<i>HOXB13</i> G84E Mutation and Prostate Cancer Risk: Kin-Cohort Analysis Using Data From the UK Genetic Prostate Cancer Study

Nyberg, Tommy; Dadaev, Tokhir; Govindasami, Koveela; Lee, Andrew; Leslie, Malgorzata; Kote-Jarai, Zsofia; Eeles, Rosalind; Antoniou, Antonis C

HOXB13 G84E Mutation and Prostate Cancer Risk: Kin-Cohort Analysis Using Data From the UK Genetic Prostate Cancer Study

dc.contributor.author	Nyberg, Tommy
dc.contributor.author	Dadaev, Tokhir
dc.contributor.author	Govindasami, Koveela
dc.contributor.author	Lee, Andrew
dc.contributor.author	Leslie, Malgorzata
dc.contributor.author	Kote-Jarai, Zsofia
dc.contributor.author	Eeles, Rosalind
dc.contributor.author	Antoniou, Antonis C
dc.contributor.orcid	Nyberg, Tommy [0000-0002-9436-0626]
dc.contributor.orcid	Lee, Andrew [0000-0003-0677-0252]
dc.contributor.orcid	Antoniou, Antonis [0000-0001-9223-3116]
dc.date.accessioned	2018-09-05T11:06:15Z
dc.date.available	2018-09-05T11:06:15Z
dc.date.issued	2017
dc.description.abstract	G84E missense mutations in HOXB13 are associated with prostate cancer. However, a wide range of risk estimates has been reported. Based on case-control studies, reported OR range from 2 to 20, often with wide confidence intervals because mutations are rare in the population. To obtain more precise risk estimates, we used a kin-cohort study design and modified segregation analysis, using family data on 11,988 PCa index-cases (4509 consecutive cases, 870 and 6609 cases recruited based on family history and young age at diagnosis, respectively) enrolled in the UK Genetic Prostate Cancer Study, who had been genotyped for G84E. Among index-cases, 182 carried at least one copy of G84E. PCa incidence was assumed to follow a mixed Cox regression model of the form λ(t)=λ_0 (t)"×exp" (G+P), where G is a fixed effect which depends on G84E, P∈N(0,σ_P^2 ) a residual polygenic random effect, and λ_0 (t) is the baseline incidence for non-carriers to age t. Using maximum likelihood, after adjusting for ascertainment, we estimated the frequency and RR (i.e. penetrance) for G84E under different genetic models, and σ_P. Preliminary results suggest that under the best fitting model, the data are consistent with a multiplicative model where each copy of G84E confers RR for PCa of 2.6 (95%CI 1.7-4.2), and a significant σ_P of 1.8 (95%CI 1.7-1.9), indicating that family history increases risk above that resulting from being a mutation carrier. Ongoing work will evaluate effect-modification of RR and/or σ_P by age, birth cohort, and mutation status, and estimate absolute risks for reference family structures.
dc.identifier.doi	10.17863/CAM.26513
dc.identifier.eissn	1098-2272
dc.identifier.issn	0741-0395
dc.identifier.uri	https://www.repository.cam.ac.uk/handle/1810/279133
dc.language.iso	eng
dc.title	<i>HOXB13</i> G84E Mutation and Prostate Cancer Risk: Kin-Cohort Analysis Using Data From the UK Genetic Prostate Cancer Study
dc.type	Conference Object
dcterms.dateAccepted	2017-06-23
prism.endingPage	676
prism.issueIdentifier	7
prism.publicationDate	2017
prism.publicationName	GENETIC EPIDEMIOLOGY
prism.startingPage	676
prism.volume	41
pubs.conference-name	International Genetic Epidemiology Society 2017 meeting
pubs.funder-project-id	Cancer Research UK (20861)
pubs.funder-project-id	Cancer Research Uk (None)
rioxxterms.licenseref.startdate	2017-11
rioxxterms.licenseref.uri	http://www.rioxx.net/licenses/all-rights-reserved
rioxxterms.type	Conference Paper/Proceeding/Abstract
rioxxterms.version	AM
rioxxterms.versionofrecord	10.17863/CAM.26513

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