Medchemexpress/ABT-199（同义词：GDC-0199；Venetoclax）/HY-15531/200mg-免疫在线蚂蚁淘旗下平台

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商品详细Medchemexpress/ABT-199（同义词：GDC-0199；Venetoclax）/HY-15531/200mg

Medchemexpress/ABT-199（同义词：GDC-0199；Venetoclax）/HY-15531/200mg

商品编号： HY-15531-10mM*1mLinDMSO

品牌： MedChemExp

市场价： ¥1600.00

美元价： 960.00

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

ABT-199isahighlypotent,orallybioavailableandBcl-2-selectiveinhibitorwithK_iof<0.01 nM.

CustomerValidation

•CancerCell.2017Oct9;32(4):490-505.e10.
•NatCellBiol.2017Oct;19(10):1226-1236.
•Haematologica.2017Apr;102(4):755-764.
•BrJCancer.2017Jun6;116(12):1572-1584.
•ACSMedChemLett.2015Jun22;6(8):948-52.
•JOvarianRes.2016Apr14;9(1):25.

•TranslationalCancerResearch(TCR).Vol6,No4.2017.

Description

ABT-199isahighlypotent,orallybioavailableandBcl-2-selectiveinhibitorwithK_iof<0.01 nm.="">

IC₅₀&Target

Ki:<0.01 nm="" (bcl-2),="" 48="" nm="" (bcl-xl),="" 245="" nm="" (bcl-w),="">444nM(Mcl-1)^[1]

InVitro

ABT-199potentlykillsFL5.12-BCL-2cells(EC₅₀=4nM),ABT-199showsmuchweakeractivityagainstFL5.12-BCL-XLcells(EC₅₀=261nM).ABT-199alsoshowsselectivityincellularmammaliantwo-hybridassays,whereitdisruptsBCL-2-BIMcomplexes(EC₅₀=3nM)butismuchlesseffectiveagainstBCL-XL-BCL-XS(EC₅₀=2.2μM)orMCL-1-NOXAcomplexes^[1].

InVivo

Afterasingleoraldoseof12.5mgperkgbodyweightinxenograftsderivedfromRS4;11cells(ALL),ABT-199causesamaximaltumorgrowthinhibition(TGI_max)of47%(P<0.001) and="" tumor="" growth="" delay="" (tgd)="" of="" 26%=""><>^[1].Treatmentofestablishedxenografted(amousexenograftmodeloftheT-ALLcelllineLOUCY)tumorswith100mgABT-199/kgfor4daysresultedinasignificantreductionofleukemicburden(P=0.0048)^[2].

ClinicalTrial

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References

[1].SouersAJ,etal.ABT-199,apotentandselectiveBCL-2inhibitor,achievesantitumoractivitywhilesparingplatelets.NatMed.2013Feb;19(2):202-8.
[2].PeirsS,etal.ABT-199mediatedinhibitionofBCL-2asanoveltherapeuticstrategyinT-cellacutelymphoblasticleukemia.Blood.2014Dec11;124(25):3738-47.
[3].BiC,etal.Inhibitionof4EBPphosphorylationmediatesthecytotoxiceffectofmechaNISTictargetofrapamycinkinaseinhibitorsinaggressiveB-celllymphomas.Haematologica.2017Apr;102(4):755-764.

PreparingStockSolutions

ConcentrationVolumeMass	1mg	5mg	10mg

1mM	1.1515mL	5.7575mL	11.5149mL
5mM	0.2303mL	1.1515mL	2.3030mL
10mM	0.1151mL	0.5757mL	1.1515mL

Pleaserefertothesolubilityinformationtoselecttheappropriatesolvent.

CellAssay
^[1]

ABT-199isdissolvedinDMSOandstored,andthendilutedwithappropriatemediabeforeuse^[1].

RS4;11cellsareseededat50,000perwellin96-wellplatesandtreatedwithcompoundsdilutedinhalf-logstepsstartingat1μMandendingat0.00005μM.Allotherleukemiaandlymphomacelllinesareseededat15,000-20,000cellsperwellintheappropriatemediumandincubatedwithABT-199orNavitoclaxfor48h.EffectsonproliferationaredeterminedusingCellTiterGloreagent.EC₅₀valuesaredeterminedbynonlinearregressionanalysisoftheconcentration-responsedata.MouseFL5.12-BCL-2andFL5.12-BCL-XLcellsarepropagatedandassessed.Bak^-/-Bax^-/-doubleknockoutmouseembryonicfibroblastsareseededinto96-wellmicrotiterplatesat5,000cellsperwellinDMEMsupplementedwith10%FBS.ABT-199inthesameculturemediumisaddedinhalf-logdilutionsstartingat5μM.Thecellsarethenincubatedat37°C(5%CO₂)for48h,andtheeffectsonproliferationaredeterminedusingCellTiterGloreagent^[1].MCEhasnotindependentlyconfirmedtheaccuracyofthesemethods.Theyareforreferenceonly.

AnimalAdministration
^[2]

ABT-199isformulatedin60%phosal50propyleneglycol,30%polyethyleneglycol400,and10%ethanol(Mice)^[2].

Mice^[2]
Nonobesediabetic/severecombinedimmunodeficientγ(NSG)miceareinjectedat6weeksofageinthetailveinwith150µLphosphate-bufferedsalinecontaining5×10⁶luciferase-labeledLOUCYcells.Atregulartimepoints,thebioluminescenceismeasuredusingtheIVISLuminaIIimagingsystem.At6weeks,thecellsareengraftedandthemicearerandomlydividedinto2groups(withanequalnumberofmalesandfemalesinbothgroups),andthetreatmentisstartedonday0.Micearetreatedwith100mgABT-199/kgbodyweightorwithvehicleviaoralgavagefor4consecutivedays.Atdays0,2,and4thebioluminesceneismeasured.Beforeimaging,themiceareinjectedintraperitoneallywith200µLofa15mg/mLfireflyD-luciferinpotassiumsaltsolutionandanesthetizedbyinhalationof5%isoflurane.Themiceareimaged10minutesafterluciferininjection.Thetotalbioluminescencesignalineachmouseiscalculatedviatheregionofinteresttool(totalcounts)intheLivingImagesoftware.MCEhasnotindependentlyconfirmedtheaccuracyofthesemethods.Theyareforreferenceonly.

References

[1].SouersAJ,etal.ABT-199,apotentandselectiveBCL-2inhibitor,achievesantitumoractivitywhilesparingplatelets.NatMed.2013Feb;19(2):202-8.
[2].PeirsS,etal.ABT-199mediatedinhibitionofBCL-2asanoveltherapeuticstrategyinT-cellacutelymphoblasticleukemia.Blood.2014Dec11;124(25):3738-47.
[3].BiC,etal.Inhibitionof4EBPphosphorylationmediatesthecytotoxiceffectofmechanistictargetofrapamycinkinaseinhibitorsinaggressiveB-celllymphomas.Haematologica.2017Apr;102(4):755-764.

MolecularWeight

868.44

Formula

C₄₅H₅₀ClN₇O₇S

CASNo.

1257044-40-8

Storage

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

Shipping

RoomtemperatureincontinentalUS;mayvaryelsewhere

Solvent&Solubility

DMSO:≥51mg/mL

ABT-199ispreparedin60%phosal50PG,30%PEG400and10%ethanol^[3].

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

References

[1].SouersAJ,etal.ABT-199,apotentandselectiveBCL-2inhibitor,achievesantitumoractivitywhilesparingplatelets.NatMed.2013Feb;19(2):202-8.
[2].PeirsS,etal.ABT-199mediatedinhibitionofBCL-2asanoveltherapeuticstrategyinT-cellacutelymphoblasticleukemia.Blood.2014Dec11;124(25):3738-47.
[3].BiC,etal.Inhibitionof4EBPphosphorylationmediatesthecytotoxiceffectofmechanistictargetofrapamycinkinaseinhibitorsinaggressiveB-celllymphomas.Haematologica.2017Apr;102(4):755-764.

Purity:99.67%

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