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Effect of age, sex, and morbidity count on trial attrition: meta-analysis of individual participant level data from phase 3/4 industry funded clinical trials
  1. Jennifer S Lees1,
  2. Peter Hanlon1,
  3. Elaine W Butterly2,
  4. Sarah H Wild3,
  5. Frances S Mair1,
  6. Rod S Taylor1,
  7. Bruce Guthrie3,
  8. Katie Gillies4,
  9. Sofia Dias5,
  10. Nicky J Welton6 and
  11. David A McAllister1
  1. 1University of Glasgow, Glasgow, UK
  2. 2Institute of Health and Wellbeing, University of Glasgow, Glasgow, UK
  3. 3University of Edinburgh, Edinburgh, UK
  4. 4University of Aberdeen, Aberdeen, UK
  5. 5University of York, York, UK
  6. 6Population Health Sciences, University of Bristol, Bristol, UK
  1. Correspondence to Dr Jennifer S Lees, University of Glasgow, Glasgow, UK; jennifer.lees{at}glasgow.ac.uk

Abstract

Objectives To estimate the association between individual participant characteristics and attrition from randomised controlled trials.

Design Meta-analysis of individual participant level data (IPD).

Data sources Clinical trial repositories (Clinical Study Data Request and Yale University Open Data Access).

Eligibility criteria for selecting studies Eligible phase 3 or 4 trials identified according to prespecified criteria (PROSPERO CRD42018048202).

Main outcome measures Association between comorbidity count (identified using medical history or concomitant drug treatment data) and trial attrition (failure for any reason to complete the final trial visit), estimated in logistic regression models and adjusted for age and sex. Estimates were meta-analysed in bayesian linear models, with partial pooling across index conditions and drug classes.

Results In 92 trials across 20 index conditions and 17 drug classes, the mean comorbidity count ranged from 0.3 to 2.7. Neither age nor sex was clearly associated with attrition (odds ratio 1.04, 95% credible interval 0.98 to 1.11; and 0.99, 0.93 to 1.05, respectively). However, comorbidity count was associated with trial attrition (odds ratio per additional comorbidity 1.11, 95% credible interval 1.07 to 1.14). No evidence of non-linearity (assessed via a second order polynomial) was seen in the association between comorbidity count and trial attrition, with minimal variation across drug classes and index conditions. At a trial level, an increase in participant comorbidity count has a minor impact on attrition: for a notional trial with high level of attrition in individuals without comorbidity, doubling the mean comorbidity count from 1 to 2 translates to an increase in trial attrition from 29% to 31%.

Conclusions Increased comorbidity count, irrespective of age and sex, is associated with a modest increased odds of participant attrition. The benefit of increased generalisability of including participants with multimorbidity seems likely to outweigh the disadvantages of increased attrition.

  • clinical trial
  • internal medicine
  • medicine
  • research design

Data availability statement

Data are available in a public, open access repository. Data may be obtained from a third party and are not publicly available. Individual patient level data are available from Clinical Study Data Request and Yale University Open Data Access platforms. Trial level results, model outputs, and analysis code are provided on the project GitHub repository (https://github.com/ChronicDiseaseEpi/como_complete_public).

https://creativecommons.org/licenses/by/4.0/

This is an open access article distributed in accordance with the Creative Commons Attribution 4.0 Unported (CC BY 4.0) license, which permits others to copy, redistribute, remix, transform and build upon this work for any purpose, provided the original work is properly cited, a link to the licence is given, and indication of whether changes were made. See: https://creativecommons.org/licenses/by/4.0/.

https://doi.org/10.1136/bmjmed-2022-000217

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    WHAT IS ALREADY KNOWN ON THIS TOPIC

    • In the general population, many patients have multimorbidity

    • In clinical trials, participants with multimorbidity are under-represented

    • This under-representation might partly be driven by concerns that participants with multimorbidity will find participation challenging, leading to high levels of attrition, imposing additional costs and burdens on trial conduct, and potentially compromising validity without increasing representativeness

    WHAT THIS STUDY ADDS

    • Individuals with multimorbidity are less likely to complete participation in clinical trials, but the effect is modest

    • Men were not evidently less likely than women to complete participation in clinical trials, nor were older people than younger people, but data suggested an association between increasing age and attrition

    HOW THIS STUDY MIGHT AFFECT RESEARCH, PRACTICE, OR POLICY

    • Improving representation of patients with multimorbidity in trials and improving trial validity is feasible, without prohibitive increases in attrition

    Introduction

    Comorbidity occurs in around half of people with any long term condition; it is increasing in prevalence but is substantially less common in participants included in randomised controlled trials.1 2 Where participants with comorbidity are under-represented within trials, the applicability of trials treatment effect estimates are uncertain, particularly for absolute treatment effects.3 Consequently, increased recruitment of participants with comorbidity might be desirable. However, one potential disincentive to enrolling more people with comorbidities is the concern that they might be less able to complete the trial,4 5 leading to increased participant attrition.

    Even when similar across treatment arms, high levels of attrition lead to a reduction of the precision with which treatment effects can be estimated for a given sample size,6 raise concerns about the interpretation of intention to treat estimates7 (as participants who no longer participate are unlikely to follow trial treatment protocols), can make trials less representative (as participants who leave the study could be different from those who complete the study),8 and might cause a loss of confidence among researchers reviewing studies since high attrition could be perceived as a marker of suboptimal trial conduct.

    Although methods to improve the retention of participants have been extensively studied,9–12 we are not aware of any study that has quantified the association between comorbidity and trial attrition. Such estimates would be valuable for informing trial design (by informing sample size calculations) and conduct (by identifying those individuals most likely to withdraw or be lost to follow-up, and devising and testing strategies to improve their retention). In a previously published meta-analysis of individual participant level data (IPD) of 92 standard phase 3 or 4 industry funded trials, we reported that multimorbidity (and hence comorbidity) was present in trials, although at a lower prevalence than found in the community.13 In the present IPD meta-analysis of this same set of trials, we aimed to determine whether comorbidity, age, and sex are associated with attrition among trial participants.

    Methods

    Study design

    We performed a meta-analysis of trial IPD to determine the association between comorbidity, age, and sex on attrition, in two stages. Firstly, for each trial, the association between comorbidity count (the number of other conditions in addition to the index condition defining the trial population) and attrition (defined as failure for any reason to complete final trial visit) was estimated in logistic regression models, adjusting for age and sex. In similar models, we estimated the associations between age and sex and trial attrition. Secondly, the resulting effect estimates were meta-analysed in bayesian linear models. We allowed partial pooling across index conditions and drug classes in order to obtain overall, drug class specific and index condition specific estimates of these associations.

    Data sources and participants

    Available IPD were obtained from phase 3 or 4 trials contained within two trial repositories: the multi-sponsored Clinical Study Data Request repository and the Yale University Open Data Access project. Appropriate trials for inclusion were identified according to prespecified criteria (PROSPERO CRD42018048202).13 Specifically, we included trials for medical conditions that are predominantly managed by drug treatments (frequently over a sustained period).13

    We classified each trial in terms of the index condition based on the stated trial indication as described previously.13 Each trial was also classified in terms of the intervention drug, using the five character WHO Anatomic Therapeutic Chemical (ATC) class.14 For example, the A10BJ (glucagon-like peptide 1 analogues) class includes the drugs A10BJ01 (exenatide) and A10BJ02 (liraglutide).

    In a previous publication,13 we defined comorbidities solely using concomitant drug treatments in order to enable comparison across trial and community settings. The comorbid conditions included cardiovascular disease, chronic pain, arthritis, affective disorders, acid related disorders, asthma or chronic obstructive pulmonary disease, diabetes mellitus, osteoporosis, thyroid disease, thromboembolic disease, inflammatory conditions, benign prostatic hyperplasia, gout, glaucoma, urinary incontinence, erectile dysfunction, psychotic disorders, epilepsy, migraine, parkinsonism, and dementia. For the current analysis, for the 80 trials that did not redact medical history data, we additionally defined the same comorbidities using prespecified codes from the Medical Dictionary for Regulatory Activities. Individuals were defined as having a comorbidity if they met required definitions based on either concomitant drug treatment or medical history. Definitions and code lists are available at the project repository15 (https://github.com/ChronicDiseaseEpi/como_complete_public). To produce a comorbidity count for each trial participant, the number of comorbidities at baseline were summed, excluding the index condition of the respective trials.

    Outcomes

    The outcome of interest was attrition, defined as failure for any reason to complete the final trial visit, including intentional and non-intentional withdrawals. The proportion of attritions was estimated as the number of participants who did not complete as a proportion of all those randomised.

    Representativeness

    Not all sponsors share trial IPD and not all trials are made available to third party researchers. Consequently, to contextualise the IPD trials included in this analysis, we also examined attrition in a wider set of trials registered on the US clinical trials registry (ClinicalTrials.gov) of which the IPD trials are a subset (PROSPERO registration number CRD42018048202).13 We restricted the 2235 trials registered on ClinicalTrials.gov to the 777 registered on or after 2010 since we saw that trials registered before this period (consistent with changes in US Food and Drug Administration requirements for trials registered on or after 2007)16 were less likely to post completion data. Of these, 593 (76.3%) trials had posted data to ClinicalTrials.gov on enrolment, randomisation, and completion, for which we produced summaries of the proportion of participants completing each trial overall and by index condition.

    Statistical analysis

    Summary statistics were calculated for each index condition for the available IPD trials including age (mean and standard deviation), sex (number and %), comorbidity count (mean and standard deviation), and proportion with two or more comorbidities. A violin plot was constructed to illustrate the proportion of attritions in IPD and ClinicalTrials.gov trials.

    Full descriptions of the modelling are provided in the online supplemental appendix and are described briefly below. In logistic regression models, for each trial, attrition was regressed on age (per 15 year increment, which was close to the standard deviation for most trials), sex (male v female (reference)), and comorbidity count (per additional comorbidity). We fitted a range of models with and without terms for comorbidity count, comorbidity count squared, age, sex, treatment arm, and a comorbidity-treatment arm interaction. The effect measure estimates (log-odds ratios) and associated standard errors for each model were then exported from the Yale University Open Data Access and Clinical Study Data Request repository safe havens. Proportions of missing baseline data within trials were very small. Logistic regression models within trial repositories were conducted on complete cases.

    Supplemental material

    The effect measure estimates for the age (adjusted for sex), sex (adjusted for age), and comorbidity (adjusted for age and sex) terms were subsequently meta-analysed separately in bayesian linear regression models. We used bayesian models because these allowed partial pooling across index conditions and drug classes and because they allowed us to obtain credible intervals for estimates at the level of index conditions and drug classes directly from the posterior without a need for post hoc calculations. We performed a range of meta-analyses for each regression coefficient. These meta-analyses were done within a bayesian framework, where the final meta-analysed estimate was a summary of the trial level estimates. This summary is a product of the precision with which the association is estimated for each trial (ie, the inverse of the squared standard error for the relevant coefficient), the variation between trials, the variation between other groups (eg, drug class or condition), and the prior distributions (a vague prior for the overall effect, and weakly informative priors for the variation parameters). Details of the selected priors are available in the online supplemental data file. For the simplest model, only variation between trials was explicitly modelled. For the (progressively) more complex models, the variation between other groups was also modelled: drug class, condition, and both drug class and condition. This modelling allowed estimates to differ for each group, while also allowing sharing of information between the groups (known as partial pooling), which has the effect of improving precision as well as shifting extreme effect estimates towards the overall mean. The variation within groups for trials, conditions, and drug classes was reported as the respective standard deviation.

    Models were fit using the brms package.17 For each model, 4000 samples from the posterior were obtained and summarised as 50%, 80%, and 95% credible intervals. The probability (bayesian P value) that comorbidity count was positively associated with attrition was estimated as the proportion of the posterior distribution of the log-odds ratio, which was above 0. An illustration of models used to assess the association between comorbidity count and attrition is displayed in figure 1.

    Figure 1
    Figure 1

    Overview of use of models for meta-analysis output. Shaded areas=analyses conducted within Clinical Study Data Request (CSDR) and Yale University Open Data Access (YODA) repository safe havens. Variance matrices of the effect estimates were exported to allow maximum flexibility in subsequent meta-analyses, if required. IPD=individual participant level data

    Using the effect estimates obtained from this meta-analysis for the association between comorbidity count and attrition among participants, we then explored the potential impact of comorbidity count at the trial level. Firstly, we constructed a set of notional trials with different plausible mean comorbidity counts (and therefore with different proportions of participants with each comorbidity count) and different risks of attrition among participants with zero comorbidities (which could differ because of trial level factors such as difference in follow-up methods or settings). Next, we applied the effect estimates to participants from these notional trials to estimate the overall percentage of participants who would be expected not to complete the trial visits. This analysis is described in detail in the online supplemental appendix.

    We conducted a sensitivity analysis using wider priors for the variances between trials, between conditions, and between drug classes (details in online supplemental data file). We also conducted a sensitivity analysis within each of the trial repositories where we reanalysed the trials having excluded any participant who had an adverse event of any kind. The model outputs for these trials were not exported but were meta-analysed within the repositories, pooling results across all trials. We fit a frequentist random effects model (which assumes effect estimates for each trial come from a normal distribution), using a restricted maximum likelihood estimator within the metafor package. This model was fit using frequentist software rather than the bayesian software used for the main analysis, because bayesian software was not available within the trial repository. The trial level results, model outputs, and analysis code are provided on the project GitHub repository (https://github.com/ChronicDiseaseEpi/como_complete_public).

    Patient and public involvement

    Patients or the public were not involved in the design, or conduct, or reporting of this study, but will be involved in dissemination plans of this research. Refer to the methods section for further details.

    Results

    Included trials

    A total of 92 IPD trials featured 20 index conditions trialling drugs from 17 ATC drug classes. The index conditions with the most trials were type 2 diabetes mellitus (18 trials), inflammatory bowel disease (10 trials), rheumatoid arthritis (10 trials), and hypertension (nine trials).

    Baseline characteristics

    The age and sex distribution for IPD trials differed by condition (table 1). In trials for atrial fibrillation and dementia, the mean age was over 70 years; in trials for migraine and inflammatory bowel disease, the mean age was under 40 years. Trials ranged from those conducted solely in men (prostate disease, 100% men) to those predominantly conducted among women (migraine, 85.4% women).

    View this table:
    Table 1

    Baseline characteristics of study trials and participants

    For each trial, the comorbidity count was summarised well with a Poisson distribution (figure S1). The mean comorbidity count across index conditions ranged from 0.3 for psoriasis to 2.7 for osteoporosis (table 1). For many trials, a substantial proportion of participants had two or more comorbidities in addition to the index disease, for example, in trials of dementia (56%; n=3 trials), osteoarthritis (54%; n=1 trial), Parkinson’s disease (41%; n=3 trials), and type 2 diabetes (29%; n=20 trials); but few participants had two or more comorbidities in hypertension trials (12%; n=9 trials) or pulmonary fibrosis trials (9%; n=2 trials).

    Trial attrition and age, sex, and comorbidity count

    We saw substantial variation in attrition in the IPD trials both within and between index conditions (table 1 and figure 2).

    Figure 2
    Figure 2

    Plots of the proportion of attritions for 593 clinical trials registered on ClinicalTrials.gov (CTG) and 92 trials with individual participant level data (IPD) available. Violin plots represent the summary estimates for CTG and IPD trials. Horizontal bars=median and interquartile ranges; dots=proportion of attrition for individual trials

    No clear association was seen between increasing age and attrition (table 2); the odds ratio for attrition per 15 year increment in age was 1.04 (95% credible interval 0.98 to 1.11), although the probability of a positive association (bayesian P value) was 89% (table 2). We saw no clear association between sex and attrition (odds ratio 0.99, 95% credible interval 0.93 to 1.05; table 2).

    View this table:
    Table 2

    Odds ratios for association between trial attrition and age, sex, and comorbidity count for different models

    By contrast, comorbidity count was associated with attrition independently of age and sex (odds ratio per additional comorbidity 1.11, 95% credible interval 1.07 to 1.14). We saw no evidence of departure from linearity (estimated via the addition of a squared term to the model) for this association (1.01-fold difference, 95% credible interval 1.00 to 1.03, in odds ratio for increment in comorbidity count of 0 to 1 v odds ratio for increment in comorbidity count from 1 to 2). Compared with individuals with zero comorbidities, the odds ratios are 1.11 (95% credible interval 1.07 to 1.14), 1.23 (1.14 to 1.30), and 1.37 (1.23 to 1.48) in those individuals with one, two, and three comorbidities respectively. Assuming a risk of attrition in individuals with no comorbidities (referred to as underlying risk) of 10%, these odds ratios translate to risks of trial attrition of 11.0% (95% credible interval 10.6 to 11.2%), 12.0% (11.3 to 12.6%) and 13.2% (12.0 to 14.1%) in those individuals with one, two, and three comorbidities, respectively. The results were similar in the simplest models, where all trial results were pooled, as well as in more complex models where trial results were partially pooled within drug classes and index conditions (table 2).

    For the association between comorbidity count and attrition, we observed roughly twice as much variation between trials as between index conditions and between drug classes (standard deviation (on log-odds scale) 0.10, 0.05, and 0.04 respectively; table 2).

    Table 3 illustrates the potential impact of these findings for the association between comorbidity count and attrition using a notional set of trials, under different assumptions about the trial mean comorbidity count and underlying risks of attrition. Except where the underlying risk was very high, the difference across trials with different mean comorbidity counts was modest. For trials with an underlying risk of 49%, the proportion of participants expected not to complete was 50% for a trial with a mean comorbidity count of 0.5, and 53% for a trial with a mean comorbidity count of 2.

    View this table:
    Table 3

    Risk of attrition for trial by mean trial comorbidity count, according to risk of attrition in those individuals with no comorbidities

    Variation in associations between trial attrition across index conditions

    For the associations between attrition and age, sex, and comorbidity count, we saw little variation across index conditions (figure 3, online supplemental table S1). For age, the strongest association was for pulmonary fibrosis (odds ratio 1.15, 95% credible interval 0.96 to 1.54) and the weakest association was for chronic idiopathic urticaria (0.98, 0.74 to 1.14). For sex, the strongest association was for inflammatory bowel disease (1.08, 0.93 to 1.30) and the weakest association was for psoriasis (1.00, 0.76 to 1.30); for comorbidity count, the strongest association was for rheumatoid arthritis (1.17, 1.08 to 1.29) and the weakest association was for osteoarthritis (1.07, 0.95 to 1.17).

    Figure 3
    Figure 3

    Forest plots showing mean odds ratio of atrial attrition (with 50%, 80%, and 95% credible intervals) by index condition and overall result from pooled model, according to age, sex, and comorbidity count at baseline assessment. Vertical line=reference line (ie, no effect, odds ratio of 1); 50% and 80% credible intervals are shown to indicate that the probability of a given estimate is not uniform across the 95% interval

    Variation in associations between trial attrition across drug classes

    The findings for variations in the associations between trial attrition and age, sex, and comorbidity count by drug classes were similar to those for index conditions (figure 4, online supplemental table S2). For age, the strongest association was for protein kinase inhibitors (odds ratio 1.11, 95% credible interval 0.96 to 1.41) and the weakest association was for dopamine agonists (1.00, 0.82 to 1.13). For sex, the strongest association was for glucagon-like peptide 1 analogues (1.08, 0.93 to 1.28) and the weakest association was for anticholinesterases (0.89, 0.73 to 1.05). For comorbidity count, the strongest association was for interleukin inhibitors (1.17, 1.08 to 1.30) and the weakest association was for oxicams (1.07, 0.93 to 1.17).

    Figure 4
    Figure 4

    Forest plots showing mean odds ratio of atrial attrition (with 50%, 80%, and 95% credible intervals) by Anatomical Therapeutic Chemical (ATC) drug class and overall result from pooled model, according to age, sex, and comorbidity count at baseline assessment. Vertical line=reference line (ie, no effect, odds ratio of 1); 50% and 80% credible intervals are shown to indicate that the probability of a given estimate is not uniform across the 95% interval

    Sensitivity analyses

    Sensitivity analyses using wider priors for the variance parameters gave the same results to two decimal places for the variances between trials, between index conditions, and between drug class (online supplemental table S3).

    In the frequentist meta-analysis conducted within the Yale University Open Data Access and Clinical Study Data Request repositories where participants with any adverse event were excluded, the associations between comorbidity count and trial attrition were similar to the results from the main analysis (odds ratios 1.08 (95% credible interval 1.03 to 1.13) and 1.13 (1.05 to 1.21) for Yale University Open Data Access and Clinical Study Data Request, respectively).

    Discussion

    Principal findings

    In more than 90 trials including more than 90 000 participants across 20 index conditions and 17 drug classes, we found that comorbidity was associated with trial attrition. Neither age nor sex was associated with attrition. The association for comorbidity was moderate, with a 1.1-fold increase in risk per each additional comorbidity after adjusting for age and sex. These findings were consistent across a wide range of index conditions and drug classes.

    Strengths and weaknesses of the study

    The strengths of this study include the fact that we analysed IPD for a large number of trials across a range of index conditions and drug classes. However, the study had several limitations. Firstly, the trials were not designed to study comorbidity, and as such our definitions were based on data collected for other reasons (and not redacted for privacy reasons when the IPD was shared): the medical and concomitant drug treatment history collected at baseline. For this reason, we defined comorbidities broadly (eg, asthma and chronic obstructive pulmonary disease were combined into one category) and are likely to have missed some diagnoses. Similarly, patients with comorbidities are likely to take many drug treatments (ie, polypharmacy) across multiple drug classes, or indeed be prescribed one drug for multiple indications. Defining comorbidity counts from drug treatments might have biased associations between comorbidity count and attrition, most likely towards the null because of non-differential misclassification. Although we did not find any evidence for non-linearity in the association between comorbidity count and attrition, we would also caution against extrapolating the findings to comorbidity counts above 3, owing to the very few individuals in the trial with comorbidity counts at this level.

    Secondly, although we have showed a clear association between increasing comorbidity count and trial attrition, we cannot be certain that the increased burden of comorbidity was the cause of attrition. An alternative explanation could be unmeasured confounding by other factors that might affect likelihood of trial completion (eg, education, ethnic origin, and socioeconomic status), and we cannot comment on potential mediators of the observed association. Thirdly, we chose to explore non-linearity using a second order polynomial (ie, linear and squared terms for comorbidity count) because this was simpler to implement than other approaches such as splines or fractional polynomials, since we were analysing data across multiple repositories rather than on a single platform. Had we been able to use these more flexible approaches, we might have detected non-linearity not apparent with the current method.

    Fourthly, this set of trials was not representative. Trials investigating cancer, infections, psychiatric disorders, and developmental disorders were excluded from the initial search for IPD trials, and among included conditions, we only obtained IPD if the sponsors participated in the data sharing repositories of Clinical Study Data Request or Yale University Open Data Access trials. Moreover, not all trials for sponsors that make data available in this platform were available at the time of our analysis, which meant that the included trials were fairly typical industry funded trials of novel drugs. Nonetheless, we did find that attrition was similarly distributed in IPD trials compared with a wider set of trials included in the US trials register (clinicaltrials.gov). Moreover, the associations within the IPD trials were very consistent across index conditions and ATC drug classes.

    Strengths and weaknesses in relation to other studies

    Identifying strategies to improve trial retention is an important research priority,18 and several randomised clinical trials have investigated different mechanisms to improve retention.12 Participant level factors have been found to be associated with attrition in isolated studies, and include patient preference,19 educational status,20 poor physical health,21 male sex,22 and older age.23 However, we are not aware of any study that has estimated the strength of the association between individual participant characteristics and attrition across a range of trials. Our study therefore adds to the literature by showing that comorbidity count is associated with attrition, but that (chronological) age and sex do not.

    Meaning of the study

    We have previously shown that community populations have about double the comorbidity counts of participants in clinical trials with the same index condition.13 In this study, we demonstrated that doubling the comorbidity count in the trial populations was generally associated with an expected absolute increase in attrition of less than 5%, assuming plausible levels of mean trial comorbidity counts and plausible levels of attrition for individuals without comorbidity. If people with a given index condition and comorbidity count in clinical trials and routine clinical practice are similar (an assumption which requires further study), more participants could be included in trials with comorbidity without substantially increasing costs, or compromising the actual or perceived validity of the trial treatment effect estimates.

    Unanswered questions and future research

    Improving the representativeness of trial populations first requires a more granular understanding of the factors affecting the retention of participants with higher levels of comorbidity. Among trial participants who did not experience an adverse event, we demonstrated a similar association between comorbidity count and risk of trial attrition as observed in the main analysis, suggesting that attrition in participants with comorbidity is not solely due to an increased risk of adverse events. The mechanisms might alternatively include increased physiological, psychological, or social difficulties in managing the burden of trial participation19 24; however, whether attrition is related to intentional (an active decision to withdraw or deliberate non-attendance) or non-intentional withdrawal (where declines in physical or cognitive health preclude further participation) is not clear.

    Two specific, potentially measurable indices of physiological wellbeing might be associated with attrition and warrant further exploration. Increasing biological age (eg, measured by DNA methylation)25 is associated with the accrual of comorbidity and predicts a variety of morbidity and mortality outcomes.26 Accounting for biological (rather than chronological) age could attenuate the association observed between comorbidity count and attrition; however, DNA methylation is not currently routinely measured or reported. Frailty is a marker of functional status that positively correlated with increasing (chronological and biological) age and comorbidity count, but is strongly and independently associated with mortality.27 Availability of validated tools to assess frailty (such as Fried28 or Rockwood29 indices) allow simple recording of these data. Although some trials (especially in disease processes common in older patients, such as dementia) do record participant frailty, the lack of uniform availability of these data from existing trial IPD prevents detailed assessment of the association between frailty and trial attrition. Assessing the impact of frailty on attrition is an important avenue for further study, and particularly whether trial design could be adapted to improve inclusiveness of frailer participants. Specifically, it would be useful to examine whether associations differ according to trial characteristics that might improve completeness of follow-up, such as the use of wearables30 or collection of routine data31 32 to measure trial endpoints.

    Involvement of representative patient and public involvement and engagement (PPIE) groups can help trialists gain a much richer appreciation of the factors driving attrition in trials. With detailed PPIE support at the point of inception, trialists might be better able to design and conduct trials that are likely to be realistic and acceptable to participants with comorbidities. Ultimately, this input could improve recruitment and retention, and drive improvement in outcomes.33 Our findings suggest that including people with multimorbidity in such groups is important.

    Wider discussions about improving access to clinical trials for under-represented groups (eg, relating to ethnic origin34 35 and socioeconomic status) have taken place.36 Clinicians might be less likely to approach patients with comorbidities for inclusion owing to concerns that these individuals might be unable to complete the trial.37 Importantly, people from more socioeconomically disadvantaged backgrounds could be at higher risk of comorbidity,38 39 and particular comorbidities might be more prevalent among people from different ancestries.39 40 Consideration should be taken on optimising the inclusion of participants with comorbidities in trials alongside wider considerations of improving access for under-represented groups.

    In conclusion, comorbidity count, but not age and sex, is associated with an increased odds of attrition from trials. Although this effect seems modest, it will still involve added costs and time to clinical trials that researchers and funders need to consider. For levels of multimorbidity and attrition typically seen in standard industry funded trials, increasing levels of multimorbidity might be feasible without causing large falls in participant completion.

    Data availability statement

    Data are available in a public, open access repository. Data may be obtained from a third party and are not publicly available. Individual patient level data are available from Clinical Study Data Request and Yale University Open Data Access platforms. Trial level results, model outputs, and analysis code are provided on the project GitHub repository (https://github.com/ChronicDiseaseEpi/como_complete_public).

    Ethics approval

    Not applicable.

    Acknowledgments

    This study, carried out under Yale University Open Data Access project number 2017-1746, used data obtained from the Yale University Open Data Access Project, which has an agreement with Janssen Research and Development. The interpretation and reporting of research using this data are solely the responsibility of the authors and does not necessarily represent the official views of the Yale University Open Data Access Project or Janssen Research and Development. This study was also carried out under ClinicalStudyDataRequest.com project number 1732, used data from the ClinicalStudyDataRequest.com repository, who provided data from Boehringer-Ingelheim, GSK, Lilly, Roche, Takeda, and Sanofi. The interpretation and reporting of research using these data are solely the responsibility of the authors and does not necessarily represent the official views of ClinicalStudyDataRequest.com or Boehringer-Ingelheim, GSK, Lilly, Roche, Takeda, or Sanofi.

    References

      1. Van Spall HGC,
      2. Toren A,
      3. Kiss A, et al
      . Eligibility criteria of randomized controlled trials published in high-impact general medical journals: a systematic sampling review. JAMA 2007;297:123340.doi:10.1001/jama.297.11.1233pmid:http://www.ncbi.nlm.nih.gov/pubmed/17374817
      OpenUrlCrossRefPubMedWeb of Science
      1. Fortin M,
      2. Dionne J,
      3. Pinho G, et al
      . Randomized controlled trials: do they have external validity for patients with multiple comorbidities? Ann Fam Med 2006;4:1048.doi:10.1370/afm.516pmid:http://www.ncbi.nlm.nih.gov/pubmed/16569712
      OpenUrlAbstract/FREE Full Text
      1. Boyd CM,
      2. Darer J,
      3. Boult C, et al
      . Clinical practice guidelines and quality of care for older patients with multiple comorbid diseases: implications for pay for performance. JAMA 2005;294:71624.doi:10.1001/jama.294.6.716pmid:http://www.ncbi.nlm.nih.gov/pubmed/16091574
      OpenUrlCrossRefPubMedWeb of Science
      1. Joseph G,
      2. Dohan D
      . Diversity of participants in clinical trials in an academic medical center: the role of the 'Good Study Patient?'. Cancer 2009;115:60815.doi:10.1002/cncr.24028pmid:http://www.ncbi.nlm.nih.gov/pubmed/19127544
      OpenUrlCrossRefPubMed
      1. Weiss CO,
      2. Varadhan R,
      3. Puhan MA, et al
      . Multimorbidity and evidence generation. J Gen Intern Med 2014;29:65360.doi:10.1007/s11606-013-2660-5
      OpenUrlCrossRefPubMed
      1. Nüesch E,
      2. Trelle S,
      3. Reichenbach S, et al
      . The effects of excluding patients from the analysis in randomised controlled trials: meta-epidemiological study. BMJ 2009;339:b3244683.doi:10.1136/bmj.b3244pmid:http://www.ncbi.nlm.nih.gov/pubmed/19736281
      OpenUrlAbstract/FREE Full Text
      1. Tierney JF,
      2. Stewart LA
      . Investigating patient exclusion bias in meta-analysis. Int J Epidemiol 2005;34:7987.doi:10.1093/ije/dyh300pmid:http://www.ncbi.nlm.nih.gov/pubmed/15561753
      OpenUrlCrossRefPubMedWeb of Science
      1. Dumville JC,
      2. Torgerson DJ,
      3. Hewitt CE
      . Reporting attrition in randomised controlled trials. BMJ 2006;332:96971.doi:10.1136/bmj.332.7547.969
      OpenUrlFREE Full Text
      1. Loudon K,
      2. Treweek S,
      3. Sullivan F, et al
      . The PRECIS-2 tool: designing trials that are fit for purpose. BMJ 2015;350:h2147.doi:10.1136/bmj.h2147pmid:http://www.ncbi.nlm.nih.gov/pubmed/25956159
      OpenUrlFREE Full Text
      1. Gillies MC,
      2. Hunyor AP,
      3. Arnold JJ, et al
      . Effect of ranibizumab and aflibercept on Best-Corrected visual acuity in Treat-and-Extend for neovascular age-related macular degeneration: a randomized clinical trial. JAMA Ophthalmol 2019;137:3729.doi:10.1001/jamaophthalmol.2018.6776pmid:http://www.ncbi.nlm.nih.gov/pubmed/30676617
      OpenUrlCrossRefPubMed
      1. Skea ZC,
      2. Newlands R,
      3. Gillies K
      . Exploring non-retention in clinical trials: a meta-ethnographic synthesis of studies reporting participant reasons for drop out. BMJ Open 2019;9:e021959.doi:10.1136/bmjopen-2018-021959pmid:http://www.ncbi.nlm.nih.gov/pubmed/31164359
      OpenUrlCrossRefPubMed
      1. Gillies K,
      2. Kearney A,
      3. Keenan C, et al
      . Strategies to improve retention in randomised trials. Cochrane Database Syst Rev 2021;3:MR000032.doi:10.1002/14651858.MR000032.pub3pmid:http://www.ncbi.nlm.nih.gov/pubmed/33675536
      OpenUrlPubMed
      1. Hanlon P,
      2. Hannigan L,
      3. Rodriguez-Perez J, et al
      . Representation of people with comorbidity and multimorbidity in clinical trials of novel drug therapies: an individual-level participant data analysis. BMC Med 2019;17.doi:10.1186/s12916-019-1427-1
      1. World Health Organization (WHO)
      . Anatomic therapeutic chemical. Geneva, 2019. Available: https://www.whocc.no/atc_ddd_index/
      1. Lees JS
      . Project GitHub Repository, 2022. Available: https://github.com/ChronicDiseaseEpi/como_complete_public
      1. Food and Drugs Administration
      . Section 801 of the food and drug administration amendments act of 2007, 2007: 90422.
      1. Bürkner PC
      . brms: an R package for Bayesian multilevel models using Stan. J Stat Softw 2017;80.
      1. Brunsdon D,
      2. Biesty L,
      3. Brocklehurst P, et al
      . What are the most important unanswered research questions in trial retention? A James Lind alliance priority setting partnership: the priority II (prioritising retention in randomised trials) study. Trials 2019;20:593.doi:10.1186/s13063-019-3687-7pmid:http://www.ncbi.nlm.nih.gov/pubmed/31615577
      OpenUrlPubMed
      1. Hui D,
      2. Glitza I,
      3. Chisholm G, et al
      . Attrition rates, reasons, and predictive factors in supportive care and palliative oncology clinical trials. Cancer 2013;119:1098105.doi:10.1002/cncr.27854
      OpenUrlCrossRefPubMedWeb of Science
      1. Dickinson HO,
      2. Rapp M,
      3. Arnaud C, et al
      . Predictors of drop-out in a multi-centre longitudinal study of participation and quality of life of children with cerebral palsy. BMC Res Notes 2012;5:300.doi:10.1186/1756-0500-5-300pmid:http://www.ncbi.nlm.nih.gov/pubmed/22704327
      OpenUrlCrossRefPubMed
      1. Applebaum AJ,
      2. Lichtenthal WG,
      3. Pessin HA, et al
      . Factors associated with attrition from a randomized controlled trial of meaning-centered group psychotherapy for patients with advanced cancer. Psychooncology 2012;21:1195204.doi:10.1002/pon.2013pmid:http://www.ncbi.nlm.nih.gov/pubmed/21751295
      OpenUrlCrossRefPubMed
      1. Warner ET,
      2. Glasgow RE,
      3. Emmons KM, et al
      . Recruitment and retention of participants in a pragmatic randomized intervention trial at three community health clinics: results and lessons learned. BMC Public Health 2013;13:192.doi:10.1186/1471-2458-13-192pmid:http://www.ncbi.nlm.nih.gov/pubmed/23496916
      OpenUrlCrossRefPubMed
      1. Weissman J,
      2. Flint A,
      3. Meyers B, et al
      . Factors associated with non-completion in a double-blind randomized controlled trial of olanzapine plus sertraline versus olanzapine plus placebo for psychotic depression. Psychiatry Res 2012;197:2216.doi:10.1016/j.psychres.2012.02.015
      OpenUrlPubMed
      1. McCambridge J,
      2. Kalaitzaki E,
      3. White IR, et al
      . Impact of length or relevance of questionnaires on attrition in online trials: randomized controlled trial. J Med Internet Res 2011;13:e96.doi:10.2196/jmir.1733pmid:http://www.ncbi.nlm.nih.gov/pubmed/22100793
      OpenUrlCrossRefPubMed
      1. Horvath S
      . Dna methylation age of human tissues and cell types. Genome Biol 2013;14:R115.doi:10.1186/gb-2013-14-10-r115
      1. Levine ME,
      2. Lu AT,
      3. Quach A, et al
      . An epigenetic biomarker of aging for lifespan and healthspan. Aging 2018;10:57391.doi:10.18632/aging.101414pmid:http://www.ncbi.nlm.nih.gov/pubmed/29676998
      OpenUrlPubMed
      1. Hanlon P,
      2. Nicholl BI,
      3. Jani BD, et al
      . Frailty and pre-frailty in middle-aged and older adults and its association with multimorbidity and mortality: a prospective analysis of 493 737 UK Biobank participants. Lancet Public Health 2018;3:e32332.doi:10.1016/S2468-2667(18)30091-4
      OpenUrlPubMed
      1. Fried LP,
      2. Tangen CM,
      3. Walston J, et al
      . Frailty in older adults: evidence for a phenotype. J Gerontol A Biol Sci Med Sci 2001;56:M14657.doi:10.1093/gerona/56.3.M146pmid:http://www.ncbi.nlm.nih.gov/pubmed/11253156
      OpenUrlCrossRefPubMedWeb of Science
      1. Rockwood K,
      2. Song X,
      3. MacKnight C, et al
      . A global clinical measure of fitness and frailty in elderly people. CMAJ 2005;173:48995.doi:10.1503/cmaj.050051pmid:http://www.ncbi.nlm.nih.gov/pubmed/16129869
      OpenUrlAbstract/FREE Full Text
      1. Berryhill S,
      2. Morton CJ,
      3. Dean A, et al
      . Effect of wearables on sleep in healthy individuals: a randomized crossover trial and validation study. J Clin Sleep Med 2020;16:77583.doi:10.5664/jcsm.8356pmid:http://www.ncbi.nlm.nih.gov/pubmed/32043961
      OpenUrlPubMed
      1. Hemkens LG,
      2. Saccilotto R,
      3. Reyes SL, et al
      . Personalized prescription feedback using routinely collected data to reduce antibiotic use in primary care: a randomized clinical trial. JAMA Intern Med 2017;177:17683.doi:10.1001/jamainternmed.2016.8040pmid:http://www.ncbi.nlm.nih.gov/pubmed/28027333
      OpenUrlPubMed
      1. Mc Cord KA,
      2. Al-Shahi Salman R,
      3. Treweek S, et al
      . Routinely collected data for randomized trials: promises, barriers, and implications. Trials 2018;19:29.doi:10.1186/s13063-017-2394-5pmid:http://www.ncbi.nlm.nih.gov/pubmed/29325575
      OpenUrlCrossRefPubMed
      1. Prost A,
      2. Colbourn T,
      3. Seward N, et al
      . Women’s groups practising participatory learning and action to improve maternal and newborn health in low-resource settings: a systematic review and meta-analysis. The Lancet 2013;381:173646.doi:10.1016/S0140-6736(13)60685-6
      OpenUrlPubMed
      1. Duma N,
      2. Vera Aguilera J,
      3. Paludo J, et al
      . Representation of minorities and women in oncology clinical trials: review of the past 14 years. J Oncol Pract 2018;14:e110.doi:10.1200/JOP.2017.025288pmid:http://www.ncbi.nlm.nih.gov/pubmed/29099678
      OpenUrlPubMed
      1. Redwood S,
      2. Gill PS
      . Under-representation of minority ethnic groups in research--call for action. Br J Gen Pract 2013;63:3423.doi:10.3399/bjgp13X668456pmid:http://www.ncbi.nlm.nih.gov/pubmed/23834862
      OpenUrlFREE Full Text
      1. Bonevski B,
      2. Randell M,
      3. Paul C, et al
      . Reaching the hard-to-reach: a systematic review of strategies for improving health and medical research with socially disadvantaged groups. BMC Med Res Methodol 2014;14:42.doi:10.1186/1471-2288-14-42pmid:http://www.ncbi.nlm.nih.gov/pubmed/24669751
      OpenUrlCrossRefPubMed
      1. Foster JM,
      2. Sawyer SM,
      3. Smith L, et al
      . Barriers and facilitators to patient recruitment to a cluster randomized controlled trial in primary care: lessons for future trials. BMC Med Res Methodol 2015;15:18.doi:10.1186/s12874-015-0012-3pmid:http://www.ncbi.nlm.nih.gov/pubmed/25887970
      OpenUrlCrossRefPubMed
      1. Nowakowska M,
      2. Zghebi SS,
      3. Ashcroft DM, et al
      . The comorbidity burden of type 2 diabetes mellitus: patterns, clusters and predictions from a large English primary care cohort. BMC Med 2019;17:145.doi:10.1186/s12916-019-1373-ypmid:http://www.ncbi.nlm.nih.gov/pubmed/31345214
      OpenUrlPubMed
      1. Vart P,
      2. Powe NR,
      3. McCulloch CE, et al
      . National trends in the prevalence of chronic kidney disease among racial/ethnic and socioeconomic status groups, 1988-2016. JAMA Netw Open 2020;3:e207932.doi:10.1001/jamanetworkopen.2020.7932pmid:http://www.ncbi.nlm.nih.gov/pubmed/32672828
      OpenUrlPubMed
      1. Lee H,
      2. Shin SH,
      3. Gu S, et al
      . Racial differences in comorbidity profile among patients with chronic obstructive pulmonary disease. BMC Med 2018;16:178.doi:10.1186/s12916-018-1159-7pmid:http://www.ncbi.nlm.nih.gov/pubmed/30285854
      OpenUrlPubMed

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    Footnotes

    • Twitter @jennifer_s_lees

    • Contributors DAM conceived the idea for the article. PH and EWB identified suitable trials for inclusion. DAM, SHW, RST, FSM, BG, NJW, and SD critically advised on statistical analysis and presentation. JSL and DAM carried out the analysis. JSL and DAM created tables and figures. JSL wrote the first draft of the manuscript. KG critically advised on presentation and interpretation. JSL and DAM are guarantors for the overall content. All authors reviewed and approved the final submitted manuscript. The corresponding author attests that all listed authors meet authorship criteria and that no others meeting the criteria have been omitted. Transparency: The lead author (the guarantor) affirms that the manuscript is an honest, accurate, and transparent account of the study being reported; that no important aspects of the study have been omitted; and that any discrepancies from the study as planned (and, if relevant, registered) have been explained.

    • Funding JSL is funded by a Chief Scientist Office (Scotland) Postdoctoral Lectureship Award (PCL/20/10). DAM is funded via an Intermediate Clinical Fellowship and Beit Fellowship from the Wellcome Trust, who also supported other costs related to this project such as data access costs and database licences (201492/Z/16/Z). PH is funded through a clinical research training fellowship from the Medical Research Council (grant reference MR/S021949/1). The funders had no role in considering the study design or in the collection, analysis, interpretation of data, writing of the report, or decision to submit the article for publication.

    • Competing interests All authors have completed the ICMJE uniform disclosure form at www.icmje.org/disclosure-of-interest/ and declare: support from the Chief Scientist Office (Scotland), Wellcome Trust, and UK Medical Research Council for the submitted work; outside the submitted work, JSL has received personal honorariums from Bristol Myers Squibb, Pfizer, and Astra Zeneca.

    • Provenance and peer review Not commissioned; externally peer reviewed.

    • Supplemental material This content has been supplied by the author(s). It has not been vetted by BMJ Publishing Group Limited (BMJ) and may not have been peer-reviewed. Any opinions or recommendations discussed are solely those of the author(s) and are not endorsed by BMJ. BMJ disclaims all liability and responsibility arising from any reliance placed on the content. Where the content includes any translated material, BMJ does not warrant the accuracy and reliability of the translations (including but not limited to local regulations, clinical guidelines, terminology, drug names and drug dosages), and is not responsible for any error and/or omissions arising from translation and adaptation or otherwise.