MAPK signaling and ARTD family members (Homo sapiens)

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ArcPathVisio Brace Ellipse EndoplasmicReticulum GolgiApparatus HexagonPathVisio MimDegradation Mitochondria Octagon PentagonPathVisio Rectangle RoundedRectangle SarcoplasmicReticulum TriangleEquilateralEast TrianglePathVisio none MAPKKKAdaptorGEFGTPaseMAP2K1MAP2K2MAPK3MAPK1TFTNKS1PARP1PARP14MAP2K4MAP2K7MAPK14MAPK11MAPK12MAPK13MAPK8MAPK9MAPK10DUSP1ATF4MAP2K3MAP2K4MAP2K6BRAFRAF1ARAFASKDLKMEKKMLKTAK1TLP2PARP1MAPK14MAPK11MAPK12MAPK13ASKDLKMEKKMLKTAK1TLP2MAPK8MAPK9MAPK10MAPKKKMEK1/2ERK1/2MAPK3MAPK1ERK1/2JNK1-3MKK4/7JNK1-3p38a/b/g/dp38a/b/g/dMKK3/4/6MKP-1Rafs / MosPARP1PARP1PARP14PARP1PARP1PARP1PARP1TNKS1TNKS2PARP1Name: MAPK signaling and ARTD family membersOrganism: Homo sapiens


Description

The mitogen-activated protein kinase (MAPK) pathway is a series of cytoplasmic phosphorylation events triggered by the binding of mitogens, growth factors, and cytokines to their receptors.


  • MAPK signaling effects on ARTD family members*

ERK signaling positively regulates both the expression and activity of PARP1. When MEK, the kinase upstream of ERK in the MAPK cascade, was inhibited in conditioned medium-stimulated endothelial cells, it decreased PARP1 expression. On the other hand, overexpressing p-ERK2 in neurons led to an increase in PARP1 activity.


ERK signaling also influences Tankyrase 1 activity. In 3T3-L1 fibroblasts and adipocytes stimulated by insulin, PDGF, and EGF, ERK phosphorylates Tankyrase 1.


JNK1 has been suggested as a positive regulator of PARP1 activation during H2O2-induced cell death in mouse embryonic fibroblasts (MEFs). In the context of multiple myeloma, JNK2 enhances PARP14 protein levels through an unknown mechanism.


  • Positive regulation*

MAPK signaling is positively regulated by PARP1 and Tankyrase 1/2. Under normal conditions, phosphorylation of ERK1/2 (p-ERK1/2) by MEK1/2 (MAPKK) induces conformational changes that activate ERK1/2, leading to the phosphorylation of downstream targets that promote cell growth, survival, and migration.


Perfusing rat hearts with a cytostatic agent increased cardiotoxicity and phosphorylation of ERK, JNK, and p38. Inhibition of PARP1-dependent ADP-ribosylation with BGP-15 significantly reduces MAPK phosphorylation.


PARP1 activation also correlates with JNK and p38 signaling in various cell types, especially in the context of ROS-dependent PARP1 activation and cell death, which depends on JNK and/or p38 signaling.


Although primarily observed in Drosophila melanogaster rather than mammalian cells, Tankyrase 1/2 have been implicated in JNK activation.


  • Negative regulation*

In the case of Salmonella infection in human colonic epithelial cells, PARP inhibitor PJ-34 treatment increases ERK phosphorylation, NF-κB signaling, and IL-6 production/secretion, even at early time points.


Inhibition of PARP1 increased ERK activation and reduced cell death in H2O2-induced apoptosis of human WRL-68 cells, while simultaneously lowering p-JNK and p-p38 levels. PARP14 interacts with and likely ADP-ribosylate JNK1, inhibiting its kinase activity and reducing JNK1-dependent apoptosis. Similarly, inhibition of PARP14 with PJ-34 leads to increased JNK1 activity and enhanced cell death.

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Quality Tags

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Ontology Terms

Bibliography

  1. Boehi F, Manetsch P, Hottiger MO; ''Interplay between ADP-ribosyltransferases and essential cell signaling pathways controls cellular responses.''; Cell Discov, 2021 PubMed Europe PMC Scholia

History

View all...
CompareRevisionActionTimeUserComment
138449
Approved
view03:05, 8 April 2025EweitzClear board dimension cache
138446view02:59, 8 April 2025EweitzAdd table of contents for ARTD pathway series
138340view01:11, 31 March 2025EweitzOntology Term : 'mitogen activated protein kinase signaling pathway' added !
138339view01:09, 31 March 2025EweitzUse gene symbols
138338view23:59, 30 March 2025EweitzAdd identifiers to genes
138337view23:51, 30 March 2025EweitzAdd identifiers to genes
138336view23:45, 30 March 2025EweitzAssign identifiers to genes
138329view23:00, 30 March 2025EweitzRefine interactions
138328view22:39, 30 March 2025EweitzModified description
138327view22:39, 30 March 2025EweitzModified description
138326view22:15, 30 March 2025EweitzRefine labels
138325view22:08, 30 March 2025EweitzAdd literature reference
138324view22:08, 30 March 2025EweitzAdd nodes, interactions
138323view15:02, 30 March 2025EweitzAdd interactions
138322view14:42, 30 March 2025EweitzAdd interactions, cell compartments
138321view14:29, 30 March 2025EweitzAdd supplementary labels
138320view14:20, 30 March 2025EweitzArrange nodes
138319view14:15, 30 March 2025EweitzUse gene symbols
138318view13:50, 30 March 2025EweitzUse gene symbols
138317view12:31, 30 March 2025EweitzUse gene symbols
138316view11:50, 30 March 2025EweitzNew pathway

External references

DataNodes

View all...
Name  ↓Type  ↓Database reference  ↓Comment  ↓
ARAFGeneProduct"Rafs / Mos" in source
ASKGeneProduct"MAPKKK" in source
ATF4GeneProduct
AdaptorGeneProduct
BRAFGeneProduct"Rafs / Mos" in source
DLKGeneProduct"MAPKKK" in source
DUSP1GeneProduct"MKP-1" in source
GEFGeneProduct
GTPaseGeneProduct
MAP2K1GeneProduct"MEK1/2" in source
MAP2K2GeneProduct"MEK1/2" in source
MAP2K3GeneProduct"MKK3/4/6" in source
MAP2K4GeneProduct"MKK3/4/6" in source
MAP2K6GeneProduct"MKK3/4/6" in source
MAP2K7GeneProduct"MKK4/7" in source
MAPK1GeneProduct"ERK1/2" in source
MAPK10GeneProduct"JNK1-3" in source
MAPK11GeneProduct"p38a/b/g/d" in source
MAPK12GeneProduct"p38a/b/g/d" in source
MAPK13GeneProduct"p38a/b/g/d" in source
MAPK14GeneProduct"p38a/b/g/d" in source
MAPK3GeneProduct"ERK1/2" in source
MAPK8GeneProduct"JNK1-3" in source
MAPK9GeneProduct"JNK1-3" in source
MEKKGeneProduct"MAPKKK" in source
MLKGeneProduct"MAPKKK" in source
PARP1GeneProduct
PARP14GeneProduct
RAF1GeneProduct"Rafs / Mos" in source
TAK1GeneProduct"MAPKKK" in source
TFGeneProduct
TLP2GeneProduct"MAPKKK" in source
TNKS1GeneProduct
TNKS2GeneProduct

Annotated Interactions

No annotated interactions

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