Src‐dependent phosphorylation of μ‐opioid receptor at Tyr336 modulates opiate withdrawal

Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A (PKA) activities within the neurocircuitry of addiction has been a leading hypothesis for opi...

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Published inEMBO molecular medicine Vol. 9; no. 11; pp. 1521 - 1536
Main Authors Zhang, Lei, Kibaly, Cherkaouia, Wang, Yu‐Jun, Xu, Chi, Song, Kyu Young, McGarrah, Patrick W, Loh, Horace H, Liu, Jing‐Gen, Law, Ping‐Yee
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group UK 01.11.2017
John Wiley and Sons Inc
Springer Nature
Subjects
EMBO27
lentivirus injection
locus coeruleus
naloxone‐precipitated opiate withdrawal
opiate addiction
Research Article
Src‐mediated phosphorylation of MOR at Tyr336
naloxone‐precipitated opiate withdrawal
lentivirus injection
opiate addiction
Src‐mediated phosphorylation of MOR at Tyr
locus coeruleus
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Abstract Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A (PKA) activities within the neurocircuitry of addiction has been a leading hypothesis for opiate addiction. This increase requires the phosphorylation of μ‐opioid receptor (MOR) at Tyr 336 by Src after prolonged opiate treatment in vitro . Here, we report that the Src‐mediated MOR phosphorylation at Tyr 336 is a prerequisite for opiate withdrawal in mice. We observed the recruitment of Src in the vicinity of MOR and an increase in phosphorylated Tyr 336 (pY336) levels during naloxone‐precipitated withdrawal. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses attenuated pY336 levels, and several somatic withdrawal signs. This was also observed in Fyn −/− mice. The stereotaxic injection of wild‐type MOR, but not mutant (Y336F) MOR, lentiviruses into the locus coeruleus of MOR −/− mice restored somatic withdrawal jumping. Regulating pY336 levels during withdrawal might be a future target for drug development to prevent opiate addictive behaviors. Synopsis The μ‐opioid receptor (MOR) non‐canonical signaling pathway involves its phosphorylation at Tyr 336 by Src kinase within the MOR signal complex. The focal event of MOR Y 336 phosphorylation may be the key for adenylyl cyclase superactivation during the withdrawal/negative stage of opiate addiction. The phosphorylation levels of MOR Y 336 and Src Y416 increased during naloxone‐precipitated withdrawal in wild‐type mice. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses reduced pMOR Y 336 and pSrc Y416 levels, and several somatic withdrawal signs. Increases of pMOR Y 336 levels as well as some somatic withdrawal signs after naloxone‐precipitated withdrawal were not observed in Fyn −/− mice. The stereotaxic injection of wild‐type MOR lentiviruses into the locus coeruleus of MOR −/− mice restored somatic withdrawal jumping and wet dog shaking. The stereotaxic injection of the phosphorylation‐deficient mutant (Y336F) MOR, in which the mutation of Tyr 336 to Phe blocks Src‐mediated phosphorylation, attenuated naloxone‐precipitated withdrawal. Graphical Abstract The μ‐opioid receptor (MOR) non‐canonical signaling pathway involves its phosphorylation at Tyr 336 by Src kinase within the MOR signal complex. The focal event of MOR Y336 phosphorylation may be the key for adenylyl cyclase superactivation during the withdrawal/negative stage of opiate addiction.
AbstractList Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A (PKA) activities within the neurocircuitry of addiction has been a leading hypothesis for opiate addiction. This increase requires the phosphorylation of μ‐opioid receptor (MOR) at Tyr 336 by Src after prolonged opiate treatment in vitro . Here, we report that the Src‐mediated MOR phosphorylation at Tyr 336 is a prerequisite for opiate withdrawal in mice. We observed the recruitment of Src in the vicinity of MOR and an increase in phosphorylated Tyr 336 (pY336) levels during naloxone‐precipitated withdrawal. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses attenuated pY336 levels, and several somatic withdrawal signs. This was also observed in Fyn −/− mice. The stereotaxic injection of wild‐type MOR, but not mutant (Y336F) MOR, lentiviruses into the locus coeruleus of MOR −/− mice restored somatic withdrawal jumping. Regulating pY336 levels during withdrawal might be a future target for drug development to prevent opiate addictive behaviors. Synopsis The μ‐opioid receptor (MOR) non‐canonical signaling pathway involves its phosphorylation at Tyr 336 by Src kinase within the MOR signal complex. The focal event of MOR Y 336 phosphorylation may be the key for adenylyl cyclase superactivation during the withdrawal/negative stage of opiate addiction. The phosphorylation levels of MOR Y 336 and Src Y416 increased during naloxone‐precipitated withdrawal in wild‐type mice. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses reduced pMOR Y 336 and pSrc Y416 levels, and several somatic withdrawal signs. Increases of pMOR Y 336 levels as well as some somatic withdrawal signs after naloxone‐precipitated withdrawal were not observed in Fyn −/− mice. The stereotaxic injection of wild‐type MOR lentiviruses into the locus coeruleus of MOR −/− mice restored somatic withdrawal jumping and wet dog shaking. The stereotaxic injection of the phosphorylation‐deficient mutant (Y336F) MOR, in which the mutation of Tyr 336 to Phe blocks Src‐mediated phosphorylation, attenuated naloxone‐precipitated withdrawal. Graphical Abstract The μ‐opioid receptor (MOR) non‐canonical signaling pathway involves its phosphorylation at Tyr 336 by Src kinase within the MOR signal complex. The focal event of MOR Y336 phosphorylation may be the key for adenylyl cyclase superactivation during the withdrawal/negative stage of opiate addiction.
Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A (PKA) activities within the neurocircuitry of addiction has been a leading hypothesis for opiate addiction. This increase requires the phosphorylation of μ‐opioid receptor (MOR) at Tyr336 by Src after prolonged opiate treatment in vitro. Here, we report that the Src‐mediated MOR phosphorylation at Tyr336 is a prerequisite for opiate withdrawal in mice. We observed the recruitment of Src in the vicinity of MOR and an increase in phosphorylated Tyr336 (pY336) levels during naloxone‐precipitated withdrawal. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses attenuated pY336 levels, and several somatic withdrawal signs. This was also observed in Fyn−/− mice. The stereotaxic injection of wild‐type MOR, but not mutant (Y336F) MOR, lentiviruses into the locus coeruleus of MOR−/− mice restored somatic withdrawal jumping. Regulating pY336 levels during withdrawal might be a future target for drug development to prevent opiate addictive behaviors. Synopsis The μ‐opioid receptor (MOR) non‐canonical signaling pathway involves its phosphorylation at Tyr336 by Src kinase within the MOR signal complex. The focal event of MORY336 phosphorylation may be the key for adenylyl cyclase superactivation during the withdrawal/negative stage of opiate addiction. The phosphorylation levels of MORY336 and SrcY416 increased during naloxone‐precipitated withdrawal in wild‐type mice. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses reduced pMORY336 and pSrcY416 levels, and several somatic withdrawal signs. Increases of pMORY336 levels as well as some somatic withdrawal signs after naloxone‐precipitated withdrawal were not observed in Fyn−/− mice. The stereotaxic injection of wild‐type MOR lentiviruses into the locus coeruleus of MOR−/− mice restored somatic withdrawal jumping and wet dog shaking. The stereotaxic injection of the phosphorylation‐deficient mutant (Y336F) MOR, in which the mutation of Tyr336 to Phe blocks Src‐mediated phosphorylation, attenuated naloxone‐precipitated withdrawal. The μ‐opioid receptor (MOR) non‐canonical signaling pathway involves its phosphorylation at Tyr336 by Src kinase within the MOR signal complex. The focal event of MORY336 phosphorylation may be the key for adenylyl cyclase superactivation during the withdrawal/negative stage of opiate addiction.
Abstract Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A (PKA) activities within the neurocircuitry of addiction has been a leading hypothesis for opiate addiction. This increase requires the phosphorylation of μ‐opioid receptor (MOR) at Tyr336 by Src after prolonged opiate treatment in vitro. Here, we report that the Src‐mediated MOR phosphorylation at Tyr336 is a prerequisite for opiate withdrawal in mice. We observed the recruitment of Src in the vicinity of MOR and an increase in phosphorylated Tyr336 (pY336) levels during naloxone‐precipitated withdrawal. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses attenuated pY336 levels, and several somatic withdrawal signs. This was also observed in Fyn−/− mice. The stereotaxic injection of wild‐type MOR, but not mutant (Y336F) MOR, lentiviruses into the locus coeruleus of MOR−/− mice restored somatic withdrawal jumping. Regulating pY336 levels during withdrawal might be a future target for drug development to prevent opiate addictive behaviors.
Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A ( PKA ) activities within the neurocircuitry of addiction has been a leading hypothesis for opiate addiction. This increase requires the phosphorylation of μ‐opioid receptor ( MOR ) at Tyr 336 by Src after prolonged opiate treatment in vitro . Here, we report that the Src‐mediated MOR phosphorylation at Tyr 336 is a prerequisite for opiate withdrawal in mice. We observed the recruitment of Src in the vicinity of MOR and an increase in phosphorylated Tyr 336 ( pY 336) levels during naloxone‐precipitated withdrawal. The intracerebroventricular or stereotaxic injection of a Src inhibitor ( AZD 0530), or Src sh RNA viruses attenuated pY 336 levels, and several somatic withdrawal signs. This was also observed in Fyn −/− mice. The stereotaxic injection of wild‐type MOR , but not mutant (Y336F) MOR , lentiviruses into the locus coeruleus of MOR −/− mice restored somatic withdrawal jumping. Regulating pY 336 levels during withdrawal might be a future target for drug development to prevent opiate addictive behaviors.
Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A (PKA) activities within the neurocircuitry of addiction has been a leading hypothesis for opiate addiction. This increase requires the phosphorylation of μ-opioid receptor (MOR) at Tyr336 by Src after prolonged opiate treatment in vitro Here, we report that the Src-mediated MOR phosphorylation at Tyr336 is a prerequisite for opiate withdrawal in mice. We observed the recruitment of Src in the vicinity of MOR and an increase in phosphorylated Tyr336 (pY336) levels during naloxone-precipitated withdrawal. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses attenuated pY336 levels, and several somatic withdrawal signs. This was also observed in Fyn-/- mice. The stereotaxic injection of wild-type MOR, but not mutant (Y336F) MOR, lentiviruses into the locus coeruleus of MOR-/- mice restored somatic withdrawal jumping. Regulating pY336 levels during withdrawal might be a future target for drug development to prevent opiate addictive behaviors.Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in the intracellular cAMP level and protein kinase A (PKA) activities within the neurocircuitry of addiction has been a leading hypothesis for opiate addiction. This increase requires the phosphorylation of μ-opioid receptor (MOR) at Tyr336 by Src after prolonged opiate treatment in vitro Here, we report that the Src-mediated MOR phosphorylation at Tyr336 is a prerequisite for opiate withdrawal in mice. We observed the recruitment of Src in the vicinity of MOR and an increase in phosphorylated Tyr336 (pY336) levels during naloxone-precipitated withdrawal. The intracerebroventricular or stereotaxic injection of a Src inhibitor (AZD0530), or Src shRNA viruses attenuated pY336 levels, and several somatic withdrawal signs. This was also observed in Fyn-/- mice. The stereotaxic injection of wild-type MOR, but not mutant (Y336F) MOR, lentiviruses into the locus coeruleus of MOR-/- mice restored somatic withdrawal jumping. Regulating pY336 levels during withdrawal might be a future target for drug development to prevent opiate addictive behaviors.
Author Kibaly, Cherkaouia
Loh, Horace H
Law, Ping‐Yee
Xu, Chi
McGarrah, Patrick W
Wang, Yu‐Jun
Liu, Jing‐Gen
Song, Kyu Young
Zhang, Lei
AuthorAffiliation 2 Key Laboratory of Receptor Research Shanghai Institute of Materia Medica and Collaborative Innovation Center for Brain Science Chinese Academy of Science Shanghai China
1 Department of Pharmacology University of Minnesota Medical School Minneapolis MN USA
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Issue 11
Keywords naloxone‐precipitated opiate withdrawal
lentivirus injection
opiate addiction
Src‐mediated phosphorylation of MOR at Tyr
locus coeruleus
Language English
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References 2017; 119
1997; 278
1993; 605
2010; 107
1997; 272
2004; 25
2004; 23
2005; 579
2002; 99
2005; 1032
1975; 193
2006; 170
2007; 32
2011; 16
2003; 278
2007; 35
2003; 54
1997; 7
2005; 25
2009; 56
1998; 18
1982; 26
2010; 24
2000; 403
2006; 69
1997; 17
2011; 22
2008; 63
2009; 284
2014; 12
1998; 282
2001; 98
2007; 27
2009; 23
2009; 63
2012; 341
2010; 35
1992; 261
1990; 37
2013; 84
2006; 17
2008
1995
1988; 242
2011; 34
2005; 82
2011; 3
1995; 6
2005; 46
2001; 276
2011; 2011
2016; 3
2001; 4
1977; 16
2006; 49
2002; 22
1996; 271
2000; 40
2009; 101
1985; 235
2003; 27
1988; 474
2011; 1415
2009; 3
1977; 195
2012; 119
2006; 103
References_xml – volume: 4
  start-page: 943
  year: 2001
  end-page: 947
  article-title: The role of withdrawal in heroin addiction: enhances reward or promotes avoidance?
  publication-title: Nat Neurosci
– volume: 69
  start-page: 1810
  year: 2006
  end-page: 1819
  article-title: Short‐ and long‐term regulation of adenylyl cyclase activity by delta‐opioid receptor are mediated by Galphai2 in neuroblastoma N2A cells
  publication-title: Mol Pharmacol
– volume: 3
  start-page: 248
  year: 2009
  end-page: 261
  article-title: Preclinical anticancer activity of the potent, oral Src inhibitor AZD0530
  publication-title: Mol Oncol
– volume: 16
  start-page: 721
  year: 1977
  end-page: 734
  article-title: Inhibition by naloxone of tolerance and dependence in mice treated acutely and chronically with morphine
  publication-title: Res Commun Chem Pathol Pharmacol
– volume: 12
  start-page: 514
  year: 2014
  end-page: 526
  article-title: FAK inhibition abrogates the malignant phenotype in aggressive pediatric renal tumors
  publication-title: Mol Cancer Res
– volume: 2011
  start-page: 865819
  year: 2011
  article-title: Regulation of SRC family kinases in human cancers
  publication-title: J Signal Transduct
– start-page: 495
  year: 1995
  end-page: 578
– volume: 46
  start-page: abst SY13‐3
  year: 2005
  article-title: Pre‐clinical and early clinical activity of the highly selective, orally available, dual Src/Abl kinase inhibitor AZD0530
  publication-title: Proc Am Assoc Cancer Res
– volume: 235
  start-page: 282
  year: 1985
  end-page: 286
  article-title: Pharmacokinetics and pharmacodynamics of subcutaneous morphine pellets in the rat
  publication-title: J Pharmacol Exp Ther
– volume: 1415
  start-page: 96
  year: 2011
  end-page: 102
  article-title: Decreased dendritic spine density and abnormal spine morphology in Fyn knockout mice
  publication-title: Brain Res
– volume: 25
  start-page: 210
  year: 2004
  end-page: 218
  article-title: Historical review: molecular and cellular mechanisms of opiate and cocaine addiction
  publication-title: Trends Pharmacol Sci
– volume: 101
  start-page: 263
  year: 2009
  end-page: 268
  article-title: Dasatinib inhibits the growth of prostate cancer in bone and provides additional protection from osteolysis
  publication-title: Br J Cancer
– volume: 63
  start-page: 224
  year: 2009
  end-page: 235
  article-title: Phosphorylation of GluR1, ERK and CREB during spontaneous withdrawal from chronic heroin self‐administration
  publication-title: Synapse
– volume: 242
  start-page: 715
  year: 1988
  end-page: 723
  article-title: Cellular and molecular mechanisms of drug dependence
  publication-title: Science
– volume: 63
  start-page: 1013
  year: 2008
  end-page: 1021
  article-title: Distinct roles of adenylyl cyclase 1 and 8 in opiate dependence: behavioral, electrophysiological, and molecular studies
  publication-title: Biol Psychiatry
– volume: 82
  start-page: 82
  year: 2005
  end-page: 89
  article-title: Context‐ and cue‐conditioned potentiation of acute morphine dependence and withdrawal
  publication-title: Pharmacol Biochem Behav
– volume: 84
  start-page: 844
  year: 2013
  end-page: 853
  article-title: A novel noncanonical signaling pathway for the mu‐opioid receptor
  publication-title: Mol Pharmacol
– volume: 193
  start-page: 876
  year: 1975
  end-page: 883
  article-title: Relationship of brain morphine levels to analgesic activity in acutely treated mice and rats and in pellet implanted mice
  publication-title: J Pharmacol Exp Ther
– volume: 3
  start-page: 449
  year: 2016
  end-page: 456
– volume: 32
  start-page: 1995
  year: 2007
  end-page: 2003
  article-title: Activation of the cAMP/PKA/DARPP‐32 signaling pathway is required for morphine psychomotor stimulation but not for morphine reward
  publication-title: Neuropsychopharmacology
– volume: 35
  start-page: 217
  year: 2010
  end-page: 238
  article-title: Neurocircuitry of addiction
  publication-title: Neuropsychopharmacology
– volume: 284
  start-page: 1990
  year: 2009
  end-page: 2000
  article-title: Src phosphorylation of mu‐receptor is responsible for the receptor switching from an inhibitory to a stimulatory signal
  publication-title: J Biol Chem
– volume: 1032
  start-page: 193
  year: 2005
  end-page: 199
  article-title: Alterations in morphine‐induced reward, locomotor activity, and thermoregulation in CREB‐deficient mice
  publication-title: Brain Res Rev
– volume: 18
  start-page: 1848
  year: 1998
  end-page: 1859
  article-title: Involvement of cAMP‐dependent protein kinase in the nucleus accumbens in cocaine self‐administration and relapse of cocaine‐seeking behavior
  publication-title: J Neurosci
– volume: 119
  start-page: 153
  year: 2017
  end-page: 168
  article-title: Spinal or supraspinal phosphorylation deficiency at the MOR C‐terminus does not affect morphine tolerance
  publication-title: Pharmacol Res
– volume: 26
  start-page: 495
  year: 1982
  end-page: 503
  article-title: Nonpharmacological bases of drug tolerance and dependence
  publication-title: J Psychosom Res
– volume: 17
  start-page: 8520
  year: 1997
  end-page: 8527
  article-title: Opposite modulation of opiate withdrawal behaviors on microinfusion of a protein kinase A inhibitor versus activator into the locus coeruleus or periaqueductal gray
  publication-title: J Neurosci
– year: 2008
– volume: 40
  start-page: 389
  year: 2000
  end-page: 430
  article-title: Molecular mechanisms and regulation of opioid receptor signaling
  publication-title: Annu Rev Pharmacol Toxicol
– volume: 605
  start-page: 128
  year: 1993
  end-page: 138
  article-title: Destruction of the locus coeruleus decreases physical signs of opiate withdrawal
  publication-title: Brain Res
– volume: 16
  start-page: 566
  year: 2011
  end-page: 578
  article-title: Current status of SRC inhibitors in solid tumor malignancies
  publication-title: Oncologist
– volume: 23
  start-page: 7906
  year: 2004
  end-page: 7909
  article-title: Src family kinases, key regulators of signal transduction
  publication-title: Oncogene
– volume: 27
  start-page: 1033
  year: 2003
  end-page: 1040
  article-title: Deletion of the Fyn‐kinase gene alters behavioral sensitivity to ethanol
  publication-title: Alcohol Clin Exp Res
– volume: 34
  start-page: 629
  year: 2011
  end-page: 637
  article-title: Src family kinases: modulators of neurotransmitter receptor function and behavior
  publication-title: Trends Neurosci
– volume: 3
  start-page: 7
  year: 2011
  end-page: 12
  article-title: Role of calcium in morphine dependence and naloxone‐precipitated withdrawal in mice
  publication-title: J Exp Pharmacol
– volume: 579
  start-page: 3271
  year: 2005
  end-page: 3277
  article-title: Second nature: biological functions of the Raf‐1 “kinase”
  publication-title: FEBS Lett
– volume: 276
  start-page: 12774
  year: 2001
  end-page: 12780
  article-title: Phosphorylation of Ser , Thr , and Ser residues within the carboxyl tail differentially regulates mu‐opioid receptor internalization
  publication-title: J Biol Chem
– volume: 22
  start-page: 3663
  year: 2002
  end-page: 3672
  article-title: Regional and cellular mapping of cAMP response element‐mediated transcription during naltrexone‐precipitated morphine withdrawal
  publication-title: J Neurosci
– volume: 49
  start-page: 6465
  year: 2006
  end-page: 6488
  article-title: N‐(5‐Chloro‐1,3‐benzodioxol‐4‐yl)‐7‐[2‐(4‐methylpiperazin‐1‐yl)ethoxyl]‐5‐(tetrahydro‐2H‐pyran‐4‐yloxoy0quinazolin‐4‐amine, a novel, highly selective, orally available, dual‐specific c‐Src/Abl kinase inhibitor
  publication-title: J Med Chem
– volume: 261
  start-page: 669
  year: 1992
  end-page: 677
  article-title: Role of different brain structures in the expression of the physical morphine withdrawal syndrome
  publication-title: J Pharmacol Exp Ther
– volume: 37
  start-page: 767
  year: 1990
  end-page: 773
  article-title: Nucleus accumbens and amygdala are possible substrates for the aversive stimulus effects of opiate withdrawal
  publication-title: Neuroscience
– volume: 98
  start-page: 11042
  year: 2001
  end-page: 11046
  article-title: ∆FosB: a sustained molecular switch for addiction
  publication-title: Proc Natl Acad Sci USA
– volume: 103
  start-page: 3908
  year: 2006
  end-page: 3913
  article-title: Adenylyl cyclase type 5 (AC5) is an essential mediator of morphine action
  publication-title: Proc Natl Acad Sci USA
– volume: 17
  start-page: 115
  year: 2006
  end-page: 119
  article-title: Role of Src family kinase in the rewarding effect and hyperlocomotion induced by morphine
  publication-title: NeuroReport
– volume: 22
  start-page: 182
  year: 2011
  end-page: 190
  article-title: Modulation of src‐kinase attenuates naloxone‐precipitated opioid withdrawal syndrome in mice
  publication-title: Behav Pharmacol
– volume: 119
  start-page: 4817
  year: 2012
  end-page: 4818
  article-title: The shady side of dasatinib
  publication-title: Blood
– volume: 403
  start-page: 430
  year: 2000
  end-page: 434
  article-title: Noradrenaline in the ventral forebrain is critical for opiate withdrawal‐induced aversion
  publication-title: Nature
– volume: 474
  start-page: 364
  year: 1988
  end-page: 368
  article-title: Aversive properties of opiate receptor blockade: evidence for exclusively central mediation in naive and morphine‐dependent rats
  publication-title: Brain Res Rev
– volume: 7
  start-page: 713
  year: 1997
  end-page: 719
  article-title: Molecular mechanisms of opiate and cocaine addiction
  publication-title: Curr Opin Neurobiol
– volume: 23
  start-page: 4327
  year: 2009
  end-page: 4334
  article-title: Biomarkers of morphine tolerance and dependence are prevented by morphine‐induced endocytosis of a mutant μ‐opioid receptor
  publication-title: FASEB J
– volume: 195
  start-page: 1000
  year: 1977
  end-page: 1002
  article-title: Conditioned narcotic withdrawal in humans
  publication-title: Science
– volume: 54
  start-page: 1422
  year: 2003
  end-page: 1426
  article-title: Analysis of genetic variations of protein tyrosine kinase fyn and their association with alcohol dependence in two independent cohorts
  publication-title: Biol Psychiatry
– volume: 272
  start-page: 5040
  year: 1997
  end-page: 5047
  article-title: Opiate‐induced adenylyl cyclase superactivation is isozyme‐specific
  publication-title: J Biol Chem
– volume: 278
  start-page: 58
  year: 1997
  end-page: 63
  article-title: Molecular and cellular basis of addiction
  publication-title: Science
– volume: 271
  start-page: 21309
  year: 1996
  end-page: 21315
  article-title: Chronic opioid treatment induces adenylyl cyclase V superactivation. Involvement of Gbetagamma
  publication-title: J Biol Chem
– volume: 278
  start-page: 698
  year: 1997
  end-page: 701
  article-title: Fyn‐kinase as a determinant of ethanol sensitivity: relation to NMDA‐receptor function
  publication-title: Science
– volume: 341
  start-page: 115
  year: 2012
  end-page: 125
  article-title: Activation of protein kinase C (PKC)α or PKCɛ as an approach to increase morphine tolerance in respiratory depression and lethal overdose
  publication-title: J Pharmacol Exp Ther
– volume: 25
  start-page: 5553
  year: 2005
  end-page: 5562
  article-title: Regulation of drug reward by cAMP response element‐binding protein: evidence for two functionally distinct subregions of the ventral tegmental area
  publication-title: J Neurosci
– volume: 107
  start-page: 12345
  year: 2010
  end-page: 12350
  article-title: Disrupting the memory of places induced by drugs of abuse weakens motivational withdrawal in a context‐dependent manner
  publication-title: Proc Natl Acad Sci USA
– volume: 278
  start-page: 49936
  year: 2003
  end-page: 49944
  article-title: GIT1 mediates Src‐dependent activation of phospholipase Cgamma by angiotensin II and epidermal growth factor
  publication-title: J Biol Chem
– volume: 35
  start-page: 1501
  year: 2007
  end-page: 1513
  article-title: Translational repression of mouse mu opioid receptor expression via leaky scanning
  publication-title: Nucleic Acid Res
– volume: 56
  start-page: 18
  issue: Suppl 1
  year: 2009
  end-page: 31
  article-title: Neurobiological substrates for the dark side of compulsivity in addiction
  publication-title: Neuropharmacology
– volume: 99
  start-page: 11435
  year: 2002
  end-page: 11440
  article-title: CREB activity in the nucleus accumbens shell controls gating of behavioral responses to emotional stimuli
  publication-title: Proc Natl Acad Sci USA
– volume: 282
  start-page: 2272
  year: 1998
  end-page: 2275
  article-title: Regulation of cocaine reward by CREB
  publication-title: Science
– volume: 69
  start-page: 1421
  year: 2006
  end-page: 1432
  article-title: Adenylyl cyclase superactivation induced by long‐term treatment with opioid agonist is dependent on receptor localized within lipid rafts and is independent of receptor internalization
  publication-title: Mol Pharmacol
– volume: 27
  start-page: 3593
  year: 2007
  end-page: 3602
  article-title: Ethanol induces long‐term facilitation of NR2B‐NMDA receptor activity in the dorsal striatum: implications for alcohol drinking behavior
  publication-title: J Neurosci
– volume: 6
  start-page: 74
  year: 1995
  end-page: 80
  article-title: Suppression of corticotropin‐releasing factor in the amygdala attenuates aversive consequences of morphine withdrawal
  publication-title: Behav Pharmacol
– volume: 24
  start-page: 723
  year: 2010
  end-page: 730
  article-title: A versatile system for the neuronal subtype specific expression of lentiviral vectors
  publication-title: FASEB J
– volume: 170
  start-page: 110
  year: 2006
  end-page: 118
  article-title: Gender‐ and morphine dose‐linked expression of spontaneous somatic opiate withdrawal in mice
  publication-title: Behav Brain Res
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Snippet Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use. Increase in...
Abstract Opiate withdrawal/negative reinforcement has been implicated as one of the mechanisms for the progression from impulsive to compulsive drug use....
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SubjectTerms EMBO27
lentivirus injection
locus coeruleus
naloxone‐precipitated opiate withdrawal
opiate addiction
Research Article
Src‐mediated phosphorylation of MOR at Tyr336
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Title Src‐dependent phosphorylation of μ‐opioid receptor at Tyr336 modulates opiate withdrawal
URI https://link.springer.com/article/10.15252/emmm.201607324
https://onlinelibrary.wiley.com/doi/abs/10.15252%2Femmm.201607324
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https://pubmed.ncbi.nlm.nih.gov/PMC5666313
https://doaj.org/article/9497773952d5463cb90d28ececad52aa
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