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非裔美国前列腺癌患者中的雄激素受体突变与多态性

Androgen receptor mutations and polymorphisms in African American prostate cancer.

作者信息

Koochekpour Shahriar, Buckles Erick, Shourideh Mojgan, Hu SiYi, Chandra Dhyan, Zabaleta Jovanny, Attwood Kristopher

机构信息

1. Department of Cancer Genetics, Center for Pharmacology and Genetics, Elm and Carlton Streets, Roswell Park Cancer Institute, Buffalo, New York. ; 2. Department of Urology, Center for Pharmacology and Genetics, Elm and Carlton streets, Roswell Park Cancer Institute, Buffalo, New York.

3. Department of Biology, Dillard University, New Orleans, Louisiana. ; 4. Stanley S. Scott Cancer Center, Louisiana State University Health Sciences Center, New Orleans, Louisiana.

出版信息

Int J Biol Sci. 2014 Jun 5;10(6):643-51. doi: 10.7150/ijbs.8974. eCollection 2014.

DOI:10.7150/ijbs.8974
PMID:24948877
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4062957/
Abstract

The Androgen receptor (AR) plays a central role in the normal development of the prostate gland, in prostate carcinogenesis, and in the progression of prostate cancer (PCa) to advanced metastatic disease. African American (AA) men with PCa present with higher tumor volume, more advanced tumor stage, and higher Gleason score. This could be in part related to the AR expression or activity in the prostate tissue of AA men, or to unique mutations or polymorphisms of the AR. In Caucasian Americans (CAs), AR mutations are rare or infrequent in organ-confined tumors, but occur at a higher rate in advanced, metastatic, or castrate-recurrent disease. In AAs, the prevalence, clinical, and biological significance of AR mutations in PCa are unknown. In this study, we investigated the occurrence of somatic and germline AR mutations in patients with primary PCa in AAs compared with CAs. Due to very limited data available on allelic distribution of E213 (G/A) single nucleotide polymorphism (SNP), we also assessed this in patients with sporadic PCa and in unrelated healthy individuals from both ethnic populations. Somatic missense AR mutations were detected at a higher rate in AAs (17 out of 200 cases) than in CAs (2 out of 100 cases). In AAs, the majority of these mutations (41.1%) were from Gleason 7 tumors, a small portion (23.5%) from Gleason 8 tumors, and the rest (35.2%) from Gleason 6 tumors. Analysis of genomic DNAs extracted from white blood cells of patients with sporadic PCa revealed that the rate of germline AR mutations were also higher (~4 times) in AAs than in CAs. With respect to E213 (G/A) SNP, the E213 A-allele expression was 5.85 times higher in healthy unrelated AA men than in CA men. However, in AAs with somatic AR mutation, the E213 G-allele distribution was almost equal to the A-allele. Silencing of one of the somatic AR mutations (i.e., 597 Ser>Gly) in a primary AA-PCa cell line (e.g., E006AA) revealed that similar AR mutation can be associated simultaneously with both "gain-of-function" phenotype (cell migration and invasion) and a "loss-of-function" phenotype (proliferation). Our data demonstrated a higher susceptibility for genetic alterations in the AR in the form of somatic mutations in sporadic PCa or in the form of germline mutations in AAs as compared with CAs. These data may support the idea that AR-specific hypermutator phenotype in combination with other genes, might serve as a contributing factor to ethnic differences in PCa and potentially different clinical outcome in AAs as a high-risk population.

摘要

雄激素受体(AR)在前列腺的正常发育、前列腺癌发生以及前列腺癌(PCa)进展为晚期转移性疾病过程中发挥核心作用。患有PCa的非裔美国(AA)男性表现出更高的肿瘤体积、更晚期的肿瘤分期以及更高的Gleason评分。这可能部分与AA男性前列腺组织中的AR表达或活性有关,或者与AR的独特突变或多态性有关。在白种美国(CA)人中,AR突变在器官局限性肿瘤中罕见或不常见,但在晚期、转移性或去势复发疾病中发生率更高。在AA人群中,PCa中AR突变的患病率、临床及生物学意义尚不清楚。在本研究中,我们调查了与CA人群相比,AA原发性PCa患者中体细胞和生殖系AR突变的发生情况。由于关于E213(G/A)单核苷酸多态性(SNP)等位基因分布的可用数据非常有限,我们还在散发性PCa患者以及来自这两个人种群体的无关健康个体中对此进行了评估。在AA人群中检测到体细胞错义AR突变的发生率(200例中有17例)高于CA人群(100例中有2例)。在AA人群中,这些突变的大多数(41.1%)来自Gleason 7级肿瘤,一小部分(23.5%)来自Gleason 8级肿瘤,其余(35.2%)来自Gleason 6级肿瘤。对散发性PCa患者白细胞中提取的基因组DNA分析显示,AA人群中生殖系AR突变率也高于CA人群(约4倍)。关于E213(G/A)SNP,健康无关AA男性中E213 A等位基因表达比CA男性高5.85倍。然而,在有体细胞AR突变的AA人群中,E213 G等位基因分布几乎与A等位基因相等。在原发性AA-PCa细胞系(如E006AA)中沉默其中一种体细胞AR突变(即597 Ser>Gly)显示,类似的AR突变可同时与“功能获得”表型(细胞迁移和侵袭)和“功能丧失”表型(增殖)相关。我们的数据表明,与CA人群相比,散发性PCa中以体细胞突变形式或AA人群中以生殖系突变形式存在的AR基因改变易感性更高。这些数据可能支持这样一种观点,即AR特异性高突变体表型与其他基因相结合,可能是PCa种族差异以及AA作为高危人群可能出现不同临床结局的一个促成因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0853/4062957/ea407537cc9b/ijbsv10p0643g004.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0853/4062957/ea407537cc9b/ijbsv10p0643g004.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0853/4062957/ea407537cc9b/ijbsv10p0643g004.jpg

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