Thalappil Sherin, Al-Nesf Maryam
Adult Allergy and Immunology Section, Department of Medicine, Hamad Medical Corporation, Doha, Qatar E-mail:
Qatar Med J. 2022 Apr 4;2022(2):4. doi: 10.5339/qmj.2022.fqac.4. eCollection 2022.
Nonsteroidal anti-inflammatory drugs (NSAIDs) cause different types of allergic and pseudo allergic reactions. This results in difficulties in clinical practice. Most cases of NSAID hypersensitivity are mediated by the inhibition of cyclooxygenase-1 enzyme (COX-1), which results in depletion of the protective prostaglandin E2, and promotes the unrestrained synthesis of inflammatory mediators from mast cells. Selective COX-2 inhibitors are considered safe alternatives in patients with NSAID allergy, although hypersensitivity reactions to COX-2 inhibitors have also been reported. Our study aimed to report the experience in Qatar for using COX2 inhibitors as an alternative treatment for nonselective NSAID allergy.
Data of patients who underwent open challenge with a single dose of oral celecoxib 200 mg were retrieved from the procedure log of the Allergy and immunology Division in Hamad medical corporation, Doha, Qatar, from 2013 to 2022. The challenge was considered positive if the patient developed cutaneous or respiratory symptoms.
A total of 31 patients were identified; 4 with a history of celecoxib allergy. The remaining 27 (23 females and 4 males); with mean ( ± SD, range) age of 42 ( ± 12, 20-65) years had hypersensitivity to one (n = 11) or more than one (n = 16) nonselective NSAID, manifested as cutaneous, respiratory, or anaphylactic symptoms. Those 4 patients with celecoxib allergy were challenged and only one with a historical reaction of anaphylaxis developed anaphylaxis during the challenge. Celecoxib was well tolerated in all 27 patients with hypersensitivity reactions to nonselective NSAIDs. Also, patients were contacted by telephone call at 24 hours and after 1 week with no evidence of delayed reactions.
Selective COX-2 and nonselective NSAIDs have similar overall efficacy as analgesic, anti-inflammatory, and antipyretic agents. Hypersensitivity reaction to COX-2 inhibitors has been reported; however, it is rare. So, it is safer to challenge the patients with COX-2 inhibitors before prescribing them as alternative medication in patients with Nonselective NSAID allergies. We plan to conduct a single-/double-blind placebo-controlled study for more patients, especially using graded challenges for high-risk profile candidates. Also, it may be of significance to test more than one type of selective COX-2 to avoid drug-specific reactions.
非甾体抗炎药(NSAIDs)会引发不同类型的过敏和类过敏反应。这给临床实践带来了困难。大多数NSAID超敏反应是由环氧化酶-1(COX-1)酶的抑制介导的,这会导致保护性前列腺素E2耗竭,并促进肥大细胞不受限制地合成炎症介质。选择性COX-2抑制剂被认为是NSAID过敏患者的安全替代药物,尽管也有对COX-2抑制剂过敏反应的报道。我们的研究旨在报告卡塔尔使用COX-2抑制剂作为非选择性NSAID过敏替代治疗的经验。
从卡塔尔多哈哈马德医疗公司过敏与免疫科2013年至2022年的手术记录中检索接受单剂量口服塞来昔布200mg开放激发试验的患者数据。如果患者出现皮肤或呼吸道症状,则激发试验被视为阳性。
共确定31例患者;4例有塞来昔布过敏史。其余27例(23例女性和
