Thrombin signaling through proteinase activated receptors (PARs) (Homo sapiens)

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Description

Thrombin activates proteinase activated receptors (PARs) that signal through heterotrimeric G proteins of the G12/13 and Gq families, thereby connecting to a host of intracellular signaling pathways. Thrombin activates PARs by cleaving an N-terminal peptide that then binds to the body of the receptor to effect transmembrane signaling. Intermolecular ligation of one PAR molecule by another can occur but is less efficient than self-ligation. A synthetic peptide of sequence SFLLRN, the first six amino acids of the new N-terminus generated when thrombin cleaves PAR1, can activate PAR1 independent of protease and receptor cleavage. PARs are key to platelet activation. Four PARs have been identified, of which PARs 1 ,3 and 4 are substrates for thrombin. In humans PAR 1 is the predominant thrombin receptor followed by PAR4 which is less responsive to thrombin. PAR 3 is not considered important for human platelet responses as it is minimally expressed, though this is not the case for mouse. PAR2 is not expressed in platelets. In mouse platelets, Gq is necessary for platelet secretion and aggregation in response to thrombin but is not necessary for thrombin-triggered shape change. G13 appears to contribute to platelet aggregation as well as shape change in response to low concentrations of thrombin but to be unnecessary at higher agonist concentrations; G12 appears to be dispensable for thrombin signaling in platelets. G alpha (q) activates phospholipase C beta thereby triggering phosphoinositide hydrolysis, calcium mobilization and protein kinase C activation. This provides a path to calcium-regulated kinases and phosphatases, GEFs, MAP kinase cassettes and other proteins that mediate cellular responses ranging from granule secretion, integrin activation, and aggregation in platelets. Gbeta:gamma subunits can activate phosphoinositide-3 kinase and other lipid modifying enzymes, protein kinases, and channels. PAR1 activation indirectly leads to activation of cell surface 'sheddases' that liberate ligands for receptor tyrosine kinases, providing a link between thrombin and receptor tyrosine kinases involved in cell growth and differentiation. The pleiotrophic effects of PAR activation are consistent with many of thrombin's diverse actions on cells. View original pathway at:Reactome.

Comments

Reactome-Converter: Pathway is converted from Reactome ID: 456926
Reactome-version: Reactome version: 64
Reactome Author: Reactome Author: Akkerman, Jan Willem N

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Bibliography

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Ogino Y, Tanaka K, Shimizu N.; ''Direct evidence for two distinct G proteins coupling with thrombin receptors in human neuroblastoma SH-EP cells.''; PubMed Europe PMC Scholia
Butkowski RJ, Elion J, Downing MR, Mann KG.; ''Primary structure of human prethrombin 2 and alpha-thrombin.''; PubMed Europe PMC Scholia
Ishihara H, Connolly AJ, Zeng D, Kahn ML, Zheng YW, Timmons C, Tram T, Coughlin SR.; ''Protease-activated receptor 3 is a second thrombin receptor in humans.''; PubMed Europe PMC Scholia
Coughlin SR.; ''Protease-activated receptors in hemostasis, thrombosis and vascular biology.''; PubMed Europe PMC Scholia
Luttrell LM, Ferguson SS, Daaka Y, Miller WE, Maudsley S, Della Rocca GJ, Lin F, Kawakatsu H, Owada K, Luttrell DK, Caron MG, Lefkowitz RJ.; ''Beta-arrestin-dependent formation of beta2 adrenergic receptor-Src protein kinase complexes.''; PubMed Europe PMC Scholia
Xu WF, Andersen H, Whitmore TE, Presnell SR, Yee DP, Ching A, Gilbert T, Davie EW, Foster DC.; ''Cloning and characterization of human protease-activated receptor 4.''; PubMed Europe PMC Scholia
Coughlin SR.; ''Thrombin signalling and protease-activated receptors.''; PubMed Europe PMC Scholia
Kuo FT, Lu TL, Fu HW.; ''Opposing effects of beta-arrestin1 and beta-arrestin2 on activation and degradation of Src induced by protease-activated receptor 1.''; PubMed Europe PMC Scholia
Vu TK, Hung DT, Wheaton VI, Coughlin SR.; ''Molecular cloning of a functional thrombin receptor reveals a novel proteolytic mechanism of receptor activation.''; PubMed Europe PMC Scholia
Offermanns S, Laugwitz KL, Spicher K, Schultz G.; ''G proteins of the G12 family are activated via thromboxane A2 and thrombin receptors in human platelets.''; PubMed Europe PMC Scholia
Degen SJ, Davie EW.; ''Nucleotide sequence of the gene for human prothrombin.''; PubMed Europe PMC Scholia
Lambert NA.; ''Dissociation of heterotrimeric g proteins in cells.''; PubMed Europe PMC Scholia

History

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Revision	Action	Time	User	Comment
116436	view	09:42, 7 May 2021	Eweitz	Modified title
114789	view	16:28, 25 January 2021	ReactomeTeam	Reactome version 75
113233	view	11:30, 2 November 2020	ReactomeTeam	Reactome version 74
112454	view	15:40, 9 October 2020	ReactomeTeam	Reactome version 73
101361	view	11:25, 1 November 2018	ReactomeTeam	reactome version 66
100899	view	20:59, 31 October 2018	ReactomeTeam	reactome version 65
100440	view	19:34, 31 October 2018	ReactomeTeam	reactome version 64
99989	view	16:18, 31 October 2018	ReactomeTeam	reactome version 63
99543	view	14:52, 31 October 2018	ReactomeTeam	reactome version 62 (2nd attempt)
99177	view	12:42, 31 October 2018	ReactomeTeam	reactome version 62
93866	view	13:41, 16 August 2017	ReactomeTeam	reactome version 61
93431	view	11:23, 9 August 2017	ReactomeTeam	reactome version 61
86523	view	09:20, 11 July 2016	ReactomeTeam	reactome version 56
83369	view	11:01, 18 November 2015	ReactomeTeam	Version54
81531	view	13:04, 21 August 2015	ReactomeTeam	Version53
77002	view	08:29, 17 July 2014	ReactomeTeam	Fixed remaining interactions
76707	view	12:07, 16 July 2014	ReactomeTeam	Fixed remaining interactions
76033	view	10:09, 11 June 2014	ReactomeTeam	Re-fixing comment source
75742	view	11:22, 10 June 2014	ReactomeTeam	Reactome 48 Update
75092	view	14:04, 8 May 2014	Anwesha	Fixing comment source for displaying WikiPathways description
74739	view	08:49, 30 April 2014	ReactomeTeam	Reactome46
68952	view	17:37, 8 July 2013	MaintBot	Updated to 2013 gpml schema
45083	view	20:47, 6 October 2011	Khanspers	Ontology Term : 'G protein mediated signaling pathway' added !
42144	view	22:00, 4 March 2011	MaintBot	Automatic update
39955	view	05:58, 21 January 2011	MaintBot	New pathway

External references

DataNodes

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Name	Type	Database reference	Comment
ARRB1	Protein	P49407 (Uniprot-TrEMBL)
ARRB1	Protein	P49407 (Uniprot-TrEMBL)
ARRB2	Protein	P32121 (Uniprot-TrEMBL)
ARRB2	Protein	P32121 (Uniprot-TrEMBL)
Activated PAR1:Beta-arrestin-1:Activated Src:Activated ERK	Complex	R-HSA-418210 (Reactome)
Activated PAR1:Beta-arrestin-1:Activated Src:ERK	Complex	R-HSA-418144 (Reactome)
Activated PAR1:Beta-arrestin-1:Src:ERK	Complex	R-HSA-418103 (Reactome)
Activated PAR1:Beta-arrestin-1	Complex	R-HSA-418080 (Reactome)
Activated PAR1:Beta-arrestin-2:Src:ERK	Complex	R-HSA-418179 (Reactome)
Activated PAR1:Beta-arrestin-2	Complex	R-HSA-418167 (Reactome)	Following receptor activation, PAR1 complexes with beta-arrestin. Beta-arrestins are adaptor proteins that play a central role in GPCR desensitization and internalization, and also act as scaffolds for the formation of signalling complexes that are independent of G-protein signalling.
Activated SRC-1	Protein	P12931-1 (Uniprot-TrEMBL)	This entity represents Src activated by an uncharacterised mechanism and phosphorylation state.
Ca2+	Metabolite	CHEBI:29108 (ChEBI)
F2R	Protein	P25116 (Uniprot-TrEMBL)
F2R(27-41)	Protein	P25116 (Uniprot-TrEMBL)	Thrombin recognizes the N-terminal exodomain of PAR1 by interacting with sites both amino and carboxyl terminal to the thrombin cleavage site. Thrombin cleaves the peptide bond between receptor residues Arg41 and Ser42. This serves to unmask a new amino terminus beginning with the sequence SFLLRN that functions as a tethered ligand, docking intramolecularly with the body of the receptor to effect transmembrane signaling. A synthetic peptide of sequence SFLLRN, which mimics the tethered ligand sequence, will function as an agonist for PAR1 independent of receptor cleavage. Thus PAR1 is, in essence, a peptide receptor that carries its own ligand, the latter being active only after receptor cleavage.
F2R(27-425)	Protein	P25116 (Uniprot-TrEMBL)	This is the inactive form of the receptor, before protease activation. Proteinase (protease) activated receptors are activated by the cleavage of an N-terminal extracellular segment by serine proteases, particularly thrombin which activates PAR1, 3 and 4. The cleaved fragment is an activating ligand for the receptor; synthetic peptide mimics of the N-terminal fragment can activate uncleaved receptors.
F2RL2	Protein	O00254 (Uniprot-TrEMBL)
F2RL2(22-374)	Protein	O00254 (Uniprot-TrEMBL)	This is the inactive form of the receptor, before protease activation. Proteinase (protease) activated receptors are activated by the cleavage of an N-terminal extracellular segment by serine proteases, particularly thrombin which activates PAR1, 3 and 4. The cleaved fragment is an activating ligand for the receptor; synthetic peptide mimics of the N-terminal fragment can activate uncleaved receptors.
F2RL2(22-38)	Protein	O00254 (Uniprot-TrEMBL)
F2RL3	Protein	Q96RI0 (Uniprot-TrEMBL)
F2RL3(18-385)	Protein	Q96RI0 (Uniprot-TrEMBL)	This is the inactive form of the receptor, before protease activation. Proteinase (protease) activated receptors are activated by the cleavage of an N-terminal extracellular segment by serine proteases, particularly thrombin which activates PAR1, 3 and 4. The cleaved fragment is an activating ligand for the receptor; synthetic peptide mimics of the N-terminal fragment can activate uncleaved receptors.
F2RL3(18-47)	Protein	Q96RI0 (Uniprot-TrEMBL)
F2R	Protein	P25116 (Uniprot-TrEMBL)
G-protein G12/G13 (inactive)	Complex	R-HSA-398082 (Reactome)
G-protein alpha (12/13):GTP	Complex	R-HSA-418572 (Reactome)
G-protein alpha (q/11): GTP	Complex	R-HSA-114534 (Reactome)
G-protein beta-gamma complex	Complex	R-HSA-167434 (Reactome)
GDP	Metabolite	CHEBI:17552 (ChEBI)
GDP	Metabolite	CHEBI:17552 (ChEBI)
GNA11	Protein	P29992 (Uniprot-TrEMBL)
GNA12	Protein	Q03113 (Uniprot-TrEMBL)
GNA13	Protein	Q14344 (Uniprot-TrEMBL)
GNA14	Protein	O95837 (Uniprot-TrEMBL)
GNA15	Protein	P30679 (Uniprot-TrEMBL)
GNAQ	Protein	P50148 (Uniprot-TrEMBL)
GNB1	Protein	P62873 (Uniprot-TrEMBL)
GNB2	Protein	P62879 (Uniprot-TrEMBL)
GNB3	Protein	P16520 (Uniprot-TrEMBL)
GNB4	Protein	Q9HAV0 (Uniprot-TrEMBL)
GNB5	Protein	O14775 (Uniprot-TrEMBL)
GNG10	Protein	P50151 (Uniprot-TrEMBL)
GNG11	Protein	P61952 (Uniprot-TrEMBL)
GNG12	Protein	Q9UBI6 (Uniprot-TrEMBL)
GNG13	Protein	Q9P2W3 (Uniprot-TrEMBL)
GNG2	Protein	P59768 (Uniprot-TrEMBL)
GNG3	Protein	P63215 (Uniprot-TrEMBL)
GNG4	Protein	P50150 (Uniprot-TrEMBL)
GNG5	Protein	P63218 (Uniprot-TrEMBL)
GNG7	Protein	O60262 (Uniprot-TrEMBL)
GNG8	Protein	Q9UK08 (Uniprot-TrEMBL)
GNGT1	Protein	P63211 (Uniprot-TrEMBL)
GNGT2	Protein	O14610 (Uniprot-TrEMBL)
GTP	Metabolite	CHEBI:15996 (ChEBI)
GTP	Metabolite	CHEBI:15996 (ChEBI)
Heterotrimeric G-protein Gq/11 (inactive)	Complex	R-HSA-114557 (Reactome)
MAPK1	Protein	P28482 (Uniprot-TrEMBL)
MAPK3	Protein	P27361 (Uniprot-TrEMBL)
MAPKs	Complex	R-HSA-169291 (Reactome)
PAR N-teminal fragments	Complex	R-HSA-453303 (Reactome)
PAR1, 3, 4	Complex	R-HSA-453302 (Reactome)
SRC-1	Protein	P12931-1 (Uniprot-TrEMBL)
SRC-1	Protein	P12931-1 (Uniprot-TrEMBL)
Thrombin activated PAR:G12/13 (inactive)	Complex	R-HSA-397883 (Reactome)
Thrombin activated PAR:G12/13 (active)	Complex	R-HSA-397884 (Reactome)
Thrombin-activated PAR:Gq (active)	Complex	R-HSA-397802 (Reactome)
Thrombin-activated PAR:Gq (inactive)	Complex	R-HSA-397803 (Reactome)
Thrombin-activated PAR	Complex	R-HSA-114530 (Reactome)
activated thrombin (factor IIa)	Complex	R-HSA-156786 (Reactome)
p-T185,Y187-MAPK1	Protein	P28482 (Uniprot-TrEMBL)
p-T202,Y204-MAPK3	Protein	P27361 (Uniprot-TrEMBL)
thrombin heavy chain	Protein	P00734 (Uniprot-TrEMBL)
thrombin light chain	Protein	P00734 (Uniprot-TrEMBL)

Annotated Interactions

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Source	Target	Type	Database reference	Comment
ARRB1			R-HSA-418091 (Reactome)
ARRB2			R-HSA-418172 (Reactome)
	Activated PAR1:Beta-arrestin-1:Activated Src:Activated ERK	Arrow	R-HSA-418163 (Reactome)
	Activated PAR1:Beta-arrestin-1:Activated Src:ERK	Arrow	R-HSA-418158 (Reactome)
Activated PAR1:Beta-arrestin-1:Activated Src:ERK			R-HSA-418163 (Reactome)
Activated PAR1:Beta-arrestin-1:Activated Src:ERK		mim-catalysis	R-HSA-418163 (Reactome)
	Activated PAR1:Beta-arrestin-1:Src:ERK	Arrow	R-HSA-418170 (Reactome)
Activated PAR1:Beta-arrestin-1:Src:ERK			R-HSA-418158 (Reactome)
	Activated PAR1:Beta-arrestin-1	Arrow	R-HSA-418091 (Reactome)
Activated PAR1:Beta-arrestin-1			R-HSA-418170 (Reactome)
	Activated PAR1:Beta-arrestin-2:Src:ERK	Arrow	R-HSA-418176 (Reactome)
	Activated PAR1:Beta-arrestin-2:Src:ERK	Arrow	R-HSA-418200 (Reactome)
Activated PAR1:Beta-arrestin-2:Src:ERK			R-HSA-418200 (Reactome)
	Activated PAR1:Beta-arrestin-2	Arrow	R-HSA-418172 (Reactome)
Activated PAR1:Beta-arrestin-2			R-HSA-418176 (Reactome)
F2R			R-HSA-418091 (Reactome)
F2R			R-HSA-418172 (Reactome)
G-protein G12/G13 (inactive)			R-HSA-396941 (Reactome)
	G-protein alpha (12/13):GTP	Arrow	R-HSA-397891 (Reactome)
	G-protein alpha (q/11): GTP	Arrow	R-HSA-397835 (Reactome)
	G-protein beta-gamma complex	Arrow	R-HSA-397835 (Reactome)
	G-protein beta-gamma complex	Arrow	R-HSA-397891 (Reactome)
	GDP	Arrow	R-HSA-114552 (Reactome)
	GDP	Arrow	R-HSA-114558 (Reactome)
GTP			R-HSA-114552 (Reactome)
GTP			R-HSA-114558 (Reactome)
Heterotrimeric G-protein Gq/11 (inactive)			R-HSA-396996 (Reactome)
MAPKs			R-HSA-418170 (Reactome)
MAPKs			R-HSA-418176 (Reactome)
	PAR N-teminal fragments	Arrow	R-HSA-114697 (Reactome)
PAR1, 3, 4			R-HSA-114697 (Reactome)
			R-HSA-114552 (Reactome)	PAR1, 3 and 4 have been shown to directly couple with G12/13 (Offermanns et al. 1994). G12 and G13 have overlapping but distinct signalling roles (Suzuki et al. 2009). Evidence from conditional knockout mice (KOs) suggests that G13 is the subtype responsible for platelet shape change and aggregation responses in response to low and intermediate concentrations of thrombin, thromboxane and collagen. Platelets from G12 KOs were indistinguishable from wild-type, while those from mice with disrupted G13 had impaired shape change and aggregation responses, failed to form stable thrombi ex vivo, and exhibited a large increase in tailbleeding times (Moers et al. 2003). Both subtypes of G12/13 are unnecessary for platelet shape change and aggregation at higher agonist concentrations. The alpha-subunits of G12 and 13 bind RhoGEFs (guanine nucleotide exchange factors, which activate small G proteins) providing a path to Rho-mediated cytoskeletal responses that are involved in shape change in platelets and permeability and migration in endothelial cells.
			R-HSA-114558 (Reactome)	Activated PAR stimulates the G alpha (q) subunit to release GDP and bind GTP (which is present in much greater concentrations physiologically). This activation is required for Gq to participate in downstream signalling events.
			R-HSA-114697 (Reactome)	Thrombin signaling is mediated at least in part by a small family of G protein-coupled Proteinase Activated Receptors (PARs). Human platelet activation by thrombin is mediated predominantly by PAR1; PAR4-induced platelet responses are less pronounced. PAR2 is not present in human platelets. PARs 1, 3 and 4 are activated when thrombin cleaves an N-terminal exodomain. This cleavage event unmasks a new N-terminus that serves as a tethered ligand that binds intramolecularly to the body of the receptor to effect transmembrane signaling. Intermolecular ligation of one PAR molecule by another can occur but, not surprisingly, appears to be less efficient than self-ligation. A synthetic peptide of sequence SFLLRN, the first six amino acids of the new N-terminus generated when thrombin cleaves PAR1, can activate PAR1 independent of protease and receptor cleavage. In addition to providing evidence for the tethered ligand mechanism, such tethered ligand-mimicking peptides have provided a convenient pharmacological tool for probing the effects of PAR activation in cells and tissues.
			R-HSA-396941 (Reactome)	Thrombin receptors activate G-proteins in the G12/13 family. Gq knockout mice exhibit defective platelet activation, but retain shape change responses to thrombin, mediated by G12/13.
			R-HSA-396996 (Reactome)	Thrombin signalling through PARs is mediated in part through the Gq family of G-proteins. Gq knockout mice have defective platelet responses to thrombin (as well as to ADP and thromboxane).
			R-HSA-397835 (Reactome)	The classical view of G-protein signalling is that the G-protein alpha subunit dissociates from the beta:gamma dimer. Activated G alpha (s) and the beta:gamma dimer then participate in separate signaling cascades. Although G protein dissociation has been contested (e.g. Bassi et al. 1996), recent in vivo experiments have demonstrated that dissociation does occur, though possibly not to completion (Lambert 2008).
			R-HSA-397891 (Reactome)	The classical view of G-protein signalling is that the G-protein alpha subunit dissociates from the beta:gamma dimer. Activated G alpha (s) and the beta:gamma dimer then participate in separate signaling cascades. Although G protein dissociation has been contested (e.g. Bassi et al. 1996), recent in vivo experiments have demonstrated that dissociation does occur, though possibly not to completion (Lambert 2008).
			R-HSA-418091 (Reactome)	Following receptor activation, PAR1 complexes with beta-arrestin. Beta-arrestins are adaptor proteins that play a central role in GPCR desensitization and internalization, and also act as scaffolds for the formation of signalling complexes that are independent of G-protein signalling.
			R-HSA-418158 (Reactome)	The activity of Src-kinase is increased when bound to Beta-arrestin-1. The mechanism for this activation is not clear. Src bound to beta -arrestin 1 is substantially dephosphorylated at Tyr530 and this is often associated with Src activation. Binding results with Y530F mutants of Src suggest that binding of Src to arrestin causes a conformational activation of the kinase, rather than a change in phosphorylation. However, increased phosphorylation of Src Tyr419 in cells overexpressing beta-arrestin-1 has been reported to correlate with PAR1 activation, beta-arrestin signalling complex formation, and increased ERK activation.
			R-HSA-418163 (Reactome)	Within the beta-arrestin-1:Src:ERK complex, activated Src phosphorylates and activates ERK. ERK activation requires dual Thr and Tyr phosphorylations, at Thr202/Tyr204 for human ERK1 and Thr185/Tyr187 for human ERK2. Significant ERK activation requires phosphorylation at both sites, with Tyr phosphorylation preceding that of Thr. This reaction is given as a black-box event because the phosphorylation state of ERK on binding to beta-arrestin-1 is unknown.
			R-HSA-418170 (Reactome)	Beta-arrestins can serve as scaffolding molecules that facilitate G-protein independent cell signaling
			R-HSA-418172 (Reactome)	Following receptor activation, PAR1 complexes with beta-arrestin. Beta-arrestins are adaptor proteins that play a central role in GPCR desensitization and internalization, and also act as scaffolds for the formation of signalling complexes that are independent of G-protein signalling.
			R-HSA-418176 (Reactome)	Beta-arrestins can serve as scaffolding molecules that facilitate G-protein independent cell signaling
			R-HSA-418200 (Reactome)	Activated PAR1 can induce the formation of signalling complexes with a beta-arrestin scaffold. When beta-arrestin-1 is incorporated this leads to Src and subsequent ERK activation. In contrast, complexes containing beta-arrestin-2 do not lead to Src and ERK activation.
SRC-1			R-HSA-418170 (Reactome)
SRC-1			R-HSA-418176 (Reactome)
	Thrombin activated PAR:G12/13 (inactive)	Arrow	R-HSA-396941 (Reactome)
Thrombin activated PAR:G12/13 (inactive)			R-HSA-114552 (Reactome)
	Thrombin activated PAR:G12/13 (active)	Arrow	R-HSA-114552 (Reactome)
Thrombin activated PAR:G12/13 (active)			R-HSA-397891 (Reactome)
	Thrombin-activated PAR:Gq (active)	Arrow	R-HSA-114558 (Reactome)
Thrombin-activated PAR:Gq (active)			R-HSA-397835 (Reactome)
	Thrombin-activated PAR:Gq (inactive)	Arrow	R-HSA-396996 (Reactome)
Thrombin-activated PAR:Gq (inactive)			R-HSA-114558 (Reactome)
	Thrombin-activated PAR	Arrow	R-HSA-114697 (Reactome)
	Thrombin-activated PAR	Arrow	R-HSA-397835 (Reactome)
	Thrombin-activated PAR	Arrow	R-HSA-397891 (Reactome)
Thrombin-activated PAR			R-HSA-396941 (Reactome)
Thrombin-activated PAR			R-HSA-396996 (Reactome)
Thrombin-activated PAR		mim-catalysis	R-HSA-114552 (Reactome)
Thrombin-activated PAR		mim-catalysis	R-HSA-114558 (Reactome)
activated thrombin (factor IIa)		mim-catalysis	R-HSA-114697 (Reactome)

Thrombin signaling through proteinase activated receptors (PARs) (Homo sapiens)

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