A case of severe corrosive esophagitis, gastritis, and liver necrosis caused by ingestion of methyl ethyl ketone peroxide
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Abstract
The plastic hardener methyl ethyl ketone peroxide is unstable peroxide that releases free oxygen radicals. Ingestion of this compound induces widespread liver necrosis, severe metabolic acidosis, corrosive esophagitis and gastritis, that is often fatal. A 49-year-old man unintentionally ingested approximately 100 mL (55%) of this compound in solution, which was purchased as plastic hardener. Despite resuscitation, he died about 11 hours after admission. We report a patient with poisoning due to methyl ethyl ketone peroxide who presented with corrosive esophagitis and gastritis, gastrointestinal bleeding, and developed ischemia of the bowel and necrosis of the liver and died of severe metabolic acidosis and multiorgan failure.
INTRODUCTION
Methyl ethyl ketone peroxide (MEKP) is a colorless liquid with an acetone-like odor. It is used as a general industrial solvent in the manufacturing of nitrocellulose coating, vinyl film, and smokeless powder [1]. Despite this widespread use, little information is available regarding what happens to MEKP once it is absorbed by the human body, although it has several physico-chemical properties that may confer toxicity. Even though ingestion of MEKP is rare, it is associated with high morbidity and mortality (Table 1) [2-8]. Herein, we report the fatal poisoning of a 49-year-old man after ingestion of MEKP.
CASE REPORT
A 49-year-old man inadvertently ingested an estimated 100 milliliters of a solution from a water bottle. The liquid was identified as a plastic hardener that contained 55% MEKP. The man was brought to the emergency medical center within 30 minutes of ingestion, with shortness of breath, nausea, vomiting, and abdominal discomfort. His medical history was unremarkable.
Upon initial physical examination, the patient was somewhat anxious, but not stridorous; he had a low blood pressure (70/50 mmHg), a pulse rate of 84 beats/min, a peripheral oxygen saturation of 99%, and a body temperature of 36.5°C. No significant abnormal findings were observed upon examination of the chest and abdomen. Laryngoscopy, which was carried out 10 minutes after the patient’s arrival in the emergency department, revealed a superficial mucosal injury without edema of the epiglottis, arytenoid, or vocal cords. Furthermore, a chest radiogram and electrocardiogram were performed 30 minutes after his arrival; these were both normal. However, radiography of the abdomen indicated paralytic ileus, and lateral radiography of the neck showed swelling of the arytenoid (Fig. 1).
Initial laboratory blood investigations showed a normal hemoglobin level (18 g/dL), a white blood cell count of 9,500/mm3, a hematocrit of 49.5%, and a platelet count of 139,000/mm3; arterial blood gas analysis (ABGA) revealed a pH of 7.704, a pCO2 of 7.4 mmHg, a pO2 of 106.3 mmHg, and an HCO3- level of 9.0 mmol/L. A coagulation screen revealed an activated partial thromboplastin time of 56.6 seconds and a prothrombin time of 11.1 seconds. Biochemical investigation revealed that blood levels of total bilirubin were 6.96 mg/dL, aspartame aminotransferase were 191 IU/L, alanine transferase were 108 IU/L, alkaline phosphatase were 762 IU/L, creatinine phosphate kinase were 1,257 IU/L, creatinine phosphate kinase myoglobin were 57 ng/mL, gamma-glutamyl transpeptidase were 523 IU/L, sodium were 133 mEq/L, potassium were 3.9 mEq/L, and lactate were 38.8 mg/dL. Blood urea nitrogen and serum creatinine levels were 11.9 and 1.28 mg/dL, respectively. The patient was given 3 L of normal saline, antibiotics, steroids, hepatotonics, and a high-dose proton pump inhibitor.
Two hours after admission, as he had developed hypotension again, dopamine and norepinephrine were administered, and a central line was inserted; his central venous pressure was 3 cm H2O. He had also developed a sore throat and chest discomfort, as well as distention and tenderness in the abdomen.
Contrast computed tomography (CT) of the chest and abdomen was performed three hours after admission; this did not reveal any perforation of a hollow viscus, but showed severe dilatation of the esophagus, severely decreased attenuation of the liver parenchyma, prominent ulcerative changes in the stomach wall that included mucosal disruption and hemorrhagic fluid collection in the stomach cavity, and dilatation of the small bowel associated with air-fluid levels (Fig. 2).
Four hours after admission, the patient had deteriorated into a stuporous mental state; he was experiencing respiratory failure, metabolic acidosis, acute renal failure, and continuous hypotension. For this reason, he was given a large amount of bicarbonate and a vasopressor. ABGA at this time revealed a pH of 7.21, a pCO2 of 27 mmHg, a pO2 of 206 mmHg, and an HCO3- level of 13.4 mmol/L.
Five hours after admission, as his condition had continued to deteriorate, he underwent orotracheal intubation to maintain the airway, and a mechanical ventilator was applied. Follow-up laryngoscopy examination revealed corrosive mucosal injury combined with severe edema of the epiglottis, arytenoids, and vocal cords.
No prominent free air was observed upon CT scanning, although we could not exclude the possibility of bowel perforation. For this reason, we considered exploratory surgery; however, we had to cancel it because the erosive nature of MEKP rendered the necessary scope of the proposed surgery too large. Regardless, the patient’s vital signs were worsening rapidly and he was unlikely to have survived surgery. The patient’s family agreed to a “do not resuscitate” request.
Seven hours after admission the patient’s blood pressure was 60/40 mmHg, and ABGA showed a pH of 7.09, a pCO2 of 25 mmHg, a pO2 of 191 mmHg, and an HCO3- level of 9.0 mmol/L.
Nine hours after admission, he was in a comatose state and showed pulseless hypotension. Ten hours after admission, the patient died of multi-organ failure before the site and extent of damage to the gastrointestinal tract could be determined and corrective surgery performed.
DISCUSSION
It has been postulated that MEKP toxicity is mediated by free radical formation that leads to lipid peroxidation, resulting in corrosive damage to the respiratory and gastrointestinal mucosa, as well as to the liver. Lipid peroxidation is a free radical-initiated chain oxidation of unsaturated lipids. Subcellular membranes are rich in unsaturated fatty acids, and therefore they are a target for lipid peroxidation that results in cellular dysfunction and death [9].
The toxic dose of MEKP has not been established, but ingestion of any amount should be regarded as serious. Based on data from cases where the dose was known, the toxic oral dose of MEKP has been estimated to be 50 to 100 mL in adults (Table 1) [2-8].
Studies have shown that, in the acute phase of MEKP intoxication, the clinical spectrum can be subdivided into respiratory complications, gastrointestinal complications, free radical-mediated liver damage, and other secondary acute complications [10].
Although ingestion of MEKP is rare, it is associated with high morbidity and mortality [7,10]. To date, 28 cases of MEKP ingestion have been reported, including our case; nine adults and two children have died (Table 1) [2-9]. Moreover, almost all patients have shown gastrointestinal tract and hepatic injury.
To our knowledge, this case is the second report of MEKP poisoning in South Korea, and we believe that the chest-abdomen CT findings were unique in the Korean context. We observed corrosive esophagitis, gastritis, and hepatic necrosis. Our case demonstrates that early gastrointestinal hemorrhage may occur, as may delayed hepatic necrosis, uncontrolled metabolic acidosis, and multi-organ failure. A CT scan is likely more informative than early endoscopy regarding transmural damage to the esophageal and gastric walls, as well as to the extent of necrosis. CT is also more valuable than endoscopy in assessing threatened or existing gastrointestinal perforation, and a CT grading system has been proposed to predict esophageal stricture (Table 2) [11]. A recent investigation supported the accuracy of CT as a diagnostic tool, showing 75% sensitivity and 90% specificity in determining injury grade and the need for surgical intervention, as well as in predicting complications such as stricture [12]. With the advantage of not being invasive, CT shows promise in the early evaluation of corrosive injury to the gastrointestinal tract, as well as in other organ injuries like hepatic necrosis.
Gastric lavage and emesis are contraindicated after ingestion of corrosive substances because of the risk of trauma or further injury to the upper gastrointestinal tract upon re-exposure; in our case, the pH of the ingested substance was 4.
Administration of fluids orally should be avoided after MEKP ingestion, because the gastrointestinal tract may have been perforated. In the acute phase, all patients should immediately be evaluated for airway obstruction. Early and repeated endoscopic evaluation of the upper respiratory and gastrointestinal tracts, as well as chest-abdomen CT, is also important. In addition, the electrocardiogram and ABGA, as well as respiratory, renal, and liver functions, should be monitored. Once past the acute phase, patients will require ongoing follow-up to monitor possible late scarring and stricture formation.
Ultimately, no free air was observed in our patient upon chest-abdomen CT; this suggests the gastrointestinal tract was not perforated at the time of the scan. However, the CT scan was performed just three hours after admission, so we cannot confirm that the bowel was not perforated during the course of the intoxication. Regardless, we did find prominent ulcerative changes in the stomach wall, combined with mucosal disruption and hemorrhaging in the stomach cavity. We considered explorative surgery at this point, but it was cancelled because the patient’s vital signs had been worsening rapidly. Additionally, prednisolone should be given to treat airway edema [13].
Delayed fibrosis and stricture formation leading to intestinal obstruction are among the main long-term complications of corrosive ingestions. Endoscopic dilatation is required to relieve strictures if present. Furthermore, endoscopic intra-lesional steroid injections may augment the effects of endoscopic dilatation and reduce further fibrosis [14].
MEKP is a potentially lethal industrial chemical; acute poisoning can occur after ingestion. Water bottles should not be used to store such toxic chemicals; all vessels containing dangerous liquids must be clearly marked. Furthermore, handlers of these uncommon toxic substances must be made aware of the potential toxicity, and safety measures must be implemented.
MEKP causes severe corrosive injury to the upper gastrointestinal tract, as well as liver necrosis. Early endoscopy and CT can be used to identify perforation or hemorrhage in the gastrointestinal tract. Although upper gastrointestinal endoscopy is considered the mainstay of diagnosis, CT can be used to assess the need for emergency surgery. If perforation and severe continuous leakage of bowel contents does occur, surgery may be needed.
Notes
No potential conflict of interest relevant to this article was reported.
References
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Capsule Summary
What is already known
Ingestion of methyl ethyl ketone peroxide induces widespread liver necrosis, severe metabolic acidosis, corrosive esophagitis and gastritis that is often fatal.
What is new in the current study
Early computed tomography can be used to identify perforation or hemorrhage in the gastrointestinal tract tract.