Identification of a prostate cancer susceptibility locus on chromosome 7q11-21 in Jewish families

被引:17
|
作者
Friedrichsen, DM
Stanford, JL
Isaacs, SD
Janer, M
Chang, BL
Deutsch, K
Gillanders, E
Kolb, S
Wiley, KE
Badzioch, MD
Zheng, SL
Walsh, PC
Jarvik, GP
Hood, L
Trent, JM
Isaacs, WB
Ostrander, EA
Xu, JF
机构
[1] Fred Hutchinson Canc Res Ctr, Div Human Biol, Seattle, WA 98109 USA
[2] Fred Hutchinson Canc Res Ctr, Div Clin Res, Seattle, WA 98109 USA
[3] Univ Washington, Dept Epidemiol, Sch Publ Hlth & Community Med, Seattle, WA 98195 USA
[4] Univ Washington, Dept Med, Div Med Genet, Seattle, WA 98195 USA
[5] Johns Hopkins Med Inst, Dept Urol, Baltimore, MD 21287 USA
[6] Johns Hopkins Med Inst, Brady Urol Inst, Res Labs, Baltimore, MD 21287 USA
[7] Inst Syst Biol, Seattle, WA 98103 USA
[8] Wake Forest Univ, Sch Med, Ctr Human Genom, Winston Salem, NC 27157 USA
[9] NHGRI, Canc Genet Branch, NIH, Bethesda, MD 20892 USA
关键词
D O I
10.1073/pnas.0308336100
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Results from over a dozen prostate cancer susceptibility genome-wide scans, encompassing some 1,500 hereditary prostate cancer families, indicate that prostate cancer is an extremely heterogeneous disease with multiple loci contributing to overall susceptibility. In an attempt to reduce locus heterogeneity, we performed a genomewide linkage scan for prostate cancer susceptibility genes with 36 Jewish families, which represent a stratification of hereditary prostate cancer families with potentially increased locus homogeneity. The 36 Jewish families represent a combined dataset of 17 Jewish families from the Fred Hutchinson Cancer Research Center-based Prostate Cancer Genetic Research Study dataset and 19 Ashkenazi Jewish families collected at Johns Hopkins University. All available family members, including 94 affected men, were genotyped at markers distributed across the genome with an average interval of <10 centimorgans. Nonparametric multipoint linkage analyses were the primary approach, although parametric analyses were performed as well. Our strongest signal was a significant linkage peak at 7q11-21, with a nonparametric linkage (NPL) score of 3.01 (P = 0.0013). Simulations indicated that this corresponds to a genomewide empirical P = 0.006. All other regions had NPL P values greater than or equal to0.02. After genotyping additional markers within the 7q11-21 peak, the NPL score increased to 3.35 (P = 0.0004) at D7S634 with an allele-sharing logarithm of odds of 3.12 (P = 0.00007). These studies highlight the utility of analyzing defined sets of families with a common origin for reducing locus heterogeneity problems associated with studying complex traits.
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收藏
页码:1939 / 1944
页数:6
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