Corticosteroid therapy for nephrotic syndrome in children.

IF 8.8 2区 医学 Q1 MEDICINE, GENERAL & INTERNAL
Deirdre Hahn, Susan M Samuel, Narelle S Willis, Jonathan C Craig, Elisabeth M Hodson
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引用次数: 0

Abstract

Background: In nephrotic syndrome, protein leaks from the blood into the urine through the glomeruli, resulting in hypoproteinaemia and generalised oedema. While most children with nephrotic syndrome respond to corticosteroids, 80% experience a relapsing course. Corticosteroids have reduced the death rate to around 3%; however, corticosteroids have well-recognised potentially serious adverse events such as obesity, poor growth, hypertension, diabetes mellitus, osteoporosis, cataracts, glaucoma and behavioural disturbances. This is an update of a review first published in 2000 and updated in 2002, 2005, 2007, 2015 and 2020.

Objectives: The aim of this review was to assess the benefits and harms of different corticosteroid regimens in children with steroid-sensitive nephrotic syndrome (SSNS). The benefits and harms of therapy were studied in two groups of children: 1) children in their initial episode of SSNS and 2) children who experience a relapsing course of SSNS.

Search methods: We contacted the Information Specialist and searched the Cochrane Kidney and Transplant Register of Studies up to 9 July 2024 using search terms relevant to this review. Studies in the Register are identified through searches of CENTRAL, MEDLINE, and EMBASE, conference proceedings, the International Clinical Trials Registry Platform (ICTRP) Search Portal, and ClinicalTrials.gov.

Selection criteria: Randomised controlled trials (RCTs) performed in children (one to 18 years) during their initial or subsequent episode of SSNS, comparing different durations, total doses or other dose strategies using any corticosteroid agent.

Data collection and analysis: Summary estimates of effects were obtained using a random-effects model, and results were expressed as risk ratios (RR) and their 95% confidence intervals (CI) for dichotomous outcomes and mean difference (MD) and 95% CI for continuous outcomes. Confidence in the evidence was assessed using the Grading of Recommendations Assessment, Development and Evaluation (GRADE) approach.

Main results: In this 2024 update, we included five new studies, resulting in 54 studies randomising 4670 children. Risk of bias methodology was often poorly performed, with only 31 studies and 28 studies respectively assessed to be at low risk for random sequence generation and allocation concealment. Ten studies were at low risk of performance bias (blinding of participants and personnel), and 12 studies were at low risk of detection bias (blinding of outcome assessment); nine of these studies were placebo-controlled RCTs. Twenty-seven studies (fewer than 50%) were at low risk for attrition bias, and 26 studies were at low risk for reporting bias (selective outcome reporting). In studies at low risk of selection bias evaluating children in their initial episode of SSNS, there is little or no difference in the number of children with frequent relapses when comparing two months of prednisone with three months or more (RR 0.96, 95% CI 0.83 to 1.10; 755 children, 5 studies; I2 = 0%; high certainty evidence) or when comparing three months with five to seven months of therapy (RR 0.99, 95% CI 0.74 to 1.33; 376 children, 3 studies; I2 = 35%; high certainty evidence). In analyses of studies at low risk of selection bias, there is little or no difference in the number of children with any relapse by 12 to 24 months when comparing two months of prednisone with three months or more (RR 0.93, 95% CI 0.81 to 1.06; 808 children; 6 studies; I2 = 47%) or when comparing three months with five to seven months of therapy (RR 0.88, 95% CI 0.70 to 1.11; 377 children, 3 studies; I2 = 53%). Little or no difference was noted in adverse events between the different treatment durations. Amongst children with relapsing SSNS, four small studies (177 children) utilising lower doses of prednisone compared with standard regimens found little or no differences between groups in the numbers with relapse (RR 1.01, 95% CI 0.85 to 1.20; I2 = 0%). A fifth study (117 children) reported little or no difference between two weeks and four weeks of alternate-day prednisone after remission with daily prednisone. A recent large, well-designed study with 271 children found that administering daily prednisone compared with alternate-day prednisone or no prednisone during viral infection did not reduce the risk of relapse. In contrast, four previous small studies in children with frequently relapsing disease had reported that daily prednisone during viral infections compared with alternate-day prednisone or no treatment reduced the risk of relapse.

Authors' conclusions: There are four well-designed studies randomising 823 children, which have demonstrated that there is no benefit of prolonging prednisone therapy beyond two to three months in the first episode of SSNS. Small studies in children with relapsing disease have identified no differences in efficacy using lower induction doses or shorter durations of prednisone therapy. Large, well-designed studies are required to confirm these findings. While previous small studies had suggested that changing from alternate-day to daily prednisone therapy at the onset of infection reduced the likelihood of relapse, a much larger and well-designed study found no reduction in the number relapsing when administering daily prednisone at the onset of infection.

皮质类固醇治疗儿童肾病综合征。
背景:在肾病综合征中,蛋白质从血液通过肾小球渗入尿液,导致低蛋白血症和全身水肿。虽然大多数肾病综合征患儿对皮质类固醇有反应,但80%的患儿病情会复发。皮质类固醇已将死亡率降至 3% 左右;然而,皮质类固醇也有公认的潜在严重不良反应,如肥胖、发育不良、高血压、糖尿病、骨质疏松症、白内障、青光眼和行为紊乱。本综述是对 2000 年首次发表的综述的更新,并于 2002 年、2005 年、2007 年、2015 年和 2020 年进行了更新:本综述旨在评估不同皮质类固醇治疗方案对类固醇敏感肾病综合征(SSNS)患儿的益处和危害。研究对象包括两类儿童:1)SSNS初次发病的儿童;2)SSNS复发的儿童:我们联系了信息专家,并使用与本综述相关的检索词检索了截至 2024 年 7 月 9 日的 Cochrane 肾脏与移植研究登记册。登记册中的研究是通过检索 CENTRAL、MEDLINE 和 EMBASE、会议论文集、国际临床试验登记平台 (ICTRP) 搜索门户和 ClinicalTrials.gov 确定的:随机对照试验(RCT):在儿童(1 至 18 岁)初次或随后出现 SSNS 时进行的试验,比较使用任何皮质类固醇药物的不同持续时间、总剂量或其他剂量策略:使用随机效应模型对效果进行简要估计,对于二分结果,用风险比(RR)及其 95% 置信区间(CI)表示,对于连续结果,用平均差(MD)及其 95% 置信区间(CI)表示。证据可信度采用建议评估、发展和评价分级法(GRADE)进行评估:在此次 2024 年更新中,我们纳入了五项新研究,共进行了 54 项研究,随机抽取了 4670 名儿童。偏倚风险评估方法通常效果不佳,分别只有 31 项研究和 28 项研究在随机序列生成和分配隐藏方面被评估为低风险。10项研究的表现偏倚风险较低(对参与者和工作人员进行盲法处理),12项研究的检测偏倚风险较低(对结果评估进行盲法处理);其中9项研究为安慰剂对照 RCT。27项研究(少于50%)的自然减员偏倚风险较低,26项研究的报告偏倚(选择性结果报告)风险较低。选择偏倚风险较低的研究对初次患 SSNS 的儿童进行了评估,在将两个月的泼尼松治疗与三个月或更长时间的治疗进行比较时(RR 0.96,95% CI 0.83 至 1.10;755 名儿童,5 项研究;I2 = 0%;高确定性证据),或将三个月的治疗与五至七个月的治疗进行比较时(RR 0.99,95% CI 0.74 至 1.33;376 名儿童,3 项研究;I2 = 35%;高确定性证据),频繁复发的儿童人数几乎没有差异。在对选择偏倚风险较低的研究进行的分析中,将泼尼松治疗两个月与三个月或更长时间进行比较时,12至24个月内复发的儿童人数几乎没有差异(RR为0.93,95% CI为0.81至1.06;808名儿童;6项研究;I2=47%),将三个月与五至七个月的治疗进行比较时,也几乎没有差异(RR为0.88,95% CI为0.70至1.11;377名儿童,3项研究;I2=53%)。不同疗程的不良反应几乎没有差异。在复发的 SSNS 儿童中,有四项小型研究(177 名儿童)使用较低剂量的泼尼松与标准疗法进行比较,结果发现不同组别在复发人数上几乎没有差异(RR 1.01,95% CI 0.85 至 1.20;I2 = 0%)。第五项研究(117 名儿童)报告称,在使用每日泼尼松缓解病情后,使用两周和四周的隔日泼尼松治疗几乎没有差异。最近一项对 271 名儿童进行的大型、精心设计的研究发现,在病毒感染期间,每日使用泼尼松与隔日使用泼尼松或不使用泼尼松相比,并不能降低复发风险。与此相反,之前有四项针对经常复发儿童的小型研究报告称,在病毒感染期间每天使用泼尼松与隔天使用泼尼松或不使用泼尼松相比,可降低复发风险:有四项精心设计的研究随机抽取了 823 名儿童,结果表明,在 SSNS 首次发作时,将泼尼松治疗时间延长至两到三个月以上并无益处。对复发儿童进行的小型研究发现,使用较低的诱导剂量或较短的泼尼松疗程,疗效并无差异。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
10.60
自引率
2.40%
发文量
173
审稿时长
1-2 weeks
期刊介绍: The Cochrane Database of Systematic Reviews (CDSR) stands as the premier database for systematic reviews in healthcare. It comprises Cochrane Reviews, along with protocols for these reviews, editorials, and supplements. Owned and operated by Cochrane, a worldwide independent network of healthcare stakeholders, the CDSR (ISSN 1469-493X) encompasses a broad spectrum of health-related topics, including health services.
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