Cisplatin Enhances NK Cells Immunotherapy Efficacy to Suppress HCC Progression Via Altering the Androgen Receptor (AR)-ULBP2 Signals

Overview

Journal Cancer Lett

Specialty Oncology

Date 2016 Jan 26

PMID 26805759

Citations 39

Authors

Liang Shi

Hui Lin

Gonghui Li

Yin Sun

Jiliang Shen

Junjie Xu

Changyi Lin

Shuyuan Yeh

Xiujun Cai

Chawnshang Chang

Affiliations

Soon will be listed here.

Abstract

The aim of this study is to investigate the influence of cisplatin on the efficacy of natural killer (NK) cells immunotherapy to suppress HCC progression, and provide valuable information on better application of cisplatin in clinical settings. By using in vitro cell cytotoxicity test and in vivo liver orthotopic xenograft mice model, we identified the role of cisplatin in modulating NK cells cytotoxicity. Luciferase report assay and chromatin immunoprecipitation assay were applied for mechanism dissection. Immunohistochemistry is performed for sample staining. We found cisplatin could enhance the efficacy of NK cells immunotherapy to better suppress HCC progression via altering the androgen receptor (AR)-UL16-binding protein 2 (ULBP2) signals both in vitro and in vivo. Mechanism dissection revealed that cisplatin could suppress AR expression via two distinct ways: increasing miR-34a-5p to suppress AR expression and altering the ubiquitination to accelerate the AR protein degradation. The suppressed AR might then function through up-regulating ULBP2, a natural-killer group 2 member D ligand, to enhance the cytotoxicity of NK cells. Together, these results indicated an unrecognized favoring effect of cisplatin in HCC treatment. By suppressing AR in HCC, cisplatin could up-regulate cytotoxicity of NK cells to better target HCC. This finding may provide a potential new approach to control HCC by combining traditional chemotherapy with immunotherapy.

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