Gastroenterology Department, Centre Hospitalier Universitaire de Liège, Liège, Belgium.
INSERM U717, Biostatistics and Clinical Epidemiology, Université Paris Diderot-Paris 7, Paris, France.
Clin Gastroenterol Hepatol. 2018 Feb;16(2):234-243.e2. doi: 10.1016/j.cgh.2017.09.061. Epub 2017 Oct 7.
BACKGROUND & AIMS: Little is known about long-term outcomes of patients with Crohn's disease (CD) after infliximab withdrawal. We aimed to describe the long-term outcomes of patients with CD in clinical remission after infliximab treatment was withdrawn.
We performed a retrospective analysis of data from the 115 patients included in the infliximab discontinuation in patients with CD in stable remission on combined therapy with antimetabolites (STORI) study, performed at 20 centers in France and Belgium from March 2006 through December 2009. The STORI cohort was a prospective analysis of risk and factors associated with relapse following withdrawal of maintenance therapy with infliximab, maintained on antimetabolites, while in clinical remission. We collected data from the end of the study until the last available follow-up examination on patient surgeries, new complex perianal lesions (indicating major complications), and need for and outcomes of restarting therapy with infliximab or another biologic agent. The de-escalation strategy was considered to have failed when a major complication or infliximab restart failure occurred.
Of the 115 patients initially included, data from 102 patients (from 19 of the 20 study centers) were included in the final analysis. The median follow-up time was 7 years. Twenty-one percent of the patients did not restart treatment with infliximab or another biologic agent and did not have a major complication 7 years after infliximab withdrawal (95% CI, 13.1-30.3). Among patients who restarted infliximab, treatment failed for 30.1% 6 years after restarting (95% CI, 18.5-42.5). Overall, at 7 years after stopping infliximab therapy, major complications occurred in 18.5% of patients (95% CI, 10.2-26.8) whereas 70.2% of patients had no failure of the de-escalation strategy (95% CI, 60.2-80.1). Factors independently associated with major complications were upper-gastrointestinal location of disease, white blood cell count ≥ 5.0 × 10/L, and hemoglobin level ≤12.5 g/dL at the time of infliximab withdrawal. Patients with at least 2 of these factors had a more than 40% risk of major complication in the 7 years following infliximab withdrawal.
In a long-term follow-up of the STORI cohort (7 years) one fifth of the patients did not restart infliximab or another biologic agent and did not develop major complications. Seventy percent of patients had no failure of the de-escalation strategy (no major complication and no failure of infliximab restart).
对于英夫利昔单抗停药后的克罗恩病(CD)患者,其长期结局鲜为人知。本研究旨在描述接受英夫利昔单抗治疗后处于缓解期的 CD 患者的长期结局。
我们对来自法国和比利时 20 个中心于 2006 年 3 月至 2009 年 12 月进行的英夫利昔单抗停药治疗稳定缓解的 CD 患者(STORI)研究中纳入的 115 例患者的数据进行了回顾性分析。STORI 队列是对接受抗代谢物联合治疗处于缓解期的患者进行的前瞻性分析,在停用英夫利昔单抗维持治疗后,患者仍在接受抗代谢物治疗。我们收集了研究结束后至患者手术、新的复杂肛周病变(表明存在严重并发症)、以及重新开始英夫利昔单抗或其他生物制剂治疗的需求和结局的最后一次随访检查的数据。当发生严重并发症或英夫利昔单抗重新开始失败时,降级策略被认为失败。
在最初纳入的 115 例患者中,有 102 例(来自 20 个研究中心中的 19 个)患者的数据纳入最终分析。中位随访时间为 7 年。21%的患者在英夫利昔单抗停药 7 年后未重新开始英夫利昔单抗或其他生物制剂治疗,也未发生严重并发症(95%CI,13.1-30.3)。在重新开始英夫利昔单抗治疗的患者中,6 年后治疗失败的比例为 30.1%(95%CI,18.5-42.5)。总体而言,在停止英夫利昔单抗治疗 7 年后,18.5%的患者发生严重并发症(95%CI,10.2-26.8),而 70.2%的患者降级策略无失败(95%CI,60.2-80.1)。与严重并发症独立相关的因素包括疾病上消化道部位、白细胞计数≥5.0×10/L和英夫利昔单抗停药时血红蛋白水平≤12.5 g/dL。至少有 2 个这些因素的患者在英夫利昔单抗停药后 7 年内发生严重并发症的风险超过 40%。
在 STORI 队列的长期随访(7 年)中,五分之一的患者未重新开始英夫利昔单抗或其他生物制剂治疗,也未发生严重并发症。70%的患者降级策略无失败(无严重并发症,英夫利昔单抗重新开始也无失败)。
