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Malate dehydrogenase as a multi-purpose target for drug discovery. | LitMetric

Malate dehydrogenase as a multi-purpose target for drug discovery.

Essays Biochem

Department of Chemistry and Biochemistry, Manhattan College, The Bronx, NY, U.S.A.

Published: October 2024

AI Article Synopsis

  • Malate dehydrogenase (MDH) enzymes are vital for cellular metabolism, converting malate to oxaloacetate and supporting processes like aerobic respiration and glycolysis.
  • Both human isoforms of MDH are important in metabolic pathways, and their overexpression in diseases like cancer makes them attractive drug targets.
  • Ongoing research is focused on developing small-molecule inhibitors of MDH, which could offer new therapeutic options for various metabolic, neurological, and infectious diseases.

Article Abstract

Malate dehydrogenase (MDH) enzymes play critical roles in cellular metabolism, facilitating the reversible conversion of malate to oxaloacetate using NAD+/NADH as a cofactor. The two human isoforms of MDH have roles in the citric acid cycle and the malate-aspartate shuttle, and thus both are key enzymes in aerobic respiration as well as regenerating the pool of NAD+ used in glycolysis. This review highlights the potential of MDH as a therapeutic drug target in various diseases, including metabolic and neurological disorders, cancer, and infectious diseases. The most promising molecules for targeting MDH have been examined in the context of human malignancies, where MDH is frequently overexpressed. Recent studies have led to the identification of several antagonists, some of which are broad MDH inhibitors while others have selectivity for either of the two human MDH isoforms. Other promising compounds have been studied in the context of parasitic MDH, as inhibiting the function of the enzyme could selectively kill the parasite. Research is ongoing with these chemical scaffolds to develop more effective small-molecule drug leads that would have great potential for clinical applications.

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Source
http://dx.doi.org/10.1042/EBC20230081DOI Listing

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