agonism of the l-opioid receptor by TRV 130 increases analgesia and reduces on-target adverse effects versus morphine : A randomized , double-blind , placebo-controlled , crossover study in healthy

Opioids provide powerful analgesia but also efficacy-limiting adverse effects, including severe nausea, vomiting, and respiratory depression, by activating l-opioid receptors. Preclinical models suggest that differential activation of signaling pathways downstream of these receptors dissociates analgesia from adverse effects; however, this has not yet translated to a treatment with an improved therapeutic index. Thirty healthy men received single intravenous injections of the biased ligand TRV130 (1.5, 3, or 4.5 mg), placebo, or morphine (10 mg) in a randomized, double-blind, crossover study. Primary objectives were to measure safety and tolerability (adverse events, vital signs, electrocardiography, clinical laboratory values), and analgesia (cold pain test) versus placebo. Other measures included respiratory drive (minute volume after induced hypercapnia), subjective drug effects, and pharmacokinetics. Compared to morphine, TRV130 (3, 4.5 mg) elicited higher peak analgesia (105, 116 seconds latency vs 75 seconds for morphine, P < .02), with faster onset and similar duration of action. More subjects doubled latency or achieved maximum latency (180 seconds) with TRV130 (3, 4.5 mg). Respiratory drive reduction was greater after morphine than any TRV130 dose ( 15.9 for morphine versus 7.3, 7.6, and 9.4 h * L/ min, P < .05). More subjects experienced severe nausea after morphine (n = 7) than TRV130 1.5 or 3 mg (n = 0, 1), but not 4.5 mg (n = 9). TRV130 was generally well tolerated, and exposure was dose proportional. Thus, in this study, TRV130 produced greater analgesia than morphine at doses with less reduction in respiratory drive and less severe nausea. This demonstrates early clinical translation of ligand bias as an important new concept in receptor-targeted pharmacotherapy. 2014 International Association for the Study of Pain. Published by Elsevier B.V. All rights reserved.

[1]  A. Rebuck,et al.  A clinical method for assessing the ventilatory response to hypoxia. , 2015, The American review of respiratory disease.

[2]  J. Violin,et al.  First Clinical Experience With TRV130: Pharmacokinetics and Pharmacodynamics in Healthy Volunteers , 2014, Journal of clinical pharmacology.

[3]  J. Violin,et al.  Structure-activity relationships and discovery of a G protein biased μ opioid receptor ligand, [(3-methoxythiophen-2-yl)methyl]({2-[(9R)-9-(pyridin-2-yl)-6-oxaspiro-[4.5]decan-9-yl]ethyl})amine (TRV130), for the treatment of acute severe pain. , 2013, Journal of medicinal chemistry.

[4]  H. Wit,et al.  The drug effects questionnaire: psychometric support across three drug types , 2013, Psychopharmacology.

[5]  Guodong Liu,et al.  A G Protein-Biased Ligand at the μ-Opioid Receptor Is Potently Analgesic with Reduced Gastrointestinal and Respiratory Dysfunction Compared with Morphine , 2013, The Journal of Pharmacology and Experimental Therapeutics.

[6]  Wing Chow,et al.  Relationship Between Potential Opioid‐Related Adverse Effects and Hospital Length of Stay in Patients Receiving Opioids After Orthopedic Surgery , 2012, Pharmacotherapy.

[7]  Maria F. Sassano,et al.  Discovery of β-Arrestin–Biased Dopamine D2 Ligands for Probing Signal Transduction Pathways Essential for Antipsychotic Efficacy , 2011, Proceedings of the National Academy of Sciences.

[8]  Lisa Nguyen,et al.  Selectively Engaging β-Arrestins at the Angiotensin II Type 1 Receptor Reduces Blood Pressure and Increases Cardiac Performance , 2010, Journal of Pharmacology and Experimental Therapeutics.

[9]  J. Vry,et al.  Differential contribution of opioid and noradrenergic mechanisms of tapentadol in rat models of nociceptive and neuropathic pain , 2010, European journal of pain.

[10]  A. Senagore,et al.  Postoperative ileus: it costs more than you expect. , 2010, Journal of the American College of Surgeons.

[11]  J. Greer,et al.  Selective Antagonism of Opioid‐Induced Ventilatory Depression by an Ampakine Molecule in Humans Without Loss of Opioid Analgesia , 2010, Clinical pharmacology and therapeutics.

[12]  Jiuhong Kang,et al.  Improvement of Morphine-Mediated Analgesia by Inhibition of β-Arrestin 2 Expression in Mice Periaqueductal Gray Matter , 2009, International journal of molecular sciences.

[13]  D. Chappell,et al.  Methylnaltrexone for opioid-induced constipation in advanced illness. , 2008, The New England journal of medicine.

[14]  T. Kenakin Functional Selectivity through Protean and Biased Agonism: Who Steers the Ship? , 2007, Molecular Pharmacology.

[15]  R. Lefkowitz,et al.  Beta-arrestins and cell signaling. , 2007, Annual review of physiology.

[16]  J. Lötsch,et al.  The Partial 5‐Hydroxytryptamine1A Receptor Agonist Buspirone does not Antagonize Morphine‐induced Respiratory Depression in Humans , 2007, Clinical pharmacology and therapeutics.

[17]  M. Koltzenburg,et al.  Differential sensitivity of three experimental pain models in detecting the analgesic effects of transdermal fentanyl and buprenorphine , 2006, Pain.

[18]  S. Shabat,et al.  The frequency and timing of respiratory depression in 1524 postoperative patients treated with systemic or neuraxial morphine. , 2005, Journal of clinical anesthesia.

[19]  A. Drewes,et al.  Experimental human pain models: a review of standardised methods for preclinical testing of analgesics. , 2004, Basic & clinical pharmacology & toxicology.

[20]  Kathryn E. McGoldrick,et al.  Postoperative Pain Experience: Results From a National Survey Suggest Postoperative Pain Continues to be Undermanaged , 2004 .

[21]  A. Cowan Buprenorphine: new pharmacological aspects. , 2003, International journal of clinical practice. Supplement.

[22]  H. Niki,et al.  Molecular mechanisms of analgesia induced by opioids and ethanol: is the GIRK channel one of the keys? , 2002, Neuroscience Research.

[23]  M. Ashburn,et al.  Adverse events associated with postoperative opioid analgesia: a systematic review. , 2002, The journal of pain : official journal of the American Pain Society.

[24]  M. Seyedsadr,et al.  Selective postoperative inhibition of gastrointestinal opioid receptors. , 2001, The New England journal of medicine.

[25]  R. Gainetdinov,et al.  Enhanced morphine analgesia in mice lacking beta-arrestin 2. , 1999, Science.

[26]  C. Kozma,et al.  A modified cold stimulation technique for the evaluation of analgesic activity in human volunteers , 1985, Pain.

[27]  R. Mccullough,et al.  Diminished ventilatory response to hypoxia and hypercapnia after morphine in normal man. , 1975, The New England journal of medicine.

[28]  J. Marshall THE PARAESTHESIAE INDUCED BY COLD , 1953, Journal of Neurology Neurosurgery & Psychiatry.

[29]  J. Hardy,et al.  STUDIES ON PAIN. OBSERVATIONS ON PAIN DUE TO LOCAL COOLING AND ON FACTORS INVOLVED IN THE "COLD PRESSOR" EFFECT. , 1941, The Journal of clinical investigation.

[30]  J. Violin,et al.  Beta-arrestin-biased ligands at seven-transmembrane receptors. , 2007, Trends in pharmacological sciences.

[31]  L. Bohn,et al.  Morphine side effects in beta-arrestin 2 knockout mice. , 2005, The Journal of pharmacology and experimental therapeutics.

[32]  R. Evie Opioids: first lessons from knockout mice , 1999 .