PMADS

Id:	acc0265
Group:	1sens
Protein:	MET
Gene Symbol:	MET
Protein Id:	P08581
Protein Name:	MET_HUMAN
PTM:	phosphorylation
Site:	Tyr1234
Site Sequence:	LARDMYDKEYYSVHNKTGAKL
Disease Category:	Cancer
Disease:	Ovarian Cancer
Disease Subtype:	MET amp
Disease Cellline:	58As9
Disease Info:
Drug:	crizotinib
Drug Info:	"Crizotinib is an oral multi-target tyrosine kinase inhibitor that primarily inhibits ALK and ROS1 kinase activity, used for treating ALK-positive or ROS1-positive non-small cell lung cancer (NSCLC). "
Effect:	modulate
Effect Info:	The drug induces apoptosis and inhibits the phosphorylation of AKT and ERK in gastric cancer with MET amplification positivity.
Note:
Score:	4.0
Pubmed(PMID):	22729845
Sentence Index:	22729845_3
Sentence:	"Inhibition of MET signaling by crizotinib or RNA interference-mediated MET depletion resulted in induction of apoptosis accompanied by inhibition of AKT and extracellular signal-regulated kinase phosphorylation in gastric cancer cells with MET amplification but not in those without it, suggesting that MET signaling is essential for the survival of MET amplification-positive cells."

Sequence & Structure:

MKAPAVLAPGILVLLFTLVQRSNGECKEALAKSEMNVNMKYQLPNFTAETPIQNVILHEHHIFLGATNYIYVLNEEDLQKVAEYKTGPVLEHPDCFPCQDCSSKANLSGGVWKDNINMALVVDTYYDDQLISCGSVNRGTCQRHVFPHNHTADIQSEVHCIFSPQIEEPSQCPDCVVSALGAKVLSSVKDRFINFFVGNTINSSYFPDHPLHSISVRRLKETKDGFMFLTDQSYIDVLPEFRDSYPIKYVHAFESNNFIYFLTVQRETLDAQTFHTRIIRFCSINSGLHSYMEMPLECILTEKRKKRSTKKEVFNILQAAYVSKPGAQLARQIGASLNDDILFGVFAQSKPDSAEPMDRSAMCAFPIKYVNDFFNKIVNKNNVRCLQHFYGPNHEHCFNRTLLRNSSGCEARRDEYRTEFTTALQRVDLFMGQFSEVLLTSISTFIKGDLTIANLGTSEGRFMQVVVSRSGPSTPHVNFLLDSHPVSPEVIVEHTLNQNGYTLVITGKKITKIPLNGLGCRHFQSCSQCLSAPPFVQCGWCHDKCVRSEECLSGTWTQQICLPAIYKVFPNSAPLEGGTRLTICGWDFGFRRNNKFDLKKTRVLLGNESCTLTLSESTMNTLKCTVGPAMNKHFNMSIIISNGHGTTQYSTFSYVDPVITSISPKYGPMAGGTLLTLTGNYLNSGNSRHISIGGKTCTLKSVSNSILECYTPAQTISTEFAVKLKIDLANRETSIFSYREDPIVYEIHPTKSFISGGSTITGVGKNLNSVSVPRMVINVHEAGRNFTVACQHRSNSEIICCTTPSLQQLNLQLPLKTKAFFMLDGILSKYFDLIYVHNPVFKPFEKPVMISMGNENVLEIKGNDIDPEAVKGEVLKVGNKSCENIHLHSEAVLCTVPNDLLKLNSELNIEWKQAISSTVLGKVIVQPDQNFTGLIAGVVSISTALLLLLGFFLWLKKRKQIKDLGSELVRYDARVHTPHLDRLVSARSVSPTTEMVSNESVDYRATFPEDQFPNSSQNGSCRQVQYPLTDMSPILTSGDSDISSPLLQNTVHIDLSALNPELVQAVQHVVIGPSSLIVHFNEVIGRGHFGCVYHGTLLDNDGKKIHCAVKSLNRITDIGEVSQFLTEGIIMKDFSHPNVLSLLGICLRSEGSPLVVLPYMKHGDLRNFIRNETHNPTVKDLIGFGLQVAKGMKYLASKKFVHRDLAARNCMLDEKFTVKVADFGLARDMYDKEYYSVHNKTGAKLPVKWMALESLQTQKFTTKSDVWSFGVLLWELMTRGAPPYPDVNTFDITVYLLQGRRLLQPEYCPDPLYEVMLKCWHPKAEMRPSFSELVSRISAIFSTFIGEHYVHVNATYVNVKCVAPYPSLLSSEDNADDEVDTRPASFWETS

Select PDB:

Known Drugs:

source: Multi-Sources

(see table)

Target	Drug name	MOA	Phase	Status	Disease	Source
MET	CABOZANTINIB S-MALATE	Hepatocyte growth factor receptor inhibitor	4	-	hepatocellular carcinoma	EMA
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	4	-	diffuse large B-cell lymphoma	DailyMed
MET	CABOZANTINIB	Hepatocyte growth factor receptor inhibitor	4	-	neoplasm	ATC
MET	AMIVANTAMAB	Hepatocyte growth factor receptor inhibitor	4	-	neoplasm	ATC
MET	CAPMATINIB	Hepatocyte growth factor receptor inhibitor	4	-	neoplasm	ATC
MET	TEPOTINIB	Hepatocyte growth factor receptor inhibitor	4	-	neoplasm	ATC
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	4	-	neoplasm	ATC
MET	CABOZANTINIB S-MALATE	Hepatocyte growth factor receptor inhibitor	4	-	renal cell carcinoma	EMA DailyMed
MET	CABOZANTINIB S-MALATE	Hepatocyte growth factor receptor inhibitor	4	-	thyroid carcinoma	DailyMed
MET	CAPMATINIB HYDROCHLORIDE	Hepatocyte growth factor receptor inhibitor	4	-	non-small cell lung carcinoma	EMA FDA DailyMed
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	4	-	non-small cell lung carcinoma	EMA DailyMed
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	4	Terminated	non-small cell lung carcinoma	ClinicalTrials
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	4	Active, not recruiting	non-small cell lung carcinoma	ClinicalTrials
MET	AMIVANTAMAB	Hepatocyte growth factor receptor inhibitor	4	-	non-small cell lung carcinoma	EMA FDA
MET	TEPOTINIB HYDROCHLORIDE	Hepatocyte growth factor receptor inhibitor	4	-	non-small cell lung carcinoma	EMA FDA DailyMed
MET	TIVANTINIB	Hepatocyte growth factor receptor inhibitor	3	Completed	hepatocellular carcinoma	ClinicalTrials
MET	CABOZANTINIB	Hepatocyte growth factor receptor inhibitor	3	Active, not recruiting	hepatocellular carcinoma	ClinicalTrials
MET	CABOZANTINIB	Hepatocyte growth factor receptor inhibitor	3	Completed	hepatocellular carcinoma	ClinicalTrials
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	3	Completed	carcinoma	ClinicalTrials
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	3	Recruiting	lung adenocarcinoma	ClinicalTrials
MET	CRIZOTINIB	Hepatocyte growth factor receptor inhibitor	3	Recruiting	neoplasm	ClinicalTrials
MET	ONARTUZUMAB	Hepatocyte growth factor receptor antagonist	3	Completed	neoplasm	ClinicalTrials
MET	CABOZANTINIB	Hepatocyte growth factor receptor inhibitor	3	Active, not recruiting	renal cell carcinoma	ClinicalTrials ClinicalTrials ClinicalTrials ClinicalTrials
MET	CABOZANTINIB	Hepatocyte growth factor receptor inhibitor	3	Terminated	renal cell carcinoma	ClinicalTrials
MET	SAVOLITINIB	Hepatocyte growth factor receptor inhibitor	3	Active, not recruiting	renal cell carcinoma	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

MET-Tyr1234
Cancer	Intensity
BRCA
COAD
HGSC
ccRCC
GBM
HNSC
LUAD
LUSC
non_ccRCC
PDAC
UCEC

PTM-Disease Association:

source: PTMD

Residue	Position	State	Disease	Class	PMID
Y	1234	P	Lung cancer/carcinoma	Phosphorylation	23973484
Y	1234	U	Prostate cancer	Phosphorylation	33705609
Y	1234	U	Bladder cancer	Phosphorylation	17062641
Y	1234	U	Hepatocellular carcinoma/hepatocarcinoma/hepatoma	Phosphorylation	21455220

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

No data.

Function score:

source: funscoR

No data.

Cross Links:

CTD
DMRdb