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Opioid Analgesics & Antagonists. By Bohlooli S. PhD School of Medicine, Ardabil University of Medical Sciences. Introduction. Opium poppy is the source of crude opium Sertürner in 1803 isolated morphine Naming it after Morpheus, the Greek god of dreams
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Opioid Analgesics & Antagonists By Bohlooli S. PhD School of Medicine, Ardabil University of Medical Sciences
Introduction • Opium poppy is the source of crude opium • Sertürner in 1803 isolated morphine • Naming it after Morpheus, the Greek god of dreams • Opioid analgesics is a widely used term for: • Natural, semi-synthetic, synthetic • Endogenous peptides
Source • Opium, the source of morphine, is obtained from the poppy, Papaversomniferum and P album • Opium contains many alkaloids, the principle one being morphine, which is present in a concentration of about 10%
Classification & Chemistry • Opioid drugs include: • Full agonists • Morphine • Partial agonists • Codeine • Antagonists • Naloxone
Chemistry • Phenanthrenes • Morphine, hydromorphone, and oxymorphone • Codeine,oxycodone, dihydrocodeine, and hydrocodone • Phenylheptylamines • Methadone • Propoxyphene • Phenylpiperidines • Fentanyl, sufentanil, alfentanil, and remifentanil • Diphenoxylate and its metabolite, difenoxin • Loperamide • Morphinans
Chemistry; Opioids with Mixed Receptor Actions • Phenanthrenes • Nalbuphine, Buprenorphine • Morphinans • Butorphanol • Benzomorphans • Pentazocine • Miscellaneous • Tramadol, Tapentadol
Opioid Receptor Subtypes, Their Functions, and Their Endogenous Peptide Affinities
Endogenous Opioid Peptides • Endorphins • Drived from: prepro-opiomelanocortin • Enkephalins • met-enkephalin • leu-enkephalin • Drived from:preproenkephalin • Dynorphins • Drived from:preprodynorphin • Endomorphins • Nociceptin / Orphanin FQ • Orphanin opioid-receptor-like subtype 1 (ORL1)
Pharmacokinetics • Absorption • Distribution • Metabolism • Excretion
Absorption • Well absorbed • Variable first-pass metabolism • Subcutaneous, intramuscular, and oral routes- other routes: • Nasal insufflation • Oral mucosa via lozenges • Transdermal patches
Metabolism • Converted to polar metabolites • Morphine • morphine-3-glucuronide ::neuroexcitatory • morphine-6-glucuronide ::potency four to six times • Accumulation can produce unexpected results • Hydromorphone like morphine • H3G has CNS excitatory properties • Esters (eg, heroin, remifentanil) are rapidly hydrolyzed • Hepatic oxidative metabolism for phenylpiperidine opioids • meperidine, fentanyl, alfentanil, sufentanil • Normeperidine cause seizures in renal failure • Polymorphism of CYP2D6 • Codeine :: no significant analgesic effect or an exaggerated response
Receptor Types • Based on pharmacologic criteria • 1, 2 • 1,2 • 1, 2, 3 • Genetically one subtype from each of the , and receptor families
Cellular Actions • Closing voltage-gated Ca2+ channels on presynaptic nerve terminals • Inhibit release of • Glutamate, acetylcholine, norepinephrine, serotonin, and substance P • Hyperpolarizing and thus inhibiting postsynaptic neurons by opening K+ channels
Relation of Physiologic Effects to Receptor Type • Opioid analgesics act primarily at the -opioid receptor • Analgesia, euphoria, respiratory depression, and physical dependence • Butorphanol and nalbuphine • Preference for opioid receptors • Greater analgesia in women
Receptor Distribution and Neural Mechanisms of Analgesia: Transmission
Receptor Distribution and Neural Mechanisms of Analgesia: Modulation
Ion Channels & Novel Analgesic Targets: chronic Pain • Capsaicin receptor, TRPV1 and TRPA1 • P2X : purines receptor • Tetrodotoxin-resistant voltage-gated sodium channel (Nav1.8)-PN3/SNS channel • Lidocaine and mexiletine • Ziconotide, a blocker of voltage-gated N-type calcium channels • Related to marine snail toxin -conotoxin • Gabapentin/Pregabalin : analogs of GABA • Ketamine: NMDA antagonists • Nicotine • 9-tetrahydrocannabinol
Tolerance and Physical Dependence • Tolerance • Physical dependence • Withdrawal or abstinence syndrome • Mechanism • receptor recycling • receptor uncoupling
Organ System Effects of Morphine • Central Nervous System Effects • Cardiovascular System • Gastrointestinal Tract • Biliary Tract • Renal • Uterus • Neuroendocrine • Pruritus
Central Nervous System Effects • Analgesia • Sensory • Affective (emotional) • Nonsteroidal anti-inflammatory analgesic drugs • Has no effect on emotional part • Euphoria • Pleasant floating sensation • Lessened anxiety and distress • Dysphoria may occure • Sedation • are common effects • no amnesia • Sleep is in the elderly • Occurs more frequently phenanthrenederivatives
Central Nervous System Effects • Respiratory Depression • Significant respiratory depression • Sepressedresponse to a carbon dioxide challenge • Influenced significantly by the degree of sensory input • Most difficult clinical challenges • Cough Suppression • Codeine • May allow accumulation of secretions • Miosis • Mediated by parasympathetic pathways • Truncal Rigidity • Intensification of tone in the large trunk muscles • Nausea and Vomiting • Activate the brainstem chemoreceptor trigger zone • Temperature • -opioid receptor agonists hyperthermia • -opioid receptor agonists hypothermia
Cardiovascular System • Bradycardia • Meperidineantimuscarinic action tachycardia • Hypotension may occur • Peripheral arterial and venous dilation • Release of histamine • Central depression of vasomotor-stabilizing mechanisms • Caution in patients with decreased blood volume
Gastrointestinal Tract • Constipation • the stomach • Motility decrease • Tone increase • Gastric secretion of hydrochloric acid is decreased • Biliary Tract • Contract biliary smooth muscle • biliary colic • Sphincter of Oddi may constrict
Other Peripheral Effects • Renal • Antidiuretic effect • Enhanced renal tubular sodium reabsorption • Increased ureteral and bladder tone • Uterus • May prolong labor • Neuroendocrine • stimulate the release of ADH, prolactin, and somatotropin • inhibit the release of luteinizing hormone
Clinical Pharmacology of the Opioid Analgesics Clinical Use of Opioid Analgesics Toxicity & Undesired Effects
Alternative Routes of Administration • Rectal suppositories • morphine and hydromorphone • Transdermal patch • Fentanyl • Intranasal • Butorphanol • Buccaltransmucosal • Fentanyl citrate lozenge • Patient-controlled analgesia (PCA) • infusion device
Toxicity & Undesired Effects • Behavioral restlessness, tremulousness, hyperactivity (in dysphoric reactions) • Respiratory depression • Nausea and vomiting • Increased intracranial pressure • Postural hypotension accentuated by hypovolemia • Constipation • Urinary retention • Itching around nose, urticaria (more frequent with parenteral and spinal administration)
Tolerance and Dependence • Does not become clinically manifest until after 2–3 weeks • Tolerance to methadone develops more slowly • Cross-tolerance is an extremely important • Butoften be partial or incomplete • Opioid rotation • Recoupling opioid receptor ketamine
Physical Dependence • Signs and symptoms • Rhinorrhea • Lacrimation • Yawning • Chills • Gooseflesh (piloerection) • Hyperventilation • Hyperthermia • Mydriasis • Muscular aches • Vomiting • Diarrhea • Anxiety, and hostility
Physical Dependence • time of onset, intensity, and duration of abstinence syndrome depend on • biologic half-life • morphine or heroin, usually start within 6–10 hours • methadone required several days
Psychologic Dependence • Euphoria, indifference to stimuli, and sedation • Abdominal effects that have been likened to an intense sexual orgasm • Reinforced by the development of physical dependence
The Opioid Antagonists • Naloxone,naltrexone, and nalmefene • Methylnaltrexonebromide • Alvimopan
