Unleashing a novel function of Endonuclease G in mitochondrial genome instability
0301 basic medicine
QH301-705.5
Science
DNA, Mitochondrial
Genomic Instability
tetraplexes
03 medical and health sciences
Endo G
Humans
Animals
Biology (General)
mitochondrial deletion
Mammals
double-strand breaks
0303 health sciences
Endodeoxyribonucleases
Q
R
Cell Biology
Mitochondria
3. Good health
mitochondrial fragility
Genome, Mitochondrial
MMEJ
Medicine
DOI:
10.7554/elife.69916
Publication Date:
2022-11-17T11:15:18Z
AUTHORS (7)
ABSTRACT
Having its genome makes the mitochondrion a unique and semiautonomous organelle within cells. Mammalian mitochondrial DNA (mtDNA) is a double-stranded closed circular molecule of about 16 kb coding for 37 genes. Mutations, including deletions in the mitochondrial genome, can culminate in different human diseases. Mapping the deletion junctions suggests that the breakpoints are generally seen at hotspots. ‘9 bp deletion’ (8271–8281), seen in the intergenic region of cytochrome c oxidase II/tRNALys, is the most common mitochondrial deletion. While it is associated with several diseases like myopathy, dystonia, and hepatocellular carcinoma, it has also been used as an evolutionary marker. However, the mechanism responsible for its fragility is unclear. In the current study, we show that Endonuclease G, a mitochondrial nuclease responsible for nonspecific cleavage of nuclear DNA during apoptosis, can induce breaks at sequences associated with ‘9 bp deletion’ when it is present on a plasmid or in the mitochondrial genome. Through a series of in vitro and intracellular studies, we show that Endonuclease G binds to G-quadruplex structures formed at the hotspot and induces DNA breaks. Therefore, we uncover a new role for Endonuclease G in generating mtDNA deletions, which depends on the formation of G4 DNA within the mitochondrial genome. In summary, we identify a novel property of Endonuclease G, besides its role in apoptosis and the recently described ‘elimination of paternal mitochondria during fertilisation.
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