Literature DB >> 22718278

A novel germline mutation in HOXB13 is associated with prostate cancer risk in Chinese men.

Xiaoling Lin1, Lianxi Qu, Zhuo Chen, Chuanliang Xu, Dingwei Ye, Qiang Shao, Xiang Wang, Jun Qi, Zhiwen Chen, Fangjian Zhou, Meilin Wang, Zhong Wang, Dalin He, Denglong Wu, Xin Gao, Jianlin Yuan, Gongxian Wang, Yong Xu, Guozeng Wang, Pei Dong, Yang Jiao, Jin Yang, Jun Ou-Yang, Haowen Jiang, Yao Zhu, Shancheng Ren, Zhengdong Zhang, Changjun Yin, Qijun Wu, Ying Zheng, Aubrey R Turner, Sha Tao, Rong Na, Qiang Ding, Daru Lu, Rong Shi, Jielin Sun, Fang Liu, S Lilly Zheng, Zengnan Mo, Yinghao Sun, Jianfeng Xu.   

Abstract

BACKGROUND: A rare mutation G84E in HOXB13 was recently identified to be associated with prostate cancer (PCa) in Caucasians. The goal of this study is to test association between HOXB13 genetic variants and PCa risk in Chinese men.
METHODS: All study subjects were part of the Chinese Consortium for Prostate Cancer Genetics (ChinaPCa). In the first stage, we screened for mutations by sequencing the HOXB13 coding region in 96 unrelated PCa patients. In stage 2, G84E and novel mutations found in stage 1 were genotyped in 671 PCa patients and 1,536 controls. In stage 3, mutation status in 751 additional PCa patients was imputed via haplotype.
RESULTS: The G84E mutation was not detected in this study. However, a novel mutation, G135E, was identified among 96 patients in stage 1. It was also observed twice in 575 additional PCa patients but not in 1,536 control subjects of stage 2. The frequency of G135E was significantly different between cases and controls, with a P-value of 0.027, based on Fisher's exact test. Haplotype estimation showed that G135E mutation carriers shared a unique haplotype that was not observed in other subjects. In stage 3, two more PCa patients were predicted to carry the G135E mutation.
CONCLUSIONS: We identified a novel rare mutation in the HOXB13 gene, G135E, which appears to be a founder mutation. This mutation is associated with increased PCa risk in Chinese men. Consistent with a previous report, our findings provide further evidence that rare mutations in HOXB13 contribute to PCa risk.
Copyright © 2012 Wiley Periodicals, Inc.

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Year:  2012        PMID: 22718278      PMCID: PMC3755486          DOI: 10.1002/pros.22552

Source DB:  PubMed          Journal:  Prostate        ISSN: 0270-4137            Impact factor:   4.104


  27 in total

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Journal:  Nat Genet       Date:  2007-04-01       Impact factor: 38.330

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9.  Predictive performance of prostate cancer risk in Chinese men using 33 reported prostate cancer risk-associated SNPs.

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Review 1.  [Familial prostate cancer and genetic predisposition].

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2.  G84E mutation in HOXB13 is firmly associated with prostate cancer risk: a meta-analysis.

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3.  Familial prostate cancer and HOXB13 founder mutations: geographic and racial/ethnic variations.

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4.  Identification of a novel germline SPOP mutation in a family with hereditary prostate cancer.

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Review 5.  Shaping Chromatin States in Prostate Cancer by Pioneer Transcription Factors.

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6.  The role of germline mutations in the BRCA1/2 and mismatch repair genes in men ascertained for early-onset and/or familial prostate cancer.

Authors:  Sofia Maia; Marta Cardoso; Paula Paulo; Manuela Pinheiro; Pedro Pinto; Catarina Santos; Carla Pinto; Ana Peixoto; Rui Henrique; Manuel R Teixeira
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7.  Prediction of prostate cancer from prostate biopsy in Chinese men using a genetic score derived from 24 prostate cancer risk-associated SNPs.

Authors:  Haowen Jiang; Fang Liu; Zhong Wang; Rong Na; Limin Zhang; Yishuo Wu; Jie Zheng; Xiaoling Lin; Deke Jiang; Jielin Sun; S Lilly Zheng; Qiang Ding; Jianfeng Xu
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8.  HOXB13 mutation and prostate cancer: studies of siblings and aggressive disease.

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9.  HOXB13 mutations in a population-based, case-control study of prostate cancer.

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10.  Prevalence of the HOXB13 G84E prostate cancer risk allele in men treated with radical prostatectomy.

Authors:  Jennifer L Beebe-Dimmer; William B Isaacs; Kimberly A Zuhlke; Cecilia Yee; Patrick C Walsh; Sarah D Isaacs; Anna M Johnson; Charles E Ewing; Elizabeth B Humphreys; Wasim H Chowdhury; James E Montie; Kathleen A Cooney
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