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Open Access

Protocol

Statistical and health economic analysis plan for a randomized controlled trial of surgical fixation with K-wires versus plaster casting in the treatment of dorsally displaced distal radius fractures: DRAFFT2



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Abstract

Aims

Describe a statistical and economic analysis plan for the Distal Radius Acute Fracture Fixation Trial 2 (DRAFFT2) randomized controlled trial.

Methods

DRAFFT2 is a multicentre, parallel, two-arm randomized controlled trial. It compares surgical fixation with K-wires versus plaster cast in adult patients who have sustained a dorsally displaced fracture of the distal radius. The primary outcome measure is the Patient-Rated Wrist Evaluation (PRWE, a validated assessment of wrist function and pain) at 12 months post-randomization. Secondary outcomes are measured at three, six, and 12 months after randomization and include the PWRE, EuroQoL EQ-5D-5L index and EQ-VAS (visual analogue scale), complication rate, and cost-effectiveness of the treatment.

Results

This paper describes the full details of the planned methods of analysis and descriptive statistics. The DRAFFT2 study protocol has been published previously.

Conclusion

The planned analysis strategy described records our intent to conduct statistical and within-trial cost-utility analyses.

Cite this article: Bone Joint Open 2020;1-6:245–252.

Introduction

Distal radius fracture is one of the most common reasons for emergency department attendance.1 ‘Manipulation’ of the bone fragments is usually recommended if there is displacement of a dorsally angulated fracture. The manipulation is intended to restore the normal anatomy, i.e. to move the bone fragments back into their normal alignment. After manipulation, the bone fragments may fall back out of normal alignment hence clinicians will apply support to the bone fragments while they heals. This trial will compare two techniques for holding the position of the bone fragments – plaster casting and surgical fixation using Kirschner wires (K-wires).

Plaster casting involves the application of a plaster cast from below the elbow to just above the metacarpal-phalangeal joints. The cast is moulded over the skin to hold the bone fragments in place. It is simple, inexpensive and has few complications but is susceptible to re-displacement especially when the swelling starts to settle a few days after the surgery. Surgical fixation with K-wires involves inserting smooth metal wires with a sharp point through the skin across the fracture site to hold the bone fragments directly in place while they heal. However, there are small risks of complications (e.g. infection and damage to nerves or blood vessels around the wrist) and K-wire fixation costs more and takes longer to apply than plaster cast.

Methods

Trial design

The DRAFFT2 trial is a randomized, multicentre, superiority trial with two parallel arms performing comparison between surgical fixation with K-wires and plaster casting in patients who have sustained a dorsally displaced fracture of the distal radius. Eligible patients are randomized in a 1:1 ratio to the two treatment groups. Randomization is stratified by centre, intra-articular extension of the fracture and age of the patient ( ≥ 50 or < 50 years of age). The trial is not blinded. It is registered in the International Standard Randomized Controlled Trials database (ISRCTN11980540). Further details of the trial design and procedures, including full eligibility criteria, are found in the DRAFFT2 study protocol.2

Outcomes

Primary outcome

The primary outcome measure is the Patient Reported Wrist Evaluation3 (PRWE) 12 months post-randomization. PRWE4 is a validated, self-reported 15-item questionnaire, that rates wrist function using a range of questions in two (equally weighted) sections concerning the patient’s experience of pain and disability. The score is out of 100 (best score = 0 and worst score = 100).

Secondary outcomes

Secondary outcome measures are: PRWE three and six months post-randomization, PRWE area under the curve (AUC), EuroQol five-dimension five-level (EQ-5D-5L) index at three, six, and 12 months, EQ-5D-5L index area under the curve (AUC), EuroQol visual analogue scale (EQ-VAS) at three, six, and 12 months, EQ-VAS AUC, complications and cost-effectiveness. To calculate EQ-5D-5L index scores we will use the Crosswalk Index Value Calculator mapping the 5 L descriptive system data onto the 3 L dataset using the mapping function5 as, at the time of writing, there is still debate about the appropriate value set for the 5 L. The data collection is summarized in Table I.

Table I.

Summary of outcomes and data collection schedule.

Time point Data collection
Baseline PRWE and EQ-5D-5L pre-injury and contemporary, routine radiographs of the wrist
6 weeks Complication records, routine radiographs of the wrist, operative record
3 months PRWE, EQ-5D-5L, record of complications/rehabilitation or other interventions and healthcare resource use questionnaire
6 months PRWE, EQ-5D-5L, record of complications/rehabilitation or other interventions and healthcare resource use questionnaire
12 months PRWE, EQ-5D-5L, record of complications/rehabilitation or other interventions and healthcare resource use questionnaire
  1. PRWE, Patient Reported Wrist Evaluation; EQ-5D-5L, EuroQol five-dimension five-level.

Sample sizest

In the DRAFFT trial,6 which recruited from the same patient population, the standard deviation (SD) of the PRWE at 12 months was 16. However, other studies of patients with fractures of the distal radius showed a SD for the PRWE which ranged between 16 and 23 points.7 Therefore, we chose a conservative estimate of the SD of 18 points.

A six-point mean difference between groups equates to a standardized effect size of 0.33, assuming a SD of 18 points. We believe the target difference (six points) would be important on both an individual patient and a population level, and could lead to a change in clinical practice in the UK.

The total number of patients required to obtain 90% power to detect a six-point difference between groups for the PRWE will be 380; i.e. 190 patients in each treatment group. With an allowance for a 20% loss to follow-up, we would plan to recruit 476 patients in total.

Statistical analysis

General analysis principles

Final analysis will occur after the final has patient has been followed up for the final time, the data has been cleaning and locked. All outcomes will be assessed at this time.

The significance level used will be two-sided 5% level with corresponding 95% confidence intervals (CIs) calculated whenever possible. Any analyses not pre-specified will be labelled as “exploratory”.

Two analysis populations will be used in the statistical analysis. Intention-to-treat (ITT): inclusion of all available randomized participants who will be analyzed in the groups to which they were randomly allocated irrespective of non-compliance. If a participant has observed data on any of the time points, they will be included in the analysis. Per protocol (PP): eligible participants who received the treatment they were randomized to. Participants did not receive their allocated intervention will not be included in this population. This population will be finalized prior to the conducting the analyses of outcomes.

Details on data checks and reliability can be found in the Supplementary Material (online supplementary appendix 1).

Supplemental Material

No formal interim analysis is planned for this study.

Descriptive analysis

The flow of participants through each stage of the trial, including the number of individuals screened, eligible, randomized to each arm, receiving allocated treatment, and included in the primary analysis will be summarized using a CONSORT flowchart (Figure 1). Reasons for ineligibility, loss to follow-up and exclusion from the primary analysis will be summarized.

Fig. 1 
            CONSORT flowchart.

Fig. 1

CONSORT flowchart.

Baseline characteristics are reported by treatment group, including the stratification factors and important prognostic, demographic and clinical covariates.

Numbers (with percentages) for binary and categorical variables and means (and standard deviations), or medians (with lower and upper quartiles) for continuous variables will be presented; there will be no tests of statistical significance nor CIs for differences between randomized groups on baseline variables.

Compliance

The compliance with treatment will be reported by treatment group. Non-compliance is defined as not receiving the treatment the participant was randomized to for any reason, for example, surgeon’s choice or a need to perform an open reduction internal fixation.

Analysis of the primary outcome

The primary outcome measure, PRWE score at 12 months post-randomisation, will be modelled using a mixed effects model. This model will account for centre (random effect), baseline (post-injury) values, other time points, articular extension of the fracture (intra and extra), and age ( ≥ 50 or < 50 years of age) (fixed effects). Treatment by timepoint interactions will also be included to allow time-specific treatment effects to be calculated including the primary outcome time point. This is a different approach from that initially suggested in the DRAFFT2 protocol2 (linear regression with cluster-robust option to control for site), but is in keeping the principle outlined there (allowing for adjustment for clustering by site as well as the other stratification variables as fixed effects).

The main comparison will be performed on an intention-to-treat basis and results presented with adjusted mean difference and the corresponding 95% CI.

Analysis of the secondary outcomes

The same mixed effects model, intention-to-treat basis and results presentation as the primary outcome will also be used to assess the secondary PRWE three and six months outcomes. The same modelling approach will be used for the EQ-5D-5L index and EQ-VAS secondary outcomes at three, six, and 12 months. The distribution of the five domains will be reported in tabular and graphical form by treatment.

The secondary outcome of complications, including those needing further surgery at one-year post-randomisation, will be analyzed as follows. Further surgery, including those in the cast arm who receive any surgery, will be analyzed by calculating the odds ratio and 95% CI using logistic regression. Other generic, non-surgical, complications: complex regional pain syndrome, deep vein thrombosis/pulmonary embolus (pooled together) will be analyzed using the same method. Other individual complications will be summarized by treatment arm, but not analyzed, and reported in tabular form.

An AUC analysis will be performed for the PRWE and EQ-5D (both EQ-5D-5L index and EQ-VAS). The estimates obtained in the mixed model for each time point used in the analysis will be used to calculate the AUC. These adjusted estimates rather than raw, unadjusted, estimates results in less bias estimates of the AUC when missing data is present.8

Missing data

Where possible the reasons for missing data will be ascertained. Withdrawals/loss to follow-up together with reasons will be reported by intervention arm. Any deaths (and their causes) will be reported separately.

The mechanism for missing items required for definition of outcomes will be investigated. Missing data will be reported and summarized by treatment arm. An ITT analysis strategy to assess assumptions about departures from randomization policies and handling of missing data will be carried out to examine the robustness of the primary results. Varying scores of the PRWE (for instance 40th, 50th, 60th percentiles) will be imputed by treatment group for data missing and these “complete” datasets will be reanalysed, using the same model used in the primary analysis. Their adjusted mean differences and 95% CIs plotted.

While there is a mechanism to deal with missing data in the PRWE (a missing item may be with the mean score of the subscale for that individual), there is no limit to how many items can be replaced in a subscale. We will explore the way missing values in the PRWE subscales are treated effect the outcome if there is substantial number of responses with individual items missing as opposed to the all of the respective PWRE subscale.

For the economic analysis, multiple imputation analysis will be used to impute missing cost and health utilities. This will be done using chained regression equations predicting missing values from the observed covariates (observed responses of participant) and creating sets of multiple datasets containing possible values for missing observations.9 Pooled estimates were then calculated using Rubin’s rules10 to obtain an overall mean estimate of the costs or quality-adjusted life years (QALYs).

Sensitivity analyses

Sensitivity analyses of the primary outcome and secondary PRWE outcomes only will be carried out on a per-protocol basis to examine robustness of conclusions to assumptions about departures from randomization.

A second sensitivity analysis will use a three level model with participant within surgeon within centre to examine the potential surgeon (random) effects. This model will formally incorporate terms that allow for possible heterogeneity in responses for patients due to the recruiting centre and the surgeon, and the fixed effects of the treatment groups, and stratification factors.

Pre-specified subgroup analysis

Subgroup analyses of the two clinical stratifying variables (age and intra-articular extension) on the primary outcome are planned. These analyses will use a model to formally test the interaction between each stratifying variable and the treatment factor; appropriate 95% CIs will be reported for the interaction effects in addition to p-values. These analyses will be labelled as exploratory and results from them will be interpreted and reported as such; in line with recommendations for subgroup analysis.11 The results will be presented in a forest plot.

Additional analysis

Bayesian re-analyses of the main analysis of the primary outcome (PRWE) at 12 months are planned. Further details can be found in Supplementary Material (online supplementary appendix 1).

Health economic analysis

A within-trial cost-effectiveness analysis (CEA) will be undertaken using the multiple imputed trial dataset to assess the cost effectiveness of K-wires versus plaster cast from the UK NHS and Personal Social Services perspective in the base case (or primary) analysis.12

Measurement of resource use

Resource use for the surgical fixation will be collected during the trial from information gathered via the trial case report forms (CRFs) by the research team, while resource use due to the wrist fracture during follow-up will be collected via trial questionnaires given to participants at three, ssix, and 12 months after randomization. The questionnaires will capture information such as: the number and duration of admissions to inpatient wards (classified as orthopaedics (wrist/arm), orthopaedics (any bones), rehabilitation unit); number of diagnostic tests; use of outpatient services (classified as orthopaedics, physiotherapy, pathology and radiology); and frequency of use of community-based health and social care services and social care services. Patients will also be asked to record direct medical costs (e.g. medications), direct nonmedical costs (e.g. aids and adaptations, help with housework/childcare and travel) and indirect costs (i.e. lost productivity) attributable to patient’s health state.

Valuation of health outcomes

Unless a validated and accepted UK valuation set for EQ-5D-5L is available at the time of analysis, the current NICE recommended method of computing the utility values will be followed: the 5 L descriptive system data will be mapped onto the 3 L valuation set via the mapping function5 and valued using the UK EQ-5D time trade-off tariff.13 Utilities will be set to zero from the date of death for deceased participants.14 QALYs will be calculated as the area under the baseline regression adjusted utility curve of EQ-5D utility scores from baseline, three, six, and 12 months' data using the trapezoidal rule.15

Valuation of costs

It is not feasible to collect unit cost data for every operative consumable used in the fixation of fractures of the distal radius from all the trauma centres participating in the trial so only the ones that would differ in terms of utilization rate between the treatment arms will be obtained (Table II). The operative costs for both plaster cast and K-wire fixation consumables will be obtained from the latest NHS Supply Chain catalogue.16 Participants in both treatment groups will receive surgery from surgeons of different grades (i.e. consultant, staff grade etc.). Unit costs for each grade of surgeons will be sourced using the latest version of the Personal Social Services Research Unit’s (PSSRU) unit costs of Health and Social Care.17 The average operating time will be obtained from the participant CRF. Other staff that might participate in the surgery include anaesthetists, technicians/operating department personnel, nurses and radiographers, but the number and type of these staff is expected to be the same in both trial arms and for that reason, this information is not being collected. The unit cost of the initial distal radius surgery fracture fixation will be assessed using NHS reference costs and the HRG code (HT45Z) for “Minor Hand Procedures for Trauma” and assigned to both trial groups. Day case costs or overnight admission costs will also be obtained from the latest NHS Reference Cost.18 If a patient reported a length of stay longer than the trim point specified in the NHS Reference Cost, the inpatient excess day cost from the NHS Reference Cost will be used where applicable.

Table II.

Unit costs of health resource items.

Resource item Unit Source
Fixation surgery
Full cast each NHS Supply Chain Catalogue16
Non-sterile gloves each NHS Supply Chain Catalogue16
Surface wipes each NHS Supply Chain Catalogue16
Black bag each NHS Supply Chain Catalogue16
Yellow bag each NHS Supply Chain Catalogue16
Polythene bag for extras each NHS Supply Chain Catalogue16
Inco pad each NHS Supply Chain Catalogue16
Fixation surgery: K-wire only
K-wire each NHS Supply Chain Catalogue16
Reinforced gown XL each NHS Supply Chain Catalogue16
Surgical visor masks each NHS Supply Chain Catalogue16
Theatre masks each NHS Supply Chain Catalogue16
Biogel gloves each NHS Supply Chain Catalogue16
Image intensifier cover each NHS Supply Chain Catalogue16
Laceration pack each DRAFFT19
Sterilisation of drill each DRAFFT19
Sterile dressing gauze each NHS Supply Chain Catalogue16
Initial hospital stay
Intensive care unit per admission NHS Reference Costs18
Acute trauma ward per day NHS Reference Costs18
Rehabilitation ward per admission NHS Reference Costs18
Treatment after index surgery per day NHS Reference Costs18
Inpatient care
Orthopaedics: wrist/arm per day NHS Reference Costs18
Orthopaedics: other bones per day NHS Reference Costs18
Other non-surgery per day NHS Reference Costs18
Day case per day NHS Reference Costs18
Rehabilitation Unit per session NHS Reference Costs18
Outpatient care
Orthopaedics/Fracture clinic per consultation NHS Reference Costs18
Physiotherapist (NHS) per session PSSRU20
Physiotherapist (private) per hour The Physiotherapy Centre21
Pathology (blood tests) per hour NHS Reference Costs18
Radiology per test NHS Reference Costs18
Emergency department: wrist per attendance NHS Reference Costs18
Emergency department: others per attendance NHS Reference Costs18
Calls to NHS 111 per call Financial Times22
Primary and community care
General Practitioner (surgery visit) per minute PSSRU23
General Practitioner (home visit) per minute PSSRU24
General Practitioner (phone contact) per minute PSSRU20
Practice nurse (surgery visit) per hour PSSRU23
Practice nurse (home visit) per hour PSSRU24
Practice nurse (phone contact) per hour PSSRU24
District nurse (surgery visit) per hour PSSRU20
District nurse (home visit) per hour PSSRU24
Physiotherapist (surgery visit) per hour PSSRU25
Physiotherapist (home visit) per hour PSSRU25
Occupational therapist (surgery visit) per hour PSSRU23
Occupational therapist (home visit) per visit PSSRU24
Medications BNF26, NHS Electronic Drug Tariff27
Aids and adaptations
Wrist support (e.g. brace/splint) each NHS Supply Chain Catalogue16
Grab rail each PSSRU23
Dressing aids each NHS Supply Chain Catalogue16
Long handled aids (e.g. shoe horn) each NHS Supply Chain Catalogue16
Bathing aids each NHS Supply Chain Catalogue16
Kitchen aids (e.g. jar openers) each NHS Supply Chain Catalogue16
Personal social services
Frozen meals-on-wheels per meal Meals on Wheels (LBM)28
Hot meals-on-wheels per meal PSSRU25
Laundry services per load North Yorkshire County Council29
Social worker per hour PSSRU23
Care worker/ help at home per hour PSSRU23
Lost productivity
Median wage per week Office for National Statistics30
  1. BNF: British National Formulary, PSSRU: Personal Social Service Research Unit

Unit cost of direct medical costs that are not part of the trial such as the inpatient care, outpatient care and community care will be sourced from the latest available NHS Reference Cost and PSSRU unit cost. The unit cost of medication related to surgical fixation will be sourced using the latest available British National Formulary26 or the NHS Electronic Drug Tariff.27

Collection of unit cost for direct nonmedical cost items such as help with housework/childcare and travel incurred by participant’s carer will be not be relevant because the cost per patient will be obtained from the questionnaire. Unit cost of aids and adaptations will be obtained from the latest NHS Supply Chain Catalogue;16 the median wage that will be used in the computation of participant’s lost productivity will be obtained from the Office for National Statistics.30

Cost of health resource use per participant will be calculated by multiplying the frequency of health resource utilization reported by the proxy with the unit cost of each resource item and adding on direct nonmedical cost, which will be obtained directly from the questionnaire. The base currency of all costs will be the year in which the data analysis was performed and in UK pounds. The medication cost taken over the study period will be calculated using the cost per dose for each product and the mean quantity taken per day during the reported number of days. All medications are assumed to be in tablets unless stated otherwise. Cost of lost productivity will be calculated using the human capital approach: the daily median wage will be multiplied by the number of days the participant had to take time off work due to participant’s injury.

Data analysis

Resource use items will be summarized by randomized group and follow-up period and differences between groups will be analyzed using t-tests for continuous variables and Pearson chi-squared (χ2) test for categorical variables. Means and standard deviations for values of each cost category will be estimated by treatment allocation and follow-up period. Differences in mean costs will assessed using t-tests and the bootstrap 95% CI will be calculated based on 1,000 replications. There will be no discounting for costs and QALYs because the time horizon is one year.

The base case analysis will adopt an intention-to-treat (“as-randomized” with imputation of missing data) perspective and an incremental cost-effectiveness ratio (ICER) will be calculated as the difference in mean costs divided by the difference in mean QALYs between the treatments. The National Institute for Health and Care Excellence31 cost effectiveness threshold of £20,000 to £30,000 per additional QALY will be used to determine the cost effectiveness of K-wire versus plaster cast after facture of the distal radius. The more effective treatment will be considered cost-effective if it has an ICER below the £20,000 per QALY threshold.

The net monetary benefit of K-wire versus plaster cast will be calculated across different cost-effectiveness thresholds. The economic evaluation will be repeated for subgroups defined by the two clinical stratifying variables (age and intra-articular extension). One-way sensitivity analyses will be performed to explore the effects of extending the study perspective (i.e. societal perspective) and assessing the impact of missing data on the ICERs (i.e. using complete case analysis). Non-parametric bootstrapping will also be performed to assess the uncertainty on the ICERs and varying levels of willingness-to-pay for an additional QALY and presented in cost-effectiveness acceptability curves.

Findings of this economic evaluation will be reported in accordance with the Consolidated Health Economic Evaluation Reporting Standards (CHEERS) statement for the reporting of health economic evaluations.32

Statistical packages

All analysis will be carried out using STATA33 or R34 statistical software. The package and version number used for analysis will be recorded and reported.

Discussion

This paper provides details of the planned statistical and health economic analyses for the DRAFFT2 trial35 to reduce the risks of reporting bias. Any changes or deviations from the analysis outlined in this paper will be described and justified fully in the final report.


Correspondence should be sent to Alexander Gert Ooms. E-mail:

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Author contributions

A. G. Ooms: Developed the statistical analysis plan, Wrote the manuscript, Reviewed and approved the final manuscript.

M. E. Png: Developed the health economic analysis plan, Wrote the manuscript, Reviewed and approved the final manuscript.

J. Cook: Developed the statistical analysis plan, Wrote the manuscript, Obtained grant funding, Reviewed and approved the final manuscript.

M. Dritsaki: Obtained grant funding, Reviewed and approved the final manuscript.

H. Dakin: Obtained grant funding, Reviewed and approved the final manuscript.

M. Costa: Obtained grant funding, Reviewed and approved the final manuscript.

Funding statement

This project was funded by the UK NIHR HTA Programme (project number 15/27/01) and was supported by NIHR Oxford Biomedical Research Centre. Although none of the authors has received or will receive benefits for personal or professional use from a commercial party related directly or indirectly to the subject of this article, benefits have been or will be received but will be directed solely to a research fund, foundation, educational institution, or other non- profit organization with which one or more of the authors are associated.

Acknowledgements

The trial is supported by the NIHR Oxford Biomedical Research Centre. We would like to thank the Trial Steering Committee: Michael Whitehouse (chair), Grey Giddins, and Penelope Harris and Data and Safety Monitoring Committee: Lee Shepstone (Chair), Jean Craig, and Simon Donnell for overseeing the study.

Ethical review statement

The National Research Ethic Committee approved this study on 6 October 2016 (16/SC/0462).

Supplementary material

Details on data checks, reliability and additional analysis

© 2020 Author(s) et al. This is an open-access article distributed under the terms of the Creative Commons Attributions licence (CC-BY-NC-ND), which permits unrestricted use, distribution, and reproduction in any medium, but not for commercial gain, provided the original author and source are credited.