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大鼠不同组织中偏头痛相关基因的甲基化

Methylation of migraine-related genes in different tissues of the rat.

作者信息

Labruijere Sieneke, Stolk Lisette, Verbiest Michael, de Vries René, Garrelds Ingrid M, Eilers Paul H C, Danser A H Jan, Uitterlinden André G, MaassenVanDenBrink Antoinette

机构信息

Dept. of Internal Medicine, Div. of Pharmacology, Erasmus Medical Center, Rotterdam, The Netherlands.

Dept. of Internal Medicine, Genetics Laboratory, Erasmus Medical Center, Rotterdam, The Netherlands.

出版信息

PLoS One. 2014 Mar 7;9(3):e87616. doi: 10.1371/journal.pone.0087616. eCollection 2014.

Abstract

17ß-Estradiol, an epigenetic modulator, is involved in the increased prevalence of migraine in women. Together with the prophylactic efficacy of valproate, which influences DNA methylation and histone modification, this points to the involvement of epigenetic mechanisms. Epigenetic studies are often performed on leukocytes, but it is unclear to what extent methylation is similar in other tissues. Therefore, we investigated methylation of migraine-related genes that might be epigenetically regulated (CGRP-ergic pathway, estrogen receptors, endothelial NOS, as well as MTHFR) in different migraine-related tissues and compared this to methylation in rat as well as human leukocytes. Further, we studied whether 17ß-estradiol has a prominent role in methylation of these genes. Female rats (n = 35) were ovariectomized or sham-operated and treated with 17β-estradiol or placebo. DNA was isolated and methylation was assessed through bisulphite treatment and mass spectrometry. Human methylation data were obtained using the Illumina 450k genome-wide methylation array in 395 female subjects from a population-based cohort study. We showed that methylation of the Crcp, Calcrl, Esr1 and Nos3 genes is tissue-specific and that methylation in leukocytes was not correlated to that in other tissues. Interestingly, the interindividual variation in methylation differed considerably between genes and tissues. Furthermore we showed that methylation in human leukocytes was similar to that in rat leukocytes in our genes of interest, suggesting that rat may be a good model to study human DNA methylation in tissues that are difficult to obtain. In none of the genes a significant effect of estradiol treatment was observed.

摘要

17β-雌二醇作为一种表观遗传调节剂,与女性偏头痛患病率增加有关。丙戊酸盐具有预防偏头痛的功效,它能影响DNA甲基化和组蛋白修饰,这表明表观遗传机制参与其中。表观遗传学研究通常在白细胞上进行,但尚不清楚甲基化在其他组织中的相似程度。因此,我们研究了可能受表观遗传调控的偏头痛相关基因(降钙素基因相关肽能通路、雌激素受体、内皮型一氧化氮合酶以及亚甲基四氢叶酸还原酶)在不同偏头痛相关组织中的甲基化情况,并将其与大鼠及人类白细胞中的甲基化进行比较。此外,我们研究了17β-雌二醇在这些基因甲基化过程中是否起重要作用。对35只雌性大鼠进行卵巢切除或假手术,并分别用17β-雌二醇或安慰剂进行处理。提取DNA,通过亚硫酸氢盐处理和质谱法评估甲基化情况。人类甲基化数据来自一项基于人群的队列研究中395名女性受试者的Illumina 450k全基因组甲基化芯片。我们发现,Crcp、Calcrl、Esr1和Nos3基因的甲基化具有组织特异性,白细胞中的甲基化与其他组织中的甲基化无关。有趣的是,不同基因和组织之间甲基化的个体间差异相当大。此外,我们还发现,在我们感兴趣的基因中,人类白细胞中的甲基化与大鼠白细胞中的甲基化相似,这表明在难以获取的组织中,大鼠可能是研究人类DNA甲基化的良好模型。在所有基因中均未观察到雌二醇处理的显著效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f6e/3946422/4985d63423d8/pone.0087616.g001.jpg

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