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Medchemexpress/Aloxistatin(同义词:E64d;E64c乙酯)/HY-100229/10mM*1mL二甲基亚砜
Description | Aloxistatin(E64d)isabroad-spectrumcell-permeablecysteineproteaseinhibitor. |
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IC50&Target | Cysteineprotease[1] |
InVitro | Inhibitionofprotease-resistantprionprotein(PrP-res)accumulationinScNBcellsbycysteineproteaseinhibitorAloxistatin(E64d)withIC50of0.5±0.11μM.ForthecellsurfacePrP-sendetection,PrP-senisimmunoprecipitatedfrommediatreatedwithphosphatidylinositol-specificphospholipaseC(PIPLC)toreleasepulse-35S-labeledPrP-senfromthecellsurface.Aloxistatinismaintainedat15μM,respectively,inthelabelingmediaofallbutthecontrolcells[1].Aloxistatin(E64d)(whichspecificallyblockscysteineproteases,butnotserineproteasessuchasgranzymes)isabletocompletelyblockturnoveroftheCatLsubstrateZ-Phe-Arg-aminomethylcoumarin,whenpre-incubatedwithNK-92orYT5cells[2].Aloxistatin(E64d)isabroad-spectrumcell-permeableinhibitorofcysteineproteases[3]. |
InVivo | OraladmiNISTrationofAloxistatin(E64d)toguineapigsresultsinadose-dependentreductioninbrain,CSFandplasmaAβ(40)andAβ(42).Aloxistatinalsocausesabiphasicdose-dependentreductioninbrainCTFβ.Aloxistatincausesadose-dependentincreaseinbrainsAβPPα.ThemeansAβPPαlevelsaresignificantlyhigherthanthenodosegroupforAloxistatindosesof5mg/kg/dayorgreaterwiththehighestAloxistatindoseresultinginthemaximumincreaseinsAβPPαofabout54%morethanthecontrolgroup.SimilartotheAβeffect,oralAloxistatinadministrationproducesabiphasicdose-dependentreductioninbraincathepsinBactivity.Theminimumeffectivedoseisabout1mg/kg/daywiththehighestAloxistatindosecausingthemaximumreductioninbraincathepsinBactivityofabout91%lowerthanthatofthecontrolgroup.Thus,AloxistatinreducesguineapigbraincathepsinBactivityinamannerwhichisconsistentwiththecompoundinhibitingcathepsinBβ-secretaseactivity[4].Aloxistatin(E64d)inhibitstheincreasesintheexpressionofAT1ARandACEgenesinrats.AdministrationofOlmesartanorAloxistatinreducestheincreaseinthesuperoxideproductionoftheintramyocardialcoronaryarteriesinHFrats[5]. |
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KinaseAssay [2] | TheCTLsandNKcells(0.8×106/mL)aretreatedwiththeinhibitorsL1(10-20μM)orAloxistatin(20-30μM)for24hrat37°Cin24-wellplates.Cellsarethenusedin51Cr-releaseassaysorarelysedtoexamineperforininWesternblots.Theinhibitorisalsoaddedatthesameconcentrationduringthe4hrreactionsinsome51Cr-releaseassays,asindicated.CelllysatesarepreparedusingNP-40lysisbuffer(25mMHEPES,250mMNaCl,2.5mMethylenediaminetetraaceticacid,0.1%volume/volumeNonidetP-40)andtotalproteinconcentrationisdeterminedusingtheBradfordassay.Equalamountsofproteinareloadedandresolvedon8%SDS-PAGEgels.Humanormouseperforinisdetectedusingtheappropriateantibodiesasindicated.Anti-actinantibodyisusedasaloADIngcontrol[2].MCEhasnotindependentlyconfirmedtheaccuracyofthesemethods.Theyareforreferenceonly. | ||||||||||||||||
CellAssay [3] | Aloxistatin(E64d)isdissolvedinDMSOandstored,andthendilutedwithappropriatemedium(finalDMSO0.1%)beforeuse[3]. CellproliferationandapoptosisareassessedbystainingforaproliferationMarker,Ki67,oranapoptoticmarker,cleavedcaspase3,followingtheprotocoldescribedaboveforthepolaritymarkers.MCF10variantsaregrownin3DrBMoverlayculturesfor4daysandaretreatedwith0.1%DMSO,5μMCA074Meor5μMAloxistatin.ThepercentageofstructuresthatarepositiveforKi67orcleavedcaspase3isdeterminedbycountingatotalof100structuresontwoseparatecoverslipswithaZeissAxiophotepifluorescentmicroscope.StructuresareconsideredKi67positiveiftheycontainedatleastonecellstainingforKi67.Structuresareconsideredtobecaspase3positiveiftheycontainedatleastonecellthatispositiveforcleavedcaspase3andthepositivecell(s)isnotlocalizedinthecenterofadevelopinglumen[3].MCEhasnotindependentlyconfirmedtheaccuracyofthesemethods.Theyareforreferenceonly. | ||||||||||||||||
AnimalAdministration [4][5] | Aloxistatin(E64d)issUSPendedinMe2SO[4]. MiceandPig[4] | ||||||||||||||||
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MolecularWeight | 342.43 | ||||||||||||
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Formula | C₁₇H₃₀N₂O₅ | ||||||||||||
CASNo. | 88321-09-9 | ||||||||||||
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Shipping | RoomtemperatureincontinentalUS;mayvaryelsewhere | ||||||||||||
Solvent&Solubility | DMSO:≥23mg/mL *"<1 mg/ml"="" means="" slightly="" soluble="" or="" insoluble.="" "≥"="" means="" soluble,="" but="" saturation="">1> Purity:98.22% 品牌介绍
托烷司琼临床评价药物相关作用适应症托烷司琼CAS号:89565-68-4英文名称:Tropisetron英文同义词:icf205-930;TROPICACID;TROPISETRON;SS-TROPISETRON;BETA-TROPISETRON;Tropisetron(ICS205930);TROPISHTRONHYDROCHLORIDE;Indole-3-carbonylchloride;3-Tropanylindole-3-carboxylate;lαH,5Αh-Tropan-3α-ylindole-3-carboxylate中文名称:托烷司琼中文同义词:托普西隆;托普西龙;曲匹西龙;托烷司琼;Β-托烷司琼;CS-348;Β-内托烷司琼;吲哚-3-甲酰氯;Β-托烷司琼(光学异构体);Β-托烷司琼,托烷司琼异构体CBNumber:CB3236404分子式:C17H20N2O2分子量:284.35MOLFile:89565-68-4.mol化学性质安全信息用途供应商112化学性质安全信息用途供应商112托烷司琼化学性质熔点:201-202°C沸点:448.5±35.0°C(Predicted)密度:1.26储存条件:2-8°C溶解度:H2O:soluble形态:solid酸度系数(pKa):15.38±0.30(Predicted)颜色:whiteCAS数据库:Chemicalbook89565-68-4(CASDataBaseReference)安全信息WGKGermany:3托烷司琼化学药品说明书托烷司琼|药物应用信息托烷司琼性质、用途与生产工艺临床评价Sorbe等报道本品对含顺铂(剂量50~89mg/m2)化疗方案引起的急性呕吐完全控制率为63%。58例恶性肿瘤化疗所致恶心、呕吐者,应用托烷司琼或昂丹司琼8mg分别在同一病人前后2个化疗周期的第1d给药前30min静脉注射,并用地塞米松10mg静脉滴注。结果两药控制急性及迟发性恶心、呕吐的疗效基本相似,均可达81%~100%。本品对强致吐化疗药物顺铂的止吐疗效突出。药物相关作用饮食可略为延长本品的吸收。本品与利福平、苯巴比妥等肝酶诱导药同时使用,可加快代谢,故快代谢型者需增加剂量,慢者则不必。西咪替丁等肝酶抑制药对本品血药浓度无明显影响。适应症托烷司琼临床用于预防和治疗癌症化疗引起的恶心和呕吐。化学性质结晶,熔点201-202℃(二氯甲烷-乙酸乙酯)。单盐酸托烷司琼(TropisetronMonohydroehloride):C17H20N2O2?HCI。[105826-92-4]。熔点283-285℃(分解)。用途有高效性和选择性的5-HT3受体拮抗剂。用于化疗所致的呕吐。用途为5-羟色胺拮抗药生产方法托品醇(I)和酰氯(Ⅱ)反应,可得托烷司琼。托烷司琼上下游产品信息上游原料托品醇下游产品
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