Dupilumab in patients with atopic dermatitis: assessing treatment response, clinical features and potential biomarkers in real-life.

IF 2.6 Q2 ALLERGY
R. Limão, R. Brás, E. Pedro, S. Silva, A. Lopes
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Abstract

Summary Background. The clinical and pathophysiological heterogeneity of atopic dermatitis (AD) endophenotypes is associated with wide diversity in response to therapy. The aim of this study was to evaluate the response to dupilumab in a group of AD patients and identify clinical/immunological features associated with different patterns of response. Methods. A retrospective observational study was performed, including 30 adults with AD who completed 12 months treatment with dupilumab, in a Portuguese Immunoallergology Department. Demographic, clinical, and immunological data were analyzed, including total serum IgE, sensitization to aeroallergens, peripheral eosinophilia and inflammatory biomarkers (sedimentation rate, C-reactive protein and lactate dehydrogenase-LDH). Patients who achieved EASI-75/EASI ≤ 7, SCORAD-75/SCORAD ≤ 24, NRS-pruritus ≤ 4 or DLQI≤5 at 6 months of treatment were considered responders and those that achieved all these goals at 16 weeks were considered super-responders. Results. Clinical evaluation revealed a significant reduction in median SCORAD, EASI, DLQI, NRS-pruritus and NRS-sleep over 12 months on dupilumab (p less than 0.01), in parallel with decrease in serum Th2 pathway biomarkers and LDH. All patients responded to dupilumab, and 26.7% were super-responders, supporting that dupilumab is highly effective in moderate to severe Th2-high AD. Conclusions. In this cohort, none of the evaluated biomarkers at baseline were associated with a better/earlier clinical response to dupilumab. Dupilumab treatment for 52 weeks resulted in a significant and sustained reduction in blood levels of total IgE and allergen-specific IgE to aeroallergens. The potential long-term clinical benefit of these effects, even after discontinuing dupilumab therapy in patients with AD, should be explored to a greater extent.
杜匹单抗在特应性皮炎患者中的应用:评估现实生活中的治疗反应、临床特征和潜在生物标记物。
摘要背景。特应性皮炎(AD)内型的临床和病理生理学异质性与治疗反应的广泛多样性有关。本研究旨在评估一组特应性皮炎患者对杜匹单抗的反应,并确定与不同反应模式相关的临床/免疫学特征。研究方法葡萄牙一家免疫变态反应科开展了一项回顾性观察研究,研究对象包括30名成年AD患者,他们接受了为期12个月的杜比鲁单抗治疗。研究分析了人口统计学、临床和免疫学数据,包括总血清 IgE、对航空过敏原的敏感性、外周嗜酸性粒细胞增多和炎症生物标志物(血沉、C 反应蛋白和乳酸脱氢酶-LDH)。治疗 6 个月后,EASI-75/EASI≤7、SCORAD-75/SCORAD≤24、NRS-瘙痒≤4 或 DLQI≤5 的患者被视为应答者,治疗 16 周后达到所有这些目标的患者被视为超级应答者。结果临床评估显示,使用杜必鲁单抗 12 个月后,SCORAD、EASI、DLQI、NRS-瘙痒和 NRS-睡眠的中位数明显下降(P 小于 0.01),同时血清 Th2 通路生物标志物和 LDH 也有所下降。所有患者都对杜比鲁单抗产生了反应,其中26.7%为超级反应者,这证明杜比鲁单抗对中度至重度Th2高AD非常有效。结论在该队列中,基线评估的生物标志物均与杜匹单抗更好/更早的临床反应无关。杜比鲁单抗治疗52周后,血液中总IgE和过敏原特异性IgE水平显著持续降低。即使 AD 患者停止使用杜匹鲁单抗治疗后,这些效果仍有可能带来长期的临床益处,我们应该对此进行更深入的探讨。
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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CiteScore
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102
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