In Utero Exposure to Gestational Diabetes Alters DNA Methylation and Gene Expression of CDKN2A/B in Langerhans Islets of Rat Offspring

Z. Nazari, Alireza Shahryari, S. Ghafari, M. Nabiuni, M. Golalipour
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引用次数: 11

Abstract

Objective DNA methylation, a major epigenetic reprogramming mechanism, contributes to the increased prevalence of type 2 diabetes mellitus (T2DM). Based on genome-wide association studies, polymorphisms in CDKN2A/B are associated with T2DM. Our previous studies showed that gestational diabetes mellitus (GDM) causes apoptosis in β-cells, leading to a reduction in their number in pancreatic tissue of GDM-exposed adult rat offspring. The aim of this study was to examine the impact of intrauterine exposure to GDM on DNA methylation, mRNA transcription, as well as protein expression of these factors in the pancreatic islets of Wistar rat offspring. Our hypothesis was that the morphological changes seen in our previous study might have been caused by aberrant methylation and expression of CDKN2A/B. Materials and Methods In this experimental study, we delineated DNA methylation patterns, mRNA transcription and protein expression level of CDKN2A/B in the pancreatic islets of 15-week-old rat offspring of streptozotocin-induced GDM dams. We performed bisulfite sequencing to determine the DNA methylation patterns of CpGs in candidate promoter regions of CDKN2A/B. Furthermore, we compared the levels of mRNA transcripts as well as the cell cycle inhibitory proteins P15 and P16 in two groups by qPCR and western blotting, respectively. Results Our results demonstrated that hypomethylation of CpG sites in the vicinity of CDKN2A and CDKN2B genes is positively related to increased levels of CDKN2A/B mRNA and protein in islets of Langerhans in the GDM offspring. The average percentage of CDKN2A promoter methylation was significantly lower in GDM group compared to the controls (P<0.01). Conclusion We postulate that GDM is likely to exert its adverse effects on pancreatic β-cells of offspring through hypomethylation of the CDKN2A/B promoter. Abnormal methylation of these genes may have a link with β-cell dysfunction and diabetes. These data potentially lead to a novel approach to the treatment of T2DM.
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子宫内暴露于妊娠糖尿病会改变大鼠后代朗格汉斯胰岛DNA甲基化和CDKN2A/B基因表达
DNA甲基化是一种主要的表观遗传重编程机制,与2型糖尿病(T2DM)患病率增加有关。基于全基因组关联研究,CDKN2A/B多态性与T2DM相关。我们之前的研究表明,妊娠期糖尿病(GDM)导致妊娠期糖尿病暴露的成年大鼠后代胰腺组织中β-细胞凋亡,导致β-细胞数量减少。本研究的目的是研究宫内暴露于GDM对Wistar大鼠后代胰岛DNA甲基化、mRNA转录以及这些因子的蛋白表达的影响。我们的假设是,我们之前研究中看到的形态学变化可能是由CDKN2A/B的异常甲基化和表达引起的。材料和方法在本实验研究中,我们描绘了15周龄链脲佐菌素诱导的GDM大鼠后代胰岛中CDKN2A/B的DNA甲基化模式、mRNA转录和蛋白表达水平。我们进行亚硫酸盐测序以确定CDKN2A/B候选启动子区域CpGs的DNA甲基化模式。此外,我们通过qPCR和western blotting分别比较了两组小鼠mRNA转录本水平以及细胞周期抑制蛋白P15和P16的表达水平。我们的研究结果表明,GDM后代朗格汉斯岛CDKN2A和CDKN2B基因附近CpG位点的低甲基化与CDKN2A/B mRNA和蛋白水平升高呈正相关。GDM组CDKN2A启动子甲基化的平均百分比显著低于对照组(P<0.01)。结论GDM可能通过CDKN2A/B启动子的低甲基化作用对后代胰腺β细胞产生不良影响。这些基因的异常甲基化可能与β细胞功能障碍和糖尿病有关。这些数据可能会导致一种治疗T2DM的新方法。
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