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靶向核酸的过渡金属基抗癌药物:串联质谱研究

Transition Metal-based Anticancer Drugs Targeting Nucleic Acids: A Tandem Mass Spectrometric Investigation.

作者信息

Eberle Rahel P, Hari Yvonne, Schürch Stefan

机构信息

Department of Chemistry and Biochemistry, University of Bern, Freiestrasse 3, CH-3012 Bern.

Department of Chemistry and Biochemistry, University of Bern, Freiestrasse 3, CH-3012 Bern;, Email:

出版信息

Chimia (Aarau). 2017 Mar 29;71(3):120-123. doi: 10.2533/chimia.2017.120.

Abstract

The search for effective drugs against cisplatin-resistant tumors resulted in a large number of organometallic compounds that are evaluated for their antiproliferative activity. Among the most promising candidates are bent metallocenes based on various transition metal ions and ligands. The elucidation of structural features and the characterization of the interaction of a drug candidate with its target require accurate and sensitive analytical tools. Tandem mass spectrometry is applied to the investigation of the adduct sites and binding patterns of metallodrugs bound to single-stranded oligonucleotides and higher-order nucleic acids. Results reveal the binding specificities of the different metallodrugs and demonstrate the influence they exert on the dissociation pathways of the adducts in the gas-phase.

摘要

对顺铂耐药肿瘤的有效药物的探索产生了大量用于评估其抗增殖活性的有机金属化合物。最有前景的候选物之一是基于各种过渡金属离子和配体的弯曲茂金属。阐明候选药物的结构特征及其与靶点的相互作用需要准确而灵敏的分析工具。串联质谱法被用于研究与单链寡核苷酸和高阶核酸结合的金属药物的加合位点和结合模式。结果揭示了不同金属药物的结合特异性,并证明了它们对气相中加合物解离途径的影响。

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