用于STxB-药物偶联疗法中澳瑞他汀的新型递送系统。

A new delivery system for auristatin in STxB-drug conjugate therapy.

作者信息

Batisse Cornélie, Dransart Estelle, Ait Sarkouh Rafik, Brulle Laura, Bai Siau-Kun, Godefroy Sylvie, Johannes Ludger, Schmidt Frédéric

机构信息

Institut Curie, CNRS, UMR 3666/INSERM U1143, 26 rue d'Ulm, 75248 Cedex 05 Paris, France; Immuno Targets SAS, 116 bd du Montparnasse, 75014 Paris, France.

Institut Curie, CNRS, UMR 3666/INSERM U1143, 26 rue d'Ulm, 75248 Cedex 05 Paris, France.

出版信息

Eur J Med Chem. 2015 May 5;95:483-91. doi: 10.1016/j.ejmech.2015.03.047. Epub 2015 Mar 28.

DOI:10.1016/j.ejmech.2015.03.047

PMID:25847766

Abstract

A key challenge in anticancer therapy is to gain control over the biodistribution of cytotoxic drugs. The most promising strategy consists in conjugating drugs to tumor-targeting carriers, thereby combining high cytotoxic activity and specific delivery. To target Gb3-positive cancer cells, we exploit the non-toxic B-subunit of Shiga toxin (STxB). Here, we have conjugated STxB to highly potent auristatin derivatives (MMA). A former linker was optimized to ensure proper drug-release upon reaching reducing environments in target cells, followed by a self-immolation step. Two conjugates were successfully obtained, and in vitro assays demonstrated the potential of this targeting system for the selective elimination of Gb3-positive tumors.

摘要

抗癌治疗中的一个关键挑战是控制细胞毒性药物的生物分布。最有前景的策略是将药物与肿瘤靶向载体结合，从而将高细胞毒性活性与特异性递送相结合。为了靶向Gb3阳性癌细胞，我们利用了志贺毒素（STxB）的无毒B亚基。在此，我们将STxB与高效澳瑞他汀衍生物（MMA）结合。对之前的连接子进行了优化，以确保在到达靶细胞的还原环境后能实现药物的适当释放，随后进行自毁步骤。成功获得了两种缀合物，体外试验证明了该靶向系统对选择性消除Gb3阳性肿瘤的潜力。

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用于STxB-药物偶联疗法中澳瑞他汀的新型递送系统。

A new delivery system for auristatin in STxB-drug conjugate therapy.

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