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Guide –Dr Jyoti Singh
   What is a poison?

      â–Ş In common usage - poisons are
        chemicals or chemical products
        that are distinctly harmful to
        human

      â–Ş More precisely - a poison is a
        foreign chemical (xenobiotic) that
        is capable of producing a harmful
        effect on a biologic system
   Most common Pediatric Exposure
     Cosmetics and personal care products (13%)
     Cleaning substances (10%)
     Analgesics (7.8%)
     Foreign Bodies (7.4%)
     Topicals (7.4%)
     Cold and Cough Preparations (5.5%)
     Plants (4.6%)
     Pesticides (4.1%)
   May be difficult because of non-specific symptoms
   High index of suspicion - especially occult poisoning
      â–Ş history may be unreliable
      â–Ş look for corroborative history - missing pills, empty
        container

   Course that a poison runs (toxidromes) ! - may help
   Toxicology screening - helpful only in a few
â–Ş It is the association of several clinically
  recognizable features, signs, symptoms,
  phenomena or characteristics which often occur
  together, so that the presence of one feature
  alerts the physician to the presence of the
  others.
 S alivation                *D iaphoresis/diarrhea
 L acrimation              *U rination
 U rination                 *M iosis
 D efecation     *B radycardia/bronchospasm
 G I secrestion/upset      *E mesis
 E mesis              *L acrimation excess
                       *S alivation excess
Hot as a hare
Dry as a bone
Red as a beet
Mad as a hatter
Blind as a bat
bowel, bladder
lose their tone, &
heart runs alone
Hot as a hare
Dry as a bone
Red as a beet
Mad as a hatter
Blind as a bat
bowel , bladder lose
their tone, &
heart runs alone
Hot as a hare
Dry as a bone
Red as a beet
Mad as a hatter
Blind as a bat
bowel , bladder
lose their tone,
&heart runs alone
disorientation      Amphetamine
                 hallucinations      Cocaine
Hallucinogenic   hyperactive bowel   Pseudoephedrine
                 panic               Phencyclidine     Benzodiazepenes
                 seizure             Ephedrine
Toxidrome        Hypertension
                 Tachycardia
                 Tachypnea
disorientation      Amphetamine
                 hallucinations      Cocaine
Hallucinogenic   hyperactive bowel   Pseudoephedrine
                 panic               Phencyclidine     Benzodiazepenes
                 seizure             Ephedrine
Toxidrome        Hypertension
                 Tachycardia
                 Tachypnea
disorientation      Amphetamine
                 hallucinations      Cocaine
Hallucinogenic   hyperactive bowel   Pseudoephedrine
                 panic               Phencyclidine     Benzodiazepenes
                 seizure             Ephedrine
Toxidrome        Hypertension
                 Tachycardia
                 Tachypnea
disorientation      Amphetamine
                 hallucinations      Cocaine
Hallucinogenic   hyperactive bowel   Pseudoephedrine
                 panic               Phencyclidine     Benzodiazepenes
                 seizure             Ephedrine
Toxidrome        Hypertension
                 Tachycardia
                 Tachypnea
   Very diverse and varied - depends on the poison

   Clinical examination should be focused on the
    possible manifestations of common poisons in the
    geographical area
   Skin and mucosal damage
   Neurotoxic manifestations
   Cardiovascular manifestations
   Metabolic consequences
   Eye manifestations
   Hepatic , renal dysfunction
   Multiorgan dysfunction
ď‚— Respiratory

    ď‚—Airway protection

    ď‚—Respiratory failure

ď‚— Cardiovascular

    ď‚—Hypotension despite fluid challenge

    ď‚—Heart block, arrhythmias, QTc prolongation as in TCA
   Neurologic
     â–Ş Low GCS
     â–Ş Seizures

   Metabolic
     â–Ş   Hypoglycaemia
     â–Ş   Significant electrolyte abnormalities
     â–Ş   metabolic acidosis
     â–Ş   Hepatic failure
     â–Ş   Coagulopathy with bleeding
ASSESSMENT & THERAPY should
      proceed in parallel
 Treat the patient, not the poison
 Assess
   General appearance
   Work of breathing
   Circulation
 ABCDs
 IV access and monitors
 High Suspicion
 Directed exam (after ABCs)


  mental status
  vital signs
  pupillary size
  skin signs
   Airway - ensure clear airway, clear secretions, check for
    cough/gag


   Breathing - check oxygenation, supplemental O2,
    breathing pattern & adequacy


   Circulation - heart rate, rhythm, blood pressure
   Neurologic - GCS, seizures, agitation, spasms, pupils,
    autonomic dysfunction


   Miscellaneous - odour, temperature, pallor, cyanosis,
    jaundice


   Abdomen - rigidity, bleeding, urine output
 Cyanosis
  methemoglobinemia secondary to nitrites,
   nitrates, phenacetin, benzocaine-refractory tp
   o2
 Red flush
  carbon monoxide, cyanide, boric acid,
   anticholinergics
  Joundice – c cl4. paracetamol
 Dry
   anticholinergics
 Salivation
   organophosphates, carbamates
 Oral lesions
   corrosives, paraquat
 Lacrimation
   caustics, organophosphates, irritant gases
 Anti-histamine
 Anti-depressant
 Anticholinergics (atropine)
 Sympathomimetics
   amphetamine, cocaine, PCP
 Cholinergics, Clonidine
 Opiates, Organophosphates
 Phenothiazine, Pilocarpine
 Sedatives (barbiturates, ethanol)
 Alcohol
 PCP / marijuana
 LSD
 Anticholinergics
 Sympathomimetics
 Phenothiazines
 Cocaine
 Heroin
 heavy metals
 Coma
  alcohols,
  anticholinergics,
  sedative hypnotics,
  opioids,
  carbon monoxide,
  TCAs, salicylates,
  organophosphates
 Weakness/paralysis
  organophosphates, carbamates, heavy metals
 Atropine
 Salicylates
 Theophylline
 Cocaine
 TCA
 Ethanol
 Narcotics
 Carbon monoxide
 Clonidine
 Bradycardia
  digitalis, sedative hypnotics, beta blockers, opioids

 Tachycardia
  anticholinergics, sympathomimetics,
   amphetamines, alcohol, aspirin, theophylline,
   cocaine, TCAs

 Arrythmias
  anticholinergics, TCAs, organophosphates,
   digoxin, phenothiazines, beta blockers, carbon
   monoxide, cyanide
 OTC cold remedies
 Amphetamine
 PCP
 TCA
 Cocaine
 Diet pills
 Calcium channel blockers
 Carbon monoxide
 Cyanide
 Iron
 Narcotics
 Anti-hypertensives
 Met-hemoglobin
 Hypoglycemia
 Oral hypoglycemic agents
 Beta-blockers
 Insulin
 Ethanol
 Salicylates
 Alcohol
 Narcotics
 Clonidine
 Sedatives
   Of limited value

   Paracetamol levels, salicylate levels, alcohol, Red
    cell/pseudocholinesterase, anti-epileptic drug levels

   Urinary drug screen - opiates, barbiturates,
    benzodiazepines, amphetamines, cocaine
   Anion gap & Osmolal gap

   Increased anion gap (Normal 12 ± 4 mEq/L)
       â–Ş Ethylene glycol
       â–Ş Methanol
       â–Ş Salicylate poisoning

   Increased osmolal gap (Normal 5 ± 7 m osmol/kg)
       â–Ş Ethylene glycol
       â–Ş Methanol
       â–Ş Acetone, ethanol, isopropyl alcohol, propylene glycol
   Electrolytes
       â–Ş Hypokalemia
        â–Ş Isuline ,oral hypoglysemics
        â–Ş Diuretics, Methyl xanthine, Toluene
      â–Ş Hyperkalemia
        â–Ş Digoxin
        â–Ş Beta-blocker
   Liver function tests
        â–Ş Acetaminophen, Ethanol, Carbon tetrachloride
   Renal function tests
        â–Ş Ethylene glycol, NSAIDS
 ECG
    Digoxin toxicity
    TCA overdose - sinus tachycardia, QT prolongation,
      increased QRS
    Beta-blockers - conduction abnormalities
Imaging

    . CXR- hydrocarbon ingestion
     .Abdominal X-ray-- iron ingestion & radioopaque
    ingestion.
    .Oesophagoscopy -for caustic ingestion.
    . Abdominal usg- recently been used as a means of
    identifying presence of pharmaceutical material in GIT.
ď‚— Opiates
ď‚— Cocaine metabolite
ď‚— Amphetamine
ď‚— Benzodiazepines
ď‚— Barbiturates




* No urine screen can confirm intoxication, only exposure
   Reduce absorption of the toxin

   Enhance elimination

   Neutralise toxin
   Removal from surface skin & eye

   Emesis induction

   Gastric lavage

   Activated charcoal administration & cathartics

   Dilution - milk/other drinks for corrosives

   Whole bowel irrigation

   Endoscopic or surgical removal of ingested chemical
 Skin decontamination

   ▪ Important aspect – not to be neglected

   â–Ş Remove contaminated clothing

   â–Ş Wash with soap and water (soaps
     containing 30% ethanol advocated)

   â–Ş However, no evidence for benefit even in OP
     poisoning
 Gastric decontamination

    â–Ş Forced emesis if patient is awake
    â–Ş Gastric lavage
    â–Ş Activated charcoal 25 gm 2 hourly
    â–Ş Sorbitol as cathartic
   Gastric lavage

      â–Ş Gastric lavage decreases absorption by 42% if done 20
        min and by 16% if performed at 60 min

      â–Ş Performed by first aspirating the stomach and then
        repetitively instilling & aspirating fluid
      â–Ş Left lateral position better - delays spont. absorption
      â–Ş No evidence that larger tube better
      â–Ş Simplest, quickest & least expensive way
      â–Ş Choice of fluid is tap water - 5-10 ml/kg
   Gastric lavage

      â–Ş Preferrably done on awake patients

      â–Ş Presence of an ET tube does not preclude
        aspiration, though preferred if GCS is low

      â–Ş No human studies in OP poisoning showing
        benefit of gastric lavage
   Single dose activated charcoal
     0.5-1 gm/kg, adolescents 50-100 grams PO;
      maximum dose 100 grams
     More benefit if administered within 1 hour of
      ingestion, but still good for poison which slows
      gastric motility (anticholinergic, opiates,
      salicylates)
     Strongly consider for acetaminophen overdose >
      4 hours
 P – Pesticides, petroleum distillates,
  unprotected airway
 H – Hydrocarbons, heavy metals, > 1h delay
  in administration
 A – Acids, alkali, alcohol, altered level of
  consciousness, aspiration risk
 I – Iron, ileus, intestinal obstruction
 L – Lithium, lack of gag reflex
 S – seizures
 Nonabsorbable, isotonic polyethylene glycol
 Toxins “pushed” through GI tract; prevents
  absorption
 Concentration gradient created by this
  allows absorbed toxin to diffuse back into GI
  tract
 Used where toxins NOT absorbed by
  charcoal
 Recommended for:
  Iron tablets
  Lead paint chips
  Theophylline
  Crack vials/packets
  Button batteries
  Sustained release calcium channel blockers
 Bowel perforation
 Bowel obstruction
 Clinically significant gastrointestinal
  hemorrhage
 Ileus
 Unprotected or compromised airway
 Hemodynamic instability
 Uncontrollable intractable vomiting
   Methods
     â–Ş Keeping a good urine output 150-200 ml/hr
     â–Ş Alkalinisation of urine - clinical efficacy
       accepted for salicylate & phenobarbital
       poisoning
     â–Ş Extracorporeal removal
       â–Ş Hemodialysis - Barbiturates, Salicylates,
         Acetaminophen, Valproate, Alcohols,
         Glycols
       â–Ş Hemoperfusion - theophylline, digitalis, lipid
         soluble drugs
 Plasmapheresis
   Works very well with highly protein (albumin)
    bound drugs
   Not a routine methodology, but has been used
    to remove theophylline and digoxin/ digibind
    complexes
 Exchange transfusion
   Use in smaller infants where vascular access for
    extracorporeal techniques can’t be done
 Renal failure.
 Congestive heart failure (relative).
 Acute lung injury.
 Persistent CNS disturbance.
 Severe acid-base or electrolyte imbalance,
  despite appropriate treatment.
 Hepatic compromise with coagulopathy.
 Salicylate concentration (acute) >100 mg/dL.
Acetaminophen               N-acetyl cysteine
Anti-cholinergics           Physostigmine
Benzodiazepenes             Flumazenil
Ca channel blockers         Glucagon, Insulin + dextrose, Calcium
Carbamate                   Atropine
Cyanide                     Thiosulphate, nitrate
Digoxin                     Digoxin antibodies
INAH                        Pyridoxine
Methanol                    Ethanol, Fomepizole
Glycol                      Ethanol, Fomepizole
Opioid                      Naloxone
Oral hypoglycaemics         Glucose
Organophosphate             Atropine, PAM
Warfarin(rat kill poison)   Vitamin K
Iron       Desferroxamine
Copper     Penicillamine, Dimercaprol, CaEDTA
Lead       CaEDTA, Dimercaprol (BAL)
Mercury    DMPS, DMSA, BAL
Arsenic    BAL & derivatives
Antimony   BAL & derivatives
   Calcium channel blockers: bradycardia and
    hypotension; 1 - 10 mg tablet of nifedipine
   Camphor: respiratory depression and seizures; 15
    mL of Vicks vapo-rub (700 mg of camphor)
   Clonidine: severe bradycardia; 0.1 mg
   Tricyclic antidepressants: cardiovascular and CNS
    toxicity; 10-20mg/kg
   Opioids: CNS and respiratory depression; 2.5 mg of
    hydrocodone.
   Lomotil: anticholinergic overdose (tachycardia,
    seizures, coma); ½ tablet

   Salicylates: cerebral edema, acidosis, coma; ½
    teaspoon of wintergreen fatal

   Sulfonylureas: severe hypoglycemia; 1 tablet

   Toxic alcohols: cardiac and CNS depression; 2.9mL
    of 95% ethylene glycol has been fatal
National Poisons Information Centre (NPIC)
Department of Pharmacology
All India Institute of Medical Sciences
New Delhi, India
 Tel. No.: 26589391, 26593677,
 Fax: 26850691, 26862663
 Email: npicaiims@hotmail.com
provides round-the-clock, 7 days-a-week, 365
  days service on telephone.
ď‚—   Poisoning a common problem in our country

ď‚—   A high index of suspicion required to diagnose

ď‚—   Know common toxidrome & antidotes

   Charcoal is only given if likely to benefit

   Patients receiving decontamination must have airway protection
   Don’t panic and follow a plan of action
      ď‚—Decreasing absorption
      ď‚—Enhancing elimination
      ď‚—Neutralising toxins
ď‚—   Avoid potentially harmful Rxs - risk vs benefit
Approach to a poisoned child

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Approach to a poisoned child

  • 2.  What is a poison? â–Ş In common usage - poisons are chemicals or chemical products that are distinctly harmful to human â–Ş More precisely - a poison is a foreign chemical (xenobiotic) that is capable of producing a harmful effect on a biologic system
  • 3.  Most common Pediatric Exposure  Cosmetics and personal care products (13%)  Cleaning substances (10%)  Analgesics (7.8%)  Foreign Bodies (7.4%)  Topicals (7.4%)  Cold and Cough Preparations (5.5%)  Plants (4.6%)  Pesticides (4.1%)
  • 4.  May be difficult because of non-specific symptoms  High index of suspicion - especially occult poisoning â–Ş history may be unreliable â–Ş look for corroborative history - missing pills, empty container  Course that a poison runs (toxidromes) ! - may help  Toxicology screening - helpful only in a few
  • 5. â–Ş It is the association of several clinically recognizable features, signs, symptoms, phenomena or characteristics which often occur together, so that the presence of one feature alerts the physician to the presence of the others.
  • 6.
  • 7.
  • 8.
  • 9.
  • 10.  S alivation *D iaphoresis/diarrhea  L acrimation *U rination  U rination *M iosis  D efecation *B radycardia/bronchospasm  G I secrestion/upset *E mesis  E mesis *L acrimation excess *S alivation excess
  • 11.
  • 12. Hot as a hare Dry as a bone Red as a beet Mad as a hatter Blind as a bat bowel, bladder lose their tone, & heart runs alone
  • 13. Hot as a hare Dry as a bone Red as a beet Mad as a hatter Blind as a bat bowel , bladder lose their tone, & heart runs alone
  • 14. Hot as a hare Dry as a bone Red as a beet Mad as a hatter Blind as a bat bowel , bladder lose their tone, &heart runs alone
  • 15. disorientation Amphetamine hallucinations Cocaine Hallucinogenic hyperactive bowel Pseudoephedrine panic Phencyclidine Benzodiazepenes seizure Ephedrine Toxidrome Hypertension Tachycardia Tachypnea
  • 16. disorientation Amphetamine hallucinations Cocaine Hallucinogenic hyperactive bowel Pseudoephedrine panic Phencyclidine Benzodiazepenes seizure Ephedrine Toxidrome Hypertension Tachycardia Tachypnea
  • 17. disorientation Amphetamine hallucinations Cocaine Hallucinogenic hyperactive bowel Pseudoephedrine panic Phencyclidine Benzodiazepenes seizure Ephedrine Toxidrome Hypertension Tachycardia Tachypnea
  • 18. disorientation Amphetamine hallucinations Cocaine Hallucinogenic hyperactive bowel Pseudoephedrine panic Phencyclidine Benzodiazepenes seizure Ephedrine Toxidrome Hypertension Tachycardia Tachypnea
  • 19.
  • 20.
  • 21.
  • 22.
  • 23.
  • 24.
  • 25.
  • 26.
  • 27.
  • 28.
  • 29.
  • 30.
  • 31.  Very diverse and varied - depends on the poison  Clinical examination should be focused on the possible manifestations of common poisons in the geographical area
  • 32.  Skin and mucosal damage  Neurotoxic manifestations  Cardiovascular manifestations  Metabolic consequences  Eye manifestations  Hepatic , renal dysfunction  Multiorgan dysfunction
  • 33. ď‚— Respiratory ď‚—Airway protection ď‚—Respiratory failure ď‚— Cardiovascular ď‚—Hypotension despite fluid challenge ď‚—Heart block, arrhythmias, QTc prolongation as in TCA
  • 34.  Neurologic â–Ş Low GCS â–Ş Seizures  Metabolic â–Ş Hypoglycaemia â–Ş Significant electrolyte abnormalities â–Ş metabolic acidosis â–Ş Hepatic failure â–Ş Coagulopathy with bleeding
  • 35. ASSESSMENT & THERAPY should proceed in parallel
  • 36.
  • 37.  Treat the patient, not the poison  Assess  General appearance  Work of breathing  Circulation  ABCDs  IV access and monitors  High Suspicion
  • 38.  Directed exam (after ABCs)  mental status  vital signs  pupillary size  skin signs
  • 39.  Airway - ensure clear airway, clear secretions, check for cough/gag  Breathing - check oxygenation, supplemental O2, breathing pattern & adequacy  Circulation - heart rate, rhythm, blood pressure
  • 40.  Neurologic - GCS, seizures, agitation, spasms, pupils, autonomic dysfunction  Miscellaneous - odour, temperature, pallor, cyanosis, jaundice  Abdomen - rigidity, bleeding, urine output
  • 41.
  • 42.  Cyanosis  methemoglobinemia secondary to nitrites, nitrates, phenacetin, benzocaine-refractory tp o2  Red flush  carbon monoxide, cyanide, boric acid, anticholinergics  Joundice – c cl4. paracetamol
  • 43.  Dry  anticholinergics  Salivation  organophosphates, carbamates  Oral lesions  corrosives, paraquat  Lacrimation  caustics, organophosphates, irritant gases
  • 44.  Anti-histamine  Anti-depressant  Anticholinergics (atropine)  Sympathomimetics  amphetamine, cocaine, PCP
  • 45.  Cholinergics, Clonidine  Opiates, Organophosphates  Phenothiazine, Pilocarpine  Sedatives (barbiturates, ethanol)
  • 46.  Alcohol  PCP / marijuana  LSD  Anticholinergics  Sympathomimetics  Phenothiazines  Cocaine  Heroin  heavy metals
  • 47.  Coma  alcohols,  anticholinergics,  sedative hypnotics,  opioids,  carbon monoxide,  TCAs, salicylates,  organophosphates  Weakness/paralysis  organophosphates, carbamates, heavy metals
  • 48.  Atropine  Salicylates  Theophylline  Cocaine  TCA
  • 49.  Ethanol  Narcotics  Carbon monoxide  Clonidine
  • 50.  Bradycardia  digitalis, sedative hypnotics, beta blockers, opioids  Tachycardia  anticholinergics, sympathomimetics, amphetamines, alcohol, aspirin, theophylline, cocaine, TCAs  Arrythmias  anticholinergics, TCAs, organophosphates, digoxin, phenothiazines, beta blockers, carbon monoxide, cyanide
  • 51.  OTC cold remedies  Amphetamine  PCP  TCA  Cocaine  Diet pills
  • 52.  Calcium channel blockers  Carbon monoxide  Cyanide  Iron  Narcotics  Anti-hypertensives  Met-hemoglobin
  • 53.  Hypoglycemia  Oral hypoglycemic agents  Beta-blockers  Insulin  Ethanol  Salicylates
  • 54.  Alcohol  Narcotics  Clonidine  Sedatives
  • 55.
  • 56.  Of limited value  Paracetamol levels, salicylate levels, alcohol, Red cell/pseudocholinesterase, anti-epileptic drug levels  Urinary drug screen - opiates, barbiturates, benzodiazepines, amphetamines, cocaine
  • 57.  Anion gap & Osmolal gap  Increased anion gap (Normal 12 ± 4 mEq/L) â–Ş Ethylene glycol â–Ş Methanol â–Ş Salicylate poisoning  Increased osmolal gap (Normal 5 ± 7 m osmol/kg) â–Ş Ethylene glycol â–Ş Methanol â–Ş Acetone, ethanol, isopropyl alcohol, propylene glycol
  • 58.  Electrolytes â–Ş Hypokalemia â–Ş Isuline ,oral hypoglysemics â–Ş Diuretics, Methyl xanthine, Toluene â–Ş Hyperkalemia â–Ş Digoxin â–Ş Beta-blocker  Liver function tests â–Ş Acetaminophen, Ethanol, Carbon tetrachloride  Renal function tests â–Ş Ethylene glycol, NSAIDS
  • 59.  ECG Digoxin toxicity TCA overdose - sinus tachycardia, QT prolongation, increased QRS Beta-blockers - conduction abnormalities Imaging . CXR- hydrocarbon ingestion .Abdominal X-ray-- iron ingestion & radioopaque ingestion. .Oesophagoscopy -for caustic ingestion. . Abdominal usg- recently been used as a means of identifying presence of pharmaceutical material in GIT.
  • 60. ď‚— Opiates ď‚— Cocaine metabolite ď‚— Amphetamine ď‚— Benzodiazepines ď‚— Barbiturates * No urine screen can confirm intoxication, only exposure
  • 61.
  • 62.
  • 63.  Reduce absorption of the toxin  Enhance elimination  Neutralise toxin
  • 64.
  • 65.  Removal from surface skin & eye  Emesis induction  Gastric lavage  Activated charcoal administration & cathartics  Dilution - milk/other drinks for corrosives  Whole bowel irrigation  Endoscopic or surgical removal of ingested chemical
  • 66.  Skin decontamination â–Ş Important aspect – not to be neglected â–Ş Remove contaminated clothing â–Ş Wash with soap and water (soaps containing 30% ethanol advocated) â–Ş However, no evidence for benefit even in OP poisoning
  • 67.  Gastric decontamination â–Ş Forced emesis if patient is awake â–Ş Gastric lavage â–Ş Activated charcoal 25 gm 2 hourly â–Ş Sorbitol as cathartic
  • 68.  Gastric lavage â–Ş Gastric lavage decreases absorption by 42% if done 20 min and by 16% if performed at 60 min â–Ş Performed by first aspirating the stomach and then repetitively instilling & aspirating fluid â–Ş Left lateral position better - delays spont. absorption â–Ş No evidence that larger tube better â–Ş Simplest, quickest & least expensive way â–Ş Choice of fluid is tap water - 5-10 ml/kg
  • 69.  Gastric lavage â–Ş Preferrably done on awake patients â–Ş Presence of an ET tube does not preclude aspiration, though preferred if GCS is low â–Ş No human studies in OP poisoning showing benefit of gastric lavage
  • 70.  Single dose activated charcoal  0.5-1 gm/kg, adolescents 50-100 grams PO; maximum dose 100 grams  More benefit if administered within 1 hour of ingestion, but still good for poison which slows gastric motility (anticholinergic, opiates, salicylates)  Strongly consider for acetaminophen overdose > 4 hours
  • 71.  P – Pesticides, petroleum distillates, unprotected airway  H – Hydrocarbons, heavy metals, > 1h delay in administration  A – Acids, alkali, alcohol, altered level of consciousness, aspiration risk  I – Iron, ileus, intestinal obstruction  L – Lithium, lack of gag reflex  S – seizures
  • 72.  Nonabsorbable, isotonic polyethylene glycol  Toxins “pushed” through GI tract; prevents absorption  Concentration gradient created by this allows absorbed toxin to diffuse back into GI tract  Used where toxins NOT absorbed by charcoal
  • 73.  Recommended for:  Iron tablets  Lead paint chips  Theophylline  Crack vials/packets  Button batteries  Sustained release calcium channel blockers
  • 74.  Bowel perforation  Bowel obstruction  Clinically significant gastrointestinal hemorrhage  Ileus  Unprotected or compromised airway  Hemodynamic instability  Uncontrollable intractable vomiting
  • 75.
  • 76.  Methods â–Ş Keeping a good urine output 150-200 ml/hr â–Ş Alkalinisation of urine - clinical efficacy accepted for salicylate & phenobarbital poisoning â–Ş Extracorporeal removal â–Ş Hemodialysis - Barbiturates, Salicylates, Acetaminophen, Valproate, Alcohols, Glycols â–Ş Hemoperfusion - theophylline, digitalis, lipid soluble drugs
  • 77.  Plasmapheresis  Works very well with highly protein (albumin) bound drugs  Not a routine methodology, but has been used to remove theophylline and digoxin/ digibind complexes  Exchange transfusion  Use in smaller infants where vascular access for extracorporeal techniques can’t be done
  • 78.  Renal failure.  Congestive heart failure (relative).  Acute lung injury.  Persistent CNS disturbance.  Severe acid-base or electrolyte imbalance, despite appropriate treatment.  Hepatic compromise with coagulopathy.  Salicylate concentration (acute) >100 mg/dL.
  • 79.
  • 80. Acetaminophen N-acetyl cysteine Anti-cholinergics Physostigmine Benzodiazepenes Flumazenil Ca channel blockers Glucagon, Insulin + dextrose, Calcium Carbamate Atropine Cyanide Thiosulphate, nitrate Digoxin Digoxin antibodies INAH Pyridoxine Methanol Ethanol, Fomepizole Glycol Ethanol, Fomepizole Opioid Naloxone Oral hypoglycaemics Glucose Organophosphate Atropine, PAM Warfarin(rat kill poison) Vitamin K
  • 81. Iron Desferroxamine Copper Penicillamine, Dimercaprol, CaEDTA Lead CaEDTA, Dimercaprol (BAL) Mercury DMPS, DMSA, BAL Arsenic BAL & derivatives Antimony BAL & derivatives
  • 82.  Calcium channel blockers: bradycardia and hypotension; 1 - 10 mg tablet of nifedipine  Camphor: respiratory depression and seizures; 15 mL of Vicks vapo-rub (700 mg of camphor)  Clonidine: severe bradycardia; 0.1 mg  Tricyclic antidepressants: cardiovascular and CNS toxicity; 10-20mg/kg  Opioids: CNS and respiratory depression; 2.5 mg of hydrocodone.
  • 83.  Lomotil: anticholinergic overdose (tachycardia, seizures, coma); ½ tablet  Salicylates: cerebral edema, acidosis, coma; ½ teaspoon of wintergreen fatal  Sulfonylureas: severe hypoglycemia; 1 tablet  Toxic alcohols: cardiac and CNS depression; 2.9mL of 95% ethylene glycol has been fatal
  • 84. National Poisons Information Centre (NPIC) Department of Pharmacology All India Institute of Medical Sciences New Delhi, India  Tel. No.: 26589391, 26593677,  Fax: 26850691, 26862663  Email: npicaiims@hotmail.com provides round-the-clock, 7 days-a-week, 365 days service on telephone.
  • 85. ď‚— Poisoning a common problem in our country ď‚— A high index of suspicion required to diagnose ď‚— Know common toxidrome & antidotes  Charcoal is only given if likely to benefit  Patients receiving decontamination must have airway protection ď‚— Don’t panic and follow a plan of action ď‚—Decreasing absorption ď‚—Enhancing elimination ď‚—Neutralising toxins ď‚— Avoid potentially harmful Rxs - risk vs benefit

Hinweis der Redaktion

  1. Assessment triangle: -general appearance (sleepy, obtunded, wired, delirious,etc.) -work of breathing (too fast, too slow, too deep, too shallow) -circulation (hypertensive, hypotensive) Most toxic exposures can be treated with basic life support measures Oxygen, dextrose, and naloxone: diagnostic and therapeutic Toxidrome: constellation of symptoms which are most likely to indicate the ingestion of a certain class of medication. H&P plus lab eval.
  2. Altered mental status: rule out other causes as clinically indicated: trauma (including abuse), infection, metabolic abnormality (DKA), etc.
  3. Paracelsus = German physician, father of modern pharmacology