| Literature DB >> 30124467 |
Kwon-Ho Song1,2,3, Jae-Hoon Kim4, Young-Ho Lee1,2,3, Hyun Cheol Bae5, Hyo-Jung Lee1,2,3, Seon Rang Woo1,2,3, Se Jin Oh1,2,3, Kyung-Mi Lee1,2, Cassian Yee6, Bo Wook Kim7, Hanbyoul Cho4, Eun Joo Chung8, Joon-Yong Chung9, Stephen M Hewitt9, Tae-Wook Chung10, Ki-Tae Ha10, Young-Ki Bae11, Chih-Ping Mao12,13,14, Andrew Yang14, T C Wu14,15,16,17, Tae Woo Kim1,2,3.
Abstract
The host immune system plays a pivotal role in the emergence of tumor cells that are refractory to multiple clinical interventions including immunotherapy, chemotherapy, and radiotherapy. Here, we examined the molecular mechanisms by which the immune system triggers cross-resistance to these interventions. By examining the biological changes in murine and tumor cells subjected to sequential rounds of in vitro or in vivo immune selection via cognate cytotoxic T lymphocytes, we found that multimodality resistance arises through a core metabolic reprogramming pathway instigated by epigenetic loss of the ATP synthase subunit ATP5H, which leads to ROS accumulation and HIF-1α stabilization under normoxia. Furthermore, this pathway confers to tumor cells a stem-like and invasive phenotype. In vivo delivery of antioxidants reverses these phenotypic changes and resensitizes tumor cells to therapy. ATP5H loss in the tumor is strongly linked to failure of therapy, disease progression, and poor survival in patients with cancer. Collectively, our results reveal a mechanism underlying immune-driven multimodality resistance to cancer therapy and demonstrate that rational targeting of mitochondrial metabolic reprogramming in tumor cells may overcome this resistance. We believe these results hold important implications for the clinical management of cancer.Entities:
Keywords: Cancer; Immunology; Oncology
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Year: 2018 PMID: 30124467 PMCID: PMC6118592 DOI: 10.1172/JCI96804
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808