差异 SLC6A4 甲基化:从出生到成年肥胖的预测性表观遗传标志物。
Differential SLC6A4 methylation: a predictive epigenetic marker of adiposity from birth to adulthood.
机构信息
Centre for Biological Sciences, Faculty of Natural and Environmental Sciences, University of Southampton, Southampton, UK.
NIHR Southampton Biomedical Research Centre, University of Southampton and University Hospital Southampton NHS Foundation Trust, Southampton, UK.
出版信息
Int J Obes (Lond). 2019 May;43(5):974-988. doi: 10.1038/s41366-018-0254-3. Epub 2019 Jan 8.
BACKGROUND
The early life environment may influence susceptibility to obesity and metabolic disease in later life through epigenetic processes. SLC6A4 is an important mediator of serotonin bioavailability, and has a key role in energy balance. We tested the hypothesis that methylation of the SLC6A4 gene predicts adiposity across the life course.
METHODS
DNA methylation at 5 CpGs within the SLC6A4 gene identified from a previous methyl binding domain array was measured by pyrosequencing. We measured DNA methylation in umbilical cord (UC) from children in the Southampton Women's Survey cohort (n = 680), in peripheral blood from adolescents in the Western Australian Pregnancy Cohort Study (n = 812), and in adipose tissue from lean and obese adults from the UK BIOCLAIMS cohort (n = 81). Real-time PCR was performed to assess whether there were corresponding alterations in gene expression in the adipose tissue.
RESULTS
Lower UC methylation of CpG5 was associated with higher total fat mass at 4 years (p = 0.031), total fat mass at 6-7 years (p = 0.0001) and % fat mass at 6-7 years (p = 0.004). Lower UC methylation of CpG5 was also associated with higher triceps skinfold thickness at birth (p = 0.013), 6 months (p = 0.038), 12 months (p = 0.062), 2 years (p = 0.0003), 3 years (p = 0.00004) and 6-7 years (p = 0.013). Higher maternal pregnancy weight gain (p = 0.046) and lower parity (p = 0.029) were both associated with lower SLC6A4 CpG5 methylation. In adolescents, lower methylation of CpG5 in peripheral blood was associated with greater concurrent measures of adiposity including BMI (p ≤ 0.001), waist circumference (p = 0.011), subcutaneous fat (p ≤ 0.001) and subscapular, abdominal and suprailiac skinfold thicknesses (p = 0.002, p = 0.008, p = 0.004, respectively). In adipose tissue, methylation of both SLC6A4 CpG5 (p = 0.019) and expression of SLC6A4 (p = 0.008) was lower in obese compared with lean adults.
CONCLUSIONS
These data suggest that altered methylation of CpG loci within SLC6A4 may provide a robust marker of adiposity across the life course.
背景
早期生活环境可能通过表观遗传过程影响生命后期肥胖和代谢疾病的易感性。SLC6A4 是 5-羟色胺生物利用度的重要介质,在能量平衡中起关键作用。我们检验了 SLC6A4 基因甲基化可预测整个生命过程中肥胖的假设。
方法
通过焦磷酸测序,对来自先前的甲基结合域阵列的 SLC6A4 基因内的 5 个 CpG 进行了 SLC6A4 基因的 DNA 甲基化检测。我们测量了南安普顿妇女调查队列(n=680)中儿童脐带(UC)中的 DNA 甲基化、西澳大利亚妊娠队列研究(n=812)中青少年的外周血中的 DNA 甲基化以及英国 BIOCLAIMS 队列(n=81)中瘦人和肥胖成年人的脂肪组织中的 DNA 甲基化。实时 PCR 用于评估脂肪组织中是否存在相应的基因表达改变。
结果
UC 中 CpG5 的低甲基化与 4 岁时总脂肪量较高相关(p=0.031)、6-7 岁时总脂肪量较高(p=0.0001)和 6-7 岁时脂肪百分比较高(p=0.004)。UC 中 CpG5 的低甲基化也与出生时(p=0.013)、6 个月时(p=0.038)、12 个月时(p=0.062)、2 岁时(p=0.0003)、3 岁时(p=0.00004)和 6-7 岁时(p=0.013)的三头肌皮褶厚度较高有关。较高的孕母体重增加(p=0.046)和较低的产次(p=0.029)均与 SLC6A4 CpG5 甲基化降低有关。在青少年中,外周血中 CpG5 的低甲基化与包括 BMI(p≤0.001)、腰围(p=0.011)、皮下脂肪(p≤0.001)和肩胛下、腹部和上髂皮褶厚度(p=0.002、p=0.008、p=0.004)在内的当前肥胖程度指标显著相关。在脂肪组织中,SLC6A4 中的 CpG5 甲基化(p=0.019)和 SLC6A4 表达(p=0.008)在肥胖个体中均低于瘦个体。
结论
这些数据表明,SLC6A4 内 CpG 位点的甲基化改变可能为整个生命过程中的肥胖提供了一个稳健的标志物。
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