Socioeconomic inequality in medication persistence in primary and secondary prevention of coronary heart disease - A population-wide electronic cohort study.

BACKGROUND: Coronary heart disease (CHD) mortality in England fell by 36% between 2000 and 2007 and it is estimated that approximately 50% of the fall was due to improved treatment uptake. Marked socio-economic inequalities in CHD mortality in the United Kingdom (UK) remain, with higher age-adjusted rates in more deprived groups. Inequalities in the persistence of medication for primary and secondary prevention of CHD may contribute to the observed social gradient and we investigated this possibility in the population of Wales (UK). METHODS AND
FINDINGS: An electronic cohort of individuals aged over 20 (n = 1,199,342) in Wales (UK) was formed using linked data from primary and secondary care and followed for six years (2004-2010). We identified indications for medication (statins, aspirin, ACE inhibitors, clopidogrel) recommended in UK National Institute for Clinical Excellence (NICE) guidance for CHD (high risk, stable angina, stable angina plus diabetes, unstable angina, and myocardial infarction) and measured the persistence of indicated medication (time from initiation to discontinuation) across quintiles of the Welsh Index of Multiple Deprivation, an area-based measure of socio-economic inequality, using Cox regression frailty models. In models adjusted for demographic factors, CHD risk and comorbidities across 15 comparisons for persistence of the medications, none favoured the least deprived quintile, two favoured the most deprived quintile and 13 showed no significant differences.
CONCLUSIONS: During our study period (2004-2010) we found no significant evidence of socio-economic inequality in the persistence of recommended medication for primary and secondary prevention of CHD.

Introduction

Although coronary heart disease (CHD) mortality has fallen in recent decades in the UK and other high-income countries a social gradient persists, with a higher age-adjusted mortality in more socioeconomically deprived groups [1]. An IMPACT modelling study estimating the proportions of the fall in CHD mortality attributable to changes in risk factors or treatments (effectiveness and provision) found that in England and Wales, between 1981 and 2000, 58% of the fall in CHD mortality could be attributed to population-level reduction in major risk factors and 42% to treatments [2]. An IMPACT study of the period 2000–2007 in England, during which CHD mortality fell by 36%, estimated that improved uptake of treatments accounted for approximately 50% of the fall [3], with lipid-lowering therapy accounting for 14%.

There is an association between the degree of compliance with CHD-related medication and CHD outcomes that is not only due to the ‘healthy adherer’ effect–the tendency for individuals with good medication adherence to have generally healthier lifestyles [4-6]. There is also evidence that better medication compliance is associated with relative affluence [7] and that this applies to lipid-lowering therapy in CHD prevention [8-11].

A review of papers published between 1997 and 2005 that examined persistence of medication for hypertension and dyslipidaemia observed that few studies explicitly stated the definition of persistence used, and that different measures of persistence were employed [12]. A meta-analysis of papers published between 2000 and 2005 examining compliance with medication for hypertension, diabetes and dyslipidaemia reported that different measures of persistence used over different time frames yielded widely differing results [4]. Studies of medication compliance have used definitions and terminology differently (compliance sometimes regarded as synonymous with adherence, and sometimes as including both adherence and persistence) and therefore standard definitions are proposed [12,13], clarifying that adherence is the proportion of prescribed doses taken in the prescribed time interval and persistence is the accumulation of time from the initiation of therapy to discontinuation of therapy.

Although health care in the UK, including Wales, is publicly funded and free at the point of delivery, the concept of the ‘inverse care law’ [14] (more deprived groups having greater health care needs yet receiving poorer health care) has been influential in public health medicine in the UK. Evidence from some UK studies suggested that more socio-economically deprived groups received poorer health care for cardiovascular disease [15,16]. Our previous study of the overall pathway of CHD health care in the population of Wales [17] identified indications for recommended interventions, examined whether these interventions were received, and measured time to their delivery. The result showed little evidence of inequity (inequality to the disadvantage of more deprived groups) other than in relation to revascularization procedures. The analyses did not examine whether recommended interventions continued to be received appropriately and therefore did not exclude the possibility of inequity in medication persistence. We investigated that possibility in the same cohort of over one million individuals during the study period, 2004–2010, measuring the accumulation of time from initiation to discontinuation of recommended medication (persistence). As in our previous study [17] the recommendations for medication were those of national guidelines in primary and secondary prevention of CHD, and we used area-based measures of socio-economic deprivation. Our data enabled us to identify indications for medication in individuals, to specify the start date of each indication, and to use a time-to-event survival technique directly measuring the accumulation of time from initiation to discontinuation of therapy. We were able to adjust for relevant covariates and the data used (with the exception of the inference of deprivation from area level measures) was available at the individual level. We are not aware of any other study of this size addressing this issue in any UK population.

Methods

The analyses were carried out within the Secure Anonymized Information Linkage databank (SAIL) at Swansea University [18,19]. The system allows researchers to link primary care data, hospital activity data, and mortality data to inform the clinical history of individuals.

Permission to undertake the analyses was obtained from the Information Governance Review Panel at SAIL in line with the Collaborative Review System (project reference number 0156).

Datasets

We defined a retrospective cohort of individuals aged 20 or over, resident in Wales and registered with SAIL-submitting general practices between 1 January 2004 and 31 December 2010. Individuals reaching the age of 20 were added to the cohort at annual time points. Routine data from the Welsh Demographic Service, Patient Episode Data for Wales (PEDW) hospital admission data (ICD 10 and Office of Population and Censuses codes for CHD-related hospital episodes and procedures), and primary care data (Read codes for diagnosis, investigation and treatment of CHD and the prescribing of antihypertensive, lipid-lowering and anti-platelet therapy) were extracted to form a linked dataset. If an individual died or ceased to be registered with a SAIL-submitting practice this was treated as a censoring event. The primary care data available for our study was available only from SAIL-submitting practices, covering approximately 40% of the population of Wales. There is no available evidence that these practices were unrepresentative. The distribution of urban and rural residency of the population resembled that of Wales as a whole. Comparison with Office of National Statistics (ONS) mid-year data (2004) for the whole of Wales showed small differences in age distribution, our cohort having 1.2% fewer in the proportion aged over 40. Comparison of the socio-economic distribution of our study population with that of Wales as a whole showed that quintiles 1 and 3 were over-represented (21.3% and 22.94% respectively) and quintiles 2, 4 and 5 were under-represented (18.34%, 18.72% and 18.55% respectively).

Assessment of socioeconomic inequalities

The Welsh Index of Multiple Deprivation (WIMD) (2008) for the individual’s residence was assessed at the Lower Super Output Area (LSOA) (mean population 1500) as a measure of socioeconomic deprivation. The 2008 WIMD is based on the resident’s income, employment status, education, housing, health and geographical access to services [20].

Inequalities were examined by comparing WIMD quintile 5 (most deprived) to quintile 1 (least deprived).

Indicated medication

The criteria for indicated medication were based on the interventions recommended in UK National Service Frameworks (NSFs) for CHD [21,22] and National Institute for Health and Care Excellence (NICE) guidelines relating to the study period [23-27]. In relation to primary prevention, the level of CHD event risk at which statin treatment was recommended by NSF and NICE guidelines was 20% over ten years [27]. Components of the risk score were systolic blood pressure, body mass index (BMI), smoking status, and cholesterol: high density lipoprotein (HDL) ratio. Those whose risk of CHD was designated high on this basis are referred to as ‘risk assessed high’ (see Table 1) and those at high risk because of a diagnosis of cerebrovascular disease, peripheral vascular disease or diabetes are referred to as ‘high-risk diagnosis’.

Table 1

Numbers of medications initiated for each indication and discontinued within observation period by indication and medication type.

Original indication	Medication initiated	Number initiating medication	Number stopping medication
Risk assessed high	Statin	33228	5378
High-risk diagnosis	Statin	29208	4041
Stable angina	Statin	11231	1711
Stable angina and diabetes	Statin	6588	782
Unstable angina	Statin	9211	1341
MI	Statin	11380	1642
Stable angina	Aspirin	10704	2590
Stable angina and diabetes	Aspirin	5472	1056
Unstable angina	Aspirin	8663	1654
MI	Aspirin	11011	1889
Stable angina and diabetes	ACE inhibitor	5620	827
Unstable angina	ACE inhibitor	7860	1443
MI	ACE inhibitor	10772	1916
Unstable angina	Clopidogrel	5783	3419
MI	Clopidogrel	10133	6536

We developed a set of algorithms based on Read codes [28] to identify all individuals for whom medication in primary and secondary prevention of CHD was indicated, and we examined provision and persistence of that medication. The 15 interventions for which we made comparisons between deprivation groups that are shown in Table 1. We did not make comparisons for the numerous possible combinations of medications used in management of hypertension.

Our routine data did not provide information on individuals’ contraindications to medication, or refusal of treatment. Data were not available on in-patient prescribing and our examination of prescription of medication was confined to the period after individuals left hospital.

Although the recommended interval between of repeat prescriptions in UK general practice is usually 28 days there is variation in practice, and there is evidence that in Wales during our study period a minority of repeat prescriptions were issued at intervals longer than longer 28 days [29, 30]. We made a simplifying assumption and designated the point at which persistence of medication had lapsed as the last issue of that prescription where it occurred at least 56 days prior to the end of the observation period for that individual.

Covariates

We examined a number of potentially confounding factors determined at the time-point at which the indication for the medication appeared. They were selected on the basis of availability and evidence from previous studies [17]. Covariates available included demographic factors (age, sex); risk-factors (systolic blood pressure, body mass index, smoking status, cholesterol: HDL ratio); co-morbidities based on the Charlson co-morbidity index [31] collapsed to a binary variable because some components were already considered as covariates (CHD, cerebrovascular disease and diabetes); and the Framingham non-laboratory risk assessment score (comprising sex, age, systolic blood pressure, BMI, smoking status, reported diabetic status, and current treatment for hypertension) [32]. We accounted for previous indications for the same medication: for example statins indicated by angina might previously have been indicated by risk-assessment.

Statistical methods

We used a Cox model with random effects (frailty models) to examine the persistence of CHD-related medication, measuring the length of time from initiation until the issue of the last prescription for medication that appeared still to be indicated (with at least 56 days without a prescription prior to the end of the observation period required to define a last prescription). For each of the comparisons we produced Kaplan-Meier plots that enabled treatment of censoring events.

We fitted the individual’s general practice or admitting hospital modelled as random effects, to allow for unobserved hospital or primary care specific factors that might cause clustering. The type 1 error probability was set to 0.05 for all analyses. Modelling was performed using the coxme package in R [33].

We used multiple imputations (n = 20 imputed datasets) with chained equations to impute values for missing covariates: systolic blood pressure, BMI, cholesterol:HDL ratio, smoking status and admission type, including all outcomes in the prediction model. We performed sensitivity analyses, re-running analyses using the 2001 Townsend deprivation quintiles and the 1991 Framingham assessment tool.

Results

The initial cohort comprised 1,201,399 subjects. After exclusion of those with an incorrectly coded date of birth (n = 202), absent coding for gender (n = 7) or with discontinuous registration with SAIL (n = 1848) the cohort was reduced to 1,199,342.

Table 1 shows the number of medications initiated for each indication and the number of those treatments subsequently discontinued during the observation period. The pattern of discontinuation is shown in the panel of Kaplan-Meier plots (Fig 1).

Fig 1

Panel of Kaplan-Meier plots for selected indications and medications showing the discontinuation in medication persistence across the seven year observation period.

Within each individual Kaplan-Meier plot, the survival curve is shown separately for each of the deprivation quintiles. Quintile 1 (red) is the least deprived quintile.

One plot for each of the medications investigated is shown. The patterns shown for each of the drugs for these indications are reflected in very similar patterns for each drug for the other indications investigated. Additional Kaplan-Meier plots for these indications are included in the supporting information for this paper; those shown are illustrative of the patterns observed.

For statins, ACE inhibitors and aspirin, a gradual decrease in persistence was observed over the seven years of observation. At five years, 75% of individuals initiated on statins for ‘risk assessed high’ were still being prescribed the medication in each of the deprivation quintiles. A similar pattern was observed for ACE inhibitors and aspirin, although the proportion of individuals still prescribed these medications at five years was slightly less than 75% for each of the quintiles. For clopidogrel, the recommendation that applied during the period of our study [23] for 12 months of treatment is reflected in the pronounced decline in persistence at one year following initiation of therapy, with a gradual decline thereafter. Each of the plots shows a decline in persistence following the initial 28-day prescription, with this pattern most pronounced for clopidogrel. Importantly, no substantial differences in persistence are observed between deprivation quintiles.

A summary of our results in the fully adjusted models is presented in Table 2. Two comparisons showed statistically significant differences: in individuals with a ‘high-risk diagnosis’ the persistence for statins favoured the most deprived quintile (HR 0.78, 95% CI 0.70, 0.88), and in individuals who had a myocardial infarction (MI) the persistence for clopidogrel (during the 12-month period for which it was indicated post-MI) also favoured the most deprived quintile (HR 0.86, 95% CI 0.78, 0.95).

Table 2

Hazard ratios (HRs) and 95% confidence intervals (CIs) for the association between socioeconomic inequalities and discontinuation of indicated medication for CHD prevention.

Hazard ratios (HRs) relate to discontinuation of medication during the indicated period. Hazard ratios less than 1 indicate that the most deprived quintile was less likely than the least deprived quintile to stop taking the medication for the given indication. HR adjusted for age, sex, smoking status, BMI, hypertension, cholesterol: HDL ratio, and comorbidities; for MI and unstable angina indications also adjusted for admission type and specialty.

Original indication	Medication initiated	Hazard ratio for comparison between quintile 5 and quintile 1 (95% confidence interval)	Statistically significant difference?	Favours
Risk assessed high	Statin	0.95 (0.86, 1.05)	No
High-risk diagnosis	Statin	0.78 (0.70, 0.88)	Yes	Most deprived
Stable angina	Statin	1.06 (0.88, 1.26)	No
Stable angina and diabetes	Statin	0.84 (0.65, 1.09)	No
Unstable angina	Statin	1.04 (0.84, 1.27)	No
MI	Statin	0.97 (0.80, 1.18)	No
Stable angina	Aspirin	1.01 (0.88, 1.17)	No
Stable angina and diabetes	Aspirin	0.86 (0.69, 1.08)	No
Unstable angina	Aspirin	0.85 (0.71, 1.02)	No
MI	Aspirin	1.13 (0.94, 1.35)	No
Stable angina and diabetes	ACE inhibitor	1.10 (0.85, 1.41)	No
Unstable angina	ACE inhibitor	1.14 (0.93, 1.38)	No
MI	ACE inhibitor	1.15 (0.96, 1.36)	No
Unstable angina	Clopidogrel	1.03 (0.91, 1.17)	No
MI	Clopidogrel	0.86 (0.78, 0.95)	Yes	Most deprived

Use of the Framingham 1991 risk assessment tool and the Townsend deprivation quintiles in ours sensitivity analyses made only small differences to the estimated hazard ratios and of the 15 comparisons the same two (for ‘high risk diagnosis’ and for MI) significantly favoured quintile 5. For ‘high risk diagnosis’ the hazard ratio was 0.78 in the fully adjusted model, 0.79 in the Framingham 1991 risk assessment analysis and 0.82 in the Townsend quintiles analysis. For MI the hazard ratios in these analyses were respectively 0.86, 0.86 and 0.88. In none of the models was there a significant difference in any of the 13 other comparisons and therefore the overall pattern remained unchanged in the sensitivity analyses.

Discussion

We found little evidence of socio-economic inequality in persistence of indicated medication in the primary and secondary prevention of CHD. Only two of the 15 indicated medications showed a difference in persistence according to levels of socio-economic deprivation, both having a longer persistence in the most deprived groups.

Persistence of medication depends on healthcare-related factors, including administrative systems, the observing and recording of indications for medication, and individual prescription review [34, 35]. The introduction in the UK in 2004 of the Quality and Outcomes Framework (QOF), a major public health intervention, incentivised such activities [36]. Persistence also depends on patient-factors including adverse reactions, emerging contra-indications, refusal of treatment, and comorbidities. Our findings indicate that the overall effects of these factors (healthcare-related and patient-related) did not cause inequity in persistence of the medication we examined.

Comparison with other studies

Our findings are consistent with those from a UK study on the use of statins after first myocardial infarction during the period 1997–2004 [8] that found approximately 80% of individuals continued to receive statins at one year and approximately 76% at 5–10 year follow-up.

In a multinational, multicentre trial of individuals with acute coronary syndromes (ACS), 1999–2003, discontinuation rates at six months were 8% for aspirin, 13% for statins, 20% for ACE inhibitors [37]. In a USA study individuals undergoing catheterization for CHD between 1998–2001 were found to have discontinuation rates at 12 months of 28% for ACE inhibitors and 18% for aspirin [38]. In a UK study of individuals after MI (2003–2009) the adjusted odds of being prescribed clopidogrel at 12 months were 53% for NSTEMI and 54% for STEMI [39].

A number of large (> 30, 000 subjects) UK studies, ecological or population-based, have examined evidence of equity in use of CHD-related medication although none primarily examined persistence. Of the seven large studies using prescribing rates to examine lipid-lowering therapy in primary prevention of CHD the results in four favoured the less deprived [40-44], two showed no difference [15, 16] and one favoured the more deprived group [45]. Of eight large UK studies examining use of anti-platelet medication (aspirin and clopidogrel) in primary and/or secondary prevention of CHD the results in primary prevention in two studies favoured the less deprived [15, 16], in one favoured the more deprived [46], and in two showed no difference [40,47]. In relation to anti-platelet medication in secondary prevention the results in one study favoured the less deprived [15], in two favoured the more deprived [48,49], and in one showed no significant difference [50]. Four studies indicating inequity in lipid-lowering therapy in primary prevention were published between 1998 and 2004, [40-43], but a large individual-level study examining the increase in utilization of medication, but not examining persistence, found no evidence of inequity in secondary prevention of CHD in the UK between 1999 and 2007 [49]. Our study found that in both primary and secondary prevention of CHD between 2004 and 2011 there was no significant evidence of inequity in medication persistence.

Policy implications

Our study period coincided with a relatively rapid improvement in the UK in a range of clinical activity indicators, including those related to the recording and delivery of CHD-related primary care [51]. This was attributed partly to the introduction in 2000 of the National Service Framework for CHD in England (2001 in Wales) and in 2004 of the Quality Outcomes Framework (QOF) [36]. Our findings suggest that if these improvements extended to the appropriate persistence of medication in CHD healthcare they did so equitably.

Strengths of the study

We based our study on data from a large number of individuals (more than one million) and used a time-to-event methodology developed to address population-level analysis of healthcare use adjusted for need.

Our study examined a health service in which healthcare is free at the point of delivery, and in Wales, unlike other parts of the UK, there is no charge for prescriptions. It has been shown in the USA that a lower level of insurance cover, and consequently higher financial cost to the individual, is associated with poorer adherence to medication used in secondary prevention of CHD [52]. The integrated system of healthcare in the UK differs significantly from systems such as those seen in the USA and results from the study of our population may form a useful comparator for studies in other healthcare systems.

Limitations of the study

Because of the complexity of recommended medication for hypertension with numerous potential permutations, and because of the difficult in distinguishing their clinical indications in an individual (as when a diuretic or a beta blocker might have been prescribed for reasons other than hypertension) we did not include antihypertensives in this analysis, although we analysed the use of ACE inhibitors in relation to stable angina with diabetes, unstable angina, and MI. Area-based measures of socio-economic status are known to underestimate inequalities and their use may therefore have reduced our ability to detect inequalities.

Conclusions

We found no significant evidence of inequity in medication persistence in primary and secondary prevention of CHD.