| Literature DB >> 31562248 |
Owen J Sansom1,2, Jurre J Kamphorst1,2,3, Grace H McGregor4,2, Andrew D Campbell4, Sigrid K Fey4,2, Sergey Tumanov4,2, David Sumpton4, Giovanny Rodriguez Blanco4, Gillian Mackay4, Colin Nixon4, Alexei Vazquez4,2.
Abstract
Statins are widely prescribed inhibitors of the mevalonate pathway, acting to lower systemic cholesterol levels. The mevalonate pathway is critical for tumorigenesis and is frequently upregulated in cancer. Nonetheless, reported effects of statins on tumor progression are ambiguous, making it unclear whether statins, alone or in combination, can be used for chemotherapy. Here, using advanced mass spectrometry and isotope tracing, we showed that statins only modestly affected cancer cholesterol homeostasis. Instead, they significantly reduced synthesis and levels of another downstream product, the mitochondrial electron carrier coenzyme Q, both in cultured cancer cells and tumors. This compromised oxidative phosphorylation, causing severe oxidative stress. To compensate, cancer cells upregulated antioxidant metabolic pathways, including reductive carboxylation, proline synthesis, and cystine import. Targeting cystine import with an xCT transporter-lowering MEK inhibitor, in combination with statins, caused profound tumor cell death. Thus, statin-induced ROS production in cancer cells can be exploited in a combinatorial regimen. SIGNIFICANCE: Cancer cells induce specific metabolic pathways to alleviate the increased oxidative stress caused by statin treatment, and targeting one of these pathways synergizes with statins to produce a robust antitumor response.See related commentary by Cordes and Metallo, p. 151. ©2019 American Association for Cancer Research.Entities:
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Year: 2019 PMID: 31562248 DOI: 10.1158/0008-5472.CAN-19-0644
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701