1. Academic Validation
  2. Autophagy inhibitors increase the susceptibility of KRAS-mutant human colorectal cancer cells to a combined treatment of 2-deoxy-D-glucose and lovastatin

Autophagy inhibitors increase the susceptibility of KRAS-mutant human colorectal cancer cells to a combined treatment of 2-deoxy-D-glucose and lovastatin

  • Acta Pharmacol Sin. 2021 Nov;42(11):1875-1887. doi: 10.1038/s41401-021-00612-9.
Xiao-Ming Huang 1 Jia-Jun Huang 1 Jing-Jing Du 1 Na Zhang 1 Ze Long 1 You Yang 1 Fang-Fang Zhong 1 Bo-Wen Zheng 1 Yun-Fu Shen 1 Zhe Huang 1 Xiang Qin 1 Jun-He Chen 1 Qian-Yu Lin 1 Wan-Jun Lin 1 Wen-Zhe Ma 2
Affiliations

Affiliations

  • 1 State Key Laboratory of Quality Research in Chinese Medicine, Macau University of Science and Technology, Macau, China.
  • 2 State Key Laboratory of Quality Research in Chinese Medicine, Macau University of Science and Technology, Macau, China. wzma@must.edu.mo.
Abstract

RAS-driven colorectal Cancer relies on glucose metabolism to support uncontrolled growth. However, monotherapy with glycolysis inhibitors like 2-deoxy-D-glucose causes limited effectiveness. Recent studies suggest that anti-tumor effects of glycolysis inhibition could be improved by combination treatment with inhibitors of Oxidative Phosphorylation. In this study we investigated the effect of a combination of 2-deoxy-D-glucose with lovastatin (a known inhibitor of mevalonate pathway and Oxidative Phosphorylation) on growth of KRAS-mutant human colorectal Cancer cell lines HCT116 and LoVo. A combination of lovastatin (>3.75 μM) and 2-deoxy-D-glucose (>1.25 mM) synergistically reduced cell viability, arrested cells in the G2/M phase, and induced Apoptosis. The combined treatment also reduced cellular oxygen consumption and extracellular acidification rate, resulting in decreased production of ATP and lower steady-state ATP levels. Energy depletion markedly activated AMPK, inhibited mTOR and Ras signaling pathways, eventually inducing Autophagy, the cellular pro-survival process under metabolic stress, whereas inhibition of Autophagy by chloroquine (6.25 μM) enhanced the cytotoxic effect of the combination of lovastatin and 2-deoxy-D-glucose. These in vitro experiment results were reproduced in a nude mouse xenograft model of HCT116 cells. Our findings suggest that concurrently targeting glycolysis, Oxidative Phosphorylation, and Autophagy may be a promising regimen for the management of RAS-driven colorectal cancers.

Keywords

2DG; OXPHOS; autophagy; chloroquine; glycolysis; human colorectal cancers; hydroxychloroquine; lovastatin.

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