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可用于研究癌症中内源性Hsp70相互作用组的亲和纯化探针。

Affinity purification probes of potential use to investigate the endogenous Hsp70 interactome in cancer.

作者信息

Rodina Anna, Taldone Tony, Kang Yanlong, Patel Pallav D, Koren John, Yan Pengrong, DaGama Gomes Erica M, Yang Chenghua, Patel Maulik R, Shrestha Liza, Ochiana Stefan O, Santarossa Cristina, Maharaj Ronnie, Gozman Alexander, Cox Marc B, Erdjument-Bromage Hediye, Hendrickson Ronald C, Cerchietti Leandro, Melnick Ari, Guzman Monica L, Chiosis Gabriela

机构信息

Program in Molecular Pharmacology and Chemistry and Department of Medicine and §Program in Molecular Biology, Proteomics Core, Memorial Sloan-Kettering Cancer Center , New York, New York 10021, United States.

出版信息

ACS Chem Biol. 2014 Aug 15;9(8):1698-705. doi: 10.1021/cb500256u. Epub 2014 Jun 17.

Abstract

Heat shock protein 70 (Hsp70) is a family of proteins with key roles in regulating malignancy. Cancer cells rely on Hsp70 to inhibit apoptosis, regulate senescence and autophagy, and maintain the stability of numerous onco-proteins. Despite these important biological functions in cancer, robust chemical tools that enable the analysis of the Hsp70-regulated proteome in a tumor-by-tumor manner are yet unavailable. Here we take advantage of a recently reported Hsp70 ligand to design and develop an affinity purification chemical toolset for potential use in the investigation of the endogenous Hsp70-interacting proteome in cancer. We demonstrate that these tools lock Hsp70 in complex with onco-client proteins and effectively isolate Hsp70 complexes for identification through biochemical techniques. Using these tools we provide proof-of-concept analyses that glimpse into the complex roles played by Hsp70 in maintaining a multitude of cell-specific malignancy-driving proteins.

摘要

热休克蛋白70(Hsp70)是一类在调节恶性肿瘤过程中起关键作用的蛋白质。癌细胞依赖Hsp70来抑制细胞凋亡、调节衰老和自噬,并维持众多癌蛋白的稳定性。尽管Hsp70在癌症中具有这些重要的生物学功能,但目前仍缺乏能够逐个肿瘤地分析Hsp70调节蛋白质组的强大化学工具。在此,我们利用最近报道的一种Hsp70配体,设计并开发了一套亲和纯化化学工具集,有望用于研究癌症中内源性Hsp70相互作用蛋白质组。我们证明,这些工具能使Hsp70与癌蛋白客户蛋白形成复合物,并通过生化技术有效分离Hsp70复合物以进行鉴定。利用这些工具,我们进行了概念验证分析,初步了解了Hsp70在维持多种细胞特异性恶性驱动蛋白方面所起的复杂作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1100/4136700/cae92e3537a1/cb-2014-00256u_0002.jpg

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