Medchemexpress/WIN 55212-2甲磺酸酯（同义词：（R）-（+）-WIN 55212）/HY-13291/10mM*1mL二甲基亚砜-免疫在线蚂蚁淘旗下平台

当前位置：首页 > 产品中心 > Small_molecule > Medchemexpress/WIN 55212-2甲磺酸酯（同义词：（R）-（+）-WIN 55212）/HY-13291/10mM*1mL二甲基亚砜

商品详细Medchemexpress/WIN 55212-2甲磺酸酯（同义词：（R）-（+）-WIN 55212）/HY-13291/10mM*1mL二甲基亚砜

Medchemexpress/WIN 55212-2甲磺酸酯（同义词：（R）-（+）-WIN 55212）/HY-13291/10mM*1mL二甲基亚砜

商品编号： HY-13291-10mM*1mLinDMSO

品牌： MedChemExp

市场价： ¥1380.00

美元价： 828.00

产地：美国(厂家直采)

公司：

产品分类：小分子

公司分类： Small_molecule

联系Q Q： 3392242852

电话号码： 4000-520-616

电子邮箱： info@ebiomall.com

立即询价

商品介绍

WIN55,212-2(Mesylate)isapotentaminoalkylindolecannABInoid(CB)receptoragoNISTwithK_isof62.3and3.3nMforhumanrecombinantCB1andCB2receptors,respectively.

CustomerValidation

•FrontMolNeurosci.2017Aug7;10:247.

Description	WIN55,212-2(Mesylate)isapotentaminoalkylindolecannabinoid(CB)receptoragonistwithK_isof62.3and3.3nMforhumanrecombinantCB1andCB2receptors,respectively.
IC₅₀&Target	Ki:62.3nM(humanrecombinantCB1),3.3nM(humanrecombinantCB2)
InVitro	WIN55,212-2ismorepotentinCHO-CB2cellsthaninCHO-CB1cellsbyafactorof6O.WIN55,212-2hasnoeffectonarachidonicacidreleaseinCHO-CB2orcontrolCHOcells.WIN55,212-2failstostimulateanyincreaseinintracellularCa²⁺upto10μM^[1].Inprimaryculturesofratcerebralcortexneurons,WIN55,212-2(0.01--100nM)increasesextracellularglutamatelevels,displayingabell-shapedconcentration-responsecurve.ThefacilitatoryeffectofWIN55,212-2(1nM)isfullycounteractedbySR141716A(10nM),bythereplacementofthenormalKrebsRinger-bicarbonatebufferwithalowCa²⁺medium(0.2mM)andbytheIP(3)receptorantagonistxestosponginC(1μM)^[2].WIN55,212-2evokesCGRPreleasefromTGneuronsinvitro(EC₅₀=26μM)inaconcentration-andcalcium-dependentmanner.WIN55,212-2-2neitherinhibitscapsaicin-evokesCGRPreleasenordoesitinhibitforskolin-,isoproteranol-orprostaglandinE2-stimulatedcAMPaccumulation.WIN55,212-2significantlyinhibits(EC₅₀=1.7μM)50mmK⁺-evokedCGRPreleasebyapproximately70%.WIN55,212-2inhibitionof50mmK⁺-evokedCGRPreleaseisnotreversedbyantagonistsofcannabinoidtype1(CB1)receptor,butismimicksinmagnitudeandpotency(EC₅₀=2.7μM)byitscannabinoid-inactiveenantiomerWIN55,212-2-3^[3].
InVivo	IntheprefrontalcortexWIN55,212-2(0.1and1mg/kgi.p.)increasesdialysateglutamatelevelsfromoftheawakerat,whilethelower(0.01mg/kg)andthehigher(2mg/kg)dosesareineffective.FurThermore,theWIN55,212-2(0.1mg/kg)-inducedincreaseofdialysateglutamatelevelsiscounteractedbypretreatmentwiththeselectiveCB(1)receptorantagonistSR141716A(0.1mg/kg,i.p.)andbythelocalperfusionwithalow-calciumRingersolution(Ca²⁺0.2mM)^[2].WIN55,212-2(0.5,1,3,5,10and15mg/kg,i.p.)doesnotaltertheseizurethresholdatlowdoses,whilehigherdosesofthedrugsignificantlyincreasesthethresholdinadose-dependentmanner.TheanticonvulsanteffectofWIN55,212-2,whichisobservedwithdosesashighas5mg/kg,canbeobservedwithdosesaslowas0.5mg/kgingroupspre-treatedwith20mg/kgofpioglitazone^[4].
References	[1].FelderCC,etal.ComparisonofthepharmacologyandsignaltransductionofthehumancannabinoidCB1andCB2receptors.MolPharmacol.1995Sep;48(3):443-50. [2].FerraroL,etal.ThecannabinoidreceptoragonistWIN55,212-2regulatesglutamatetransmissioninratcerebralcortex:aninvivoandinvitrostudy.CerebCortex.2001Aug;11(8):728-33. [3].PriceTJ,etal.Cannabinoidreceptor-independentactionsoftheaminoalkylindoleWIN55,212-2ontrigeminalsensoryneurons.BrJPharmacol.2004May;142(2):257-66. [4].PayandemehrB,etal.InvolvementofPPARreceptorsintheanticonvulsanteffectsofacannabinoidagonist,WIN55,212-2.ProgNeuropsychopharmacolBiolPsychiatry.2015Mar3;57:140-5.

PreparingStockSolutions

ConcentrationVolumeMass	1mg	5mg	10mg

1mM	1.9135mL	9.5674mL	19.1347mL
5mM	0.3827mL	1.9135mL	3.8269mL
10mM	0.1913mL	0.9567mL	1.9135mL

Pleaserefertothesolubilityinformationtoselecttheappropriatesolvent.

AnimalAdministration
^[3]

WIN55,212-2isformulatedin1%aqueoussolutionofDMSO.

Inexperiment1,differentdosesofWIN55,212-2(0.5,1,3,5,10and15mg/kg)areinjected60minpriortothedeterminationofclonicseizurethresholdinducedbyintravenousadministrationofPTZsolution.Controlanimalsreceivethesamevolumeofthevehicle(1%aqueoussolutionofDMSO).Thedosesandtimepointarechosenonthebasisofpilotstudies.Inexperiment2,inordertoconfirmtheanticonvulsanteffectsofpioglitazone,differentdoses(10,20,40and80mg/kg)areadministered4hpriortoPTZindistinctgroupsofmice.Thecorrespondingcontrolgroupreceivetheappropriatevehicle(CMC1%)atthesametimepoint.Inexperiment3,TheadditiveantiepilepticeffectsofWIN55,212-2andpioglitazoneareexamined;micereceiveacuteadministrationofpioglitazone(10or20mg/kg)3hbeforeWIN55,212-2(0.5or1mg/kg)and4hbeforePTZ.MCEhasnotindependentlyconfirmedtheaccuracyofthesemethods.Theyareforreferenceonly.

References

[1].FelderCC,etal.ComparisonofthepharmacologyandsignaltransductionofthehumancannabinoidCB1andCB2receptors.MolPharmacol.1995Sep;48(3):443-50.
[2].FerraroL,etal.ThecannabinoidreceptoragonistWIN55,212-2regulatesglutamatetransmissioninratcerebralcortex:aninvivoandinvitrostudy.CerebCortex.2001Aug;11(8):728-33.
[3].PriceTJ,etal.Cannabinoidreceptor-independentactionsoftheaminoalkylindoleWIN55,212-2ontrigeminalsensoryneurons.BrJPharmacol.2004May;142(2):257-66.
[4].PayandemehrB,etal.InvolvementofPPARreceptorsintheanticonvulsanteffectsofacannabinoidagonist,WIN55,212-2.ProgNeuropsychopharmacolBiolPsychiatry.2015Mar3;57:140-5.

MolecularWeight

522.61

Formula

C₂₈H₃₀N₂O₆S

CASNo.

131543-23-2

Storage

Powder	-20°C	3years
	4°C	2years
Insolvent	-80°C	6months
	-20°C	1month

Shipping

RoomtemperatureincontinentalUS;mayvaryelsewhere

Solvent&Solubility

DMSO:≥34mg/mL

*"<1 mg/ml"="" means="" slightly="" soluble="" or="" insoluble.="" "≥"="" means="" soluble,="" but="" saturation="">

Purity:98.98%

SelectBatch: