Mitophagy (Homo sapiens)

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Bibliography

1. Youle RJ, Narendra DP.; ''Mechanisms of mitophagy.''; PubMed Europe PMC Scholia
2. Sun F, Kanthasamy A, Anantharam V, Kanthasamy AG.; ''Mitochondrial accumulation of polyubiquitinated proteins and differential regulation of apoptosis by polyubiquitination sites Lys-48 and -63.''; PubMed Europe PMC Scholia
3. Tanida I.; ''Autophagosome formation and molecular mechanism of autophagy.''; PubMed Europe PMC Scholia
4. Narendra DP, Youle RJ.; ''Targeting mitochondrial dysfunction: role for PINK1 and Parkin in mitochondrial quality control.''; PubMed Europe PMC Scholia
5. Chen G, Han Z, Feng D, Chen Y, Chen L, Wu H, Huang L, Zhou C, Cai X, Fu C, Duan L, Wang X, Liu L, Liu X, Shen Y, Zhu Y, Chen Q.; ''A regulatory signaling loop comprising the PGAM5 phosphatase and CK2 controls receptor-mediated mitophagy.''; PubMed Europe PMC Scholia
6. Wu W, Tian W, Hu Z, Chen G, Huang L, Li W, Zhang X, Xue P, Zhou C, Liu L, Zhu Y, Zhang X, Li L, Zhang L, Sui S, Zhao B, Feng D.; ''ULK1 translocates to mitochondria and phosphorylates FUNDC1 to regulate mitophagy.''; PubMed Europe PMC Scholia
7. Narendra DP, Jin SM, Tanaka A, Suen DF, Gautier CA, Shen J, Cookson MR, Youle RJ.; ''PINK1 is selectively stabilized on impaired mitochondria to activate Parkin.''; PubMed Europe PMC Scholia
8. Jin SM, Lazarou M, Wang C, Kane LA, Narendra DP, Youle RJ.; ''Mitochondrial membrane potential regulates PINK1 import and proteolytic destabilization by PARL.''; PubMed Europe PMC Scholia
9. Liu L, Feng D, Chen G, Chen M, Zheng Q, Song P, Ma Q, Zhu C, Wang R, Qi W, Huang L, Xue P, Li B, Wang X, Jin H, Wang J, Yang F, Liu P, Zhu Y, Sui S, Chen Q.; ''Mitochondrial outer-membrane protein FUNDC1 mediates hypoxia-induced mitophagy in mammalian cells.''; PubMed Europe PMC Scholia

History

External references

DataNodes

Name	Type	Database reference	Comment
ADP	Metabolite	CHEBI:456216 (ChEBI)
ATG12	Protein	O94817 (Uniprot-TrEMBL)
ATG5	Protein	Q9H1Y0 (Uniprot-TrEMBL)
ATG5:ATG12:LC3:K48polyUB Mitophagy Substrates:SQSTM1	Complex	R-HSA-5205648 (Reactome)
ATG5:ATG12	Complex	R-HSA-5205638 (Reactome)
ATP	Metabolite	CHEBI:30616 (ChEBI)
CSNK2A1	Protein	P68400 (Uniprot-TrEMBL)
CSNK2A2	Protein	P19784 (Uniprot-TrEMBL)
CSNK2B	Protein	P67870 (Uniprot-TrEMBL)
Casein kinase II	Complex	R-HSA-201711 (Reactome)
FUNDC1	Protein	Q8IVP5 (Uniprot-TrEMBL)
K48polyUB Mitophagy Substrates:SQSTM1	Complex	R-HSA-5205659 (Reactome)
K48polyUb-MFN1	Protein	Q8IWA4 (Uniprot-TrEMBL)
K48polyUb-MFN1	Protein	Q8IWA4 (Uniprot-TrEMBL)
K48polyUb-MFN2	Protein	O95140 (Uniprot-TrEMBL)
K48polyUb-MFN2	Protein	O95140 (Uniprot-TrEMBL)
K48polyUb-MTERFD1	Protein	Q96E29 (Uniprot-TrEMBL)
K48polyUb-MTERFD1	Protein	Q96E29 (Uniprot-TrEMBL)
K48polyUb-VDAC1	Protein	P21796 (Uniprot-TrEMBL)
K48polyUb-VDAC1	Protein	P21796 (Uniprot-TrEMBL)
LC3:K48polyUB Mitophagy Substrates:SQSTM1	Complex	R-HSA-5205670 (Reactome)
LC3	Complex	R-HSA-5205658 (Reactome)
MAP1LC3A	Protein	Q9H492 (Uniprot-TrEMBL)
MAP1LC3B	Protein	Q9GZQ8 (Uniprot-TrEMBL)
MFN1	Protein	Q8IWA4 (Uniprot-TrEMBL)
MFN2	Protein	O95140 (Uniprot-TrEMBL)
MTERFD1	Protein	Q96E29 (Uniprot-TrEMBL)
PARK2	Protein	O60260 (Uniprot-TrEMBL)
PARK2:PINK1	Complex	R-HSA-5205683 (Reactome)
PARK2	Protein	O60260 (Uniprot-TrEMBL)
PGAM5-S	Protein	Q96HS1-2 (Uniprot-TrEMBL)
PINK1	Protein	Q9BXM7 (Uniprot-TrEMBL)
PINK1(111-581)	Protein	Q9BXM7 (Uniprot-TrEMBL)
PINK1	Protein	Q9BXM7 (Uniprot-TrEMBL)
RPS27A(1-76)	Protein	P62979 (Uniprot-TrEMBL)
SQSTM1	Protein	Q13501 (Uniprot-TrEMBL)
SQSTM1	Protein	Q13501 (Uniprot-TrEMBL)
SRC-1	Protein	P12931-1 (Uniprot-TrEMBL)
TOMM20	Protein	Q15388 (Uniprot-TrEMBL)
TOMM22	Protein	Q9NS69 (Uniprot-TrEMBL)
TOMM40 Complex	Complex	R-HSA-1252240 (Reactome)
TOMM40	Protein	O96008 (Uniprot-TrEMBL)
TOMM5	Protein	Q8N4H5 (Uniprot-TrEMBL)
TOMM6	Protein	Q96B49 (Uniprot-TrEMBL)
TOMM7	Protein	Q9P0U1 (Uniprot-TrEMBL)
TOMM70A	Protein	O94826 (Uniprot-TrEMBL)
UBA52(1-76)	Protein	P62987 (Uniprot-TrEMBL)
UBB(1-76)	Protein	P0CG47 (Uniprot-TrEMBL)
UBB(153-228)	Protein	P0CG47 (Uniprot-TrEMBL)
UBB(77-152)	Protein	P0CG47 (Uniprot-TrEMBL)
UBC(1-76)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(153-228)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(229-304)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(305-380)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(381-456)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(457-532)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(533-608)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(609-684)	Protein	P0CG48 (Uniprot-TrEMBL)
UBC(77-152)	Protein	P0CG48 (Uniprot-TrEMBL)
ULK1	Protein	O75385 (Uniprot-TrEMBL)
Ub	Complex	R-HSA-113595 (Reactome)
VDAC1	Protein	P21796 (Uniprot-TrEMBL)
p-S13,Y18-FUNDC1	Protein	Q8IVP5 (Uniprot-TrEMBL)
p-S13-FUNDC1	Protein	Q8IVP5 (Uniprot-TrEMBL)
p-S17-FUNDC1	Protein	Q8IVP5 (Uniprot-TrEMBL)
p-S17-FUNDC1:LC3:ATG5:ATG12	Complex	R-HSA-8959570 (Reactome)
p-S17-FUNDC1:LC3	Complex	R-HSA-8959568 (Reactome)
p-S17-FUNDC1	Protein	Q8IVP5 (Uniprot-TrEMBL)

Annotated Interactions

Source	Target	Type	Database reference	Comment
	ADP	Arrow	R-HSA-8948039 (Reactome)
	ADP	Arrow	R-HSA-8948143 (Reactome)
	ADP	Arrow	R-HSA-8948146 (Reactome)
	ATG5:ATG12:LC3:K48polyUB Mitophagy Substrates:SQSTM1	Arrow	R-HSA-5205663 (Reactome)
ATG5:ATG12			R-HSA-5205663 (Reactome)
ATG5:ATG12			R-HSA-8959571 (Reactome)
ATP			R-HSA-8948039 (Reactome)
ATP			R-HSA-8948143 (Reactome)
ATP			R-HSA-8948146 (Reactome)
Casein kinase II		mim-catalysis	R-HSA-8948039 (Reactome)
	FUNDC1	Arrow	R-HSA-8948139 (Reactome)
FUNDC1			R-HSA-8948039 (Reactome)
FUNDC1			R-HSA-8948146 (Reactome)
	K48polyUB Mitophagy Substrates:SQSTM1	Arrow	R-HSA-5205673 (Reactome)
K48polyUB Mitophagy Substrates:SQSTM1			R-HSA-5205649 (Reactome)
	K48polyUb-MFN1	Arrow	R-HSA-5205682 (Reactome)
K48polyUb-MFN1			R-HSA-5205673 (Reactome)
	K48polyUb-MFN2	Arrow	R-HSA-5205682 (Reactome)
K48polyUb-MFN2			R-HSA-5205673 (Reactome)
	K48polyUb-MTERFD1	Arrow	R-HSA-5205682 (Reactome)
K48polyUb-MTERFD1			R-HSA-5205673 (Reactome)
	K48polyUb-VDAC1	Arrow	R-HSA-5205682 (Reactome)
K48polyUb-VDAC1			R-HSA-5205673 (Reactome)
	LC3:K48polyUB Mitophagy Substrates:SQSTM1	Arrow	R-HSA-5205649 (Reactome)
LC3:K48polyUB Mitophagy Substrates:SQSTM1			R-HSA-5205663 (Reactome)
LC3			R-HSA-5205649 (Reactome)
LC3			R-HSA-8959573 (Reactome)
MFN1			R-HSA-5205682 (Reactome)
MFN2			R-HSA-5205682 (Reactome)
MTERFD1			R-HSA-5205682 (Reactome)
	PARK2:PINK1	Arrow	R-HSA-5205652 (Reactome)
PARK2:PINK1		mim-catalysis	R-HSA-5205682 (Reactome)
PARK2			R-HSA-5205652 (Reactome)
PGAM5-S		mim-catalysis	R-HSA-8948139 (Reactome)
	PINK1(111-581)	Arrow	R-HSA-5205681 (Reactome)
	PINK1	Arrow	R-HSA-5205661 (Reactome)
	PINK1	Arrow	R-HSA-5205672 (Reactome)
PINK1			R-HSA-5205652 (Reactome)
PINK1			R-HSA-5205661 (Reactome)
PINK1			R-HSA-5205672 (Reactome)
PINK1			R-HSA-5205681 (Reactome)
			R-HSA-5205649 (Reactome)	p62 links to the microtubule-associated protein Autophagy marker Light Chain 3 (LC3). This begins the recruitment of the autophagy machinery to the damaged mitochondria, targeting it for autophagic degradation.
			R-HSA-5205652 (Reactome)	Parkin promotes the ubiquitination of outer mitochondrial membrane emedded proteins including the mitofusin mitochondrial assembly regulatory factor (MARF), mitofusin 1, mitofusin 2 and voltage dependent anion selective channel protein 1 (vDAC1).
			R-HSA-5205661 (Reactome)	PINK1 is constitutively synthesized and imported into all mitochondria. In healthy mitochondria PINK1 is cleaved by voltage-sensitive proteolysis.
			R-HSA-5205663 (Reactome)	The mitochondria are engulfed after elongation of the isolation membrane. Once the autophagosome is formed, its outer membrane fuses with lysosomes to form the autolysosome. The lysosomal hydrolases (cathepsins and lipases) ultimately degrade the damaged mitochondria and its associated proteins.
			R-HSA-5205672 (Reactome)	On damaged mitochondria that have lost their membrane potential, however, PINK1 cleavage is inhibited, leading to high PINK1 protein accumulation on the inner leaf of the OMM of dysfunctional mitochondria. Full-length mitochondrial PINK1 is the active form in the PINK1/Parkin pathway.
			R-HSA-5205673 (Reactome)	After the ubiquitination events, p62 is recruited to mitochondria, binding the Parkin-ubiquitinated substrates
			R-HSA-5205681 (Reactome)	Full-length PINK1 (63 kDa), which is in the inner mitochondrial space, is proteolytically cleaved into an 52-kDa cytosolic fragment (111 - 581) that is released back into the cytoplasm by an unknown mechanism and degraded by the proteasome. cleavage of PINK1 into an unstable cytosolic form maintains low levels of PINK1 on healthy mitochondria in order to suppress the PINK1/Parkin pathway in the absence of mitochondrial damage. At present, not all of the proteases mediating the cleavage of PINK1 in mammalian cells have been identified.
			R-HSA-5205682 (Reactome)	Parkin promotes the ubiquitination of the mitofusin mitochondrial assembly regulatory factor (MARF), mitofusin 1, mitofusin 2 and voltage-dependent anion-selective channel protein 1 (vDAC1), all of which are embedded in the OMM.
			R-HSA-8948039 (Reactome)	FUNDC1-mediated mitophagy is inhibited by its phosphorylation at the Serine 13 positions in the LIR motif by CK2kinase under normoxia conditions. These phosphorylation events insure that FUNDC1 cannot bind LC3.
			R-HSA-8948136 (Reactome)	ULK1 is critical for the induction of autophagy, translocating to fragmented mitochondria upon mitophagy induction by either hypoxia or mitochondrial uncouplers. At mitochondria, ULK1 interacts with FUNDC1.
			R-HSA-8948139 (Reactome)	Mitochondria are selectively removed by interactions between LC3 and the FUNDC1 mitophagy receptor which harbors an LC3-interacting region (LIR). When mitochondrial stresses are sensed mitochondrially localized PGAM5 phosphatase interacts with and dephosphorylates FUNDC1 at serine 13 (Ser-13) upon hypoxia.
			R-HSA-8948143 (Reactome)	FUNDC1-mediated mitophagy is inhibited by its phosphorylation at the Tyr 18 position in the LIR motif by Src kinase under normoxia conditions. These phosphorylation events insure that FUNDC1 cannot bind LC3.
			R-HSA-8948146 (Reactome)	At mitochondria, ULK1 interacts with FUNDC1, phosphorylating it at serine 17, which enhances FUNDC1 binding to LC3. FUNDC1 regulates ULK1 recruitment to damaged mitochondria; FUNDC1 phosphorylation by ULK1 is crucial for mitophagy.
			R-HSA-8959571 (Reactome)	The mitochondria are engulfed after elongation of the isolation membrane. Once the autophagosome is formed, its outer membrane fuses with lysosomes to form the autolysosome. The lysosomal hydrolases (cathepsins and lipases) ultimately degrade the damaged mitochondria and its associated proteins.
			R-HSA-8959573 (Reactome)	s17 Phosphorylated FUNDC1 links to the microtubule-associated protein Autophagy marker Light Chain 3 (LC3). This begins the recruitment of the autophagy machinery to the damaged mitochondria, targeting it for autophagic degradation.
SQSTM1			R-HSA-5205673 (Reactome)
SRC-1		mim-catalysis	R-HSA-8948143 (Reactome)
TOMM40 Complex		mim-catalysis	R-HSA-5205661 (Reactome)
	ULK1	Arrow	R-HSA-8948136 (Reactome)
ULK1			R-HSA-8948136 (Reactome)
ULK1		mim-catalysis	R-HSA-8948146 (Reactome)
Ub			R-HSA-5205682 (Reactome)
VDAC1			R-HSA-5205682 (Reactome)
	p-S13,Y18-FUNDC1	Arrow	R-HSA-8948143 (Reactome)
	p-S13-FUNDC1	Arrow	R-HSA-8948039 (Reactome)
p-S13-FUNDC1			R-HSA-8948139 (Reactome)
p-S13-FUNDC1			R-HSA-8948143 (Reactome)
	p-S17-FUNDC1:LC3:ATG5:ATG12	Arrow	R-HSA-8959571 (Reactome)
	p-S17-FUNDC1:LC3	Arrow	R-HSA-8959573 (Reactome)
p-S17-FUNDC1:LC3			R-HSA-8959571 (Reactome)
	p-S17-FUNDC1	Arrow	R-HSA-8948146 (Reactome)
p-S17-FUNDC1			R-HSA-8959573 (Reactome)