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铂配合物与人铜转运蛋白 1 C 端基序的相互作用。

Interaction between platinum complexes and the C-terminal motif of human copper transporter 1.

机构信息

CAS Key Laboratory of Soft Matter Chemistry, School of Chemistry and Materials Science, University of Science and Technology of China, Hefei Anhui 230026, China.

出版信息

Inorg Chem. 2013 May 20;52(10):6153-9. doi: 10.1021/ic400495w. Epub 2013 May 3.

Abstract

Human copper transporter 1 (hCTR1) facilitates the cellular uptake of cisplatin, and the extracellular N-terminal domain has been proven to coordinate to platinum drugs. It has been reported that the intracellular C-terminal motif is crucial for the function of hCTR1 in cisplatin influx. In this work, we conduct reactions of the intracellular motif with platinum drugs. The octapeptide from the C-terminal domain of hCTR1 is used, and the reactions are investigated using ultraviolet, high-performance liquid chromatography, electrospray ionization mass spectrometry, and nuclear magnetic resonance spectroscopy. Results show that the C8 peptide is highly reactive to cisplatin and oxaliplatin, and the -HCH sequence is the most favorable binding site of platinum agents. Cisplatin first binds to the cysteine residues in the reaction with the C8 peptide. The ammine ligand, even trans to a thiol ligand, can remain coordinated in platination adducts for a >12 h reaction. Intramolecular platinum migration was observed in the C8 peptide, and the ammine ligands remain coordinated to platinum during this process. This result indicates that hCTR1 can transfer cisplatin in the active form through a trans chelation process. These findings provide insight into the mechanism of the C-terminus of hCTR1 in the transfer of platinum drugs from the trimeric pore of hCTR1 to the cytoplasm.

摘要

人铜转运蛋白 1(hCTR1)促进顺铂的细胞摄取,并且已经证明细胞外 N 端结构域与铂类药物协调。据报道,细胞内 C 端基序对于 hCTR1 在顺铂流入中的功能至关重要。在这项工作中,我们进行了细胞内基序与铂类药物的反应。使用 hCTR1 C 端结构域的八肽,并用紫外、高效液相色谱、电喷雾电离质谱和核磁共振光谱研究反应。结果表明,C8 肽与顺铂和奥沙利铂高度反应,-HCH 序列是铂类药物最有利的结合位点。顺铂首先与 C8 肽反应中的半胱氨酸残基结合。即使在与硫醇配体反式配位的情况下,氨配体在长达 12 小时的反应中仍能保持配位。在 C8 肽中观察到分子内铂迁移,在此过程中,氨配体仍与铂配位。这一结果表明 hCTR1 可以通过反式螯合过程将顺铂以活性形式转移。这些发现为 hCTR1 的 C 末端在将铂类药物从 hCTR1 的三聚体孔转移到细胞质中的机制提供了深入的了解。

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