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蚂蚁淘在线 / 品牌中心 / Smartox / Smartox/Selective blocker of small conductance chloride channels/08CHL001-00100/0.1mg

Smartox/Selective blocker of small conductance chloride channels/08CHL001-00100/0.1mg

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￥1747.20

货号：08CHL001-00100

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商品描述

Chlorotoxin(Cltx) isaneurotoxinthatwasoriginallyisolatedfromthevenomofLeiurusquinquestriatus. Chlorotoxin isaspecificligandof gliomacells. Chlorotoxin bindstoCl^–channels(smallconductanceepithelialchloridechannels)inthebrainandspinalcordandinhibitsCl^– influx. Chlorotoxin mostprobablyactsasaspecificblocker,althoughresiduesbothinsideandoutsideoftheporeregionoftheCl^– channelsparticipateinchlorotoxinbinding.Itwasdemonstratedthat chlorotoxin inhibitsspecificallytheactivityof matrixmetalloproteinase-2(MMP-2) withoutaffectingMMP-1,MMP-3andMMP-9.MMP-2areupregulatedingliomacellsandrelatedcellsmaking chlorotoxin apromisingantitumoraldruganddiagnosistool.

Description:

Productcode:N/A.Category:Chloridechannels.Tags:163515-35-3,Chloride.

AAsequence: Met-Cys²-Met-Pro-Cys⁵-Phe-Thr-Thr-Asp-His-Gln-Met-Ala-Arg-Lys-Cys¹⁶-Asp-Asp-Cys¹⁹-Cys²⁰-Gly-Gly-Lys-Gly-Arg-Gly-Lys-Cys²⁸-Tyr-Gly-Pro-Gln-Cys³³-Leu-Cys³⁵-Arg-NH₂Disulfidebonds: Cys²-Cys¹⁹,Cys⁵-Cys²⁸,Cys¹⁶-Cys³³ andCys²⁰-Cys³⁵
Length(aa): 36
Formula: C₁₅₈H₂₄₉N₅₃O₄₇S₁₁
MolecularWeight: 3995.8Da
Appearance: Whitelyophilizedsolid
Solubility: waterandsalinebuffer
CASnumber: [163515-35-3]Source: Synthetic
Purityrate: >95%

Reference:

Chlorotoxininhibitsgliomacellinvasionviamatrixmetalloproteinase-2

Primarybraintumors(gliomas)havetheunusualABIlitytodiffuselyinfiltratethenormalbraintherebyevADIngsurgicaltreatment.Chlorotoxinisascorpiontoxinthatspecificallybindstothesurfaceofgliomacellsandimpairstheirabilitytoinvade.UsingarecombinantHis-CltxweisolatedandidentifiedtheprincipalCltxreceptoronthesurfaceofgliomacellsasmatrixmetalloproteinase-2(MMP-2).MMP-2isspecificallyup-regulatedingliomasandrelatedcancers,butisnotnormallyexpressedinbrain.WedemonstratethatCltxspecificallyandselectivelyinteractswithMMP-2isoforms,butnotwithMMP-1,-3,and-9,whicharealsoexpressedinmalignantgliomacells.Importantly,weshowthattheanti-invasiveeffectofCltxongliomacellscanbeexplainedbyitsinteractionswithMMP-2.CltxexertsadualeffectonMMP-2:itinhibitstheenzymaticactivityofMMP-2andcausesareductioninthesurfaceexpressionofMMP-2.ThesefindingssuggestthatCltxisaspecificMMP-2inhibitorwithsignificanttherapeuticpotentialforgliomasandotherdiseasesthatinvoketheactivityofMMP-2.

DeshaneJ.etal.(2003)Chlorotoxininhibitsgliomacellinvasionviamatrixmetalloproteinase-2.JBiolChem. PMID:12454020

Chlorotoxin,ascorpion-derivedpeptide,specificallybindstogliomasandtumorsofneuroectodermalorigin.

Highlymigratoryneuroectodermalcellsshareacommonembryonicoriginwithcellsofthecentralnervoussystem(CNS).Theyincludeenteric,parasympathetic,sympathoadrenal,andsensoryneuronsoftheperipheralnervoussystem,Schwanncells,melanocytes,endocrinecells,andcellsformingconnectivetissueofthefaceandneck.Becauseoftheircommonembryologicorigin,thesecellsandthetumorsthatderivefromthemcansharegeneticandantigenicphenotypeswithgliomas,tumorsderivedfromCNSglia.Werecentlydiscoveredthatchlorotoxin(ClTx),a4-kDpeptidepurifiedfromLeiurusquinquestriatusscorpion,isahighlyspecificMarkerforgliomacellsinbiopsytissues(Soroceanuetal.CancerRes58:4871-4879,1998)thatcantargettumorsinanimalmodels.WereportonthespecificityofClTxasamarkerfortumorsofneuroectodermaloriginthatincludeperipheralneuroectodermaltumors(PNET)andgliomas.Specifically,wehistochemicallystainedfrozenandparaffintissuesectionsofhumanbiopsytissuesfrom262patientswithasyntheticallymanufacturedandBIOLOGicallyactiveClTxbearinganN-terminalbiotin.Thevastmajority(74of79)ofprimaryhumanbraintumorsinvestigatedshowedabundantbindingofClTxwithgreaterthan90%ClTx-positivecellsineachsection.Bycomparison,32biopsiesofuninvolvedbrainusedforcomparisonwerelargelyClTx-negative,withonlyafewisolatedreactiveastrocytesshowingsomeClTxbinding.However,aswithgliomas,thevastmajorityofPNETsexaminedshowedspecificClTxbinding(31of34).Theseincludemedulloblastomas(4of4),neuroblastomas(6of7),ganglioneuromas(4of4),melanomas(7of7),adrenalpheochromocytomas(5of6),primitivePNET(1),smallcelllungcarcinoma(2of3),andEwing’ssarcoma(2of2).Underidenticalstainingconditions,normaltissuesfrombrain,skin,kidney,andlungwereconsistentlynegativeforClTx.Theseresultssuggestthatchlorotoxinisareliableandspecifichistopathologicalmarkerfortumorsofneuroectodermaloriginandthatchlorotoxinderivativeswithcytolyticactivitymayhavetherapeuticpotentialforthesecancers.

LyonsSA.,etal.(2002)Chlorotoxin,ascorpion-derivedpeptide,specificallybindstogliomasandtumorsofneuroectodermalorigin.Glia. PMID:12112367

Purificationandcharacterizationofchlorotoxin,achloridechannelligandfromthevenomofthescorpion

WehavepreviouslydemonstratedthatthevenomofthescorpionLeiurusquinquestriatusblockssmall-conductanceCl-channels,derivedfromepithelialcells,whenappliedtothecytoplasmicsurface.Wehavenowpurifiedtonearhomogeneity,andcharacterized,thecomponentresponsIBLeforthisblockingactivity.Itisasmallbasicpeptideof4,070Da.Theprimaryaminoacidstructureshowsconsiderablehomologytoaclassofpreviouslydescribedputativeshortinsectotoxins.AbriefcharacterizationofthekineticsofCl-channelblockaswellasademonstrationoftoxicitytoarthropodsisalsopresented.

DebinJA, etal.Purificationandcharacterizationofchlorotoxin,achloridechannelligandfromthevenomofthescorpion.Am.J.Physiol. PMID:8383429

ModulationofgliomacellmigrationandinvasionusingCl(-)andK(+)ionchannelblockers

Humanmalignantgliomasarehighlyinvasivetumors.Mechanismsthatallowgliomacellstodisseminate,migratingthroughthenarrowextracellularbrainspacesarepoorlyunderstood.Werecentlydemonstratedexpressionoflargevoltage-dependentchloride(Cl(-))currents,selectivelyexpressedbyhumangliomacellsinvitroandinsitu(Ullrichetal.,1998).CurrentsaresensitivetoseveralCl(-)channelblockers,includingchlorotoxin(Ctx),(UllrichandSontheimer;1996;Ullrichetal;1996),tetraethylammoniumchloride(TEA),andtamoxifen(RansomandSontheimer,1998).UsingTranswellmigrationassays,weshowthatblockadeofgliomaCl(-)channelsspecificallyinhibitstumorcellmigrationinadose-dependentmanner.Ctx(5microM),tamoxifen(10microM),andTEA(1mM)alsopreventedinvasionofhumangliomacellsintofetalratbrainaggregates,usedasaninvitromodeltoassesstumorinvasiveness.Anionreplacementstudiessuggestthatpermeationofchlorideionsthroughgliomachloridechannelisobligatoryforcellmigration.Osmoticallyinducedcellswellingandsubsequentregulatoryvolumedecrease(RVD)inculturedgliomacellswerereversiblypreventedby1mMTEA,10microMtamoxifen,andirreversiblyblockedby5microMCtxaddedtothehypotonicmedia.Cl(-)fluxesassociatedwithadaptiveshapechangeselicitedbycellswellingandRVDingliomacellswereinhibitedby5microMCtx,10microMtamoxifen,and1mMTEA,asdeterminedusingtheCl(-)-sensitivefluorescentdye6-methoxy-N-ethylquinoliniumiodide.Collectively,thesedatasuggestthatchloridechannelsingliomacellsmayenabletumorinvasiveness,presumablybyfacilitatingcellshapeandcellvolumechangesthataremoreconducivetomigrationandinvasion.

SoroceanuL.ModulationofgliomacellmigrationandinvasionusingCl(-)andK(+)ionchannelblockers. JNeurosci.PMID:10407033

Smartox生物素ProTx-I电压门控钠通道和T型Cav的阻断剂毒素I（ProTx-1；β-theraphotoxin-Tp1a）是一种毒素，最初是从Prixopelma pruriens（秘鲁绿色天鹅绒狼蛛）的毒液中分离出来的。此毒素可逆地抑制抗河豚毒素（TTX）的通道 Na v 1.8（IC 50 = 27 nM）和 Na v 1.2，Na v 1.5和Na v 1.7 ，IC 50 值为50至100 nM。此外， ProTx-I 改变了T型Ca v 3.1通道的电压依赖性活动（IC 50 = 50 nM），而不会影响灭活的电压依赖性。生物素ProTx-I是ProTx-I的生物素标签版本。

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