Endothelial NO-synthase intron 4 polymorphism is associated with disturbed in vivo nitric oxide production in individuals prone to type 2 diabetes

Endothelial NO-synthase intron 4 polymorphism is associated with disturbed in vivo nitric oxide production in individuals prone to type 2 diabetes

Insulin resistance, as well as vascular disease, both share a relevant genetic background taking the influence of a positive family history of these disorders. On the other hand, insulin resistance is associated with a proatherosclerotic disturbance in nitric oxide dependent vasodilation, probably c...

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Bibliographic Details
Published in:Hormone and metabolic research Vol. 40; no. 1; p. 13
Main Authors: Rittig, K, Holder, K, Stock, J, Tschritter, O, Peter, A, Stefan, N, Fritsche, A, Machicao, F, Häring, H-U, Balletshofer, B
Format: Journal Article
Language:English
Published: Germany 01-01-2008
Subjects:
Cardiovascular Diseases - complications
Cardiovascular Diseases - genetics
Diabetes Mellitus, Type 2 - complications
Diabetes Mellitus, Type 2 - genetics
Female
Genetic Predisposition to Disease
Glucose - metabolism
Haplotypes
Humans
Introns - genetics
Male
Middle Aged
Nitric Oxide - biosynthesis
Nitric Oxide Synthase Type III - genetics
Polymorphism, Genetic
Risk Factors
Vasodilation
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Summary:Insulin resistance, as well as vascular disease, both share a relevant genetic background taking the influence of a positive family history of these disorders. On the other hand, insulin resistance is associated with a proatherosclerotic disturbance in nitric oxide dependent vasodilation, probably contributing to the link between these two disorders. We examined the association between nitric oxide dependent vasodilation (measured with high resolution ultrasound at 13 MHz) and three relevant NO-synthase (eNOS)-polymorphisms in 200 insulin resistant subjects participating in the Tuebinger Lifestyle Intervention Program (TULIP). This study revealed that carriers of the eNOS intron 4 polymorphism (aa 2.16%; ab 24.2%; bb 73.2%) show significantly worse endothelial, and thereby eNOS dependent vasodilation (p=0.03, multivariate ANOVA), as compared to wildtype carriers. The 5' UTR T-786C and the G894 T polymorphism did not show any influence on eNOS-activity. In subjects at increased risk to develop type 2 diabetes, the eNOS intron 4 polymorphism is independently associated with endothelial function as indicated by disturbed endothelial NO production. Due to the high prevalence and the relatively strong effect, this polymorphism might help to identify subjects at increased risk for atherosclerosis associated with overweight and insulin resistance.
ISSN:0018-5043
DOI:10.1055/s-2007-1004527