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Assessment of DNA damage and mRNA/miRNA transcriptional expression profiles in hyperglycemic versus non-hyperglycemic patients with type 2 diabetes mellitus

机译:评估高血糖和非高血糖2型糖尿病患者的DNA损伤和mRNA / miRNA转录表达谱

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The development of type 2 diabetes mellitus (T2D) is associated with a number of genetic and environmental factors. Hyperglycemia, a T2D hallmark, is related to several metabolic complications, comorbidities and increased DNA damage. However, the molecular alterations of a proper glucose control are still unclarified. In this study, we aimed to evaluate DNA damage (comet assay), as well as to compare the transcriptional expression (mRNA and miRNA analyzed by the microarray technique) displayed by peripheral blood mononuclear cells (PBMCs) from three distinct groups: hyperglycemic T2D patients (T2D-H, n = 14), non-hyperglycemic T2D patients (T2D-N, n = 15), and healthy non-diabetic individuals (n = 16). The comet assay revealed significantly (p<0.05) higher levels of DNA damage in T2D-H group compared to bothT2D-N and control groups, while a significant difference was not observed between the control and T2D-N groups. After bioinformatics analysis, the differentially expressed mRNAs were subjected to functional enrichment analysis (DAVID) and inflammatory response was among the enriched terms found when comparing T2D-N with controls and T2D-H with T2D-N. Concerning the gene set enrichment and gene set analyses, among the differentially expressed gene sets, three were of interest: regulation of DNA repair (T2D-H versus T2D-N), superoxide response (T2D-H versus control group), and response to endoplasmic reticulum stress (T2D-H versus control group). We also identified miRNAs related with T2D and hyperglycemia not yet associated with these conditions in the literature. Some of the differentially expressed mRNAs were among the predicted targets of the differentially expressed miRNAs. Our results showed the association of hyperglycemia with increased DNA damage and aberrant expression of miRNAs and genes related to several biological processes, such as inflammation, DNA repair, ROS production and antioxidant defense, highlighting the importance of proper glycemic control. Moreover, the transcriptional expression of miRNAs provided novel information for understanding the regulatory mechanisms involved in the T2D progression.
机译:2型糖尿病(T2D)的发展与许多遗传和环境因素有关。高血糖是T2D的标志,与几种代谢并发症,合并症和DNA损伤增加有关。然而,尚不清楚适当的葡萄糖控制的分子改变。在这项研究中,我们旨在评估DNA损伤(彗星测定),并比较来自三个不同组的外周血单核细胞(PBMC)显示的转录表达(通过微阵列技术分析的mRNA和miRNA):高血糖T2D患者(T2D-H,n = 14),非高血糖T2D患者(T2D-N,n = 15)和健康的非糖尿病患者(n = 16)。彗星试验显示,与T2D-N和对照组相比,T2D-H组的DNA损伤水平显着(p <0.05),而对照组和T2D-N组之间未观察到显着差异。经过生物信息学分析后,将差异表达的mRNA进行功能富集分析(DAVID),并且在比较T2D-N与对照和T2D-H与T2D-N时发现了炎症反应。关于基因组富集和基因组分析,在差异表达的基因组中,三个是令人感兴趣的:DNA修复的调控(T2D-H与T2D-N),超氧化物反应(T2D-H与对照组)以及对内质网应激(T2D-H与对照组相比)。我们还在文献中鉴定了与T2D和高血糖症相关的miRNA,但尚未与这些疾病相关联。一些差异表达的mRNA属于差异表达的miRNA的预测目标。我们的结果表明,高血糖症与DNA损伤增加以及miRNA和基因异常表达的关联与多种生物学过程有关,例如炎症,DNA修复,ROS产生和抗氧化防御,突显了正确控制血糖的重要性。此外,miRNA的转录表达为理解T2D进程中涉及的调控机制提供了新的信息。

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