Cureus. 2025 Sep;17(9): e93331
The Warburg effect, characterized by the preferential conversion of glucose to lactate despite adequate oxygen availability, constitutes a regulated metabolic adaptation rather than a mere dysfunctional response to hypoxia. This metabolic shift arises because lactate dehydrogenase (LDH) exhibits a significantly higher catalytic capacity compared to pyruvate dehydrogenase (PDH), resulting in a substantial reduction of pyruvate to lactate once PDH becomes saturated. In cancer cells, this kinetic preference is further amplified by the upregulation of glucose and monocarboxylate transporters (GLUT1, MCT1, and MCT4) and alterations to the plasma membrane, which enhance transport efficiency. These adaptations maintain a high glycolytic flux, facilitate continuous lactate efflux, and circumvent traditional feedback inhibition. The accumulation of glycolytic intermediates supports the biosynthesis of nucleotides, lipids, and proteins, thereby promoting tumorigenesis. Over time, metabolite-induced DNA methylation and chromatin remodeling reinforce this metabolic state, stabilizing the oxygen-independent proliferative phenotype. Consequently, the Warburg effect is best conceptualized as a primary metabolic strategy initiated by membrane remodeling, sustained by kinetic flux imbalances, and perpetuated by epigenetic feedback, collectively enabling tumor growth and survival in adverse microenvironments.
Keywords: atp; cancer; cell proliferation; epigenetic; glucose transporter; glycolysis; lactate; lactate dehydrogenase; monocarboxylate transporters; warburg effect