PMADS

Id:	acc0075
Group:	2sens
Protein:	ERK1
Gene Symbol:	MAPK3
Protein Id:	P27361
Protein Name:	MK03_HUMAN
PTM:	phosphorylation
Site:	Tyr204
Site Sequence:	HDHTGFLTEYVATRWYRAPEI
Disease Category:	Cancer
Disease:	Hepatocellular Carcinoma
Disease Subtype:
Disease Cellline:	HuH-7-EGFRvIII
Disease Info:
Drug:	CH12 + sorafenib
Drug Info:	"Sorafenib: Sorafenib is an oral multi-kinase inhibitor developed by Bayer Pharmaceuticals, approved by the FDA in 2005, primarily used for treating advanced renal cell carcinoma, unresectable hepatocellular carcinoma, and radioactive iodine-refractory differentiated thyroid cancer by targeting tumor cell proliferation and angiogenesis. CH12: - "
Effect:	modulate
Effect Info:	"The combination of CH12 and sorafenib more significantly down - regulates the phosphorylation of ERK, Akt (Thr308), and STAT3, and the tumor growth inhibitory effect is significantly enhanced."
Note:	drug comb
Score:	4.0
Pubmed(PMID):	22787432
Sentence Index:	22787432_8-9
Sentence:	"The results showed that, when CH12 was combined with sorafenib, the tumor growth suppression effect was significantly increased, and the concentration of sorafenib required for growth inhibition was substantially reduced. Mechanistically, the combination could more noticeably downregulate the phosphorylation of constitutively active extracellular signal-regulated kinase (ERK), Akt (Thr308), and signal transducer and activator of transcription 3 (STAT3) than sorafenib alone."

Sequence & Structure:

MAAAAAQGGGGGEPRRTEGVGPGVPGEVEMVKGQPFDVGPRYTQLQYIGEGAYGMVSSAYDHVRKTRVAIKKISPFEHQTYCQRTLREIQILLRFRHENVIGIRDILRASTLEAMRDVYIVQDLMETDLYKLLKSQQLSNDHICYFLYQILRGLKYIHSANVLHRDLKPSNLLINTTCDLKICDFGLARIADPEHDHTGFLTEYVATRWYRAPEIMLNSKGYTKSIDIWSVGCILAEMLSNRPIFPGKHYLDQLNHILGILGSPSQEDLNCIINMKARNYLQSLPSKTKVAWAKLFPKSDSKALDLLDRMLTFNPNKRITVEEALAHPYLEQYYDPTDEPVAEEPFTFAMELDDLPKERLKELIFQETARFQPGVLEAP

Select PDB:

Known Drugs:

source: Multi-Sources

(see table)

Target	Drug name	MOA	Phase	Status	Disease	Source
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	2	Terminated	neoplasm	ClinicalTrials
MAPK3	TEMUTERKIB	Mitogen-activated protein kinase; ERK1/ERK2 inhibitor	2	Completed	pancreatic carcinoma	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	2	Recruiting	histiocytic neoplasm	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	2	Active, not recruiting	Uveal Melanoma	ClinicalTrials
MAPK3	TEMUTERKIB	Mitogen-activated protein kinase; ERK1/ERK2 inhibitor	2	Terminated	cancer	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	1	Completed	acute myeloid leukemia	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	1	Completed	myelodysplastic syndrome	ClinicalTrials
MAPK3	TEMUTERKIB	Mitogen-activated protein kinase; ERK1/ERK2 inhibitor	1	Recruiting	acute myeloid leukemia	ClinicalTrials
MAPK3	RAVOXERTINIB	MAP kinase ERK1 inhibitor	1	Completed	neoplasm	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	1	Completed	neoplasm	ClinicalTrials ClinicalTrials
MAPK3	MK-8353	MAP kinase ERK1 inhibitor	1	Completed	neoplasm	ClinicalTrials
MAPK3	MK-8353	MAP kinase ERK1 inhibitor	1	Terminated	neoplasm	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	1	Recruiting	pancreatic carcinoma	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	1	Terminated	pancreatic carcinoma	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	1	Recruiting	metastatic colorectal cancer	ClinicalTrials
MAPK3	KO-947	Mitogen-activated protein kinase; ERK1/ERK2 inhibitor	1	Terminated	cancer	ClinicalTrials
MAPK3	MK-8353	MAP kinase ERK1 inhibitor	1	Completed	colorectal cancer	ClinicalTrials
MAPK3	TEMUTERKIB	Mitogen-activated protein kinase; ERK1/ERK2 inhibitor	0.5	Recruiting	glioblastoma multiforme	ClinicalTrials
MAPK3	ULIXERTINIB	MAP kinase ERK1 inhibitor	0.5	Recruiting	Paraganglioma	ClinicalTrials

Note: Only show clinically investigational or approved drugs with protein targets.

Protein Tractability:

source: Open Targets

Small molecule

Antibody

PROTAC

Other modalities

Approved Drug

Advanced Clinical

Phase 1 Clinical

Structure with Ligand

High-Quality Ligand

High-Quality Pocket

Med-Quality Pocket

Druggable Family

Approved Drug

Advanced Clinical

Phase 1 Clinical

UniProt loc high conf

GO CC high conf

UniProt loc med conf

UniProt SigP or TMHMM

GO CC med conf

Human Protein Atlas loc

Approved Drug

Advanced Clinical

Phase 1 Clinical

Literature

UniProt Ubiquitination

Database Ubiquitination

Half-life Data

Small Molecule Binder

Approved Drug

Advanced Clinical

Phase 1 Clinical

PTM Intensity:

source: CPTAC

MAPK3-Tyr204
Cancer	Intensity
BRCA	1.299
COAD	0.294
HGSC	1.686
ccRCC	-0.456
GBM	0.155
HNSC	0.082
LUAD	-0.027
LUSC	0.328
non_ccRCC	-0.355
PDAC	-1.055
UCEC	-1.949

PTM-Disease Association:

source: PTMD

Residue	Position	State	Disease	Class	PMID
Y	204	D	Acute lymphocytic leukemia	Phosphorylation	26073130
Y	204	D	Head and neck squamous cell carcinoma	Phosphorylation	21281788
Y	204	U	Breast cancer	Phosphorylation	31944568
Y	204	U	Acute myelogenous leukemia	Phosphorylation	26073130
Y	204	U	Alzheimer's disease	Phosphorylation	35847683
Y	204	U	Glioma	Phosphorylation	33820494
Y	204	U	Pulmonary emphysema	Phosphorylation	14764579
Y	204	U	Triple-negative breast cancer	Phosphorylation	28415597
Y	204	U	Tuberous sclerosis complex	Phosphorylation	17671177

State Note: Based on the distinct PTM states in diseases, PTMD classified all disease-associated PTMs into six classes, including whether the up-regulation (U) or down-regulation (D) of PTM levels, the absence (A) or presence (P) of PTMs, and the creation (C) or disruption (N) of PTM sites are associated with diseases.

PTM-Drug Perturbation Response:

source: DecryptM

Protein	Gene	PTM	Position	Modified sequence	Cell	Drug	pEC50	Regulation
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	BT-474	Lapatinib	6.5402	down
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	MDA-MB-175	Lapatinib	7.4061	down
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	MDA-MB-175	Pertuzumab	-4.6099	down
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	BT-474	Pertuzumab	-1.9536	-
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	BT-474	Trastuzumab	-1.9524	-
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	MDA-MB-175	Trastuzumab	5	-
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	SK-BR-3	Lapatinib	6.25	-
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	SK-BR-3	Pertuzumab	-1.7417	-
P27361	MAPK3	P	Tyr204	IADPEHDHTGFLTEY(ph)VATR	SK-BR-3	Trastuzumab	-0.8941	-

pEC50 Note: pEC50 is the negative logarithm of EC50 (half-maximal effective concentration, dosage unit Mol), calculated as pEC50 = -log10(EC50), which quantifies the potency of a drug or compound.

Function score:

source: funscoR

No data.

Cross Links:

CTD
DMRdb