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一种调节前列腺甾体5α-还原酶活性的常见错义替换。

A prevalent missense substitution that modulates activity of prostatic steroid 5alpha-reductase.

作者信息

Makridakis N, Ross R K, Pike M C, Chang L, Stanczyk F Z, Kolonel L N, Shi C Y, Yu M C, Henderson B E, Reichardt J K

机构信息

Department of Biochemistry and Molecular Biology, University of Southern California School of Medicine, USC/Norris Comprehensive Cancer Center, Los Angeles 90033-1034, USA.

出版信息

Cancer Res. 1997 Mar 15;57(6):1020-2.

PMID:9067262
Abstract

Prostate cancer is the most common serious cancer diagnosed in men in the United States. This disease is also characterized by a striking racial/ethnic variation in incidence: highest in African-Americans, intermediate in Caucasians, slightly lower in Latinos, and lowest in Asians. Ample biochemical and epidemiological evidence suggests a role for androgens, particularly testosterone and dihydrotestosterone, in prostate cancer etiology. We have analyzed a candidate gene for prostate cancer, SRD5A2, encoding prostatic steroid 5alpha-reductase type II, which converts testosterone into the more bioactive dihydrotestosterone, for mutations. We report here one amino acid substitution, V89L, which replaces valine at codon 89 with leucine. This substitution is a "germline" (constitutional) DNA polymorphism, and it is common, panethnic, and reduces in vivo steroid 5alpha-reductase activity. This substitution is particularly common among Asians and may explain the low risk for prostate cancer in this population.

摘要

前列腺癌是美国男性中最常见的严重癌症。这种疾病的发病率在种族/族裔方面也存在显著差异:非裔美国人中最高,白种人居中,拉丁裔略低,亚洲人最低。大量的生化和流行病学证据表明,雄激素,尤其是睾酮和双氢睾酮,在前列腺癌病因学中发挥作用。我们分析了一个前列腺癌候选基因SRD5A2,它编码II型前列腺类固醇5α-还原酶,该酶将睾酮转化为生物活性更强的双氢睾酮,以寻找突变。我们在此报告一个氨基酸替换,V89L,即第89密码子处的缬氨酸被亮氨酸取代。这种替换是一种“种系”(构成性)DNA多态性,它很常见,存在于所有种族中,并且会降低体内类固醇5α-还原酶的活性。这种替换在亚洲人中尤为常见,可能解释了该人群中前列腺癌风险较低的原因。

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