| Literature DB >> 33671400 |
Yeonmi Lee1, Taeho Kim2, Miju Lee1, Seongjun So1, Mustafa Zafer Karagozlu1, Go Hun Seo2, In Hee Choi2, Peter C W Lee3, Chong-Jai Kim4, Eunju Kang1, Beom Hee Lee2.
Abstract
Defects in the mitochondrial genome (mitochondrial DNA (mtDNA)) are associated with both congenital and acquired disorders in humans. Nuclear-encoded DNA polymerase subunit gamma (POLG) plays an important role in mtDNA replication, and proofreading and mutations in POLG have been linked with increased mtDNA deletions. SSBP1 is also a crucial gene for mtDNA replication. Here, we describe a patient diagnosed with Pearson syndrome with large mtDNA deletions that were not detected in the somatic cells of the mother. Exome sequencing was used to evaluate the nuclear factors associated with the patient and his family, which revealed a paternal POLG mutation (c.868C > T) and a maternal SSBP1 mutation (c.320G > A). The patient showed lower POLG and SSBP1 expression than his healthy brothers and the general population of a similar age. Notably, c.868C in the wild-type allele was highly methylated in the patient compared to the same site in both his healthy brothers. These results suggest that the co- deficient expression of POLG and SSBP1 genes could contribute to the development of mtDNA deletion.Entities:
Keywords: POLG; Pearson syndrome; SSBP1; human; mtDNA deletion
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Year: 2021 PMID: 33671400 PMCID: PMC7922481 DOI: 10.3390/genes12020284
Source DB: PubMed Journal: Genes (Basel) ISSN: 2073-4425 Impact factor: 4.096