Sleep Apnea, Obstructive Clinical Trial
Specific Aim
1. To identify specific SNPs of HIF-1 gene related to cardiovascular disease in OSA
patients (CVD-OSA)
2. To assay the functional activity of high risk SNPs of HIF-1 on the transcription of
VEGF gene
3. To confirm that the serum level of VEGF in CVD-OSA patients with high risk SNPs of
HIF-1 are higher than CVD-OSA patients without
Obstructive sleep apnea syndrome(OSAS) is characterized with recurrent collapse of upper
airway during sleep and results in hypoxia and sleep fragmentation. The repeated episodes of
hypoxia and sympathetic hyperactivity result in cardiovascular complications, including
atherosclerosis, hypertension, coronary artery disease and heart failure. Our data showed
among 309 consecutively-admitted OSA patients, 54% patients had cardiovascular diseases.
The hypoxia in OSA is characterized as chronic and intermittent, which leads to
sophisticated adaptive mechanisms, like activations of transcriptional factors and critical
signaling pathways. HIF-1 is a central component of transcriptional factors involved in
hypoxia-induced transcription of specific genes. There are two subunits of HIF-1
transcription factor, which interact with the consensus hypoxia response element in the
target genes. The HIF-1 alpha activity is regulated by proline hydroxylation modification
and ubiquitination, which is oxygen-tension dependent. HIF-1 alpha target genes encode
proteins that increase oxygen delivery, such as vascular endothelial growth factor(VEGF).
Our oligo-microarray study showed both HIF and VEGF expression in OSA patients was 1.3 times
of control group, which decreased to 46% and 57% respectively after one-month CPAP
treatment.
HIF-1 alpha polymorphism could result in increased HIF-1 alpha activity and microvessel
density. In clinical observation, HIF-1 polymorphism has been reported to be associated with
high altitude adaptation, formation of coronary collaterals in CAD and phenotype of cancer.
These findings were possibly explained with effect of HIF on modulation of VEGF.
Several genetic polymorphisms were reported to be associated with OSA, which included TNF
alpha, angiotensin converting enzyme and haptoglobin. Only hepatoglobin phenotype is proved
to be a risk factor for cardiovascular disease in OSA. In most studies, the patient number
is less than suggested.
Therefore, in this study, we hypothesized that HIF-1 gene polymorphism was associated with
cardiovascular disease in OSA. And by using large-scale of study population(1000 OSA
patients), we examined all regions of the HIF-1 alpha to detect single-nucleotide
polymorphisms(SNPs), evaluated the pattern of linkage disequilibrium to compose haplotypes
in the gene, and performed association studies in OSA patients with and without
cardiovascular disease to achieve the following 3 objectives:(1)To identify specific SNPs of
HIF-1 alpha gene related to cardiovascular disease in OSA patients (CVD-OSA).(2)To assay the
functional activity of high risk SNPs of HIF-1 alpha on the transcription of VEGF gene.(3)To
confirm that the serum level of VEGF in CVD-OSA patients with high risk SNPs of HIF-1 are
higher than CVD-OSA patients without. The findings are expected to stratify the risk of OSA
patients to specific outcome, or response to specific therapy.
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Observational Model: Case Control, Time Perspective: Prospective
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