Klotho is a genetic risk factor for ischemic stroke caused by cardioembolism in Korean females
Male
0301 basic medicine
Korea
Polymorphism, Genetic
Genotype
Heart Diseases
Dementia, Vascular
Embolism
Middle Aged
Brain Ischemia
3. Good health
Stroke
03 medical and health sciences
Risk Factors
Acute Disease
Humans
Female
Klotho Proteins
Aged
Glucuronidase
DOI:
10.1016/j.neulet.2006.08.039
Publication Date:
2006-09-15T08:13:35Z
AUTHORS (8)
ABSTRACT
An aging-suppressor gene, klotho, is a candidate factor for vascular disease because its deficiency leads to impaired endothelium-dependent vasodilation and impaired angiogenesis. We investigated the association of polymorphisms in klotho with ischemic stroke. We searched for sequence variants in promoter and exons of klotho gene. For the association study, selected variants were genotyped in control subjects and in patients with ischemic stroke and vascular dementia. The association with ischemic stroke was further investigated with its subtypes classified based on Trial of Org 10172 in Acute Stroke Treatment (TOAST). No significant association was observed for both G-395A and C1818T with ischemic stroke and vascular dementia (P>0.05). The analysis with subtypes of ischemic stroke revealed the associations that the A allele of G-395A increased the risk of cardioembolic stroke (CE, OR=2.60; P=0.006), and subjects carrying the A allele were susceptible to CE in both of dominant (AA+GA versus GG; OR=2.50; P=0.046) and recessive (AA versus GA+GG; OR=6.52; P=0.007) models. Further analysis of data partitioned by gender showed that the associations of G-395A with CE only existed in women (A versus G; OR=4.33; P=0.002), AA+GA versus GG; OR=5.68; P=0.014, and AA versus GA+GG; OR=9.07; P=0.012), but the significance disappeared in men (P>0.05). The sequence variant of G-395A in klotho might be a genetic risk factor for CE in females.
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