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The androgen receptor CAG repeat length polymorphism associates with prostate volume in Finnish men with benign prostatic hyperplasia

机译:芬兰男性前列腺增生症中雄激素受体CAG重复长度多态性与前列腺体积相关

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The development of benign prostatic hyperplasia requires the presence of testicular androgens during prostate development, puberty, and ageing. We thus examined the association of three polymorphisms, namely, CYP3A5 6986A>G, CYP19A1 1531C>T, and androgen receptor (AR) gene CAG repeat length, which have previously been linked to the androgen pathway and with clinical characteristics of benign prostatic hyperplasia. Tissue samples from 262 consecutive prostate operations were used for genotyping. Prostate volumes and prostate-specific antigen values were collected from patient records. Linear regression analysis was performed to study the polymorphisms in an age-adjusted model. We did not find any association between the CYP3A5 6986A>G polymorphism and clinical characteristics of benign prostatic hyperplasia. Further, the previously published CYP19A1 1531C>T polymorphism association with an enlarged prostate could not be confirmed with this material. However, we detected an association between short AR gene CAG repeat length and a small prostate volume, which confirms a previous finding in the Finnish population. The data presented suggest a negligible role for the CYP3A5 6986A>G polymorphism in benign prostate enlargement in the Finnish population. However, the results presented do provide further evidence for potentially different genetic mechanisms behind benign prostatic hyperplasia in Finnish and other Caucasian populations. This is based on the conflicting results for AR gene CAG repeat length associations with benign prostatic hyperplasia found in published works.
机译:良性前列腺增生的发展需要在前列腺发育,青春期和衰老期间存在睾丸雄激素。因此,我们检查了三种多态性的关联,即CYP3A5 6986A> G,CYP19A1 1531C> T和雄激素受体(AR)基因CAG重复长度,这些以前已与雄激素途径相关并与良性前列腺增生的临床特征有关。来自262个连续的前列腺手术的组织样品被用于基因分型。从患者记录中收集前列腺体积和前列腺特异性抗原值。进行线性回归分析以研究年龄校正模型中的多态性。我们未发现CYP3A5 6986A> G多态性与良性前列腺增生的临床特征之间存在任何关联。此外,该材料无法确认先前发表的CYP19A1 1531C> T多态性与前列腺肥大的关联。但是,我们检测到较短的AR基因CAG重复长度与较小的前列腺体积之间存在关联,这证实了芬兰人群中的先前发现。提出的数据表明CYP3A5 6986A> G多态性在芬兰人群良性前列腺肿大中的作用微不足道。但是,所提供的结果确实为芬兰人和其他白种人人口中前列腺增生症背后的潜在遗传机制提供了进一步的证据。这是基于在已发表的著作中发现的AR基因CAG重复长度与良性前列腺增生的矛盾结果。

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