Single Pill Regimen Leads to Better Adherence and Clinical Outcome in Daily Practice in Patients Suffering from Hypertension and/or Dyslipidemia: Results of a Meta-Analysis.

INTRODUCTION: Cardiovascular diseases (CVD) represent the first cause of mortality in western countries. Hypertension and dyslipidemia are strong risk factors for CVD, and are prevalent either alone or in combination. Although effective substances for the treatment of both factors are available, there is space for optimization of treatment regimens due to poor patient's adherence to medication, which is usually a combination of several substances. Adherence decreases with the number of pills a patient needs to take. A combination of substances in one single-pill (single pill combination, SPC), might increase adherence, and lead to a better clinical outcome. AIM: We conducted a meta-analysis to compare the effect of SPC with that of free-combination treatment (FCT) in patients with either hypertension, dyslipidemia or the combination of both diseases under conditions of daily practice.
METHODS: Studies were identified by searching in PubMed from November 2014 until February 2015. Search criteria focused on trials in identical hypertension and/or dyslipidemia treatment as FCT therapy or as SPC. Adherence and persistence outcome included proportion-of-days-covered (PDC), medication possession ratio (MPR), time-to treatment gap of 30 and 60 days and no treatment gap of 30 days (y/n). Clinical outcomes were all cause hospitalisation, hypertension-related hospitalisation, all cause emergency room visits, hypertension-related emergency room visits, outpatient visits, hypertension-related outpatient visits, and number of patients reaching blood pressure goal. Randomized clinical studies were excluded because they usually do not reflect daily practice.
RESULTS: 11 out of 1.465 studies met the predefined inclusion criteria. PDC ≥ 80% showed an odds ratio (OR) of 1.78 (95% CI: 1.30-2.45; p = 0.004) after 6 months and an OR of 1.85 (95% CI: 1.71; 2.37; p < 0.001) after ≥ 12 months in favour to the SPC. MPR ≥ 80% after 12 months also was in favour to SPC (OR 2.13; 95% CI: 1.30; 3.47; p = 0.003). Persistence was positively affected by SPC after 6, 12, and 18 months. Time to treatment gap of 60 days resulted in a hazard ratio (HR) of 2.03 (95% CI: 1.77; 2.33, p < 0.001). The use of SPC was associated with a significant improvement in systolic blood pressure reduction, leading to a higher number of patients reaching individual blood pressure goals (FCT vs SPC results in OR = 0.77; 95% CI: 0.69; 0.85, p < 0.001). Outpatient visits, emergency room visits and hospitalisations, both overall and hypertension-related were reduced by SPC: all-cause hospitalisation (SPC vs FCT: 15.0% vs 18.2%, OR 0.79, 95% CI 0.67; 0.94, p = 0.009), all-cause emergency room visits (SPC vs FCT: 25.7% vs 31.4%, OR 0.75, 95% CI 0.65; 0.87, p = 0.001) and hypertension related emergency room visits (SPC vs FCT: 9.7% vs 14.1%, OR 0.65, 95% CI 0.54; 0.80, p < 0.001).
CONCLUSIONS: SPC improved medication adherence and clinical outcome parameter in patients suffering from hypertension and/or dyslipidemia and led to a better clinical outcome compared to FCT under conditions of daily practice.

Introduction

Cardiovascular diseases (CVD)represent the first cause of mortality in many western countries. In 2015, 76,013 people died due to coronary heart disease, 49,210 from myocardial infarction, and 47,414 from heart failure in Germany [1]. Hypertension and dyslipidemia are strong risk factors associated with CVD and are prevalent either alone or in combination [2]. In Germany, more than half of the adults ≥ 18 years have elevated cholesterol > 190 mg/dl, about 20% above 240 mg/dl [3]. 30% of German women, and 33% of men are suffering from hypertension. The prevalence is nearly unchanged since 1998 [4]. Although effective antihypertensive agents are available, only half of the medically treated patients reach a blood pressure (BP) of <140/90 mmHg [5].

An explanation for the poor management of both, dyslipidemia, and hypertension, could be the treatment conditions. Multiple antihypertensive agents are required to achieve target BP in most patients [2]. It has also been observed, that initial low-dose treatment with two or three antihypertensive agents is more efficacious than the standard dose of each monotherapy [6]. However, the number of pills might have an influence on medical adherence. Recent data indicate that each increase in the number of antihypertensive medications might lead in addition to around 80% increase in nonadherence [7]. This will have clinical implications: non-adherence to guideline-recommended therapies regards hypertension and dyslipidemia was associated with a significant higher rate of major cardiovascular events (MACE) [8].

Reduction of pills by combining different substances in one single pill could be a solution to cover these issues. However, it remains unclear whether this will be a model for daily practice.

The objective of this meta-analysis was to compare adherence and clinical outcomes between single pill (SPC) and lose combination (FCT) in daily practice.

Methods

A literature search of PubMed was undertaken to identify relevant studies. Studies were eligible for investigation if they fulfilled the following inclusion criteria: (1) patients suffering from hypertension, dyslipidemia, or mixed hypertension and dyslipidemia, (2) compared individual drugs exactly, (3) prospective or retrospective cohort studies, (4) included at least one outcome variable that is recommended for the measurement of adherence or persistence by the ISPORi or one of the societies of the indications in question or included other relevant clinical outcome/effectiveness parameter, (5) were conducted in a real-world setting, (6) follow-up period of 6 or more months, and (6) were published in English.

Data from controlled clinical trials are not valid to conclude, whether a combination therapy given as a single pill will have advantages compared with the identical substances in several pills, because patients are closely monitored and reminded to take their medication. Therefore, those studies were excluded from the analysis.

Identified publications were cross-checked for doubles and all remaining abstracts read and checked for eligibility first based on title and abstract and second based on full-text review. Publications remaining were categorized according to the criterion whether the comparison was performed as an exact substance comparison or inaccurately as a comparison of overall substance classes.

Statistical Methods

Two parameters of adherence to medication were used. The Medical Possession Rate (MPR) is calculated as the ratio of the number of days a patient has their medicine on hand to the number of days a patient has to take the medication. The Proportion of Days Covered (PDC) calculates the ratio of number of days the patient is covered by all medications in a period to the total number of days in the period. Therefore, PDC is recommended for patients on multiple therapies.

Odds ratios (OR) associated with the use of SPC vs FCT were calculated for the adherence outcomes PDC ≥ 80%, MPR ≥ 80%, and persistence outcome variable no treatment gap of 30 days. Likewise, ORs are given for reaching JNC-VII blood pressure goal and the effectiveness outcomes all-cause emergency room visits, hypertension-related emergency room visits, all-cause hospitalisation, hypertension-related outpatient visits, outpatient visits and hypertension-related outpatient visits. Hazard ratios (HR) are used for time to 30-days treatment gap and time to 60-days treatment gap. PDC and MPR are analyzed by mean differences. ORs are either already given in the original publication, or calculated by using the numbers of events and the sample size per treatment group. For mean differences, actual means, the sample sizes and the standard deviations (or standard errors) were used. If events had been reported as percentages, results are recalculated into patient numbers to allow the calculation of ORs. In cases in which a transformation of the ORs or HRs was necessary in order to standardize the direction of the effect sizes, this was done by using the transformation 1/x. Z-values are computed for testing the null hypothesis that the OR or HR is 1.0 or that the mean difference is 0. The I2-statistic is computed to measure heterogeneity of effects. If significant heterogeneity was demonstrated, a random-effects model will be used for analysis. All statistical analyses were performed with the statistic software R. Specifically, the R package “meta” with the R function “metagen” was applied for the statistical models (meta-analytical models) assuming a random effects model.

Results

From 1.465 initial studies, 11 publications where finally included for further consideration (Fig. 1). Studies are presented in Table 1.

Fig. 1

Flowchart of study selection process

Table 1

Eligible studies for meta-analysis

Study	Indication	No. of participants (SPC)	Age in years, mean (SPC/FCT)	Gender, % female (SPC/FCT)	Compounds	Class	Dose of medication
Combination with statins
Hussein et al. (2010) [9]	Hyp/Dys	35 430 (3136)	50.0–55.2/54.4–56.9a	34.4–44.0/41.0–54.6a	AML/ATOR	CCB/Statin	NA
Patel et al. (2008) [10]	Hyp/Dys	4703 (795)	61.4/62.1–64.4a	42.5/47.8–57.5b	AML/ATOR	CCB/Statin	NA
Simons et al. (2011) [11]	Hyp/Dys	10 350 (4146)	70.7/71.2	54.0/54.0	AML/ATOR	CCB/Statin	NA
Balu et al. (2009) [12]	Dys	8988 (6638) MPR	51.9/56.0–56.1a	26.9/77.7–83.0	Niacin/Lovastatin	Niacin/Statin	NA
Kamat et al (2011) [13]	Dys	42460 (38847)	56.4/54.8	44.8/37.7	(Niacin or Ezetimibe)/Simvastatin Niacin/Lovastatin	(Niacin or Ezetimibe)/Statin	NA
Combination without statins
Ram et al. (2012) [14]	Hyp	46706 (32807)	Only numbers per age range are given	64.4–65.9/59.5–63.5	AML/OLM (& AML/VAL)	CCB/ARB	NA
Levi et al. (2016) [15]	Hyp	4890 (3057)	66.6/68.1	52.2/50.8	AML/OLM	CCB/ARB	NA
Brixner et al. (2008) [16]	Hyp	2189 (1628)	Only numbers per age range are given	49/41.5	VAL/HCTZ	ARB/HCTZ	NA
Machnicki et al. (2015) [17]	Hyp	3768 (1884)	48.4/48.0	66.4/66.8	AML/VAL/HCTZ	CCB/ARB/HCTZ	NA
Jackson et al. (2008) [18]	Hyp	908 (619)	Only numbers per age range are given	57.6–58.5/55.4	AML/VAL/HCTZ	CCB/ARB/HCTZ	NA
Xie et al. (2014) [19]	Hyp	17465 (8516)	54.8/59.1–63.9a	45.2/49.5–51.3	AML/(VAL or OLM)/HCTZ	CCB/ARB/HCTZ	NA

SPC single pill combination, FCT free-combination treatment, Hyp hypertension, Dys dyslipidemia, AML amlodipine, ATOR atorvastatin, VAL valsartan, OLM olmesartan, HCTZ hydrochlorothiazide, CCB calcium channel blocker, ARB angiotensin receptor blocker, NA not applicable

aThe study population was stratified into different cohorts and/or patient characteristics are given based on the use of CCB and/or statin therapies

The number of patients included in the studies is shown in Table 1. The non-weighted mean age was slightly higher in the FCT-group with a mean age of 58.3 ± 6.9 years in the SPC, and 59.9 ± 6.3 years in the FCT-group.

Persistence, measured as time to a treatment gap of 30 or 60 days or as the occurrence of a 30 days treatment gap within the study period, was higher under SPC. Time to treatment gap of 30 days resulted in HR 1.23 (95% CI: 1.15; 1.33, p < 0.001) and time to treatment gap of 60 days in HR 2.03 (95% CI: 1.77; 2.33; p < 0.001). The endpoint “30 days gap of treatment” resulted in OR 3.51 (95% CI: 3.06; 4.02; p = 0.001).

For the adherence variable PDC ≥ 80%, the OR were 1.78 (95% CI: 1.30; 2.45, p = 0.004) after 6 months and OR 1.85 (95% CI: 1.71; 2.37, p < 0.001) after ≥12 months in favor to SPC (Figs. 2, 3).

Fig. 2

Proportion-of-days-covered (PDC) ≥ 80% after 6 months

Fig. 3

Proportion-of-days-covered (PDC) ≥ 80% after ≥ 12 months

MPR after 12 months was significantly higher for the SPC formulations (OR 2.13; 95% CI: 1.30; 3.47, p < 0.0025). Difference in mean MPR at 12 months was also higher for SPC (MD 0.08, 95% CI: 0.03; 0.13, p = 0.0017).

The clinical outcome as measured by reaching individual blood pressure goals was found to be OR 1.22; 95% CI: 1.10–1.35, p < 0.001 for one publication.

While there was only a slight reduction in all-cause outpatient visits for SPC (SPC: vs FCT: 97.6% vs 97.9%, OR 0.89, 95% CI: 0.58–1.36, p = 0.58) and HTN-specific outpatient visits (SPC: vs FCT: 82.3% vs 82.4%, OR = 1.00, 95% CI 0.84–1.18, p = 0.97), HTN-specific hospitalization was about the same (SPC vs FCT: 0.7% vs 0.6, OR = 1.18, 95% CI 0.91 – 1.53, p = 0.21). Significant advantages for SPC were seen in the clinical outcomes all-cause hospitalisation (SPC vs FCT: 15.0% vs 18.2%, OR 0.79; 95% CI: 0.67–0.94, p = 0.009), all-cause emergency room visits (SPC vs FCT: 25.7% vs 31.4%, OR 0.75; 95% CI: 0.65–0.87, p = 0.0001) and hypertension related emergency room visits (SPC vs FCT: 9.7% vs 14.1%, OR 0.65; 95% CI: 0.54–0.80, p < 0.001).

Discussion

The results of our meta-analysis indicate that combining several agents for CVD treatment in one single pill could be an effective solution to reach treatment targets under conditions of daily practice. The main findings of this study were that a single pill combination was beneficial with regard to adherence, persistence, and clinical outcomes.

Clinical data indicate that initial combination therapy is beneficial in the treatment of arterial hypertension [20, 21]. Wald et al. conducted a meta-analysis of 42 clinical trials involving almost 11,000 patients. They found that combining any two drugs decreased blood pressure approximately 5 times greater than doubling the standard dose of one drug. The reduction in blood pressure with combined drugs was approximately 5 times greater than doubling the dose of one drug [6, 22]. In a recent study [23], blood pressure control with a fixed-dose triple combination therapy was superior to the free combination of the three drugs (perindopril/indapamide/amlodipine). Combination therapy seems to be mandatory to reach target blood pressure; the average number of drugs required to reach blood pressure goals amounted to more than 3 in trials focusing on cardiovascular morbidity and mortality [24]. However, low adherence to medication is a hurdle to reach these goals in daily practice, especially when patients suffer from comorbidities and intake of additional drugs is required. Chowdhury et al. performed a systematic review and meta-analysis of prospective epidemiological studies in 1,978,919 non-overlapping participants, with 135,627 CVD events and 94,126 cases of all-cause mortality. They found a poor adherence to CVD medication in 40% of patients and concluded, that a considerable proportion of all CVD events (~9% in Europe) could be attributed to poor adherence to vascular medications alone, and that the enhancement of adherence could help to maximize the potentials of effective cardiac therapies in the clinical setting [25].

In the present study, clinical trials were excluded from the analysis as patients are forced to be more compliant compared to everyday life. In an interventional study, less or no difference in compliance can be deduced due to the specific design of the study. Focusing on data from real world settings is more important because the differences between FCT and SPC therapy arise from the way medications are used, and patterns of medication used in clinical trials may not be generalizable. Andrade et al. compared the rates of drug discontinuation in primary care settings with the rates reported in clinical trials. The risks of discontinuation were substantially higher in the primary care settings than in randomized clinical trials [26].

To minimize bias, a rigorous selection of available studies has been performed. Selected studies needed to perform an exact substance comparison. Additionally, only outcomes that were clearly marked as adjusted for baseline conditions and confounders (e.g. by matching) were considered eligible. Among patients receiving antihypertensives or a combination of antihypertensive and cholesterol-lowering therapy, single pill treatment was associated with a significantly better adherence and better clinical outcomes compared with the identical lose substance combination under conditions of daily practice.

A clear benefit of SPC treatment strategy was seen on adherence, persistence, and clinical outcomes. First, there was evidence for a significant benefit of SPC over FCT on medication adherence measured either as PDC ≥ 80%, MPR ≥ 80% or mean PDC or MPR values. Differences between both treatment strategies could be demonstrated at 3 months, 6 months and ≥ 12 months. In most of the studies, the effect sizes were more evident after 12 months compared to 3 or 6 months, which is consistent with the common reasoning that an advantage of single pill combinations over LP—if existent—should increase over time. A limitation might be that we could not identify studies following our inclusion criteria with an observation period of more than 12 months. However, poor adherence already seems to be an issue immediately after initiation of CVD treatment. Chapman et al. conducted a retrospective cohort study in 8,406 enrollees in managed care who planned treatment with antihypertensive (AH) and lipid-lowering (LL) drugs. They measured adherence as PDC in 3-months intervals following initiation of concomitant therapy (mean follow-up, 12.9 months). Patients were considered adherent if they had filled prescriptions sufficient to cover at least 80% of days with both classes of medication. They found only 1 in 3 patients adherent to both medications after 6 months [27].

Heterogeneity between trials for each outcome was high and a major limitation of the study. We considered the different methods to determine persistence, analysed time points and specific basal characteristics for each trial as the most likely causes of this heterogeneity. However, each study showed superiority of SPC treatment regarding persistence. This was independent from the methods used or the time points investigated. Overall, both adherence and persistence were consistently higher for SPs.

We also investigated whether high adherence and persistence will result into better clinical outcomes. Ram et al. demonstrate a significant benefit of combination therapy with respect to the main goal of reaching the blood pressure target recommended by international guidelines [14]. This was supported by additional analyses regarding the mean change of systolic and diastolic blood pressure. Similarly, Kumagai et al. enrolled 196 patients with hypertension already being treated with FCT of angiotensin-II receptor blockers (ARB) and amlodipine. The FCT of ARB and amlodipine were replaced with the same dose of the SPC combinations. The average home measured blood pressure in all patients receiving SPC was significantly lower than those receiving FCT accompanied with increasing drug adherence [28].

With respect to clinical outcomes, Machnicki et al. showed a significant advantage of SPC treatment regarding hospitalizations, emergency room visits and hypertension-related emergency room visits. Thus, the positive effects on adherence and persistence were seen to be translated into clinical outcome and effectiveness parameters as well [17]. These findings are supported by a recent published study by Verma et al. [28]. They conducted a population-based retrospective cohort study of 13,350 individuals with up to 5 years of follow-up. Patients received an angiotensin-converting enzyme inhibitor (ACEI) or angiotensin II-receptor blocker (ARB) plus one thiazide diuretic. The authors conducted 2 analyses to examine the association between adherence and patient outcomes. First, they performed an on-treatment analysis to determine whether outcomes differed between groups while patients were on treatment. Second, they conducted an intention-to-treat analysis that followed individuals allowing for breaks in treatment to quantify the difference in drug adherence between groups and assessed its impact on clinical outcomes. They did not observe a significant difference in the primary outcome between groups in the on-treatment analysis. However, in the intention-to-treat analysis, the proportion of total follow-up days covered with medications was significantly higher in the SPC group than in the FCT, and the primary outcome was less frequent in SPC recipients [28]. This study prescribes a simple, but important rationale: 1. SPC improved medication intake 2. Improved medication intake enhances prognosis, 3. SPC improves prognosis.

The strict inclusion criteria of our study lead to a few limitations. Only four studies used ICD-codes for the identification of patients’ eligibility. All other studies identified eligible patients by prescription data only. This might lead to an additional variance as lipid lowering and antihypertensive drugs can be prescribed in various indications and for various reasons. Lipid lowering drugs can be prescribed in hypercholesterinaemia, in conditions of primary, secondary, and tertiary prevention; antihypertensive drugs in hypertension, coronary heart disease or heart failure. However, data gathered in this analysis have originally been adjusted for baseline characteristics and confounders and rigid criteria for study inclusion were applied to ensure correct statistical adjustment (e.g. matching). Although many studies could be identified that investigate the effects on adherence and persistence, it is a limitation that only a few studies were found to provide comparable outcome data for clinical outcomes and effectiveness. Unfortunately, it was not possible to do any subgroup analyses for men and women in order to consider differences in medication adherence due to a lack of data specific to gender.

Our analysis does not provide any safety data. Thus, any information about potential harmful effects of a SPC or FCT approach are missing. This should be considered by the planning of future studies.

“Drugs don’t work in patients, that do not take them”. This famous statement from C. Everett Koop, MD, an US General Surgeon given in 1985 sounds simple. However, the transfer of the reverse conclusion into daily practice does not seem to be that easy. The results of our analysis suggest that an SPC regimen could support patients to take their drugs which might easily to be implemented into daily practice. Certainly, the present meta-analysis gathered an important amount of information, but, at the same time, relevant limitations must be considered and a careful approach should be demanded to avoid misleading conclusions.

Conclusions

SPC improved medication adherence, persistence and clinical outcome parameter in patients suffering from hypertension and/or dyslipidemia compared to FCT under conditions of daily practice. The data of our analysis suggest that SPC could be a tool to maximize the potentials of effective cardiac therapies in the clinical setting.