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热休克蛋白90:癌症伴侣蛋白

Heat shock protein 90: the cancer chaperone.

作者信息

Neckers Len

机构信息

Urologic Oncology Branch, National Cancer Institute, Bethesda, MD 20892, USA.

出版信息

J Biosci. 2007 Apr;32(3):517-30. doi: 10.1007/s12038-007-0051-y.

Abstract

Heat shock protein 90 (Hsp90) is a molecular chaperone required for the stability and function of a number of conditionally activated and/or expressed signalling proteins, as well as multiple mutated, chimeric, and/or over-expressed signalling proteins, that promote cancer cell growth and/or survival. Hsp90 inhibitors are unique in that, although they are directed towards a specific molecular target, they simultaneously inhibit multiple cellular signalling pathways. By inhibiting nodal points in multiple overlapping survival pathways utilized by cancer cells, combination of an Hsp90 inhibitor with standard chemotherapeutic agents may dramatically increase the in vivo efficacy of the standard agent. Hsp90 inhibitors may circumvent the characteristic genetic plasticity that has allowed cancer cells to eventually evade the toxic effects of most molecularly targeted agents. The mechanism-based use of Hsp90 inhibitors, both alone and in combination with other drugs, should be effective toward multiple forms of cancer. Further, because Hsp90 inhibitors also induce Hsf-1-dependent expression of Hsp70, and because certain mutated Hsp90 client proteins are neurotoxic, these drugs display ameliorative properties in several neurodegenerative disease models, suggesting a novel role for Hsp90 inhibitors in treating multiple pathologies involving neurodegeneration.

摘要

热休克蛋白90(Hsp90)是一种分子伴侣,对于许多条件激活和/或表达的信号蛋白以及多种突变、嵌合和/或过表达的信号蛋白的稳定性和功能是必需的,这些蛋白促进癌细胞的生长和/或存活。Hsp90抑制剂的独特之处在于,尽管它们针对特定的分子靶点,但它们同时抑制多种细胞信号通路。通过抑制癌细胞利用的多个重叠存活通路中的节点,将Hsp90抑制剂与标准化疗药物联合使用可能会显著提高标准药物的体内疗效。Hsp90抑制剂可能会规避癌细胞最终逃避大多数分子靶向药物毒性作用所具有的特征性遗传可塑性。基于机制使用Hsp90抑制剂,无论是单独使用还是与其他药物联合使用,都应对多种形式的癌症有效。此外,由于Hsp90抑制剂还诱导Hsf-1依赖性的Hsp70表达,并且由于某些突变的Hsp90客户蛋白具有神经毒性,这些药物在几种神经退行性疾病模型中表现出改善特性,这表明Hsp90抑制剂在治疗涉及神经退行性变的多种病症中具有新的作用。

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