On the Origin of ATP Synthesis in Cancer

Thomas N Seyfried; Gabriel Arismendi-Morillo; Purna Mukherjee; Christos Chinopoulos

doi:10.1016/j.isci.2020.101761

On the Origin of ATP Synthesis in Cancer

iScience. 2020 Nov 2;23(11):101761. doi: 10.1016/j.isci.2020.101761. eCollection 2020 Nov 20.

Authors

Thomas N Seyfried¹, Gabriel Arismendi-Morillo², Purna Mukherjee¹, Christos Chinopoulos³

Affiliations

¹ Biology Department, Boston College, 140 Commonwealth Avenue, Chestnut Hill, MA 02467, USA.
² Electron Microscopy Laboratory, Biological Researches Institute, Faculty of Medicine, University of Zulia, Maracaibo, Venezuela.
³ Department of Medical Biochemistry, Semmelweis University, Budapest, 1094, Hungary.

Abstract

ATP is required for mammalian cells to remain viable and to perform genetically programmed functions. Maintenance of the ΔG'_ATP hydrolysis of -56 kJ/mole is the endpoint of both genetic and metabolic processes required for life. Various anomalies in mitochondrial structure and function prevent maximal ATP synthesis through OxPhos in cancer cells. Little ATP synthesis would occur through glycolysis in cancer cells that express the dimeric form of pyruvate kinase M2. Mitochondrial substrate level phosphorylation (mSLP) in the glutamine-driven glutaminolysis pathway, substantiated by the succinate-CoA ligase reaction in the TCA cycle, can partially compensate for reduced ATP synthesis through both OxPhos and glycolysis. A protracted insufficiency of OxPhos coupled with elevated glycolysis and an auxiliary, fully operational mSLP, would cause a cell to enter its default state of unbridled proliferation with consequent dedifferentiation and apoptotic resistance, i.e., cancer. The simultaneous restriction of glucose and glutamine offers a therapeutic strategy for managing cancer.

Keywords: Biochemistry; Biological Sciences; Cancer Systems Biology; Cell Biology.

Publication types

Review