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人前列腺癌细胞中存在一种锌摄取转运体的证据,该转运体受催乳素和睾酮调节。

Evidence for a zinc uptake transporter in human prostate cancer cells which is regulated by prolactin and testosterone.

作者信息

Costello L C, Liu Y, Zou J, Franklin R B

机构信息

Cellular and Molecular Biology Section, Department of Oral and Craniofacial Biological Sciences, University of Maryland Dental School, Baltimore, Maryland 21201, USA.

出版信息

J Biol Chem. 1999 Jun 18;274(25):17499-504. doi: 10.1074/jbc.274.25.17499.

Abstract

The glandular epithelial cells of the human prostate gland have the unique capability and function of accumulating the highest zinc levels of any soft tissue in the body. Zinc accumulation in the prostate is regulated by prolactin and testosterone; however, little information is available concerning the mechanisms associated with zinc accumulation and its regulation in prostate epithelial cells. In the present studies the uptake and accumulation of zinc were determined in the human malignant prostate cell lines LNCaP and PC-3. The results demonstrate that LNCaP cells and PC-3 cells possess the unique capability of accumulating high levels of zinc. Zinc accumulation in both cell types is stimulated by physiological concentrations of prolactin and testosterone. The studies reveal that these cells contain a rapid zinc uptake process indicative of a plasma membrane zinc transporter. Initial kinetic studies demonstrate that the rapid uptake of zinc is effective under physiological conditions that reflect the total and mobile zinc levels in circulation. Correspondingly, genetic studies demonstrate the expression of a ZIP family zinc uptake transporter in both LNCaP and PC-3 cells. The rapid zinc uptake transport process is stimulated by treatment of cells with physiological levels of prolactin and testosterone, which possibly is the result of the regulation of the ZIP-type zinc transporter gene. These zinc-accumulating characteristics are specific for prostate cells. The studies support the concept that these prostate cells express a unique hormone-responsive, plasma membrane-associated, rapid zinc uptake transporter gene associated with their unique ability to accumulate high zinc levels.

摘要

人类前列腺的腺上皮细胞具有独特的能力和功能,能够积累体内任何软组织中最高水平的锌。前列腺中的锌积累受催乳素和睾酮调节;然而,关于前列腺上皮细胞中锌积累及其调节的相关机制,目前所知甚少。在本研究中,测定了人类恶性前列腺细胞系LNCaP和PC-3中锌的摄取和积累情况。结果表明,LNCaP细胞和PC-3细胞具有积累高水平锌的独特能力。两种细胞类型中的锌积累均受到生理浓度的催乳素和睾酮的刺激。研究表明,这些细胞含有一种快速的锌摄取过程,这表明存在一种质膜锌转运体。初步动力学研究表明,在反映循环中总锌和可移动锌水平的生理条件下,锌的快速摄取是有效的。相应地,遗传学研究表明,LNCaP和PC-3细胞中均表达一种ZIP家族锌摄取转运体。用生理水平的催乳素和睾酮处理细胞会刺激快速的锌摄取转运过程,这可能是ZIP型锌转运体基因受到调节的结果。这些锌积累特性是前列腺细胞特有的。这些研究支持了这样一种观点,即这些前列腺细胞表达一种独特的、与激素反应相关的、与质膜相关的、快速锌摄取转运体基因,这与其积累高锌水平的独特能力有关。

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