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Common Drug Poisonings: Tricyclic Antidepressants, Benzodiazepines, and Antipsychotics

This article provides information on common drug poisonings, including tricyclic antidepressant poisoning, benzodiazepine poisoning, and antipsychotic poisoning. It covers clinical manifestations, management, and antidotes for each type of poisoning.

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Common Drug Poisonings: Tricyclic Antidepressants, Benzodiazepines, and Antipsychotics

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  1. مسمومیتهاي شايعداروئی منابع • -1- Goldfrank’sToxicologic Emergencies2015 • 2- www.emedicine / Emergency Medicine / Toxicology

  2. فراواني مسموميت های دارویی • Mixed drug ingestion • مواد مخدر –مواد محرک • ضد افسردگي سه حلقه اي • أنتي سايكوتيكها • بنزو ديازپين ها • بتابلوکرها • مسكن ها

  3. Tricyclic antidepressant poisoning داروهاي ضد افسردگي

  4. داروهاي ضد افسردگي • آ مي تريپتيلين - نورتريپتيلين...ما پروتيلين -آموكساپين • > 1 g : Life treatening • one pill can kill (children) • شروع علائم سريع )خطرناکترین لحظات 1-2 ساعت اول پس از خوردن تا 6 ساعت ) • تغییر وضعیت ناگهانی

  5. Clinical manifestations Delirium, Hallucination, Hypertermia, ….

  6. Hypotension Wide QRS (> 0.10 s) Ventricular Tachycardia

  7. Tricyclic AntidepressantsSymptoms • 1- Midriasis ; Tachycardia • 2- Coma, 3- Delirium • 4- Seizures • 5- Hypotension • 6- QRS > 0.1s ; R avR>= 3 mm ; Right Axis deviation ; Arrhythmias (VT) • ECG is the single most important test to determine diagnosis and prognosis

  8. Management of TCA poisoning 1- ABCD ( Antidote) • A:Airway compromise (Artificial airway, Intubation) • B: Breathing difficulties (Oxygen, Intubation, Mechanical ventilation) • C:Circulation Problems (IV line; ECG, Manage hypotension, VT) • D: Drugs (Coma : Thiamine- Glucose-Naloxone –Oxygen)

  9. Antidote: Sodium Bicarbonate Hypotension Arrythmia, Wide QRS > 0.1 s, R avR 3 mm Seizure (wide QRS) 1-2 mEq / kg bolus , Infusion (50-150 mEq / L D5W) + repeated bolus (ABG) End point: Serum pH ( 7.45-7.55)

  10. Seizure: Diazepam 0.1-0.2 mg/kg (5-10 mg), Midazolam 0.1 mg/kg, NaHCO3 • Hyotension: N.S., NaHCO3, Norepinephrine (0.1-0.2 ug/kg/min), Dopamine (10-20 ug/kg/min) • Wide QRS, R/avR>3 mm: NaHCO3 • Coma: Glucose, Naloxone, Thiamine • Delirium: Benzodiazepines

  11. Ventricular Arrhythmias (VT) • NaHCO3 (1-2 meq/kg) 5 min • Lidocaine: 1-1.5 mg/kg slow IV bolus over 2-3 min • up to 3 mg/kg total • infusion: 1-4 mg/min IV • IO/ET • Monitor: ECG • PH: 7.45-7.55

  12. Management of TCA Poisoning • ABCD , Antidote • Gastric Lavage (GL) • Activated Charcoal(AC) 1 g/kg, 50-100 g • urine toxicology screen

  13. Contraindicated medications • beta-blockers, • calcium channel blockers, • class IA (procainamide, quinidine, disopyramide, moricizine), • class IC (flecainide, propafenone), • and possibly class III (bretylium, amiodarone,sotalol) antidysrhythmics.

  14. Management of TCA Poisoning • Rapidly transport all patients with possible TCA ingestion to the hospital because clinical deterioration often occurs rapidly after overdose. • Supplemental oxygen and airway support (Intubation,..) • Intravenous access, Cardiac monitoring • Rapid glucose determination (finger stick) • GL + Activated charcoal • Sodium bicarbonate should be considered in life-threatening circumstances in the pre-hospital setting.

  15. Antipsychotics • Large toxic to therapeutic ratio • Clinical manifestations • Antichlinergic (midriasis, Tachycardia,….) •  receptor blocking (Hypotension, Miosis):Chlorpromazine • CNS (Coma, seizure,…) • Dystonic reaction (Thiotexene, halloperidol, Perphenazine, Trifluperazine,..) • Cardiovascular (Mesoridazime, Thioridazine, Chlorpromazine, Halloperidol) • Respiratory depression ( Coma)

  16. Management ABCD اكسيژن لوله گذاري داخل تراشه + ساكشن كردن بررسي نياز به گلوكز ((Counsciousness نالوكسان (Respiratory depression , pin point pupil ) Gastric Evacuation دادن زغالفعال 1 g/kg Close Observation; Supportive treatment

  17. Seizure: Diazepam 0.1-0.2 mg/kg (5-10 mg), Midazolam 0.1 mg/kg • Hyotension: N.S., Norepinephrine (0.1-0.2 ug/kg/min), Dopamine (10-20 ug/kg/min) • Coma: Glucose, Naloxone, Thiamine • Dystonic reaction: Diphenhydramine or Biperdine or Benzodiazepine (alternative) • Wide QRS: NaHCO3

  18. Benzodiazepine Poisoning • CNS Depression (Somnolence, Stupor, Coma), Miosis, Ataxia • Deep Coma, respiratory arrest (rare)

  19. Symptoms of BZD overdose may include the following • Dizziness • Confusion • Drowsiness • Blurred vision • Anxiety • Agitation

  20. Findings on physical examination may include the following: • Nystagmus, Slurred speech • Ataxia, Coma, Hypotonia • Weakness, impairment of cognition • Amnesia, Paradoxical agitation • urine toxicology screen

  21. Managment of BZD Poisoning ABCD Antagonist: Flumazenil pure BZD overdose + verbally unresponsive +no history of long-term BZD use or seizure disorder not recommended for use by pre-hospital personnel Contraindication(past history of seizure, co ingestion with drugs induced seizure e.g. TCA; BZD addiction) • Decontamination within 1-2 h of ingestion Gastric Lavage + Activated charcoal

  22. Flumazenil • 0.1-0.2 mg IV over 15-30 sec • IF no response after 30 sec, administer 0.3 mg over 30 sec 1 min later • Rarely patient may require titration up to total dose 5 mg; IF no response after 5 min, sedation unlikely to be secondary to benzodiazepines

  23. Beta-Adrenergic Receptor Antagonists

  24. In use for nearly 50 years. • treating hypertension and other cardiovascular disorders • migraine headaches, • anxiety, • and various other disorders. • As a result of their expanded use, the incidence of overdose with these agents has also increased.

  25. Table 1-1* B-Adrenergic Receptor Antagonist Pharmacologic Profile

  26. Clinical Manifestations of B-Adrenergic Antagonist Toxicity

  27. Increased PR intervals • Loss of atrial activity • Atrioventricularjunctional rhythm • Widening of the QRS complex • Atrioventricular block • Asystole • prolonged QT interval: sotalol overdose. • VF, VT: uncommon (sotalol)

  28. Diagnosis • History • Clinical presentation • ECG, ABG/VBG • serum glucose and potassium levels.

  29. Treatment end points • HR>60 • SBP>90mmHg • Evidence of good organ perfusion Evidence of good organ perfusion (improved mentation or urine output)

  30. Mangement • ABCD Bradycardia • Atropine (1 mg..>3 mg) • Pace

  31. Mangement (Hypotension) • Isotonic IV fluid (20 mL/kg) • Glucagon (5-10 mg IV slow) (50-150 mcg/kg IV over 1 minute) Infusion: 3-5 mg/hr or 50-100 mcg/kg/hrIV titrate to response • Epinephrine for hypotension, bradycardiaUnresponsive to atropine or pacing: 2-10 mcg/min by IV infusion or 0.1-0.5 mcg/kg/min (7-35 mcg/min in 70 kg patient); titrate to response • Calcium Chloride (1g IV central line/ over 10-20 min (emergent 5 min) slow infusion • Insulin: 0.1-1 U/kg/h + Hypertonic glucose (10%,20,%, 50% 1 g/kg, check BS/30min) (Dextrose infusion of 10-75 g/h may be required) • Dopamine (5-20 ug/kg/min),Norepinephrine (0.1-0.2 ug/kg/min)

  32. Insulin-Glucose • should be considered for overdoses that are refractory to crystalloids, glucagon, and catecholamine infusions. • monitoring serum glucose and potassium levels • Monitoring must be conducted regularly during high-dose insulin therapy and for up to 24 hours after its discontinuation. • Dextrose supplementation is typically required to maintain euglycemia

  33. Benzodiazepines : if seizures occur. • Hemodialysis: severe cases of atenolol overdoses because atenolol is less than 5% protein bound and 40-50% is excreted unchanged in urine. Nadolol, sotalol, and atenolol (low lipid solubility, low protein binding) reportedly are removed by hemodialysis. Acebutolol is dialyzable. • Consider hemodialysis or hemoperfusiononly when treatment with glucagon and other pharmacotherapy fails. • Cardiac pacing: Cardiac pacing may be effective in increasing the rate of myocardial contraction. • cardiac pacing for patients unresponsive to pharmacologic therapy torsade de pointes unresponsive to magnesium • Resuscitation should be aggressive and prolonged.

  34. Gastric lavagemay be beneficial if the patient presents to the ED within 1-2 hours of ingestion. • Activated charcoal • Although most useful if used within 4 h of ingestion, repeated doses may be used, especially with ingestions of sustained-released agents. • Adult:1 g/kg PO up to 50-100 g • Pediatric: 1-2 g/kg PO , up to 15-30 g

  35. با تشكر

  36. Glucagon can enhance myocardial contractility, heart rate, and atrioventricular conduction; • Load: 50-150 mcg/kg IV over 1 minute, THEN  • 3-5 mg/hr or 50-100 mcg/kg/hr IV; titrate infusion to achieve adequate clinical response

  37. Dopamine • 5-15 mcg/kg/min IV (medium dose): May increase heart rate, and cardiac contractitlity • 20-50 mcg/kg/min IV (high dose): May increase blood pressure and stimulate vasoconstriction; may not have a beneficial effect in blood pressure; may increase risk of tachyarrhythmias • May increase infusion by 1-4 mcg/kg/min at 10-30 min intervals until optimum response obtained • Titrate to desired response

  38. calcium • Beta-blocker Overdose, Refractory to Glucagon & High Dose Vasopressor • Calcium chloride 1000 mg IV bolus via central line  over 10-20 min (emergent 5 min)

  39. Insulin-Glucose •  The currently recommended regimen is a 1 U/kg of an insulin bolus followed by continuous infusion of 1-10 U/kg/h, but boluses of up to 10 U/kg and continuous infusions as high as 22 U/kg/h have been used with good outcomes and minimal adverse events.  Dextrose infusion of 10-75 g/h may be require

  40. Acetaminophen • Commonest drug used DANGEROUS , PEOPLE DON’T KNOW IT • YOU FEEL WELL AND THEN THE LIVER FAILURE SETS IN.. • NAPQI (TOXIC mtetabolite) • Glutathione • Toxic dose: 7.5 g , 150 mg/kg

  41. Acetaminophen poisoning Phase 1 (0-24 h) Asymptomatic Anorexia, Nausea or vomiting, Malaise serum transaminases levels 12 hours postingestion Phase 2 (18-72 h) Right upper quadrant abdominal pain, anorexia, nausea, vomiting, rise in serum transaminases Phase 3 (72-96 h) Hepatic necrosis with continued abdominal pain, Jaundice , Coagulopathy, Hepatic encephalopathy, Renal failure, Fatality • Phase 4 (4 d to 3 wk) • Complete resolution of symptoms (7-10 days), or death, • Complete heaptic recovery (3-6 months)

  42. Acetaminophen ingestion should be considered as a potential cause of illness in patients who present with hepatic dysfunction of unknown etiology. • Acetaminophen crosses the placenta, and the fetal liver is able to elaborate NAPQI by 14 weeks of gestation. A delay in treating pregnant patients with antidotal therapy is associated with fetal demise.

  43. Acetaminophen Overdose-management • ABCD ( usually well systemically) • Gastric lavage, Activated charcoal • Antidote: N-Acetylcysteine, IV (20 h) • Shown to be advantageous if given in the first 8 hours • Early administration of NAC, within 8 hours of ingestion, is nearly 100% hepatoprotective • NAC should be administered if the patient presents close to or later than 8 hours after an acute ingestion or if the patient is pregnant. • Follow up

  44. ارگانوفسفره • موارداستفا د ه • براي ازبين بردن حشرات دركشاورزي • پاراتيون ؛ديازينون؛مالاتيون • بعنوانگازهاي جنگي • گاز جنگيسارين ؛سومان

  45. فارماكو كينتيك • جذب : گوارشي ؛ پوستي ؛ تنفسي ؛ چشمي • متابوليسم : كبد • دفع : دفعمتابوليتها ازطريق ادرار • نيمه عمر دفعي : 2/89ساعتدرمالاتيونو2/1روزدرمتيل پاراتيون

  46. مكانيسم اثر • مهار كننده غیر قابل برگشت آنزيم كليناستراز • شروع علا ئم : در طي چند دقيقه تا چند ساعت

  47. 1-علائم موسكاريني • افزايش ترشح بزاق (سيالوره)،اشكريزش • ابريزش از بيني • تعريق • ميوز • اسهال، درد شکمی • بی اختیاری ادرار و مدفوع • برادي كاردي ؛ هيپو تانسيون

  48. 2-علائم نيكوتيني • ضعف • فاسيكولاسيون……….فلج عضلات • تاكيكاردي • هيپر تانسيون • ميدرياز

  49. 3-علائم سيستمعصبي مركزي • اضطراب • گيجي • كما • تشنج • دپرسیون مركز تنفس و قلبي

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