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通过解析其蛋白加合物的晶体结构揭示溶液中砷铂-1 聚集的第一步。

The first step of arsenoplatin-1 aggregation in solution unveiled by solving the crystal structure of its protein adduct.

机构信息

Department of Chemistry, University of Florence, Via della Lastruccia 3, 50019 Sesto Fiorentino, FI, Italy.

出版信息

Dalton Trans. 2021 Jan 7;50(1):68-71. doi: 10.1039/d0dt04068a. Epub 2020 Dec 15.

Abstract

Arsenoplatin-1 (AP-1) is an innovative dual-action anticancer agent that contains a platinum(ii) center coordinated to an arsenous acid moiety. We found that AP-1 spontaneously aggregates in aqueous solutions generating oligomeric species of increasing length. Afterward, we succeeded in solving the crystal structure of the adduct formed between the model protein lysozyme and an early AP-1 oligomer that turned out to be a trimer. Remarkably, this crystal structure traps an early stage of AP-1 aggregation offering detailed insight into the molecular process of the oligomer's growth.

摘要

砷铂-1(AP-1)是一种创新的双作用抗癌药物,其中包含一个与砷酸部分配位的铂(ii)中心。我们发现 AP-1 在水溶液中自发聚集,生成长度不断增加的寡聚物。此后,我们成功解决了模型蛋白溶菌酶与早期 AP-1 寡聚物形成的加合物的晶体结构,结果证明它是一个三聚体。值得注意的是,该晶体结构捕获了 AP-1 聚集的早期阶段,为寡聚物生长的分子过程提供了详细的见解。

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