| Literature DB >> 34048705 |
Haifeng Jiao1, Dong Jiang1, Xiaoyu Hu2, Wanqing Du1, Liangliang Ji2, Yuzhuo Yang2, Xiaopeng Li1, Takami Sho1, Xuan Wang1, Ying Li1, Yu-Ting Wu3, Yau-Huei Wei3, Xiaoyu Hu2, Li Yu4.
Abstract
Damaged mitochondria need to be cleared to maintain the quality of the mitochondrial pool. Here, we report mitocytosis, a migrasome-mediated mitochondrial quality-control process. We found that, upon exposure to mild mitochondrial stresses, damaged mitochondria are transported into migrasomes and subsequently disposed of from migrating cells. Mechanistically, mitocytosis requires positioning of damaged mitochondria at the cell periphery, which occurs because damaged mitochondria avoid binding to inward motor proteins. Functionally, mitocytosis plays an important role in maintaining mitochondrial quality. Enhanced mitocytosis protects cells from mitochondrial stressor-induced loss of mitochondrial membrane potential (MMP) and mitochondrial respiration; conversely, blocking mitocytosis causes loss of MMP and mitochondrial respiration under normal conditions. Physiologically, we demonstrate that mitocytosis is required for maintaining MMP and viability in neutrophils in vivo. We propose that mitocytosis is an important mitochondrial quality-control process in migrating cells, which couples mitochondrial homeostasis with cell migration.Entities:
Keywords: migrasome; mitochondrial quality control; mitochondrion; mitocytosis; mitosome
Mesh:
Year: 2021 PMID: 34048705 DOI: 10.1016/j.cell.2021.04.027
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582