偏头痛患者中 CHRNA7 基因、hsa-miR-3158-5p 和 15q13.3 热点 CNV 的整体方法。

IF 2.8 3区 医学 Q2 NEUROSCIENCES Molecular Pain Pub Date : 2023-01-01 DOI:10.1177/17448069231152104
Sedat Yasin, Şenay Görücü Yılmaz, Sırma Geyik, Sibel Oğuzkan Balcı
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引用次数: 0

摘要

偏头痛是一种以严重头痛发作为特征的神经系统疾病。不同基因变异(如基因中的拷贝数变异(CNV)和微RNA(miRNA)表达)的组合可为该疾病的病理生理学、诊断和治疗提供整体方法。研究人员对 15-60 岁偏头痛患者(n=102;有先兆,n=43;无先兆,n=59)和非偏头痛患者(n=120)的 CNVs、胆碱能受体尼古丁α7 亚基(CHRNA7)基因和基因靶向 miRNAs(hsa-miR-548e-5p 和 hsa-miR-3158-5p)的表达进行了病例对照比较研究。遗传标记与生化指标(BMI、WBC、尿素、GFR、ESR、CRP、HBG)进行了比较。所有分析均通过实时定量 PCR(q-PCR)进行,并采用 2-ΔΔCT 方法计算折叠变化。用接收者操作曲线(ROC)分析了CHRNA7基因、CNV和miRNA的诊断能力。偏头痛患者的CHRNA7基因和hsa-miR-3158-5p下调,该基因通过CNV受miRNA控制(p < .05)。在偏头痛患者中,CVN 数量均检测到缺失和重复(p = .05)。CNV缺失的数量高于重复的数量。在 ROC 分析中将 CHRNA7-CNV-hsa-miR-3158-5p 一起建模时,曲线下面积(AUC)为 0.805,诊断能力为 "良好"。在偏头痛患者中,CHRNA7 基因可通过 CNVs 受控于 hsa-miR-3158-5p,从而调节疼痛机制。这三个遗传标记具有诊断潜力,可用于抗偏头痛治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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The holistic approach to the CHRNA7 gene, hsa-miR-3158-5p, and 15q13.3 hotspot CNVs in migraineurs.

Migraine is a neurological disease characterized by severe headache attacks. Combinations of different genetic variations such as copy number variation (CNV) in a gene and microRNA (miRNA) expression can provide a holistic approach to the disease as a pathophysiological, diagnostic, and therapeutic target. CNVs, the Cholinergic Receptor Nicotinic Alpha 7 Subunit (CHRNA7) gene, and expression of gene-targeting miRNAs (hsa-miR-548e-5p and hsa-miR-3158-5p) in migraineurs (n = 102; with aura, n = 43; without aura, n = 59) and non-migraines (n = 120) aged 15-60 years, comparative, case-control study was conducted. Genetic markers were compared with biochemical parameters (BMI, WBC, Urea, GFR, ESR, CRP, HBG). All analyzes were performed by quantitative Real-Time PCR (q-PCR) and fold change was calculated with the 2-ΔΔCT method. The diagnostic power of the CHRNA7 gene, CNV, and miRNAs were analyzed with the receiver operating curve (ROC). CHRNA7 gene and hsa-miR-3158-5p are down-regulated in migraineurs and the gene is controlled by this miRNA via CNVs (p < .05). Both deletion and duplication were detected in patients with migraine for CVN numbers (p = .05). The number of CNV deletions was higher than duplications. When CHRNA7-CNV-hsa-miR-3158-5p was modeled together in the ROC analysis, the area under the curve (AUC) was 0.805, and the diagnostic power was "good". In migraineurs, the CHRNA7 gene can be controlled by hsa-miR-3158-5p via CNVs to modulate the mechanism of pain. These three genetic markers have diagnostic potential and may be used in antimigraine treatments.

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来源期刊
Molecular Pain
Molecular Pain 医学-神经科学
CiteScore
5.60
自引率
3.00%
发文量
56
审稿时长
6-12 weeks
期刊介绍: Molecular Pain is a peer-reviewed, open access journal that considers manuscripts in pain research at the cellular, subcellular and molecular levels. Molecular Pain provides a forum for molecular pain scientists to communicate their research findings in a targeted manner to others in this important and growing field.
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