PMADS

Id:	acc2193
Group:	2sens
Protein:	PKCdelta
Gene Symbol:	PRKCD
Protein Id:	Q05655
Protein Name:	KPCD_HUMAN
PTM:	phosphorylation
Site:	Thr507
Site Sequence:	NIFGESRASTFCGTPDYIAPE
Disease Category:	Cancer
Disease:	Colorectal Cancer
Disease Subtype:
Disease Cellline:	CT26
Disease Info:
Drug:	magnolol
Drug Info:	"Magnolol is a bioactive lignan derived from the bark of Magnolia officinalis, exhibiting anti-inflammatory, antioxidant, and neuroprotective properties, and has been studied for potential therapeutic applications in conditions such as cancer, neurodegenerative diseases, and metabolic disorders."
Effect:	modulate
Effect Info:	"Both magnolol and the PKCdelta inhibitor rottlerin can reduce the activity of NF-κB, decrease the phosphorylation of proteins related to tumor progression, and attenuate the invasive ability of CRC cells."
Note:
Score:	4.0
Pubmed(PMID):	32429376
Sentence Index:	32429376_6-7
Sentence:	Results from Western blotting also indicated that phosphorylation of PKCdelta and NF-kappaB -related proteins involved in tumor progression were effectively decreased by magnolol treatment. The invasion capacity of CRC cells was also attenuated by both magnolol and rottlerin.

Sequence & Structure:

MAPFLRIAFNSYELGSLQAEDEANQPFCAVKMKEALSTERGKTLVQKKPTMYPEWKSTFDAHIYEGRVIQIVLMRAAEEPVSEVTVGVSVLAERCKKNNGKAEFWLDLQPQAKVLMSVQYFLEDVDCKQSMRSEDEAKFPTMNRRGAIKQAKIHYIKNHEFIATFFGQPTFCSVCKDFVWGLNKQGYKCRQCNAAIHKKCIDKIIGRCTGTAANSRDTIFQKERFNIDMPHRFKVHNYMSPTFCDHCGSLLWGLVKQGLKCEDCGMNVHHKCREKVANLCGINQKLLAEALNQVTQRASRRSDSASSEPVGIYQGFEKKTGVAGEDMQDNSGTYGKIWEGSSKCNINNFIFHKVLGKGSFGKVLLGELKGRGEYFAIKALKKDVVLIDDDVECTMVEKRVLTLAAENPFLTHLICTFQTKDHLFFVMEFLNGGDLMYHIQDKGRFELYRATFYAAEIMCGLQFLHSKGIIYRDLKLDNVLLDRDGHIKIADFGMCKENIFGESRASTFCGTPDYIAPEILQGLKYTFSVDWWSFGVLLYEMLIGQSPFHGDDEDELFESIRVDTPHYPRWITKESKDILEKLFEREPTKRLGVTGNIKIHPFFKTINWTLLEKRRLEPPFRPKVKSPRDYSNFDQEFLNEKARLSYSDKNLIDSMDQSAFAGFSFVNPKFEHLLED

Select PDB:

Known Drugs:

source: Multi-Sources

(see table)

Target	Drug name	MOA	Phase	Status	Disease	Source
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	4	-	acute myeloid leukemia	FDA
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	4	-	neoplasm	ATC
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	4	-	mast-cell leukemia	DailyMed FDA
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	4	-	Mastocytosis	DailyMed
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	4	-	systemic mastocytosis	FDA
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	3	Recruiting	acute myeloid leukemia	ClinicalTrials ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	3	Completed	acute myeloid leukemia	ClinicalTrials ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	3	Unknown status	leukemia	ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Active, not recruiting	acute myeloid leukemia	ClinicalTrials ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Completed	acute myeloid leukemia	ClinicalTrials ClinicalTrials ClinicalTrials ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Recruiting	acute myeloid leukemia	ClinicalTrials ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Terminated	acute myeloid leukemia	ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Withdrawn	acute myeloid leukemia	ClinicalTrials ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Active, not recruiting	myelodysplastic syndrome	ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Recruiting	myelodysplastic syndrome	ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Completed	leukemia	ClinicalTrials
PRKCD	DELCASERTIB	Protein kinase C delta inhibitor	2	Completed	myocardial infarction	ClinicalTrials
PRKCD	UCN-01	Protein kinase C (PKC) inhibitor	2	Terminated	lymphoma	ClinicalTrials
PRKCD	SOTRASTAURIN	Protein kinase C (PKC) inhibitor	2	Completed	psoriasis	ClinicalTrials
PRKCD	UCN-01	Protein kinase C (PKC) inhibitor	2	Completed	small cell lung carcinoma	ClinicalTrials
PRKCD	SOTRASTAURIN	Protein kinase C (PKC) inhibitor	2	Completed	ulcerative colitis	ClinicalTrials
PRKCD	UCN-01	Protein kinase C (PKC) inhibitor	2	Terminated	melanoma	ClinicalTrials
PRKCD	UCN-01	Protein kinase C (PKC) inhibitor	2	Completed	pancreatic carcinoma	ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Completed	mast-cell leukemia	ClinicalTrials
PRKCD	MIDOSTAURIN	Protein kinase C (PKC) inhibitor	2	Recruiting	Blast Phase Chronic Myelogenous Leukemia, BCR-ABL1 Positive	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

PRKCD-Thr507
Cancer	Intensity
BRCA
COAD	-1.097
HGSC	0.862
ccRCC	0.235
GBM
HNSC
LUAD
LUSC
non_ccRCC
PDAC
UCEC

PTM-Disease Association:

source: PTMD

Residue	Position	State	Disease	Class	PMID
Y	52	A	Glioma/adult gliomas	Phosphorylation	11927579
Y	64	A	Glioma/adult gliomas	Phosphorylation	11927579
Y	155	A	Glioma/adult gliomas	Phosphorylation	11927579
T	505	P	Huntington's disease	Phosphorylation	23896721
T	505	U	Chronic lymphocytic leukemia	Phosphorylation	12393602
-	-	U	Chronic lymphocytic leukemia	Phosphorylation	20660292
Y	313	U	Colorectal cancer	Phosphorylation	24260357

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
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Afatinib	7.9987	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Afatinib	8.1559	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Afatinib	7.6297	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Dasatinib	12.2755	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Dasatinib	10.165	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Dasatinib	5.2618	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Dasatinib	8.2615	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Gefitinib	5.7367	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Gefitinib	7.7103	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Gefitinib	9.2754	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	A431	Gefitinib	2	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	K562	Dasatinib	10.4618	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	K562	Imatinib	7.712	-
Q05655	PRKCD	P	Thr507	AST(ph)FCGTPDYIAPEILQGLK	PC-9	AZD4547	5.7449	-

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