Division of Gastroenterology, and Nutrition, McMaster Children's Hospital, Hamilton, Ontario, Canada.
J Pediatr Gastroenterol Nutr. 2013 May;56(5):512-8. doi: 10.1097/MPG.0b013e31828390ba.
Infliximab (IFX), an established therapy for pediatric Crohn disease (CD), is also efficacious in treating psoriasis, a skin disorder, in which tumor necrosis factor-α is implicated pathogenically. Paradoxically, there have been numerous reports of new-onset psoriasis following tumor necrosis factor-α antagonist therapy in adult patients with inflammatory bowel disease, but pediatric data are sparse.
A retrospective review of all IFX-treated patients with CD, who subsequently developed psoriasis, at a single pediatric inflammatory bowel disease center, was performed. A subset of affected patients (10/18) and CD controls (147 of 172) treated with IFX but without the development of psoriasis were genotyped for polymorphisms in the interleukin-23 receptor (IL-23R) gene, which has been identified as conferring susceptibility to both CD and psoriasis.
Eighteen (10.5%) of 172 IFX-treated patients with CD developed new-onset psoriasis (n = 17) or worsening of existing psoriasis (n = 1). The duration of IFX exposure was variable, ranging from 1 to 25 infusions. Three patients discontinued IFX because of this complication. Most patients responded well to topical steroid therapy. In comparison to disease-matched controls, patients with CD developing psoriasis following IFX therapy were more likely to be homozygous for specific polymorphisms in the IL-23R gene (rs10489628, rs10789229, and rs1343151).
As in adults, the development of psoriasis or psoriasiform skin lesions occurs in pediatric patients with CD treated with IFX. Adequately powered studies are required to further explore the preliminary findings reported here to determine whether polymorphisms in the IL-23R gene have a role in the pathogenesis of this paradoxical process, which presently remains unexplained.
英夫利昔单抗(IFX)是一种治疗小儿克罗恩病(CD)的成熟疗法,在治疗银屑病方面也同样有效,银屑病是一种皮肤疾病,其病理机制涉及肿瘤坏死因子-α。矛盾的是,在接受炎症性肠病的成年患者中,使用肿瘤坏死因子-α拮抗剂治疗后,有大量新发病例银屑病的报告,但儿科数据很少。
在一家儿科炎症性肠病中心,对所有接受 IFX 治疗后出现银屑病的 CD 患者进行了回顾性研究。对一部分受影响的患者(18 例中的 10 例)和接受 IFX 治疗但未发生银屑病的 CD 对照患者(172 例中的 147 例)进行了白细胞介素-23 受体(IL-23R)基因多态性的基因分型,该基因已被确定为 CD 和银屑病的易感基因。
172 例接受 IFX 治疗的 CD 患者中有 18 例(10.5%)出现新发银屑病(n = 17)或原有银屑病恶化(n = 1)。IFX 暴露的时间长短不一,范围从 1 到 25 次输注。有 3 例患者因该并发症停用 IFX。大多数患者对局部皮质类固醇治疗反应良好。与疾病匹配的对照组相比,在接受 IFX 治疗后出现银屑病的 CD 患者更有可能是 IL-23R 基因特定多态性的纯合子(rs10489628、rs10789229 和 rs1343151)。
与成年人一样,接受 IFX 治疗的 CD 患儿也会出现银屑病或银屑病样皮肤病变。需要进行充分的研究来进一步探索这里报告的初步发现,以确定 IL-23R 基因多态性是否在这一矛盾过程的发病机制中起作用,目前这一过程仍然无法解释。
