Unexpected sequences and structures of mtDNA required for efficient transcription from the first heavy-strand promoter.
Akira UchidaDivakaran MurugesapillaiMarkus KastnerYao WangMaria F LodeiroShaan PrabhakarGuinevere V OliverJamie J ArnoldL James MaherMark C WilliamsCraig E CameronPublished in: eLife (2017)
Human mtDNA contains three promoters, suggesting a need for differential expression of the mitochondrial genome. Studies of mitochondrial transcription have used a reductionist approach, perhaps masking differential regulation. Here we evaluate transcription from light-strand (LSP) and heavy-strand (HSP1) promoters using templates that mimic their natural context. These studies reveal sequences upstream, hypervariable in the human population (HVR3), and downstream of the HSP1 transcription start site required for maximal yield. The carboxy-terminal tail of TFAM is essential for activation of HSP1 but not LSP. Images of the template obtained by atomic force microscopy show that TFAM creates loops in a discrete region, the formation of which correlates with activation of HSP1; looping is lost in tail-deleted TFAM. Identification of HVR3 as a transcriptional regulatory element may contribute to between-individual variability in mitochondrial gene expression. The unique requirement of HSP1 for the TFAM tail may enable its regulation by post-translational modifications.
Keyphrases
- heat shock protein
- heat shock
- transcription factor
- gene expression
- heat stress
- oxidative stress
- endothelial cells
- atomic force microscopy
- dna methylation
- mitochondrial dna
- copy number
- genome wide
- induced pluripotent stem cells
- pluripotent stem cells
- deep learning
- high resolution
- optical coherence tomography
- heart rate
- single molecule
- resistance training
- case control
- blood pressure
- body composition
- molecularly imprinted
- liquid chromatography