Abstract

Both strict blood pressure (BP) control and improvements in BP profile such as BP variability are important for suppression of renal deterioration and cardiovascular complication in hypertension and chronic kidney disease (CKD). In the present study, we examined the beneficial effects of the single pill-based combination therapy of amlodipine and atorvastatin on achievement of the target BP and clinic BP profile, as well as markers of vascular and renal damages in twenty hypertensive CKD patients. The combination therapy with amlodipine and atorvastatin for 16 weeks significantly decreased clinic BP, and achievement of target BP control was attained in an average of 45% after the combination therapy in spite of the presence of no achievement at baseline. In addition, the combination therapy significantly decreased the within-visit BP variability. With respect to the effects on renal damage markers, combination therapy with amlodipine and atorvastatin for 16 weeks significantly decreased albuminuria (urine albumin-to-creatinine ratio, versus  mg/g-Cr, ) without decline in estimated glomerular filtration rate. Concerning parameters of vascular function, the combination therapy significantly improved both brachial-ankle pulse wave velocity (baPWV) and central systolic BP (cSBP) (baPWV, versus  cm/s, ; cSBP, versus  mmHg, ). Collectively, these results suggest that the combination therapy with amlodipine and atorvastatin may exert additional beneficial effects on renal and vascular damages as well as BP profile in addition to BP lowering in hypertension with CKD.

1. Introduction

Chronic kidney disease (CKD) patients are reportedly increasing in number, and cardiovascular complications are the most common cause of death in these patients. Thus, it would be a considerable advance in the management of this condition to elucidate the mechanisms involved in the renal deterioration and the cardiovascular events associated with hypertension complicated by CKD and to identify therapeutic approaches to treat them. Accumulated results of clinical trials also showed that strict control of blood pressure (BP) is essential to prevent target organ damage and to reduce cardiovascular mortality in hypertensive CKD patients [1, 2]. The dihydropyridine calcium channel blocker (CCB) is one of the first-line antihypertensive drugs for most patients with hypertension and is known to exert an efficient BP lowering effect and a strong inhibitory effect on cardiovascular events [3, 4].

In addition, therapies that lower lipid levels also slow the progression of atherosclerosis and reduce morbidity and mortality in patients with hypertension or atherosclerotic disease. The Anglo-Scandinavian Cardiac Outcomes Trial (ASCOT) demonstrated an additive benefit of combined antihypertensive and lipid-lowering therapy on the prevention of cardiovascular complication in high-risk hypertension [5]. Vascular dysfunction, with associated changes in endothelial function and vascular structure, is a risk factor for cardiovascular events through its contribution to the development of atherosclerotic vascular disease. Previous investigations demonstrated improved vascular function and arterial compliance with statins and several antihypertensive drugs such as renin-angiotensin system inhibitors and CCB [68]. Both amlodipine and atorvastatin have independently been noted to exert favorable effects on arterial compliance and endothelial dysfunction [8, 9]. This study aimed to examine the beneficial effects of single pill-based combination therapy with amlodipine and atorvastatin on clinic BP profile including within-visit BP variability, a recently emerging marker of linking between kidney and vasculature, and parameters of vascular and renal function in Japanese hypertensive CKD patients who did not achieve the target BP level according to the Japanese Society of Hypertension Guidelines for the Management of Hypertension (JSH2009) [10].

2. Materials and Methods

This study was conducted in accordance with the ethical principles of the Declaration of Helsinki and was approved by the Ethics Committees of Yokohama City University Hospital (UMIN 000009045; http://www.umin.ac.jp/ctr/). All of the patients provided written informed consent prior to the start of the study.

2.1. Study Participants and Design

Hypertensive patients with CKD who have already been treated with antihypertensive therapy were eligible for the study if they could not achieve the BP goal (clinic systolic BP ≥ 130 mmHg and/or diastolic BP ≥ 80 mmHg), and their low-density lipoprotein (LDL) cholesterol levels were 100 mg/dL or more. CKD was diagnosed by the presence for more than 3 months of albuminuria (urine albumin-to-creatinine ratio, UACR ≥ 30 mg/g-Cr), proteinuria (urine protein-to-creatinine ratio, UPCR ≥ 0.15 g/g-Cr), or estimated glomerular filtration rate (eGFR) < 60 mL/min/1.73 m2. We calculated the eGFR using a revised equation for the Japanese population: eGFR (mL/min/1.73 m2) = 194 × serum creatinine−1.094  × age−0.287  × 0.739 (if female) [11]. The exclusion criteria included CKD patients of G5 category, patients who were 19 years old or younger, women who were nursing or pregnant, clinically significant heart disease, stroke, renal artery stenosis, hepatic dysfunction, and known hypersensitivity to any ingredient in the study medications.

After the run-in period, eligible patients were given a single pill of amlodipine/atorvastatin tablet (CADUET, amlodipine besylate/atorvastatin calcium; 2.5/5, 2.5/10, 5/5, and 5/10 mg) for 16 weeks. The starting dose of the single amlodipine/atorvastatin tablet was determined according to each physician’s choice, and it was titrated up as needed to achieve the BP and lipid goal (clinic systolic BP < 130 mmHg, diastolic BP < 80 mmHg, and LDL-cholesterol < 100 mg/dL). If patients had already been treated with another calcium channel blocker or statin before the start of the study, they were switched to the single amlodipine/atorvastatin tablet of same dose during the run-in period. If the BP and lipid goal could not be achieved by maximum doses of amlodipine and atorvastatin (10 mg/day and 20 mg/day), another antihypertensive drug and lipid-lowering drug were considered to be added. The doses of other drugs such as oral glucose lowering agents and anticoagulant agents were not changed during the treatment period.

2.2. Clinic BP and Within-Visit BP Variability

The clinic BP was measured in sitting position using a calibrated standard mercury sphygmomanometer and the recommended cuff size [12]. Three measurements were taken at 1-minute interval, and their average was regarded as the clinic BP. Within-visit BP variability, which has been reported to be associated with the risk of stroke and cardiovascular risk factors [13, 14], is defined as the within-patient standard deviation (SD) of three measurements of clinic systolic and diastolic BP (within-visit BP variability, SD) and those divided by the each mean clinic BP (within-visit BP variability, CV%).

2.3. Central Hemodynamics

The central systolic blood pressure (cSBP) and augmentation index (AI) were measured using an HEM-9000AI (Omron Healthcare, Kyoto, Japan) with an automatic tonometry probe wrapped onto the wrist to record radial waveforms, which were calibrated against the contralateral arm cuff brachial BP taken immediately after tonometry. An algorithm based on a linear regression model was then applied to estimate the cSBP from the “late systolic shoulder” (pSBP2) of the radial pulse waveform, which has been shown to closely agree with the cSBP [1518]. This device uses the maxima of the “multidimensional derivatives” on the recorded pressure waveforms to detect the first and second inflection points corresponding to the early and late systolic (pSBP2) pressure readings.

2.4. Brachial-Ankle Pulse Wave Velocity (baPWV)

The baPWV values were determined by a PP analyzer (model: BP-203RPE2; Omron Healthcare, Kyoto, Japan), as described previously [1921]. The baPWV values obtained by this method are reported to be significantly correlated with the aortic PWV determined by the catheter method [22].

2.5. Laboratory Measurements

Blood and urine sampling were performed in fasted state at baseline and after a period of 16-week treatment, respectively. All parameters were determined by routine methods in the Department of Clinical Chemistry, Yokohama City University School Hospital.

2.6. Statistical Analysis

All data were presented as the mean ± SD or as a percentage. For the statistical analysis of the difference between baseline and 16 weeks of treatment, analysis of variance was compared by a paired comparison -test. Univariate and multivariate linear regression analyses were performed to identify the factors affecting the changes in cSBP and UACR. The independent variables entered into the multivariate model were those that were significantly associated in the univariate analyses or were significantly different after a period of 16-week treatment. Analysis was performed using SPSS version 19.0 (IBM Corporation), and a value of was considered statistically significant.

3. Results

3.1. Baseline Patient Characteristics

Table 1 shows the baseline characteristics of the total 20 hypertensive CKD patients enrolled from September, 2012, to November, 2013. The causes of CKD were hypertensive nephrosclerosis (), diabetic nephropathy (), chronic glomerulonephritis (), and obstructive nephropathy due to urinary tract stones (). None of the enrolled patients discontinued participation in the study. Mean age was years, and the number of males and females was 14 and 6, respectively. Body mass index was  kg/m2, suggesting that the participants correspond to obese hypertensive patients as a whole. With respect to BP control, clinic BP did not at all achieve the target BP level according to the JSH2009 guideline (clinic SBP/DBP / mm Hg) [10].

3.2. Effects of Combination Therapy with Amlodipine and Atorvastatin on BP Profile, Glucose and Lipid Metabolism, and Inflammatory and Oxidative Stress Markers

As a whole, the combination therapy with amlodipine and atorvastatin for 16 weeks significantly decreased clinic SBP and DBP (Table 2), and clinic pulse rate was also reduced by the combination therapy (Table 2). In addition, achievement of target BP control, which was defined as BP values less than 130/80 mmHg for CKD patients according to the JSH2009, was attained in an average of 45% after the combination therapy in spite of the presence of no achievement at baseline. Furthermore, the combination therapy significantly decreased the within-visit SBP and DBP variability (BP-SD and BP-CV) (Table 2).

With respect to the glucose and lipid metabolism, the combination therapy with amlodipine and atorvastatin significantly lowered total and LDL-cholesterol levels, without evident changes in parameters of glucose metabolism and inflammation (Table 3). In addition, achievement of the lipid goal, which was defined as LDL-cholesterol level less than 100 mg/dL, was attained in an average of 70% after the combination therapy in spite of the presence of no achievement at baseline. On the other hand, the serum pentosidine level was significantly increased by the combination therapy (Table 3). During a period of 16-week treatment, only two patients who could not achieve the BP goal by the maximum dose of amlodipine (10 mg/day) were additionally administered valsartan 80 mg/day and hydrochlorothiazide 12.5 mg/day, respectively. On the other hand, none of patients was additionally administered lipid-lowering drugs other than atorvastatin. The average doses of amlodipine and atorvastatin were  mg/day and  mg/day, respectively.

3.3. Effects of Combination Therapy with Amlodipine and Atorvastatin on Renal and Vascular Function Parameters

Combination therapy with amlodipine and atorvastatin for 16 weeks significantly decreased UACR (Table 4; UACR, versus  mg/g-Cr, ). In addition, the reduction of UACR by the combination therapy was not accompanied with decline in eGFR (Table 4; eGFR, versus  mL/min/1.73 m2). Concerning parameters of vascular function, the combination therapy with amlodipine and atorvastatin for 16 weeks significantly improved both baPWV and cSBP (Table 4; baPWV, 1903 ± 353 versus  cm/s, ; cSBP, versus  mmHg, ).

3.4. Multivariate Regression Analysis for Assessment of Factors Contributing to Improvements in Central BP and Albuminuria

Multivariate regression analysis of the independent variables, which showed significant correlations in the univariate analyses or were significantly different after a period of 16-week treatment, indicated that there were significant associations between the changes in cSBP and those in SBP and total cholesterol and changes in UACR and those in serum creatinine and total cholesterol (Table 5).

4. Discussion

The main finding of this study was that the single pill-based administration for combinatorial antihypertensive and LDL cholesterol-lowering therapy with amlodipine and atorvastatin successfully decreased clinic BP so as to improve the achievement of target BP in hypertensive CKD patients already being treated before the start of the combination therapy. In addition, the combination therapy was able to significantly reduce UACR without decrease in eGFR and resulted in significant improvements in vascular function and lipid metabolism. These pleiotropic therapeutic effects by combination therapy with amlodipine and atorvastatin on biomarkers of renal and vascular damage deserve further discussion.

Recent clinical guidelines for hypertensive patients recommend combination therapy such as renin-angiotensin system inhibitors and CCB or diuretics, and, in this study, the combination therapy with amlodipine and atorvastatin was effective for efficient lowering of clinic BP and inhibition of within-visit BP variability in Japanese hypertensive CKD patients. With respect to BP-lowering efficacy of amlodipine, we previously showed that the amlodipine add-on group exerted greater reductions of clinic BP and home BP than the ARB add-on group [23].

Accumulated evidence indicates that renin-angiotensin system inhibitors such as ARB and ACE inhibitors are able to improve albuminuria better than CCB such as amlodipine through the reduction of intraglomerular pressure [24]. However, the combination therapy with amlodipine and atorvastatin exerted a significant reduction in albuminuria in the present study. Of note, in multivariate analysis, the decrease in total-cholesterol level was an independent contributing factor to the decrease in UACR. This result suggests that statin therapy may have a favorable effect on albuminuria and is confirmed with previous studies [2528].

A previous study showed that the decreases in BP significantly contributed to the decreases in albuminuria by CCB in hypertensive and CKD patients [23, 29]. Although analysis of patient characteristics at baseline unexpectedly revealed that all participants were already treated with CCB in spite of only 30% of the participants being treated with statin, the combination therapy with amlodipine and atorvastatin for 16 weeks succeeded to efficiently suppress albuminuria, irrespective of preceding medication, without further decline in eGFR. This is likely to be an important advantage of the combination therapy with amlodipine and atorvastatin, since several recent epidemiological studies and intervention trials demonstrated that efficient reduction of albuminuria with preserved eGFR is important to inhibit the progression of CKD and to prevent the development of cardiovascular complication [3032].

The combination therapy with amlodipine and atorvastatin exhibited a significant improvement in vascular functional parameters such as baPWV and cSBP in this study. A previous study showed that the add-on amlodipine therapy had benefits in terms of the vascular function and vascular structure of hypertensive patients already treated with renin-angiotensin inhibitors, which were independent of its depressor effects but with a concomitant decrease in ambulatory BP variability [33]. Also, these results are consistent with a previous study showing that coadministered amlodipine and atorvastatin produced early improvements in arterial wall compliance in hypertensive patients with dyslipidemia [34]. Since statins may exert their vascular beneficial effects by inhibiting small GTPase protein synthesis, such as Ras and Rho kinase [35, 36], the combination therapy of amlodipine and atorvastatin may have an additive beneficial effect on the vasculature so as to improve vascular atherosclerotic changes [8, 9].

Recently, parameters of BP variability obtained by clinic BP measurement are suggested to be associated with target organ damage including CKD and cardiovascular complication [3739]. Variation in BP that is captured at sequential office visits is called visit-to-visit variability, and BP variation that is captured within each office visit is called within-visit BP variability. Accumulated evidence has indicated that greater degrees of clinic BP variability such as visit-to-visit BP variability and within-visit BP variability are associated with renal deterioration and cardiovascular complication [14, 3740]. Almost all reported results showed that these parameters of BP variability, such as clinic BP variability and home-measured BP variability in addition to ambulatory BP variability, reflect organ damages and are potential predictors of cardiovascular events [37, 41, 42]. Furthermore, these analyses also displayed that CCB is the most effective drug class for reduction of BP variability [43].

A recent study showed that alteration of vascular function is an important factor in the correlation between clinic BP variability and cardiovascular disease [44], and clinic BP variability is recently suggested to correlate significantly with renal function and renal arteriosclerotic change as an emerging candidate of linking factor between vascular alteration and renal damage [38]. The results of the present study demonstrated that the combination therapy with amlodipine and atorvastatin significantly decreased clinic BP and its variability concomitant with improvements in parameters of vascular and renal function. In the present study, there was no significant relationship between the improvement in lipid metabolism and that in clinic BP and within-visit BP variability on univariate analysis (data not shown). Therefore, the association between statin therapy and BP or BP variability is still to be determined in the future study.

In the present study, pulse rate was significantly decreased by combination therapy of amlodipine and atorvastatin in spite of BP reduction. It has been reported that amlodipine tends to increase pulse rate via the reflex stimulation of sympathetic nervous system [45]. On the other hand, there are several previous studies suggesting that statins can reduce sympathetic activity, thereby resulting in pulse rate reduction [46, 47]. Thus, the decrease in pulse rate may be caused by concomitant statin therapy. However, since there is no direct data which support this possibility in the present study, further investigation is needed to elucidate this issue.

There are several limitations in the present study. Firstly, the present study is not randomized parallel-group control trial, and the numbers are small. Secondly, the patient’s adherence was not examined in the present study. Since there are several previous studies suggesting that single-pill amlodipine/atorvastatin rather than 2-pill regimen may reduce cardiovascular events by improving the patient’s adherence [48, 49], the improving effect of single-pill amlodipine/atorvastatin therapy on patient’s adherence may have an influence on the results of this study. Further studies are needed to estimate the true long-term advantage of the amlodipine/atorvastatin combination in lowering blood pressure and improve vascular damage.

5. Conclusions

In summary, the results of the present study suggest that the combination therapy with amlodipine and atorvastatin may exert additional beneficial effects on renal and vascular damages as well as BP profile in addition to BP lowering in hypertension with CKD.

Disclosure

Kouichi Tamura received honoraria, consulting fees, or funds from Novartis, Takeda, Daiichi-Sankyo, Dainippon-Sumitomo, Kyowa-Hakko Kirin, Chugai, Shionogi, Boehringer Ingelheim, Astellas, Mochida, Pfizer, and Mitsubishi Tanabe.

Conflict of Interests

The authors declare that there is no conflict of interests regarding the publication of this paper.

Authors’ Contribution

Kengo Azushima and Kazushi Uneda equally contributed to this work.

Acknowledgments

This work was supported by a Health and Labor Sciences Research grant and by Grants from the Japanese Ministry of Education, Science, Sports and Culture, the Salt Science Research Foundation (nos. 1134 and 1428), the Yokohama Foundation for Advancement of Medical Science, the Kidney Foundation, Japan (JKFB13-17), and the Novartis Foundation for Gerontological Research (2012).