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首页> 外文期刊>Archives of Toxicology >Heat shock proteins and heat shock factor 1 in carcinogenesis and tumor development: An update
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Heat shock proteins and heat shock factor 1 in carcinogenesis and tumor development: An update

机译:在致癌物和肿瘤发育中,热休克蛋白和热休克因子1:更新

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摘要

Heat shock proteins (HSP) are a subset of the molecular chaperones, best known for their rapid and abundant induction by stress. HSP genes are activated at the transcriptional level by heat shock transcription factor 1 (HSF1). During the progression ofmany types of cancer, this heat shock transcriptional regulon becomes co-opted by mechanisms that are currently unclear, although evidently triggered in the emerging tumor cell. Concerted activation of HSF1 and the accumulation of HSPs then participate in many of the traits that permit the malignant phenotype. Thus, cancers of many histologies exhibit activated HSF1 and increased HSP levels that may help to deter tumor suppression and evade therapy in the clinic. We review here the extensive work that has been carried out and is still in progress aimed at (1) understanding the oncogenic mechanisms by which HSP genes are switched on, (2) determining the roles of HSF1/HSP in malignant transformation and (3) discovering approaches to therapy based on disrupting the influence of the HSF1-controlled transcriptome in cancer.
机译:热休克蛋白(HSP)是分子伴侣的子集,最令人着称其应激急救。通过热冲击转录因子1(HSF1)在转录水平上激活HSP基因。在癌症类型的进展过程中,这种热休克转录调节件通过目前不清楚的机制共选择,尽管在新出现的肿瘤细胞中显然触发。 HSF1的协调激活和HSP的积累然后参与许多允许恶性表型的性状。因此,许多组织学的癌症表现出活性的HSF1和增加的HSP水平,可能有助于阻止临床肿瘤抑制和逃避治疗。我们在这里审查已经进行的广泛工作,仍然是(1)理解HSP基因接通的致癌机制,(2)确定HSF1 / HSP在恶性转化中的作用和(3)基于破坏癌症HSF1控制转录组的影响的治疗方法。

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