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首页> 外文期刊>Angewandte Chemie >Organometallic Rhenium Complexes Divert Doxorubicin to the Mitochondria
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Organometallic Rhenium Complexes Divert Doxorubicin to the Mitochondria

机译:有机金属R配合物将阿霉素转移至线粒体

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摘要

Doxorubicin, a well-established chemotherapeutic agent, is known to accumulate in the cell nucleus. By using ICP-MS, we show that the conjugation of two small organometallic rhenium complexes to this structural motif results in a significant redirection of the conjugates from the nucleus to the mitochondria. Despite this relocation, the two bioconjugates display excellent toxicity toward HeLa cells. In addition, we carried out a preliminarily investigation of aspects of cytotoxicity and present evidence that the conjugates disrupt the mitochondrial membrane potential, are strong inhibitors of human Topoisomerase II, and induce apoptosis. Such derivatives may enhance the therapeutic index of the aggressive parent drug and overcome drug resistance by influencing nuclear and mitochondrial homeostasis.
机译:众所周知,阿霉素(一种成熟的化学治疗剂)会在细胞核中蓄积。通过使用ICP-MS,我们显示了两个小的有机金属rh配合物与该结构基序的缀合导致缀合物从核到线粒体的显着重定向。尽管进行了这种重新定位,这两种生物结合物对HeLa细胞仍显示出优异的毒性。此外,我们对细胞毒性方面进行了初步研究,并提供了证据表明缀合物破坏了线粒体膜电位,是人拓扑异构酶II的强抑制剂,并诱导凋亡。这样的衍生物可以通过影响核和线粒体的体内平衡来增强攻击性母体药物的治疗指数并克服耐药性。

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