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. 2023 May 21;19(9):2756–2771. doi: 10.7150/ijbs.83348

Table 2.

Dynamic regulation of mitochondria

Pathways Key genes Mechanisms Roles
Mitochondrial fission DRP1-mediated pathway DRP1, Mff, Fis1, MiD49, MiD51 The recruited DRP1 binds to the protein receptor (Mff, Fis1, MiD49 and MiD51), which breaks the inner and MOM, leading to mitochondrial fission. Splitting of damaged mitochondria into two types of mitochondria with normal and abnormal function.
Mitochondrial fusion MFN1, MFN2 and OPA1-mediated pathways MFN1, MFN2, OPA1 The fusion of the MOM is mainly mediated by MFN1 and MFN2, while the fusion of the MIM is mediated by OPA1. Maintains mitochondrial homeostasis by fusing damaged mitochondria with normal mitochondria to perform relatively normal functions.
Mitophagy PINK1/Parkin pathways PINK1/Parkin PINK1 aggregates at the MOM and recruits and activates Parkin, which in turn activates Parkin to polyubiquitinate a variety of mitochondrial protein substrates. Ultimately, mitophagy is induced by the action of LC3. Mitophagy can wrap and remove damaged mitochondria from the cell through the autophagic pathway, thereby maintaining intracellular mitochondrial homeostasis.
PINK1/Parkin-independent pathways OPTN, NDP52, ULK1, DFCP1, WIPI1, synphilin-1 PINK1 directly recruits OPTN and NDP52 to damaged mitochondria and subsequently recruits and activates ULK1, DFCP1 and WIPI1, which in turn induce mitophagy.
PINK1-synphilin-1 complex induces mitophagy by recruiting SIAH-1 to accelerate the ubiquitination of proteins in damaged mitochondria.
Receptor-mediated pathways Receptors in the MOM NIX/BNIP3L, BNIP3, FUNDC1, NLRX1, FKBP8, Bcl2L13 The receptors located in the MOM all contain a binding site for the LC3 receptor, which can directly bind LC3 to induce mitophagy.
Receptors in the MIM PHB2 and CL Mitochondrial damage leads to the exposure of PHB2, which in turn binds to LC3; moreover, PHB2 induces mitophagy by stabilizing PINK1 and promoting PRKN/Parkin recruitment, protein ubiquitination and OPTN recruitment to mitochondria.
CL transfer from MIM to MOM directly interacts with LC3 to induce mitophagy

DRP1: dynamin-related protein 1; Fis1: mitochondrial fission protein 1; Mff: mitochondrial fission factor; MFN1: mitochondrial fusion protein 1; MFN2: mitochondrial fusion protein 2; MiD49: mitochondrial dynamics protein 49; MiD51: mitochondrial dynamics protein 51; MIM: mitochondrial inner membrane; MOM: mitochondrial outer membrane; OPA1: optic atrophy 1 protein; OPTN: Optineurin; PINK1: PTEN-induced kinase 1; ULK1: unc-51 like kinase 1; WIPI1: WD repeat domain phosphoinositide interacting 1