INTRODUCTION

Furosemide is a widely used Henle's loop diuretic. Although it belongs to the sulfonamides family, a difference in an aryl-amine group at the N4 position justified its inclusion in the non-aromatic sulfonamides group. Most frequent side effects of furosemide are alterations in the acid-base status and electrolyte disturbances, but some cutaneous reactions have been reported (exanthematic pustulosis1, bullous dermatosis2 or lichenoid drug eruption3). However, type-1 allergic reactions are exceedingly rare. A case of anaphylaxis after oral administration of furosemide is reported.

CASE REPORT

A 24-year-old woman, without any allergic background, who suffered from a polycystic ovary, shortly after the intake of one pill of Seguril 40 mg® (Aventis-Pharma), experienced oral itching, generalized papulae and maculae, facial angioedema, dysphonia, dyspnea and low blood pressure (60/30 mmHg). She was recovered after the administration of parental adrenaline, methyl-prednisolone and dyphenhydramine. The patient was kept at the hospital centre for clinical observation. She had previously taken furosemide one year ago without any reaction and she had not eaten any food and had not being doing exercise in the previous 4 hours.

In the Allergy Unit at our hospital, skin prick tests (SPT) were performed with commercial extracts, Anisakis simplex (1 mg/ml), latex, and a common food battery (legumes, nuts, fish, fruits, milk, egg and wheat (IPI, Madrid, Spain and Leti, Barcelona, Spain). They were all negatives with a normal response to the histamine control. A prick test with furosemide (10 mg/ml) was performed and it was negative. The intradermal skin tests were positive to furosemide (1 %) as well as sulfamethoxazole (0.03 mg/ml). 5 non-atopic and 5 atopic controls were all negatives to both drugs. To rule out an allergy to the para-amine group4, epicutaneous test with paraphenylenediamine and parental challenge test with paracetamol (1 g) and procaine (10 mg) were performance and they were both well tolerated with no symptoms or cutaneous reactions 3 and 24 hours after the test. The patient did not consent the performance of an oral challenge test with sulfamethoxazole.

DISCUSSION

Data of immediate anaphylactic reaction after sulfonamide treatment are very scarce and most have been obtained with co-trimoxazol5. IgE­mediated reactions to furosemide are infrequent. Although a case of anaphylaxis due to furosemide was previously reported in 19876, it seems it occurs very rarely, since no other cases have been communicated. In this patient, immediate hypersensitivity was documented by positive skin tests, but the way of sensitization remains unclear. The previous administration of the drug could probably the mechanism of sensitization, but the positive intradermal test to sulfamethoxazole would open the hypothesis of a cross-reactivity between non-aromatic and antimicrobial sulfonamides7. We should not forget that there are enough similarities in chemical structure between both groups to justify a cross-reactivity mechanism between them. Although the patient did not know if she had been ever treated with antimicrobial sulfonamides, we should remember that the use of these drugs to treat paediatric infections was widely extended twenty years ago. Unfortunately, the patient refused the performance of an oral challenge test with sulfamethoxazole.

In conclusion, furosemide is a very well tolerated diuretic but it could rarely be implicated in cases of anaphylaxis through an IgE-mediated mechanism, as it has been demonstrated in this case with a positive cutaneous test, even if the drug is orally administrated. The possible mechanism of cross-reactivity between different drugs of the sulfamides family, could make necessary the performance of an oral challenge test with furosemide in allergic patients to sulfamides.