Sedative-Hypnotic Drugs PDF
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Abenezer Aklog
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This document provides a detailed overview of sedative-hypnotic drugs. It covers their mechanisms of action, clinical uses, and side effects. The document is aimed at medical students.
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Central Nervous system pharmacology for medical students Sedative-hypnotic drugs 1 Abenezer Aklog (B.Pharm, MSc.) Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic Drugs 2 A sedative drug...
Central Nervous system pharmacology for medical students Sedative-hypnotic drugs 1 Abenezer Aklog (B.Pharm, MSc.) Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic Drugs 2 A sedative drug (aka Anxiolytic) decreases activity, moderates excitement, and calms the recipient Commonly used in the management of Anxiety Anxiety is an unpleasant state of tension, apprehension, or uneasiness mostly to perceived threat GAD, Panic Disorder, SAD, PTSD, OCD A hypnotic drug produces drowsiness and facilitates the onset and maintenance of a state of sleep that resembles natural sleep Hypnotic effects involve more pronounced depression of the CNS than sedation This can be achieved simply by increasing the dose of sedative- hypnotic drug Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 3 Sedatives produce therapeutic effects at concentrations lower than those causing substantial CNS depression E.g. Benzodiazepine sedative-hypnotics do not produce generalized CNS depression (like surgical anesthesia, or respiratory depression) Important exception is midazolam (dec. tidal volume and RR) Whereas, older sedative-hypnotics, like barbiturates, produce a dose dependent generalized depression that may even lead to Dose-response curves for two death hypothetical sedative-hypnotics. Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 4 Benzodiazepines (BZDs) Promote the binding of the major inhibitory neurotransmitter GABA to the GABAA receptor A number of distinct mechanisms of action, reflecting involvement of specific subunits of the GABAA receptor Likely contribute to distinct effects of various benzodiazepines Sedative-hypnotic, Muscle-relaxant, Amnesic, and Anticonvulsant effects Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 5 Benzodiazepines (BZDs) Examples of BZDs o “Azepam”s o “Azolam”s Chlordiazepoxide Diazepam Midazolam Clorazepate Lorazepam Alprazolam Clonazepam Triazolam Flurazepam Estazolam Oxazepam Quazepam Temazepam Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 6 Benzodiazepines (BZDs) Mechanism of Action Are allosteric modulators of GABAA receptor function Enhance GABA binding and increase Cl- conductance resulting in hyperpolarization and decrease in synaptic transmission BZDs intensify GABA mediated increase in Cl- conductance (by inc frequency of channel opening) GABAA R has 5subunits (most are composed of 2α1, 2β2, and 1γ2) GABA binds between adjacent α1 and β2 subunits BZDs bind between adjacent α1 and γ2 subunits Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 7 Benzodiazepines (BZDs) Mechanism of Action In pharmacodynamic terms, agonists at the BZD binding site shift the GABA concentration-response curve to the left BZD effects depend on the presynaptic release of GABA; In the absence of GABA, BZDs have no effects on GABAA receptor function Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 8 Benzodiazepines (BZDs) Pharmacokinetics All BZDs are absorbed completely except clorazepate Clorazepate, a prodrug, is converted to its active form nordiazepam by acid hydrolysis in the stomach which is then absorbed Rate of oral absorption is affected by many factors including lipophilicity Absorption of triazolam, diazepam, and nordiazepam is more rapid Lipid solubility also plays a major role in determining the rate at which a BZDs enters the CNS Highly lipophilic agents have rapid onset of action Sedative-Hypnotic Drugs Abenezer Aklog 9 Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 10 Benzodiazepines (BZDs) Pharmacokinetics Hepatic metabolism accounts for the clearance of all BZDs Metabolism takes place both by dealkylation (phase 1 especially by CYP 3A4) and conjugation (phase 2) reactions Oxazepam, lorazepam are directly conjugated by phase2 enzymes Many phase I metabolites of BZDs are pharmacologically active, some with long half-lives Desmethyldiazepam (t1/2>40hrs) is an active metabolite of diazepam, chlordiazepoxide, prazepam, and clorazepate Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 11 Benzodiazepines (BZDs) Pharmacokinetics Biotransformation of benzodiazepines. Boldface, drugs available for clinical use in various countries;*, active metabolite. Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 12 Benzodiazepines (BZDs) System effects o CNS effects Reduction of anxiety and aggression- at low doses Induction of sleep- at high doses Reduction of muscle tone and coordination Anticonvulsant effects o CVS When BZPs are given per orally –no effect on HR and BP However, after IV route they cause profound hypotension and cardiac arrest Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 13 Benzodiazepines (BZDs) System effects o Respiratory effects They have little respiratory depression when used alone w/out CNS depressant However, it exacerbate some respiratory disorder such: Hypoventilation and hypoxemia-in patients with COPD Apnea (pause in breathing) o Skeletal muscle They cause relaxation of skeletal muscle Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 14 Benzodiazepines (BZDs) Clinical Uses o Anxiety Effective in the management of acute anxiety states They reduce anxiety through their effects on the limbic system, a neuronal network associated with emotionality o Insomnia Decrease latency time to falling asleep, reduce awakenings, and increase total sleeping time Promote sleep through effect on cortical areas and the sleep- wakefulness clock Triazolam, Temazepam, Flurazepam, Estazolam Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 15 Benzodiazepines (BZDs) Clinical Uses o Amnesia Shorter-acting agents are often employed as premedication for anxiety-provoking and unpleasant procedures (e.g. Endoscopy) Resulted from effect on hippocampus and cerebral cortex o Acute alcohol withdrawal- Alleviate the withdraw syndromes BZDs’ benefits derived from cross-tolerance with alcohol Reduce the risk of withdrawal-related seizures Chlordiazepoxide, Clorazepate, Diaz, Loraz, and Oxazepam Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 16 Benzodiazepines (BZDs) Clinical Uses o Seizure/Epilepsy Inhibit the development and spread of epileptiform electrical activity in the CNS Clonazepam (seizure), Lorazepam, and Diazepam (Status Epilepticus) o Muscular disorders Relaxing the spasticity of skeletal muscle, probably by increasing presynaptic inhibition in the spinal cord and cerebellum Diazepam Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 17 Benzodiazepines (BZDs) Side Effects Hypnotic doses of cause varying degrees of Light-headedness, lassitude, increased reaction time Motor incoordination, impairment of mental and motor functions, confusion, and anterograde amnesia Impair driving and other psychomotor skills, especially if combined with ethanol Other common side effects Weakness, headache, blurred vision, vertigo, nausea and vomiting, epigastric distress Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 18 Novel Benzodiazepine Receptor Agonists Hypnotics in this class are commonly referred to as “Z compounds” Zolpidem, Zaleplon, and EsZopiclone Z compounds are structurally unrelated to each other and to BZDs But therapeutic efficacy as hypnotics is due to agonist effects at the BZD site of the GABAA receptor Z compounds are less effective as anticonvulsants or muscle relaxants May be due to selectivity for GABAA receptors containing the α1 subunit Have replaced BZDs for the treatment of insomnia Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 19 Novel Benzodiazepine Receptor Agonists Zaleplon Bind to GABAA receptors containing the α1 receptor subunit Decreases the latency of sleep onset with little effect on total sleep time (t1/2 is short) FDA-approved for use up to 7–10 days at a time Has sustained hypnotic efficacy without occurrence of rebound insomnia on abrupt discontinuation Not associated with morning sedation, delayed reaction time, and anterograde amnesia at therapeutic doses Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 20 Novel Benzodiazepine Receptor Agonists Zaleplon Pharmacokinetics Absorbed rapidly and reaches peak plasma conce. in about 1h Presystemic metabolism limits its bioavailability (BA-30%) Metabolized largely by aldehyde oxidase and to a lesser extent by CYP3A4 and has shorter t1/2 (~1hr) Cimetidine increases the peak plasma conce. of Zaleplon Dosage should be reduced in patients with hepatic impairment and in the elderly Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 21 Novel Benzodiazepine Receptor Agonists Zolpidem Effective in shortening sleep latency and prolonging total sleep time in patients with insomnia (t1/2 is relatively long) After D/C, the beneficial effects on sleep reportedly persist for up to 1week (with mild rebound insomnia on the 1st day of D/C) Approved only for the short-term treatment of insomnia (7-10days) Differ from Zaleplon in that late night admin. results in residual effects Morning sedation, delayed reaction time, and anterograde amnesia Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 22 Novel Benzodiazepine Receptor Agonists Zolpidem Pharmacokinetics Absorbed readily from the GI tract; First-pass hepatic metabolism results in an bioavailability of ~70% BA may decrease when the drug is ingested with food Eliminated almost entirely by conversion to inactive products in the liver (CYP3A4) Has a t1/2 of ~2hrs, which is sufficient to cover most of a typical 8hr sleep period Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 23 Novel Benzodiazepine Receptor Agonists Eszopiclone Used for the long-term (~12 months) treatment of insomnia, for sleep maintenance, and to decrease the latency to onset of sleep No tolerance was observed, and no signs of serious withdrawal, such as seizures or rebound insomnia, were seen on D/C of the drug Pharmacokinetics Absorbed rapidly after oral administration (BA~80%) 50%–60% bound to plasma proteins (has large Vd) Metabolized by CYPs 3A4 and 2E1, and has a t1/2 of about 6hr Sedative-Hypnotic Drugs Abenezer Aklog 24 Onset and duration of action of the commonly used nonbenzodiazepine hypnotic agents Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 25 Benzodiazepine Receptor Antagonist Flumazenil Binds with high affinity to the BZD binding site on the GABAA R It competitively antagonizes the binding and allosteric effects of BZDs and other ligands (like “Z Cpds”) Antagonizes both the electrophysiological and behavioral effects of agonist and inverse-agonist (β-Carboline) Available only for intravenous administration (Oral BA only 25%) Eliminated almost entirely by hepatic metabolism to inactive products with a t1/2 of about 1hr Duration of clinical effects usually is only 30–60 min Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 26 Benzodiazepine Receptor Antagonist Flumazenil Primarily indicated for Management of suspected benzodiazepine overdose and Reversal of sedative effects produced by benzodiazepines Because all BZDs have a longer duration of action than flumazenil Sedation commonly recurs, requiring repeated administration Seizures or other withdrawal signs may be precipitated in patients in whom tolerance or dependence may have developed ADRs- Agitation, confusion, dizziness, and nausea Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 27 Benzodiazepine Overdose May be intentional or secondary to accumulation of doses Symptoms: somnolence, impaired coordination, slurred speech, diminished reflexes, confusion, respiratory depression, hypotension Treatment options Supportive and symptomatic care Gastric lavage (removing poison from GIT) Activated Charcoal (adsorb poisonous substance) IV hydration and maintain adequate airway IV Flumazenil:-1mg infused over 1-3min Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 28 Barbiturates Once used extensively as sedative-hypnotic drugs Largely replaced by much safer BZDs and Z cpds Barbiturates induce Tolerance, Drug-metabolizing enzymes, Physical dependence, and Very severe withdrawal symptoms Increase in lipid solubility of barbs decrease latency to onset of activity, Decrease duration of action Accelerate metabolic degradation, and increase hypnotic potency Sedative-Hypnotic Drugs Abenezer Aklog THERAPEUTIC USES OF BARBITURATES 29 Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 30 Barbiturates Pharmacological properties Reversibly depress the activity of all excitable tissues in CNS Direct effects on peripheral excitable tissues are weak Pharmacokinetics For sedative-hypnotic use, they usually are administered orally Na+ salts are absorbed more rapidly than the corresponding free acids Onset of action varies from 10 to 60 min and is delayed by the presence of food Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 31 Barbiturates Pharmacokinetics Intravenous route usually is reserved for Management of status epilepticus (phenobarbital sodium) or Induction/maintenance of general anesthesia (thiopental/methohexital) Distribute widely in the body and readily cross the placenta Can injure developing fetus and may cause dependence (3rd trimester) Except for the less lipid-soluble aprobarbital and phenobarbital Nearly complete metabolism or conjugation of barbiturates in the liver precedes their renal excretion Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 32 Barbiturates Pharmacokinetics Oxidation of radicals at C5 is the most important biotransformation that terminates biological activity About 25% of phenobarbital and nearly all of aprobarbital are excreted unchanged in the urine Renal excretion can be increased greatly by osmotic diuresis or alkalinization of the urine t1/2 of biotransformable barbs increase in cirrhosis pts, elderly, infants, and pregnant woman Repeated administration, especially of phenobarbital, shortens the t1/2 of barbiturates (b/c of induction of enzymes) Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 33 Barbiturates Pharmacodynamics Bind to a distinct allosteric site on the GABAA R and enhance inhibition of synaptic transmission mediated by GABA Binding leads to an increase in the mean open time of Cl- channel At higher conce., barbs directly activate channel opening, even in the absence of GABA Also reportedly inhibit excitatory AMPA/kainate R and inhibit glutamate release (Via effect on VG Ca2+ channel) These multiple actions, may explain the potent CNS depressant effects of barbs compared to BZDs Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 34 Barbiturates Pharmacodynamics o Effects in the CNS Can produce all degrees of depression of the CNS, ranging from mild sedation to general anesthesia Those containing a 5-phenyl substituent (e.g., phenobarbital and mephobarbital), have selective anticonvulsant activity Except for anticonvulsant activity, they show low degree of selectivity and have low therapeutic index Barbiturates increase reactions to painful stimuli Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 35 Barbiturates Pharmacodynamics o Effects on stages of sleep Hypnotic doses increase the total sleep time and alter the stages of sleep in a dose-dependent manner Tolerance to the effects on sleep occurs within a few days Rebound insomnia may occur up on discontinuation o Tolerance, Abuse, and Dependence With chronic administration of gradually increasing doses, pharmacodynamics tolerance continues to develop over months Readily to sedative, hypnotic, and euphoric effects than toxic effects Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 36 Barbiturates Pharmacodynamics o Tolerance, Abuse, and Dependence Pharmacodynamic tolerance to barbiturates confers cross-tolerance to all general CNS depressant drugs, including ethanol Pharmacokinetic tolerance reaches its peak in a few days to a week Increase in the rate of drug metabolism (metabolic tolerance) Like other CNS depressant drugs, barbiturates are abused, and some individuals develop physical dependence Perceived relief of anxiety, euphoria, disinhibition, and promotion of sleep Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 37 Barbiturates Pharmacodynamics o Respiration Only slightly depress protective reflexes until the degree of intoxication is sufficient to produce severe respiratory depression Coughing, sneezing, hiccoughing, and laryngospasm may occur Doses three times greater than that used normally to induce sleep Eliminate neurogenic, hypoxic, and chemoreceptor drive for respiration o Cardiovascular system Sedative/hypnotic doses don’t produce significant overt CV effect Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 38 Barbiturates Pharmacodynamics o Cardiovascular system Barbiturates can blunt cardiovascular reflexes by partial inhibition of ganglionic transmission Other CV effects include a decrease in renal and cerebral blood flow with a marked fall in CSF pressure o GI Tract Decrease the tone of the GI musculature and the amplitude of rhythmic contractions A hypnotic dose doesn’t significantly delay gastric emptying Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 39 Barbiturates Pharmacodynamics o Liver Acutely, they inhibit the biotransformation of other drugs (Compete) Chronic Admn. Increases the metabolism of drugs (Induction) Glucuronic transferases and CYPs 1A2, 2C9, 2C19, and 3A4 o Kidney Severe oliguria or anuria may occur in acute barbiturate poisoning largely as a result of the marked hypotension Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 40 Barbiturates Side Effects Residual CNS depression sometimes is evident the following day Distorted Mood, impaired judgment and fine motor skill Vertigo, N,V,D, and sometimes excitement Allergic reactions occur, especially in persons with asthma, urticaria, angioedema, or similar conditions Attributed to Histamine release from the mast cells Absolutely contraindicated in pts with acute intermittent porphyria or porphyria variegata Barbiturates enhance porphyrin synthesis Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 41 Barbiturates Drug Interactions Cause severe depression when combined with other CNS depressant Ethanol, 1st gen. Antihistamine, and Antipsychotics Isoniazid, Methylphenidate, MAOIs increase CNS depressant effect Greatest number of DIs results from induction of hepatic CYPs Endogenous steroid hormones- Endocrine disturbance Oral contraceptives- unwanted pregnancy Barbiturates also induce the hepatic generation of toxic metabolites of chlorocarbons Facilitates periportal necrosis of the liver Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 42 Barbiturates Barbiturate Poisoning Most of the cases are the result of attempts at suicide But some are from accidental poisonings in children or drug abusers Severe poisoning likely occurs when >10 times the full hypnotic dose has been ingested at once In severe intoxication Patient is comatose; respiration is affected early (shallow breathing) BP falls (Depression of cardiac contractility and sympathetic ganglia) Pulmonary complications (atelectasis, edema, and bronchopneumonia) Renal failure- fatal complications of barbs poisoning Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 43 Barbiturates Treatment of acute Barbiturate Poisoning Is based on general supportive measures Use of CNS stimulants is contraindicated (inc. mortality rate) Hypovolemia must be corrected, and if necessary, the BP can be supported with dopamine If renal and cardiac functions are satisfactory, and the patient is hydrated Forced diuresis and alkalinization of the urine will hasten the excretion of phenobarbital Mechanical ventilation and hemodialysis –used when indicated Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 44 Miscellaneous Sedative-Hypnotic Drugs Except ramelteon and meprobamate, the pharmacological action of paraldehyde and chloral hydrate resembles that of barbiturates Are general CNS depressants that can produce profound hypnosis Effects on the stages of sleep are similar to those of the barbiturates Therapeutic indices are low, and acute intoxication, which produces respiratory depression and hypotension, are managed same as barbs Chronic use can result in tolerance and physical dependence Syndrome after chronic use can be severe and life threatening Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 45 Miscellaneous Sedative-Hypnotic Drugs Buspirone Has selective anxiolytic effects (mainly chronic treatment of GAD) Relieves anxiety without causing marked sedative, hypnotic, or euphoric effects (has no muscle relaxant/anticonvulsant effect) Exert its anxiolytic effects by acting as a partial agonist at brain 5- HT1A receptors (also has affinity for D2 R) Has a slow onset of action and is not effective for acute anxiety state Rapidly absorbed orally but undergoes extensive first-pass metabolism Elimination half-life is 2-4hrs but increase with liver dysfunction Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 46 Melatonin Congeners Melatonin is serotonin derivative (N-acetyl-5-methoxytryptamine) Produced and released primarily at night from pineal gland Play a role in the sleep-wake behavior of humans In the brain, MT1 and MT2 receptors are found in the suprachiasmatic nucleus of the hypothalamus Are seven-transmembrane Gi protein-coupled receptors Activation of the MT1 receptor results in sleepiness, Whereas the MT2 receptor may be related to the light-dark synchronization of the biologic circadian clock Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 47 Melatonin Congeners Ramelteon Synthetic tricyclic analogue of melatonin, approved in the U.S. for the treatment of insomnia, specifically difficulties of sleep onset Has agonistic effect on both MT1 and MT2 R Clinical Pharmacology Prescribing guidelines suggest that an 8-mg tablet be taken about 30min before bedtime Rapidly absorbed from the GI tract but has high first-pass effect Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 48 Melatonin Congeners Ramelteon Clinical Pharmacology Largely metabolized by hepatic CYPs 1A2, 2C, and 3A4, with a t1/2 of about 2h Fluvoxamine, strong inhibitors of CYP1A2, can increase the levels of ramelteon Tolerance doesn’t develop to the sleep induction effect even after long periods of admn. (~6months) No evidence of rebound insomnia and withdrawal effect Ramelteon is not a controlled substance (no risk of dependence) Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 49 Miscellaneous Sedative-Hypnotic Drugs Meprobamate An antianxiety and sedative-hypnotic agent Pharmacological actions resemble those of BZDs, although it can cause CNS depression, it cannot produce anesthesia Have a mild analgesic effect in pts with musculoskeletal pain Well absorbed when administered orally Metabolized in the liver by hydroxylation and glucuronidation Abrupt D/c evokes a withdrawal syndrome usually characterized by anxiety, insomnia, and tremors Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 50 Miscellaneous Sedative-Hypnotic Drugs Other Agents Etomidate- an IV anesthetic Clomethiazole- has sedative, muscle relaxant, and anticonvulsant properties. High therapeutic index but affected by alcohol Propofol- has profound use in intensive care sedation in adults Non-prescription Hypnotic Drugs Antihistamines diphenhydramine and doxylamine are FDA- approved as OTC sleep aids Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 51 Miscellaneous Sedative-Hypnotic Drugs New and Emerging Agents Suvorexant Inhibitor of orexin 1 and 2 receptors (GPCRs) used to treat insomnia Orexins are peptide NTs found in specific hypothalamic neurons Involved in the control of wakefulness and that are silent during sleep Orexins promote wakefulness, while antagonists at orexin receptors enhance REM and non-REM sleep Should be taken within 30min of going to bed Common adverse reaction is daytime somnolence Sedative-Hypnotic Drugs Abenezer Aklog Sedative-Hypnotic cont... 52 Miscellaneous Sedative-Hypnotic Drugs New and Emerging Agents Doxepine- a tricyclic antidepressant Indicated for the treatment of difficulties with sleep maintenance Acts presumably via antagonism of H1 R function at low doses Can worsen suicidal ideation and depression Pregabalin Anxiolytic agent that binds to Ca2+ channel Used to manage insomnia in pts with GAD For induction and maintenance of sleep Sedative-Hypnotic Drugs Abenezer Aklog 53 Sedative-Hypnotic Drugs Abenezer Aklog
