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Clinical Features of Immediate Hypersensitivity to Isopropylantipyrine

机译:立即对异丙基安替比林过敏的临床特征

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Hypersensitivities induced by isopropylantipyrine (IPA), a pyrazolone derivative within the wider family of non-steroidal anti-inflammatory drugs (NSAIDs), are rarely reported. We characterized the clinical features of 12 patients with IPA-induced hypersensitivity. Twelve patients with immediate hypersensitivity to IPA were enrolled and classified into two groups: group I, consisting of eight patients (66.7%) with selective hypersensitivity; and group II, consisting of four patients (33.3%) showing cross-intolerance to other NSAIDs. Skin prick and intradermal and oral provocation tests with IPA were performed. To confirm selective hypersensitivity, an aspirin oral provocation test was also conducted. The most common manifestations were cutaneous reactions (91.7%), followed by anaphylaxis (66.7%), respiratory (41.7%), ocular (16.7%), and gastrointestinal reactions (16.7%). The median age and the median age at onset were 34.5 (range, 23-55) years and 28.0 (range, 7-47) years, respectively. In both groups I and II, all patients showed negative responses to skin prick testing, whereas only two patients in group I were positive in response to intradermal IPA tests. The response time after drug exposure was shorter in group I than in group II. Here, we report on two types of IPA hypersensitivity: selective and cross-intolerant NSAID hypersensitivity. An immediate IgE-mediated reaction may be involved in patients with selective hypersensitivity, whereas a cyclooxygenase-1-related inhibition mechanism may be a responsible mechanism for the patients with cross-intolerance to multiple NSAIDs.
机译:很少有人报道由异丙基安替比林(IPA)引起的超敏反应,异丙基安替比林是更广泛的非甾体抗炎药(NSAIDs)系列中的吡唑啉酮衍生物。我们表征了12例IPA引起的超敏反应的临床特征。招募了12名对IPA立即过敏的患者,并将其分为两组:第一组,包括8名(66.7%)具有选择性过敏的患者;第二组由四名患者(33.3%)组成,他们对其他NSAIDs交叉不耐受。进行了IPA皮肤刺和皮内和口服激发试验。为了证实选择性超敏反应,还进行了阿司匹林口服激发试验。最常见的表现是皮肤反应(91.7%),其次是过敏反应(66.7%),呼吸道(41.7%),眼部(16.7%)和胃肠道反应(16.7%)。中位年龄和发病年龄中位数分别为34.5(范围23-55)岁和28.0(范围7-47)岁。在第一组和第二组中,所有患者对皮肤点刺试验均显示阴性反应,而第一组中只有两名患者对皮内IPA试验呈阳性反应。与第一组相比,第一组药物接触后的响应时间短。在这里,我们报告两种类型的IPA超敏反应:选择性和交叉不耐受的NSAID超敏反应。选择性超敏反应患者可能会参与立即的IgE介导的反应,而环氧合酶1相关的抑制机制可能是对多种NSAID交叉耐受的患者的负责任机制。

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