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Overcoming HSP27-mediated resistance by altered dimerization of HSP27 using small molecules.


ABSTRACT: Heat shock protein 27 (HSP27, HSPB1) is an anti-apoptotic protein characterized for its tumorigenic and metastatic properties, and now referenced as a major therapeutic target in many types of cancer. The biochemical properties of HSP27 rely on a structural oligomeric and dynamic organization that is important for its chaperone activity. Down-regulation by small interfering RNA or inhibition with a dominant-negative mutant efficiently counteracts the anti-apoptotic and protective properties of HSP27. However, unlike other HSPs such as HSP90 and HSP70, small molecule approaches for neutralization of HSP27 are not well established because of the absence of an ATP binding domain. Previously, we found that a small molecule, zerumbone (ZER), induced altered dimerization of HSP27 by cross linking the cysteine residues required to build a large oligomer, led to sensitization in combination with radiation. In this study, we identified another small molecule, a xanthone compound, more capable of altering dimeric HSP27 than ZER and yielding sensitization in human lung cancer cells when combined with HSP90 inhibitors or standard anticancer modalities such as irradiation and cytotoxic anticancer drugs. Therefore, altered dimerization of HSP27 represents a good strategy for anticancer therapy in HSP27-overexpressing cancer cells.

SUBMITTER: Kim JH 

PROVIDER: S-EPMC5288177 | biostudies-literature | 2016 Aug

REPOSITORIES: biostudies-literature

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Overcoming HSP27-mediated resistance by altered dimerization of HSP27 using small molecules.

Kim Jee Hye JH   Jung Ye Jin YJ   Choi Byeol B   Lee Na Lim NL   Lee Hae Jun HJ   Kwak Soo Yeon SY   Kwon Youngjoo Y   Na Younghwa Y   Lee Yun-Sil YS  

Oncotarget 20160801 33


Heat shock protein 27 (HSP27, HSPB1) is an anti-apoptotic protein characterized for its tumorigenic and metastatic properties, and now referenced as a major therapeutic target in many types of cancer. The biochemical properties of HSP27 rely on a structural oligomeric and dynamic organization that is important for its chaperone activity. Down-regulation by small interfering RNA or inhibition with a dominant-negative mutant efficiently counteracts the anti-apoptotic and protective properties of H  ...[more]

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