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首页> 外文期刊>International Journal of Molecular Sciences >Deleterious Effect of Advanced CKD on Glyoxalase System Activity not Limited to Diabetes Aetiology
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Deleterious Effect of Advanced CKD on Glyoxalase System Activity not Limited to Diabetes Aetiology

机译:晚期CKD对乙二醛酶系统活性的有害作用并不局限于糖尿病病因

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Methylglyoxal production is increased in diabetes. Methylglyoxal is efficiently detoxified by enzyme glyoxalase 1 (GLO1). The aim was to study the effect of diabetic and CKD milieu on (a) GLO1 gene expression in peripheral blood mononuclear cells; (b) GLO1 protein levels in whole blood; and (c) GLO1 activity in RBCs in vivo in diabetic vs. non-diabetic subjects with normal or slightly reduced vs. considerably reduced renal function (CKD1-2 vs. CKD3-4). A total of 83 subjects were included in the study. Gene expression was measured using real-time PCR, and protein levels were quantified using Western blotting. Erythrocyte GLO1 activity was measured spectrophotometrically. GLO1 gene expression was significantly higher in subjects with CKD1-2 compared to CKD3-4. GLO1 protein level was lower in diabetics than in non-diabetics. GLO1 activity in RBCs differed between the four groups being significantly higher in diabetics with CKD1-2 vs. healthy subjects and vs. nondiabeticsfig with CKD3-4. GLO1 activity was significantly higher in diabetics compared to nondiabetics. In conclusion, both diabetes and CKD affects the glyoxalase system. It appears that CKD in advanced stages has prevailing and suppressive effects compared to hyperglycaemia. CKD decreases GLO1 gene expression and protein levels (together with diabetes) without concomitant changes of GLO1 activity.
机译:糖尿病中甲基乙二醛的产量增加。乙二醛酶1(GLO1)可有效地将甲基乙二醛解毒。目的是研究糖尿病和CKD环境对(a)外周血单个核细胞中GLO1基因表达的影响; (b)全血中的GLO1蛋白水平; (c)肾功能正常或轻微降低或显着降低的糖尿病患者与非糖尿病患者的体内红细胞体内的GLO1活性(CKD1-2与CKD3-4)。该研究共包括83名受试者。使用实时PCR测量基因表达,并使用蛋白质印迹法定量蛋白质水平。用分光光度法测定红细胞的GLO1活性。与CKD3-4相比,CKD1-2受试者的GLO1基因表达明显更高。糖尿病患者的GLO1蛋白水平低于非糖尿病患者。四组患者在红细胞中的GLO1活性差异显着,其中CKD1-2的糖尿病患者比健康受试者和CKD3-4的非糖尿病患者明显更高。与非糖尿病患者相比,糖尿病患者的GLO1活性明显更高。总之,糖尿病和CKD都会影响乙二醛酶系统。与高血糖症相比,晚期CKD似乎具有盛行和抑制作用。 CKD降低了GLO1基因的表达和蛋白质水平(与糖尿病一起发生),而不会伴随GLO1活性的改变。

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