.
dc.contributor.authorKraft, P.
dc.contributor.authorLe Marchand, L.
dc.contributor.authorLindström, S.
dc.contributor.authorMachiela, M.J.
dc.contributor.authorOstrander, E.A.
dc.contributor.authorRiboli, E.
dc.contributor.authorSchumacher, F.
dc.contributor.authorSiddiq, A.
dc.contributor.authorStanford, J.L.
dc.contributor.authorStevens, V.L.
dc.contributor.authorTravis, R.C.
dc.contributor.authorTsilidis, K.K.
dc.contributor.authorVirtamo, J.
dc.contributor.authorWeinstein, S.
dc.contributor.authorWilkund, F.
dc.contributor.authorXu, J.
dc.contributor.authorLilly Zheng, S.
dc.contributor.authorYu, K.
dc.contributor.authorWheeler, W.
dc.contributor.authorZhang, H.
dc.contributor.authorSampson, J.
dc.contributor.authorBlack, A.
dc.contributor.authorJacobs, K.
dc.contributor.authorHoover, R.N.
dc.contributor.authorTucker, M.
dc.contributor.authorChanock, S.J.
dc.date.accessioned2018-09-18T15:56:04Z
dc.date.available2018-09-18T15:56:04Z
dc.date.issued2015-05
dc.description.abstractMost men diagnosed with prostate cancer will experience indolent disease; hence, discovering genetic variants that distinguish aggressive from nonaggressive prostate cancer is of critical clinical importance for disease prevention and treatment. In a multistage, case-only genome-wide association study of 12,518 prostate cancer cases, we identify two loci associated with Gleason score, a pathological measure of disease aggressiveness: rs35148638 at 5q14.3 (RASA1, P=6.49 × 10(-9)) and rs78943174 at 3q26.31 (NAALADL2, P=4.18 × 10(-8)). In a stratified case-control analysis, the SNP at 5q14.3 appears specific for aggressive prostate cancer (P=8.85 × 10(-5)) with no association for nonaggressive prostate cancer compared with controls (P=0.57). The proximity of these loci to genes involved in vascular disease suggests potential biological mechanisms worthy of further investigation.en_US
dc.identifier.otherdoi: 10.1038/ncomms7889.
dc.identifier.urihttp://ugspace.ug.edu.gh/handle/123456789/24244
dc.language.isoenen_US
dc.publisherNature Communicationsen_US
dc.subjectlocien_US
dc.subjectprostate canceren_US
dc.subjectindolent diseaseen_US
dc.subjectgeneticen_US
dc.subjecttreatmenten_US
dc.subjectGleason scoreen_US
dc.titleTwo susceptibility loci identified for prostate cancer aggressiveness.en_US
dc.typeArticleen_US

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