An adaptable implementation package targeting evidence-based indicators in primary care: A pragmatic cluster-randomised evaluation

Authors: Thomas A. Willis ^aff001; Michelle Collinson ^aff002; Liz Glidewell ^aff003; Amanda J. Farrin ^aff002; Michael Holland ^aff002; David Meads ^aff001; Claire Hulme ^aff004; Duncan Petty ^aff005; Sarah Alderson ^aff001; Suzanne Hartley ^aff002; Armando Vargas-Palacios ^aff001; Paul Carder ^aff006; Stella Johnson ^aff006; Robbie Foy ^aff001;
Authors place of work: Leeds Institute of Health Sciences, University of Leeds, Leeds, United Kingdom ^aff001; Clinical Trials Research Unit, Leeds Institute of Clinical Trials Research, University of Leeds, Leeds, United Kingdom ^aff002; Department of Health Sciences, Hull York Medical School, University of York, York, United Kingdom ^aff003; College of Medicine and Health, University of Exeter, Exeter, United Kingdom ^aff004; School of Pharmacy and Medical Sciences, University of Bradford, Bradford, United Kingdom ^aff005; West Yorkshire Research and Development, NHS Bradford Districts CCG, Bradford, United Kingdom ^aff006
Published in the journal: An adaptable implementation package targeting evidence-based indicators in primary care: A pragmatic cluster-randomised evaluation. PLoS Med 17(2): e32767. doi:10.1371/journal.pmed.1003045
Category: Research Article
doi: https://doi.org/10.1371/journal.pmed.1003045

Summary

Background

In primary care, multiple priorities and system pressures make closing the gap between evidence and practice challenging. Most implementation studies focus on single conditions, limiting generalisability. We compared an adaptable implementation package against an implementation control and assessed effects on adherence to four different evidence-based quality indicators.

Methods and findings

We undertook two parallel, pragmatic cluster-randomised trials using balanced incomplete block designs in general practices in West Yorkshire, England. We used ‘opt-out’ recruitment, and we randomly assigned practices that did not opt out to an implementation package targeting either diabetes control or risky prescribing (Trial 1); or blood pressure (BP) control or anticoagulation in atrial fibrillation (AF) (Trial 2). Within trials, each arm acted as the implementation control comparison for the other targeted indicator. For example, practices assigned to the diabetes control package acted as the comparison for practices assigned to the risky prescribing package. The implementation package embedded behaviour change techniques within audit and feedback, educational outreach, and computerised support, with content tailored to each indicator. Respective patient-level primary endpoints at 11 months comprised the following: achievement of all recommended levels of haemoglobin A1c (HbA1c), BP, and cholesterol; risky prescribing levels; achievement of recommended BP; and anticoagulation prescribing. Between February and March 2015, we recruited 144 general practices collectively serving over 1 million patients. We stratified computer-generated randomisation by area, list size, and pre-intervention outcome achievement. In April 2015, we randomised 80 practices to Trial 1 (40 per arm) and 64 to Trial 2 (32 per arm). Practices and trial personnel were not blind to allocation. Two practices were lost to follow-up but provided some outcome data. We analysed the intention-to-treat (ITT) population, adjusted for potential confounders at patient level (sex, age) and practice level (list size, locality, pre-intervention achievement against primary outcomes, total quality scores, and levels of patient co-morbidity), and analysed cost-effectiveness. The implementation package reduced risky prescribing (odds ratio [OR] 0.82; 97.5% confidence interval [CI] 0.67–0.99, p = 0.017) with an incremental cost-effectiveness ratio of £1,359 per quality-adjusted life year (QALY), but there was insufficient evidence of effect on other primary endpoints (diabetes control OR 1.03, 97.5% CI 0.89–1.18, p = 0.693; BP control OR 1.05, 97.5% CI 0.96–1.16, p = 0.215; anticoagulation prescribing OR 0.90, 97.5% CI 0.75–1.09, p = 0.214). No statistically significant effects were observed in any secondary outcome except for reduced co-prescription of aspirin and clopidogrel without gastro-protection in patients aged 65 and over (adjusted OR 0.62; 97.5% CI 0.39–0.99; p = 0.021). Main study limitations concern our inability to make any inferences about the relative effects of individual intervention components, given the multifaceted nature of the implementation package, and that the composite endpoint for diabetes control may have been too challenging to achieve.

Conclusions

In this study, we observed that a multifaceted implementation package was clinically and cost-effective for targeting prescribing behaviours within the control of clinicians but not for more complex behaviours that also required patient engagement.

Trial registration

The study is registered with the ISRCTN registry (ISRCTN91989345).

Keywords:

HbA1c – Cost-effectiveness analysis – blood pressure – chronic kidney disease – Primary care – NSAIDs – atrial fibrillation – diabetes mellitus

Introduction

Clinical research can only benefit patient and population health if findings are incorporated into routine care. There are delays and inappropriate variations in uptake of effective treatments and withdrawal of less effective or harmful treatments [1]. This translation gap is important to policy makers, healthcare systems, and research funders because it limits the health, social, and economic impacts of clinical research [2].

United Kingdom primary care presents particular implementation challenges: growing demand, increasing complexity of care, and limited workforce capacity, against a background of frequent organisational reconfigurations [3,4]. We identified 107 clinical guidelines produced by the National Institute for Health and Care Excellence (NICE) relevant to UK general practice [5]. Many implementation studies focus on a single clinical condition or problem (e.g., diabetes, antibiotic stewardship), limiting generalisability, as it is uncertain whether an implementation strategy developed for one condition will work for another. It is impracticable and inefficient to devise an implementation strategy for every new guideline. Furthermore, the clinical significance of behaviours often targeted in implementation studies, such as receipt of processes of care or investigations, is doubtful [6]. Implementation strategies are required, capable of integration into primary care systems and adaptable to different clinical priorities.

We earlier derived evidence-based indicators that could be measured using routinely collected data [5]. We found marked variations in indicator achievement and scope for improvement in a sample of 89 general practices [7]. We subsequently focused our efforts on four ‘high impact’ indicators that would benefit population health if implemented more consistently: achievement of recommended treatment targets for all of haemoglobin A1c (HbA1c), blood pressure (BP), and cholesterol in type 2 diabetes [8]; avoidance of risky prescribing of nonsteroidal anti-inflammatory drugs (NSAIDs) and anti-platelet drugs [9]; achievement of recommended BP levels in patients at high risk of cardiovascular events [10]; and anticoagulant prescribing for stroke prevention in atrial fibrillation (AF) [11]. We drew upon systematic reviews of implementation strategies [6,12–14], theory-guided interviews with primary care staff [15], and workshops with health professionals and patients to develop a multifaceted implementation package [16]. We compared the effects of the adaptable implementation package against implementation control on adherence to four different evidence-based high impact indicators.

Methods

Study design and participants

We conducted two parallel, cluster-randomised trials using balanced incomplete block designs. In implementation trials, there may be positive attention or negative demotivation effects from participant knowledge of allocation to an intervention or control group, respectively. Balanced incomplete block designs aim to balance any such nonspecific effects across trial arms, as each arm receives an intervention, thereby increasing confidence that any difference in outcomes is attributable to the intervention [17]. The design is incomplete, as each arm receives only one of the interventions. General practices providing National Health Service (NHS) care were the unit of allocation, as the intervention was delivered at the practice level. We maximised pragmatism in trial design and execution to ensure ‘real-world’ relevance [18].

Practices were recruited from West Yorkshire, England, which covers a diverse population of 2.2 million residents, albeit with deprivation levels above the national average [19]. Around 300 general practices were then organised within 10 clinical commissioning groups (CCGs).

Eligible general practices used SystmOne, the computerised clinical system used by approximately two thirds of West Yorkshire practices (The Phoenix Partnership, http://www.tpp-uk.com). We excluded 31 practices that had contributed to earlier intervention development work. We invited practices via recorded post and email, with reminders at two weeks. The UK National Research Ethics Service granted ethical approval (14/SC/1393). This permitted use of an opt-out approach: all eligible practices were included, unless actively declined within four weeks of invitation. The study protocol has previously been published [20]. The study is registered with the ISRCTN registry (ISRCTN91989345). This study is reported as per the CONSORT guideline for cluster-randomised trials (S1 CONSORT checklist).

Randomisation and masking

The trial statistician performed the two-stage randomisation using a bespoke computer-generated minimisation programme implemented in R, software version 2.15.2 (R Foundation for Statistical Computing, Vienna, Austria) (incorporating a random element). First, practices were stratified by CCG and list size, and randomised to Trial 1 (implementation packages targeting either diabetes control or risky prescribing), Trial 2 (BP control or anticoagulation in AF), or no intervention (80:64:34). As recruitment exceeded expectations, we included a ‘no intervention’ arm to allow us to evaluate any nonspecific effects of research participation (this paper presents comparisons within Trials 1 and 2; analysis of the no intervention group will be reported elsewhere). Secondly, within each trial we stratified practices by CCG, list size, and pre-intervention adherence to the two relevant targeted indicators and randomised them 1:1 to individual trial arms (Fig 1). Within each trial, we assumed that any clinical effects of either implementation package would be independent of one another; each intervention arm therefore acted as the control arm for the other intervention arm in the same trial. For example, practices assigned to the diabetes control package acted as the implementation control comparison for practices assigned to the risky prescribing package. Practices from one CCG (29 practices) involved in a concurrent initiative targeting one of our study priorities, anticoagulation in AF, were excluded from Trial 2. Practices and trial personnel were not blind to allocation.

Fig. 1. Trial profile.
^aSafe haven practices are for those patients who have demonstrated violent tendencies, who have been removed from usual general practice, or for ex-offenders. ^bThe flow diagram presents the whole randomisation process, but this paper reports the planned comparisons within Trials 1 and 2. The no intervention arm is shaded to indicate that it was not included in the analyses described here; analysis of this group will be reported elsewhere. ^cOne practice in the risky prescribing arm merged with a non-ASPIRE practice in advance of the fourth feedback report. However, as they received the first three feedback reports, some outcome data are available, and they are included in the final analyses. ^dOne practice in the BP control arm closed in advance of the third feedback report. However, as they received the first two feedback reports, some outcome data are available and they are included in the final analyses. As an example, for the diabetes control practices: there were 14,522 patients acting as the intervention group for the diabetes control implementation package and 18,131 patients acting as the control group for the risky prescribing implementation package. A&F follow-up: delivery of audit and feedback reports during the intervention period; AF, atrial fibrillation; BP, blood pressure; RP, risky prescribing.

General practice and trial personnel involved in intervention delivery and trial statisticians responsible for analysis were, of necessity, aware of allocation assignment. Data collection for all endpoints was masked to allocation.

Procedures

The implementation package (detailed elsewhere [16]) embedded behaviour change techniques within typical primary care interventions: audit and feedback, educational outreach, and computerised support. Implementation package content, specifically the clinical content and embedded behaviour change techniques, was adapted for each of the four targeted indicators and delivered to practices May 2015 to March 2016.

Audit and feedback aimed to give comparative feedback on achievement, inform and prompt recall of clinical goals, highlight consequences of changing or not changing practice, suggest strategies for change, and encourage goal setting and reflection on progress towards goals. Quarterly electronic and paper practice–specific reports presented achievement ranked by practice and compared over time for relevant trial indicators in graphical and numerical forms, using remotely gathered, individualised practice data. Reports also contained brief, evidence-based clinical messages; responses to common queries; and action-planning templates. Practices received computerised search tools to identify relevant patients for review. We encouraged practices to use the feedback reports as supporting materials for professional appraisal and revalidation.

Educational outreach aimed to enhance feedback reports by facilitating individual and group reflection, discussing barriers to action, sharing models of good practice, enhancing motivation, and action planning. We trained pharmacists over two days to deliver 30-minute sessions, designed to fit with existing practice meetings and offered to all staff involved in patient and practice management. We identified a key clinical contact to support practice engagement. We offered a second, follow-up session to review progress and refine action plans, as well as two days of pharmacist support for patient identification and review.

Prompts and reminders reinforced clinical messages and indicator adherence. Computerised prompts for risky prescribing were offered to practices and had to be accepted before they became active on their system. If accepted, they were triggered during consultations and repeat prescribing through an algorithm for patient age, diagnosis, drug, and duration. A one-click justification (ignore, or add or stop medication) was required before users could proceed. Other targeted indicators had existing prompts on practice computer systems, usually to support the Quality Outcomes Framework (QOF), a performance management system whereby general practices are remunerated according to achievement of targets reflecting quality of care [21]. We provided laminated reminders to convey key clinical information (e.g., management pathways) for BP control, anticoagulation for AF, and risky prescribing. We also developed checklists to facilitate shared decision-making with patients for managing BP and diabetes, but we could not make them available in a satisfactory format within the study time lines [16].

We deliberately aligned intervention delivery with the QOF year to fit with existing practice schedules. We assumed that any actions prompted by the implementation package would occur within this period.

Outcomes

Anonymised patient-level outcome data were obtained remotely from general practices from SystmOne. We planned to measure all outcomes at 12 months post-randomisation. However, a one-month delay in randomisation effectively meant that we were only able to assess outcomes at 11 rather than 12 months.

The primary outcomes for each intervention arm comprised the following:

Trial 1

Proportion of patients with type 2 diabetes achieving all three treatment targets:
- BP below 140/80 mmHg (or 130/80 mmHg if kidney, eye, or cerebrovascular damage);
- HbA1c value below or equal to 59 mmol/mol;
- cholesterol level below or equal to 5.0 mmol/L.
Proportion of patients meeting at least one of nine indicators of high-risk NSAID and anti-platelet prescribing:
- prescription of a traditional oral NSAID or low-dose aspirin in patients with a history of peptic ulceration without co-prescription of gastro-protection;
- traditional oral NSAID in patients aged 75 years or over without co-prescription of gastro-protection;
- traditional oral NSAID and aspirin in patients aged 65 years or over without co-prescription of gastro-protection;
- aspirin and clopidogrel in patients aged 65 years or over without co-prescription of gastro-protection;
- warfarin and traditional oral NSAID;
- warfarin and low-dose aspirin or clopidogrel without co-prescription of gastro-protection;
- oral NSAID in patients with heart failure;
- oral NSAID in patients prescribed both a diuretic and an angiotensin-converting-enzyme inhibitor (ACE-I) or angiotensin receptor blocker (ARB);
- oral NSAID in patients with chronic kidney disease (CKD).

Trial 2

Proportion of patients achieving the lowest appropriate BP target:
- under 140/90 mmHg if aged under 80 years with hypertension, coronary heart disease, peripheral arterial disease, a history of stroke or transient ischemic attack, or a 10-year cardiovascular disease risk of 20% or higher;
- under 150/90 mmHg if aged 80 years and over with hypertension;
- under 140/80 mmHg if aged under 80 years with diabetes, under 130/80 mmHg if complications of diabetes or aged under 80 years with CKD and proteinuria.
Combined proportion of men with AF and a congestive heart failure, hypertension, age ≥75, diabetes, stroke, vascular disease, age between 65 and 74, and female sex (CHA₂DS₂-VASc) score of 1 and women with a CHA₂DS₂-VASc score of 2 or above prescribed anticoagulation therapy.

Secondary outcomes (S1–S4 Tables) included individual indicators contributing to composite primary outcomes, processes of care, and continuous intermediate clinical outcomes (last recorded BP, HbA1c, cholesterol). We assessed QOF indicators relevant to implementation packages (diabetes control, BP control, and anticoagulation for AF) to examine any effects on existing routine indicators. We assessed QOF indicators not directly targeted by the implementation packages to assess any unintended wider impacts. These included coronary heart disease and asthma as example long-term physical conditions, mental health (long-term nonphysical condition), and smoking (health promotion).

We obtained practice characteristic data from publicly available sources (Health Education England, Health and Social Care Information Centre): practice list size (number of registered patients); number of general practitioner (GP) partners and salaried GPs; practice training status; practice level Index of Multiple Deprivation (IMD); ethnic profile of practice register; achievement of QOF indicators (2014–2015); patient satisfaction (proportion who would recommend the practice to others); patient-rated practice accessibility (proportion able to speak with GP or nurse within 48 hours of approach); and practice prescribing costs. Patient characteristics (age, sex, comorbidity [number of QOF disease registers on which the patient appeared]) and outcome data were extracted from SystmOne by the local primary care commissioning support unit.

We monitored intervention delivery and fidelity via standardised report forms completed by outreach facilitators following each visit. We recorded reasons for declining visits. We monitored which practices accepted the invitation to join indicator-specific SystmOne organisational groups to access patient searches and any related computerised prompts.

Sample size

Median effect sizes on processes and outcomes of care for a range of guideline implementation studies are around 4%–9% [6]. Given our enhanced interventions and targeting of indicators with scope for improvement [12], we judged an absolute difference of 15% for outcomes related to diabetes, BP control, and anticoagulation for AF as realistic and clinically relevant. Baseline achievement rates in risky prescribing were considerably higher and, considering a potential ceiling effect, a 5% decrease was realistic and clinically relevant.

We aimed to recruit 144 practices: 80 in Trial 1 (diabetes and risky prescribing) and 64 in Trial 2 (BP control and AF), giving 90% power at 2.5% significance (adjusting for two comparisons per trial) to detect the specified effect sizes, allowing for 10% attrition. The mean cluster size (number of patients per practice by indicator), coefficient of variation, intra-cluster correlation coefficient (ICC), and control group achievement rates were estimated from previously collected data [7,20] (S5 Table).

Statistical analysis

Analyses, conducted in SAS software version 9.4 (SAS Institute Inc., Cary, NC) according to the prespecified statistical analysis plan (S1 statistical analysis plan), were based on intention-to-treat (ITT), with two-sided significance testing at the 2.5% level to preserve an overall 5% Type I error rate per trial. We analysed primary outcomes using two-level binary logistic regression models, with patients (level 1) nested within randomised practices (level 2). We analysed binary secondary outcomes for individual indicators within the composite primary outcomes, and recorded processes of care using similar multilevel logistic models. We analysed continuous intermediate clinical outcomes using two-level linear models. All analyses adjusted for patient-level (sex, age) and practice-level covariates (baseline practice list size, CCG, pre-intervention achievement against primary outcomes, total QOF score 2014–2015 [covering clinical and management domains], proportion of patients with 0–3 comorbidities). Sensitivity analyses were conducted when model assumptions were violated. Data completeness for these analyses depended on the completeness of SystmOne medical records and could not be assessed within the trial data set. Missing data in a patient’s record could have led to their incorrect inclusion or exclusion from the denominator of a particular quality indicator or resulted in the patient being incorrectly classified as achieving that indicator. For the primary and secondary analyses, we assumed that data were missing at random. Imputation was not performed for any outcome variables. Complete case analyses were performed for the continuous clinical outcomes. No adjustment for multiple comparisons was made in the secondary endpoint analyses.

Cost-effectiveness

We conducted economic evaluations of three implementation packages using a decision-analytic modelling approach. Given resource constraints, we were unable to evaluate the anticoagulation for AF package. Implementation package costs included researcher and healthcare professional time and materials in delivery and resulting from change in practice. Trial estimates of effectiveness were inputted into decision models, with the main output being cost (UK £, 2017 prices) per incremental quality-adjusted life year (QALY) over a lifetime horizon from the perspective of the UK health and social care provider. Where possible we used models, parameters, and assumptions that had informed the original NICE guidance. For diabetes control, we used the UK Prospective Diabetes Study Outcomes Model (UKPDS-OM) version 2 [22]. For BP control, we recreated and adapted the model used to inform NICE guidance [23], identifying additional parameters through targeted searches and risk engines such as QRISK. We based the risky prescribing model on a previous model of NSAID prescribing used in a NICE osteoarthritis guideline (CG177). We adapted this model and populated it using results reported for three of the most commonly prescribed NSAIDs in the UK (diclofenac, naproxen, and ibuprofen) and aspirin. We created an additional model based on that used to inform the NICE Acute Kidney Injury guideline (CG169), covering NSAID prescribing in patients with CKD. Individual indicators were evaluated and their cost-effectiveness aggregated within each implementation package. We conducted a series of deterministic sensitivity analyses and a probabilistic sensitivity analysis. We used a willingness to pay threshold of £20,000 per QALY gained to indicate cost-effectiveness. We applied a 3.5% discount rate to costs and benefits post one year.

Results

We assessed 278 practices for eligibility in January 2015, excluding 35 because of closure or earlier participation in the programme (Fig 1). We invited 243 (87%) practices to participate in February 2015; 56 (23%) opted out, largely because of workload pressures, and nine were excluded for other reasons.

In April 2015, we randomised 178 (73%) practices to Trial 1 (80 practices), Trial 2 (64 practices), or no intervention (34 practices). Analyses of the no intervention arm will be reported elsewhere. Within each trial, practices were randomised 1:1 to intervention arms.

Baseline characteristics for general practices and patients were well balanced by trial and intervention (Tables 1 and 2). The mean practice IMD was 30.22 (SD 13.86) within the top quarter of UK social deprivation [24].

**Tab. 1. General practice characteristics at baseline by trial arm.**

**Tab. 2. Patient characteristics at baseline by trial arm (all patients from all practices in each intervention arm).**

No practices actively withdrew from the trial. One practice closed (BP intervention arm), another merged (risky prescribing) with a non-trial practice during the intervention period, and two trial practices merged (diabetes and risky prescribing). As outcome data for these practices were available up to the times of the second, third, and fourth feedback reports, respectively, all were included in the analysis using their most recent data.

Between May 2015 and April 2016, all intervention practices received feedback reports as intended, including an end-of-study report (S6 Table summarises intervention delivery). Educational outreach visits were delivered to 67 (47%) of 144 practices; 52 (68%) of the 77 practices declining visits gave no reason. Sixteen practices (24% of those receiving educational outreach visits) utilised additional pharmacist support. One hundred twenty-six (88%) practices joined the organisational groups, allowing them to access searches and computerised prompts (risky prescribing practices only). Second educational visits were delivered to eight (6%) practices.

Primary analyses demonstrated varying results across the implementation packages at 11 months post-randomisation (Table 3).

**Tab. 3. Primary outcome achievement: Baseline rates, outcome rates, and ORs adjusted for baseline achievement and covariates.**

The diabetes implementation package had no observed effect on diabetes treatment targets. Achievement was 24.2% in intervention practices; 23.7% in control practices (adjusted odds ratio [OR] 1.03; 97.5% confidence interval [CI] 0.89–1.18; p = 0.693; ICC = 0.015).

The risky prescribing implementation package reduced high-risk NSAID and anti-platelet prescribing. In intervention practices, 4.9% of patients had a record of risky prescribing; 6.0% in control practices (adjusted OR 0.82; 97.5% CI 0.67–0.99; p = 0.017; ICC = 0.022).

The BP implementation package had no observed effect on BP control. Achievement was 53.6% in intervention practices; 52.3% in control practices (adjusted OR 1.05, 97.5% CI 0.96–1.16; p = 0.215; ICC = 0.006).

The AF implementation package had no observed effect on anticoagulant prescribing. Achievement was 73.2% in intervention practices; 75.2% in control practices (adjusted OR 0.90; 97.5% CI 0.75–1.09; p = 0.214, ICC = 0.009).

There was little evidence of any intervention effects for any secondary outcome (S3–S6 Tables) except the risky prescribing implementation package, which showed some evidence of improvement against an individual indicator: patients aged 65 years or over prescribed aspirin and clopidogrel without co-prescription of gastro-protection. Adjusted prescribing levels were 25.3% in intervention practices, compared to 35.2% in control practices (adjusted OR 0.62; 97.5% CI 0.39–0.99; p = 0.021). The conclusions for total serum cholesterol and HbA1c were robust to log transformation of the outcomes in a sensitivity analysis conducted following model diagnostic checks. We observed no intervention effects on any QOF indicators, including those not targeted by the implementation packages.

In estimating cost-effectiveness, we assumed equal costs for all four implementation packages. We conservatively doubled the cost per package. The total cost of package delivery was £175,592, and cost per practice was £2,439 (£175,592/144*2). Costs per patient (not only those eligible for indicator criteria) for an average practice list size of 7,130 were negligible (£0.28). No interventions were cost-saving. The risky prescribing package is highly likely to be cost-effective with an ICER of £1,359 and 79% chance of cost-effectiveness (Table 4), with results largely driven by two indicators. While the deterministic ICER for the BP package indicates cost-effectiveness, this is highly uncertain, with the probabilistic results indicating only a 52% chance of cost-effectiveness. We have not presented model results for the diabetes package as incremental costs and benefits were negligible, making model results unreliable. Results were robust to deterministic sensitivity analyses when, for example, we increased and reduced intervention costs. S1–S4 Figs present cost-effectiveness planes and acceptability curves for the risky prescribing and BP control implementation packages.

**Tab. 4. Cost-effectiveness analysis: Mean probability sensitivity analysis outcomes at the practice level for the primary risky prescribing and BP control outcomes.**

Discussion

Our pragmatic, randomised trials found that an adaptable, multifaceted implementation package improved clinical care for only one of four high-impact indicators in general practices serving relatively socially deprived populations. The odds of risky prescribing for a patient in an intervention practice were 18.5% lower than for a patient with the same characteristics in a control practice, which could ultimately be associated with changes in mortality, morbidity, and health service use, depending on generalisability to the general population. There was insufficient evidence of an effect upon diabetes control, BP control, and anticoagulation for AF. Our findings suggest that the design and delivery of implementation strategies need to account for differences in the nature of targeted clinical behaviours and go further than the kinds of adaptations in content that we applied.

Commonly used interventions to implement evidence-based practice, such as audit and feedback, educational outreach, and computerised prompts generally have modest if variable effects on clinical performance [12–14]. Tailoring such interventions to identified needs and barriers offers a means to enhance their effects, but how best to do this and improve patient outcomes remains uncertain [25].

Our findings confirm the effectiveness, generalisability, and value of interventions incorporating audit and feedback to improve prescribing safety in UK primary care [26–28]. The PINCER trial compared one-off feedback with pharmacist outreach visits to one-off feedback alone, whilst the D-QIP study provided financial incentives in addition to weekly feedback. Given our pragmatic approach to practice recruitment, our intervention and findings compare most closely to those of the EFIPPS trial, which found that quarterly feedback, with or without embedded behaviour change techniques, reduced risky prescribing by a similar magnitude [28]. Our modelling also indicated relative cost-effectiveness, mainly driven by improved levels of gastro-protection. It is noteworthy that the cost of the risky prescribing package was only £0.28 per patient.

We found no benefit of the implementation package on the management and outcomes of our targeted long-term conditions. Systematic review evidence suggests that interventions targeting systems of patient management along with patient-mediated interventions (which we did not include) are likely to be important components of strategies in this context [29].

The balanced incomplete block designs permitted comparison of intervention effects while mitigating any potential nonspecific performance effects of trial participation [30]. Our trials were pragmatic in three ways. Opt-out recruitment ensured that participating practices were generally representative of the wider population [19]. Data collection was minimally intrusive. For intervention delivery, all practices received but were not obliged to act on feedback reports, whilst outreach visits were optional. Hence, the implementation packages were tested under real-world conditions, increasing confidence in wider applicability to routine general practice settings. We further demonstrated no adverse impacts on incentivised indicators of care not targeted by the implementation package.

Our evaluation had five main limitations. First, the use of routinely collected data may have compromised the precision of trial outcomes and hence ability to demonstrate effects. However, we extracted structured data that are reasonably reliably coded in general practice, partly incentivised by QOF. Second, given the multifaceted nature of the implementation package, we cannot make any inferences about the relative effects of individual intervention components. Third, educational outreach visits were delivered by facilitators not allocated to specific trial arms, thereby risking contamination between arms. We had instructed facilitators to focus only on delivering the implementation package to which each practice was assigned. Fourth, an 11-month follow-up period may have been too short to detect changes in patient outcomes, such as those related to diabetes or BP control, especially if a number of general practices only received educational outreach visits later in this period. This explanation is unlikely, as other trials have demonstrated changed clinical outcomes within similar durations of follow-up [29]; we also did not detect any improvements in processes of care for diabetes and BP control, respectively. Fifth, our composite endpoint for diabetes control requiring achievement of all HbA1c, BP, and cholesterol treatment goals may have been too demanding. Our clinical and patient advisors had considered this endpoint fair, if challenging.

Our work highlights three methodological issues. First, the implementation package effect on risky prescribing was modest but important at a population level. Foregoing a randomised design, as has been suggested for quality improvement research [31], would have reduced confidence in the validity of our findings and risked false positive conclusions. For example, the trial design accounted for temporal changes, including improvements in risky prescribing and anticoagulation achievement and declines in BP and diabetes achievement (Table 3), which would otherwise be difficult to interpret. Second, whilst we see the pragmatic design as a strength, a more explanatory approach could have made full engagement with our implementation package a condition of trial participation. Such mandating is seldom possible or even desirable in quality improvement programmes dependent upon professional engagement, particularly if they encourage ‘gaming’ behaviours to achieve goals whilst circumventing real action. Similarly, our opt-out approach to recruitment may have reduced self-selection of more enthusiastic practices, as well as administrative burden. Those responsible for leading quality improvement initiatives often specifically wish to include less enthusiastic or poorer performing practices. Third, a critical challenge prior to pragmatic evaluations is to develop interventions that are sufficiently durable to withstand the relatively hard-pressed and evolving environments of clinical practice. Whilst we followed the UK Medical Research Council framework for the development and evaluation of complex interventions, practice engagement with our implementation package was highly variable [32]. We would now recommend more intensive field work involving iterative cycles of testing and refining interventions prior to scaling up for definitive evaluation.

We had set out to develop an implementation package that could be adapted for different clinical priorities in primary care. We offer four interrelated explanations for the observed differences in intervention effects. First, the targeted clinical behaviour(s) and associated endpoints varied according to the extent of control held over them by clinical staff. Clinicians could make relatively straightforward changes to reduce risky prescribing, such as adding gastro-protection for prescribed aspirin, with limited input from patients. The observed significant difference in achievement of the associated secondary outcome on gastro-protection provides evidence to support such a mechanism (although we would still advise cautious interpretation, given that these analyses were not formally adjusted as we tested across multiple secondary endpoints). In contrast, improving BP control can require at least two consultations and changes in patient behaviour, as well as finding a pharmacological agent that is acceptable to and effective for an individual patient. This is consistent with evidence that adherence to clinical recommendations that are more complex or disruptive to routine practice is lower compared with simpler recommendations [33]. Interventions involving audit and feedback have also been shown to reduce other discouraged prescribing behaviours, namely of antibiotics [34], and offer a means to address urgent priorities such as rising opioid prescribing [35]. Second, the risky prescribing package included an automated computerised prompt requiring a one-step justification for continued prescribing. Such prompts are generally effective in changing prescribing behaviour [14]. However, a recent UK trial found that on-screen reminders did not improve adherence to the other prescribing behaviour we targeted, anticoagulation prescribing for AF [36]. With the benefit of hindsight, this is unsurprising. Qualitative work we undertook before the trials revealed that anticoagulation prescribing comprises a series of deceptively complex considerations and behaviours, which include balancing benefits and risks with patients [15]. Clinicians sometimes lacked confidence in starting treatment, given that they encountered it relatively infrequently in routine practice and felt frustrated by complicated guidance that made treatment difficult to explain to patients. Third, the number of patients requiring action to achieve indicators varied by trial arm, with far more in the diabetes and BP control arms relative to risky prescribing and anticoagulation for AF (see S5 Table). Hence, the larger numbers of patients requiring action may have undermined clinicians’ perceived feasibility and motivation. Moreover, making changes for even a small number of patients within the risky prescribing indicator set would have had a comparatively larger effect upon achievement relative to other indicators. Fourth, the indicators for three targeted long-term conditions were incentivised in the QOF. As well as aligning the implementation package with existing quality improvement schemes, our intention had been to encourage practices to move beyond the QOF by adopting more challenging, evidence-based goals. Within the present constraints of UK primary care, it was hard for practices to take on additional, unrewarded work. Clinicians may, nevertheless, have been motivated to address risky prescribing because it concerned patient safety.

In conclusion, an adaptable implementation package improved prescribing safety in general practice. However, we observed no benefits of the package within the context of an existing financial incentive system targeting similar aspects of care for three long-term conditions. Improving patient outcomes for long-term conditions requiring relatively complex management may require systemised approaches that target patient as well as professional behaviour.

Supporting information

S1 Table [docx]
Secondary outcomes from Trial 1: Achievement of individual indicators that contributed to composite outcomes; processes of care; and continuous intermediate clinical outcomes.

S2 Table [docx]
Secondary outcomes from Trial 1: Achievement of QOF indicators relating to the implementation packages; and non-trial related QOF indicators.

S3 Table [docx]
Secondary outcomes from Trial 2: Achievement of individual indicators that contributed to composite outcomes; processes of care; and continuous intermediate clinical outcomes.

S4 Table [docx]
Secondary outcomes from Trial 2: Achievement of QOF indicators relating to the implementation packages; and non-trial-related QOF indicators.

S5 Table [docx]
Key sample size assumptions.

S6 Table [docx]
Intervention delivery across trial practices.

S1 Fig [tif]
Scatterplot of simulated incremental cost and QALY for the composite indicator of risky prescribing.

S2 Fig [tif]
Cost-effectiveness acceptability curve for the composite indicator of risky prescribing.

S3 Fig [tif]
Scatterplot of simulated incremental cost and QALY for the composite indicator of BP control.

S4 Fig [tif]
Cost-effectiveness acceptability curve for the composite indicator of BP control.

S1 CONSORT Checklist [docx]

S1 Statistical Analysis Plan [docx]

S1 Trial Protocol [doc]

Zdroje

1. Levine DM, Linder JA, Landon BE. The quality of outpatient care delivered to adults in the United States, 2002 to 2013. JAMA Intern Med. 2016;176(12): 1778–1790. doi: 10.1001/jamainternmed.2016.6217 27749962

2. Cooksey R. A review of UK health research funding. London: HMSO; 2006.

3. Baird B, Charles A, Honeyman M, Maguire D, Das P. Understanding pressures in general practice. London: The King’s Fund; 2016.

4. Hobbs FDR, Bankhead C, Mukhtar T, Stevens S, Perera-Salazar R, Holt T, et al. Clinical workload in UK primary care: a retrospective analysis of 100 million consultations in England, 2007–14. Lancet. 2016;387(10035): 2323–2330. doi: 10.1016/S0140-6736(16)00620-6 27059888

5. Rushforth B, Stokes T, Andrews E, Willis TA, McEachan R, Faulkner S, et al. Developing ‘high impact’ guideline-based quality indicators for UK primary care: a multi-stage consensus process. BMC Fam Pract. 2015;16(1): 156.

6. Grimshaw JM, Thomas RE, MacLennan G, Fraser C, Ramsay CR, Vale L, et al. Effectiveness and efficiency of guideline dissemination and implementation strategies. Health Technol Assess. 2004;8(6): iii–iv, 1–72. doi: 10.3310/hta8060 14960256

7. Willis TA, Rushforth B, West R, Faulkner S, Stokes T, Glidewell L, et al. Variations in achievement of evidence-based, high-impact quality indicators in general practice: an observational study. PLoS ONE. 2017;12(7): e0177949. doi: 10.1371/journal.pone.0177949 28704407

8. National Institute for Health and Care Excellence. Type 2 diabetes in adults: management. London: Royal College of Physicians; 2015.

9. Howard RL, Avery AJ, Slavenburg S, Royal S, Pipe G, Lucassen P, et al. Which drugs cause preventable admissions to hospital? A systematic review. Brit J Clin Pharmacol. 2007;63(2): 136–147.

10. The Blood Pressure Lowering Treatment Trialists’ Collaboration. Blood pressure-lowering treatment based on cardiovascular risk: a meta-analysis of individual patient data. Lancet. 2014;384(9943): 591–598. doi: 10.1016/S0140-6736(14)61212-5 25131978

11. National Institute for Health and Care Excellence. Atrial fibrillation: the management of atrial fibrillation. London: National Institute for Health and Care Excellence; 2014.

12. Ivers N, Jamtvedt G, Flottorp S, Young JM, Odgaard-Jensen J, French SD, et al. Audit and feedback: effects on professional practice and patient outcomes. Cochrane Database Syst Rev. 2012(6). Art. No.: CD000259. doi: 10.1002/14651858.CD000259.pub3 22696318

13. O’Brien MA, Rogers S, Jamtvedt G, Oxman AD, Odgaard-Jensen J, Kristoffersen DT, et al. Educational outreach visits: effects on professional practice and health care outcomes. Cochrane Database Syst Rev. 2007(4). Art. No.: CD000409. doi: 10.1002/14651858.CD000409.pub2 17943742

14. Shojania KG, Jennings A, Mayhew A, Ramsay CR, Eccles MP, Grimshaw J. The effects of on-screen, point of care computer reminders on processes and outcomes of care. Cochrane Database Syst Rev. 2009(3). Art.No.: CD001096. doi: 10.1002/14651858.CD001096.pub2 19588323

15. Lawton R, Heyhoe J, Louch G, Ingleson E, Glidewell L, Willis TA, et al. Using the Theoretical Domains Framework (TDF) to understand adherence to multiple evidence-based indicators in primary care: a qualitative study. Implement Sci. 2016;11(113).

16. Glidewell L, Willis TA, Petty D, Lawton R, McEachan RRC, Ingleson E, et al. To what extent can behaviour change techniques be identified within an adaptable implementation package for primary care? A prospective directed content analysis. Implement Sci. 2018;13(32).

17. Eccles M, Grimshaw J, Campbell M, Ramsay C. Research designs for studies evaluating the effectiveness of change and improvement strategies. Qual Saf Health Care. 2003;12(1): 47–52. doi: 10.1136/qhc.12.1.47 12571345

18. Loudon K, Treweek S, Sullivan F, Donnan P, Thorpe KE, Zwarenstein M. The PRECIS-2 tool: designing trials that are fit for purpose. BMJ. 2015;350: h2147. doi: 10.1136/bmj.h2147 25956159

19. Lord PA, Willis TA, Carder P, West RM, Foy R. Optimizing primary care research participation: a comparison of three recruitment methods in data-sharing studies. Fam Pract. 2016;33(2): 200–204. doi: 10.1093/fampra/cmw003 26921610

20. Willis TA, Hartley S, Glidewell L, Farrin AJ, Lawton R, McEachan RRC, et al. Action to Support Practices Implement Research Evidence (ASPIRE): protocol for a cluster-randomised evaluation of adaptable implementation packages targeting ‘high impact’ clinical practice recommendations in general practice. Implement Sci. 2016;11(1): 1–11.

21. Doran T, Fullwood C, Gravelle H, Reeves D, Kontopantelis E, Hiroeh U, et al. Pay-for-performance programs in family practices in the United Kingdom. N Engl J Med. 2006;355(4): 375–384. doi: 10.1056/NEJMsa055505 16870916

22. Hayes AJ, Leal J, Gray AM, Holman RR, Clarke PM. UKPDS Outcomes Model 2: a new version of a model to simulate lifetime health outcomes of patients with type 2 diabetes mellitus using data from the 30 year United Kingdom Prospective Diabetes Study: UKPDS 82. Diabetologia. 2013;56(9): 1925–1933. doi: 10.1007/s00125-013-2940-y 23793713

23. Lovibond K, Jowett S, Barton P, Caulfield M, Heneghan C, Hobbs FD, et al. Cost-effectiveness of options for the diagnosis of high blood pressure in primary care: a modelling study. Lancet. 2011;378(9798): 1219–1230. doi: 10.1016/S0140-6736(11)61184-7 21868086

24. Department for Communities and Local Government. English indices of deprivation 2015 [Cited 2019 Nov 12]. https://www.gov.uk/government/statistics/english-indices-of-deprivation-2015

25. Baker R, Camosso-Stefinovic J, Gillies C, Shaw EJ, Cheater F, Flottorp S, et al. Tailored interventions to address determinants of practice. Cochrane Database Syst Rev. 2015(4). Art. No.: CD005470. doi: 10.1002/14651858.CD005470.pub3 25923419

26. Avery AJ, Rodgers S, Cantrill JA, Armstrong S, Cresswell K, Eden M, et al. A pharmacist-led information technology intervention for medication errors (PINCER): a multicentre, cluster randomised, controlled trial and cost-effectiveness analysis. Lancet. 2012;379(9823): 1310–1319. doi: 10.1016/S0140-6736(11)61817-5 22357106

27. Dreischulte T, Donnan P, Grant A, Hapca A, McCowan C, Guthrie B. Safer prescribing—a trial of education, informatics, and financial incentives. N Engl J Med. 2016;374(11): 1053–1064. doi: 10.1056/NEJMsa1508955 26981935

28. Guthrie B, Kavanagh K, Robertson C, Barnett K, Treweek S, Petrie D, et al. Data feedback and behavioural change intervention to improve primary care prescribing safety (EFIPPS): multicentre, three arm, cluster randomised controlled trial. BMJ. 2016;354: i4079. doi: 10.1136/bmj.i4079 27540041

29. Tricco AC, Ivers NM, Grimshaw JM, Moher D, Turner L, Galipeau J, et al. Effectiveness of quality improvement strategies on the management of diabetes: a systematic review and meta-analysis. Lancet. 2012;379(9833): 2252–2261. doi: 10.1016/S0140-6736(12)60480-2 22683130

30. McCambridge J, Witton J, Elbourne DR. Systematic review of the Hawthorne effect: new concepts are needed to study research participation effects. J Clin Epidemiol. 2014;67(3): 267–277. doi: 10.1016/j.jclinepi.2013.08.015 24275499

31. Berwick DM. The science of improvement. JAMA. 2008;299(10): 1182–1184. doi: 10.1001/jama.299.10.1182 18334694

32. Craig P, Dieppe P, Macintyre S, Michie S, Nazareth I, Petticrew M. Developing and evaluating complex interventions: the new Medical Research Council guidance. BMJ. 2008;337: a1655. doi: 10.1136/bmj.a1655 18824488

33. Grol R, Dalhuijsen J, Thomas S, Veld C, Rutten G, Mokkink H. Attributes of clinical guidelines that influence use of guidelines in general practice: observational study. BMJ. 1998;317(7162): 858–861. doi: 10.1136/bmj.317.7162.858 9748183

34. Hallsworth M, Chadborn T, Sallis A, Sanders M, Berry D, Greaves F, et al. Provision of social norm feedback to high prescribers of antibiotics in general practice: a pragmatic national randomised controlled trial. Lancet. 2016;387(10029): 1743–1752. doi: 10.1016/S0140-6736(16)00215-4 26898856

35. Foy R, Leaman B, McCrorie C, Petty D, House A, Bennett M, et al. Prescribed opioids in primary care: cross-sectional and longitudinal analyses of influence of patient and practice characteristics. BMJ Open. 2016;6(5): e010276. doi: 10.1136/bmjopen-2015-010276 27178970

36. Holt TA, Dalton A, Marshall T, Fay M, Qureshi N, Kirkpatrick S, et al. Automated software system to promote anticoagulation and reduce stroke risk: cluster-randomized controlled trial. Stroke. 2017;48(3): 787–790. doi: 10.1161/STROKEAHA.116.015468 28119433

Článek An evaluation of Chile’s Law of Food Labeling and Advertising on sugar-sweetened beverage purchases from 2015 to 2017: A before-and-after study

Článek A multicomponent secondary school health promotion intervention and adolescent health: An extension of the SEHER cluster randomised controlled trial in Bihar, India

Článek Association of moderate alcohol intake with in vivo amyloid-beta deposition in human brain: A cross-sectional study

Článek Impact of the announcement and implementation of the UK Soft Drinks Industry Levy on sugar content, price, product size and number of available soft drinks in the UK, 2015-19: A controlled interrupted time series analysis

Článek Estimating progress towards meeting women’s contraceptive needs in 185 countries: A Bayesian hierarchical modelling study

Článek Emerging priorities for HIV service delivery

Článek Digitally enabled aged care and neurological rehabilitation to enhance outcomes with Activity and MObility UsiNg Technology (AMOUNT) in Australia: A randomised controlled trial

Článek Association of coincident self-reported mental health problems and alcohol intake with all-cause and cardiovascular disease mortality: A Norwegian pooled population analysis

Článek The effect of assessing genetic risk of prostate cancer on the use of PSA tests in primary care: A cluster randomized controlled trial

Článek Virological suppression and clinical management in response to viremia in South African HIV treatment program: A multicenter cohort study

Článek Safety and immune responses after a 12-month booster in healthy HIV-uninfected adults in HVTN 100 in South Africa: A randomized double-blind placebo-controlled trial of ALVAC-HIV (vCP2438) and bivalent subtype C gp120/MF59 vaccines

Článek Improving air quality needs to be a policy priority for governments globally