PMADS

Id:	acc2214
Group:	2sens
Protein:	PRAS40
Gene Symbol:	AKT1S1
Protein Id:	Q96B36
Protein Name:	AKTS1_HUMAN
PTM:	phosphorylation
Site:	Thr246
Site Sequence:	GDLPRPRLNTSDFQKLKRKY-
Disease Category:	Cancer
Disease:	Breast Cancer
Disease Subtype:
Disease Cellline:	BT474c
Disease Info:
Drug:	AZD5363
Drug Info:	"Capivasertib (AZD5363) is an orally active pan-AKT kinase inhibitor that inhibits Akt1, Akt2, and Akt3 with IC50 values of 3, 7, and 7 nM, respectively."
Effect:	modulate
Effect Info:	"AZD5363 can effectively reduce the growth of various tumor models. AZD5363 effectively inhibits the phosphorylation of S6 and 4E - BP1 in these cell lines, and at the same time increases the phosphorylation of AKT at the ser473 and thr308 sites."
Note:
Score:	4.0
Pubmed(PMID):	22294718
Sentence Index:	22294718_5-6
Sentence:	"Oral dosing of AZD5363 to nude mice caused dose- and time-dependent reduction of PRAS40, GSK3beta, and S6 phosphorylation in BT474c xenografts (PRAS40 phosphorylation EC(50) ~ 0.1 mumol/L total plasma exposure), reversible increases in blood glucose concentrations, and dose-dependent decreases in 2[18F]fluoro-2-deoxy-D-glucose ((18)F-FDG) uptake in U87-MG xenografts. Chronic oral dosing of AZD5363 caused dose-dependent growth inhibition of xenografts derived from various tumor types, including HER2(+) breast cancer models that are resistant to trastuzumab."

Sequence & Structure:

MASGRPEELWEAVVGAAERFRARTGTELVLLTAAPPPPPRPGPCAYAAHGRGALAEAARRCLHDIALAHRAATAARPPAPPPAPQPPSPTPSPPRPTLAREDNEEDEDEPTETETSGEQLGISDNGGLFVMDEDATLQDLPPFCESDPESTDDGSLSEETPAGPPTCSVPPASALPTQQYAKSLPVSVPVWGFKEKRTEARSSDEENGPPSSPDLDRIAASMRALVLREAEDTQVFGDLPRPRLNTSDFQKLKRKY

Select PDB:

Known Drugs:

source: Multi-Sources

(see table)

No data.

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

AKT1S1-Thr246
Cancer	Intensity
BRCA
COAD	-0.468
HGSC	0.953
ccRCC
GBM	-1.179
HNSC
LUAD
LUSC
non_ccRCC
PDAC
UCEC	0.694

PTM-Disease Association:

source: PTMD

Residue	Position	State	Disease	Class	PMID
T	246	P	Gastric cancer	Phosphorylation	24701227
T	246	U	Breast cancer	Phosphorylation	36797347
T	246	U	Cervical cancer/carcinoma	Phosphorylation	16174443
T	246	U	Sjogren's syndrome	Phosphorylation	34948236
T	246	U	Liver cancer	Phosphorylation	35058442

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
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A549	AZD8055	7.7295	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A549	Dactolisib	7.8299	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A549	Nintedanib	5.3092	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A549	Pictilisib	7.08	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A431	Dasatinib	6.2964	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	SK-BR-3	Lapatinib	7.9773	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	MDA-MB-175	Lapatinib	6.7493	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	BT-474	Lapatinib	6.4247	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	MDA-MB-175	Pertuzumab	-4.554	down
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	Ramos	Rituximab	-1.2537	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	K562	Dasatinib	9.0864	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	K562	Imatinib	7.5422	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	KYSE-520	SHP099	6.7746	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	MDA-MB-175	Trastuzumab	-0.1496	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	Ramos	Rituximab	-0.3957	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	Ramos	Rituximab	-2.9741	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	K562	Dasatinib	9.2526	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	Ramos	Rituximab	-2.821	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	SK-BR-3	Pertuzumab	-2.9561	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	SK-BR-3	Trastuzumab	-2.2203	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	SU-DHL-4	Rituximab	-3.2261	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	K562	Dasatinib	9.1109	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	K562	Dasatinib	8.7719	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	K562	Dasatinib	8.792	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	K562	Dasatinib	12.9407	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	HeLa	SAHA	5.8683	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	HeLa	A486	5.2478	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	HeLa	A485	14	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	BT-474	Trastuzumab	-1.46	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	BT-474	Pertuzumab	-4.7058	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	ARH-77	Rituximab	-1.277	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	ARH-77	Rituximab	-1.235	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	ARH-77	Rituximab	-1.1261	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A549	Tideglusib	6.3981	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A549	Dasatinib	6.8808	-
Q96B36	AKT1S1	P	Thr246	LNT(ph)SDFQK	A431	Imatinib	16.5229	-

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