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dc.contributor.authorSpurdle ABen
dc.contributor.authorGiles GGen
dc.contributor.authorArmes Jen
dc.contributor.authorVenter DJen
dc.contributor.authorHopper JLen
dc.contributor.authorChenevix-Trench Gen
dc.contributor.authorDite GSen
dc.contributor.authorChen Xen
dc.contributor.authorMayne CJen
dc.contributor.authorSouthey MCen
dc.contributor.authorBatten LEen
dc.contributor.authorChy Hen
dc.contributor.authorTrute Len
dc.contributor.authorMcCredie MRen
dc.date.issued1999
dc.date.issued1999
dc.identifier.urihttps://hdl.handle.net/2123/30755
dc.description.abstractBACKGROUND: We conducted a population-based, case-control-family study to determine whether androgen receptor (AR) exon 1 polymorphic CAG repeat length (CAGn) was a risk factor for early-onset breast cancer in the Australian population. METHODS: Case subjects under 40 years of age at diagnosis of a first primary breast cancer and age-matched control subjects were interviewed to assess family history and other risk factors. AR CAGn length was determined for 368 case subjects and 284 control subjects. Distributions in the two groups were compared by linear and logistic regression, allowing adjustment for measured risk factors. All statistical tests were two-tailed. RESULTS: When analyzed as either a continuous or a dichotomous variable, there was no association between CAG, length and breast cancer risk, before or after adjustment for risk factors. Mean (95% confidence interval [CI]) CAGn lengths were 22.0 (21.8-22.2) for case subjects and 22.0 (21.7-22.3) for control subjects (P = .9). The frequency (95% CI) of alleles with 22 or more CAGn repeats was 0.531 (0.494-0.568) for case subjects and 0.507 (0.465-0.549) for control subjects (P = .4). After adjustment, the average effect on log OR (odds ratio) per allele was 0.16 (95% CI = -0.03 to 0.40; P = .2), and the effect of any allele was equivalent to an OR of 1.40 (95% CI = 0.94-2.09; P = .1). Stratification by family history also failed to reveal any association. Similar results were obtained when alleles were defined by other cutoff points. CONCLUSION: We found no evidence for an association between AR exon 1 CAGn length and breast cancer risk in women under the age of 40, despite having 80% power to detect modest effectsen
dc.publisherJournal of the National Cancer Instituteen
dc.rightsOther
dc.subjectAdulten
dc.subjectExonsen
dc.subjectFamilyen
dc.subjectFemaleen
dc.subjectgeneticsen
dc.subjectGenotypeen
dc.subjecthistoryen
dc.subjectHumansen
dc.subjectImmunohistochemistryen
dc.subjectLinear Modelsen
dc.subjectLogistic Modelsen
dc.subjectAge of Onseten
dc.subjectmetabolismen
dc.subjectmethodsen
dc.subjectOdds Ratioen
dc.subjectPolymorphism,Geneticen
dc.subjectReceptors,Androgenen
dc.subjectResearchen
dc.subjectResearch Support,Non-U.S.Gov'ten
dc.subjectRisken
dc.subjectRisk Factorsen
dc.subjectTrinucleotide Repeatsen
dc.subjectAllelesen
dc.subjectWomenen
dc.subjectAustraliaen
dc.subjectbreasten
dc.subjectBreast Neoplasmsen
dc.subjectcanceren
dc.subjectCase-Control Studiesen
dc.subjectdiagnosisen
dc.subject.otherEtiology - Endogenous Factors in the Origin and Cause of Canceren
dc.subject.otherCancer Type - Breast Canceren
dc.titleAndrogen receptor exon 1 CAG repeat length and breast cancer in women before age forty yearsen
dc.typeArticleen
usyd.facultySeS faculties schools::Faculty of Medicine and Healthen


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