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《內(nèi)皮抑素的多硫酸化肝素修飾及修飾物的二級結(jié)構(gòu)和抗新生血管生成活性研究》由會員上傳分享���,免費在線閱讀,更多相關(guān)內(nèi)容在教育資源-天天文庫����。
1、內(nèi)皮抑素的多硫酸化肝素修飾及修飾物的二級結(jié)構(gòu)和抗新生血管生成活性研究譚海寧?,?��,王鳳山?*,?(?山東大學(xué)藥學(xué)院�����,?山東大學(xué)國家糖工程技術(shù)研究中心��,山東濟南250012fax:0086-531-88382548;E-mail:fswang@sdu.edu.cn)CovalentModificationofEndostatinwithPolysulfatedHeparinandTheirSecondaryStructureandAnti-angiogenesisActivityStudyHainingTan?,?,YuhongLiu?,?andFengshanWang?*,?(I
2��、nstituteofBiochemicalandBiotechnologicalDrug,SchoolofPharmaceuticalScience,ShandongUniversity,Jinan,250012,China,andNationalGlycoengineeringResearchCenter,ShandongUniversity,Jinan,250012,China.)ABSTRACTEndostatin(ES)isa20kDC-terminalfragmentofcollagenXVIIIthatinhibitsendothelialcellproliferat
3��、ion,angiogenesisandthegrowthofseveralprimarytumors.However,someobstacleslimititsclinicaluse,suchasneedofhighdosetomaintainitsefficacy,expensive,andpoorstability,etc.Inordertoovercometheseshortcomings,wechemicallymodifiedESbypoly-sulfatedheparin(PSH).Westudiedtheinhibitionson131endothelialcell
4�����、proliferationandangiogenesisofESanditsmodifiedproduct,respectively.ThechangesofthesecondarystructurewerealsostudiedbyCirculardichroism(CD)spectratoobtainbetterESderivatives.OurstudydemonstratedthatthemodifiedproducthasabetterheattolerancethanESandtheinhibitionsonendothelialcellproliferationan
5�����、dangiogenesisisbetterthanES.Theresultofsecondary-structureanalysissuggestedthatthepercentageofβ-turninthemodifiedproduct,animportantfactorontheactivityandstability,hadlittlechangecomparedwiththatofES.Collectively,thesefindingsdemonstratedthatthemodifiedproductofES(PSH-ES),withlittlesecondarys
6�、tructurechange,hasabetterheatstabilityandanti-angiogenesisactivitythanES.INTRODUCTIONNewbloodvesselsnourishingtumorgrowthformbyangiogenesis,whichmakeinhibitionofvesselformationanexcellenttargetforcancertherapy.Endostatin(ESAbbreviations:BCS,bovinecalfserum;CAM,chorioallantoicmembraneassay;CD,
7���、Circulardichroism;CM-II,Carboxymethylcellulose-II;DS,degreeofsubstitution;ES,endostatin;HUVEC,humanumbilicalveinendothelialcell;IR,inhibitionratio;ISV,intersegmentalvessels;LMWH,lowmolecularweightheparin;MTT,3-(4,5-dimethylthiazol-2-yl)-2,5-d
