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基于網(wǎng)絡藥理學及分子對接技術探討杞菊地黃丸治療干眼癥的作用機制

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[Abstract]ObjectiveToexploretheactiveingredientsand mechanismofactionof Qiju Dihuang Pilsinthetreatmentof dry eyebynetworkpharmacologyandmoleculardocking.MethodsTheactiveingredientsofQijuDihuangPilswereobtainedfromTCMSPand PharmacopoeiaofthePeople’sRepublicofChina,andtheirtargetswereconvertedintostandardgenenamesthroughtheUniProtplatfo. DiseasetargetserescrenedfromGeneCards,OMMandDisGeNETdatabases.TheCytoscape3.9.1softwareasusedtoconstructandanalyzetheompoundnetworktoobtaintemainactiveingredientsofthedrugProteininteractionsetwengenesintersectingwithQijuDihuangPillsnddryeereaalydoeGplafondtenmporedintothesoftaretoeenforyargetseesetio geneswereanalyzedforGOfunctionandKEGGpathwayenrichmentusingtheDAVIDdatabase,andfinaly,moleculardockingvalidation wascompletedbyAutoock4.2.6softare.Results149activeingredintsofQijuDiuangPilsand2O14dryeyeargetsweresreeed, withatotafil nin,stigmasterol,soetinndhargesicdedroteinaseB(AK)oosisctor),rote (TP53),nterleukin6(6),nteleukinbeta(B),strognreceptor1(ESR1)Keypathwaysicudedtedvanedglatiodproducts(AGE)-reeptorforadvancedglycationend-products(RAGE)signalingpathwayindiabeticcomplications,phospoiositide3- kinase(PI3K)-AKTsignalingpathwaymitogen-activatedproteinkinase(MAPK)signalingpathway,etc.ConclusionQijuDiuang PillsmaytratdyeytouhectiofqueceionyargessuchasTF5,6dsoItaexetattoryandinhibitapoptosisbyregulating theAGE-RAGEsignalingpathway,PI3K-AKTsignalingpathwayandMAPKsignalingpathway.

徐晨,等,基于網(wǎng)絡藥理學及分子對接技術探討杞菊地黃丸治療干眼癥的作用機制

干眼癥作為一種常見的多因素慢性眼表疾病,其主要病理特性是不穩(wěn)定淚膜引起的不適甚至視力障礙,同時伴有眼表炎癥、損傷及神經感覺異常[1]。(剩余14096字)

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