Maps_Modules
HMC:AVOIDING_IMMUNE_DESTRUCTION
Adaptive Immune Response / TCR_SIGNALING
References
PMID:18784374 PMID:23077238 PMID:25456276
References
CASCADE:IFNAB
PMID:18784374, PMID:23077238
PKC-theta requires DAG for activation. DAG is generated by PLCG through enzymatic cleavage of PIP2
Identifiers
Diacylglycerol
CAS:N/A PUBCHEM:3914 CHEBI:17815 KEGGCOMPOUND:C00165
References
su_mpk1_mpk1_re45( Survival ):
PLCG acts on PIP2 in the PM to produce DAG and IP3.
PMID:16488589
IP3 diffuses through the cytosol and binds to receptors on the endoplasmic reticulum causing the release of calcium ions (Ca2+) into the cytosol.
http://users.rcn.com/jkimball.ma.ultranet/BiologyPages/S/Second_messengers.html
su_mpk1_mpk1_re46( Survival ):
RasGRP1 is a C1-domain containing protein that is activated by DAG and Ca2+ in a manner analogous to members of the PKC family.
PMID:17496910
DAG remains in the inner layer of the plasma membrane. It recruits Protein Kinase C (PKC) ??? a calcium-dependent kinase that phosphorylates many other proteins that bring about the changes in the cell.
su_mpk1_mpk1_re263( Survival ):
Recruitment to the membrane and tyrosine phosphorylation enhance the enzymatic activity of PLC-g leading to the formation of two second messengers diacylglycerol (DAG) and inositol 145-trisphosphate (IP3). IP3 releases Ca2+ from internal stores which in turn acts in concert with DAG to translocate protein kinase C (PKC) to the cell membrane and stimulate its enzymatic activity.
PMID:15567848
References
Ca2+/Wnt MODULE
s_wnc1_re26:( Survival ) PMID:16054198
+ DAG@T_cell → DAG:PRKCQ@T_cell
→ IP3@T_cell + DAG@T_cell
→ (DAG:PRKCQ|pho)|active@cSMAC
→ DAG:PRKCQ@cSMAC
+ DAG@T_cell → DAG:RASGRP1@T_cell
+ DAG@Cytosol → (DAG:PKC*)|active@Cytosol
→ Fibroblast_proliferation@Cytosol
→ DAG@INNATE_IMMUNE_CELL_Cytosol + IP3@INNATE_IMMUNE_CELL_Cytosol
+ PRKCQ@INNATE_IMMUNE_CELL_Cytosol → DAG:PRKCQ@INNATE_IMMUNE_CELL_Cytosol
→ DAG:PRKCQ|pho@INNATE_IMMUNE_CELL_Cytosol
+ DAG@Plasma Membrane + Ca2+@Cytoplasm → Ca2+:DAG:PKC*@Plasma Membrane
+ Ca2+:DAG:RASGRP1@Golgi Apparatus → Ca2+:DAG:RAS*|pho:RASGRP1@Golgi Apparatus
→ IP3@Endoplasmic Reticulum + DAG@Plasma Membrane
+ RASGRP1@Cytoplasm → DAG:RASGRP1@Plasma Membrane
+ Ca2+@Cytoplasm → Ca2+:DAG:RASGRP1@Plasma Membrane
→ Ca2+:DAG:RASGRP1@Golgi Apparatus
+ Ca2+:DAG:RAS*|pho:RASGRP1@Golgi Apparatus → Ca2+:DAG:RAF1|pho:RAS*|pho:RASGRP1@Golgi Apparatus
→ DAG@Cytoplasm + IP3@Cytoplasm
→ CARD11|pho|active@T_cell
+ GTP@T_cell → (GTP:HRAS)|active@T_cell + GDP@T_cell
→ STK39|pho|active@T_cell
→ (PIP3*:TEC|pho)|active@T_cell
+ MAP3K7@T_cell → MAP3K7:TAB*|pho@T_cell
→ BAD|pho@T_cell
→ rIRF9@INNATE_IMMUNE_CELL_Cytosol
→ NFAT*@INNATE_IMMUNE_CELL_Cytosol
→ STAT1|pho|active@INNATE_IMMUNE_CELL_Cytosol
→ WASP*|pho:WIPF1|pho@INNATE_IMMUNE_CELL_Cytosol
→ GZMB@SECRETORY_GRANULE
→ GZMA@SECRETORY_GRANULE
+ RTK*@Plasma Membrane → GRB2:RTK*:SOS*@Plasma Membrane
→ RAF1|pho@Cytoplasm
+ SRC@Cytoplasm → RTK*:SRC@Plasma Membrane
→ ERK*|pho|pho:MEK*|pho|pho:SEF*@Cytoplasm
→ PKC*@Cytoplasm