Vol 29, No 2 (2022)
Original articles — Clinical cardiology
Published online: 2020-04-22

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Influence of lipid profile and statin administration on arterial stiffness in renal transplant recipients

Zbigniew T. Heleniak1, Sarah Illersperger2, Susanne Brakemeier2, Alicja Dębska-Ślizień1, Paul Bach3, Klemens Budde2, Fabian Halleck2
Pubmed: 32329037
Cardiol J 2022;29(2):263-271.

Abstract

Background: Hyperlipidemia is one of the major risk factors for developing a cardiovascular disease (CVD) and it is a frequent post-transplant complication, occurring in up to 60% of the renal transplant recipients (RTRs). Lipid lowering therapy with HMG-CoA reductase inhibitors (statins) is generally recommended and may reduce the overall cardiovascular risk. The aim of this study was to evaluate the lipid profile, statin administration and their relationship with arterial stiffness parameters in RTRs.
Methods: Three hundred and forty-four stable RTRs (62.5% male) transplanted between 1994 and 2018 were randomly enrolled to the study. The following parameters of arterial stiffness was measured in each patient: ankle brachial index, carotid femoral pulse wave velocity (baPWV left and right, cfPWV) and pulse pressure (PP right and left). The study group was divided based on the use statins: 143 (41.6%) and 201 (58.4%). RTRs were qualified to the statin (+) and the statin (–) group, respectively.
Results: In the statin (+) as compared to statin (–) group there were more patients with a CVD (32.9% vs. 14.9%) and diabetes (25.2% vs. 14.4%). In the whole study group, CVD was associated with a significant increase of both baPWV and cfPWV as well as PP (8.5 mmHg). There were significant differences in arterial stiffness parameters (baPWV, cfPWV, PP) between the statin (+) and the statin (–) group.
Conclusions: Arterial stiffness was increased in RTRs with CVD and hyperlipidemia. The control of hyperlipidemia was poor in RTRs.

Original article

clinical cardiology

Cardiology Journal 2022, Vol. 29, No. 2, 263–271

DOI: 10.5603/CJ.a2020.0063

Copyright © 2022 Via Medica

ISSN 1897–5593

eISSN 1898018X

Influence of lipid profile and statin administration on arterial stiffness in renal transplant recipients

Zbigniew T. Heleniak1Sarah Illersperger2Susanne Brakemeier2Alicja Dębska-Ślizień1Paul Bach3Klemens Budde2Fabian Halleck2
1Department of Nephrology, Transplantology and Internal Medicine, Medical University of Gdansk, Poland
2Medizinische Klinik mit Schwerpunkt Nephrologie und Internistische Intensivmedizin, Charité – Universitätsmedizin, Berlin, Germany
3Institut für Biometrie und Klinische Epidemiologie, Charité – Universitätsmedizin, Berlin, Germany

Address for correspondence: Dr. Zbigniew T. Heleniak, Department of Nephrology, Transplantology and Internal Medicine, Medical University of Gdansk, ul. Dębinki 7, 80–952 Gdańsk, Poland, tel: +48 502 987 604, fax: +48 58 345 25 51, e-mail: zbigniew.heleniak@gumed.edu.pl

Received: 13.12.2019 Accepted: 15.02.2020 Early publication date: 22.04.2020

This article is available in open access under Creative Common Attribution-Non-Commercial-No Derivatives 4.0 International (CC BY-NC-ND 4.0) license, allowing to download articles and share them with others as long as they credit the authors and the publisher, but without permission to change them in any way or use them commercially.

Abstract
Background: Hyperlipidemia is one of the major risk factors for developing a cardiovascular disease (CVD) and it is a frequent post-transplant complication, occurring in up to 60% of the renal transplant recipients (RTRs). Lipid lowering therapy with HMG-CoA reductase inhibitors (statins) is generally recommended and may reduce the overall cardiovascular risk. The aim of this study was to evaluate the lipid profile, statin administration and their relationship with arterial stiffness parameters in RTRs.
Methods: Three hundred and forty-four stable RTRs (62.5% male) transplanted between 1994 and 2018 were randomly enrolled to the study. The following parameters of arterial stiffness was measured in each patient: ankle brachial index, carotid femoral pulse wave velocity (baPWV left and right, cfPWV) and pulse pressure (PP right and left). The study group was divided based on the use statins: 143 (41.6%) and 201 (58.4%). RTRs were qualified to the statin (+) and the statin (–) group, respectively.
Results: In the statin (+) as compared to statin (–) group there were more patients with a CVD (32.9% vs. 14.9%) and diabetes (25.2% vs. 14.4%). In the whole study group, CVD was associated with a significant increase of both baPWV and cfPWV as well as PP (8.5 mmHg). There were significant differences in arterial stiffness parameters (baPWV, cfPWV, PP) between the statin (+) and the statin (–) group.
Conclusions: Arterial stiffness was increased in RTRs with CVD and hyperlipidemia. The control of hyperlipidemia was poor in RTRs. (Cardiol J 2022; 29, 2: 263–271)
Key words: arterial stiffness, kidney transplantation, statin, hyperlipidemia

Introduction

In spite of the improvement in rejection rates long-term survival in renal transplant recipients (RTRs) has remained unchanged and cardiovascular disease (CVDs) are a major cause of death in this patient population [1, 2]. Moreover, hyperlipidemia is the major cardiovascular (CV) risk factor and is a frequent post-transplant complication, occurring in up to 60% of the patients [1, 3, 4]. Lipid lowering therapy statins reduce the CV risk in patients after kidney transplantation [5, 6].

Saran et al. [7] showed that: “the occurrence of CVDs in kidney transplant recipients is affected not only by the traditional risk factors but also by immunosuppressive therapy, earlier dialysis therapy, proteinuria, inflammation or anemia”. All these factors lead to increased arterial stiffness [8, 9].

Carotid-femoral pulse wave velocity (PWV), as an arterial stiffness parameter, is an independent predictor of CV complications in the general population and high CV patients [10, 11]. Statins treatment mitigates an arterial stiffness, beyond their effects on the lipid profile [10]. Additionally, lipid lowering treatment has pleiotropic effects by enhancing nitric oxide bioavailability, antioxidant effect, and interaction with the renin–angiotensin–aldosterone (RAA) system [10, 12]. There are no essential data available concerning the influence of statins on arterial stiffness in RTRs. The main aim of the study was to evaluate the lipid profile, statin administration and their relationship to arterial stiffness parameters in renal transplant recipients.

Methods

This cross-sectional study enrolled 344 stable RTRs, transplanted between 1994 and 2018, who attended the outpatient unit of the Department of Nephrology Charité – Universitätsmedizin Berlin, Germany, between February and July 2018.

Patients gave their written informed consent. The study was conducted in accordance with the Declaration of Helsinki.

Demographic and clinical information including: renal transplant, CV and diabetic status was analyzed. Additionally, the immunosuppressive protocol, hypertensive and statin treatment were assessed. Data concerning serum creatinine, potassium concentration, hemoglobin, proteinuria, albuminuria and lipids levels refer to a single assessment obtained from medical files of patients.

Furthermore, we investigated the following parameters of arterial stiffness: brachial ankle and carotid femoral pulse wave velocity (baPWV left and right, cfPWV), ankle brachial index (ABI) and also blood pressure (BP), pulse pressure (PP) in each patient using ABI system 100 (Boso Bosch and Sohn, Germany). Additionally, pulsatile stress test (left and right), as a marker of arterial stiffness was assessed using the equation: pulsatile stress test = heart rate × pulse pressure.

Statistical analyses

Statistical analyses were performed using the STATSTICA 13.3 PL for Windows software package. Categorical variables are presented as absolute numbers (percentages). Continuous variables are presented as mean value ± standard deviation (SD) or as median and interquartile range (IQR) for highly skewed variables. Differences in the distribution of continuous variables were assessed using the two-sample t-test or the Mann-Whitney U-test, respectively. The c2 test was used for the categorical variables. Correlation coefficients were calculated using the Spearman test. Additionally, a simple linear regression model was used to model the relationship between a scalar response (or dependent variable) and one or more explanatory variables (or independent variables). The Shapiro-Wilk test was used to assess normality. In all statistical tests, a p-value < 0.05 was considered as statistically significant.

Results

Overall, 344 stable patients were enrolled to the study. The definition of stable patient included: constant level of creatinine and immunosuppressive drugs in the blood and the lack of any CV events during 6 and 12 months before enrolment to the study, respectively.

The study population was divided in two groups based on the statin application. 143 (41.6%) and 201 (58.4%) were qualified to the group statin (+) and statin (–), respectively. Overall, 86% of the RTRs under statin treatment received fluvastatin in a mean dose of 44.7 mg/day (55.9% of the maximal dose). 7% used pravastatin in a mean dose of 30 mg (75% of the maximal dose), 4.9% used atorvastatin in a mean dose of 35.7 mg (44.6% of the maximal dose) and 2.1% used simvastatin in a mean dose of 23.3 mg (58.2% of maximal dose).

Study population characteristics

In the group of statins (+) as compared to statin (–) there were more patients with CV (32.9% vs. 14.9%, p < 0.05) and diabetes (25.2% vs. 14.4%, p = NS). There were more males and the average body mass index (BMI) was higher in the statin (+) group (p < 0.05). The general characteristics of the study participants are summarized in Table 1.

Table 1. Characteristics of the study population.

Total study population

Statin (+)

Statin ()

P

RTRs

344

143 (41.6%)

201 (58.4%)

< 0.05

Sex: men

215 (62.5%)

94 (65.7%)

121 (60.2%)

< 0.05

Age [years]

52.7 ± 13.9

56.7 ± 12.0

49.8 ± 14.4

NS

Body mass index [kg/m2]

25.62 ± 4.78

29.91 ± 5.11

24.69 ± 4.31

< 0.05

Weight [kg]

76.16 ± 17.22

79.83 ± 17.65

73.53 ± 16.44

< 0.05

Diabetes mellitus (any type 1, 2, NODAT)

64 (18.6%)

36 (25.2%)

29 (14.4%)

NS

Cardiovascular disease (CAD, POAD)

77 (22.4%)

47 (32.9%)

30(14.9%)

< 0.05

Hypertension

298 (86.6%)

126 (88.1%)

172 (85.5%)

NS

Reasons of ESRD and KTx:

Primary glomerulonephritis

186 (54.1%)

73 (55.0%)

113 (56.2%)

NS

Diabetic nephropathy

5 (1.5%)

1 (0.7%)

4 (2%)

NS

Polycystic kidney disease

56 (16.3%)

26 (18.2%)

30 (14.9%)

NS

Tubulointerstitial nephritis

70 (20.3%)

30 (20.9%)

40 (20%)

NS

Hypertensive nephropathy

18 (5.2%)

11 (7.7%)

7 (3.5%)

NS

Unknown etiology

10 (2.9%)

2 (1.4%)

8 (4%)

NS

Time of RRT [months]

58.5 (19–97)

48 (14–83)

44 (6–94)

NS

Time after KTx [months]

73 (28–140)

88 (46–161)

51 (12–89)

< 0.05

Preemptive KTx

46 (13.4%)

17 (11.9%)

29 (14.4%)

NS

Serum creatinine level [mg/dL]

1.47 (1.19–1.92)

1.56 (1.18–2.06)

1.44 (1.19–1.85)

NS

eGFR CKD-EPI [mL/min/1.73 m2]

50.4 ± 19.8

47.4 ± 19.9

52.4 ± 19.5

< 0.05

Potassium [mmol/L]

4.3 ± 0.6

4.3 ± 0.58

4.3 ± 0.56

NS

Hemoglobin [g/dL]

12.7 ± 1.7

12.9 ± 1.8

12.6 ± 1.7

NS

Total cholesterol [mg/dL]

195 (164–222)

198 (168–222)

191 (162–221)

NS

LDL [mg/dL]

122 (99–146)

120 (100–139)

123 (98–149)

NS

HDL [mg/dL]

51 (42–64)

48 (39–63)

53 (44–66)

< 0.05

Non-HDL [mg/dL]

138 (113–166)

145 (119–171)

134 (107–165)

< 0.05

Triglycerides [mg/dL]

155 (113–221)

185 (128–256)

137 (106–195)

<0.05

LDL < 100 mg/dL

93 (27%)

38 (26.6%)

55 (27.4%)

NS

Non-HDL < 130 mg/dL

147 (42.7%)

54 (38.3%)

93 (46.3%)

< 0.05

Triglycerides < 150 mg/dL

168 (48.8%)

52 (36.4%)

116 (57.7%)

< 0.05

Albumin [g/L]

43.46 ± 3.28

43.59 ± 3.12

43.64 ± 3.09

NS

Albuminuria [mg/day]

41.5 (9.3–145)

31 (8–176)

45 (11–145)

NS

Proteinuria [mg/day]

171 (114–380)

172 (108–365)

170 (120–385)

NS

Albuminuria [mg/g] creatinine

49 (15–156)

60 (15–203)

48 (15–136)

NS

Proteinuria [mg/g] creatinine

138 (84–322)

137 (88–357)

138 (82–321)

NS

Cyclosporine

73 (21.2%)

39 (27.3%)

34 (16.9%)

< 0.05

Tacrolimus

212 (61.6%)

69 (48.2%)

143 (71.1%)

< 0.05

Steroids

176 (51.2%)

68 (47.5%)

108 (53.4 %)

NS

Mycophenolate mofetil

150 (43.6%)

78 (36.4%)

98 (48.7%)

< 0.05

Mycophenolate sodium

171 (49.7%)

107 (54.5%)

93 (46.3%)

NS

Azathioprin

5 (1.5%)

4 (2.8%)

1 (0.5%)

NS

mTOR

10 (2.9%)

6 (4.2%)

4 (2%)

NS

Belatacept

41 (11.9%)

25 (17.5%)

16 (8%)

< 0.05

RAA system blockade

204 (59.3%)

94 (65.7%)

110 (54.7%)

< 0.05

Calcium channel blockers

158 (45.9%)

71 (49.6 %)

87 (43.3 %)

NS

Beta-blockers

241 (70.1%)

119 (83.2%)

124 (61.7%)

< 0.05

Diuretics

120 (34.9%)

72 (50.3%)

48 (23.9%)

< 0.05

Erythropoietin stimulating agent

47 (13.7%)

31 (21.7%)

36 (17.9%)

NS

Table 2. Arterial stiffness parameters and blood pressure in the study population.

Total study population

Statin (+)

Statin ()

P

baPWV right [m/s]

11.8 (10.7–13.3)

12.0 (10.0–13.7)

11.7 (10.6–12.9)

< 0.05

baPWV left [m/s]

12.0 (10.9–13.5)

12.3 (11.2–14.4)

11.7 (10.6–13.0)

< 0.05

cfPWV [m/s]

7.9 (6.9–9.5)

8.1 (7–9.8)

7.7 (6.7–9.2)

< 0.05

SBP right arm [mmHg]

140.7 ± 17.7

143.8 ± 18.2

138.5 ± 17

< 0.05

SBP left arm [mmHg]

139.6 ± 20.1

142.7 ± 20.4

137.4 ± 19.7

< 0.05

DBP right arm [mmHg]

85.8 ± 10.3

86.5 ± 10.0

85.4 ± 10.4

NS

DBP left arm [mmHg]

85.7 ± 10.9

86.2 ± 10.2

85.2 ± 10.9

NS

PP right arm [mmHg]

54.6 ± 14.7

56.8 ± 15.0

53.1 ± 14.3

< 0.05

PP left arm [mmHg]

54.0 ± 15.9

56.5 ± 15.7

52.1 ± 15.9

< 0.05

Pulsatile stress right

3521 ± 1012

3599 ± 994

3469 ± 1024

< 0.05

Pulsatile stress left

3520 ± 1225

3611 ± 1258

3454 ± 1202

< 0.05

ABI right

1.08 ± 0.17

1.08 ± 0.23

1.09 ± 0.10

NS

ABI left

1.09 ± 0.13

1.07 ± 0.16

1.10 ± 0.11

NS

Table 3. Arterial stiffness parameters and blood pressure in groups with different level of lowdensity lipoprotein (LDL) cholesterol.

LDL ≥ 100 mg/dL

LDL < 100 mg/dL

P

Renal transplant recipients

251

93

< 0.05

SBP right arm [mmHg]

141.9 ± 17.3

137.1 ± 18.2

< 0.05

SBP left arm [mmHg]

141.9 ± 15.3

133.6 ± 19.7

< 0.05

DBP right arm [mmHg]

86.1 ± 10.6

85.2 ± 9.1

NS

DBP left arm [mmHg]

86.8 ± 10.2

82.5 ± 12.4

< 0.05

Pulse pressure right

55.8 ± 15.3

51.2 ±12.4

< 0.05

Pulse pressure left

55.1 ± 16.3

51.1 ± 14.3

0.07

ABI right

1.08 ± 0.17

1.10 ± 0.18

NS

ABI left

1.08 ± 0.11

1.11 ± 0.17

NS

Pulsatile stress right

3603 ± 1054

3291 ± 853

< 0.05

Pulsatile stress left

3324 ± 1274

3256 ± 1050

< 0.05

baPWV right [m/s]

11.8 (10.8–13.5)

11.6 (10.6–13.3)

NS

baPWV left [m/s]

12.0 (10.9–13.8)

11.8 (10.7–13.1)

NS

cfPWV [m/s]

8.0 (7–9.5)

7.5 (6.6–8.7)

< 0.05

Table 4. Arterial stiffness parameters and blood pressure in groups with different level of non–high density lipoprotein (HDL) cholesterol.

Non–HDL ≥ 130 mg/dL

Non–HDL < 130 mg/dL

P

Renal transplant recipients

195

149

SBP right arm [mmHg]

142.4 ± 17.3

138.1 ± 17.8

NS

SBP left arm [mmHg]

143.1 ± 19.1

134.7 ± 19.2

< 0.05

DBP right arm [mmHg]

86.0 ± 10.0

85.4 ± 10.6

NS

DBP left arm [mmHg]

87.1 ± 10.4

83.5 ± 11

< 0.05

Pulse pressure right

56.3 ± 15.4

52.2 ±12.9

0.07

Pulse pressure left

56.1 ± 16.3

51.2 ± 14.9

< 0.05

ABI right

1.07 ± 0.11

1.10 ± 0.23

NS

ABI left

1.08 ± 0.12

1.10 ± 0.14

NS

Pulsatile stress right

3626 ± 1119

3382 ± 843

NS

Pulsatile stress left

3650 ± 1332

3344 ± 1058

NS

baPWV right [m/s]

12.0 (11.0–13.3)

11.7 (10.5–13.3)

NS

baPWV left [m/s]

12.0 (10.9–13.5)

11.9 (10.6–13.8)

NS

cfPWV [m/s]

8.0 (7.2–9.4)

7.6 (6.6–9.5)

NS

Table 5. Arterial stiffness parameters and blood pressure in groups with different level of triglicerydes.

Triglicerydes ≥ 150 mg/dL

Triglicerydes < 150 mg/dL

P

Renal transplant recipients

175

169

NS

SBP right arm [mmHg]

141.5 ± 17.3

139.6 ± 17.9

NS

SBP left arm [mmHg]

140.4 ± 18.4

138.5 ± 21.5

NS

DBP right arm [mmHg]

86.6 ± 10.0

85.9 ± 10.5

NS

DBP left arm [mmHg]

86.3 ± 10.1

84.8 ± 11.4

NS

Pulse pressure right

55.8 ± 15.3

53.2 ±13.9

NS

Pulse pressure left

54.2 ± 15,1

53.6 ± 16.8

NS

ABI right

1.08 ± 0.10

1.09 ± 0.22

NS

ABI left

1.08 ± 0.10

1.10 ± 0.15

NS

Pulsatile stress right

3578 ± 1056

3382 ± 843

NS

Pulsatile stress left

3511 ± 1164

3344 ± 1058

NS

baPWV right [m/s]

11.8 (11.0–13.7)

11.7 (10.5–12.9)

NS

baPWV left [m/s]

12.3 (11.2–13.8)

11.6 (10.6–13.2)

< 0.05

cfPWV [m/s]

8.0 (7.0–9.8)

7.6 (6.7–9.1)

< 0.05

The main causes of end stage renal disease (ESRD) in the study population were glomerulonephritis (the majority were biopsy proven, but the histopathological results weren’t available in patient’s files), tubulointerstitial nephropathy and polycystic kidney disease. In the statin (+) group the average serum creatinine was higher and estimated glomerular filtration rate (eGFR; CKD-EPI) was significantly lower as compared to the statin (–) group (p < 0.05). The level of albumin in the blood, proteinuria and albuminuria were similar in the statin (+) and (–) groups.

The groups did not differ significantly with respect to the time of renal replacement therapy before transplantation, but the time after transplantation was longer (88 vs. 51 months, p < 0.05) in the statin (+) group.

Immunosuppressive regimen in the study population

Calcineurin inhibitors were used in 82.8% of the study population. Cyclosporine was administered in 27.3% vs. 16.9% (p < 0.05) and tacrolimus in 48.2% vs. 71.1% (p < 0.05) of the patients in the statin (+) and (–) group, respectively. 36.4% vs. 48.7% of the participants used mycophenolate mofetil (MMF) in the statin (+) and (–) group, respectively. No significant differences were observed in terms of MMF/mycophenolate sodium (MPS), azathioprin and mammalian target of rapamycin (mTOR) agents between both groups. In the statin (+) cohort more patients received belatacept 17.5% vs. 8% (p < 0.05). In 59.3% of the participants RAA blockers were implemented. In the statin (+) and (–) group 65.7% vs. 54.7% of the patients received RAA blockers (p < 0.05). Beta-blockers and diuretics were prescribed more often in the statin (+) group (p < 0.05).

The control and treatment of hypertension

The control of systolic BP (SBP) and diastolic BP (DBP) was significantly worse in the statin (+) group (p < 0.05). Moreover, PP value was higher in statin (+) patients (Table 2).

In group with lipid parameters as: low density lipoprotein (LDL) ≥ 100 mg/dL and non-high density lipoprotein (non-HDL) ≥ 130 mg/dL; SBP (p < 0.05), DBP (p = NS) and PP (p < 0.05) were higher as compare to group with LDL < 100 mg/dL and non-HDL < 130 mg/dL, respectively. The differences in SBP, DBP and PP value did not differ significantly between patients with the level of triglycerides ≥ 150 mg/dL and < 150 mg/dL. The statin (+) participants used significantly more RAA blockers, beta-blockers and diuretics (p < 0.05). No difference in terms of calcium channel blockers administration were noticed.

Lipid parameters in study group

The level of non-HDL and triglycerides was higher (p < 0.05) in the statin (+) group. No differences in total and LDL cholesterol (LDL-C) levels between statin (+) and statin (–) were observed. The values of HDL-cholesterol (HDL-C) differed significantly in statin (+) and statin (–) groups (48 vs. 53 mg/dL; p < 0.05).

The aim of treatment of hyperlipidemia (LDL < 100 mg/dL) was achieved in 26.6% vs. 27.4% (p = NS) in statin (+) and statin (–) groups, respectively. In 38.3% vs. 46.3% of patients (p < 0.05) in statin (+) and statin (–) groups, non-HDL < 130 mg/dL was observed.

Arterial stiffness in study group

The values of arterial stiffness parameters (baPWV, cfPWV, PP, pulsatile stress test) and SBP were higher (p < 0.05) in the statin (+) as compared to the statin (–) group. There were no differences in terms of DBP and ABI between both groups (Table 2).

Lipids, blood pressure and arterial stiffness parameters

Patients with LDL-C level < 100 mg/dL, had better control of SBP and DBP (p < 0.05) as compared to LDL-C ≥ 100 mg/dL. There were significantly lower values of arterial stiffness parameters (PP, pulsatile stress test and cfPWV) in the group with LDL < 100 mg/dL (p < 0.05). No differences were observed for ABI and baPWV (Table 3).

In the group with non-HDL-C ≥ 130 mg/dL SBP and DBP were higher. Moreover, PP right and left were 56.3 vs. 52.2 mmHg (p = 0.07) and 56.1 vs. 51.2 mmHg (p < 0.05) in the group with non-HDL-C ≥ 130 mg/dL and < 130 mg/dL, respectively. The arterial stiffness parameters ABI, pulsatile stress test, baPWV and cfPWV did not differ between both groups (Table 4).

There were no significant differences in SBP and DBP between patients with triglycerides ≥ 150 mg/dL and < 150 mg/dL. The values of baPWV left and cfPWV were significantly lower in patients with triglycerides < 150 mg/dL. ABI, PP, pulsatile stress test and baPWV left did not differ between both groups (Table 5).

Relationship between treatment with statins and arterial stiffness parameters

In the statin (+) group the mean value of PP right, PP left and baPWV left was higher by 1.83 mmHg, 2.18 mmHg and 0.34 m/s as compared to the statin (–) group, respectively.

The level of LDL ≥ 100 mg/dL was associated with a significant increase of PP right (2.33 mmHg) and PP left (2.1 mmHg) as compared to patients with LDL < 100 mg/dL. In patients with LDL ≥ 100 mg/dL, the pulsatile stress right and left was higher by 156 and 181 relative to the group with LDL < 100 mg/dL, respectively. The relationship between the treatment with statins and arterial stiffness parameters is presented in Tables 3, 4 and 5. It is worth to underline, that arterial stiffness was higher in the statin (+) group.

Multivariate analysis

Adjusted for age, sex, diabetes and CV status, the pulse pressure right/left measured in both groups, the value was higher in the statin (+) group, but the difference was not statistically significant. Similar results were attained for participants with non-HDL ≥ 130 mg/dL vs. < 130 mg/dL and LDL ≥ 100 mg/dL vs. < 100 mg/dL.

Discussion

Statin treatment, lipids level and cardio- and renal protection in RTRs

A protective effect of statin treatment on cardiac endpoints has consistently been confirmed in different populations [13]. Statins protect nephrological patients from CV complications, but the effect is lower in groups with severe renal failure [14]. However, although cardio- and reno-protective effects of statins have been well documented in the general population, the effects have been less studied in RTRs. Moreover, only 36% of RTRs are treated with statins according to Clinical Practice Guidelines for Managing Dyslipidemias in Kidney Transplant Patients [15]. The results of the Assessment of Lescol in Renal Transplantation (ALERT) study, showed that fluvastatin (40 mg/day) decreased the level of LDL-C by 32%. On the other hand, the primary endpoint composed of cardiac death, nonfatal myocardial infarction or coronary intervention procedure, was reduced by 17%, but this difference was not statistically significant [14]. Moreover, the outcomes revealed that only 41.6% of participants used statins [14]. The present study showed that treatment with statins was insufficient, because only 26.6% of the RTRs achieved the main aim of hypolipidemic treatment (LDL < 100 mg/dL). It should be underlined, that on average, patients received between 44.6% and 75% of the maximal dose of statins (atorvastatin, fluvastatin, simvastatin, pravastatin).

Statins are known to have pleiotropic effects such as anti-inflammatory, antiproliferative, and immunosuppressive effects, which suggested their possible impact on acute allograft rejection [16]. Regarding vascular remodeling, interstitial fibrosis, and tubular atrophy (IF-TA) intensive statin treatment may halt the progression of IF-TA protecting it from atherosclerosis [17, 18]. The beneficial effects of statins on coronary atherosclerosis progression have been attributed not only to lipid-lowering effects, but probably also to their anti-inflammatory properties. Furthermore, nephroprotective aspects of statins have been ascribed to regulate fibrogenic mechanisms and their effect on endothelial dysfunction [19]. Cochrane meta-analysis showed in 22 studies, that statins may reduce the relative risk of CV events in RTRs [20].

Relationship between lipids, blood pressure and arterial stiffness parameters

Pulse wave velocity and PP are a non-invasive method to assess a central arterial stiffness that predicts independently CVD morbidity and mortality [21]. Increased PWV serves as target organ damage in subjects with hypertension and is included in risk stratification for CVD events [21].

Moreover, Korogiannou et al. [22] provide an overview of the field of arterial stiffness in renal transplantation and the prognostic significance of arterial stiffness for CV events, renal events and mortality in these individuals, as well as studies examining the changes in arterial stiffness following renal transplantation. PWV is considered as the ‘gold standard’ method for the assessment of arterial stiffness [21]. Increased aortic stiffness leads to a premature return in heart’s late systole and increases central PP and SBP. It resulted in left ventricular hypertrophy, a well-established risk factor for coronary events [21]. In addition, PP, as the difference between SBP and DBP, is a major CV risk factor directly related to CV events [23].

In the current study values of arterial stiffness parameters (baPWV, cfPWV, PP, pulsatile stress test) and SBP were higher (p < 0.05) in the statin (+) as compared to the statin (–) group. It is worth mentioning that in the statin (+) group, there were more patients with diabetes, CVD and hypertension. Additionally, it is prudent to underline, that current patients with a lower level of LDL (< 100 mg/dL) and non-HDL (< 130 mg/dL), better values of BP and arterial stiffness parameters were observed.

Theilade et al. [24] failed to show an independent relationship between brachial PP and CV events in a high-risk population with diabetes, CKD and anemia. In transplant patients, increased stiffness of the common carotid artery predicts the occurrence of CV events [25]. More recently, in RTRs, PWV was associated with the combined end point of doubling plasma creatinine and CV events [25].

Additionally, D’elia et al. [10] indicated: “a direct association between statin use and decreased arterial stiffness in the controlled randomized intervention trial of statin use having PWV changes as the main endpoint in the general population, patients with chronic kidney disease, hypercholesterolemia, cardiovascular disease and obturative sleep apnea”.

Navarro-Muñoz et al. [26] showed the improvement of LDL profile after atorvastatin treatment in patients after kidney transplantation with worse PWV (> 9.75 m/s), transforming growth factor-beta 1 levels were significantly reduced after 3 months of treatment.

Limitations of the study

There are several limitations of this study that should be considered when interpreting the results. First, the present results do not prove direct decreasing of arterial stiffness by statins. Additionally, the duration of statin therapy, indications and adherence for this treatment were not assessed. Nevertheless, it can be considered that more intensive statin treatment in RTRs could mitigate aortic stiffness. Second, in spite of the fact that the study population was divided in statin (+) and statin (–), it was a heterogenous group, with different comorbidity conditions and dissimilar time of dialysis and the period after renal transplantation. Third, there are the limitations of using high doses of statins in renal transplant recipients due to interaction with calcineurin inhibitor and impaired graft function.

Fourth, the use of office blood pressure readings, done once, to monitor the quality of BP control may be subject to significant error due to white-coat syndrome. In reality therefore, treatment results may even be better. In addition, the assessment of antihypertensive treatment was based on medical records. Hence, there might be small differences between these data and real-life data.

However, despite these limitations, the study highlights some important information for the RTRs. In this matter, longer observation time are needed as well as repeated measurements of all arterial stiffness parameters.

Conclusions

In summary the studied population had intended to show that the administration of statin was low. Additionally, hyperlipidemia was poorly controlled. On the other hand, arterial stiffness was lower in patients with better control of hyperlipidemia. Therefore, there is a necessity for more frequent lipid-lowering therapy implementation. It may contribute to the reduction of arterial stiffness and can result in the reduction of CV risk of RTRs.

Conflict of interest: None declared

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