典型文献
Integrating systematic pharmacology-based strategy and experimental validation to explore mechanism of Tripterygium glycoside on cholangiocyte-related liver injury
文献摘要:
Objective:Tripterygium glycoside(TG)is widely used in clinical practice for its multiple bioactivities including anti-inflammatory and immunosuppressive effects.However,emerging studies have fre-quently reported TG-induced adverse reactions to multiple organs,especially liver.Here,this study aimed to investigate the mechanism of liver damage induced by TG and explore representative compo-nents to reflect TG hepatotoxicity.Methods:Network pharmacology was used to determine the potential targets of bile duct injury caused by TG.Next,the hepatotoxic effects of TG,triptolide(TP)and celastrol(CEL)were investigated and com-pared in vivo and in vitro.Liver function was determined by measuring serum transaminase and histopathology staining.The cell proliferation and apoptosis were determined by cell viability assay,scratch assay and flow cytometry.The expression of gene of interest was determined by qPCR and Western blot.Results:Based on the network pharmacological analysis of 12 bioactive ingredients found in TG,a total of 35 targets and 15 pathways related to bile duct injury were obtained.Both TG and TP resulted in cholan-giocyte damage and liver injury,as illustrated by increased levels of serum transaminase and oxidative stress,stimulated portal edema and lymphocytic infiltration and decreased expression of cholangiocyte marker,cytoskeletal 19.In addition,TG and TP inhibited cell proliferation and migration,arrested cell cycle and promoted Caspase-dependent apoptosis of cholangiocytes via suppressing the phosphorylation of extracellular regulated protein kinases 1/2(ERK1/2)and protein kinase B(AKT).While,CEL at equiv-alent dosage had no obvious hepatotoxicity.Conclusion:We revealed that TG-stimulated liver injury was specifically characterized by cholangiocyte damage and TP might be the decisive ingredient to reflect TG hepatotoxicity.Our results not only provide novel insights into the mechanism underlying the hepatotoxicity effects of TG but also offer reference for clinical rational use of TG.
文献关键词:
中图分类号:
作者姓名:
Yajing Li;Sen Li;Xiaoyong Xue;Ting Wang;Xiaojiaoyang Li
作者机构:
School of Life Sciences,Beijing University of Chinese Medicine,Beijing 100029,China;Beijing Research Institute of Chinese Medicine,Beijing University of Chinese Medicine,Beijing 100029,China
文献出处:
引用格式:
[1]Yajing Li;Sen Li;Xiaoyong Xue;Ting Wang;Xiaojiaoyang Li-.Integrating systematic pharmacology-based strategy and experimental validation to explore mechanism of Tripterygium glycoside on cholangiocyte-related liver injury)[J].中草药(英文版),2022(04):563-575
A类:
cholangiocyte,hepatotoxic,giocyte,cholangiocytes
B类:
Integrating,systematic,pharmacology,strategy,experimental,validation,explore,mechanism,Tripterygium,glycoside,related,liver,injury,Objective,widely,clinical,practice,its,multiple,bioactivities,including,anti,inflammatory,immunosuppressive,effects,However,emerging,studies,have,fre,quently,reported,induced,adverse,reactions,organs,especially,Here,this,study,aimed,damage,by,representative,compo,nents,reflect,hepatotoxicity,Methods,Network,was,potential,targets,bile,duct,caused,Next,triptolide,TP,celastrol,CEL,were,investigated,pared,vivo,vitro,Liver,function,determined,measuring,serum,transaminase,histopathology,staining,proliferation,apoptosis,viability,assay,scratch,flow,cytometry,expression,gene,interest,qPCR,blot,Results,Based,network,pharmacological,analysis,bioactive,ingredients,found,total,pathways,obtained,Both,resulted,illustrated,increased,levels,oxidative,stress,stimulated,portal,edema,lymphocytic,infiltration,decreased,marker,cytoskeletal,addition,inhibited,migration,arrested,cycle,promoted,Caspase,dependent,suppressing,phosphorylation,extracellular,regulated,protein,kinases,ERK1,AKT,While,equiv,alent,dosage,had,obvious,Conclusion,revealed,that,specifically,characterized,might,be,decisive,Our,results,not,only,provide,novel,insights,into,underlying,but,also,offer,reference,rational
AB值:
0.584542
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