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患者和公众参与对临床试验入组和保留的影响:系统评价和荟萃分析。

Impact of patient and public involvement on enrolment and retention in clinical trials: systematic review and meta-analysis.

机构信息

Health Experiences Research Group, Nuffield Department of Primary Care Health Sciences, University of Oxford, Oxford OX2 6GG, UK

National Institute for Health Research (NIHR) Oxford Biomedical Research Centre (BRC), John Radcliffe Hospital, Oxford, UK.

出版信息

BMJ. 2018 Nov 28;363:k4738. doi: 10.1136/bmj.k4738.

Abstract

OBJECTIVE

To investigate the impact of patient and public involvement (PPI) on rates of enrolment and retention in clinical trials and explore how this varies with the context and nature of PPI.

DESIGN

Systematic review and meta-analysis.

DATA SOURCES

Ten electronic databases, including Medline, INVOLVE Evidence Library, and clinical trial registries.

ELIGIBILITY CRITERIA

Experimental and observational studies quantitatively evaluating the impact of a PPI intervention, compared with no intervention or non-PPI intervention(s), on participant enrolment and/or retention rates in a clinical trial or trials. PPI interventions could include additional non-PPI components inseparable from the PPI (for example, other stakeholder involvement).

DATA EXTRACTION AND ANALYSIS

Two independent reviewers extracted data on enrolment and retention rates, as well as on the context and characteristics of PPI intervention, and assessed risk of bias. Random effects meta-analyses were used to determine the average effect of PPI interventions on enrolment and retention in clinical trials: main analysis including randomised studies only, secondary analysis adding non-randomised studies, and several exploratory subgroup and sensitivity analyses.

RESULTS

26 studies were included in the review; 19 were eligible for enrolment meta-analysis and five for retention meta-analysis. Various PPI interventions were identified with different degrees of involvement, different numbers and types of people involved, and input at different stages of the trial process. On average, PPI interventions modestly but significantly increased the odds of participant enrolment in the main analysis (odds ratio 1.16, 95% confidence interval and prediction interval 1.01 to 1.34). Non-PPI components of interventions may have contributed to this effect. In exploratory subgroup analyses, the involvement of people with lived experience of the condition under study was significantly associated with improved enrolment (odds ratio 3.14 1.07; P=0.02). The findings for retention were inconclusive owing to the paucity of eligible studies (odds ratio 1.16, 95% confidence interval 0.33 to 4.14), for main analysis).

CONCLUSIONS

These findings add weight to the case for PPI in clinical trials by indicating that it is likely to improve enrolment of participants, especially if it includes people with lived experience of the health condition under study. Further research is needed to assess which types of PPI work best in particular contexts, the cost effectiveness of PPI, the impact of PPI at earlier stages of trial design, and the impact of PPI interventions specifically targeting retention.

SYSTEMATIC REVIEW REGISTRATION

PROSPERO CRD42016043808.

摘要

目的

研究患者和公众参与(PPI)对临床试验入组率和保留率的影响,并探讨其如何随 PPI 的背景和性质而变化。

设计

系统评价和荟萃分析。

资料来源

10 个电子数据库,包括 Medline、INVOLVE 证据库和临床试验注册处。

入选标准

定量评估 PPI 干预对临床试验中参与者入组和/或保留率影响的实验和观察性研究,与无干预或非 PPI 干预相比。PPI 干预可包括与 PPI 不可分割的其他非 PPI 组成部分(例如,其他利益攸关方的参与)。

数据提取和分析

两名独立审查员提取了关于入组和保留率以及 PPI 干预背景和特征的数据,并评估了偏倚风险。采用随机效应荟萃分析确定 PPI 干预对临床试验入组和保留的平均影响:主要分析仅包括随机研究,次要分析增加了非随机研究,以及几项探索性亚组和敏感性分析。

结果

综述纳入 26 项研究;19 项研究符合入组荟萃分析的条件,5 项研究符合保留荟萃分析的条件。确定了各种 PPI 干预措施,其参与程度不同,涉及的人数和类型不同,并且在试验过程的不同阶段都有投入。平均而言,PPI 干预适度但显著增加了主要分析中参与者入组的可能性(比值比 1.16,95%置信区间和预测区间为 1.01 至 1.34)。干预措施的非 PPI 组成部分可能促成了这一效果。在探索性亚组分析中,与所研究疾病有亲身体验的人的参与与入组率的提高显著相关(比值比 3.14,1.07;P=0.02)。由于合格研究的缺乏,保留分析的结果不确定(主要分析的比值比 1.16,95%置信区间 0.33 至 4.14)。

结论

这些发现通过表明 PPI 可能提高参与者的入组率,特别是如果它包括对所研究健康状况有亲身体验的人,为临床试验中的 PPI 提供了更多的依据。需要进一步研究以评估哪种类型的 PPI 在特定情况下效果最好、PPI 的成本效益、PPI 在试验设计早期阶段的影响以及专门针对保留率的 PPI 干预措施的影响。

系统评价注册

PROSPERO CRD42016043808。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fcbc/6259046/27497f565a32/croj045186.f1.jpg

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