Prolactin receptor signaling (Homo sapiens)

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3-518102, 67898pActivated PRLRJAK2 dimer PRLR ligandspPRLR ligandspPRLR ligandspPlacental lactogen Activated PRLRJAK2 pActivated PRLRpProlactin receptor ligands PRLRJAK2 Prolactin receptor ligands PRLR ligandsActivated PRLRJAK2 dimer Prolactin receptor ligands pActivated Growth Hormone ReceptorppPRLRJAK2 dimer PRLR ligandspPlacental lactogen Growth Hormone Placental lactogen Prolactin receptor ligands Activated PRLRJAK2 dimer Placental lactogen Growth Hormone p-STAT5A/B ppPRLR ligandspGrowth Hormone PRLR ligandspPlacental lactogen PRLRJAK2 dimer pPlacental lactogen Placental lactogen Placental lactogen Growth Hormone pPRLRJAK2 Activated PRLRJAK2 Prolactin receptor ligands PRLRJAK2 Prolactin receptor ligands PRLR ligandspProlactin receptor ligands Activated Growth Hormone ReceptorJAK2 dimer PRLR ligandsActivated PRLRJAK2 dimerSH2B1 beta ppPRLR ligandspPlacental lactogen Growth Hormone pActivated Growth Hormone ReceptorpSCF beta-TrCP complex pActivated PRLRJAK2 Prolactin receptor ligands SCF beta-TrCP complex PRLR ligandspGrowth Hormone Placental lactogen PRLR ligandspActivated PRLRpPlacental lactogen Activated cytokine-like hormone receptors Growth Hormone PRLR ligandsActivated PRLRJAK2 dimer PRLR ligandsActivated PRLRpGrowth Hormone cytosolPRLR ligandsActivated PRLRJAK2 dimer Activated PRLRJAK2 dimer Growth Hormone Prolactin receptor ligands Growth Hormone Activated Growth Hormone Receptor-JAK2 dimer STAT5 Activated PRLRpProlactin receptor ligands Growth Hormone Activated cytokine-like hormone receptors, pPRLR ligandsppActivated PRLRppPlacental lactogen Placental lactogen PRLR ligandsActivated PRLRpGrowth Hormone Growth Hormone PRLR ligandsPRLRJAK2 dimer PRLR ligandsppProlactin receptor ligands PRLR ligandspProlactin receptor ligands Activated Growth Hormone ReceptorJAK2 Growth Hormone Prolactin receptor ligands Placental lactogen Prolactin receptor ligands Growth Hormone Activated Growth Hormone Receptor- pendosome lumenpGrowth Hormone SKP1 PRLR ADPGH2 JAK2 p-Y1007-JAK2 PRLR ligandspp-Y1007-JAK2 PRL JAK2 JAK2 ATPGH2 Zn2+ PRL CSH1 PRL CSH1 PRL PRLR ligandspADPp-Y611-PRLR RBX1 PRL PRLR PRLR PRLR ligandsActivated PRLRJAK2 dimerSH2B1 betaATPp-Y1007-JAK2 PRLR PRLR ligandspCUL1 Zn2+ PRLR ligandspGH2 BTRC JAK2 ADPPRLR ligandspGH2 p-Y1007-JAK2 Zn2+ PRL GH1 GH1 GHR activated PRLR PTPN11Zn2+ Zn2+ Activated cytokine-like hormone receptors, pZn2+ GH2 JAK2 GH2 GH2 p-Y1007-JAK2 STAT5GH1 p-Y611-PRLR CUL1 CSH1 Zn2+ Zn2+ GH1 RBX1 CSH1 GH2 JAK2 PRLRPRLR ligandspSH2B1-2p-Y611-PRLR p-Y1007-JAK2 PRLR ligandsActivated PRLRJAK2 dimerGH1 PRL GH1 CSH1 PRLR SKP1 PRL Zn2+ ATPp-Y611-PRLR GH2 PRLRJAK2 dimerPRL GH2 PRLR ligandsPRLRJAK2 dimerADPPRLR ligandspATPPRL p-Y611-PRLR GH1 Prolactin receptor ligandsPTPN11 GH1 p-Y611-PRLR GH1 ATPPRL JAK2 GH1 PRLR GH1 CSH1 PRL p-Y546-PTPN11 GHR activated Zn2+ GH2 CSH1 JAK2JAK2 p-Y1007-JAK2 p-Y699-STAT5B PRLR ligandsActivated PRLRpSCF beta-TrCP complexSTAT5A p-Y694-STAT5A STAT5B PRLRJAK2GH2 p-Y611-PRLR PRL CSH1 JAK2 PRLR ligandspp-Y611-PRLR CSH1 Zn2+ GH1 CSH1 Zn2+ CSH1 PRLR Zn2+ CSH1 GH1 BTRC GH1 GH2 CSH1 GH2 CSH1 ADPActivated cytokine-like hormone receptorsSH2B1-2 Zn2+


Description

Prolactin (PRL) is a hormone secreted mainly by the anterior pituitary gland. It was originally identified by its ability to stimulate the development of the mammary gland and lactation, but is now known to have numerous and varied functions (Bole-Feysot et al. 1998). Despite this, few pathologies have been associated with abnormalities in prolactin receptor (PRLR) signaling, though roles in various forms of cancer and certain autoimmune disorders have been suggested (Goffin et al. 2002). A vast body of literature suggests effects of PRL in immune cells (Matera 1996) but PRLR KO mice have unaltered immune system development and function (Bouchard et al. 1999). In addition to the pituitary, numerous other tissues produce PRL, including the decidua and myometrium, certain cells of the immune system, brain, skin and exocrine glands such as the mammary, sweat and lacrimal glands (Ben-Jonathan et al. 1996). Pituitary PRL secretion is negatively regulated by inhibitory factors originating from the hypothalamus, the most important of which is dopamine, acting through the D2 subclass of dopamine receptors present in lactotrophs (Freeman et al. 2000). PRL-binding sites or receptors have been identified in numerous cells and tissues of adult mammals. Various forms of PRLR, generated by alternative splicing, have been reported in several species including humans (Kelly et al. 1991, Clevenger et al. 2003).

PRLR is a member of the cytokine receptor superfamily. Like many other members of this family, the first step in receptor activation was generally believed to be ligand-induced dimerization whereby one molecule of PRL bound to two molecules of receptor (Elkins et al. 2000). Recent reports suggest that PRLR pre-assembles at the plasma membrane in the absence of ligand (Gadd & Clevenger 2006, Tallet et al. 2011), suggesting that ligand-induced activation involves conformational changes in preformed PRLR dimers (Broutin et al. 2010).

PRLR has no intrinsic kinase activity but associates (Lebrun et al. 1994, 1995) with Janus kinase 2 (JAK2) which is activated following receptor activation (Campbell et al. 1994, Rui et al. 1994, Carter-Su et al. 2000, Barua et al. 2009). JAK2-dependent activation of JAK1 has also been reported (Neilson et al. 2007). It is generally accepted that activation of JAK2 occurs by transphosphorylation upon ligand-induced receptor activation, based on JAK activation by chimeric receptors in which various extracellular domains of cytokine or tyrosine kinase receptors were fused to the IL-2 receptor beta chain (see Ihle et al. 1994). This activation step involves the tyrosine phosphorylation of JAK2, which in turn phosphorylates PRLR on specific intracellular tyrosine residues leading to STAT5 recruitment and signaling, considered to be the most important signaling cascade for PRLR. STAT1 and STAT3 activation have also been reported (DaSilva et al. 1996) as have many other signaling pathways; signaling through MAP kinases (Shc/SOS/Grb2/Ras/Raf/MAPK) has been reported as a consequence of PRL stimuilation in many different cellular systems (see Bole-Feysot et al. 1998) though it is not clear how this signal is propagated. Other cascades non exhaustively include Src kinases, Focal adhesion kinase, phospholipase C gamma, PI3 kinase/Akt and Nek3 (Clevenger et al. 2003, Miller et al. 2007). The protein tyrosine phosphatase SHP2 is recruited to the C terminal tyrosine of PRLR and may have a regulatory role (Ali & Ali 2000). PRLR phosphotyrosines can recruit insulin receptor substrates (IRS) and other adaptor proteins to the receptor complex (Bole-Feysot et al. 1998).

Female homozygous PRLR knockout mice are completely infertile and show a lack of mammary development (Ormandy et al. 1997). Hemizogotes are unable to lactate following their first pregnancy and depending on the genetic background, this phenotype can persist through subsequent pregnancies (Kelly et al. 2001). Original Pathway at Reactome: http://www.reactome.org/PathwayBrowser/#DB=gk_current&FOCUS_SPECIES_ID=48887&FOCUS_PATHWAY_ID=1170546

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Bibliography

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  1. Kelly PA, Binart N, Freemark M, Lucas B, Goffin V, Bouchard B.; ''Prolactin receptor signal transduction pathways and actions determined in prolactin receptor knockout mice.''; PubMed Europe PMC Scholia
  2. Walsh ST, Kossiakoff AA.; ''Crystal structure and site 1 binding energetics of human placental lactogen.''; PubMed Europe PMC Scholia
  3. Lebrun JJ, Ali S, Sofer L, Ullrich A, Kelly PA.; ''Prolactin-induced proliferation of Nb2 cells involves tyrosine phosphorylation of the prolactin receptor and its associated tyrosine kinase JAK2.''; PubMed Europe PMC Scholia
  4. Nishi M, Werner ED, Oh BC, Frantz JD, Dhe-Paganon S, Hansen L, Lee J, Shoelson SE.; ''Kinase activation through dimerization by human SH2-B.''; PubMed Europe PMC Scholia
  5. Gadd SL, Clevenger CV.; ''Ligand-independent dimerization of the human prolactin receptor isoforms: functional implications.''; PubMed Europe PMC Scholia
  6. Goffin V, Binart N, Touraine P, Kelly PA.; ''Prolactin: the new biology of an old hormone.''; PubMed Europe PMC Scholia
  7. Argetsinger LS, Campbell GS, Yang X, Witthuhn BA, Silvennoinen O, Ihle JN, Carter-Su C.; ''Identification of JAK2 as a growth hormone receptor-associated tyrosine kinase.''; PubMed Europe PMC Scholia
  8. Tallet E, Fernandez I, Zhang C, Salsac M, Gregor N, Ayoub MA, Pin JP, Trinquet E, Goffin V.; ''Investigation of prolactin receptor activation and blockade using time-resolved fluorescence resonance energy transfer.''; PubMed Europe PMC Scholia
  9. Broutin I, Jomain JB, Tallet E, van Agthoven J, Raynal B, Hoos S, Kragelund BB, Kelly PA, Ducruix A, England P, Goffin V.; ''Crystal structure of an affinity-matured prolactin complexed to its dimerized receptor reveals the topology of hormone binding site 2.''; PubMed Europe PMC Scholia
  10. Bole-Feysot C, Goffin V, Edery M, Binart N, Kelly PA.; ''Prolactin (PRL) and its receptor: actions, signal transduction pathways and phenotypes observed in PRL receptor knockout mice.''; PubMed Europe PMC Scholia
  11. Li Y, Kumar KG, Tang W, Spiegelman VS, Fuchs SY.; ''Negative regulation of prolactin receptor stability and signaling mediated by SCF(beta-TrCP) E3 ubiquitin ligase.''; PubMed Europe PMC Scholia

History

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114990view16:52, 25 January 2021ReactomeTeamReactome version 75
113434view11:51, 2 November 2020ReactomeTeamReactome version 74
112637view16:02, 9 October 2020ReactomeTeamReactome version 73
101552view11:41, 1 November 2018ReactomeTeamreactome version 66
101088view21:25, 31 October 2018ReactomeTeamreactome version 65
100617view19:59, 31 October 2018ReactomeTeamreactome version 64
100168view16:44, 31 October 2018ReactomeTeamreactome version 63
99718view15:11, 31 October 2018ReactomeTeamreactome version 62 (2nd attempt)
99294view12:46, 31 October 2018ReactomeTeamreactome version 62
93741view13:33, 16 August 2017ReactomeTeamreactome version 61
93255view11:18, 9 August 2017ReactomeTeamreactome version 61
88119view10:09, 26 July 2016RyanmillerOntology Term : 'cytokine mediated signaling pathway' added !
88118view10:09, 26 July 2016RyanmillerOntology Term : 'cytokine and chemokine mediated signaling pathway' added !
88117view10:08, 26 July 2016RyanmillerOntology Term : 'signaling pathway' added !
86333view09:15, 11 July 2016ReactomeTeamreactome version 56
83281view10:37, 18 November 2015ReactomeTeamVersion54
81403view12:55, 21 August 2015ReactomeTeamVersion53
78711view14:25, 18 January 2015EgonwRemoved a @GroupRef to a that didn't exist in the GPML.
76870view08:14, 17 July 2014ReactomeTeamFixed remaining interactions
76575view11:55, 16 July 2014ReactomeTeamFixed remaining interactions
75908view09:56, 11 June 2014ReactomeTeamRe-fixing comment source
75608view10:46, 10 June 2014ReactomeTeamReactome 48 Update
74963view13:48, 8 May 2014AnweshaFixing comment source for displaying WikiPathways description
74607view08:39, 30 April 2014ReactomeTeamNew pathway

External references

DataNodes

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NameTypeDatabase referenceComment
ADPMetaboliteCHEBI:16761 (ChEBI)
ATPMetaboliteCHEBI:15422 (ChEBI)
Activated cytokine-like hormone receptors, pComplexREACT_111453 (Reactome)
Activated cytokine-like hormone receptorsComplexREACT_111865 (Reactome)
BTRC ProteinQ9Y297 (Uniprot-TrEMBL)
CSH1 ProteinP01243 (Uniprot-TrEMBL)
CUL1 ProteinQ13616 (Uniprot-TrEMBL)
GH1 ProteinP01241 (Uniprot-TrEMBL) Growth hormone is typically used to refer to the endogenous hormone - somatotropin is reserved for synthetic hormone produced by recombinant technology.
GH2 ProteinP01242 (Uniprot-TrEMBL)
GHR activated ProteinP10912 (Uniprot-TrEMBL)
JAK2 ProteinO60674 (Uniprot-TrEMBL)
JAK2ProteinO60674 (Uniprot-TrEMBL)
PRL Protein
PRL ProteinP01236 (Uniprot-TrEMBL)
PRLR JAK2 dimerComplexREACT_117889 (Reactome)
PRLR JAK2ComplexREACT_111285 (Reactome)
PRLR ProteinP16471 (Uniprot-TrEMBL)
PRLR ligands

Activated PRLR JAK2 dimer

SH2B1 beta
ComplexREACT_116998 (Reactome)
PRLR ligands

Activated PRLR

JAK2 dimer
ComplexREACT_111809 (Reactome)
PRLR ligands

Activated PRLR

p
ComplexREACT_117043 (Reactome)
PRLR ligands

PRLR

JAK2 dimer
ComplexREACT_116278 (Reactome)
PRLR ligands pComplexREACT_116867 (Reactome)
PRLR ligands pComplexREACT_116992 (Reactome)
PRLR ligands pComplexREACT_117018 (Reactome)
PRLR ligands pComplexREACT_117024 (Reactome)
PRLR ligands pComplexREACT_117210 (Reactome)
PRLR ligands pComplexREACT_117494 (Reactome)
PRLR ligands pComplexREACT_117717 (Reactome)
PRLR ligands pComplexREACT_117721 (Reactome)
PRLRProteinP16471 (Uniprot-TrEMBL)
PTPN11 ProteinQ06124 (Uniprot-TrEMBL)
PTPN11ProteinQ06124 (Uniprot-TrEMBL)
Prolactin receptor ligandsComplexREACT_111382 (Reactome)
RBX1 ProteinP62877 (Uniprot-TrEMBL)
SCF beta-TrCP complexComplexREACT_22981 (Reactome)
SH2B1-2 ProteinQ9NRF2-2 (Uniprot-TrEMBL)
SH2B1-2ProteinQ9NRF2-2 (Uniprot-TrEMBL)
SKP1 ProteinP63208 (Uniprot-TrEMBL)
STAT5A ProteinP42229 (Uniprot-TrEMBL)
STAT5B ProteinP51692 (Uniprot-TrEMBL)
STAT5ProteinREACT_24211 (Reactome)
Zn2+ MetaboliteCHEBI:29105 (ChEBI)
p-Y1007-JAK2 ProteinO60674 (Uniprot-TrEMBL)
p-Y546-PTPN11 ProteinQ06124 (Uniprot-TrEMBL)
p-Y611-PRLR ProteinP16471 (Uniprot-TrEMBL)
p-Y694-STAT5A ProteinP42229 (Uniprot-TrEMBL)
p-Y699-STAT5B ProteinP51692 (Uniprot-TrEMBL)

Annotated Interactions

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SourceTargetTypeDatabase referenceComment
ADPArrowREACT_111076 (Reactome)
ADPArrowREACT_115719 (Reactome)
ADPArrowREACT_115844 (Reactome)
ADPArrowREACT_115938 (Reactome)
ADPArrowREACT_116161 (Reactome)
ATPREACT_111076 (Reactome)
ATPREACT_115719 (Reactome)
ATPREACT_115844 (Reactome)
ATPREACT_115938 (Reactome)
ATPREACT_116161 (Reactome)
Activated cytokine-like hormone receptors, pArrowREACT_111076 (Reactome)
Activated cytokine-like hormone receptorsREACT_111076 (Reactome)
JAK2REACT_116102 (Reactome)
PRLR JAK2 dimerREACT_116060 (Reactome)
PRLR ligands

Activated PRLR JAK2 dimer

SH2B1 beta
ArrowREACT_111076 (Reactome)
PRLR ligands

Activated PRLR

JAK2 dimer
REACT_115792 (Reactome)
PRLR ligands

Activated PRLR

JAK2 dimer
REACT_115844 (Reactome)
PRLR ligands

Activated PRLR

p
REACT_116161 (Reactome)
PRLR ligands pArrowREACT_115719 (Reactome)
PRLR ligands pArrowREACT_115844 (Reactome)
PRLR ligands pArrowREACT_115907 (Reactome)
PRLR ligands pArrowREACT_115938 (Reactome)
PRLR ligands pArrowREACT_116161 (Reactome)
PRLR ligands pREACT_115719 (Reactome)
PRLR ligands pREACT_115782 (Reactome)
PRLR ligands pREACT_115790 (Reactome)
PRLR ligands pREACT_115938 (Reactome)
PRLR ligands pREACT_116156 (Reactome)
PRLR ligands pTBarREACT_116060 (Reactome)
PRLRREACT_116102 (Reactome)
PTPN11REACT_115782 (Reactome)
Prolactin receptor ligandsREACT_116060 (Reactome)
REACT_111076 (Reactome) Similar models explain JAK activation by the cytokine-like hormone receptors (GHR and PRLR) and interleukin receptors. JAK2 activation is believed to occur as mutual transactivation whereby JAK2 bound to one receptor chain phosphorylates JAK2 bound to the other receptor chain in the dimeric receptor. Transactivation is widely accepted (Herrington & Carter-Su 2001) having been originally proposed in the 1990's (Quelle et al. 1994, Hou et al. 2002). JAK phosphorylation is thought to lock the kinase domain in an active state; prior to this JAK2 is held in an inactive state by interactions between its kinase and pseudokinase domains (Giordanetto & Kroemer 2002). Although there are structures of JAK kinase domains (e.g. Lucet et al. 2006), no complete JAK structures are available and the activation mechanism remains poorly understood (Brooks & Waters 2010). The trigger for JAK activation is believed to be a conformational change in the receptor when ligand is bound, leading to a rotation of the cytoplasmic regions which brings the catalytic domains of bound JAK2 molecules into close proximity and frees them from inhibition by the pseudokinase domains. Supporting observations for cytokine-like hormone receptors include: JAK2 becomes tyrosine phosphorylated as a consequence of GHR activation by GH (Argetsinger et al. 1993); JAK2 is activated following PRLR activation (Campbell et al. 1994, Rui et al. 1994); forced dimerization of GH receptor domains is sufficient to activate signaling (Behncken et al. 2000); phosphorylation of JAK2 at Y1007 is critical for kinase activation (Feng et al. 1997, Lucet et al. 2006); JAK autophosphorylation at several other sites appears to regulate activity (e.g. Feener et al. 2004, Argetsinger et al. 2004, 2010). Only the Y1007 phosphorylation is represented in this reaction.
REACT_115719 (Reactome) Prolactin stimulation leads to tyrosine phosphorylation of the C-terminal SH2 domain of SHP2 and requires JAK2 (Ali et al. 1996). This has a positive regulatory influence on PRLR signaling. SHP2 has a number of signaling-capable interactors such as signal regulatory proteins (SIRPs, Kharitonenkov et al. 1997), SH2-containing inositol phosphatase (SHIP, Liu et al. 1997), insulin receptor substrates 1 and 2 (Myers et al. 1998), JAK2 (Jiao et al. 1996) and GRB2 associated binder 2 (GAB2) an adaptor protein that links activated receptor tyrosine kinase and cytokine receptors to downstream signaling molecules. PRL stimulation leads to SHP2-GAB2 association, GAB2 tyrosine phosphorylation, and GAB2-PI3K p85 subunit association, though it is not clear that this is the order of events, nor that SHP2 serves as a link between PRLR and GAB2 (Ali & Ali 2000).
REACT_115782 (Reactome) Tyrosine-phosphorylated PRLR can bind the protein-tyrosine Phosphatase SHP2 (PTPN11) via its C-terminal SH2 Domain. This binding does not occur when the most C-terminal PRLR tyrosine residue (residue 611 in the human canonical Uniprot sequence, equivalent to 587 in the mature protein with signal peptide removed) is mutated to alanine (Ali & Ali 2000).
REACT_115790 (Reactome) Phosphorylation of PRLR on Ser-349 by an unidentified kinase enables recruitment of the SCF beta-TrCP ubiquitin ligase complex, which catalyzes ubiquitination of the receptor (Li et al. 2004). This downregulation mechanism is impaired in some forms of breast cancer (Li et al. 2006).
REACT_115792 (Reactome) The SH2 domains of SH2B beta (Uniprot isoform Q9NRF2-2) binds JAK2 at Tyr813. SH2B beta is able to homodimerize while bound to JAK2 molecules, suggesting that SH2B binding and dimerization may help induce JAK2 transactivation (Nishi et al. 2005). Computational modeling suggests that SH2B beta can enhance Jak2 activation (Barua et al. 2009). The relevance of this for PRLR signalling has yet to be demonstrated.
REACT_115800 (Reactome) Ligand binding activates the PRLR, probably by causing a subtle conformational change (Broutin et al. 2010).
REACT_115844 (Reactome) The PRL responsiveness of target cells is negatively regulated by receptor internalization, ubiquitination and degradation, which limit the duration and intensity of receptor signaling (Djiane et al. 1981, 1982, Lu et al. 2002). The PRLR is phosphorylated on Ser-349 by an unidentified kinase (Li et al. 2006) enabling subsequent recruitment of the SCF beta-TrCP ubiquitin ligase complex (Li et al. 2004).
REACT_115881 (Reactome) The prolactin receptor (PRLR) peptide is a single transmembrane domain protein that functions as a dimer. Recent reports suggest that like many other cytokine receptors, the prolactin receptor (PRLR) pre-assembles at the plasma membrane in the absence of ligand (Gadd & Clevenger 2006, Tallet et al. 2011), suggesting that ligand-induced activation involves conformational changes in the preformed receptor dimer (Broutin et al. 2010).
REACT_115907 (Reactome) PRLR is regulated by ubiquitination of the activated receptor, leading to lysosomal degradation (Djiane et al. 1981, 1982, Lu et al. 2002). Recruitment of the SCFbeta-TrCP ubiquitin ligase complex enables receptor ubiquitination and internalization (Li et al. 2004). This limits the duration and intensity of receptor signaling. Deregulation of this negative control lead to pathological conditions including cancer (Swaminathan et al. 2008).
REACT_115938 (Reactome) Co-immunoprecipitation of rat Stat5 and Prlrs mutated to have a single intracellular tyrosine suggests that phosphorylation of these tyrosines is required for Stat5 binding and leads to Stat5 tyrosine phosphorylation (Pezet et al. 1997). STAT1 and STAT3 have both been reported to be activated by PRLR (DaSilva et al. 1996), but the region(s) of PRLR required for activation of these Stats remains poorly documented.
REACT_116060 (Reactome) Human PRLR binds at least 3 related peptide ligands namely prolactin, placental lactogen (PL) and growth hormone (GH). In non primates, GH is not able to bind the PRLR. Human GH binding to the PRLR is zinc-dependent (Cunningham et al. 1990). All three ligands bind the extracellular domain and have apparently identical actions. Two disulfide-linked cysteines in the D1 subdomain are involved in ligand binding while the WSXWS motif in the D2 subdomain is probably required for folding and cellular trafficking.
REACT_116102 (Reactome) PRLR has no intrinsic kinase activity but associates with Janus kinase 2 (JAK2) (Lebrun et al. 1994, 1995, Campbell et al. 1994, Rui et al. 1994). PRLR to JAK2 binding has been described as constitutive but a recent computational model suggests that roughly half of dimerized Growth Hormone receptors are bound with JAK2 (Barua et al. 2009), a model that may apply to other receptors that promote JAK2 trans-activation. The box 1 region of PRLR is a membrane proximal proline-rich region in the intracellular domain, conserved in all members of the growth hormone rereptor family. This region is critical for JAK2 association; deletion of box 1 virtually abolishes PRLR signaling (Edery et al. 1994). Alanine substitutions of individual residues within box 1 of rat PRLR have shown that the most C-terminal proline (P269 in the Uniprot canonical sequence, 250 in the mature peptide) is critical for association with and subsequent activation of JAK2 (Pezet et al. 1997). It is not known whether the interaction of JAK2 with PRLR is direct or involves an adaptor protein.

When the receptor is activated by ligand binding JAK2 (receptor pre-bound or recruited after ligand binding) becomes activated and phosphorylates the dimerized receptor preferentially at Y611 (position 587 in the mature peptide), a consensus tyrosine phosphorylation site. This is followed by the phosphorylation, dimerization and nuclear translocation of STAT5. There are nine other tyrosines in the cytoplasmic domain, some of which may undergo phosphorylation and may participate in signal transduction.
REACT_116156 (Reactome) PRLRs contain intracellular phosphorylated tyrosine residues that are able to bind and activate STATs, demonstrated by the co-immunoprecipitation of rat Stat5 and Prlrs mutated to have a single intracellular tyrosine (Pezet et al. 1997). Prlr mutants with a single tyrosine residue at positions 599, 498 or 492 (reported according to their position in the mature peptide as 580, 479 or 473 in Pezet et al. 1997) were all able to activate Stat5; Y599 gave a much stronger response. Short forms of PRLR lacking these tyrosines did not bind STAT5. The equivalent human tyrosine residues are Y509 and Y611; Y492 is not conserved in humans.
Activation of STAT1 and STAT3 by PRLR has been reported (Da Silva et al. 1996) but the interaction has been suggested to be indirect and possibly mediated by JAK2.
REACT_116161 (Reactome) The model for PRL-induced PRLR activation suggests that JAK2 phosphorylates PRLR on specific tyrosine residues. Consistent with this, JAK2 and PRLR are phosphorylated in response to activating ligand (Lebrun et al. 1994) and PRLR tyrosine phosphorylation is required for subsequent Stat signaling (Pezet et al. 1997). Though this evidence is consistent with a role for JAK2, it has not been formally demonstrated that JAK2 is the kinase responsible for PRLR tyrosine phosphorylation.
SCF beta-TrCP complexArrowREACT_115907 (Reactome)
SCF beta-TrCP complexREACT_115790 (Reactome)
SH2B1-2REACT_115792 (Reactome)
STAT5REACT_116156 (Reactome)
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