Mushroom poisoning has a high rate of morbidity and mortality in India. These guidelines should help manage reported cases better.

In the recent years because of increased awareness and patients seeking health care early, the incidence of mushroom poisoning is now being documented accurately. Many cases have been reported in the tribal areas of South India, Eastern Ghats, Northern India, and North Eastern parts of the country as mushrooms are a part of their diet.

Diagnosis of mushroom poisoning

Evaluation of a patient for mushroom poisoning is done by considering the key elements such as a proper history, identification of the mushroom species, symptoms, and signs. The gastrointestinal tract, liver and kidneys are affected after six hours of ingestion of the toxic mushrooms.

• A complete haemogram, renal, and liver function tests, PT/INR creatinine kinase, and serum lactate at presentation are the standard baseline laboratory investigations that are performed to assess different clinical syndromes
• These are again followed by serial measurement of CMP, lactate, and PT/INR every 6 to 8 hours
• Identification of the toxic mushrooms and their toxins is done mainly by a medical toxicologist and professional mycologist
• ELISA is a rapid and specific diagnostic test for the detection of amatoxin in serum and urine but it is still not available for the clinical use

Management of cases

• Patients presenting within one hour of the toxic mushroom ingestion are benefitted mostly by gastrointestinal decontamination with activated charcoal
• Least benefits are seen with gastric emptying by gastric lavage or ipecac syrup is given, and there is also an increased risk of aspiration in these cases
• An enhanced reduction in circulation of amatoxins after the ingestion of the toxins is seen with the use of multiple activated charcoals, the proposed dosage being 50 g (0.5 g/kg) given four hourly for four days

Significant amounts of mushroom toxins cannot be removed by haemodialysis or haemoperfusion so, they are not recommended for the removal of toxins. They can only be of use as long as the patient has signs of acute renal failure that requires haemodialysis when there is hyperkalaemia, metabolic acidosis, uremic signs, and encephalopathy.

Biliary drainage

In a rising number of cases, biliary drainage using interventional radiology (simple/serial gallbladder aspiration, percutaneous cholecystostomy), general surgery (open cholecystostomy), or GI (nasobiliary drainage with suction placed by ERCP) has proven effective. Amatoxin laden bile, when removed from the gallbladder eliminates chances of enterohepatic exposure to the poison, and thus ensures absolute protection to the uninvolved hepatocytes.

Therapies in use

1. Benzodiazepines are used to treat agitation, delirium, and hallucination. Treatment with the short-acting benzodiazepines i.e. midazolam or lorazepam is done in cases of seizures caused by mushrooms containing muscimol, ibotenic acid, and gyromitrin.
2. Phenytoin sodium is given in case the patient doesn’t respond to the above treatment as per epilepsy management protocols.
3. Amatoxin uptake inhibitors such as silibinin or intravenous penicillin G guarantee higher patient survival. They cause diversion of amatoxin back into the general circulation for renal clearance. It is, however, essential to maintain good renal function and a brisk urine output to ensure the amatoxin uptake inhibitor's efficacy.
   • Silibinin 5 mg/kg bolus followed by 20 mg/kg/day is the recommended dosage to be given for 6 days or till the patient recovers.
   • An infusion of intravenous Penicillin G at a dose of 300,000 to 1,000,000 units/kg/day for the same period can be used in case silibilin is not available
4. Anticonvulsant therapy using pyridoxine (70 mg/kg to 5 g) per day is given in cases of gyromitrin toxicity with seizures.
5. In gyromitrin poisoning, intravenous methylene blue is given in detected cases of methemoglobinaemia.