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Involvement of Human Multidrug and Toxic Compound Extrusion (MATE) Transporters in Testosterone Transport

机译:人类多药和有毒复合挤出(配合)转运蛋白在睾酮运输中的参与

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摘要

Multidrug and toxic compound extrusion (MATE) transporters are primarily expressed in the kidneys and liver, where they contribute to the excretion of organic cations. Our previous study suggested that pig MATE2 (class III) participates in testosterone secretion from Leydig cells. In humans, it is unclear which MATE class is involved in testosterone transport. In this study, we aimed to clarify whether human MATE1 (hMATE1) or human MATE2K (hMATE2K) mediates testosterone transport. To confirm that testosterone inhibits transporter-mediated tetraethylammonium (TEA) uptake, a cis-inhibition assay was performed using cells that stably expressed hMATE1 or hMATE2K. Docking simulations were performed to characterize differences in the binding of hMATE1 and hMATE2K to testosterone. Transport experiments in LLC-PK1 cells that stably expressed hMATE1 were used to test whether hMATE1 mediates testosterone transport. We detected differences between the amino acid sequences of the substrate-binding sites of hMATE1 and hMATE2K that could potentially be involved in testosterone binding. Testosterone and estradiol inhibited TEA uptake mediated by hMATE1 but not that mediated by hMATE2K. Transport experiments in LLC-PK1 cells indicated that testosterone might be transported via hMATE1. This study suggested that hMATE1, but not hMATE2K, is involved in human testosterone transport.
机译:多药和有毒化合物挤出(配合)转运蛋白主要在肾脏和肝脏中表达,在那里它们有助于有机阳离子的排泄。我们以前的研究表明,猪Mate2(III类)参与来自Leydig细胞的睾酮分泌物。在人类中,尚不清楚哪种伴侣类涉及睾酮运输。在这项研究中,我们旨在阐明人类mate1(hmate1)或人类mate2k(hmate2k)介导睾酮运输。为了确认睾酮抑制转运蛋白介导的四乙基铵(茶)摄取,使用稳定表达HMATE1或HMATE2K的细胞进行CIS抑制测定。对解码模拟进行了表征含有HMATE1和HMATE2K与睾酮的结合的差异。稳定表达HMate1的LLC-PK1细胞中的运输实验用于测试HMate1是否介导睾酮运输。我们检测到HMATE1和HMATE2K的底物结合位点的氨基酸序列之间的差异,其可能涉及睾酮结合。睾酮和雌二醇抑制由HMATE1介导的茶吐痰,但不是由HMATE2K介导的。 LLC-PK1细胞中的运输实验表明睾酮可以通过HMate1运输。本研究表明,HMATE1但不是HMATE2K,参与人体睾酮运输。

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