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Identification of Altered Regulatory Pathways in Diabetes Type II and Complieations through Expression Networks

机译:鉴定II型糖尿病II型的改变的调节途径和通过表达网络的促进

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Type 2 diabetes mellitus (T2D) is characterised by impaired glucose homeostasis and insulin resistance. Alteration in various biological cascades is observed during diabetes and its associated complications. Differentially expressed genes obtained from microarray data are used to construct co-expression networks integrated with interaction data. Our study uses this integrated functional networks concept to discover significantly altered pathways and regulations involved in T2D condition Major findings of our work include: novel interactions of GAPDH with SUMO4 and EGFR in GAPDH-EGFR_MicrovascularComplication; endothelial dysfunction due to impaired AKT1 expression caused by PXN and SRC interaction with altered eNOS expression as perceived in Inflammation_VascularDysfunction network; vascular complications due to altered interactions of β-catenin, VEGF and wnt signalling genes set off by oxidative stress as envisaged in the Wnt_VascularComplication network.
机译:2型糖尿病(T2D)的特征在于葡萄糖稳态和胰岛素抵抗力受损。在糖尿病期间观察到各种生物级联的改变及其相关的并发症。从微阵列数据获得的差异表达基因用于构造与交互数据集成的共表达网络。我们的研究使用这种集成的功能网络概念来发现我们工作的主要结果的显着改变的途径和法规包括:GAPDH与SUMO4和EGFR在GAPDH-EGFR_MICROVACULUSCOMPLICACACACACACACE中的新型相互作用;由PXT和SRC相互作用引起的AKT1表达受损引起的内皮功能障碍,与改变的ENOS表达在炎症中感觉到炎症_血管障碍网络;由于WNT_VASCULACUCLICACEL网络中设想的氧化胁迫,β-连环蛋白,VEGF和WNT信号传导基因的相互作用改变而导致的血管并发症。

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