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New Zealand National Poisons Centre New Zealand National Poisons Centre.

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Presentation on theme: "New Zealand National Poisons Centre New Zealand National Poisons Centre."— Presentation transcript:

1 New Zealand National Poisons Centre New Zealand National Poisons Centre

2 IRON OVERDOSE

3 In healthy adults ~ 2 to 10% of dietary iron absorbed In iron deficiency states (including children) 80 to 90% is absorbed In overdose, there is proportionally less of an ingested dose absorbed compared to a therapeutic dose, however, damage to intestinal mucosa can increase absorption Following absorption iron is bound to transferring and actively taken up by the liver during “first pass”. The remaining iron is transported by transferrin, primarily to the bone marrow. IRON

4 In overdose total iron binding capacity is surpassed and free Ferric iron (Fe +++ ) is present in the blood: Free protons are liberated leading to acidosis Fe 3+ + 3H2O  FE(OH) 3 + 3H + Fe +++ leads to production of the OH. radical, in turn causing lipid peroxidation and: - Local tissue injury – primarily the gut and liver -Mitochondrial damage with loss of cellular aerobic respiration Free iron is a vasodilator Direct depression of coagulation factors TOXIC MECHANISM

5 “Classic” stages of iron poisoning Stage I Gastrointestinal30m to 6 hrs Stage II Latent phase2 to 4 hrs Stage III Shock / multiorgan failure / acidosis2 to 24 hrs Stage IV Hepatotoxicity12 to 24 hrs Stage V Gastrointestinal obstruction1 to 7 wks SIGNS AND SYMPTOMS

6 Initial symptoms are secondary to direct irritant and corrosive effect of iron. In larger overdoses, lipid peroxidation causes further injury. Complaints include: Epigastric pain Nausea / vomiting Diarrhoea In more severe cases Haematemesis Vasodilation Third spacing Hypotension Metabolic acidosis may also develop during this initial stage leading to the latent phase being “by-passed”. STAGE I – GASTROINTESTINAL

7 A period where there is a deceptive apparent improvement in the patient’s gastrointestinal condition. It is often tempting to discharge such patients. However, in the seriously poisoned, a metabolic acidosis is evolving. This may be compounded by a lack of adequate fluid resuscitation. STAGE II – LATENT PHASE

8 Loss of adequate tissue perfusion and multiorgan failure: most deaths occur during this stage. Shock occurs secondary to gastrointestinal haemorrhage, vomiting, third-spacing, vasodilation, and reduced cardiac output (due to myocardial toxicity). Multiorgan failure related to inadequate perfusion and direct toxicity ensues and results in: Altered mental status / coma Seizure Acute renal failure Pulmonary oedema STAGE III – SHOCK, MULITORGAN FAILURE, ACIDOSIS

9 Hepatic dysfunction is a poor prognostic sign. Patients suffer related: Hypoglycaemia Coagulopathy and haemorrhage Jaundice Hepatic encephalopathy / coma STAGE IV – HEPATOTOXICITY

10 In survivors mucosal injury may lead to the formation of strictures. Though usually occurring at the pylorus, they may be found throughout the gastrointestinal tract. Actual obstruction is, however, rare. STAGE V – GASTROTINESTINAL OBSTRUCTION

11 History of ingestion Ingestions of 40 to 60 mg/kg should be medically assessed; those above 60 mg/kg should be decontaminated. Investigation Abdominal x-ray Serum iron concentration at 2 to 4 hours post-ingestion DIAGNOSIS

12 Note that the elemental quantity of iron in tablets needs calculation. 5 x Fergon tablets (300 mg ferrous gluconate) ingested by a child: 5 x 300 mg / 10 kg = 150 mg/kg In fact only 11% (33 mg) of the tablet is elemental iron: 5 x 33 mg/10 kg = 16.5 mg/kg HISTORY OF INGESTION

13 Activated charcoal will not bind iron, therefore it is necessary to administer whole bowel irrigation. Appropriate decontamination is recommended: -For ingestions greater than 60 mg/kg elemental iron Follow WBI with AXR to ensure removal of iron DECONTAMINATION

14 Less than 60 umol/L (335 ug/dL) Discharge into the care of a responsible guardian if: - Asymptomatic, and - Iron not detected on abdominal x-ray, and - Formulation ingested was not sustained release or enteric-coated Observe and repeat iron serum concentration at 4 to 6 hours post-ingestion if: - Patient symptomatic (treatment may be indicated by severity), or - Iron detected on abdominal x-ray, or - Sustained release or enteric-coated formulation ingested INTERVENTION CRITERIA

15 60 to 90 umol/L (335 to 500 ug/dL) Observe and repeat serum iron concentration at 4 to 6 hours post-ingestion if: - Asymptomatic, and - Iron not detected on abdominal x-ray, and - Sustained release or enteric-coated formulation ingested Admit for management if: - Symptomatic - Iron detected on abdominal x-ray INTERVENTION CRITERIA

16 Greater than 90 umol/L (500 ug/dL) Admit regardless of symptoms for management, including treatment with desferrioxamine INTERVENTION CRITERIA

17 Indicated in all cases with signs of systemic intoxication and especially those with an high anion gap metabolic acidosis. Desferrioxamine 15 mg/kg/hr up to 80 mg/kg/d Continue until acidosis reversed and symptoms have resolved (do not rely on vin rosè coloured urine). Note: Hypotension following too rapid infusion Renal failure in hypovolaemic patients Prolonged (>24 hour) infusion associated with ARDS Interference with serum iron measurement CHELATION

18 Cardiovascular Hypotension is a significant problem and may be due to haemorrhage, third spacing, vasodilation and compromised cardiac output. Initially robust fluid replacement is required. In severe cases invasive blood pressure monitoring is warranted to guide management. SUPPORTIVE CARE

19 Acute Renal Failure Acute renal failure generally occurs secondary to shock. Haemodialysis should be employed increase removal of iron-chelate, it will not remove iron itself. Acute Liver Failure A poor prognostic sign: requires management of hypoglycaemia, coagulopathy (factor replacement), and early consultation with a liver unit. SUPPORTIVE CARE

20 Fe Fe-Trans Fe CNS Lungs Heart Liver Pancreas CNS Lungs Heart Liver Pancreas GITPLASMALABILE POOL TISSUES Fe-Trans Fe


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