西伯利亚(俄罗斯)原发性头痛的遗传方面
引用次数: 2
摘要
原发性头痛是世界上常见的神经系统疾病。偏头痛(M)和紧张性头痛(TTH)是人群原发性头痛的主要结构;(1)背景:研究MTHFR(亚甲基四氢叶酸还原酶)和HTR2C(5-羟色胺受体2C)基因单核苷酸变异(SNVs)与西伯利亚(俄罗斯)欧洲人群M和TTH发生的关系;(2)方法:对192只成人进行调查,其中男性82只(42.7%),女性110只(57.3%)。对照组:健康成人81例,中位年龄49.5 [36];59)年;男性53例(66.7%),女性27例(33.3%)。头痛组包括111例原发性头痛患者,中位年龄54 [45];64]年,包括两个亚组:亚组1 (M) 39例;2亚组(TTH) 72例。采用TaqMan等位基因鉴别技术,采用PCR-RT检测MTHFR基因rs1801133、rs1801131和HTR2C基因rs6318等位基因及其基因型的携带情况;(3)结果:携带MTHFR基因A等位基因rs1801133与M的形成(p = 0.025)、TTH的形成(p = 0.022)、GA基因型与TTH的发生(p = 0.024)有统计学意义。携带G等位基因和MTHFR基因的TG和GG基因型,与MTHFR酶活性降低相关,不影响原发性头痛的发展。携带HTR2C基因杂合GC基因型(rs6318)与M的形成有统计学意义(p = 0.013);(4)结论:携带A等位基因(OR 1.77;95% CI 1.09-2.89)和GA基因型(OR 2.24;MTHFR基因的rs1801133是TTH发生的危险因素(95% CI 1.17-4.29) (p <0.05)。携带MTHFR基因的A等位基因rs1801133是M发生的危险因素(OR 1.97;95% ci 1.08-3.57;p < 0.05)。携带变异G等位基因和与MTHFR酶活性降低相关的rs1801131 GT和GG基因型并不影响原发性头痛的发展。在对照组中,与正常酶活性相关的T等位基因的患病率被注意到(p = 0.024)。携带HTR2C基因的杂合基因型CG SNV rs6318可使患偏头痛的风险增加3.6倍。本文章由计算机程序翻译,如有差异,请以英文原文为准。
Genetic aspects of primary headaches in Siberia (Russia)
Primary headaches are common neurological problem in the world. Migraine (M) and tension type headache (TTH) are the leaders in the structure of primary headaches in the population; (1) Background: The study of the association of single nucleotide variants (SNVs) of MTHFR (meth-ylenetetrahydrofolate reductase) and HTR2C (5-Hydroxytryptamine Receptor 2C) genes with M and TTH development in the European population in Siberia (Russia); (2) Methods: 192 adults were examined: 82 (42.7%) males and 110 (57.3%) females. Control group: 81 healthy adults, median age 49.5 [36; 59] years; 53 (66.7%) males and 27 (33.3%) females. Headache group consisted of 111 patients with primary headache, median age 54 [45; 64] years, including two subgroups: subgroup 1 (M) of 39 patients; subgroup 2 (TTH) of 72 patients. Carriage of alleles and genotypes rs1801133 and rs1801131 of the MTHFR gene and rs6318 of the HTR2C gene was determined using PCR-RT by TaqMan allelic discrimination technology; (3) Results: A statistically significant association of the carriage of the A allele rs1801133 of the MTHFR gene with the formation of M (p = 0.025) and TTH (p = 0.022), as well as the GA genotype with the development of TTH (p = 0.024) was revealed. Carriage of the G allele and the TG and GG genotypes of the MTHFR gene, associated with a decreased activity of the MTHFR enzyme, does not affect the development of primary headache. A statistically significant association was revealed between the carriage of the heterozygous GC genotype (rs6318) of the HTR2C gene and the formation of M (p = 0.013); (4) Conclusions: Carriage of the A allele (OR 1.77; 95% CI 1.09-2.89) and the GA genotype (OR 2.24; 95% CI 1.17-4.29) rs1801133 of the MTHFR gene is a risk factor for the development of TTH (p <0.05). Carriage of the A allele rs1801133 of the MTHFR gene is a risk factor for the development of M (OR 1.97; 95% CI 1.08-3.57; p <0.05). Carriage of the variant G allele and rs1801131 GT and GG genotypes associated with reduced activity of the MTHFR enzyme does not affect the development of primary headache. In the control group, the prevalence of the T allele associated with normal enzymatic activity was noted (p = 0.024). Carriage of the heterozygous genotype CG SNV rs6318 of the HTR2C gene increases the risk of developing migraine by 3.6 times.
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