Combined inhibition of HMGCoA reductase and mitochondrial complex I induces tumor regression of BRAF inhibitor-resistant melanomas

Evelyn de Groot; Sruthy Varghese; Lin Tan; Barbara Knighton; Mary Sobieski; Nghi Nguyen; Yong Sung Park; Reid Powell; Philip L Lorenzi; Bin Zheng; Clifford Stephan; Y N Vashisht Gopal

doi:10.1186/s40170-022-00281-0

Combined inhibition of HMGCoA reductase and mitochondrial complex I induces tumor regression of BRAF inhibitor-resistant melanomas

Cancer Metab. 2022 Feb 22;10(1):6. doi: 10.1186/s40170-022-00281-0.

Authors

Evelyn de Groot¹, Sruthy Varghese², Lin Tan³, Barbara Knighton¹, Mary Sobieski⁴, Nghi Nguyen⁴, Yong Sung Park⁴, Reid Powell⁴, Philip L Lorenzi³, Bin Zheng⁵, Clifford Stephan⁴, Y N Vashisht Gopal^{6

7}

Affiliations

¹ Department of Melanoma Medical Oncology, University of Texas M.D. Anderson Cancer Center, Houston, TX, USA.
² Department of Translational Molecular Pathology, University of Texas M.D. Anderson Cancer Center, Houston, TX, USA.
³ Department of Bioinformatics and Computational Biology, University of Texas M.D. Anderson Cancer Center, Houston, TX, USA.
⁴ Institute of Bioscience and Technology, Texas A&M University, Houston, TX, USA.
⁵ Cutaneous Biology Research Center, Massachusetts General Hospital and Harvard Medical School, Charlestown, MA, USA.
⁶ Department of Melanoma Medical Oncology, University of Texas M.D. Anderson Cancer Center, Houston, TX, USA. vynanda@mdanderson.org.
⁷ Department of Translational Molecular Pathology, University of Texas M.D. Anderson Cancer Center, Houston, TX, USA. vynanda@mdanderson.org.

Abstract

Background: Primary and posttreatment resistance to BRAF^V600 mutation-targeting inhibitors leads to disease relapse in a majority of melanoma patients. In many instances, this resistance is promoted by upregulation of mitochondrial oxidative phosphorylation (OxPhos) in melanoma cells. We recently showed that a novel electron transport chain (ETC) complex I inhibitor, IACS-010759 (IACS), abolished OxPhos and significantly inhibited tumor growth of high-OxPhos, BRAF inhibitor (BRAFi)-resistant human melanomas. However, the inhibition was not uniform across different high OxPhos melanomas, and combination with BRAFi did not improve efficacy.

Methods: We performed a high-throughput unbiased combinatorial drug screen of clinically relevant small molecules to identify the most potent combination agent with IACS for inhibiting the growth of high-OxPhos, BRAFi-resistant melanomas. We performed bioenergetics and carbon-13 metabolite tracing to delineate the metabolic basis of sensitization of melanomas to the combination treatment. We performed xenograft tumor growth studies and Reverse-Phase Protein Array (RPPA)-based functional proteomics analysis of tumors from mice fed with regular or high-fat diet to evaluate in vivo molecular basis of sensitization to the combination treatment.

Results: A combinatorial drug screen and subsequent validation studies identified Atorvastatin (STN), a hydroxymethylglutaryl-coenzyme A reductase inhibitor (HMGCRi), as the most potent treatment combination with IACS to inhibit in vitro cell growth and induce tumor regression or stasis of some BRAFi-resistant melanomas. Bioenergetics analysis revealed a dependence on fatty acid metabolism in melanomas that responded to the combination treatment. RPPA analysis and carbon-13 tracing analysis in these melanoma cells showed that IACS treatment decreased metabolic fuel utilization for fatty acid metabolism, but increased substrate availability for activation of the mevalonate pathway by HMGCR, creating a dependence on this pathway. Functional proteomic analysis showed that IACS treatment inhibited MAPK but activated AKT pathway. Combination treatment with STN counteracted AKT activation.

Conclusions: STN and other clinically approved HMGCRi could be promising combinatorial agents for improving the efficacy of ETC inhibitors like IACS in BRAFi-resistant melanomas.

Keywords: Fatty acid metabolism; HMGCoA reductase; Melanoma; Oxidative phosphorylation; Statin; Therapeutic resistance.

Abstract

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