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• W3214358109 abstract "Mitochondrial DNA (mtDNA) associated mitochondrial diseases hold a crucial position but comprehensive and systematic studies are relatively rare. Among the 262 patients of four children's hospitals in China, 96%-point mutations (30 alleles in 11 genes encoding tRNA, rRNA, Complex I and V) and 4%-deletions (seven of ten had not been reported before) were identified as the cause of 14 phenotypes. MILS presented the highest genetic heterogeneity, while the m.3243A > G mutation was the only hotspot mutation with a wide range of phenotypes. The degrees of heteroplasmy in the leukocytes of MM were higher than MELAS. The heteroplasmy level of patients was higher than that in mild and carrier group, while we found low-level heteroplasmy pathogenic mutations as well. Some homoplasmic variations (e.g., m.9176 T > C mutation) are having high incomplete penetrance. For a suspected MELAS, m.3243A > G mutation was recommended to detect first; while for a suspected LS, trios-WES and mtDNA genome sequencing by NGS were recommended first in both blood and urine." @default.
• W3214358109 created "2021-11-22" @default.
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• W3214358109 date "2022-01-01" @default.
• W3214358109 modified "2023-09-26" @default.
• W3214358109 title "Phenotypes and genotypes of mitochondrial diseases with mtDNA variations in Chinese children: A multi-center study" @default.
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• W3214358109 doi "https://doi.org/10.1016/j.mito.2021.11.006" @default.
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