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一种短寿命但高细胞毒性的钒(V)配合物,可作为脑癌瘤内注射治疗的潜在药物先导物。

A Short-Lived but Highly Cytotoxic Vanadium(V) Complex as a Potential Drug Lead for Brain Cancer Treatment by Intratumoral Injections.

机构信息

School of Chemistry and Sydney Analytical, University of Sydney, Sydney, NSW, 2006, Australia.

Department of Chemistry and the Cell and Molecular Biology Program, Colorado State University, Fort Collins, CO, 80523, USA.

出版信息

Angew Chem Int Ed Engl. 2020 Sep 7;59(37):15834-15838. doi: 10.1002/anie.202005458. Epub 2020 Aug 11.

Abstract

The chemistry and short lifetimes of metal-based anti-cancer drugs can be turned into an advantage for direct injections into tumors, which then allow the use of highly cytotoxic drugs. The release of their less toxic decomposition products into the blood will lead to decreased toxicity and can even have beneficial effects. We present a ternary V complex, 1 ([VOL L ], where L is N-(salicylideneaminato)-N'-(2-hydroxyethyl)ethane-1,2-diamine and L is 3,5-di-tert-butylcatechol), which enters cells intact to induce high cytotoxicity in a range of human cancer cells, including T98g (glioma multiforme), while its decomposition products in cell culture medium were ≈8-fold less toxic. 1 was 12-fold more toxic than cisplatin in T98g cells and 6-fold more toxic in T98g cells than in a non-cancer human cell line, HFF-1. Its high toxicity in T98g cells was retained in the presence of physiological concentrations of the two main metal-binding serum proteins, albumin and transferrin. These properties favor further development of 1 for brain cancer treatment by intratumoral injections.

摘要

基于金属的抗癌药物的化学性质和短寿命可以转化为直接注射到肿瘤中的优势,这使得能够使用高细胞毒性药物。它们毒性较低的分解产物释放到血液中会导致毒性降低,甚至可能产生有益的效果。我们提出了一种三元 V 配合物 1([VOL L],其中 L 是 N-(水杨醛亚氨基)-N'-(2-羟乙基)乙二胺和 L 是 3,5-二叔丁基儿茶酚),它完整地进入细胞,在包括 T98g(多形性成胶质细胞瘤)在内的多种人类癌细胞中诱导高细胞毒性,而其在细胞培养基中的分解产物的毒性约低 8 倍。1 在 T98g 细胞中的毒性比顺铂高 12 倍,在 T98g 细胞中的毒性比非癌细胞系 HFF-1 高 6 倍。在存在两种主要金属结合血清蛋白白蛋白和转铁蛋白的生理浓度的情况下,其在 T98g 细胞中的高毒性得以保留。这些特性有利于通过肿瘤内注射进一步开发 1 用于脑癌治疗。

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