原发性动脉高压患者内皮功能生物标志物和颈动脉内膜中层厚度变化与NOS3(rs2070744)和GNB3(rs5443)基因多态性的关系

Q3 Medicine Endocrine regulations Pub Date : 2022-04-01 DOI:10.2478/enr-2022-0012
A. Sydorchuk, L. Sydorchuk, A.F. Gutnitska, V. Dzhuryak, I. I. Kryvetska, R. Sydorchuk, Y. Ursuliak, O. Iftoda
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The connection of NOS3 (rs2070744) with decreased total NO metabolites (F=71.11; p<0.001), reduced NOS3 genes transcription activity (F=8.71; p<0.001) and increased sVCAM-1 (F=6.96; p=0.002), especially in the C-allele carriers (particularly in CC-genotype patients with lower NO – 16.46% and 40.88%; p<0.001), lowered the transcription activity of NOS3 gene – 46.03% 7 times (p<0.001), and become higher sVCAM-1 – 35.48% and 89.48% (p<0.001), respectively. ANOVA did not confirm the association of GNB3 (rs5443) gene with endothelial function and carotid IMT. Severe EAH was associated with increased carotid IMT – 50.0% (p<0.001) and 57.14% (p=0.007), wider carotid arteries – 17.36% (p=0.012) and 21.79% (p=0.004), and decreased NOS3 genes transcription activity – 34.54% (p=0.003). Atherosclerotic plaques were unilateral – 24.77% (χ2=5.35; p=0.021) or bilateral – 27.62% (χ2=5.79; p=0.016). 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引用次数: 3

摘要

摘要目标。本研究的目的是阐明原发性动脉高压(EAH)中内皮功能生物标志物和颈动脉“内膜-中膜”厚度(IMT)变化与GNB3(rs5443)和NOS3(rs2070744)基因多态性的关系。方法。100名EAH患者(48名对照)参与了病例对照研究。研究了可溶性血管细胞粘附分子(sVCAM-1)、总NO代谢产物(NO2-+NO3-)、NOS3基因的转录活性、内皮依赖性血流介导的肱动脉扩张(FMD-BA)和颈动脉IMT。通过TaqMan探针(CFX96)进行GNB3(rs5443)和NOS3(rs2070744)基因分型™实时PCR)。后果NOS3(rs2070744)与总NO代谢产物减少(F=77.11;p<0.001)、NOS3基因转录活性降低(F=8.71;p=0.001)和sVCAM-1增加(F=6.96;p=0.002,sVCAM-1分别升高了35.48%和89.48%(p<0.001)。ANOVA未证实GNB3(rs5443)基因与内皮功能和颈动脉IMT的相关性。严重EAH与颈动脉IMT增加相关——50.0%(p<0.001)和57.14%(p=0.007),颈动脉较宽——17.36%(p=0.012)和21.79%(p=0.0024),NOS3基因转录活性降低34.54%(p=0.003)。动脉粥样硬化斑块单侧为24.77%(χ2=5.35;p=0.021)或双侧为27.62%(χ2=5.79;p=0.016),FMD BA随着颈动脉直径的代偿性增加而减少11.80%——17.38%和21.99%(p<0.001),sVCAM-1减少20.49%(p=0.005)。NOS3(rs2070744),而不是GNB3(rs5443),与依赖内皮功能损伤的原发性动脉高压严重程度相关的基因,NOS3基因降低了转录活性。
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Endothelium function biomarkers and carotid intima-media thickness changes in relation to NOS3 (rs2070744) and GNB3 (rs5443) genes polymorphism in the essential arterial hypertension
Abstract Objective. The aim of the present study was to clarify the endothelial function biomarkers and carotid “intima media” thickness (IMT) changes in relation to GNB3 (rs5443) and NOS3 (rs2070744) genes polymorphism in the essential arterial hypertension (EAH). Methods. One-hundred EAH patients (48 – control) participated in the case-control study. Soluble vascular cell adhesion molecule (sVCAM-1), total NO metabolites (NO2–+NO3–), transcriptional activity of NOS3 gene, endothelium-dependent flow-mediated dilation of the brachial artery (FMD BA), and carotid IMT were studied. GNB3 (rs5443) and NOS3 (rs2070744) genotyping was performed by TaqMan probes (CFX96™Real-Time PCR). Results. The connection of NOS3 (rs2070744) with decreased total NO metabolites (F=71.11; p<0.001), reduced NOS3 genes transcription activity (F=8.71; p<0.001) and increased sVCAM-1 (F=6.96; p=0.002), especially in the C-allele carriers (particularly in CC-genotype patients with lower NO – 16.46% and 40.88%; p<0.001), lowered the transcription activity of NOS3 gene – 46.03% 7 times (p<0.001), and become higher sVCAM-1 – 35.48% and 89.48% (p<0.001), respectively. ANOVA did not confirm the association of GNB3 (rs5443) gene with endothelial function and carotid IMT. Severe EAH was associated with increased carotid IMT – 50.0% (p<0.001) and 57.14% (p=0.007), wider carotid arteries – 17.36% (p=0.012) and 21.79% (p=0.004), and decreased NOS3 genes transcription activity – 34.54% (p=0.003). Atherosclerotic plaques were unilateral – 24.77% (χ2=5.35; p=0.021) or bilateral – 27.62% (χ2=5.79; p=0.016). IMT---gt---0.9 mm was followed by a higher BP (p<0.001), FMD BA 11.80% decrease with compensatory increase in carotid arteries diameters – 17.38% and 21.99% (p<0.001) and sVCAM-1 by 20.49% (p=0.005). Conclusion. NOS3 (rs2070744), but not GNB3 (rs5443), gene associated with the essential arterial hypertension severity relying upon the endothelial function impairment and NOS3 genes reduced transcription activity.
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来源期刊
Endocrine regulations
Endocrine regulations Medicine-Endocrinology, Diabetes and Metabolism
CiteScore
2.70
自引率
0.00%
发文量
33
审稿时长
8 weeks
期刊最新文献
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