p75 NTR receptor-mediated signaling (Homo sapiens)

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13, 31, 402039374628163537242023, 47423371847302020, 32, 3462112, 4129, 47271044717, 41, 481929181, 315, 36205, 11241nucleoplasmcytosolendosomeRELA p-S32,S36-NFKBIA UBA52(1-76) UBC(533-608) RELA TRAF6ADPNGFRGTP NFKBIA NGFligand:p75NTR:NRAGE:CHE1NGFRAP1UBB(77-152) NGFR(273-427)RPS27A(1-76) NGFR NGFR:RTN4R:LINGO1UBC(1-76) NGFR:RTN4R:LINGO1:RTN4,MAG,OMGSOS1 ARHGEF40 GDP GDPUBB(1-76) TIAM2 PSEN1(1-298) SQSTM1 UBC(229-304) MAPK8PSEN2(298-448) ADPIKBKB UBC(381-456) ADPGDP NFKB1(1-433):RELAp-S,T-IRAK1-1 MCF2ARHGEF38 NF-kB:p75NTRICD:TRAF6ARHGEF12 IRAK1:MYD88VAV1 ATPUBC(153-228) IRAK1 RAC1:GTPNGFRAP1 NGFR UBC(533-608) ARHGDIA LINGO1LINGO1 NGF:p75NTR:PRDM4NGFR NGF ECT2 UBA52(1-76) NGFR RPS27A(1-76) PRDM4:HistonedeacetylaseNGF ITGB3BP UBB(77-152) NGFR:RTN4RUBB(153-228) RELA CASP2(2-452) ATPUBC(77-152) MAG SORCS3(?-?) p-S177,S181-IKBKB NGF:p75NTR:NADEMYD88 NGFR UBC(533-608) p-T,Y-MAPK8Ubiquitinatedphospho-IkBUBC(305-380) ARHGDIA ARHGEF33 GDP SPHMNGF NGFligand:p75NTR:p-IRAK1:MYD88UBC(457-532) NGF ITSN1 UBC(609-684) SOS2 ADPTRAF6 homotrimerMYD88 UBC(229-304) NGF HDAC1 UBB(153-228) UBC(305-380) NFKB1(1-433) UBB(153-228) LINGO1 UBC(77-152) RELA UBC(305-380) PSEN1(299-467) BADUBC(229-304) UBB(153-228) UBC(609-684) UBB(77-152) UBB(1-76) MAGED1 UBB(77-152) NGFligand:p75NTR:NRIF:TRAF6RHOA NGF mature NGFhomodimer:p75NTRUBC(1-76) RPS27A(1-76) BCL2L11NGF(19-241) NGFRRHOA PRDM4 RASGRF2 APH1A CASP2(348-452) Active Caspases 2, 3RELA SQSTM1 TRAF6 NGF UBC(609-684) NGF SQSTM1NGEF SQSTM1OMG MAPK8PLEKHG2 FGD1 ADPHDAC3 ITGB3BP UBC(381-456) Zn2+ UBC(229-304) mature NGFhomodimer:p75NTRRTN4,MAG,OMGMAG UBC(153-228) ATPmature beta-NGFhomodimerNGF UBC(457-532) RIPK2 RTN4 GDP HDAC3 UBC(229-304) UBC(381-456) NFKB1(1-433) ARHGDIA RHOA ARHGEF37 SQSTM1 NGF ADPNGFR(29-250)UBB(1-76) p-S,T-IRAK1 Histone deacetylaseTRAF6 ITGB3BPUBC(229-304) p-S32,S36-NFKBIARHOA p-S,T-IRAK1 UBC(77-152) ARHGEF1 NGFR MAGED1 NGF NGFR PSEN1(1-298) UBC(153-228) UBC(305-380) NGFR NCSTN APH1A AATFpro-betaNGF:p75NTR:sortilinNGFligand:p75NTR:Phospho-IRAK1:TRAF6GDP APH1B NGFligand:p75NTR:Phospho-IRAK1:TRAF6:p62p-T,Y-MAPK8p-S,T-IRAK1 UBC(77-152) ARHGEF7 p75NTR:sortilincomplexUBC(609-684) PRKCIRIPK2p-T,Y-MAPK8NGFR Ubiquitinated NRIFNGFR NGFR UBC(457-532) K63polyUb-TRAF6 UBB(77-152) NGF NGFR p-S,T-ADAM17(215-827):Zn2+NGFligand:p75NTR:NADE:14-3-3epsilonUBC(609-684) UBC(609-684) ARHGEF2 RTN4R multimerARHGEF18 NGFR(251-427)ChoPUBC(1-76) RTN4R multimer GGC-PalmC-RAC1 KALRN NGF(19-241) RTN4 NGF:p75NTR:RIP2AKAP13 p-S,T-IRAK1 p-S,T-IRAK1 RHOA:GTPNGF MYD88 unknown kinaseUBC(1-76) APH1B NGFR UBC(153-228) TRAF6 p-S128-BADUBC(1-76) MAG TRAF6 UBB(1-76) TIAM1 SMPD2VAV3 ARHGDIA CASP3(176-277) NGF NGFRAP1 SQSTM1 NGFR NET1 RHOA GDP UBA52(1-76) p-S,T-IRAK1 NGFR PRDM4FGD2 UBC(1-76) ATPUBA52(1-76) OMG pro-beta-NGFhomodimerp-S65-BCL2L11IRAK1 NGFR SMPD2 NGF processingMAGED1SQSTM1 ARHGDIA:NGFR:RTN4R:LINGO1:RTN4,MAG,OMGATPCASP3(1-277) UBB(153-228) ABR UbTRAF6 N-acylsphingosineSORCS3(?-?) NGFR RPS27A(1-76) ARHGDIA MCF2L GTPRPS27A(1-76) ITGB3BP AATF HDAC2 FGD4 PRKCI PSEN1(299-467) ARHGEF3 OMG UBA52(1-76) NFKB1(1-433):RELARTN4R multimer TRAF6 UBB(1-76) HDAC2 UBC(153-228) RHOA UBC(305-380) RPS27A(1-76) ARHGEF9 MYD88 OMG NFKB1(1-433) YWHAE dimerPLEKHG5 UbITGB3BP RTN4 UBC(457-532) NGFligand:p75NTR:Phospho-IRAK1:polyubiquitinated TRAF6:p62Mg2+ NGFligand:p75NTR:Phospho-IRAK1:TRAF6:p62:IKK-betaRTN4R multimer NGFR UBC(305-380) RHOA:GDP:ARHGDIA:NGFR:NGFMCF2 ADPgamma-secretasecomplexActive N-SMase:Mg2+ARHGEF19 Mg2+RTN4R multimer PRDM4PSENEN CASP3(29-175) NGFligand:p75NTR:NRIFNGFR SQSTM1 p-S,T-IRAK1 YWHAE NGFR RHOA:GDP:ARHGDIA:NGFR:RTN4R:LINGO1:RTN4,MAG,OMGUBC(457-532) GTP NGF NGFRYWHAE GTP Zn2+ NGFligand:p75NTR:Phospho-IRAK1:MYD88:TRAF6UBC(457-532) ARHGEF6 UBA52(1-76) UBB(77-152) NFKB1(1-433):RELAVAV2 RHOA:GDPProcaspases 2, 3gamma-secretasecomplexNGFR ARHGEF5 LINGO1 RAC1:GDPTRAF6ITGB3BP RHOA:GDP:ARHGDIA:NGFRRTN4 PSENEN UBC(229-304) IKBKB NGFR(273-427)HDAC1 NGF TRAF6 ADAM17(215-827) ARHGEF4 UBC(381-456) PREX1 LINGO1 TRAF6 H2OMAG UBC(153-228) NGF UBC(381-456) PSEN2(1-297) MYD88 UbiquitinatedNRIF:SequestosomeRPS27A(1-76) UBC(533-608) NGFR NGF UBC(609-684) GEFsNGF NGFR NCSTN NGFR UBB(77-152) NGFR TRAF6 UBB(153-228) UBC(77-152) NGFR UbiquitinatedNRIF:SequestosomeOBSCN ARHGEF35 NGFR RHOA:GDP:ARHGDIAFGD3 NFKB1(1-433) UBA52(1-76) ARHGEF10L ARHGEF26 NGFligand:p75NTR:Phospho-IRAK1:TRAF6:p62:aPKCiPSEN2(1-297) RTN4R multimer CASP2(170-325) NGF p-T,Y-MAPK8IKBKB dimerATPARHGEF10 NFKB1(1-433) TRIO UBC(305-380) NGF:p75NTR:NRAGESignaling by NTRK1(TRKA)UBC(381-456) UBC(77-152) UBC(533-608) SQSTM1 UBC(533-608) UBC(457-532) ARHGEF17 K63 linkedpolyubiquitin chainNGFR(251-272)NGFR UBC(77-152) ATPUBC(1-76) GNA13 PRDM4 MYD88 dimerGGC-PalmC-RAC1 PSEN2(298-448) NGFR(251-427)NGFligand:p75NTR:Phospho-IRAK1:TRAF6:p62:Phospho-IKK-betaUBB(153-228) ARHGEF16 MAPK8mature NGFhomodimer:p75NTRUBB(1-76) UBC(381-456) NGF UBB(1-76) ARHGEF39 UBC(533-608) NGFR(273-427) NGFR NGFligand:p75NTR:IRAK1:MYD88ARHGEF11 UBC(153-228) NGF IkB(alpha):NF-kBcomplexARHGEF15 8, 382222449, 14, 25, 438, 382645268


Description

Besides signalling through the tyrosine kinase receptors TRK A, B, and C, the mature neurotrophins NGF, BDNF, and NT3/4 signal through their common receptor p75NTR. NGF binding to p75NTR activates a number of downstream signalling events controlling survival, death, proliferation, and axonogenesis, according to the cellular context. p75NTR is devoid of enzymatic activity, and signals by recruiting other proteins to its own intracellular domain. p75 interacting proteins include NRIF, TRAF2, 4, and 6, NRAGE, necdin, SC1, NADE, RhoA, Rac, ARMS, RIP2, FAP and PLAIDD. Here we annotate only the proteins for which a clear involvement in p75NTR signalling was demonstrated.
A peculiarity of p75NTR is the ability to bind the pro-neurotrophins proNGF and proBDNF. Proneurotrophins do not associate with TRK receptors, whereas they efficiently signal cell death by apoptosis through p75NTR. The biological action of neurotrophins is thus regulated by proteolytic cleavage, with proforms preferentially activating p75NTR, mediating apoptosis, and mature forms activating TRK receptors, to promote survival. Moreover, the two receptors are utilised to differentially modulate neuronal plasticity. For instance, proBDNF-p75NTR signalling facilitates LTD, long term depression, in the hippocampus (Woo NH, et al, 2005), while BDNF-TRKB signalling promotes LTP (long term potentiation). Many biological observations indicate a functional interaction between p75NTR and TRKA signaling pathways.
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Comments

Reactome-Converter 
Pathway is converted from Reactome ID: 193704
Reactome-version 
Reactome version: 73
Reactome Author 
Reactome Author: Nasi, Sergio, Annibali, D

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Bibliography

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History

View all...
CompareRevisionActionTimeUserComment
116430view09:28, 7 May 2021EweitzModified title
115014view16:55, 25 January 2021ReactomeTeamReactome version 75
113459view11:53, 2 November 2020ReactomeTeamReactome version 74
112658view16:04, 9 October 2020ReactomeTeamReactome version 73
102024view16:11, 26 November 2018Marvin M2Ontology Term : 'PW:0000003' removed !
102023view16:11, 26 November 2018Marvin M2Ontology Term : 'nerve growth factor signaling pathway' added !
101688view14:08, 1 November 2018DeSlOntology Term : 'signaling pathway' added !
101574view11:44, 1 November 2018ReactomeTeamreactome version 66
101110view21:27, 31 October 2018ReactomeTeamreactome version 65
100731view20:12, 31 October 2018ReactomeTeamNew pathway

External references

DataNodes

View all...
NameTypeDatabase referenceComment
AATF ProteinQ9NY61 (Uniprot-TrEMBL)
AATFProteinQ9NY61 (Uniprot-TrEMBL)
ABR ProteinQ12979 (Uniprot-TrEMBL)
ADAM17(215-827) ProteinP78536 (Uniprot-TrEMBL)
ADPMetaboliteCHEBI:456216 (ChEBI)
AKAP13 ProteinQ12802 (Uniprot-TrEMBL)
APH1A ProteinQ96BI3 (Uniprot-TrEMBL)
APH1B ProteinQ8WW43 (Uniprot-TrEMBL)
ARHGDIA ProteinP52565 (Uniprot-TrEMBL)
ARHGDIA:NGFR:RTN4R:LINGO1:RTN4,MAG,OMGComplexR-HSA-194528 (Reactome)
ARHGEF1 ProteinQ92888 (Uniprot-TrEMBL)
ARHGEF10 ProteinO15013 (Uniprot-TrEMBL)
ARHGEF10L ProteinQ9HCE6 (Uniprot-TrEMBL)
ARHGEF11 ProteinO15085 (Uniprot-TrEMBL)
ARHGEF12 ProteinQ9NZN5 (Uniprot-TrEMBL)
ARHGEF15 ProteinO94989 (Uniprot-TrEMBL)
ARHGEF16 ProteinQ5VV41 (Uniprot-TrEMBL)
ARHGEF17 ProteinQ96PE2 (Uniprot-TrEMBL)
ARHGEF18 ProteinQ6ZSZ5 (Uniprot-TrEMBL)
ARHGEF19 ProteinQ8IW93 (Uniprot-TrEMBL)
ARHGEF2 ProteinQ92974 (Uniprot-TrEMBL)
ARHGEF26 ProteinQ96DR7 (Uniprot-TrEMBL)
ARHGEF3 ProteinQ9NR81 (Uniprot-TrEMBL)
ARHGEF33 ProteinA8MVX0 (Uniprot-TrEMBL)
ARHGEF35 ProteinA5YM69 (Uniprot-TrEMBL)
ARHGEF37 ProteinA1IGU5 (Uniprot-TrEMBL)
ARHGEF38 ProteinQ9NXL2 (Uniprot-TrEMBL)
ARHGEF39 ProteinQ8N4T4 (Uniprot-TrEMBL)
ARHGEF4 ProteinQ9NR80 (Uniprot-TrEMBL)
ARHGEF40 ProteinQ8TER5 (Uniprot-TrEMBL)
ARHGEF5 ProteinQ12774 (Uniprot-TrEMBL)
ARHGEF6 ProteinQ15052 (Uniprot-TrEMBL)
ARHGEF7 ProteinQ14155 (Uniprot-TrEMBL)
ARHGEF9 ProteinO43307 (Uniprot-TrEMBL)
ATPMetaboliteCHEBI:30616 (ChEBI)
Active Caspases 2, 3ComplexR-HSA-205013 (Reactome)
Active N-SMase:Mg2+ComplexR-HSA-194354 (Reactome)
BADProteinQ92934 (Uniprot-TrEMBL)
BCL2L11ProteinO43521 (Uniprot-TrEMBL)
CASP2(170-325) ProteinP42575 (Uniprot-TrEMBL)
CASP2(2-452) ProteinP42575 (Uniprot-TrEMBL)
CASP2(348-452) ProteinP42575 (Uniprot-TrEMBL)
CASP3(1-277) ProteinP42574 (Uniprot-TrEMBL)
CASP3(176-277) ProteinP42574 (Uniprot-TrEMBL)
CASP3(29-175) ProteinP42574 (Uniprot-TrEMBL)
ChoPMetaboliteCHEBI:18132 (ChEBI)
ECT2 ProteinQ9H8V3 (Uniprot-TrEMBL)
FGD1 ProteinP98174 (Uniprot-TrEMBL)
FGD2 ProteinQ7Z6J4 (Uniprot-TrEMBL)
FGD3 ProteinQ5JSP0 (Uniprot-TrEMBL)
FGD4 ProteinQ96M96 (Uniprot-TrEMBL)
GDP MetaboliteCHEBI:17552 (ChEBI)
GDPMetaboliteCHEBI:17552 (ChEBI)
GEFsComplexR-HSA-194849 (Reactome)
GGC-PalmC-RAC1 ProteinP63000 (Uniprot-TrEMBL)
GNA13 ProteinQ14344 (Uniprot-TrEMBL)
GTP MetaboliteCHEBI:15996 (ChEBI)
GTPMetaboliteCHEBI:15996 (ChEBI)
H2OMetaboliteCHEBI:15377 (ChEBI)
HDAC1 ProteinQ13547 (Uniprot-TrEMBL)
HDAC2 ProteinQ92769 (Uniprot-TrEMBL)
HDAC3 ProteinO15379 (Uniprot-TrEMBL)
Histone deacetylaseComplexR-HSA-205005 (Reactome)
IKBKB ProteinO14920 (Uniprot-TrEMBL)
IKBKB dimerComplexR-HSA-193897 (Reactome)
IRAK1 ProteinP51617 (Uniprot-TrEMBL)
IRAK1:MYD88ComplexR-HSA-193874 (Reactome)
ITGB3BP ProteinQ13352 (Uniprot-TrEMBL)
ITGB3BPProteinQ13352 (Uniprot-TrEMBL)
ITSN1 ProteinQ15811 (Uniprot-TrEMBL)
IkB(alpha):NF-kB complexComplexR-HSA-193938 (Reactome)
K63 linked polyubiquitin chainComplexR-HSA-204940 (Reactome)
K63polyUb-TRAF6 ProteinQ9Y4K3 (Uniprot-TrEMBL)
KALRN ProteinO60229 (Uniprot-TrEMBL)
LINGO1 ProteinQ96FE5 (Uniprot-TrEMBL)
LINGO1ProteinQ96FE5 (Uniprot-TrEMBL)
MAG ProteinP20916 (Uniprot-TrEMBL)
MAGED1 ProteinQ9Y5V3 (Uniprot-TrEMBL)
MAGED1ProteinQ9Y5V3 (Uniprot-TrEMBL)
MAPK8ProteinP45983 (Uniprot-TrEMBL)
MCF2 ProteinP10911 (Uniprot-TrEMBL)
MCF2L ProteinO15068 (Uniprot-TrEMBL)
MCF2ProteinP10911 (Uniprot-TrEMBL)
MYD88 ProteinQ99836 (Uniprot-TrEMBL)
MYD88 dimerComplexR-HSA-193932 (Reactome)
Mg2+ MetaboliteCHEBI:18420 (ChEBI)
Mg2+MetaboliteCHEBI:18420 (ChEBI)
N-acylsphingosineMetaboliteCHEBI:52639 (ChEBI)
NCSTN ProteinQ92542 (Uniprot-TrEMBL)
NET1 ProteinQ7Z628 (Uniprot-TrEMBL)
NF-kB:p75NTR ICD:TRAF6ComplexR-HSA-197481 (Reactome)
NFKB1(1-433) ProteinP19838 (Uniprot-TrEMBL)
NFKB1(1-433):RELAComplexR-HSA-194043 (Reactome)
NFKB1(1-433):RELAComplexR-HSA-194047 (Reactome)
NFKBIA ProteinP25963 (Uniprot-TrEMBL)
NGEF ProteinQ8N5V2 (Uniprot-TrEMBL)
NGF ligand:p75NTR:IRAK1:MYD88ComplexR-HSA-209570 (Reactome)
NGF ligand:p75NTR:NADE:14-3-3epsilonComplexR-HSA-205018 (Reactome)
NGF ligand:p75NTR:NRAGE:CHE1ComplexR-HSA-205048 (Reactome)
NGF ligand:p75NTR:NRIF:TRAF6ComplexR-HSA-204977 (Reactome)
NGF ligand:p75NTR:NRIFComplexR-HSA-205100 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:MYD88:TRAF6ComplexR-HSA-209574 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:IKK-betaComplexR-HSA-209533 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:Phospho-IKK-betaComplexR-HSA-209565 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:aPKCiComplexR-HSA-209558 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62ComplexR-HSA-209577 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6ComplexR-HSA-209569 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:polyubiquitinated TRAF6:p62ComplexR-HSA-209542 (Reactome)
NGF ligand:p75NTR:p-IRAK1:MYD88ComplexR-HSA-209572 (Reactome)
NGF ProteinP01138 (Uniprot-TrEMBL)
NGF processingPathwayR-HSA-167060 (Reactome) All neurotrophins (NTs) are generated as pre-pro-neurotrophin precursors. The signal peptide is cleaved off as NT is associated with the endoplasmic reticulum (ER). The resulting pro-NT can form a homodimer spontaneously which then transits to the Golgi apparatus and then onto the trans-Golgi network (TGN). Resident protein convertases (PCs) can cleave off the pro-sequence and mature NT is is targeted to constitutively released vesicles. The pro-NT form can also be released to the extracellular region.
NGF(19-241) ProteinP01138 (Uniprot-TrEMBL)
NGF:p75NTR:NADEComplexR-HSA-204978 (Reactome)
NGF:p75NTR:NRAGEComplexR-HSA-205059 (Reactome)
NGF:p75NTR:PRDM4ComplexR-HSA-204972 (Reactome)
NGF:p75NTR:RIP2ComplexR-HSA-209578 (Reactome)
NGFR ProteinP08138 (Uniprot-TrEMBL)
NGFR(251-272)ProteinP08138 (Uniprot-TrEMBL)
NGFR(251-427)ProteinP08138 (Uniprot-TrEMBL)
NGFR(273-427) ProteinP08138 (Uniprot-TrEMBL)
NGFR(273-427)ProteinP08138 (Uniprot-TrEMBL)
NGFR(29-250)ProteinP08138 (Uniprot-TrEMBL)
NGFR:RTN4R:LINGO1:RTN4,MAG,OMGComplexR-HSA-194499 (Reactome)
NGFR:RTN4R:LINGO1ComplexR-HSA-194583 (Reactome)
NGFR:RTN4RComplexR-HSA-194513 (Reactome)
NGFRAP1 ProteinQ00994 (Uniprot-TrEMBL)
NGFRAP1ProteinQ00994 (Uniprot-TrEMBL)
NGFRProteinP08138 (Uniprot-TrEMBL)
OBSCN ProteinQ5VST9 (Uniprot-TrEMBL)
OMG ProteinP23515 (Uniprot-TrEMBL)
PLEKHG2 ProteinQ9H7P9 (Uniprot-TrEMBL)
PLEKHG5 ProteinO94827 (Uniprot-TrEMBL)
PRDM4 ProteinQ9UKN5 (Uniprot-TrEMBL)
PRDM4:Histone deacetylaseComplexR-HSA-205111 (Reactome)
PRDM4ProteinQ9UKN5 (Uniprot-TrEMBL)
PREX1 ProteinQ8TCU6 (Uniprot-TrEMBL)
PRKCI ProteinP41743 (Uniprot-TrEMBL)
PRKCIProteinP41743 (Uniprot-TrEMBL)
PSEN1(1-298) ProteinP49768 (Uniprot-TrEMBL)
PSEN1(299-467) ProteinP49768 (Uniprot-TrEMBL)
PSEN2(1-297) ProteinP49810 (Uniprot-TrEMBL)
PSEN2(298-448) ProteinP49810 (Uniprot-TrEMBL)
PSENEN ProteinQ9NZ42 (Uniprot-TrEMBL)
Procaspases 2, 3ComplexR-HSA-204948 (Reactome)
RAC1:GDPComplexR-HSA-217287 (Reactome)
RAC1:GTPComplexR-HSA-217289 (Reactome)
RASGRF2 ProteinO14827 (Uniprot-TrEMBL)
RELA ProteinQ04206 (Uniprot-TrEMBL)
RHOA ProteinP61586 (Uniprot-TrEMBL)
RHOA:GDP:ARHGDIA:NGFR:NGFComplexR-HSA-194506 (Reactome)
RHOA:GDP:ARHGDIA:NGFR:RTN4R:LINGO1:RTN4,MAG,OMGComplexR-HSA-194481 (Reactome)
RHOA:GDP:ARHGDIA:NGFRComplexR-HSA-194466 (Reactome)
RHOA:GDP:ARHGDIAComplexR-HSA-194533 (Reactome)
RHOA:GDPComplexR-HSA-8964174 (Reactome)
RHOA:GTPComplexR-HSA-5665993 (Reactome)
RIPK2 ProteinO43353 (Uniprot-TrEMBL)
RIPK2ProteinO43353 (Uniprot-TrEMBL)
RPS27A(1-76) ProteinP62979 (Uniprot-TrEMBL)
RTN4 ProteinQ9NQC3 (Uniprot-TrEMBL)
RTN4,MAG,OMGComplexR-HSA-194580 (Reactome)
RTN4R multimer R-HSA-194455 (Reactome)
RTN4R multimerR-HSA-194455 (Reactome)
SMPD2 ProteinO60906 (Uniprot-TrEMBL)
SMPD2ProteinO60906 (Uniprot-TrEMBL)
SORCS3(?-?) ProteinQ17R88 (Uniprot-TrEMBL)
SOS1 ProteinQ07889 (Uniprot-TrEMBL)
SOS2 ProteinQ07890 (Uniprot-TrEMBL)
SPHMMetaboliteCHEBI:17636 (ChEBI)
SQSTM1 ProteinQ13501 (Uniprot-TrEMBL)
SQSTM1ProteinQ13501 (Uniprot-TrEMBL)
Signaling by NTRK1 (TRKA)PathwayR-HSA-187037 (Reactome) Trk receptors signal from the plasma membrane and from intracellular membranes, particularly from early endosomes. Signalling from the plasma membrane is fast but transient; signalling from endosomes is slower but long lasting. Signalling from the plasma membrane is annotated here. TRK signalling leads to proliferation in some cell types and neuronal differentiation in others. Proliferation is the likely outcome of short term signalling, as observed following stimulation of EGFR (EGF receptor). Long term signalling via TRK receptors, instead, was clearly shown to be required for neuronal differentiation in response to neurotrophins.
TIAM1 ProteinQ13009 (Uniprot-TrEMBL)
TIAM2 ProteinQ8IVF5 (Uniprot-TrEMBL)
TRAF6 ProteinQ9Y4K3 (Uniprot-TrEMBL)
TRAF6 homotrimerComplexR-HSA-421373 (Reactome)
TRAF6ProteinQ9Y4K3 (Uniprot-TrEMBL)
TRIO ProteinO75962 (Uniprot-TrEMBL)
UBA52(1-76) ProteinP62987 (Uniprot-TrEMBL)
UBB(1-76) ProteinP0CG47 (Uniprot-TrEMBL)
UBB(153-228) ProteinP0CG47 (Uniprot-TrEMBL)
UBB(77-152) ProteinP0CG47 (Uniprot-TrEMBL)
UBC(1-76) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(153-228) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(229-304) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(305-380) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(381-456) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(457-532) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(533-608) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(609-684) ProteinP0CG48 (Uniprot-TrEMBL)
UBC(77-152) ProteinP0CG48 (Uniprot-TrEMBL)
UbComplexR-HSA-113595 (Reactome)
Ubiquitinated NRIF:SequestosomeComplexR-HSA-205035 (Reactome)
Ubiquitinated NRIF:SequestosomeComplexR-HSA-210946 (Reactome)
Ubiquitinated phospho-IkBComplexR-HSA-209535 (Reactome)
Ubiquitinated NRIFComplexR-HSA-204965 (Reactome)
VAV1 ProteinP15498 (Uniprot-TrEMBL)
VAV2 ProteinP52735 (Uniprot-TrEMBL)
VAV3 ProteinQ9UKW4 (Uniprot-TrEMBL)
YWHAE ProteinP62258 (Uniprot-TrEMBL)
YWHAE dimerComplexR-HSA-194364 (Reactome)
Zn2+ MetaboliteCHEBI:29105 (ChEBI)
gamma-secretase complexComplexR-HSA-157343 (Reactome)
mature NGF homodimer:p75NTRComplexR-HSA-205123 (Reactome)
mature beta-NGF homodimerComplexR-HSA-187031 (Reactome)
p-S,T-ADAM17(215-827):Zn2+ComplexR-HSA-9662806 (Reactome)
p-S,T-IRAK1 ProteinP51617 (Uniprot-TrEMBL)
p-S,T-IRAK1-1 ProteinP51617-1 (Uniprot-TrEMBL)
p-S128-BADProteinQ92934 (Uniprot-TrEMBL)
p-S177,S181-IKBKB ProteinO14920 (Uniprot-TrEMBL)
p-S32,S36-NFKBIA ProteinP25963 (Uniprot-TrEMBL)
p-S32,S36-NFKBIAProteinP25963 (Uniprot-TrEMBL)
p-S65-BCL2L11ProteinO43521 (Uniprot-TrEMBL)
p-T,Y-MAPK8ProteinP45983 (Uniprot-TrEMBL)
p75NTR:sortilin complexComplexR-HSA-193698 (Reactome)
pro-beta NGF:p75NTR:sortilinComplexR-HSA-193678 (Reactome)
pro-beta-NGF homodimerComplexR-HSA-187029 (Reactome)
unknown kinaseR-HSA-3159312 (Reactome)

Annotated Interactions

View all...
SourceTargetTypeDatabase referenceComment
AATFR-HSA-204958 (Reactome)
ADPArrowR-HSA-193647 (Reactome)
ADPArrowR-HSA-193703 (Reactome)
ADPArrowR-HSA-193705 (Reactome)
ADPArrowR-HSA-204949 (Reactome)
ADPArrowR-HSA-205075 (Reactome)
ADPArrowR-HSA-205132 (Reactome)
ADPArrowR-HSA-205136 (Reactome)
ARHGDIA:NGFR:RTN4R:LINGO1:RTN4,MAG,OMGArrowR-HSA-193696 (Reactome)
ATPR-HSA-193647 (Reactome)
ATPR-HSA-193703 (Reactome)
ATPR-HSA-193705 (Reactome)
ATPR-HSA-204949 (Reactome)
ATPR-HSA-205075 (Reactome)
ATPR-HSA-205132 (Reactome)
ATPR-HSA-205136 (Reactome)
Active Caspases 2, 3ArrowR-HSA-205117 (Reactome)
Active N-SMase:Mg2+ArrowR-HSA-193672 (Reactome)
Active N-SMase:Mg2+mim-catalysisR-HSA-193706 (Reactome)
BADR-HSA-205075 (Reactome)
BCL2L11R-HSA-205075 (Reactome)
ChoPArrowR-HSA-193706 (Reactome)
GDPArrowR-HSA-205039 (Reactome)
GEFsmim-catalysisR-HSA-205039 (Reactome)
GTPR-HSA-205039 (Reactome)
H2OR-HSA-193706 (Reactome)
Histone deacetylaseR-HSA-205056 (Reactome)
IKBKB dimerR-HSA-193641 (Reactome)
IRAK1:MYD88R-HSA-193686 (Reactome)
ITGB3BPArrowR-HSA-205112 (Reactome)
ITGB3BPR-HSA-193677 (Reactome)
ITGB3BPR-HSA-205118 (Reactome)
IkB(alpha):NF-kB complexR-HSA-193705 (Reactome)
K63 linked polyubiquitin chainR-HSA-205118 (Reactome)
LINGO1R-HSA-209573 (Reactome)
MAGED1R-HSA-205115 (Reactome)
MAPK8R-HSA-204949 (Reactome)
MAPK8R-HSA-205132 (Reactome)
MAPK8R-HSA-205136 (Reactome)
MCF2mim-catalysisR-HSA-194518 (Reactome)
MYD88 dimerArrowR-HSA-193665 (Reactome)
Mg2+R-HSA-193672 (Reactome)
N-acylsphingosineArrowR-HSA-193706 (Reactome)
NF-kB:p75NTR ICD:TRAF6ArrowR-HSA-193700 (Reactome)
NFKB1(1-433):RELAArrowR-HSA-193691 (Reactome)
NFKB1(1-433):RELAArrowR-HSA-193705 (Reactome)
NFKB1(1-433):RELAR-HSA-193691 (Reactome)
NFKB1(1-433):RELAR-HSA-193700 (Reactome)
NGF ligand:p75NTR:IRAK1:MYD88ArrowR-HSA-193686 (Reactome)
NGF ligand:p75NTR:IRAK1:MYD88R-HSA-193647 (Reactome)
NGF ligand:p75NTR:NADE:14-3-3epsilonArrowR-HSA-204981 (Reactome)
NGF ligand:p75NTR:NRAGE:CHE1ArrowR-HSA-204958 (Reactome)
NGF ligand:p75NTR:NRIF:TRAF6ArrowR-HSA-193669 (Reactome)
NGF ligand:p75NTR:NRIF:TRAF6R-HSA-205112 (Reactome)
NGF ligand:p75NTR:NRIF:TRAF6mim-catalysisR-HSA-204949 (Reactome)
NGF ligand:p75NTR:NRIFArrowR-HSA-193677 (Reactome)
NGF ligand:p75NTR:NRIFR-HSA-193669 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:MYD88:TRAF6ArrowR-HSA-193695 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:MYD88:TRAF6R-HSA-193665 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:IKK-betaArrowR-HSA-193641 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:IKK-betaR-HSA-193703 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:IKK-betamim-catalysisR-HSA-193703 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:Phospho-IKK-betaArrowR-HSA-193703 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:Phospho-IKK-betamim-catalysisR-HSA-193705 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62:aPKCiArrowR-HSA-193684 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62ArrowR-HSA-193694 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62R-HSA-193641 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62R-HSA-193684 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6:p62R-HSA-209566 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6ArrowR-HSA-193665 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:TRAF6R-HSA-193694 (Reactome)
NGF ligand:p75NTR:Phospho-IRAK1:polyubiquitinated TRAF6:p62ArrowR-HSA-209566 (Reactome)
NGF ligand:p75NTR:p-IRAK1:MYD88ArrowR-HSA-193647 (Reactome)
NGF ligand:p75NTR:p-IRAK1:MYD88R-HSA-193695 (Reactome)
NGF:p75NTR:NADEArrowR-HSA-193650 (Reactome)
NGF:p75NTR:NADER-HSA-204981 (Reactome)
NGF:p75NTR:NADEmim-catalysisR-HSA-205117 (Reactome)
NGF:p75NTR:NRAGEArrowR-HSA-205115 (Reactome)
NGF:p75NTR:NRAGER-HSA-204958 (Reactome)
NGF:p75NTR:NRAGEmim-catalysisR-HSA-205132 (Reactome)
NGF:p75NTR:PRDM4ArrowR-HSA-193643 (Reactome)
NGF:p75NTR:RIP2ArrowR-HSA-193656 (Reactome)
NGFR(251-272)ArrowR-HSA-193682 (Reactome)
NGFR(251-427)ArrowR-HSA-193679 (Reactome)
NGFR(251-427)ArrowR-HSA-209532 (Reactome)
NGFR(251-427)R-HSA-193682 (Reactome)
NGFR(251-427)R-HSA-209532 (Reactome)
NGFR(273-427)ArrowR-HSA-193682 (Reactome)
NGFR(273-427)ArrowR-HSA-193702 (Reactome)
NGFR(273-427)R-HSA-193700 (Reactome)
NGFR(273-427)R-HSA-193702 (Reactome)
NGFR(29-250)ArrowR-HSA-193679 (Reactome)
NGFR:RTN4R:LINGO1:RTN4,MAG,OMGArrowR-HSA-193655 (Reactome)
NGFR:RTN4R:LINGO1:RTN4,MAG,OMGR-HSA-9012761 (Reactome)
NGFR:RTN4R:LINGO1ArrowR-HSA-209573 (Reactome)
NGFR:RTN4R:LINGO1R-HSA-193655 (Reactome)
NGFR:RTN4RArrowR-HSA-193636 (Reactome)
NGFR:RTN4RR-HSA-209573 (Reactome)
NGFRAP1R-HSA-193650 (Reactome)
NGFRR-HSA-193636 (Reactome)
NGFRR-HSA-193653 (Reactome)
NGFRR-HSA-193668 (Reactome)
NGFRR-HSA-193679 (Reactome)
PRDM4:Histone deacetylaseArrowR-HSA-205056 (Reactome)
PRDM4ArrowR-HSA-193661 (Reactome)
PRDM4R-HSA-193643 (Reactome)
PRDM4R-HSA-193661 (Reactome)
PRDM4R-HSA-205056 (Reactome)
PRKCIR-HSA-193684 (Reactome)
Procaspases 2, 3R-HSA-205117 (Reactome)
R-HSA-193636 (Reactome) The p75NTR extracellular domain interacts with NOGO receptor (NgR), a glycosyl phosphatidylinositol (GPI)-anchored protein present as a homomultimer at the cell surface. As NgR lacks an intracellular domain, it utilizes p75NTR as a co-receptor for intracellular signalling.
R-HSA-193641 (Reactome) NGF stimulation results in recruitment of IKK-beta (Inhibitor of nuclear factor kappa-B kinase subunit beta) to the p75NTR receptor complex. IKK-beta recruitment involves p62 (Wooten et al. 2001, Cao et al. 1996a, et al. 1996b ).
R-HSA-193642 (Reactome) Sortilin is a membrane protein that acts as co-receptor for p75NTR. Superior cervical ganglion (SCG) neurons, vascular smooth muscle (SM-11) cells, oligodendrocytes and CNS neurons (including basal forebrain neurons) (Volosin et al, 2006) express significant levels of sortilin and p75NTR. Schwann cells, instead, do not express sortilin. It is expressed during embryogenesis in areas where NGF and proNGF have well-characterized effects. It is important for proNGF signalling, but has little or no role on mature NGF initiated signalling. ProNGF preferentially binds to a p75NTR:sortilin complex, whereas mature NGF preferentially binds p75NTR alone. ProNGF binds to p75NTR with a dissociation constant (Kd) ~15-20 nM, and to sortilin with a Kd ~5 nM. In the presence of sortilin, proNGF binds to p75NTR with a Kd 0.2 nM. In contrast, mature NGF binds to p75NTR with a Kd of 1-2 nM, whereas it binds sortilin very weakly (Kd ~ 90 nM). Therefore, in the presence of sortilin, p75NTR binds more strongly to proNGF than to NGF, and proNGF signalling predominates. In the absence of sortilin, NGF binding is stronger than proNGF, and it is the mature NGF signalling that prevails. proNGF interacts with sortilin via its pro-domain, whereas the interaction with p75NTR is mediated by the mature domain.
R-HSA-193643 (Reactome) PRDM4, usually named SC1, for Schwann Cell factor 1, is a zinc finger protein that functions as a repressor of transcription. It is present in many tissues, and abundant in brain. It interacts with the NGF:p75NTR complex to signal cell cycle arrest. It is unclear whether it already forms a complex with p75NTR before NGF binding to p75.
R-HSA-193646 (Reactome) Neurotrophin (NGF or BDNF) binding to p75NTR increases RHO-GDI activity, possibly by loosening the grip of p75NTR on RHO-GDI, which prevents the dissociation of GDP thus allowing axonal growth to occur (Gehler et al. 2004).
R-HSA-193647 (Reactome) Upon recruitment to p75NTR, Interleukin-1 receptor-associated kinase (IRAK) is rapidly phosphorylated and activated by an unknown mechanism and protein.
R-HSA-193650 (Reactome) The NADE protein interacts with p75NTR to mediate cell death. The interaction is mediated by NADE NES (nuclear export signal), also responsible for self-association of NADE (Mukai J et al, 2002).
R-HSA-193653 (Reactome) p75NTR exists in a multimeric form both in presence or absence of NGF. In the NGF:p75NTR complex, a single p75 molecule is asymmetrically bound to a NGF homodimer, along the homodimeric interface of NGF. This causes an allosteric conformational change, which disables the NGF symmetry-related second p75 binding site. Therefore, it is possible that NGF has to perturb or alter the preformed p75 dimer orientation in order to initiate intracellular signalling. NGF:p75NTR complexes are not so long living as the NGF:TRKA complexes. This is due, at least in part, to the fact that TRKA homodimers are internalized, and continue signalling in endosomes.
Contrary to what is commonly believed, NGF bind to p75NTR and TRKA, individually, with a similar equilibrium binding constant (Kd ~ 1-2 nM). As a matter of fact, the association constant for NGF binding to p75NTR (k+1 = 8x10 to power of 6 M-1 s-1) is faster than for TRKA (k+1 = 8x10 to power of 5 M-1 s-1). On the other hand, the off rate of the NGF:TRKA complex ( k-1 = 7.2x10 to power of -5 s-1) is much slower than the NGF:p75NTR complex (k-1 = 1x10 to power of -3 s-1) . p75NTR and TRK receptors functionally interact, but the precise means by which this occurs has remained unresolved. This could result from a direct physical interaction or be explained by convergent signalling of these two receptors. Co-expression of both p75NTR and TRKA at the cell surface appears to result in the formation of a “high-affinity� binding site that has an accelerated rate of NGF association and a 30- to 100-fold higher affinity for NGF (Kd ~ 1-3 x 10 to power of -11 M) than either receptor alone.
The high-affinity binding sites appear to constitute 10%–15% of the total NGF binding sites. The nature of such high affinity binding sites is still unclear. They could be due to a multimeric complex of p75:TRKA proteins. Alternatively, NGF might first rapidly bind to p75NTR and then be presented to TRKA in a conformation that lowers its TRKA association rate. Some authors even question the existence of these high affinity sites. Structural data on NGF complexes with p75NTR and TRKA extracellular domains suggest that formation of a ternary complex TRKA:NGF:p75NTR in a 1:2:1 ration is theoretically possible, although unlikely. However, biochemical data so far failed to show that this complex forms.
R-HSA-193655 (Reactome) A group of myelin components named MDGIs (myelin-derived growth-inhibitors), bind to NgR and inhibit neurite outgrowth. Examples of such components are NOGO, OMGP (oligodendrocyte myelin glycoprotein) and MAG (myelin-associated glycoprotein). The amino-terminal region of NgR, covering eight leucine-rich repeats (LRR) and the LRR carboxy-terminal domain (LRRCT) is sufficient to interact with MAG, OMGP and NOGO. Their binding to NgR enhances the NgR-p75 interaction.These inhibitors bind to a receptor complex made up of the NOGO receptor, NgR, and p75NTR. Such complexes then activate RHOA, thereby inhibiting axonal growth.
R-HSA-193656 (Reactome) The RIP2 (receptor-interacting protein-2) kinase is a mediator of NGF-dependent NF-kB activity. It contains a serine/threonine kinase domain and a caspase recruitment domain (CARD) at the C terminus. It binds to the death domain of p75NTR via its CARD domain in an NGF-dependent manner. RIP2 may also bind TRAF proteins, suggesting the existence of complexes of TRAF and RIP2 proteins with the p75 receptor. RIP2 is also able to interact with p62. It is highly expressed in Schwann cells.
R-HSA-193661 (Reactome) PRDM4 is found in the cytoplasm. Following binding of NGF to p75NTR, after 1 hour of NGF treatment, PRDM4 is redistributed from the cytoplasm to the nucleus. The relocalisation of PRDM4 appears to be specific for NGF, as it is not affected by BDNF or NT3.
R-HSA-193665 (Reactome) After recruiting IRAK, MYD88 leaves the receptor complex. The amount of MYD88 that associates with p75 peaks at 1 min of NGF treatment and declines thereafter.
R-HSA-193666 (Reactome) The different molecules listed (NRAGE, NRIF, NADE, TRAF6) mediate, through unclear mechanisms, JNK activation by threonine and tyrosine phosphorylation. While active JNK does move to the nucleus and phosphorylates and activate transcription factors such as c-JUN and ATF2, these have not been implicated in p75-mediated cell death, but rather the direct activation of the cell death machinery by JNK has been implicated. p75 activates the intrinsic caspase pathway (involving mitochondrial release of cytochrome c, Apaf-1, and caspases-9) rather than the extrinsic (caspase-8) pathway activated by most other death receptors.
R-HSA-193668 (Reactome) p75NTR directly complexes with RHO-GDI (RHO-GDP Dissociation Inhibitor). RHO-GDI inhibits the dissociation of GDP and the subsequent binding of GTP to RHOA, thus preventing formation of active RHOA. Once bound to p75NTR, RHOA-GDI is less active. p75NTR acts on RHOB in a similar mechanism.
R-HSA-193669 (Reactome) Upon neurotrophin stimulation, p75NTR interacts with the ubiquitin 3 ligase TRAF6 (TNF receptor-associated factor 6). It is unclear whether TRAF6 binds to p75NTR directly, or whether it needs to be recruited through an adaptor protein such as MyD88.Recruitment of NRIF and TRAF6 to p75NTR is followed by an interaction between the two cytoplasmic proteins, It is possible that the NRIF:TRAF6 interaction promotes formation of a multimeric signalling complex. TRAF6 appears to promote NRIF release from p75NTR
R-HSA-193672 (Reactome) NGF binding to p75NTR activates N-SMase (Neutral sphingomyelinase), and possibly A-SMase (acid sphingomyelinase), an enzyme that converts sphingomyelin to ceramide. The mode and mechanism of interaction between p75 and N-SMase have not been determined but is thought to involve the recruitment of Mg2+ to the active site of the enzyme.
R-HSA-193677 (Reactome) NRIF is a ubiquitously expressed zinc finger protein of the Kruppel family that may transduce cell death signals during development and functions in association with TRAF6 to induce activation of JNK. NRIF-induced cell death through p75NTR requires p53 and NRIF nuclear translocation, which is modulated by TRAF6-mediated polyubiquitination of NRIF at lysine 63.
R-HSA-193679 (Reactome) alpha-secretase (ADAM17) is a metalloprotese that has the ability to cleave the p75NTR extracellular domain, in proximity of the transmembrane region. The cleaved extracellular domain is shed from the cell membrane, whereas the rest of the protein, the C-terminal fragment, stays anchored to the membrane. The released extracellular domain represents a binding protein for many potential ligands, including neurotrophins, pro-neurotrophin precursors, beta-amyloid. Shedding of the p75NTR extracellular region can be both constituve and stimulated. The constitutive shedding is dependent on signalling via the p38 MAP kinase. Shedding can be stimulated by the phorbol ester PMA, acting through protein kinase C and ERK activation, and by a tyrosine phosphatase inhibitor. Activation of TRKA by NGF (or TRKB by BDNF) also induces release of the p75NTR extracellular domain. The alpha-secretase cleavage is required for the subsequent cleavage by gamma-secretase.
R-HSA-193682 (Reactome) Within early endosomes, p75NTR C-Terminal Fragment undergoes processing by gamma-secretase, a complex composed of a presenilin homodimer (PSEN1 or PSEN2), nicastrin (NCSTN), APH1 (APH1A or APH1B) and PEN2. Such a minimal complex is sufficient for secretase activity, although other components may exist. The p75NTR cleavage by gamma-secretase gives rise to a 20-kD ICD (IntraCellular Domain) fragment, and to a small peptide, the significance of which is unknown but that is analogous to the A-beta peptides generated from amyloid precursor protein. p75NTR ICD may have cytoplasmic and nuclear signalling functions and it is unstable.
R-HSA-193684 (Reactome) The atypical protein kinase C-iota isoform (aPKC-i) is recruited to the p75NTR receptor complex by p62 and becomes active. p62 recruits aPKC both via TRAF6 and RIP2.
R-HSA-193686 (Reactome) The serine/threonine kinase IRAK (interleukin-1 receptor-associated kinase) is necessary for NF-kB activation. Under basal conditions, IRAK is not bound to the p75 receptor, and stays inactive in the cytoplasm. It associates with p75NTR following neurotrophin binding. MYD88 functions as an adapter, by recruiting IRAK to the p75 receptor. Upon stimulation with NGF, a MYD88: IRAK1 complex quickly forms that is recruited to p75NTR.
R-HSA-193691 (Reactome) Once dissociated from IkB, NF-kB moves to the nucleus. Once in the nucleus, NF-kB binds DNA at promoters of target genes. This entails transcription of several genes including the two HLH transcriptional regulators HES1 and HES5. HES1 and HES5 transcription can also be activated via NOTCH signalling. Increased production of HES1 and HES5 reduces the number of primary dendrites and promotes dendrite elongation.
R-HSA-193694 (Reactome) NGF binding to p75NTR induces recruitment of the atypical PKC interacting protein, p62, necessary for coupling IKKbeta with p75NTR. The kinase activity of IRAK1 is necessary for p62 (sequestosome-1) recruitment. IRAK1 interaction with TRAF6 precedes (1 min) its interaction with p62 (5 min). p62 has two protein interaction domains, named UBA and PB1. The UBA domain binds non-covalently to polyubiquitin chains. The PB1 domain has structural homology with the UbL (ubiquitin like) domain, and is able to interact with the 26S proteasome subunit Rpt1. Other protein interaction domains also exist within p62, suggesting that it may have a role in the formation of multimeric signalling complexes.p62 forms a complex with TRAF6, which involves the two domains PB1 at the p62 C-terminal end, and UBA, at the N-terminus.
R-HSA-193695 (Reactome) Neurotrophin binding to p75NTR leads to recruitment of TRAF6. This protein is an E3 ubiquitin ligase, which, together with an E2 Ubiquitin conjugating enzyme, mediates the assembly of lysine 63-linked polyubiquitin chains and their attachment to a lysine of a substrate protein. Activation of IRAK1 promotes recruitment of TRAF6. TRAF6 is able to bind to p75NTR (juxtamembrane region, residues 113-128), IRAK1 (N-terminal residues 1-198 and C-terminal residues 523-618), and MYD88. It might be recruited through the MYD88:IRAK1 complex.
R-HSA-193696 (Reactome) In the presence of a myelin component (GMDI), such as MAG, NOGO or OMG, bound to a complex of the NOGO receptor (RTN4R, also known as NgR) and NGFR (p75NTR), binding of NGFR to ARHGDIA, a RHO-GDI, associated with RHOA:GDP, is strengthened (Yamashita and Tohyama 2003). The presence of LINGO1 in the complex of NGFR, RTN4R and MAG, NOGO or OMG is needed for NGFR-dependent activation of RHOA (Mi et al. 2004).
R-HSA-193700 (Reactome) The p75NTR ICD has the potential to bind many intracellular proteins, including TRAF6, SC1, NADE, NRAGE, and RHOA. It may bring these proteins to function in different cellular compartments. p75NTR ICD was shown to activate NF-kB via TRAF6.
R-HSA-193702 (Reactome) A portion of the p75NTR ICD produced by gamma-secretase cleavage moves to the nucleus where it may participate in transcriptional regulation.
R-HSA-193703 (Reactome) Atypical PKC isoforms phosphorylate the beta subunit of the IKK complex (on Serines 177 and 181) thereby serving as an IKK kinase. TRAF6 and p62 as well appear to have a role in IKK activation. TRAF6 mediates the assembly of K63-linked poly-Ub chains required for IKK activation. The ubiquitin binding property of p62 may also be relevant in regulating IKK activation.
R-HSA-193705 (Reactome) IkB is an inhibitory protein that sequesters NF-kB in the cytoplasm, by masking a nuclear localization signal, located just at the C-terminal end in each of the NF-kB subunits. A key event in NF-kB activation involves phosphorylation of IkB by an IkB kinase (IKK). NGF stimulates the activity of the IkB kinase IKK-beta, and, possibly, IKK-alpha as well. Once IkB is phosphorylated, the IkB:NF-kB complex dissociates.
R-HSA-193706 (Reactome) Sphingomyielinase promotes the conversion of sphingomyelin to ceramide. Ceramide can activate JNK and other targets. The molecular details of the p75NTR-activated ceramide signalling cascade are only partially understood.
R-HSA-194518 (Reactome) RHOA is activated by guanine nucleotide exchange factors (RhoGEFs), exchanging GDP for GTP. RHOA, activated following binding of MDGIs (RTN4, MAG or OMG) to the complex of NOGO receptor (RTN4R, also known as NgR) and NGFR (p75NTR), rigidifies the actin cytoskeleton, thereby inhibiting axonal elongation and causing growth cone collapse. MCF2 (Dbl) RHO GEF was used to demonstrate activation of RHOA downstream of NGFR and RTN4R-mediated sequestration of ARHGDIA, a RHO-GDI, but other RHO GEFs may also be involved in RHOA activation (Yamashita and Tohyama 2003).
R-HSA-204947 (Reactome) NRIF polyubiquitination is necessary for nuclear translocation. The carboxyl terminus of NRIF mediates nuclear localization, whereas the amino terminus prevents it. Once in the nucleus, NRIF regulates gene expression, acting as a transcriptional repressor.
R-HSA-204949 (Reactome) NRIF and TRAF6 appear to cooperate in JNK activation. TRAF6 is involved both in JNK activation and in NF-kB activation. Although the NRIF:TRAF6 interaction enhances by threefold the TRAF6-mediated activation of JNK, it only modestly affects TRAF6-mediated activation of NF-kB.
R-HSA-204958 (Reactome) CHE1, also named AATF, is an Apoptosis Antagonizing Transcription Factor in cortical neurons. NRAGE binds to CHE1, inhibiting its nuclear localization by sequestering it in the cytoplasm, and, consequently, antagonizes its anti-apoptotic function.
R-HSA-204981 (Reactome) NADE forms a complex with the 14-3-3epsilon isoform. The last one interacts with caspase 3 through its C terminal region. The NADE:4-3-3epsilon complex negatively regulates p75NTR-mediated apoptosis, probably by down regulating caspase activity.
R-HSA-205008 (Reactome) Binding of NRIF to p62 (Sequestosome) is suspected to modulate NRIF transcriptional activity.
R-HSA-205039 (Reactome) Following NGF binding, p75NTR activates the RAC (Ras-related C3 botulinum toxin substrate) GTPase.
R-HSA-205056 (Reactome) Within the nucleus, PRDM4 is found in a complex with HDACs (histone deacetylases) 1, 2, and 3. It interacts with the regulatory regions of the cyclin E gene, strongly inhibiting transcription. It was also shown to weakly affect cyclib B transcription. PRDM4 is believed to interact with regulatory regions of other genes, which are unknown.
R-HSA-205075 (Reactome) Once activated, JNK phosphorylates targets in cytoplasm, including BIM and BAD that promote the release of cytochrome c and activation of caspases 9, 6 and 3.
R-HSA-205112 (Reactome) Neurotrophin or proneurotrophin signalling promotes p75NTR cleavage by gamma-secretase, allowing the release of p75 ICD and NRIF. This mechanism was shown in sympathetic neurons.
Gamma-secretase can be activated in a number of ways, including signalling via p75NTR. The phorbol esther PMA induces p75 cleavage, followed by NRIF nuclear translocation, after 30 min. Neurotrophin binding to p75, instead, triggers the same events only after 12 h.
R-HSA-205115 (Reactome) NRAGE (neurotrophin receptor-interacting MAGE homolog), a member of the MAGE family of proteins, is a cytoplasmic protein that mediates neurotrophin-induced cell death. NRAGE binding is stimulated following NGF (or proNGF) binding to p75NTR. Some studies indicate that NRAGE expression is limited to proliferative neural populations, whereas others indicate its presence in differentiated neurons in hippocampus. Another MAGE protein, Necdin, was reported to interact with p75NTR and affect cell death.
R-HSA-205117 (Reactome) Once bound to the NGF:p75NTR complex, NADE contributes to cell death signalling by promoting activation of caspases 2 and 3. It is unclear whether JNK activation is involved. The apoptotic function of NADE was observed in oligodendrocytes (Mukai et al. 2002).
R-HSA-205118 (Reactome) TRAF6 attaches a lysine 63-linked polyubiquitin chain to lysine 19 of NRIF. Mutation of NRIF lysine 19 prevents p75-mediated apoptosis. p75NTR cleavage by gamma-secretase is required for NRIF ubiquitination.
R-HSA-205132 (Reactome) The NGF:p75:NRAGE complex promotes threonine and tyrosine phosphorylation, and activation of JNK, by an unknown mechanism.
R-HSA-205136 (Reactome) Ras-related C3 botulinum toxin substrate 1 (RAC1) activation was described as essential for p75NTR to induce MAPK8 (aka JNK) and apoptosis in cortical oligodendrocytes (Bazenet et al. 1998). The simultaneous activation of TRKA counteracts the apoptotic action of p75, by modulating the kinetics of p75-mediated RAC activation.
R-HSA-209532 (Reactome) Most of the p75NTR C-terminal fragment resulting from alpha-secretase cleavage enters the early/recycling endosomal compartment.
R-HSA-209536 (Reactome) Once dissociated from NF-kB, the phosphorylated IkB protein is ubiquitinated at lysines 21 and 22, and degraded by the proteosome (Baldi et al 1996).
R-HSA-209566 (Reactome) The activity of TRAF6 is regulated by autoubiquitination. This process, in turn, is regulated by p62. Cells devoid of p62 exhibit low basal TRAF6 polyubiquitination. When p62 is expressed, auto-ubiquitination of TRAF6 is enhanced. The details curated in this event represent the ubiquitination of TRAF6, even as ubiquitin is shown as 1 stoichiometrically.
R-HSA-209573 (Reactome) The NgR1:p75NTR complex also interacts with LINGO1, a nervous system-specific transmembrane protein. LINGO1 is a potent axonal inhibitor of oligodendrocyte differentiation and myelination, and is regulated by NGF and its receptor TRKA .
R-HSA-9012761 (Reactome) In the presence of a myelin component (GMDI), such as MAG, NOGO or OMG, bound to a complex of the NOGO receptor (RTN4R, also known as NgR) and NGFR (p75NTR), binding of NGFR to ARHGDIA, a RHO-GDI, associated with RHOA:GDP, is strengthened (Yamashita and Tohyama 2003). The presence of LINGO1 in the complex of NGFR, RTN4R and MAG, NOGO or OMG is needed for NGFR-dependent activation of RHOA (Mi et al. 2004).
RAC1:GDPR-HSA-205039 (Reactome)
RAC1:GTPArrowR-HSA-205039 (Reactome)
RAC1:GTPArrowR-HSA-205136 (Reactome)
RHOA:GDP:ARHGDIA:NGFR:NGFArrowR-HSA-193646 (Reactome)
RHOA:GDP:ARHGDIA:NGFR:RTN4R:LINGO1:RTN4,MAG,OMGArrowR-HSA-9012761 (Reactome)
RHOA:GDP:ARHGDIA:NGFR:RTN4R:LINGO1:RTN4,MAG,OMGR-HSA-193696 (Reactome)
RHOA:GDP:ARHGDIA:NGFRArrowR-HSA-193668 (Reactome)
RHOA:GDP:ARHGDIA:NGFRR-HSA-193646 (Reactome)
RHOA:GDP:ARHGDIAR-HSA-193668 (Reactome)
RHOA:GDP:ARHGDIAR-HSA-9012761 (Reactome)
RHOA:GDPArrowR-HSA-193696 (Reactome)
RHOA:GDPR-HSA-194518 (Reactome)
RHOA:GTPArrowR-HSA-194518 (Reactome)
RIPK2R-HSA-193656 (Reactome)
RTN4,MAG,OMGR-HSA-193655 (Reactome)
RTN4R multimerR-HSA-193636 (Reactome)
SMPD2R-HSA-193672 (Reactome)
SPHMR-HSA-193706 (Reactome)
SQSTM1R-HSA-193694 (Reactome)
SQSTM1R-HSA-205008 (Reactome)
SQSTM1mim-catalysisR-HSA-205008 (Reactome)
TRAF6 homotrimerArrowR-HSA-205112 (Reactome)
TRAF6 homotrimerR-HSA-193669 (Reactome)
TRAF6 homotrimermim-catalysisR-HSA-205118 (Reactome)
TRAF6R-HSA-193695 (Reactome)
TRAF6R-HSA-193700 (Reactome)
UbR-HSA-209536 (Reactome)
UbR-HSA-209566 (Reactome)
Ubiquitinated NRIF:SequestosomeArrowR-HSA-204947 (Reactome)
Ubiquitinated NRIF:SequestosomeArrowR-HSA-205008 (Reactome)
Ubiquitinated NRIF:SequestosomeR-HSA-204947 (Reactome)
Ubiquitinated phospho-IkBArrowR-HSA-209536 (Reactome)
Ubiquitinated NRIFArrowR-HSA-205118 (Reactome)
Ubiquitinated NRIFR-HSA-205008 (Reactome)
YWHAE dimerR-HSA-204981 (Reactome)
gamma-secretase complexmim-catalysisR-HSA-193682 (Reactome)
gamma-secretase complexmim-catalysisR-HSA-205112 (Reactome)
mature NGF homodimer:p75NTRArrowR-HSA-193653 (Reactome)
mature NGF homodimer:p75NTRArrowR-HSA-205112 (Reactome)
mature NGF homodimer:p75NTRR-HSA-193643 (Reactome)
mature NGF homodimer:p75NTRR-HSA-193650 (Reactome)
mature NGF homodimer:p75NTRR-HSA-193656 (Reactome)
mature NGF homodimer:p75NTRR-HSA-193677 (Reactome)
mature NGF homodimer:p75NTRR-HSA-193686 (Reactome)
mature NGF homodimer:p75NTRR-HSA-205115 (Reactome)
mature NGF homodimer:p75NTRmim-catalysisR-HSA-193672 (Reactome)
mature beta-NGF homodimerR-HSA-193646 (Reactome)
mature beta-NGF homodimerR-HSA-193653 (Reactome)
p-S,T-ADAM17(215-827):Zn2+mim-catalysisR-HSA-193679 (Reactome)
p-S128-BADArrowR-HSA-205075 (Reactome)
p-S32,S36-NFKBIAArrowR-HSA-193705 (Reactome)
p-S32,S36-NFKBIAR-HSA-209536 (Reactome)
p-S65-BCL2L11ArrowR-HSA-205075 (Reactome)
p-T,Y-MAPK8ArrowR-HSA-193666 (Reactome)
p-T,Y-MAPK8ArrowR-HSA-204949 (Reactome)
p-T,Y-MAPK8ArrowR-HSA-205132 (Reactome)
p-T,Y-MAPK8ArrowR-HSA-205136 (Reactome)
p-T,Y-MAPK8R-HSA-193666 (Reactome)
p-T,Y-MAPK8mim-catalysisR-HSA-205075 (Reactome)
p75NTR:sortilin complexR-HSA-193642 (Reactome)
pro-beta NGF:p75NTR:sortilinArrowR-HSA-193642 (Reactome)
pro-beta-NGF homodimerR-HSA-193642 (Reactome)
unknown kinasemim-catalysisR-HSA-193647 (Reactome)
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