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Kawasaki Disease Diagnosis and Treatment in over 1000 Patients: A Continuum of Dysregulated Inflammatory Responses

机译:超过 1000 名患者的川崎病诊断和治疗:连续的失调炎症反应

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摘要

Background: Kawasaki disease (KD) is a pediatric vasculitis, leading to coronary artery aneurysms (CAAs) in ~4–14%. Attention to the etiology and course of KD was generated by the close mimic of a SARS-CoV-2-induced phenotype, called multisystem inflammatory syndrome in children (MIS-C). Methods: A total of 1179 cases were collected from 2012 with ~50% of cases retrospectively included. Clinical characteristics were described and risk factors for CAA (persistence) were investigated. Phenotypic patterns of the prospectively included KD patients were evaluated. These patterns were also compared to the seronegative KD and seropositive MIS-C cases identified during the SARS-CoV-2 pandemic. Results: KD mostly affected boys and children < 5 years. IVIG resistance, CAAs, and giant CAAs occurred in 24.5%, 21.4%, and 6.6%, respectively. Giant CAAs were significantly more likely to normalize to a normal Z score in patients that were younger than 2.5 years old at the time of initial giant CAA (χ2 test p = 0.02). In our prospective (SARS-CoV-2-seronegative) KD series, there was a diminishing male predominance over time, whereas the proportions of incomplete presentations (p < 0.001) and patients with circulatory shock (p = 0.04) increased since the COVID-19 pandemic. Pre- and post-pandemic KD cases presented with different levels of C-reactive protein, thrombocyte counts, and hemoglobin levels over the years. Compared to pandemic KD, SARS-CoV-2-seropositive MIS-C patients were older (p < 0.001), and more often required intensive care admission (p < 0.001), with a gradual decrease over time between 2020 and 2022 (p = 0.04). KD carried a substantial risk of CAA development in contrast to MIS-C. Conclusion: the phenotypic changes seen over the last twelve years of our prospective follow-up study suggest a spectrum of hyperinflammatory states with potentially different triggering events within this clinical entity.
机译:背景:川崎病 (KD) 是一种小儿血管炎,导致 ~4-14% 的冠状动脉瘤 (CAA)。对 KD 病因和病程的关注是由 SARS-CoV-2 诱导的表型(称为儿童多系统炎症综合征 (MIS-C))的密切模拟引起的。方法: 从 2012 年共收集 1179 例病例,其中 ~50% 的病例回顾性纳入。描述了临床特征并调查了 CAA (持续性) 的危险因素。评估前瞻性纳入的 KD 患者的表型模式。这些模式还与 SARS-CoV-2 大流行期间发现的血清阴性 KD 和血清阳性 MIS-C 病例进行了比较。结果: KD 主要影响 5 <男孩和儿童。IVIG 耐药、 CAAs 和巨型 CAAs 分别发生于 24.5% 、 21.4% 和 6.6% 。在初始巨型 CAA 时年龄小于 2.5 岁的患者中,巨型 CAA 显著更有可能正常化为正常 Z 评分 (χ2 检验 p = 0.02)。在我们的前瞻性 (SARS-CoV-2 血清阴性) KD 系列中,随着时间的推移,男性优势逐渐减少,而不完全表现 (p < 0.001) 和循环休克患者 (p = 0.04) 的比例自 COVID-19 大流行以来有所增加。多年来,大流行前后的 KD 病例表现出不同水平的 C 反应蛋白、血小板计数和血红蛋白水平。与大流行性 KD 相比,SARS-CoV-2 血清阳性 MIS-C 患者年龄较大 (p < 0.001),更经常需要重症监护入院 (p < 0.001),在 2020 年至 2022 年期间随着时间的推移逐渐减少 (p = 0.04)。与 MIS-C 相比,KD 具有发生 CAA 的巨大风险。结论:我们在过去 12 年的前瞻性随访研究中观察到的表型变化表明,该临床实体中存在一系列高炎症状态,具有可能不同的触发事件。

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