Literature DB >> 31045494

The long non-coding RNA Cerox1 is a post transcriptional regulator of mitochondrial complex I catalytic activity.

Tamara M Sirey1,2, Kenny Roberts2, Wilfried Haerty2, Oscar Bedoya-Reina1,2, Sebastian Rogatti-Granados1,2, Jennifer Y Tan2, Nick Li2, Lisa C Heather3, Roderick N Carter4, Sarah Cooper5, Andrew J Finch1, Jimi Wills1, Nicholas M Morton4, Ana Claudia Marques2, Chris P Ponting1,2.   

Abstract

To generate energy efficiently, the cell is uniquely challenged to co-ordinate the abundance of electron transport chain protein subunits expressed from both nuclear and mitochondrial genomes. How an effective stoichiometry of this many constituent subunits is co-ordinated post-transcriptionally remains poorly understood. Here we show that Cerox1, an unusually abundant cytoplasmic long noncoding RNA (lncRNA), modulates the levels of mitochondrial complex I subunit transcripts in a manner that requires binding to microRNA-488-3p. Increased abundance of Cerox1 cooperatively elevates complex I subunit protein abundance and enzymatic activity, decreases reactive oxygen species production, and protects against the complex I inhibitor rotenone. Cerox1 function is conserved across placental mammals: human and mouse orthologues effectively modulate complex I enzymatic activity in mouse and human cells, respectively. Cerox1 is the first lncRNA demonstrated, to our knowledge, to regulate mitochondrial oxidative phosphorylation and, with miR-488-3p, represent novel targets for the modulation of complex I activity.
© 2019, Sirey et al.

Entities:  

Keywords:  biochemistry; chemical biology; energy metabolism; genetics; genomics; human; long noncoding RNA; miRNA; mitochondria; mouse; post-transcriptional regulation

Mesh:

Substances:

Year:  2019        PMID: 31045494      PMCID: PMC6542586          DOI: 10.7554/eLife.45051

Source DB:  PubMed          Journal:  Elife        ISSN: 2050-084X            Impact factor:   8.140


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