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依那西普联合 IVIg 治疗急性川崎病:一项随机对照试验。

Etanercept With IVIg for Acute Kawasaki Disease: A Randomized Controlled Trial.

机构信息

Seattle Children's Research Institute, School of Medicine, University of Washington, Seattle, Washington;

Sainte Justine University Hospital Center, University of Montreal, Montreal, Canada.

出版信息

Pediatrics. 2019 Jun;143(6). doi: 10.1542/peds.2018-3675. Epub 2019 May 2.

Abstract

OBJECTIVES

Patients with Kawasaki disease can develop life-altering coronary arterial abnormalities, particularly in those resistant to intravenous immunoglobulin (IVIg) therapy. We tested the tumor necrosis factor α receptor antagonist etanercept for reducing both IVIg resistance and coronary artery (CA) disease progression.

METHODS

In a double-blind multicenter trial, patients with Kawasaki disease received either etanercept (0.8 mg/kg; = 100) or placebo ( = 101) subcutaneously starting immediately after IVIg infusion. IVIg resistance was the primary outcome with prespecified subgroup analyses according to age, sex, and race. Secondary outcomes included echocardiographic CA measures within subgroups defined by coronary dilation ( score >2.5) at baseline. We used generalized estimating equations to analyze score change and a prespecified algorithm for change in absolute diameters.

RESULTS

IVIg resistance occurred in 22% (placebo) and 13% (etanercept) of patients ( = .10). Etanercept reduced IVIg resistance in patients >1 year of age ( = .03). In the entire population, 46 (23%) had a coronary score >2.5 at baseline. Etanercept reduced coronary score change in those with and without baseline dilation ( = .04 and = .001); no improvement occurred in the analogous placebo groups. Etanercept ( = 22) reduced dilation progression compared with placebo ( = 24) by algorithm in those with baseline dilation ( = .03). No difference in the safety profile occurred between etanercept and placebo.

CONCLUSIONS

Etanercept showed no significant benefit in IVIg resistance in the entire population. However, preplanned analyses showed benefit in patients >1 year. Importantly, etanercept appeared to ameliorate CA dilation, particularly in patients with baseline abnormalities.

摘要

目的

川崎病患者可能会出现危及生命的冠状动脉异常,尤其是那些对静脉注射免疫球蛋白(IVIg)治疗有抵抗力的患者。我们测试了肿瘤坏死因子-α受体拮抗剂依那西普,以减少 IVIg 耐药和冠状动脉(CA)疾病进展。

方法

在一项双盲多中心试验中,川崎病患者在 IVIg 输注后立即接受依那西普(0.8mg/kg;n=100)或安慰剂(n=101)皮下注射。IVIg 耐药是主要结局,根据年龄、性别和种族进行了预先指定的亚组分析。次要结局包括根据基线时冠状动脉扩张( score >2.5)定义的亚组中超声心动图 CA 指标的变化。我们使用广义估计方程分析了 score 的变化,并使用预先指定的算法分析了绝对直径的变化。

结果

安慰剂组和依那西普组分别有 22%(安慰剂)和 13%(依那西普)的患者发生 IVIg 耐药( =.10)。依那西普降低了 1 岁以上患者的 IVIg 耐药性( =.03)。在整个人群中,46 人(23%)在基线时有冠状动脉 score >2.5。依那西普降低了基线无扩张和有扩张患者的冠状动脉 score 变化( =.04 和 =.001);基线扩张的类似安慰剂组没有改善。依那西普( = 22)与安慰剂( = 24)相比,通过算法减少了基线扩张患者的扩张进展( =.03)。依那西普和安慰剂的安全性特征没有差异。

结论

依那西普在整个人群中对 IVIg 耐药没有显著益处。然而,预先计划的分析显示,1 岁以上患者受益。重要的是,依那西普似乎改善了 CA 扩张,特别是在基线异常的患者中。

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