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人铜转运蛋白 1(hCTR1)介导的铜与顺铂转运的比较。

Comparison between copper and cisplatin transport mediated by human copper transporter 1 (hCTR1).

机构信息

Department of Chemistry, The University of Hong Kong, Hong Kong, China.

出版信息

Metallomics. 2012 Jul;4(7):679-85. doi: 10.1039/c2mt20021j. Epub 2012 May 3.

Abstract

Copper transporter 1 (CTR1) is a transmembrane protein that imports copper(i) into yeast and mammalian cells. Surprisingly, the protein also mediates the uptake of platinum anticancer drugs, e.g. cisplatin and carboplatin. To study the effects of several metal-binding residues/motifs of hCTR1 on the transport of both Cu(+) and cisplatin, we have constructed Hela cells that stably express a series of hCTR1 variant proteins including H22-24A, NHA, C189S, hCTR1ΔC, H139R and Y156A, and compared their abilities to regulate the accumulation and cytotoxicity of these metal compounds. Our results demonstrated that the cells expressing the hCTR1 mutants of histidine-rich motifs in the N-terminus (H22-24A, NHA) resulted in a higher basal copper level in the steady state compared to those expressing wild-type protein. However, the cellular accumulation of both copper and cisplatin in these variants was found at a similar level to that of wild type when incubated with an excess of metal compounds (100 μM). The cells expressing hCTR1 variants of H139R and Y156A exhibit lower capacities towards accumulation of copper but not cisplatin. Significantly, cells with the C189S variant partially retained the ability of the wild-type hCTR1 protein to accumulate both copper and cisplatin, while for cells expressing the C-terminus truncated variant of hCTR1 (hCTR1ΔC) this ability was absolutely abolished, suggesting that this motif is crucial for the function of the transporter.

摘要

铜转运蛋白 1(CTR1)是一种跨膜蛋白,可将铜(i)导入酵母和哺乳动物细胞。令人惊讶的是,该蛋白还介导铂类抗癌药物(如顺铂和卡铂)的摄取。为了研究 hCTR1 的几个金属结合残基/基序对 Cu(+)和顺铂转运的影响,我们构建了稳定表达一系列 hCTR1 变体蛋白的 Hela 细胞,包括 H22-24A、NHA、C189S、hCTR1ΔC、H139R 和 Y156A,并比较了它们调节这些金属化合物积累和细胞毒性的能力。我们的结果表明,与表达野生型蛋白的细胞相比,表达 N 端富含组氨酸基序(H22-24A、NHA)的 hCTR1 突变体的细胞在稳态下具有更高的基础铜水平。然而,当用过量的金属化合物(100 μM)孵育时,这些变体中铜和顺铂的细胞积累水平与野生型相似。表达 H139R 和 Y156A 的 hCTR1 变体的细胞对铜的积累能力较低,但对顺铂的积累能力没有影响。重要的是,C189S 变体的细胞部分保留了野生型 hCTR1 蛋白积累铜和顺铂的能力,而表达 hCTR1 C 端截断变体(hCTR1ΔC)的细胞则完全丧失了这种能力,表明该基序对转运蛋白的功能至关重要。

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