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Small molecules targeting the NADH-binding pocket of VDAC modulate mitochondrial metabolism in hepatocarcinoma cells

Biomed Pharmacother. 2022-04; 
Kareem A Heslop, Pieter Burger, Christiana Kappler, Ashish K Solanki, Monika Gooz, Yuri K Peterson, Catherine Mills, Thomas Benton, Stephen A Duncan, Patrick M Woster, Eduardo N Maldonado
Products/Services Used Details Operation
Plasmid DNA Preparation … pET-29a recombinant human VDAC1 (rhuVDAC1) Open Reading Frame (ORF) clone plasmid construct, was purchased from GenScript and confirmed using sequencing. The plasmid … Get A Quote

摘要

Voltage dependent anion channels (VDAC) control the flux of most anionic respiratory substrates, ATP, ADP, and small cations, crossing the outer mitochondrial membrane. VDAC closure contributes to the partial suppression of mitochondrial metabolism that favors the Warburg phenotype of cancer cells. Recently, it has been shown that NADH binds to a specific pocket in the inner surface of VDAC1, also conserved in VDAC2 and 3, closing the channel. We hypothesized that binding of small molecules to the NADH pocket, maintain VDAC in an open configuration by preventing closure induced by NADH and possible other endogenous regulators. We screened in silico, the South Carolina Compound Collection SC (~100,000 proprietar... More

关键词

Cancer, Mitochondrial dysfunction, Mitochondrial metabolism, NADH-binding pocket, VDAC