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Blocking the survival of the nastiest by HSP90 inhibition

机译:通过抑制HSP90阻止最讨厌的动物的生存

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摘要

It is now recognised that genetic, epigenetic and phenotypic heterogeneity within individual human cancers is responsible for therapeutic resistance – knowledge that is having a profound impact on current thinking and experimentation. There has been concern that molecularly targeted therapy is doomed to failure, with resistant clones emerging in response to the Darwinian selective pressure of any drug treatment. However, two studies have shown that the evolution of drug resistance can be restrained by co-administration of a pharmacologic inhibitor of the HSP90 molecular chaperone.
机译:现在已经认识到,人类癌症中的遗传,表观遗传和表型异质性导致了治疗抗性-这些知识对当前的思维和实验产生了深远的影响。人们一直担心分子靶向疗法注定要失败,随着任何药物治疗的达尔文选择压力的产生,耐药性克隆都会出现。但是,两项研究表明,通过共同施用HSP90分子伴侣的药理抑制剂可以抑制耐药性的演变。

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