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Common Environmental Toxins

Common Environmental Toxins. By ANNERIE HATTINGH 18 February 2009. Common Environmental Toxins. Hydrocarbons Inhaled toxins Pesticides Heavy Metals. Introduction: One of most frequently reported poisonings Presentation to ED classified into 4 types: 1.) Accidental ingestion,

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Common Environmental Toxins

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  1. Common Environmental Toxins By ANNERIE HATTINGH 18 February 2009

  2. Common Environmental Toxins • Hydrocarbons • Inhaled toxins • Pesticides • Heavy Metals

  3. Introduction: One of most frequently reported poisonings Presentation to ED classified into 4 types: 1.) Accidental ingestion, - most common - in children less 5yrs 2.) Intentional inhalation, - abuse of volatile hydrocarbons - recreational 3.)Accidental inhalation / exposure, - household or workplace 4.) Massive oral ingestion, - suicide attempts Hydrocarbons

  4. Hydrocarbons Pharmacology: • Diverse group of organic compounds • Contain hydrogen and carbon • Most are petroleum distillates (e.g. gasoline) - derived from crude oil and coal - turpentine derived from pine oil • 2 Main categories (classified by structure) (i) Aliphatics – straight chain hydrocarbons ~ paraffin (lamp oil) ~ mineral turpentine ~ thinners ~ petrol ~ diesel ~ benzine

  5. Hydrocarbons Pharmacology: (ii) Aromatics – ring structure hydrocarbons ~ lubricating oil ~ liquid paraffin ~ baby oil ~ suntan oils ~ petroleum jelly ~ grease • Hydrocarbons commonly used as solvent base for toxic chemicals like • insecticides and metals

  6. Hydrocarbons Pathophysiology: • 3 main target organs effected: # CNS # Lungs # Heart • Most acute damage in the lungs • Potential for acute toxicity depends on 4 characteristics 1.) Viscosity(resistance to flow) low viscosity = high toxicity eg. Lubricants + mineral oil * high viscosity + low toxicity Furniture oil * low viscosity + high toxicity + aspiration

  7. Pathophysiology: 2.) Volatility(capacity of liquid to turn into gas) - displaces alveolar O2 - petrol 3.) Surface tension 4.) Chemical side chains - often high toxicity - e.g.. Heavy metals Hydrocarbons

  8. Hydrocarbons Pathophysiology: LUNG DISEASE: • Fatalities after ingestion, accompanied by aspiration • 1ml in trachea can cause chemical pneumonitis Mechanisms • Penetrates lower airways ~ produces bronchospasm + inflammation • Displaces alveolar O2 (volatile hydrocarbon) • Inhibits surfactant • Damaging alveoli and capillaries

  9. Hydrocarbons Pathophysiology: These effects cause: • Alveolar disfx • Vent / Perfusion mismatch • Hypoxia • Resp. failure

  10. Hydrocarbons CNS: • Narcotic – like effects: ~ euphoria ~ disinhibition ~ confusion • Usually substance abusers - recreational use • Single exposure with rapid onset of intoxication + recovery • Chronic use causes: ~ peripheral neuropathy ~ cerebellar degeneration ~ neuropsychiatric disorders ~ dementia ~ chronic encephalopathy

  11. Hydrocarbons CARDIAC: • Sudden death • Sudden physical activity during / after intentional inhalation • Myocardial sensitization to endogenous + exogenous catecholamines • Precipitates vent. dysrythmias + myocardial dysfx

  12. Hydrocarbons Clinical presentation: 4 typical presentations: 1.) Accidental ingestion: • Usually toddlers • Reused beverage containers storing hydrocarbon • Mild Sx include ~tachypnoea ~dyspnoea ~bronchospasm ~fever within 6 hours

  13. Hydrocarbons Clinical presentation:(cont.) 1.) Accidental ingestion:(cont.) • Severe poisonings ~ early resp. Sx ~ cyanosis ~ grunting ~ coughing ~ repeated vomiting ~ these findings suggests aspiration • Change in mental status ~ direct CNS effect OR ~ caused by hypoxia

  14. Hydrocarbons Clinical presentation: 2.) Intentional inhalation: • Substance abuse • Mechanisms include: - “bagging”- hydrocarbon poured into bag/container + deeply inhaled - “huffing” - inhaling through a saturated cloth - “sniffing” • Mostly volatile hydrocarbons - petrol - paint - glue

  15. Hydrocarbons Clinical presentation: 2.) Intentional inhalation: (cont.) • Presentation: - sudden cardiac arrest - CNS intoxication with euphoria, agitation, hallucinations + confusion • Chronic abusers similar to long-term alcoholics - peripheral neuropathy - cerebellar degeneration - encephalopathy

  16. Hydrocarbons Clinical presentation: 3.) Accidental dermal exposure or inhaled resp. exposure: • In workplace / home • Not life threatening • Asymptomatic or transient non-specific symptoms • Sx resolve with fresh air / removal from offending environment 4.) Intentional ingestion / intravenous injection: • Rare • Suicide attempts • Used in combination with other substances • Massive oral ingestion not associated with significant morbidity

  17. Hydrocarbons Diagnosis: • Clinically • History from parents / family / bystanders • Contact local poison control centre to identify product • CXR: - radiographic changes can occur within 30 min - findings of chemical pneumonitis include: 1.) bilat. perihilar infiltrates 2.) gradually: forms patchy infiltrates 3.) finally: large areas of consolidation • Pulse oximetry • ABG

  18. Hydrocarbons Management: • Observe for 4 – 6 hours (even if asymptomatic) • If any Sx present: do CXR, pulse oximetry, ABG • Supportive care • Gastric lavage should be avoided - increased risk of aspiration • No antidote • If any Sx present suggestive of aspiration – admit for 24 hour observation • Manage resp. complications appropriately – give O2, intubate + ventilate if necessary • No prophylactic A/B!!

  19. INHALED TOXINS • Smoke inhalation • Cyanide • Carbon monoxide

  20. Smoke inhalation Introduction: • Inhalation injury common • Fires in enclosed spaces like homes / factories • Injury typically irritant in nature • Heated particulate matter + absorbed toxins injure normal mucosa • Carbon monoxide + Cyanide poisoning often associated with smoke inhalation - these are systemic ( not resp.) toxins

  21. Smoke inhalation Principles: • Fires involves variable fuels + burning conditions - character of smoke not always identified • Irritant toxins are produced which damages the airway mucosa Clinical presentation: • Morbidity + mortality related to resp. tract damage - thermal / irritant in nature • Time between smoke exposure + onset of Sx – highly variable • May always be delayed • Depend on degree + nature of exposure

  22. Smoke inhalation Clinical presentation: (cont.) • Cough + stridor - thermal + irritant induced laryngeal injury • Cough, stridor + bronchospasm - caused by soot + irritant toxins in the airways • Subsequently – a cascade of: - airway inflammation - acute lung injury with pulm. edema - resp. failure • Burned nasal hair + soot in the sputum suggest substantial exposure • Always consider CO + cyanide inhalation - in pt`s exposed to filtered / distant smoke ( different room) OR - relatively smokeless combustion

  23. Smoke inhalation Management: • Rapid assessment of the airway + early intubation mandatory (prior to deterioration!!) • Supportive care • Intraveneous fluid resuscitation • Maintenance of adequate oxygenation - suctioning + pulm. toilet • Admit to ICU / transfer to Burn Centre

  24. Cyanide • One of the most rapidly acting poisons Causes: 1.) Smoke inhalation: - most common - compounds containing carbon + nitrogen produce hydrogen CN gas when burned - natural compounds (silk + wood) produces HCN as a combustion product - burning of household furniture + plastics also causes HCN gas

  25. Cyanide Causes: (cont.) 2.) Intentional poisoning: -uncommon - cyanide salts in hospitals + labs 3.) Industrial exposure: - Occupations with easy access to cyanide * chemists * jewelers * pest control * mineral refining * photography * electroplating * dying + printing

  26. Cyanide Pathophysiology: • Cyanide inhibits mitochondrial cytochrome oxidase + blocks electron transport ( binding with ferric iron Fe3+ ) • aerobic metabolism + O2 utilization decreases • Lactic acidosis occurs as a consequence of anaerobic metabolism • O2 metabolism @ cellular level is grossly hampered • Cyanide rapidly absorbed from: - stomach - lungs - mucosal surfaces - skin

  27. Cyanide Clinical presentation: • Sx appear seconds to minutes after exposure • HCN gas can lead to cardioresp. arrest + death within minutes • Onset of effects after ingestion / skin contamination: - much slower (several hours) -early signs: i) dizziness ii) bronchospasm iii) dyspnoea iv) confusion v) paresis -Later: i) cardiovasc. collapse ii) seizers iii) coma

  28. Cyanide Prognostic features: 1.) Ingestion of few hundred mg of cyanide salt = FATAL 2.) Pt`s surviving to reach the hospital after HCN inhalation - unlikely to have suffered significant poisoning 3.) Lactic acidosis + pulm. edema = severe poisoning

  29. Cyanide Management: • Avoid mouth – to – mouth resuscitation! • Give 100% O2 - tight fitting facemask - ventilate via ET tube if necessary • O2 contributes to reversal of cyanide-citochrome complex • Skin contamination – wash thorough with soap + H2O • Antidote therapy: - given ASAP, if available - Regimens: 1.) dicobalt edetate ~ toxic ~ only given in confirmed cyanide poisoning

  30. Cyanide Management: (cont.) 2.) Nitrate / Sodium Thiosulphate Regimen ~ safer ~ antidote kit with: * amyl nitrate * sodium nitrate * sodium thiosulphate ~ Nitrates oxidizes Hb to MetHb - which has greater affinity for cyanide - leading to dissociation of cyanide citochrome complex ~ Thiosulphate mediates conversion of cyanide to less toxic substance - excreted in urine

  31. Cyanide Management: (cont.) Doses: 1.) Inhalation of 0.3ml amyl nitrate (emptied on a gauze) 2.) Then 10ml Sodium Nitrate given ivi over 3min. 3.) 50ml 50% Sodium Thiosulphate given over 10min.

  32. Carbon Monoxide • Most common cause of poison - + fire – related deaths • Generated through incomplete combustion of all carbon – containing products Sources: 1.) Smoke inhalation 2.) Poorly maintained domestic gas appliances 3.) Deliberate inhalation of car exhaust fumes

  33. Carbon Monoxide Pathophysiology: Intense tissue hypoxia + cell injury caused by 2 mechanisms: 1.) Interrupts electron transport in the mitochondria (like cyanide), leading to anaerobic metabolism 2.) Reduces O2 delivery by: - competing with O2 for binding to Hb (CO has much higher affinity for Hb, than O2!) - Shifting the HbO2 dissociation curve to the left

  34. Carbon Monoxide Pathophysiology: (cont.) REMEMBER!! Affinity of fetal Hb for CO even higher than that of adult Hb! Therefore fetal exposure higher than that of predicted maternal exposure!

  35. Carbon Monoxide Clinical presentation: • Hypoxia without cyanosis • Myocardium + Brain mostly affected ( high O2 consumption) • Sx include: - dizziness - convulsions - headaches - coma - confusion - cardio/resp. dysfx + death - chest pain - dyspnoea - palpitations - syncope

  36. Carbon Monoxide Clinical presentation: (cont.) • COHb levels correlate poorly with clinical features – only used to confirm exposure • “cherry – red” skin + mucus membranes found post mortem

  37. Carbon Monoxide Complications: • Outcome depends on degree + duration of peripheral tissue hypoxia 1.) CNS: - cerebral, cerebellar + midbrain fx affected 2.) Myocardium: - ischemia + infarction 3.) Skeletal muscle: - rhabdomyolysis - myoglobinuria

  38. Carbon Monoxide Complications:(cont.) 4.) Skin: - erythema - severe blistering

  39. Carbon Monoxide Management: • AIM: minimize + Rx Complications • Admit to ICU • Give 100% O2 - tight fitting facemask -ventilate via ET-tube if necessary ( O2 decreases half life of COHb) • Continuous cardiac monitoring • Pulse oximeter useless!! - cannot distinguish COHb from HbO2

  40. Carbon Monoxide Management:(cont.) • Hyperbaric O2 preferred only if readily available in: - unconscious pt - severe metabolic acidosis - pregnancy - COHb level 25 – 40% - neurological signs • Supportive care: - Rx arrhythmias - correction of acid base + electrolyte abnormalities - Rx convulsions

  41. Carbon Monoxide Management:(cont.) • Ensure F/U as neuropsychiatric squeal may take many weeks to evolve!

  42. Pesticides 1.) Organophosphates + Carbamates 2.) Paraquat + Diquat Poisoning

  43. Organophosphates + Carbamates • Poisoning commonly seen in: - accidental ingestion (kids) - suicide attempts - agricultural workers - pest control Introduction: • Potent cholinesterase inhibitors • Accumulation of acetylcholine (Ach) • Indirect stimulation of nicotinic + muscarinic receptors

  44. Organophosphates + Carbamates Introduction: (cont.) • Absorbed through: - skin - inhalation - ingestion • Carbamate + OP poisoning clinically indistinguishable • Differences: - OP forms irreversible complex with cholinesterase - Carbamate complex reversible, with shorter duration of action ( less than 24 h) - Carbamates penetrates blood-brain barrier poorly, therefore less CNS effects

  45. Organophosphates + Carbamates Clinical presentation: • Minutes to 12 hours after exposure 1.) Muscarinic effects: (post ganglionic) - hyper secretion (sweating, salivation + bronchial secretions) - constricted pupils - bradycardia + hypotension - vomiting + diarrhoea - urinary incontinence - bronchoconstriction - Also commonly referred to SLUDGE syndrome:

  46. Organophosphates + Carbamates Clinical presentation: (cont.) S – salivation L – lacrimation U – urinary incontinence D – diarrhoea G – G.I cramps E – emesis

  47. Organophosphates + Carbamates Clinical presentation: (cont.) 2.) Nicotinic effects: (preganglionic) - muscle weakness - fasciculations - resp. muscle weakness NB: Sometimes nicotinic effects overrides muscarinic effects! Causes: - tachycardia - hypertension - dilated pupils

  48. Organophosphates + Carbamates Clinical presentation: (cont.) 3.) CNS effects: - restlessness - anxiety - headaches - convulsions - coma

  49. Organophosphates + Carbamates Complications: Mortality + Morbidity caused by: 1.) Seizers / Coma 2.) Pulm. hypersectretion 3.) Resp. muscle weakness

  50. Organophosphates + Carbamates Diagnosis: 1.) Clinically (cholinergic syndrome) 2.) Cholinesterase level

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