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A white paper on Phospholipid Hydroperoxide Glutathione Peroxidase (GPx4) forty years later

Journal

FREE RADICAL BIOLOGY AND MEDICINE
Volume 188, Issue -, Pages 117-133

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.freeradbiomed.2022.06.227

Keywords

Ferroptosis; Lipid peroxidation; Vitamin E; Redox homeostasis; Selenium

Funding

  1. Progetto di Ricerca Dipartimentale fondi SID 2020'' of the University of Padova

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GPx4 is an enzyme that inhibits lipid peroxidation and plays a crucial role in cell death and various biological processes. The details of its interaction at the membrane cytosol interface and its expression control mechanisms are still poorly defined. Additionally, GPx4 is also involved in sperm maturation independent of lipid peroxidation.
The purification of a protein inhibiting lipid peroxidation led to the discovery of the selenoperoxidase GPx4 forty years ago. Thus, the evidence of the enzymatic activity was reached after identifying the biological effect and unambiguously defined the relationship between the biological function and the enzymatic activity. In the syllogism where GPx4 inhibits lipid peroxidation and its inhibition is lethal, cell death is operated by lipid peroxidation. Based on this rationale, this form of cell death emerged as regulated iron-enforced oxygen toxicity and was named ferroptosis in 2012. In the last decades, we learned that reduction of lipid hydroperoxides is indispensable and, in cooperation with prooxidant systems, controls the critical steady state of lipid peroxidation. This concept defined the GPx4 reaction as both the target for possible anti-cancer therapy and if insufficient, as cause of degenerative diseases. We know the reaction mechanism, but the details of the interaction at the membrane cytosol interface are still poorly defined. We know the gene structure, but the knowledge about expression control is still limited. The same holds true for post-transcriptional modifications. Reverse genetics indicate that GPx4 has a role in inflammation, immunity, and differentiation, but the observations emerging from these studies need a more specifically addressed biochemical evidence. Finally, the role of GPx4 in spermato-genesis disclosed an area unconnected to lipid peroxidation. In its mitochondrial and nuclear form, the perox-idase catalyzes the oxidation of protein thiols in two specific aspects of sperm maturation: stabilization of the mid-piece and chromatin compaction. Thus, although available evidence converges to the notion that GPx4 activity is vital due to the inhibition of lipid peroxidation, it is reasonable to foresee other unknown aspects of the GPx4 reaction to be disclosed.

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