心包炎和自身炎症:国家转诊中心特发性复发性心包炎和单基因自身炎症患者的临床和遗传分析

Claire J Peet, D. Rowczenio, E. Omoyinmi, C. Papadopoulou, B. R. Mapalo, Michael R. Wood, F. Capon, H. Lachmann
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Methods and Results We retrospectively analyzed the medical records of patients with IRP (n=136) and monogenic autoinflammatory diseases (n=1910) attending a national center (London, UK) between 2000 and 2021. We examined 4 genes (MEFV, MVK, NLRP3, TNFRSF1A) by next‐generation sequencing in 128 patients with IRP and compared the frequency of rare deleterious variants to controls obtained from the Genome Aggregation Database. In this cohort of patients with IRP, corticosteroid dependence was common (39/136, 28.7%) and was associated with chronic pain (adjusted odds ratio 2.8 [95% CI, 1.3–6.5], P=0.012). IRP frequently manifested with systemic inflammation (raised C‐reactive protein [121/136, 89.0%] and extrapericardial effusions [68/136, 50.0%]). Pericarditis was observed in all examined monogenic autoinflammatory diseases (0.4%–3.7% of cases). 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引用次数: 8

摘要

背景:特发性复发性心包炎(IRP)是一种发病率很高的孤儿病,部分由皮质类固醇依赖引起。先天免疫调节剂,秋水仙碱和抗白细胞介素- 1药物,在单基因自身炎症疾病中率先出现,在试验中显示出显著的疗效,表明自身炎症可能有助于IRP。本研究确定了IRP和单基因自身炎症性疾病患者的表型特征,并确定了自身炎症性疾病基因是否与IRP相关。方法和结果我们回顾性分析了2000年至2021年间在英国伦敦国家中心就诊的IRP (n=136)和单基因自身炎症性疾病(n=1910)患者的病历。我们对128例IRP患者的4个基因(MEFV、MVK、NLRP3、TNFRSF1A)进行了下一代测序,并比较了从基因组聚集数据库中获得的罕见有害变异与对照的频率。在这组IRP患者中,皮质类固醇依赖很常见(39/136,28.7%),并与慢性疼痛相关(校正优势比为2.8 [95% CI, 1.3-6.5], P=0.012)。IRP常表现为全身性炎症(C反应蛋白升高[121/ 136,89.0%]和心包外积液[68/ 136,50.0%])。在所有检查的单基因自身炎症性疾病中均观察到心包炎(0.4%-3.7%)。罕见的有害MEFV变异在IRP中比在祖先匹配的对照组中更常见(等位基因频率为9/200比2932/129 200,P=0.040)。心包炎是白介素- 1驱动的单基因自身炎症性疾病的一个特征,IRP与MEFV变异有关,MEFV是参与白介素- 1β加工的基因。我们还发现IRP中的皮质类固醇依赖与慢性非炎症性疼痛有关。综上所述,这些数据暗示了IRP中的自身炎症,并支持减少对皮质类固醇的依赖。
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Pericarditis and Autoinflammation: A Clinical and Genetic Analysis of Patients With Idiopathic Recurrent Pericarditis and Monogenic Autoinflammatory Diseases at a National Referral Center
Background Idiopathic recurrent pericarditis (IRP) is an orphan disease that carries significant morbidity, partly driven by corticosteroid dependence. Innate immune modulators, colchicine and anti‐interleukin‐1 agents, pioneered in monogenic autoinflammatory diseases, have demonstrated remarkable efficacy in trials, suggesting that autoinflammation may contribute to IRP. This study characterizes the phenotype of patients with IRP and monogenic autoinflammatory diseases, and establishes whether autoinflammatory disease genes are associated with IRP. Methods and Results We retrospectively analyzed the medical records of patients with IRP (n=136) and monogenic autoinflammatory diseases (n=1910) attending a national center (London, UK) between 2000 and 2021. We examined 4 genes (MEFV, MVK, NLRP3, TNFRSF1A) by next‐generation sequencing in 128 patients with IRP and compared the frequency of rare deleterious variants to controls obtained from the Genome Aggregation Database. In this cohort of patients with IRP, corticosteroid dependence was common (39/136, 28.7%) and was associated with chronic pain (adjusted odds ratio 2.8 [95% CI, 1.3–6.5], P=0.012). IRP frequently manifested with systemic inflammation (raised C‐reactive protein [121/136, 89.0%] and extrapericardial effusions [68/136, 50.0%]). Pericarditis was observed in all examined monogenic autoinflammatory diseases (0.4%–3.7% of cases). Rare deleterious MEFV variants were more frequent in IRP than in ancestry‐matched controls (allele frequency 9/200 versus 2932/129 200, P=0.040). Conclusions Pericarditis is a feature of interleukin‐1 driven monogenic autoinflammatory diseases and IRP is associated with variants in MEFV, a gene involved in interleukin‐1β processing. We also found that corticosteroid dependence in IRP is associated with chronic noninflammatory pain. Together these data implicate autoinflammation in IRP and support reducing reliance on corticosteroids in its management.
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