BACKGROUND
Individual Patient Data (IPD) meta-analyses from clinical trials bring together information from completed studies, and help in identifying effective interventions, and plan new clinical trials. During a public health emergency such as the COVID-19 pandemic, identifying effective interventions in a timely manner becomes crucial for informed clinical management. In such contexts, providing access to IPD from clinical trial(s) is a cornerstone for meta-analyses.
OBJECTIVE
We undertook this review is to map the extent to which clinical trial investigators share IPD during the COVID-19 pandemic.
METHODS
All published COVID-19 therapeutic drug, and vaccine trials from January 1, 2020 to October 31, 2021 were identified. A literature search was conducted in PubMed. Only randomized controlled trial (RCT) publications were included; the publications included were retrospectively traced to clinical trial registries in order to get access to information on trial details. Data sharing statements in the published protocol(s), and published trial finding(s) were separately analysed to describe IPD sharing intentions(s), intended time frame and reason(s), if any, for not sharing IPD.
RESULTS
After screening 796 publications, 180 were included. Out of 180 publications, 33 were protocol publications and 157 were findings from the RCTs. Amongst RCT protocol publications, one third (11/33) of the principal investigators (PIs) committed to share IPD, of which only 27.27% (3/11) described specific time frame. Around 9.09% (3/33) trials did not intend to share IPD; whereas 57.58% (19/33) did not disclose intention to share IPD in the published RCT protocol.
On the other hand, publication of the RCT findings showed that more than half (52.23%, 82/157) of the PIs intended to share IPD. Amongst those who were willing to share IPD and had time frame to share IPD, 56.1% (46/82) described varying time frame such as at “6 months” (2.27%, 1/46) of trial completion. Similarly, 6.52% (3/46) of the PIs intended to share IPD “within or at one month” following trial publication.
CONCLUSIONS
Despite challenges in clinical trial data sharing, it is essential to recognise the need to make IPD available. As evident in our review, even during a pandemic the intentions to share IPD and the practice of IPD sharing has been suboptimal. Investigators’ commitment to share IPD varies greatly and there a need for systematic evaluation of the factors that prevent IPD sharing. We need collaborative efforts to promote IPD sharing in a legal and ethical manner involving various stakeholders. The COVID 19 clinical research coalition through its data sharing working group is engaging the various stakeholders, accelerating these efforts towards building consensus and mainstreaming best practices is critical in preparedness towards future public health emergencies. As governments are negotiating a proposal for an international instrument on pandemic prevention, preparedness and response, contextually appropriate IPD sharing requirements and regulations would be critical.
CLINICALTRIAL
Not applicable