| Literature DB >> 30801875 |
Daniela Verrigni1, Michela Di Nottia1, Anna Ardissone2,3, Enrico Baruffini4, Alessia Nasca5, Andrea Legati5, Emanuele Bellacchio6, Gigliola Fagiolari7, Diego Martinelli8, Lucia Fusco9, Domenica Battaglia10, Giulia Trani1, Gianmarco Versienti5, Silvia Marchet5, Alessandra Torraco1, Teresa Rizza1, Margherita Verardo1, Adele D'Amico1, Daria Diodato1, Isabella Moroni2, Costanza Lamperti5, Stefania Petrini11, Maurizio Moggio7, Paola Goffrini4, Daniele Ghezzi5,12, Rosalba Carrozzo1, Enrico Bertini1.
Abstract
Mitochondria are highly dynamic organelles, undergoing continuous fission and fusion. The DNM1L (dynamin-1 like) gene encodes for the DRP1 protein, an evolutionary conserved member of the dynamin family, responsible for fission of mitochondria, and having a role in the division of peroxisomes, as well. DRP1 impairment is implicated in several neurological disorders and associated with either de novo dominant or compound heterozygous mutations. In five patients presenting with severe epileptic encephalopathy, we identified five de novo dominant DNM1L variants, the pathogenicity of which was validated in a yeast model. Fluorescence microscopy revealed abnormally elongated mitochondria and aberrant peroxisomes in mutant fibroblasts, indicating impaired fission of these organelles. Moreover, a very peculiar finding in our cohort of patients was the presence, in muscle biopsy, of core like areas with oxidative enzyme alterations, suggesting an abnormal distribution of mitochondria in the muscle tissue.Entities:
Keywords: DNM1L; epileptic encephalopathy; mitochondrial disorders; mitochondrial dynamics; mitochondrial fission; muscle biopsy
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Year: 2019 PMID: 30801875 DOI: 10.1002/humu.23729
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878