Wyneski Matthew J, Green Alex, Kay Marsha, Wyllie Robert, Mahajan Lori
Department of Pediatric Gastroenterology and Nutrition, Children's Hospital, Cleveland Clinic, Cleveland, OH 44195, USA.
J Pediatr Gastroenterol Nutr. 2008 Jul;47(1):19-25. doi: 10.1097/MPG.0b013e318174e886.
Adalimumab has recently become available for adult patients with Crohn disease (CD) as a viable alternative tumor necrosis factor-alpha inhibitor to infliximab. To our knowledge, there have been no studies reviewing the use of adalimumab in pediatric patients with CD. Our aim was to examine the safety and efficacy of adalimumab therapy in pediatric patients with CD.
We performed a retrospective chart review of 15 pediatric patients with CD who received adalimumab at a single institution between January 2003 and March 2007. All of the patients had a history of an attenuated response or anaphylaxis to infliximab. Each patient's chart was reviewed for age at diagnosis, sex, extent of disease, age at start of adalimumab therapy, course of therapy, side effects noted during therapy, concurrent medications, and response to adalimumab. Clinical response to adalimumab was classified as complete, partial, or no response based on the patients' ability to be weaned from steroids, increased or decreased need for steroids, or need for surgery during the course of treatment. This study was approved by the Cleveland Clinic Institutional Review Board.
Fifteen pediatric patients with CD received adalimumab for a 33-month period. Of those, 14 patients had adequate follow-up, and 1 patient was lost to follow-up. The mean age at initiation of therapy was 16.6 years (median 17.9 years, range 10.3-21.8 years, SD 3.1 years). The majority of patients received an 80-mg loading dose administered subcutaneously and 40-mg doses subsequently every 2 weeks. The median duration of therapy was 6.5 months (range 1-31 months). A total of 272 injections were given. Of the 14 patients with sufficient data for follow-up, 7 (50%) had a complete response, 2 (14%) had a partial response, and 5 (36%) had no response to adalimumab. Complete response was achieved after a median of 5 injections (range 3-11). Of the 14 patients with adequate follow-up, 5 had fistulizing disease; 3 of these maintained fistula closure, 1 had temporary closure, and 1 required surgery to assist with closure. Twenty-six adverse events occurred during therapy. Eight (57%) patients had at least 1 adverse effect. The most common events were abdominal pain and nausea. No serious adverse events were reported, no serious infections occurred, and no adverse events required discontinuation of adalimumab.
Adalimumab was well tolerated in pediatric patients with CD. Complete or partial response was observed in 64% of patients. No serious adverse events occurred during therapy. Additional studies are needed to evaluate the efficacy and to determine optimal dosing of adalimumab in the pediatric population with CD.
阿达木单抗最近已可用于成年克罗恩病(CD)患者,作为英夫利昔单抗可行的替代肿瘤坏死因子-α抑制剂。据我们所知,尚无关于阿达木单抗在儿童CD患者中应用的研究。我们的目的是研究阿达木单抗治疗儿童CD患者的安全性和有效性。
我们对2003年1月至2007年3月期间在单一机构接受阿达木单抗治疗的15例儿童CD患者进行了回顾性病历审查。所有患者均有对英夫利昔单抗反应减弱或过敏反应的病史。审查了每位患者的病历,包括诊断时的年龄、性别、疾病范围、开始阿达木单抗治疗时的年龄、治疗过程、治疗期间记录的副作用、同时使用的药物以及对阿达木单抗的反应。根据患者在治疗过程中能否停用类固醇、类固醇需求增加或减少或是否需要手术,将对阿达木单抗的临床反应分为完全缓解、部分缓解或无反应。本研究经克利夫兰诊所机构审查委员会批准。
15例儿童CD患者接受了33个月的阿达木单抗治疗。其中,14例患者有充分的随访,1例失访。开始治疗时的平均年龄为16.6岁(中位数17.9岁,范围10.3 - 21.8岁,标准差3.1岁)。大多数患者接受皮下注射80mg的负荷剂量,随后每2周注射40mg。治疗的中位持续时间为6.5个月(范围1 - 31个月)。共注射272次。在14例有足够随访数据的患者中,7例(50%)完全缓解,2例(14%)部分缓解,5例(36%)对阿达木单抗无反应。中位5次注射(范围3 - 11次)后实现完全缓解。在14例有充分随访的患者中,5例有瘘管病;其中3例维持瘘管闭合,1例暂时闭合,1例需要手术辅助闭合。治疗期间发生26起不良事件。8例(57%)患者至少有1次不良反应。最常见的事件是腹痛和恶心。未报告严重不良事件,未发生严重感染,且无不良事件需要停用阿达木单抗。
阿达木单抗在儿童CD患者中耐受性良好。64%的患者观察到完全或部分缓解。治疗期间未发生严重不良事件。需要进一步研究以评估阿达木单抗在儿童CD患者中的疗效并确定最佳剂量。
