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Expression Profiling of Nme7 Interactome in Experimental Models of Metabolic Syndrome

机译:NME7蛋白酶在代谢综合征实验模型中的表达分析

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Nucleoside diphosphate kinase 7, non-metastatic cells 7 (NME7) is an acknowledged member of ciliome and is involved in the biogenesis or function of cilia. As obesity and diabetes are common in several ciliopathies, we aimed to analyze changes of gene expression within Nme7interactome in genetically designed rat models of metabolic syndrome. We assessed the liver transcriptome by Affymetrix microarrays in adult males of 14 PXO recombinant inbred rat strains and their two progenitor strains, SHR-Lx and BXH2. In the strains with the lowest expression of Nme7, we have identified significant enrichment of transcripts belonging to Nme7 interactome. In the subsequent network analysis, we have identified three major upstream regulators - Hnf4a, Ppara and Nr1h4 and liver steatosis (p=0.0001) and liver necrosis/cell death (apoptosis of liver cells, p=0.0003) among the most enriched Tox categories. The mechanistic network reaching the top score showed substantial overlap with Assembly of non-motile cilium and Glucose metabolism disorder gene lists. In summary, we show in a genetic model of metabolic syndrome that rat strains with the lowest expression of Nme7 present gene expression shifts of Nme7 interactome that are perturbing networks relevant for carbohydrate and lipid metabolism as well as ciliogenesis.
机译:核苷二磷酸激酶7,非转移细胞7(NME7)是Cileiome的确认成员,并且参与纤毛的生物发生或功能。随着肥胖症和糖尿病在几种纤毛病中常见,我们旨在分析遗传设计的代谢综合征大鼠模型中NME7内酯内基因表达的变化。我们通过14pXO重组近交大鼠菌株及其两个祖母菌菌株,SHR-LX和BXH2评估了14个PXO重组近似大鼠菌株的患者雄性的肝脏转录组。在NME7表达最低的菌株中,我们已经确定了属于NME7蛋白酶的转录物的显着富集。在随后的网络分析中,我们已经确定了三个主要上游调节因子 - HNF4A,PPARA和NR1H4和肝脏脂肪变性(P = 0.0001)和肝脏坏死/细胞死亡(肝细胞凋亡,P = 0.0003)中最丰富的TOX类别。达到顶部得分的机械网络与非运动纤毛和葡萄糖代谢障碍基因名单的组装显着重叠。总之,我们展示了代谢综合征的遗传模型,即NME7蛋白酶蛋白表达的最低表达的大鼠菌株是扰动碳水化合物和脂质代谢以及纤毛发生的扰动网络。

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