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General Anesthesia

General Anesthesia. Myomi Tse April 17, 2007 CHEM 5398. Overview of Discussion. Historical Perspective What is General Anesthesia? Definition Principles of Surgical Anesthesia Hemodynamic and Respiratory Effects Hypothermia Nausea and Vomiting Emergence Mechanisms of Anesthesia

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General Anesthesia

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  1. General Anesthesia Myomi Tse April 17, 2007 CHEM 5398

  2. Overview of Discussion • Historical Perspective • What is General Anesthesia? • Definition • Principles of Surgical Anesthesia • Hemodynamic and Respiratory Effects • Hypothermia • Nausea and Vomiting • Emergence • Mechanisms of Anesthesia • Early Ideas • Cellular Mechanisms • Structures • Molecular Actions: GABAA Receptor • Mechanism of Propofol (Diprivan®) • Metabolism and Toxicity • Adverse Affects of Propofol • Remaining Questions Concerning the GABAA Receptor • Latest Discoveries and Current Events

  3. Historical Perspective • Original discoverer of general anesthetics • Crawford Long: 1842, ether anesthesia • Chloroform introduced • James Simpson: 1847 • Nitrous oxide • Horace Wells 19th Century physician administering chloroform

  4. Historical Perspective • William Morton • October 16, 1846 • Gaseous ether • Public demonstration gained world-wide attention • Public demonstration consisted of an operating room, “ether dome,” where Gilbert Abbot underwent surgery in an unconscious state at the Massachusetts General Hospital • Ether no longer used in modern practice, yet considered to be the first “ideal” anesthetic

  5. Historical Perspective • Cyclopropane: 1929 • Most widely used general anesthetic for the next 30 years • Halothane: 1956 • Team effort between the British Research Council and chemists at Imperial Chemical Industries • Preferred anesthetic of choice • Thiopental: Intravenous anesthetic

  6. Definition of General Anesthesia • Reversible, drug-induced loss of consciousness • Depresses the nervous system • Anesthetic state • Collection of component changes in behavior or perception • Amnesia, immobility in response to stimulation, attenuation of autonomic responses to painful stimuli, analgesia, and unconsciousness

  7. Principles of General Anesthesia • Minimizing the potentially harmful direct and indirect effects of anesthetic agents and techniques • Sustaining physiologic homeostasis during surgical procedures • Improving post-operative outcomes

  8. The Body and General Anesthesia • Hemodynamic effects: decrease in systemic arterial blood pressure • Respiratory effects: reduce or eliminate both ventilatory drive and reflexes maintaining the airway unblocked • Hypothermia: body temperature < 36˚C • Nausea and Vomiting • Chemoreceptor trigger zone • Emergence • Physiological changes

  9. Mechanism • Early Ideas • Unitary theory of anesthesia • Anesthesia is produced by disturbance of the physical properties of cell membranes • Problematic: theory fails to explain how the proposed disturbance of the lipid bilayer would result in a dysfunctional membrane protein • Inhalational and intravenous anesthetics can be enantio-selective in their action • Focus on identifying specific protein binding sites for anesthetics

  10. Cellular Mechanism • Intravenous Anesthetics • Substantial effect on synaptic transmission • Smaller effect on action-potential generation or propagation • Produce narrower range of physiological effects • Actions occur at the synapse • Effects the post-synaptic response to the released neurotransmitter • Enhances inhibitory neurotransmission

  11. Structures • Intravenous • Inhalational Ketamine Etomidate Propofol Isoflurane Sevoflurane Halothane

  12. Molecular Actions: GABAA Receptor • Ligand-gated ion channels • Chloride channels gated by the inhibitory GABAA receptor • GABAA receptor mediates the effects of gamma-amino butyric acid (GABA), the major inhibitory neurotransmitter in the brain • GABAA receptor found throughout the CNS • Most abundant, fast inhibitory, ligand-gated ion channel in the mammalian brain • Located in the post-synaptic membrane

  13. Molecular Actions: GABAA Receptor • GABAA receptor is a 4-transmembrane (4-TM) ion channel • 5 subunits arranged around a central pore: 2 alpha, 2 beta, 1 gamma • Each subunit has N-terminal extracellular chain which contains the ligand-binding site • 4 hydrophobic sections cross the membrane 4 times: one extracellular and two intracellular loops connecting these regions, plus an extracellular C-terminal chain

  14. Molecular Action: GABAA Receptor

  15. Molecular Action: GABAA Receptor • Receptor sits in the membrane of its neuron at the synapse • GABA, endogenous compound, causes GABA to open • Receptor capable of binding 2 GABA molecules, between an alpha and beta subunit • Binding of GABA causes a conformational change in receptor • Opens central pore • Chloride ions pass down electrochemical gradient • Net inhibitory effect, reducing activity of the neuron

  16. Mechanism of Propofol • Action of anesthetics on the GABAA receptor • Binding of anesthetics to specific sites on the receptor protein • Proof of this mechanism is through point mutations • Can eliminate the effects of the anesthetic on ion channel function • General anesthetics do not compete with GABA for its binding on the receptor

  17. Mechanism of Propofol • Inhibits the response to painful stimuli by interacting with beta3subunit of GABAA receptor • Sedative effects of Propofol mediated by the same GABAA receptor on the beta2 subunit • Indicates that two components of anesthesia can be mediated by GABAA receptor • Action of Propofol • Positive modulation of inhibitory function of GABA through GABAA receptors

  18. Mechanism of Propofol • Parenteral anesthetic • Small, hydrophobic, substituted aromatic or heterocyclic compound • Propofol partitions into lipophilic tissues of the brain and spinal cord • Produces anesthesia within a single circulation time

  19. Metabolism and Toxicity • Recovery after doses/infusion of Propofol is fast • Half-life is “context-sensitive” • Based on its own hydrophobicity and metabolic clearance, Propofol’s half-life is 1.8 hours • Accounts for the quick 2-4 minute distribution to the entire body • Expected for a highly lipid-soluble drug • Anesthetic of choice

  20. Metabolism and Toxicity • Propofol is extensively metabolized • 88% of an administered dose appearing in the urine • Eliminated by the hepatic conjugation of the inactive glucuronide metabolites which are excreted by the kidney

  21. Adverse Effects of Propofol • Hypotension • Arrhythmia • Myocardial ischemia • Restriction of blood supply • Confusion • Rash • Hyper-salivation • Apnea

  22. Remaining Questions • At the molecular level, where are the binding sites on the GABAA receptor? • Which neuronal structures are most important for the anesthetic end points of interest?

  23. Latest Discoveries: Implications for the Medicinal Chemist • Explosion of new information on the structure and function of GABAA receptors • Cloning and sequencing multiple subunits • Advantageous: large number of different subunits (16) allows for a great variety of different types of GABAA receptors that will likely differ in drug sensitivity • Propofol delivery technology • Mechanically driven pumps • Computer-controlled infusion systems • “target controlled infusion” (TCI)

  24. Latest Discoveries: Implications for the Medicinal Chemist • Findings collectively enhance the understanding on the mechanism of action of Propofol • Allows the medicinal chemist to rationally design analogues with better pharmacological profiles

  25. Current News • March 30, 2007 • The Wall Street Journal: “FDA Wants More Research on Anesthesia Risk to Kids” • Anesthesia can be harmful to the developing brain, studies on animals suggest, raising concerns about potential risks in putting young children under for surgery • Prolonged changes in behavior; memory and learning impairments • Relevance of the animal findings to pediatric patients is unknown

  26. Thank you!

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