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ERdj 同源物的化学生物组学和生物信息学分析为其在癌症中的独特作用提供了依据。

Chemogenomic and bioinformatic profiling of ERdj paralogs underpins their unique roles in cancer.

机构信息

Department of Biological Sciences, University of North Carolina Charlotte, Charlotte, NC, 28223, USA.

出版信息

Cell Stress Chaperones. 2021 Mar;27(2):135-147. doi: 10.1007/s12192-022-01256-2. Epub 2022 Feb 7.

Abstract

The ER-resident Hsp70 paralog BiP is important in cellular homeostasis as well as in cancer cell progression. Although several BiP inhibitors have been developed, they have not succeeded in clinical trials due to toxicity issues. ER-resident co-chaperones (ERdjs) tailor the activity and specificity of BiP. Here, we report multiple-cancer analyses of BiP and ERdj genomic alterations including mRNA expression from cancer patients using available data from The Cancer Genome Atlas (TCGA). We examine the individual roles of BiP co-chaperones ERdj1-8 in mediating anticancer drug resistance through chemogenomic screening of ERdj1-8 CRISPR KO cells. In keeping with the idea that ERdjs regulate distinct facets of proteostasis, we find that each ERdj KO displays a unique signature of drug resistance. Taken together, our results demonstrate a novel way to understand functional specificity of ERdjs, suggesting a future personalized medicine approach, whereby ERdj mutation status is assessed to design an effective anticancer treatment plan.

摘要

内质网驻留的 Hsp70 同源蛋白 BiP 在细胞内稳态以及癌细胞进展中都很重要。尽管已经开发了几种 BiP 抑制剂,但由于毒性问题,它们在临床试验中并未成功。内质网驻留的共伴侣(ERdjs)调节 BiP 的活性和特异性。在这里,我们利用癌症基因组图谱(TCGA)中提供的癌症患者的 mRNA 表达数据,对包括 BiP 和 ERdj 基因组改变在内的多种癌症进行了分析。我们通过对 ERdj1-8 CRISPR KO 细胞进行化学生物学筛选,研究了 BiP 共伴侣 ERdj1-8 在介导抗癌药物耐药性方面的个体作用。与 ERdjs 调节蛋白质稳态不同方面的观点一致,我们发现每个 ERdj KO 都显示出独特的耐药特征。总之,我们的结果表明了一种理解 ERdjs 功能特异性的新方法,这提示了未来的个性化医疗方法,即评估 ERdj 突变状态以设计有效的抗癌治疗方案。

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