Narula Neeraj, Dhillon Amit, Zhang Dongni, Sherlock Mary E, Tondeur Melody, Zachos Mary
Division of Gastroenterology, McMaster University, 1280 Main Street West, Hamilton, ON, Canada, L8S 4K1.
Cochrane Database Syst Rev. 2018 Apr 1;4(4):CD000542. doi: 10.1002/14651858.CD000542.pub3.
Corticosteroids are often preferred over enteral nutrition (EN) as induction therapy for Crohn's disease (CD). Prior meta-analyses suggest that corticosteroids are superior to EN for induction of remission in CD. Treatment failures in EN trials are often due to poor compliance, with dropouts frequently due to poor acceptance of a nasogastric tube and unpalatable formulations. This systematic review is an update of a previously published Cochrane review.
To evaluate the effectiveness and safety of exclusive EN as primary therapy to induce remission in CD and to examine the importance of formula composition on effectiveness.
We searched MEDLINE, Embase and CENTRAL from inception to 5 July 2017. We also searched references of retrieved articles and conference abstracts.
Randomized controlled trials involving patients with active CD were considered for inclusion. Studies comparing one type of EN to another type of EN or conventional corticosteroids were selected for review.
Data were extracted independently by at least two authors. The primary outcome was clinical remission. Secondary outcomes included adverse events, serious adverse events and withdrawal due to adverse events. For dichotomous outcomes, we calculated the risk ratio (RR) and 95% confidence interval (CI). A random-effects model was used to pool data. We performed intention-to-treat and per-protocol analyses for the primary outcome. Heterogeneity was explored using the Chi and I statistics. The studies were separated into two comparisons: one EN formulation compared to another EN formulation and EN compared to corticosteroids. Subgroup analyses were based on formula composition and age. Sensitivity analyses included abstract publications and poor quality studies. We used the Cochrane risk of bias tool to assess study quality. We used the GRADE criteria to assess the overall quality of the evidence supporting the primary outcome and selected secondary outcomes.
Twenty-seven studies (1,011 participants) were included. Three studies were rated as low risk of bias. Seven studies were rated as high risk of bias and 17 were rated as unclear risk of bias due to insufficient information. Seventeen trials compared different formulations of EN, 13 studies compared one or more elemental formulas to a non-elemental formula, three studies compared EN diets of similar protein composition but different fat composition, and one study compared non-elemental diets differing in glutamine enrichment. Meta-analysis of 11 trials (378 participants) demonstrated no difference in remission rates. Sixty-four per cent (134/210) of patients in the elemental group achieved remission compared to 62% (105/168) of patients in the non-elemental group (RR 1.02, 95% CI 0.88 to 1.18; GRADE very low quality). A per-protocol analysis (346 participants) produced similar results (RR 1.04, 95% CI 0.91 to 1.18). Subgroup analyses performed to evaluate the different types of elemental and non-elemental diets (elemental, semi-elemental and polymeric) showed no differences in remission rates. An analysis of 7 trials including 209 patients treated with EN formulas of differing fat content (low fat: < 20 g/1000 kCal versus high fat: > 20 g/1000 kCal) demonstrated no difference in remission rates (RR 1.03; 95% CI 0.85 to 1.26). Very low fat content (< 3 g/1000 kCal) and very low long chain triglycerides demonstrated higher remission rates than higher content EN formulas. There was no difference between elemental and non-elemental diets in adverse event rates (RR 1.00, 95% CI 0.63 to 1.60; GRADE very low quality), or withdrawals due to adverse events (RR 1.29, 95% CI 0.80 to 2.09; GRADE very low quality). Common adverse events included nausea, vomiting, diarrhea and bloating.Ten trials compared EN to steroid therapy. Meta-analysis of eight trials (223 participants) demonstrated no difference in remission rates between EN and steroids. Fifty per cent (111/223) of patients in the EN group achieved remission compared to 72% (133/186) of patients in the steroid group (RR 0.77, 95% CI 0.58 to 1.03; GRADE very low quality). Subgroup analysis by age showed a difference in remission rates for adults but not for children. In adults 45% (87/194) of EN patients achieved remission compared to 73% (116/158) of steroid patients (RR 0.65, 95% CI 0.52 to 0.82; GRADE very low quality). In children, 83% (24/29) of EN patients achieved remission compared to 61% (17/28) of steroid patients (RR 1.35, 95% CI 0.92 to 1.97; GRADE very low quality). A per-protocol analysis produced similar results (RR 0.93, 95% CI 0.75 to 1.14). The per-protocol subgroup analysis showed a difference in remission rates for both adults (RR 0.82, 95% CI 0.70 to 0.95) and children (RR 1.43, 95% CI 1.03 to 1.97). There was no difference in adverse event rates (RR 1.39, 95% CI 0.62 to 3.11; GRADE very low quality). However, patients on EN were more likely to withdraw due to adverse events than those on steroid therapy (RR 2.95, 95% CI 1.02 to 8.48; GRADE very low quality). Common adverse events reported in the EN group included heartburn, flatulence, diarrhea and vomiting, and for steroid therapy acne, moon facies, hyperglycemia, muscle weakness and hypoglycemia. The most common reason for withdrawal was inability to tolerate the EN diet.
AUTHORS' CONCLUSIONS: Very low quality evidence suggests that corticosteroid therapy may be more effective than EN for induction of clinical remission in adults with active CD. Very low quality evidence also suggests that EN may be more effective than steroids for induction of remission in children with active CD. Protein composition does not appear to influence the effectiveness of EN for the treatment of active CD. EN should be considered in pediatric CD patients or in adult patients who can comply with nasogastric tube feeding or perceive the formulations to be palatable, or when steroid side effects are not tolerated or better avoided. Further research is required to confirm the superiority of corticosteroids over EN in adults. Further research is required to confirm the benefit of EN in children. More effort from industry should be taken to develop palatable polymeric formulations that can be delivered without use of a nasogastric tube as this may lead to increased patient adherence with this therapy.
在克罗恩病(CD)的诱导治疗中,皮质类固醇通常比肠内营养(EN)更受青睐。先前的荟萃分析表明,皮质类固醇在诱导CD缓解方面优于EN。EN试验中的治疗失败通常是由于依从性差,而退出试验的常见原因是对鼻胃管接受度低和制剂口感不佳。本系统评价是对先前发表的Cochrane评价的更新。
评估单纯EN作为诱导CD缓解的主要治疗方法的有效性和安全性,并探讨配方组成对有效性的重要性。
我们检索了从数据库建立至2017年7月5日的MEDLINE、Embase和CENTRAL。我们还检索了检索文章的参考文献和会议摘要。
纳入涉及活动性CD患者的随机对照试验。选择比较一种EN与另一种EN或传统皮质类固醇的研究进行综述。
数据由至少两名作者独立提取。主要结局是临床缓解。次要结局包括不良事件、严重不良事件和因不良事件而退出。对于二分法结局,我们计算风险比(RR)和95%置信区间(CI)。采用随机效应模型汇总数据。我们对主要结局进行了意向性分析和符合方案分析。使用卡方检验和I²统计量探讨异质性。研究分为两个比较:一种EN配方与另一种EN配方比较,以及EN与皮质类固醇比较。亚组分析基于配方组成和年龄。敏感性分析包括摘要发表文章和质量较差的研究。我们使用Cochrane偏倚风险工具评估研究质量。我们使用GRADE标准评估支持主要结局和选定次要结局的证据的总体质量。
纳入27项研究(1011名参与者)。3项研究被评为低偏倚风险。7项研究被评为高偏倚风险,17项因信息不足被评为偏倚风险不明确。17项试验比较了不同的EN配方,13项研究比较了一种或多种要素配方与非要素配方,3项研究比较了蛋白质组成相似但脂肪组成不同的EN饮食,1项研究比较了谷氨酰胺富集程度不同的非要素饮食。对11项试验(378名参与者)的荟萃分析表明缓解率无差异。要素组中64%(134/210)的患者实现缓解,而非要素组为62%(105/168)(RR 1.02,95%CI 0.88至1.18;GRADE极低质量)。符合方案分析(346名参与者)得出了类似结果(RR 1.04,95%CI 0.91至1.18)。为评估不同类型的要素和非要素饮食(要素、半要素和聚合型)进行的亚组分析显示缓解率无差异。对7项试验(包括209名接受不同脂肪含量EN配方治疗的患者,低脂:<20 g/1000 kCal与高脂:>20 g/1000 kCal)的分析表明缓解率无差异(RR 1.03;95%CI 0.85至1.26)。极低脂肪含量(<3 g/1000 kCal)和极低长链甘油三酯的配方显示出比高脂肪含量EN配方更高的缓解率。要素饮食和非要素饮食在不良事件发生率(RR 1.00,95%CI 0.63至1.60;GRADE极低质量)或因不良事件而退出(RR 1.29,95%CI 0.80至2.09;GRADE极低质量)方面无差异。常见不良事件包括恶心、呕吐、腹泻和腹胀。10项试验比较了EN与类固醇疗法。对8项试验(223名参与者)的荟萃分析表明EN与类固醇之间的缓解率无差异。EN组中50%(111/223)的患者实现缓解,而类固醇组为72%(133/186)(RR 0.77,95%CI 0.58至1.03;GRADE极低质量)。按年龄进行的亚组分析显示成人缓解率存在差异,但儿童无差异。在成人中,EN组45%(87/194)的患者实现缓解,而类固醇组为73%(116/158)(RR 0.65,95%CI 0.52至0.82;GRADE极低质量)。在儿童中,EN组83%(24/29)的患者实现缓解,而类固醇组为61%(17/28)(RR 1.35,95%CI 0.92至1.97;GRADE极低质量)。符合方案分析得出了类似结果(RR 0.93,95%CI 0.75至1.14)。符合方案亚组分析显示成人(RR 0.82,95%CI 0.70至0.95)和儿童(RR 1.43,95%CI 1.03至1.97)的缓解率均存在差异。不良事件发生率无差异(RR 1.39,95%CI 0.62至3.11;GRADE极低质量)。然而,与接受类固醇治疗的患者相比,接受EN治疗的患者因不良事件而退出的可能性更大(RR 2.95,95%CI 1.02至8.48;GRADE极低质量)。EN组报告的常见不良事件包括烧心、肠胃气胀、腹泻和呕吐,类固醇治疗的不良事件包括痤疮、满月脸、高血糖、肌肉无力和低血糖。最常见的退出原因是无法耐受EN饮食。
极低质量的证据表明,皮质类固醇疗法在诱导活动性CD成人患者临床缓解方面可能比EN更有效。极低质量的证据还表明,EN在诱导活动性CD儿童患者缓解方面可能比类固醇更有效。蛋白质组成似乎不影响EN治疗活动性CD的有效性。对于儿科CD患者或能够依从鼻胃管喂养或认为制剂口感良好的成人患者,或当不能耐受或最好避免类固醇副作用时,应考虑使用EN。需要进一步研究以证实皮质类固醇在成人中优于EN。需要进一步研究以证实EN在儿童中的益处。行业应更加努力开发无需使用鼻胃管即可给药的可口聚合型制剂,因为这可能会提高患者对该疗法的依从性。
