Abstract:ObjectiveTo investigate effect of cordycepin on p38MAPK pathway and TGF-β1express in NRK52E cells stimulated by high glucose.MethodsNRK52E cells were cultured in the mediun with normal glucose concentration(group NG),high glucose concentration(group HG)and high glucose concentration+cordycepin(group HG+C).The expression of p38MAPK and TGF-β1mRNA was measured by quantitative RT-PCR;the expression level of p-p38MAPK and TGF-β1protein was detected by Western blot.ResultsThe p38MAPK and TGF-β1mRNA in NRK52E cells were highly expressed in group HGcompared with group NG(P<0.01);the tendency of p-p38MAPK and TGF-β1protein expressed was accordance with expression of mRNA.However,cordycepin can significantly inhibit the activation of p38MAPK pathway and TGF-β1express in NRK52E cells stimulated by high glucose.ConclusionCordycepin can significantly inhibit the activation of p38MAPK pathway and TGF-β1express in NRK52E cells stimulated by high glucose.
梁泽智;黄洁平. 虫草素对高糖介导大鼠肾小管上皮细胞p38MAPK通路及TGF-β1表达的影响[J]. 中国当代医药, 2017, 24(17): 4-7.
LIANG Ze-zhi;HUANG Jie-ping. Effect of cordycepin on p38MAPK pathway and TGF-β1express in NRK52E cells stimulated by high glucose. 中国当代医药, 2017, 24(17): 4-7.
Nazir N,Siddiqui K,Al-Qasim S,et al.Meta-analysis of diabeticnephropathyassociatedgeneticvariantsin inflammation and angiogenesis involved in different biochemical pathways[J].BMC Med Genet,2014,15(1):103.
[2]
Sasai Y,Iwakawa K,Yanagida K,et al.Advanced glycation endproducts stimulate renal epithelial cells to release chemokines that recruit macrophages,leading to renal fibrosis[J]. Biosci Biotechnol Biochem,2012,76(9):1741-1745.
[3]
Goldberg R,Rubinstein AM,Gil N,et al.Role of heparanasedriven inflammatory cascade in pathogenesis of diabetic nephropathy[J].Diabetes,2014,63(12):4302-4313.
[4]
Marketou NP,Chrousos GP,Kanaka-Gantenbein C.Diabetic nephropathy in type 1 diabetes:a review of early natural history,pathogenesis and diagnosis[J].Diabetes Metab Res Rev,2016.
[5]
Rane MJ,Song Y,Jin S,et al.Interplay between Akt and p38 MAPK pathways in the regulation of renal tubular cell apoptosis associated with diabetic nephropathy[J].Am J Physiol Renal Physiol,2010,298(1):F49-F61.
[6]
Li X,Liu W,Wang Q,et al.Emodin suppresses cell proliferation and fibronectin expression via p38MAPK pathway in rat mesangial cells cultured under high glucose[J].Mol Cell Endocrinol,2009,307(1):157-162.
[7]
Xu Q,Tan Y,Zhang K,et al.Crosstalk between p38 and Smad3 through TGF-β1 in JEG-3 choriocarcinoma cells[J]. Int J Oncol,2013,43(4):1187-1193.
[8]
Kanasaki K,Taduri G,Koya D.Diabetic nephropathy:the role of inflammation in fibroblast activation and kidney fibrosis[J].Front Endocrinol,2013,4(1):7.
[9]
Chung ACK,Lan HY.Molecular mechanisms of TGF-β signaling in renal fibrosis[J].Curr Pathobiol Rep,2013,1(4):291-299.
Lan HY.Diverse roles of TGF-beta/Smads in renal fibrosis and inflammation[J].Int J Biol Sci,2011,7(7):1056-1067.
[12]
Meng XM,Chung ACK,Lan HY.Role of the TGF-β/BMP-7/ Smad pathways in renal diseases[J].Clin Sci(Lond),2013,124(4):243-254.
[13]
Lv ZM,Wang Q,Wan Q,et al.The role of the p38 MAPK signaling pathway in high glucose-induced epithelial-mesenchymal transition of cultured human renal tubular epithelial cells[J].PLoS One,2011,6(7):e22806.
[14]
Lan HY.Transforming growth factor-β/Smad signalling in diabetic nephropathy[J].Clin Exp Pharmacol Physiol,2012,39(8):731-738.
[15]
Rhyu DY,Yang Y,Ha H,et al.Role of reactive oxygen species in TGF-β1-induced mitogen-activated protein kinase activation and epithelial-mesenchymal transition in renal tubular epithelial cells[J].J Am Soc Nephrol,2005,16(3):667-675.
[16]
Tzeng TF,Liou SS,Chang CJ,et al.The ethanol extract of Lonicera japonica(Japanese honeysuckle)attenuates diabetic nephropathy by inhibiting p-38 MAPK activity in streptozotocin-induced diabetic rats[J].Planta Med,2014,80(2/3):121-129.
Cui J,Culbertson R,Mao Z,et al.A novel therapeutic treatment utilizing cordycepin and cladribine synergy to decrease adverse treatment effects in various cancer cell lines[J]. JESS,2013,2:20-24.
京公网安备 11010502046607号