Patient-reported outcomes in randomized clinical trials: development of ISOQOL reporting standards

Patient-reported outcome (PRO) data, including health-related quality of life (HRQL), from randomised clinical trials (RCTs) may be used to inform clinical decision making, health policy, and reimbursement decisions [1]. PRO data can also be used to meet patients’ information needs and to establish treatment preferences [2‐6]. However, the collection of PRO data in RCTs is not without costs, including patient and investigator time, and costs associated with questionnaire administration and analysis. For PRO data from RCTs to provide value, the RCTs and PROs need to be well designed, analyzed appropriately, and reported in a way that makes the results accessible and useful to end-users. Inadequate or poor-quality reporting limits the valid application of PRO findings in clinical practice [7‐9] and can limit synthesis of trial results across studies, using meta-analytic or other synthesis approaches.

Although a number of publications provide guidelines for reporting HRQL outcomes, their implementation in RCTs remains suboptimal. In a recent review of 794 trials that reported HRQL outcomes of biomedical interventions across a range of clinical areas, less than 60 % provided a rationale for the selected outcome measure or a HRQL hypothesis, 33 % did not discuss the HRQL findings within the context of other trials outcomes, and only 28 % provided information on missing HRQL data [10].

Inadequacies in trial reporting in general have been addressed through the development of the Consolidated Standards of Reporting Trials (CONSORT) Statement [11]. This is ‘an evidence-based, minimum set of recommendations for reporting RCTs’ which ‘offers a standard way for authors to prepare reports of trial findings, facilitating their complete and transparent reporting, and aiding their critical appraisal and interpretation.’[11] The original CONSORT statement and its subsequent ‘extensions’ have been widely endorsed by a number of leading international journals [12]. CONSORT standards specific to PROs, and specifically HRQL, do not currently exist. Recognizing the need for improved reporting of quality of life outcomes, the International Society for Quality of Life Research (ISOQOL) formed a Task Force to lead the development of an official CONSORT extension. This work has been undertaken in collaboration with the CONSORT executive, MRC Midland and ConDuCT Hubs for Trials Methodology Research, leading international journal editors, policy makers, and patient representatives [11, 13, 14]. In this paper, we describe the process that was undertaken by the Task Force to establish an ISOQOL consensus on standards for PRO reporting and report the resultant suite of ISOQOL-recommended standards for PRO reporting. The suite of standards is intended to inform the process of establishing a CONSORT extension for reporting PRO outcomes of RCTs based on broader stakeholder input.

Synthesis of a systematic review of the literature and survey of the ISOQOL membership has informed the development of ISOQOL reporting guidelines for PROs in the primary publication of RCTs. More specifically, we provide reporting standards for RCTs reporting any PRO outcome and make additional recommendations for those trials in which PROs are the primary outcome. This work will be used to inform an official CONSORT extension for PRO reporting in RCTs.

While current CONSORT guidelines for trial reporting include several standards that apply to HRQL and PRO endpoints, the Task Force felt that further clarification was needed [11]. For example, the 2010 CONSORT guidance states that ‘a table showing baseline demographic and clinical characteristics for each group should be reported.’ However, neither the guideline nor the explanatory document explicitly recommends that publications report baseline values relating to the primary or secondary PRO endpoints with a measure of their variability. There is also a lack of clarity about the appropriate level of detail required for reporting missing outcome data, which is particularly critical when interpreting PRO trial endpoints.

The new ISOQOL reporting guidelines have important implications beyond improved documentation of trial outcomes if they also act to influence the design of future trials with PRO measures. Evidence for this type of impact is apparent in other areas; since the publication of the original CONSORT guidance, there is now work being undertaken to provide trialists and clinicians with standards for trial protocol development [30]. Future international collaborations among stakeholder groups could include similar efforts for informing trial design with respect to PROs.

The reality of journal word limits may constrain comprehensive reporting of all of the ISOQOL-recommended standards, particularly when the PRO is a secondary study outcome. A recent review of HRQL reporting in clinical trials across a range of clinical areas showed that HRQL was a secondary outcome in 75 % of studies (594/794) [10]. Without transparent reporting of these secondary outcomes, it may be impossible for readers or consumers to assess the quality of the results and identify any potential bias. Journal web appendices are a relatively new option that may, in part, alleviate this problem.

The process used to establish PRO reporting standards for RCTs has a number of strengths. The candidate reporting standards were identified through a formal systematic review, and the guidance was developed through a comprehensive iterative process with multiple opportunities for feedback from the experts within the ISOQOL membership who have a collective, extensive international experience in this field. A modified Delphi approach was used to assess member opinions and to reach consensus on a final list of reporting standards; this approach is consistent with the development of other CONSORT guidelines [31]. The consistency of endorsement of each standard across different areas of respondents’ expertise is an indication of the reliability of the survey data. One notable, but perhaps not surprising, exception to this consistency is that a higher proportion of clinicians rated reporting of the clinical significance of results as essential, demonstrating the potential importance of this item for translation of HRQL results into practice.

The interpretation of the survey results and the consensus recommendations are limited in some ways including the use of the online survey method to poll ISOQOL members. Although we attempted to invite all ISOQOL members to respond, it is unknown how many members actually received or viewed the email, and an accurate response rate cannot be calculated. Likewise, the ‘view rate’ of email invitations cannot be calculated due to the anonymous nature of the research method [32]. Further, it is likely that some ISOQOL members felt that they did not have sufficient expertise or interest in this academic topic to respond, and regrettably, we did not allow such a response option in our design. Likewise, it is possible that some respondents with only passing interest in the topic may have completed the survey without sufficient knowledge or experience in designing, analyzing, reporting, or interpreting RCTs. With regard to the latter possibility, however, we note that the majority of respondents did report having significant expertise in HRQL research. Again, the consistency of responses across expertise groups suggests reliability of the findings. Although there was clearly underlying variation in ISOQOL member opinions, particularly when HRQL is a secondary outcome, the systematic approach to the data by the Task Force led to final recommended standards that are in keeping with the majority view of the member survey results for each standard considered in the survey. Finally, while the literature search and survey focussed on HRQL standards, rather than all PROs, the consensus process endorsed the expanded scope.