| Literature DB >> 35437313 |
Xiao-Yan Fan1,2, Lei Guo1, Lei-Ning Chen1, Shen Yin2, Jiarong Wen3, Sen Li1, Jun-Yu Ma1, Tao Jing1, Man-Xi Jiang1, Xiao-Hong Sun1, Meilan Chen1, Feng Wang1,4, Zhen-Bo Wang4, Chang-Fa Zhang1, Xing-Hua Wang2, Zhao-Jia Ge2, Chun Hu3, Lizhang Zeng3, Wei Shen2, Qing-Yuan Sun5,6,7, Xiang-Hong Ou8, Shi-Ming Luo9,10.
Abstract
Mitochondrial replacement therapy (MRT) has been used to prevent maternal transmission of disease-causing mutations in mitochondrial DNA (mtDNA). However, because MRT requires nuclear transfer, it carries the risk of mtDNA carryover and hence of the reversion of mtDNA to pathogenic levels owing to selective replication and genetic drift. Here we show in HeLa cells, mouse embryos and human embryos that mtDNA heteroplasmy can be reduced by pre-labelling the mitochondrial outer membrane of a donor zygote via microinjection with an mRNA coding for a transmembrane peptide fused to an autophagy receptor, to induce the degradation of the labelled mitochondria via forced mitophagy. Forced mitophagy reduced mtDNA carryover in newly reconstructed embryos after MRT, and had negligible effects on the growth curve, reproduction, exercise capacity and other behavioural characteristics of the offspring mice. The induction of forced mitophagy to degrade undesired donor mtDNA may increase the clinical feasibility of MRT and could be extended to other nuclear transfer techniques.Entities:
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Year: 2022 PMID: 35437313 DOI: 10.1038/s41551-022-00881-7
Source DB: PubMed Journal: Nat Biomed Eng ISSN: 2157-846X Impact factor: 29.234