Publication | Open Access
A histone deacetylase 3 and mitochondrial complex I axis regulates toxic formaldehyde production
18
Citations
41
References
2023
Year
Epigenetic ChangeGeneticsMolecular BiologyFormaldehyde DetoxificationEpigeneticsRedox BiologyOxidative StressHistone Deacetylase 3Cellular Formaldehyde ProductionMitochondrial BiogenesisConsiderable Genotoxic FormaldehydeBiochemistryMedicineGene ExpressionEpigenetic RegulationChromatin FunctionReductive StressChromatinChromatin StructureMitochondrial FunctionChromatin RemodelingNatural SciencesEpigenomicsCellular BiochemistryMetabolismMitochondrial ComplexGenome EditingCarbonyl Metabolism
Cells produce considerable genotoxic formaldehyde from an unknown source. We carry out a genome-wide CRISPR-Cas9 genetic screen in metabolically engineered HAP1 cells that are auxotrophic for formaldehyde to find this cellular source. We identify histone deacetylase 3 (HDAC3) as a regulator of cellular formaldehyde production. HDAC3 regulation requires deacetylase activity, and a secondary genetic screen identifies several components of mitochondrial complex I as mediators of this regulation. Metabolic profiling indicates that this unexpected mitochondrial requirement for formaldehyde detoxification is separate from energy generation. HDAC3 and complex I therefore control the abundance of a ubiquitous genotoxic metabolite.
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