Serum Vitamin D and Risk of Secondary Cardiovascular Disease Events in Patients with Stable Coronary Heart Disease

Overview

Journal Am Heart J

Specialty Cardiology & Vascular Diseases

Date 2010 Jun 24

PMID 20569718

Citations 20

Authors

Norma Christine Grandi

Lutz Philipp Breitling

Carla Yvonne Vossen

Harry Hahmann

Bernd Wusten

Winfried Marz

Dietrich Rothenbacher

Hermann Brenner

Affiliations

Soon will be listed here.

Abstract

Background: Recent longitudinal analyses suggested that low levels of serum 25-hydroxyvitamin D (25-OH-D) predict incident cardiovascular disease in initially healthy populations. Because the prognostic value of vitamin D for the occurrence of secondary cardiovascular events remains unclear, we examined the association of baseline 25-OH-D levels with prognosis in patients with stable coronary heart disease (CHD).

Methods: Serum 25-OH-D levels from 1,125 CHD patients of 2 German clinics undergoing a 3-week rehabilitation program after an acute cardiovascular event were measured, and participants were followed for up to 8 years. We used multivariate Cox regression analysis to model cardiovascular event incidence (fatal and nonfatal, including myocardial infarction, stroke, and death due to cardiovascular diseases) and all-cause mortality according to 25-OH-D quartiles, categories based on cut points of 15 and 30 ng/mL, or continuous vitamin D concentrations.

Results: During follow-up, 148 cardiovascular events and 121 deaths were recorded. Elevation of risk for the lowest quartile or category in comparison to the highest category was weak and nonsignificant for both incidence (hazard ratio [HR](quartile1) = 1.15 [0.72-1.84], HR(<15 ng/mL) = 1.17 [0.61-2.23]) and mortality (HR(quartile1) = 1.29 [0.77-2.14], HR(<15 ng/mL) = 1.87 [0.91-3.82]) in unadjusted Cox regression analysis and disappeared entirely after adjustment for potential confounders (cardiovascular events: HR(quartile1) = 0.84 [0.47-1.50], HR(<15 ng/mL) = 0.90 [0.41-1.96]; mortality: HR(quartile1) = 0.63 [0.33-1.21], HR(<15 ng/mL) = 0.93 [0.39-2.21]). Models treating vitamin D as a continuous variable likewise suggested no significant associations.

Conclusions: Unlike previous population-based studies, our analysis in high-risk patients with stable CHD does not support a prognostic value of baseline-25-OH-D levels for secondary cardiovascular event incidence or all-cause mortality.

Citing Articles

How Follow-Up Period in Prospective Cohort Studies Affects Relationship Between Baseline Serum 25(OH)D Concentration and Risk of Stroke and Major Cardiovascular Events.

Grant W, Boucher B Nutrients. 2024; 16(21).

PMID: 39519592 PMC: 11547645. DOI: 10.3390/nu16213759.

Vitamin D Deficiency, Inflammation, and Diminished Endogenous Regenerative Capacity in Coronary Heart Disease.

Desai S, Ko Y, Liu C, Hafeez Z, Park J, Faaborg-Andersen C JACC Adv. 2024; 3(2):100804.

PMID: 38939377 PMC: 11198268. DOI: 10.1016/j.jacadv.2023.100804.

Association between Multiplate-measured aspirin resistance and vitamin D deficiency in stable coronary artery disease.

Surmen S, Karaca Ozer P, Emet S, Govdeli E, Elitok A Arch Med Sci Atheroscler Dis. 2022; 6:e203-e208.

PMID: 36161218 PMC: 9487833. DOI: 10.5114/amsad.2021.112242.

Predictive value of 25-hydroxyvitamin D level in patients with coronary artery disease: A meta-analysis.

Zhang H, Wang P, Jie Y, Sun Y, Wang X, Fan Y Front Nutr. 2022; 9:984487.

PMID: 36034916 PMC: 9399797. DOI: 10.3389/fnut.2022.984487.

A single-oral bolus of 100,000 IU of cholecalciferol at hospital admission did not improve outcomes in the COVID-19 disease: the COVID-VIT-D-a randomised multicentre international clinical trial.

Cannata-Andia J, Diaz-Sottolano A, Fernandez P, Palomo-Antequera C, Herrero-Puente P, Mouzo R BMC Med. 2022; 20(1):83.

PMID: 35177066 PMC: 8853840. DOI: 10.1186/s12916-022-02290-8.