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Vitamin D and Aspects of Cardiovascular Disease | OMICS International
ISSN: 2155-6156
Journal of Diabetes & Metabolism

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Vitamin D and Aspects of Cardiovascular Disease

Anna Deleskog1* and Claes-Goran Ostenson2

1Division of Epidemiology, Institute of Environmental Medicine, Karolinska Institute, Stockholm, Sweden

2Department of Molecular Medicine and Surgery, Karolinska Institute, Stockholm, Sweden

*Corresponding Author:
Anna Deleskog, MPH, PhD
Division of Epidemiology
Institute of Environmental Medicine
Karolinska Institute, SE-17177 Stockholm, Sweden
Tel: +46-70-6173464
Fax: +46-8-311101
E-mail: [email protected]

Received date: April 01, 2015; Accepted date: May 04, 2015; Published date: May 07, 2015

Citation: Deleskog A, Ostenson CG (2015) Vitamin D and Aspects of Cardiovascular Disease. J Diabetes Metab 6:545. doi: 10.4172/2155-6156.1000545

Copyright: © 2015 Deleskog A, et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

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Abstract

Vitamin D deficiency is widely prevalent worldwide and is primarily caused by lack of ultraviolet B (UVB) radiation from reduced sun exposure and the consequent limiting of vitamin D production in the skin. Epidemiological studies support the concept that vitamin D is involved in the pathogenesis of cardiovascular disease (CVD). There are several lines of evidence for a number of potential mechanisms whereby vitamin D status may influence CVD risk. Vitamin D receptors (VDR) are known to be expressed in cells throughout the cardiovascular system. In addition, 1α-hydroxylase which converts 25-hydroxyvitamin D to calcitriol is produced in many cell types including vascular, smooth muscle cells, endothelial cells and cardiomyocytes. However, as reported in this review previous observational and vitamin D supplemental studies have shown conflicting results regarding vitamin D and CVD.

Keywords

Cardiovascular disease; Vitamin D

Introduction

Vitamin D insufficiency affects almost 50% of the population worldwide [1]. The high prevalence of vitamin D insufficiency is an important public health issue, and vitamin D insufficiency is an independent risk factor for total mortality in the general population [2]. The main source of vitamin D is synthesis in the skin after exposure to sunlight. Some vitamin D also derives from the diet [1]. Both sources are metabolized in the liver to 25-hydroxyvitamin D (25(OH)D) which is used to determine vitamin D status (Figure 1). This form of vitamin D is biologically inactive and must be converted in the kidney by the 1α-hydroxylase to the active form 1,25-dihydroxyvitamin D (1,25(OH)2D or calcitriol) [3]. Many extra-renal tissues also express 1α-hydroxylase which can produce significant tissue levels of 1,25(OH)2D. Vitamin D receptors (VDRs) are present in most tissues and cells, among them pancreatic β-cells, skeletal muscle cells, cardiomyocytes, smooth muscle cells, vascular endothelial cells, neurons and immmune cells. The binding of 1,25(OH)2D to the VDR leads to transcription of genes that are directly or indirectly influenced by 1,25(OH)2D. These genes control cellular proliferation, differentiation, and apoptosis as well as insulin, renin and cathelicidin production [3].

diabetes-metabolism-Metabolism-vitamin

Figure 1: Metabolism of vitamin D.

At extreme northern and southern latitudes, one major risk factor for vitamin D insufficiency is pigmented skin. Other risk factors are obesity, strict use of sunscreen or concealing clothes. Elderly and intitutionalised individuals are at risk because they spend large amount of time indoors and have reduced dermal capacity to generate vitamin D [4]. There are also seasonal variations in circulating 25(OH)D levels, vitamin D concentrations being higher in summer than winter [1].

Vitamin D and cardiovascular disease

Laboratory experiments and epidemiological studies suggest a protective effect for vitamin D against CVD. There are several lines of evidence for a number of potential mechanisms whereby vitamin D status may influence CVD risk (Figure 2) [3]. The VDRs are expressed in cells throughout the vascular system. Many cell types including vascular smooth muscle cells, endothelial cells, and cardiomyocytes produce 1α-hydroxylase and thus have potential for autocrine and paracrine production of 1,25(OH)2D [3]. This process may be involved in a wide range of physiological functions where 1,25(OH)2D has been shown to inhibit vascular smooth cell proliferation, regulate the renin-angiotensin system, decrease insulin resistance, decrease coagulation and exhibit anti-inflammatory properties [3]. Apart from a direct impact on cardiomyocytes and CVD, it has been suggested that 25(OH)D indirectly influences CVD by modifying cardiovascular risk factors like diabetes, obesity, cholesterol concentration, hypertension, and effects of smoking [5,6]. Thus, in the National Health and Nutrition Examination III survey, including 15,088 women and men, 20 years or older, the prevalences of hypertension, diabetes and hypertriglyceridemia were significantly higher in those with the lowest concentration of 25(OH)D [5].

diabetes-metabolism-insufficient-vitamin-D

Figure 2: Potential mechanisms for the effects of insufficient vitamin D levels on CVD.

Evidence from observational studies

A meta-analysis comprising four studies of incident CVD and five independent mortality studies, and vitamin D deficiency, demonstrated a pooled HR of 1.54 and 1.83 respectively [7]. Participants in the incidence studies were initially healthy in contrast to studies on CVD mortality where the general population or patients with cardiovascular symptoms, or samples enriched for diabetes, were studied. The two largest incidence studies provided the strongest support for an association between vitamin D deficiency and incident CVD (fatal or non-fatal coronary heart disease or myocardial infarction). The Health Professional Follow-up Study exhibited 2-fold increased risk of myocardial infarction (MI) in vitamin D-deficient (25(OH)D < 37.5 nmol/L) subjects after 10 year follow-up [8]. In the Framingham Offspring Study, severe vitamin D deficiency (< 25 nmol/L) was associated with a HR of 1.8 for first cardiovascular event after 5 year follow-up [6]. However, only 5 out of the 9 individual studies included in the meta-analysis reported a significantly increased risk in subjects with low serum 25(OH)D concentration [7]. Similar, the associations between vitamin D concentrations and arrhythmia (atrial fibrillation) and stroke have shown mixed results with no clear consensus [9].

The association between 25(OH)D levels and CVD risk may be nonlinear and reach a plateau between 50 to 70 nmol/L or U-shaped, with an increase in CVD risk at 25(OH)D levels both <50 and > 125 nmol/L. The meta-analysis by Grandi et al. found that cardiovacular risk was increased in individuals with 25(OH)D levels below cut-off ranging from 25 nmol/L to 50 nmol/L [7]. In addition, a meta-analysis of prospective studies investigating vitamin D deficiency in relation to mortality reported a nonlinear decrease in mortality risk as circulating 25(OH)D increases, with optimal concentrations around 75-87.5 nmol/L [10]. The data demonstrated a 31% reduction in mortality risk at levels between 75-87.5 nmol/L compared with concentrations of 27.5 nmol/L. Some researchers consider 25(OH)D concentrations of 50 nmol/L to be adequate for bone and overall health in healthy individuals [11], while others have pointed out that advantageous serum concentrations start at the level of 75 nmol/L and that further improvement is achieved between 90 to 100 nmol/L [12].

A case-control study from our research group included a total of 387 survivors of a first MI before the age of 60 and 387 sex and agematched controls [13]. Fasting blood samples, drawn three months after MI in cases and at the same time in matched controls, were used for biochemical analyses. Low 25(OH)D levels were associated with a range of cardiovascular risk factors but were not related to MI. Among those risk factors, 25(OH)D concentrations were indepently associated with PAI-1 activity and pro-insulin levels [13]. PAI-1 is an inhibitor of plasminogen activation and constitutes an important regulatory protein in fibrinolysis. High plasma levels of PAI-1 have been shown to be associated with increased CVD [14]. High plasma proinsulin levels may indicate pancreatic β-cell stress, and deficient levels of 25(OH)D have been proposed to affect pancreatic β-cell dysfunction. Interestingly, there was also an inverse association of 25(OH)D levels with proinsulin, which suggests a connection with development of type 2 diabetes (T2D) and CVD.

The IMPROVE study is a multicentre, longitudinal cohort study that enrolled individuals aged 54 to 80 years, who had at least three cardiovascular risk factors and no history of CVD, from 7 centers in Finland, Sweden, the Netherlands, France, and Italy [15]. Participants underwent carotid ultrasound examinations at baseline, month 15 and month 30. Blood samples, clinical data and information about life-style factors were collected at baseline from a total of 3,711 subjects, whereof 900 with diabetes. The results demonstrated that levels of 25(OH)D differed across Europe and were not consistently and independently related to measures of carotid intima media thickness (cIMT) [15]. In the same study population, 25(OH)D-associated genetic variants, serum 25(OH)D concentration and measures of cIMT in subjects with and without T2D were examined [16]. The results showed a significant association between the 25(OH)D-decreasing allele of rs3829251 in the DHCR7 locus (gene involved in vitamin D metabolism which converts 7-dehydrocholesterol to cholesterol) and faster progression of cIMT, which depended on interaction with T2D status and was independent of serum 25(OH)D levels and established cardiovascular risk factors [16]. These findings suggest that a pathway associated with the metabolism of vitamin D is causally implicated in subclinical atherosclerosis in subjects with T2D. However, the serum 25(OH)D concentration might be a poor reflection of vitamin D actions in target cells and tissues.

Randomized clinical trials

Two RCTs of vitamin D supplementation report a slight but nonstatistically significant reduction in CVD events [17,18]. Similarly, the Women´s Health Initiative Calcium-Vitamin D trials, in which 36,282 women were randomized to calcium 1000 g/d plus vitamin D 400 IU/ day or placebo for 7 years, found no reduction in CVD morbidity [19]. The median increase in 25(OH)D levels was however rather small, from 42.3 nmol/L to 54.1 nmol/L. Supplementation with at least 1,000 IU/day would be required to attain 25(OH)D concentration above 75 nmol/L [12]. A recent meta-analysis including six RCTs assessing the effect of vitamin D supplementation on risk of MI showed nonsignificant pooled RR of 1.02 [20]. RCTs using higher vitamin D doses are required to determine whether vitamin D protects against coronary heart disease. Currently, there are two ongoing RCTs, expected to provide results within 2 years (the Vitamin D Assessment - ViDA and the Vitamin D and Omega-3 Trial - VITAL).

Conclusion

Experimental and epidemiological studies support that vitamin D exerts various positive effects on the cardiovascular system and associations between several cardiovascular risk factors. Moreover, meta-analysis of prospective studies suggests that a low level of 25(OH) D is an independent risk marker for future cardiovascular events and mortality (Table 1) [21-26]. In contrast, the results from RCTs on vitamin D treatment and cardiovascular risk are inconsistent and it is not possible to make definite conclusions regarding the effects of vitamin D on cardiovascular risk. Therefore larger RCTs with sufficient vitamin D doses to assess cardiovascular endpoints are warranted.

Incidence studies Follow-up length Country Clinical endpoint
Marniemi et al. [21] 10 years Finland Fatal/non-fatal coronary events
Giovannucci et al. [8] 10 years USA Fatal coronary heart disease events  and non-fatal MI
Wang et al. [6] 7.6 years USA First fatal/non-fatal cardiovascular events
Bolland et al. [22] 5 years New Zealand MI
Mortality studies    
Dobnig et al. [23] 7.7 years Germany Cardiovascular death
Melamed et al. [2] 8.7 years USA Cardiovascular death
Pilz et al. [24] 6.2 years Netherlands Cardiovascular death
Kilkkinen et al. [25] 27.1 years Finland Cardiovascular death
Semba et al. [26] 6.5 years Italy Cardiovascular death

Table 1: Prospective studies assessing the association between 25OHD concentrations with incidence of cardiovascular events and mortality.

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