Among 16 men screened, carriers of a novel functional mutation of DDAH-1 had a significantly elevated risk for cardiovascular disease and a tendency to develop hypertension.
Observational (n=16)
Are DDAH gene polymorphisms associated with increased cardiovascular risk?
DDAH-1 mutations may contribute to increased cardiovascular risk by affecting ADMA metabolism and endothelial NO synthase regulation.
The crucial role of nitric oxide (NO) for normal endothelial function is well known. In many conditions associated with increased risk of cardiovascular diseases such as hypercholesterolemia, hypertension, abdominal obesity, diabetes and smok ing, NO biosynthesis is dysregulated, leading to endothelial dysfunction. The grow ing evidence from animal and human studies indicates that endogenous inhibitors of endothelial NO synthase such as asymmetric dimethylarginine (ADMA) and NG-monomethyl-L-arginine (L-NMMA) are associated with the endothelial dysfunc tion and potentially regulate NO synthase. The major route of elimination of ADMA is metabolism by the enzymes dimethylarginine dimethylaminohydrolase-1 and -2 (DDAH). In our recent study 16 men with either low or high plasma ADMA concen trations were screened to identify DDAH polymorphisms that could potentially be associated with increased susceptibility to cardiovascular diseases. In that study a novel functional mutation of DDAH-1 was identified; the mutation carriers had a significantly elevated risk for cardiovascular disease and a tendency to develop hypertension. These results confirmed the clinical role of DDAH enzymes in ADMA metabolism. Furthermore, it is possible that more common variants of DDAH genes contribute more widely to increased cardiovascular risk.
Valkonen et al. (Fri,) conducted a observational in Cardiovascular disease (n=16). DDAH-1 mutation was evaluated on Cardiovascular disease risk and hypertension. Among 16 men screened, carriers of a novel functional mutation of DDAH-1 had a significantly elevated risk for cardiovascular disease and a tendency to develop hypertension.
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