Clinical severity of LTP syndrome is associated with an expanded IgE repertoire, FDEIA, FDHIH, and LTP mono reactivity.

IF 2.6 Q2 ALLERGY
E Scala, D Abeni, V Villella, D Villalta, L Cecchi, V Pravettoni, M Giani, E Caprini, R Asero
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引用次数: 0

Abstract

Summary: Background. LTP allergy is often a challenge for clinicians. We evaluated a multiplex diagnostic approach with diverse cofactors to stratify LTP syndrome risk. Methods. Of the 1,831 participants screened with 'Allergy Explorer-ALEX-2', 426 had reactions to at least one LTP. Data was gathered and recorded via an electronic database. Results. Reactivity to peach Pru p 3 was found in 77% of individuals with LTP allergy. Higher levels of specific IgE and concurrent sensitization to more than 5 molecules (50% of all LTP-sensitised participants, 62% of symptomatic cases) were significantly associated with an increased risk of severe reactions (p = 0.001). Several cofactors, either alone or in combination, also influenced patients' clinical outcomes. Some cofactors increased the risk of severe reactions, such as mono reactivity to LTP in 44.6% of cases (p = 0.001), FDEIA in 10.8% of patients (p = 0.001), and FDNIH in 11.5% (p = 0.005). On the other hand, reactivity to PR10 (24.2%; p = 0.001), profilin hypersensitivity (10.3%; p = 0.001), and/or atopic dermatitis (16.7%; p = 0.001) had a mitigating effect on symptom severity. Conclusions. Clinical severity of LTP syndrome is associated with an expanded IgE repertoire in terms of the number of LTP components recognized and increased IgE levels in individual molecules. Ara h 9, Cor a 8, and Mal d 3 showed the strongest association with clinical severity. In addition, several cofactors may either exacerbate (FDEIA, FDHIH, and LTP monoreactivity) or ameliorate (atopic dermatitis and co-sensitization to profilin and/or PR10) individual patient outcomes. These factors may be utilized for the daily clinical management of LTP syndrome.

LTP综合征的临床严重程度与扩大的IgE库、FDEIA、FDHIH和LTP单反应性有关。
摘要:背景。LTP过敏通常是临床医生面临的挑战。我们评估了一种具有多种辅助因素的多重诊断方法来对LTP综合征的风险进行分层。方法。在1831名接受“过敏探索者- alex2”筛查的参与者中,426人对至少一种LTP有反应。数据是通过电子数据库收集和记录的。结果。77%的LTP过敏患者对桃子Pru p3有反应。较高水平的特异性IgE和同时致敏超过5个分子(50%的ltp致敏参与者,62%的症状病例)与严重反应的风险增加显著相关(p = 0.001)。几个辅助因素,无论是单独的还是联合的,也会影响患者的临床结果。一些辅助因素增加了严重反应的风险,如44.6%的病例对LTP单一反应(p = 0.001), 10.8%的患者为FDEIA (p = 0.001), 11.5%的患者为FDNIH (p = 0.005)。另一方面,对PR10的反应性为24.2%;P = 0.001), profilin过敏(10.3%;P = 0.001),和/或特应性皮炎(16.7%;P = 0.001)对症状严重程度有缓解作用。结论。LTP综合征的临床严重程度与可识别的LTP成分数量和单个分子中IgE水平的增加有关。Ara h 9、Cor a 8和Mal d 3与临床严重程度的相关性最强。此外,一些辅助因素可能加剧(FDEIA, fdhh和LTP单反应性)或改善(特应性皮炎和对profilin和/或PR10的共同敏感)个体患者的结果。这些因素可用于LTP综合征的日常临床管理。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
4.00
自引率
0.00%
发文量
102
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