ISSN: 1885-5857 Impact factor 2023 7.2
Vol. 62. Num. 1.
Pages 96-99 (January 2009)

Susceptibility to Atherosclerosis in Patients With Psoriasis and Psoriatic Arthritis as Determined by Carotid-Femoral (Aortic) Pulse-Wave Velocity Measurement

Vulnerabilidad a la aterosclerosis en pacientes con psoriasis y artritis psoriásica, según las determinaciones de la velocidad de la onda de pulso carótido-femoral (aórtica)

Mehmet SoyaMustafa YildizbMehmet Sevki UyanikaNuran KaracacGökhan GüferaSüleyman Piskinc

Options

Introduction and objectives. In this study we analyzed the susceptibility to atherosclerosis of patients with psoriasis and psoriatic arthritis (PsA) by determining the femoral-carotid pulse wave velocity (PWV), which is a measure of the viscoelastic properties of blood vessels. Methods. The study included 25 patients with psoriasis (age 18-63 years; 13 male), of whom nine had arthritis, as well as 39 sex- and age-matched healthy control subjects (age 24-70 years, 25 male). The systolic blood pressure (SBP), diastolic blood pressure (DBP), heart rate, body mass index (BMI) and waist-to-hip ratio (WHR) of all participants were recorded and, in patients, skin lesions were assessed using the psoriasis area and severity index (PASI). Arterial distensibility was determined by automatic carotid-femoral PWV measurement using the Complior Colson device. Results. Mean PWV, SBP and DBP were significantly higher in psoriatic patients than in control subjects (P=.036, P<.001, and P=.005, respectively). In PsA patients, the mean WHR, SBP, DBP and PWV were all significantly higher than in control subjects (P=.001, P=.031, P=.001, and P=.014, respectively). Conclusions. The carotid-femoral PWV is increased in patients with psoriasis and PsA.

Keywords

Psoriasis
Psoriatic arthritis
Atherosclerosis
Pulse wave velocity

INTRODUCTION

Psoriasis is a hereditary, chronic inflammatory skin disorder and psoriatic arthritis (PsA), which has been defined as an inflammatory arthritis associated with psoriasis, appears to be linked to increased cardiovascular mortality and morbidity.1 Several factors might explain the raised cardiovascular risk: smoking, hypertension, reduced physical activity, an altered lipid profile, chronic inflammation with elevated levels of inflammatory factors (eg, platelet-activating factor), hyperhomocysteinemia or hypercoagulability.2-4 Measurement of the pulse-wave velocity (PWV) and carotid intima-media thickness (CIMT) have been used to evaluate the viscoelastic properties of large arteries. The PWV is an index of arterial wall stiffness, which is inversely related to arterial distensibility and relative arterial compliance.5

In this study, we investigated arterial distensibility in patients with psoriasis and PsA by measuring the PWV.

METHODS

This cross-sectional study involved 25 patients with psoriasis (age, 18-63 years; 13 male), which was diagnosed on the basis of its clinical characteristics, and 39 sex- and age-matched healthy control subjects (age, 24-70 years; 25 male). Nine of the patients also had arthritis, which was considered to be PsA. Systolic blood pressure (SBP), diastolic blood pressure (DBP), heart rate, body mass index (BMI), and the waist-to-hip ratio (WHR) were coded for all participants and, in patients, the psoriasis area and severity index (PASI) score was derived.

Exclusion criteria were previous myocardial infarction, congestive heart failure, renal failure (ie, plasma creatinine >1.8 mg/dL), valvular heart disease, atrial fibrillation, anemia (ie, hematocrit <35%), obesity (ie, BMI >35 kg/m2) and a WHR ≥1.

The carotid-femoral PWV and arterial blood pressure were measured in each participant by the same observer with the subject in the supine position after resting for at least 20 minutes. Arterial distensibility was assessed by automatic carotidfemoral PWV measurement using the Complior Colson device (France); the technical characteristics of this device have been described elsewhere, and indicate that inter- and intra-observer repeatability coefficients are >0.9.6 The PWV was calculated by measuring the pulse transit time and the distance traveled by the pulse between the 2 recording sites (ie, the right femoral and common carotid arteries): PWV = distance (m) / transit time (s).

Statistical Analysis

Statistical analysis was carried out using SPSS version 8.0. All values are expressed as a mean (standard deviation). The results obtained were assessed by a Mann-Whitney U test. Pearson correlation coefficients were calculated. Finally, a Pvalue less than .05 was considered significant.

RESULTS

The mean ages of the patients and control subjects were 45.7 (11.5) years (range, 18-63 years) and 42.0 (11.7) (range, 24-70 years), respectively. The mean PWV, SBP, and DBP in psoriatic patients were significantly higher than in control subjects (U=335, P=.036; U=237, P<.001; and U=294, P=.005, respectively). The mean serum cholesterol, triglyceride and high-density lipoprotein levels in patients were 202 (54) mg/dL, 160 (96) mg/dL, and 48 (11) mg/dL, respectively. Seven patients (28%) had dyslipidemia or hypertension or both. When only normolipemic and normotensive patients were considered, the results were the same: the mean PWV, SBP, and DBP were significantly higher in patients than in control subjects (U=210, P=.030; U=185, P=.006; and U=194, P=.013, respectively).

The demographic and cardiovascular characteristics of patients and healthy control subjects are summarized in Table.

There were good correlations between BMI, SBP, DBP and heart rate and the PWV in all groups (r=0.392, P=.001; r=0.397, P=.001; r=0.288, P=.021; and r=0.307, P=.014, respectively). In patients with psoriasis, there were good correlations between the PWV and age, WHR and low-density lipoprotein level (r=0.773, P<.001; r=0.623, P=.001; and r=0.584, P=.017, respectively).

The mean PASI score in patients was 8.82 (9.1) (range, 0-34). There was no correlation between the PWV and the PASI score.

Nine psoriatic patients (36%) were regarded as having PsA. The differences between parameters for patients with and without arthritis were not significant (ie, P>.05 for all). However, the mean WHR, SBP, DBP, and PWV in PsA patients were significantly higher than in control subjects (P=.001; P=.031; P=.001; and P=.014, respectively).

DISCUSSION

Atherosclerosis is a multifocal, immunoinflammatory disease affecting medium and large arteries. There is growing evidence that, in addition to traditional risk factors, vascular wall inflammation plays a key role in the pathogenesis of vascular diseases and the atherosclerotic process.7 In disorders that are inflammatory in nature, the chronic inflammatory state per se has been linked to an acceleration in the atherosclerotic process. The existence of this link is supported by the increased incidence of cardiovascular disease observed in disorders such as systemic lupus erythematosus and rheumatoid arthritis.8,9

Psoriasis is a hereditary, chronic inflammatory skin disorder that may have systemic effects, involving, for example, the kidneys, eyes and joints, and leading to amyloidosis.10 It has been demonstrated that psoriasis and PsA are associated with increased cardiovascular mortality and morbidity.1 Traditional and non-traditional cardiovascular risk factors might explain the enhanced cardiovascular risk. Seishima et al11 showed that apolipoprotein levels were elevated in psoriasis and suggested that abnormal lipoprotein metabolism may be related to the high incidence of atherosclerosis in the condition. Vanizor Kural et al3,4 demonstrated that biochemical markers for susceptibility to atherosclerosis, such as an elevated homocysteine concentration, altered endothelial cell-mediated protein levels, increased lipid levels and increased high-density lipoprotein oxidation, may be important in the development of atherothrombotic complications in patients with psoriasis. Recently, González-Juanatey et al12,13 demonstrated the existence of susceptibility to atherosclerosis and endothelial dysfunction in patients with PsA by measuring the CIMT and flow-mediated endothelial dependent vasodilatation. Several traditional and non-traditional risk factors might explain the increased cardiovascular risk. Alternatively, genetic factors associated with susceptibility to inflammatory arthritis may also lead to a high prevalence of atherosclerosis.14 It seems that increased susceptibility to atherosclerosis is a major risk factor for cardiovascular morbidity and mortality in patients with psoriasis.15 In this study, we evaluated the susceptibility to atherosclerosis of patients with psoriasis by measuring the carotid-femoral PWV. The mean PWV was found to be significantly higher in psoriatic patients than in control subjects (P<.05). The present study is the first to demonstrate that the PWV, which is a measure of the viscoelastic properties of blood vessels, is increased in patients with psoriasis and PsA.

Both blood pressure and heart rate are known to be determinants of the arterial PWV.6,16 Arterial distensibility depends on the variation in blood pressure level, and especially on pulse pressure. With increasing age, systolic blood pressure and pulse pressure gradually become more important than diastolic blood pressure.17 Stiffness is greater when blood pressure is high and lower when blood pressure is low because of mechanical changes related to arterial wall stretching and the resulting changes in the relative contributions of elastin and collagen fibers to the elastic modulus.18 On PWV measurement, patients with psoriasis and PsA had a higher SBP and DBP. High blood pressure may also have resulted in reduced arterial distensibility in the patient group. There were good correlations between age, SBP and DBP and PWV in our study, which is in agreement with other reports in the literature.

Obesity, which is a traditional cardiovascular risk factor, could be a sign of inactivity and may be associated with insulin resistance. In addition, the WHR in patients with PsA was significantly higher than in control subjects (P=.001). This finding indicates that arteries become less elastic as the BMI and WHR increase, and that arterial stiffening is observed at higher BMIs and WHRs.

There was a good correlation with heart rate in both patients and healthy control subjects. An increased resting heart rate is associated with increased cardiovascular mortality.20 Mangoni et al16 showed that, in rats, arterial distensibility increased in parallel with the increase in heart rate. A high heart rate shortens the time available for recoil, which leads to arterial stiffening.

A raised BMI or WHR, which are traditional cardiovascular risk factors, could be a sign of inactivity and could be associated with hyperlipidemia, hyperinsulinemia, hypertension, and inflammation. In addition, they might also have an adverse affect on the vascular system by decreasing arterial distensibility.19,20 In this study, we found significant correlations between the carotid-femoral PWV and BMI and WHR.

In conclusion, in this study we showed that the viscoelastic properties of blood vessels are altered in patients with psoriasis and PsA.

Study Limitations

Subjects with known cardiovascular disease or cardiovascular risk factors, such as a previous myocardial infarction, diabetes mellitus, peripheral arterial disease, and cerebrovascular disease, were carefully excluded from the study, which resulted in a small sample size. Therefore, the results of this study will need to be confirmed in a larger group of patients.


Correspondence: Mehmet Soy, MD,
Department of Internal Medicine-Rheumatology, Faculty of Medicine, Abant Izzet Baysal University, Bolu, Turkey
E-mail: msoy_2000@yahoo.com

Received September 25, 2007
Accepted for publication March 14, 2008.

Bibliography
[1]
Peters MJ, Van der Horst-Bruinsma IE, Dijkmans BA, Nurmohamed MT..
Cardiovascular risk profile of patients with spondylarthropathies, particularly ankylosing spondylitis and psoriatic arthritis..
Semin Arthritis Rheum, (2004), 34 pp. 585-92
[2]
Stern RS, Lange R..
Cardiovascular disease, cancer, and cause of death in patients with psoriasis: 10 years prospective experience in a cohort of 1380 patients..
J Invest Dermatol, (1988), 91 pp. 197-201
[3]
Vanizor Kural B, Orem A, Cimsit G, Yandi YE, Calapoglu M..
Evaluation of the atherogenic tendency of lipids and lipoprotein content and their relationships with oxidantantioxidant system in patients with psoriasis. Clin Chim Acta. 2003;328:71-82. 4. Vanizor Kural B, Orem A, Cimsit G, Uydu HA, Yandi YE, Alver A. Plasma homocysteine and its relationships with atherothrombotic markers in psoriatic patients..
Clin Chim Acta, (2003), 332 pp. 23-30
[5]
Imura T, Yamamoto K, Kanamori K, Mikami T, Yasuda H..
Non-invasive ultrasonic measurement of the elastic properties of the human abdominal aorta..
Cardiovasc Res, (1986), 20 pp. 208-14
[6]
Asmar R, Benetos A, Topouchian J, Laurent P, Pannier B, Brisac AM, et al..
Assessment of arterial distensibility by automatic pulse wave velocity measurement: validation and application studies..
Hypertension, (1995), 26 pp. 485-90
[7]
Libby P, Ridker PM, Maseri A..
Inflammation and atherosclerosis..
Circulation, (2002), 105 pp. 1135-43
[8]
Manzi S..
Systemic lupus erythematosus:a model for atherogenesis? Rheumatology (Oxf), (2000), 39 pp. 353-9
[9]
Klocke R, Cockcroft JR, Taylor GJ, Hall IR, Blake DR..
Arterial stiffness and central blood pressure, as determined by pulse wave analysis, in rheumatoid arthritis..
Ann Rheum Dis, (2003), 62 pp. 414-8
[10]
Myers W, Opeola M, Gottlieb AB..
Common clinical features and disease mechanisms of psoriasis and psoriatic arthritis..
Curr Rheumatol Rep, (2004), 6 pp. 306-13
[11]
Seishima M, Seishima M, Mori S, Noma A..
Serum lipid and apolipoprotein levels in patients with psoriasis..
Br J Dermatol, (1994), 130 pp. 738-42
[12]
González-Juanatey C, Llorca J, Amigo-Díaz E, Dierssen T, Martín J, González-Gay MA..
High prevalence of subclinical atherosclerosis in psoriatic arthritis patients without clinically evident cardiovascular disease or classic atherosclerosis risk factors..
Arthritis Rheum, (2007), 57 pp. 1074-80
[13]
González-Juanatey C, Llorca J, Miranda-Filloy JA, Amigo-Díaz E, Testa A, García-Porrúa C, et al..
Endothelial dys-function in psoriatic arthritis patients without clinically evident cardiovascular disease or classic atherosclerosis risk factors..
Arthritis Rheum, (2007), 57 pp. 287-93
[14]
González-Gay MA, Gonzalez-Juanatey C, López-Díaz MJ, Piñeiro A, García-Porrúa C, Miranda-Filloy JA, et al..
HLA-DRB1 and persistent chronic inflammation contribute to cardiovascular events and cardiovascular mortality in patients with rheumatoid arthritis..
Arthritis Rheum, (2007), 57 pp. 125-32
[15]
Sattar N, McCarey DW, Capell H, McInnes IB..
Explaining how high-grade systemic inflammation accelerates vascular risk in rheumatoid arthritis..
Circulation, (2003), 108 pp. 2957-63
[16]
Mangoni AA, Mircoli L, Giannattasio C, Ferrari AU, Mancia G..
Heart rate-dependence of arterial distensibility in vivo..
J Hypertens, (1996), 14 pp. 897-901
[17]
Franklin SS, Khan SA, Wong ND, Larson MG, Levy D..
Is pulse pressure useful in predicting risk for coronary heart disease? The Framingham Heart Study..
Circulation, (1999), 100 pp. 354-60
[18]
Olivetti G, Anversa P, Melissari M, Loud AV..
Morphometry of medial hypertrophy in the rat thoracic aorta..
Lab Invest, (1980), 42 pp. 559-65
[19]
Kannel WB, Kannel C, Paffenbarger RS Jr, Cupples LA..
Heart rate and cardiovascular mortality: the Framingham Study..
Am Heart J, (1987), 113 pp. 1489-94
[20]
Anuurad E, Shiwaku K, Nogi A, Kitajima K, Enkhmaa B, Shimono K, et al..
The new BMI criteria for Asians by the regional office for the Western Pacific Region of WHO are suitable for screening of overweight to prevent metabolic syndrome in elder Japanese workers..
J Occup Health, (2003), 45 pp. 335-43
Are you a healthcare professional authorized to prescribe or dispense medications?