CONTINUOUS MISSING PARTICIPANT DATA IN RANDOMIZED CONTROLLED TRIALS

Zhang, Yuqing

11 1900

Background and Objectives: Missing participant data are likely to bias the results of randomized control trials (RCTs) when the reason for missingness is associated with status on the outcome of interest. Unlike dichotomous MPD in RCTs, which have been thoroughly investigated, knowledge regarding continuous MPD in RCTs is much more limited. Our objectives were 1) using an adapted checklist, to assess the reporting quality of simulation studies comparing methods to deal with continuous MPD; 2) identify optimal methods proposed by biostatisticians and tested in simulations studies for continuous MPD in RCTs; 3) evaluate how authors report MPD, and how they plan and conduct analyses to deal with MPD in RCTs. Methods: We conducted two systematic surveys. The first identified methods papers published till 2015 January that compared statistical approaches to deal with continuous MPD in RCTs using at least one simulation. In this sample, we considered both the quality of reporting and the results. The second survey identified a representative sample of individual RCTs published in 2014 in core journals reporting the results of at least one continuous variable addressing a patient-important outcome. Results and conclusion: Our survey identified important limitations in reporting quality of simulation studies that compared statistical approaches to deal with continuous MPD, particularly in the reporting of simulation procedures. Only one of 60 studies reported the random number generator used and none reported starting seeds or failures during simulation. Less then half reported software used to perform simulation (41.7%) or analysis (48.3%), and only 4 (5%) reported justification of number of simulations. When facing continuous MPD in RCTs, results of simulation studies demonstrate that trialists seeking optimal approaches may choose robust regression or mixed models and avoid using last observation caring forward. Continuous MPD frequently occurs in RCTs and the extent is typically substantial (median greater than 10%). Methods sections in trial reports typically do not provide adequate detail on how they dealt with MPD in their primary analysis. Among methods actually implemented to deal with MPD, most authors use only available data, thus excluding MPD from the analysis. Seldom do investigators apply statistical approaches to impute or taking into account of MPD nor conduct sensitivity analysis to address the impact of it. A comprehensive knowledge synthesis summarizing current available statistical approaches and its relative merits, as well as the current used methods in RCTs provide clear implications on how the practise of using methods to handle continuous MPD should shift in individual RCTs. Trialists should use mixed models and robust regressions and avoid using last observation caring forward method. / Thesis / Doctor of Philosophy (PhD)

Missing participant data

Randomized controlled trials

Continuous outcome

Issues Related to Determining Optimal Management of Patients in Receipt of Disability Benefits

Ebrahim, Shanil

10 1900

<p>Approximately 4.2 million Canadian adults suffer from a physical or psychological disability, of whom up to 30% suffer from depression. Those receiving disability benefits versus those not receiving benefits may be at greater risk of unsatisfactory outcomes because their circumstances or psychological status may interfere with successful implementation of standard therapies. This thesis addresses the effectiveness of therapies for depression in patients receiving disability benefits, using an individual patient data meta-analysis of all published randomized controlled trials evaluating Cognitive Behavioural Therapy and a secondary analysis of an administrative database from a large, private, Canadian insurer. Additionally, this thesis addresses an important methodological issue: assessing the impact of missing participant data for continuous outcomes in systematic reviews. Missing participant data may bias results of individual trials or systematic reviews of individual trials if participants with missing data have different expected outcomes from those with available data. No methods have been proposed for investigating the extent to which missing participant data for continuous outcomes might bias the results of systematic reviews, and this dissertation addresses that gap.</p> / Doctor of Philosophy (PhD)

Disability Benefits

Optimal Management

Psychotherapy

Depression

Missing Participant Data

Lost to Follow-Up

Mental and Social Health

Rehabilitation and Therapy

Mental and Social Health