Recent Adv Inflamm Allergy Drug Discov. 2026 Mar 26. doi: 10.2174/0127722708420100260210104129. Online ahead of print.
ABSTRACT
INTRODUCTION: Angiotensin II receptor blockers (ARBs) are a group of drugs widely used in the treatment of high blood pressure, cardiovascular and renal diseases, and diabetes. ARBs have a low incidence of adverse effects and are usually well tolerated. A limited number of cutaneous reactions to ARBs have been reported. To date, there are no published reports of immediate drug hypersensitivity reactions to any ARB.
CASE PRESENTATION: We present a 50-year-old woman with a personal history of arterial hypertension and dyslipidemia. She started treatment with valsartan at 160 mg per day. A year later, she began to experience daily episodes of papular and pruritic skin lesions. She was treated with oral and topical corticosteroids and antihistamines, but the exanthema persisted and progressively worsened. Valsartan was finally discontinued, and she has not experienced any new flares since then. A punch skin biopsy was performed, and histological results were consistent with an eczematous pattern of toxicodermia. Blood analysis, including serum immunoglobulins, complement proteins, and peripheral eosinophils, showed normal values. Patch tests and a skin prick test with valsartan were negative. A controlled oral challenge with valsartan was performed, yielding a positive result. Thirty minutes after the second dose of the drug (cumulative dose of 160 mg), the patient developed an urticarial rash, which resolved within the following two hours. An alternative ARB was selected for challenge, and a controlled oral challenge test with losartan was successfully completed without adverse reactions.
CONCLUSION: This is the first immediate reaction to an ARB, specifically valsartan, reported in the literature. Only a few cases of cutaneous exanthemas suggestive of non-immediate drug hypersensitivity reactions have been reported previously. We present a patient with an initial suspicion of a delayed drug hypersensitivity reaction to valsartan, based on a biopsy consistent with an eczematous pattern of toxicodermia. After re-exposure to the drug four months later, the patient experienced an immediate urticarial reaction, suggestive of an IgE-mediated drug allergy. Cross-reactivity between ARBs is uncertain, but losartan, despite belonging to the same group of biphenyltetrazoles as valsartan, was demonstrated to be a safe ARB option for this patient. We also hypothesize that the concept of the "converter phenotype," currently described in patients treated with chemotherapy drugs and monoclonal antibodies, may be applicable to other drugs as well.
PMID:41931666 | DOI:10.2174/0127722708420100260210104129