Heart Failure Clinical Trial
Official title:
Vitamin D Supplementation in Chronic Stable Heart Failure: a Randomized, Double-blind, Placebo-controlled Trial
In cross-sectional and prospective cohort studies, vitamin D deficiency is associated with increased mortality, cardiovascular events including sudden cardiac death and stroke, diabetes, hypertension and impaired function of the immune and musculoskeletal system. The action of vitamin D on the cardiovascular system regulates cardiac function, endothelial and vascular smooth muscle, and, the renin-angiotensin system. Treatment with sufficiently high doses of vitamin D may represent a promising and inexpensive intervention option. To date, there are few data on the effect of cholecalciferol treatment in patients with chronic heart failure. The primary objective of this study is to investigate whether oral vitamin D supplementation improves chronic heart failure (measured with the surrogate parameter of NT-proBNP levels at month 0 and 6).
A growing body of data suggests that low vitamin D levels may adversely affect
cardiovascular health. For many cardiovascular events, seasonal variability with peak
incidence in the winter months is proven. This may be attributable at least in part to
declining body stores of vitamin D beginning with September. Recently, there have been
several case reports about severe cardiomyopathy caused by vitamin D deficiency, especially
in dark-skinned children who had low vitamin D levels. The heart is an important target
organ for vitamin D, both on a genomic and nongenomic level. Myocytes express the vitamin D
receptor and several models of hypertension in animal studies have shown that vitamin D
treatment is able to prevent cardiac hypertrophy [9-10]. Vitamin D seems to inhibit
activation of the cardiac renin-angiotensin system as well as the expression of genes
involved in the development of myocardial hypertrophy. There is accumulating evidence that
vitamin D deficiency may be an important factor in the development of congestive heart
failure and sudden cardiac death.
In chronic hemodialysis patients, vitamin D supplementation has been associated with
reduction of cardiac hypertrophy and a reduction of QT dispersion, the latter being
considered a major risk factor for sudden cardiac death. A small study from 1984 showed an
improvement in left ventricular function after treatment with cholecalciferol in
hemodialysis patients. A recent study from our group has reported a negative correlation of
25(OH)D levels with NT-pro-BNP levels, New York Heart Association functional classes and
impaired left ventricular function. Furthermore, hazard ratios for death attributable to
heart failure and sudden cardiac death were 2.84 and 5.05, respectively, when patients with
25(OH)D <25ng/ml were compared with those having serum levels of 25(OH)D >75 ng/ml [11]. The
anti-inflammatory properties of vitamin D also appear to play a role in congestive heart
failure, as studied in a recent interventional trial. In animal models, vitamin D deficiency
was proven to be associated with developing myocardial hypertrophy and fibrosis with
aberrant cardiac contractility and relaxation. Moreover, vitamin D deficiency can raise
parathyroid hormone secretion, which in turn may increase insulin resistance and be
associated with the development of diabetes, hypertension and inflammation. In summary,
vitamin D seems to exert a multitude of different effects all working in concert to protect
the vascular and cardiac system by influencing various hierarchical levels of biologic
response.
Recently, a randomized controlled trial in a subgroup of patients with heart failure(n=105,
≥ 70 years) was able to demonstrate a significant decrease in BNP levels at 10 and 20 weeks,
while the primary endpoint "functional capacity" and quality of life did not differ between
intervention and placebo group.
Because in this latter trial, even the intervention group did not reach normal vitamin D
levels, we will use a higher dose of vitamin D given in shorter intervals.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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