Nuclear Translocation and Activation of YAP by Hypoxia Contributes to the Chemoresistance of SN38 in Hepatocellular Carcinoma Cells

Overview

Journal Oncotarget

Specialty Oncology

Date 2016 Jan 16

PMID 26771844

Citations 40

Authors

Xiao-Yang Dai

Lin-Han Zhuang

Dan-Dan Wang

Tian-Yi Zhou

Lin-Lin Chang

Ren-Hua Gai

Di-Feng Zhu

Bo Yang

Hong Zhu

Qiao-Jun He

Affiliations

Soon will be listed here.

Abstract

Although hypoxia is a prominent feature contributing to the therapeutic resistance of hepatocellular carcinoma cells (HCC) against chemotherapeutic agents, including the Topoisomerase I inhibitor SN38, the underlying mechanism is not fully understood and its understanding remains a major clinical challenge. In the present study, we found that hypoxia-induced nuclear translocation and accumulation of YAP acted as a survival input to promote resistance to SN38 in HCC. The induction of YAP by hypoxia was not mediated by HIF-1α because manipulating the abundance of HIF-1α with CoCl2, exogenous expression, and RNA interference had no effect on the phosphorylation or total levels of YAP. The mevalonate-HMG-CoA reductase (HMGCR) pathway may modulate the YAP activation under hypoxia. Combined YAP inhibition using either siRNA or the HMGCR inhibitor statins together with SN38 treatment produced improved anti-cancer effects in HCC cells. The increased anti-cancer effect of the combined treatment with statins and irinotecan (the prodrug of SN-38) was further validated in a human HepG2 xenograft model of HCC in nude mice. Taken together, our findings identify YAP as a novel mediator of hypoxic-resistance to SN38. These results suggest that the administration of SN28 together with the suppression of YAP using statins is a promising strategy for enhancing the treatment response in HCC patients, particularly in advanced stage HCC cases presenting hypoxic resistance.

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