Abstract
Fasting hyperhomocysteinemia is an independent risk factor for coronary artery disease,
stroke, peripheral vascular atherosclerosis, and for arterial and venous thromboembolism.
The risk for cardiovascular disease with homocysteine is similar to conventional risk
factors. The interaction of hyperhomocysteinemia with hypertension and smoking is
strong and the combined effect is more than multiplicative. The combined effect of
homocysteine and cholesterol is additive. Homocysteine produces atherosclerosis, thromboembolism,
and vascular endothelial cell injury. Vascular dysfunction produced by homocysteine
may be due to endothelial cell damage. Homocysteinemia-induced atherosclerosis is
probably due to various factors including endothelial cell injury, inability to sustain
S-nitroso-homocysteine formation because of imbalance between production of nitric
oxide by dysfunctional endothelium and homocysteine, smooth muscle cell proliferation,
and thromboembolism. There is strong evidence that endothelial cell injury is associated
with oxidative stress produced by homocysteine. Hyperhomocysteinemia is associated
with numerous conditions, including coronary disease, stroke, peripheral vascular
disease (carotid artery and cerebrovascular atherosclerosis), venous thrombosis, renal
disease, diabetes mellitus, and organ transplant. Folic acid, vitamin B12 and B6 have been shown to be beneficial in reducing plasma homocysteine levels. Folic acid
is specifically very effective, safe and inexpensive.
