The GAPDH redox switch safeguards reductive capacity and enables survival of stressed tumour cells.
Deepti TalwarColin G MillerJustus GrossmannLukasz SzyrwielTorsten SchweckeVadim DemichevAna-Matea Mikecin DrazicAnand MayakondaPavlo LutsikCarmen VeithMichael D MilsomKarin Müller-DeckerMichael MullederMarkus RalserTobias P DickPublished in: Nature metabolism (2023)
Glyceraldehyde 3-phosphate dehydrogenase (GAPDH) is known to contain an active-site cysteine residue undergoing oxidation in response to hydrogen peroxide, leading to rapid inactivation of the enzyme. Here we show that human and mouse cells expressing a GAPDH mutant lacking this redox switch retain catalytic activity but are unable to stimulate the oxidative pentose phosphate pathway and enhance their reductive capacity. Specifically, we find that anchorage-independent growth of cells and spheroids is limited by an elevation of endogenous peroxide levels and is largely dependent on a functional GAPDH redox switch. Likewise, tumour growth in vivo is limited by peroxide stress and suppressed when the GAPDH redox switch is disabled in tumour cells. The induction of additional intratumoural oxidative stress by chemo- or radiotherapy synergized with the deactivation of the GAPDH redox switch. Mice lacking the GAPDH redox switch exhibit altered fatty acid metabolism in kidney and heart, apparently in compensation for the lack of the redox switch. Together, our findings demonstrate the physiological and pathophysiological relevance of oxidative GAPDH inactivation in mammals.
Keyphrases
- induced apoptosis
- hydrogen peroxide
- oxidative stress
- cell cycle arrest
- endoplasmic reticulum stress
- fatty acid
- nitric oxide
- heart failure
- squamous cell carcinoma
- electron transfer
- type diabetes
- dna damage
- photodynamic therapy
- rectal cancer
- radiation induced
- heat stress
- stress induced
- drug delivery
- sensitive detection
- cell proliferation
- free survival