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FOXM1 nuclear transcription factor translocates into mitochondria and inhibits oxidative phosphorylation

Markaisa Black, Paritha Arumugam, Samriddhi Shukla, Arun Pradhan, Vladimir Ustiyan, David Milewski, Vladimir V. Kalinichenko, Tanya V. Kalin

2020Molecular Biology of the Cell39 citationsDOIOpen Access PDF

Abstract

Forkhead box M1 (FOXM1), a nuclear transcription factor that activates cell cycle regulatory genes, is highly expressed in a majority of human cancers. The function of FOXM1 independent of nuclear transcription is unknown. In the present study, we found the FOXM1 protein inside the mitochondria. Using site-directed mutagenesis, we generated FOXM1 mutant proteins that localized to distinct cellular compartments, uncoupling the nuclear and mitochondrial functions of FOXM1. Directing FOXM1 into the mitochondria decreased mitochondrial mass, membrane potential, respiration, and electron transport chain (ETC) activity. In mitochondria, the FOXM1 directly bound to and increased the pentatricopeptide repeat domain 1 (PTCD1) protein, a mitochondrial leucine-specific tRNA binding protein that inhibits leucine-rich ETC complexes. Mitochondrial FOXM1 did not change cellular proliferation. Thus, FOXM1 translocates into mitochondria and inhibits mitochondrial respiration by increasing PTCD1. We identify a new paradigm that FOXM1 regulates mitochondrial homeostasis in a process independent of nuclear transcription.

Topics & Concepts

BiologyMitochondrionOxidative phosphorylationCell biologyTranscription factorPhosphorylationNuclear transportTranscription (linguistics)Cell nucleusBiochemistryGeneNucleusLinguisticsPhilosophyFOXO transcription factor regulationMitochondrial Function and PathologyAdipose Tissue and Metabolism