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首页> 外文期刊>The Journal of Allergy and Clinical Immunology >Individual IL-3 priming is crucial for consistent in vitro activation of donor basophils in patients with chronic urticaria
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Individual IL-3 priming is crucial for consistent in vitro activation of donor basophils in patients with chronic urticaria

机译:单独的IL-3引发对于慢性荨麻疹患者供体嗜碱性粒细胞的持续体外激活至关重要

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Background: The in vivo autologous serum skin test (ASST) is the diagnostic gold standard to detect autoantibodies against FcεRI or IgE itself, as well as other autoreactive serum components, in patients with chronic spontaneous urticaria (CU). Coincubation of patient sera with donor basophils and measuring their degranulation in vitro could be a safe alternative but has shown inconsistent results. Objective: Optimization of the basophil activation test to detect autoreactive serum components in patients with CU. Methods: The ability of patient sera to induce CD63 and CD203c in donor basophils (n = 15) was measured by means of flow cytometry. Sera of 20 patients with CU (10 with positive ASST results), 15 patients with cold urticaria, and 27 healthy control subjects were included to optimize test conditions with donor basophils and a basophil cell line (RBL703/21) followed by testing of 110 consecutive patients from clinical routine. Results: We demonstrate that individual IL-3 priming normalized the initially inconsistent basophil reactivity and led to reproducible and comparable test results irrespective of the basophil donors used. CD203c as an activation marker and the use of a basophil cell line were less suitable for this purpose. Conclusion: The basophil activation test with individualized IL-3 priming for each basophil donor is a reproducible and reliable alternative to the ASST. There are several advantages over the ASST: no risk of accidental infection, no influence of antihistamines on the test result, quantifiable results, and a potential in providing treatment monitoring. The exact nature of the degranulating factor or factors in patient sera remains an open question.
机译:背景:体内自体血清皮肤测试(ASST)是诊断慢性自发性荨麻疹(CU)患者中针对FcεRI或IgE自身以及其他自身反应性血清成分的自身抗体的诊断金标准。将患者血清与供体嗜碱性粒细胞共孵育并在体外测量其脱颗粒可能是一种安全的选择,但结果却不一致。目的:优化嗜碱性粒细胞活化测试以检测CU患者自身反应性血清成分。方法:通过流式细胞术检测患者血清诱导供体嗜碱性粒细胞(n = 15)中CD63和CD203c的能力。包括20例CU患者的血清(10例ASST结果呈阳性),15例冷荨麻疹患者和27例健康对照受试者的血清,以优化供体嗜碱性粒细胞和嗜碱性粒细胞系(RBL703 / 21)的测试条件,随后连续测试110例患者从临床常规。结果:我们证明了单独的IL-3引发可以使最初不一致的嗜碱性粒细胞反应性正常化,并导致可重现和可比较的测试结果,而与所用的嗜碱性粒细胞供体无关。 CD203c作为激活标记和嗜碱细胞系的使用不太适合于此目的。结论:针对每个嗜碱性粒细胞供体进行个性化IL-3引发的嗜碱性粒细胞活化测试是ASST的可再现且可靠的替代方法。相对于ASST,有几个优点:无意外感染的风险,抗组胺药对测试结果的影响,可量化的结果,以及提供治疗监测的潜力。患者血清中一种或多种脱粒因子的确切性质仍然是一个悬而未决的问题。

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