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  2. Membrane Transporter/Ion Channel
  3. BCRP
  4. Ko 143

Ko 143 是有效且選擇性的 ATP 結(jié)合盒亞家族 G 成員 2 (ABCG2/BCRP) 抑制劑。Ko 143 比 P-gp 和 MRP-1 運輸?shù)鞍赘叱?200 倍的選擇性。

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Ko 143 Chemical Structure

Ko 143 Chemical Structure

CAS No. : 461054-93-3

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Customer Review

MCE 顧客使用本產(chǎn)品發(fā)表的 39 篇科研文獻(xiàn)

IF
Proliferation Assay

    Ko 143 purchased from MCE. Usage Cited in: Drug Deliv. 2017 Nov;24(1):1453-1459.  [Abstract]

    Fluorescent substrates accumulate in the organoids. The organoids are incubated in Hoechst 33342 with or without YHO-13177 or Ko143 for 20, 60 and 100?minutes, respectively. Ko143 and YHO-13177 notably decrease the fluorescence intensity of Hoechst 33342 in the organoids.

    Ko 143 purchased from MCE. Usage Cited in: J Drug Target. 2016;24(5):441-9.  [Abstract]

    Cells are co-treated with 5?μM of free LY156758 or an equivalent dose of SMA-LY156758 and either vehicle control (0.01% DMSO), Elacridar (1?μM), KO143 (5?μM), Valspodar (1?μM) or a combination of efflux inhibitors for 6?h.

    Ko 143 purchased from MCE. Usage Cited in: J Pharm Biomed Anal. 2012 Jul;66:232-9.  [Abstract]

    Effect of pharmacological inhibition of drug efflux transporters on brain distribution of FLZ in rats. The rats receive 35 mg/kg FLZ via tail vein injection 10 min after intravenous administration of 20 mg/kg Zosuquidar or 7.5 mg/kg ko143.

    • 生物活性

    • 實驗參考方法

    • 純度 & 產(chǎn)品資料

    • 參考文獻(xiàn)

    生物活性

    Ko 143 is a potent and selective ATP-binding cassette subfamily G member 2 (ABCG2/BCRP) inhibitor. Ko 143 displays >200-fold selectivity over P-gp and MRP-1 transporters[1][2].

    IC50 & Target

    EC90: 26 nM (BCRP)
    細(xì)胞效力
    (Cellular Effect)
    Cell Line Type Value Description References
    A549 IC50
    122.83 nM
    Compound: Ko143
    Chemo-sensitizing activity against becatecarin-selected ABCG2-overexpressing human A549/Bec150 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 1625.4 +/-413.42 nM)
    Chemo-sensitizing activity against becatecarin-selected ABCG2-overexpressing human A549/Bec150 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 1625.4 +/-413.42 nM)
    		[PMID: 34496204]
    A549 IC50
    127.7 nM
    Compound: Ko143
    Chemo-sensitizing activity against becatecarin-selected ABCG2-overexpressing human A549/Bec150 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 1162.92 +/-250.73 nM)
    Chemo-sensitizing activity against becatecarin-selected ABCG2-overexpressing human A549/Bec150 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 1162.92 +/-250.73 nM)
    		[PMID: 34496204]
    A549 IC50
    236.09 nM
    Compound: Ko143
    Chemo-sensitizing activity against human A549 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 376.13 +/-60.17 nM)
    Chemo-sensitizing activity against human A549 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 376.13 +/-60.17 nM)
    		[PMID: 34496204]
    A549 IC50
    326.96 nM
    Compound: Ko143
    Chemo-sensitizing activity against human A549 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb =555.44 +/-125.7 nM)
    Chemo-sensitizing activity against human A549 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb =555.44 +/-125.7 nM)
    		[PMID: 34496204]
    A549 IC50
    37.17 nM
    Compound: Ko143
    Chemo-sensitizing activity against becatecarin-selected ABCG2-overexpressing human A549/Bec150 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 552.97 +/-106.74 nM)
    Chemo-sensitizing activity against becatecarin-selected ABCG2-overexpressing human A549/Bec150 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 552.97 +/-106.74 nM)
    		[PMID: 34496204]
    A549 IC50
    41.83 nM
    Compound: Ko143
    Chemo-sensitizing activity against human A549 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 82.47 +/-24.25 nM)
    Chemo-sensitizing activity against human A549 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 82.47 +/-24.25 nM)
    		[PMID: 34496204]
    Caco-2 IC50
    > 30 μM
    Compound: Ko143
    Inhibition of P-gp transporter in human Caco2 cells using [3H]-digoxin as substrate measured at 30 to 120 mins by microplate scintillation and luminescence counting analysis
    Inhibition of P-gp transporter in human Caco2 cells using [3H]-digoxin as substrate measured at 30 to 120 mins by microplate scintillation and luminescence counting analysis
    		[PMID: 26642765]
    HEK293 EC50
    0.012 μM
    Compound: Ko143
    Inhibition of ABCG2 (unknown origin) transfected in HEK293 cells assessed as inhibition of mitoxantrone efflux at 5 uM after 30 mins in presence of 0.1 uM (2E,2'E)-1,1'-(1,4-Phenylene)bis(3-(2,6-dimethoxyphenyl)-prop-2-en-1-one) by flow cytometry
    Inhibition of ABCG2 (unknown origin) transfected in HEK293 cells assessed as inhibition of mitoxantrone efflux at 5 uM after 30 mins in presence of 0.1 uM (2E,2'E)-1,1'-(1,4-Phenylene)bis(3-(2,6-dimethoxyphenyl)-prop-2-en-1-one) by flow cytometry
    		[PMID: 24611893]
    HEK293 EC50
    0.029 μM
    Compound: Ko143
    Inhibition of ABCG2 (unknown origin) transfected in HEK293 cells assessed as inhibition of mitoxantrone efflux after 30 mins by flow cytometry relative to control
    Inhibition of ABCG2 (unknown origin) transfected in HEK293 cells assessed as inhibition of mitoxantrone efflux after 30 mins by flow cytometry relative to control
    		[PMID: 24611893]
    HEK293 IC50
    0.05 μM
    Compound: Ko143
    Inhibition of ABCG2-mediated mitoxantrone efflux in HEK293 cells by flow cytometry
    Inhibition of ABCG2-mediated mitoxantrone efflux in HEK293 cells by flow cytometry
    		[PMID: 22165858]
    HEK293 EC50
    0.074 μM
    Compound: Ko143
    Inhibition of ABCG2 (unknown origin) expressed in HEK293 cells assessed as reduction in mitoxantrone efflux after 30 mins by flow cytometric analysis
    Inhibition of ABCG2 (unknown origin) expressed in HEK293 cells assessed as reduction in mitoxantrone efflux after 30 mins by flow cytometric analysis
    		[PMID: 27376492]
    HEK293 IC50
    0.09 μM
    Compound: Ko143
    Inhibition of ABCG2 (unknown origin) expressed in HEK293 cells assessed as reduction in mitoxantrone efflux after 30 mins by FACS method
    Inhibition of ABCG2 (unknown origin) expressed in HEK293 cells assessed as reduction in mitoxantrone efflux after 30 mins by FACS method
    		[PMID: 25272055]
    HEK293 EC50
    0.09 μM
    Compound: Ko143
    Inhibition of ABCG2 (unknown origin)-mediated mitoxantrone efflux expressed in HEK293 cells after 30 mins by flow cytometric analysis
    Inhibition of ABCG2 (unknown origin)-mediated mitoxantrone efflux expressed in HEK293 cells after 30 mins by flow cytometric analysis
    		[PMID: 24304387]
    HEK293 IC50
    2.53 nM
    Compound: Ko143
    Chemo-sensitizing activity against human HEK293 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 2.74 +/-0.69 nM)
    Chemo-sensitizing activity against human HEK293 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 2.74 +/-0.69 nM)
    		[PMID: 34496204]
    HEK293 IC50
    2.69 nM
    Compound: Ko143
    Chemo-sensitizing activity against human HEK293 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 2.78 +/-0.58 nM)
    Chemo-sensitizing activity against human HEK293 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 2.78 +/-0.58 nM)
    		[PMID: 34496204]
    HEK293 IC50
    38.59 nM
    Compound: Ko143
    Chemo-sensitizing activity against human HEK293 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 35.17 +/-8.65 nM)
    Chemo-sensitizing activity against human HEK293 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 35.17 +/-8.65 nM)
    		[PMID: 34496204]
    HEK293 IC50
    8.36 nM
    Compound: Ko143
    Chemo-sensitizing activity against ABCG2-overexpressing human HEK293/482R cells cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 99.55 +/-7.35 nM)
    Chemo-sensitizing activity against ABCG2-overexpressing human HEK293/482R cells cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 99.55 +/-7.35 nM)
    		[PMID: 34496204]
    HEK293 IC50
    9.94 nM
    Compound: Ko143
    Chemo-sensitizing activity against ABCG2-overexpressing human HEK293/482R cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 239.91 +/-25 nM)
    Chemo-sensitizing activity against ABCG2-overexpressing human HEK293/482R cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 239.91 +/-25 nM)
    		[PMID: 34496204]
    HEK293 IC50
    96.43 nM
    Compound: Ko143
    Chemo-sensitizing activity against ABCG2-overexpressing human HEK293/482R cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 558.68 +/-81.31 nM)
    Chemo-sensitizing activity against ABCG2-overexpressing human HEK293/482R cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 558.68 +/-81.31 nM)
    		[PMID: 34496204]
    K562 IC50
    71.53 μM
    Compound: Ko143
    Cytotoxicity against human K562 cells incubated for 48 hrs by MTT assay
    Cytotoxicity against human K562 cells incubated for 48 hrs by MTT assay
    		[PMID: 33938746]
    K562/A02 IC50
    58.74 μM
    Compound: Ko143
    Cytotoxicity against P-gp overexpressing human K562/A02 cells incubated for 48 hrs by MTT assay
    Cytotoxicity against P-gp overexpressing human K562/A02 cells incubated for 48 hrs by MTT assay
    		[PMID: 33938746]
    MCF7 IC50
    0.23 μM
    Compound: Ko143
    Inhibition of BCRP expressed in MCF7 MX cells by Hoechst 33342 staining
    Inhibition of BCRP expressed in MCF7 MX cells by Hoechst 33342 staining
    		[PMID: 19932960]
    MCF7 IC50
    0.39 μM
    Compound: Ko143
    Inhibition of BCRP expressed in MCF-7 MX cells using Hoechst 33342 staining
    Inhibition of BCRP expressed in MCF-7 MX cells using Hoechst 33342 staining
    		[PMID: 21354800]
    MDCK IC50
    > 50000 nM
    Compound: 2, Ko143
    Inhibition of ABCC2 overexpressed in MDCK cells at 100 uM by flow cytometric-based chloromethylfluorescein-diacetate accumulation assay
    Inhibition of ABCC2 overexpressed in MDCK cells at 100 uM by flow cytometric-based chloromethylfluorescein-diacetate accumulation assay
    		[PMID: 19170519]
    MDCK IC50
    0.074 μM
    Compound: Ko143
    Inhibition of BCRP expressed in MDCK cells by pheophorbide A assay
    Inhibition of BCRP expressed in MDCK cells by pheophorbide A assay
    		[PMID: 19932960]
    MDCK IC50
    0.21 μM
    Compound: Ko143
    Inhibition of BCRP expressed in MDCK cells using Hoechst 33342 staining
    Inhibition of BCRP expressed in MDCK cells using Hoechst 33342 staining
    		[PMID: 21354800]
    MDCK IC50
    93.27 μM
    Compound: Ko143
    Cytotoxicity against dog MDCK cells after 48 hrs by MTT assay
    Cytotoxicity against dog MDCK cells after 48 hrs by MTT assay
    		[PMID: 35247755]
    MDCK-II IC50
    0.128 μM
    Compound: Ko143
    Inhibition of GFP-tagged human BCRP expressed in MDCK2 cells pre-incubated for 30 mins followed by Hoechst 33342 addition and further incubated for 120 mins by Hoechst 33342 accumulation assay
    Inhibition of GFP-tagged human BCRP expressed in MDCK2 cells pre-incubated for 30 mins followed by Hoechst 33342 addition and further incubated for 120 mins by Hoechst 33342 accumulation assay
    		[PMID: 25855895]
    MDCK-II IC50
    0.215 μM
    Compound: Ko143
    Inhibition of human BCRP expressed in MDCK2 cells assessed as accumulation of Hoechst 33342 preincubated for 30 mins before Hoechst 33342 addition measured after 120 mins by fluorescence assay
    Inhibition of human BCRP expressed in MDCK2 cells assessed as accumulation of Hoechst 33342 preincubated for 30 mins before Hoechst 33342 addition measured after 120 mins by fluorescence assay
    		[PMID: 23851114]
    MDCK-II IC50
    0.221 μM
    Compound: Ko143
    Inhibition of recombinant human GFP-fused ABCG2 expressed in MDCK2 cells assessed as reduction in Hoechst 33342 efflux preincubated for 30 mins followed by Hoechst 33342 addition measured immediately at 60 sec time interval for 120 mins by fluorescence as
    Inhibition of recombinant human GFP-fused ABCG2 expressed in MDCK2 cells assessed as reduction in Hoechst 33342 efflux preincubated for 30 mins followed by Hoechst 33342 addition measured immediately at 60 sec time interval for 120 mins by fluorescence as
    		[PMID: 27676469]
    MDCK-II IC50
    0.24 μM
    Compound: Ko143
    Inhibition of human C-terminal GFP-tagged ABCG2 expressed in MDCK2 cells using pheophorbide A as substrate preincubated for 20 mins followed by substrate addition measured after 120 mins by flow cytometry
    Inhibition of human C-terminal GFP-tagged ABCG2 expressed in MDCK2 cells using pheophorbide A as substrate preincubated for 20 mins followed by substrate addition measured after 120 mins by flow cytometry
    		[PMID: 27100033]
    MDCK-II IC50
    0.25 μM
    Compound: Ko143
    Inhibition of human BCRP expressed in MDCK2 cells assessed as Hoechst 33342 accumulation treated 30 mins before Hoechst 33342 addition measured up to 120 mins by fluorescence assay
    Inhibition of human BCRP expressed in MDCK2 cells assessed as Hoechst 33342 accumulation treated 30 mins before Hoechst 33342 addition measured up to 120 mins by fluorescence assay
    		[PMID: 24184213]
    MDCK-II IC50
    0.25 μM
    Compound: Ko143
    Inhibition of human BCRP expressed in MDCK2 cells preincubated for 30 mins prior to Hoechst 33342 addition measured every 60 secs up to 120 mins by Hoechst 33342 accumulation assay
    Inhibition of human BCRP expressed in MDCK2 cells preincubated for 30 mins prior to Hoechst 33342 addition measured every 60 secs up to 120 mins by Hoechst 33342 accumulation assay
    		[PMID: 23017888]
    MDCK-II IC50
    0.26 μM
    Compound: Ko143
    Inhibition of human BCRP expressed in MDCK2 cells assessed as Hoechst 33342 accumulation preincubated for 30 mins by fluorimetry
    Inhibition of human BCRP expressed in MDCK2 cells assessed as Hoechst 33342 accumulation preincubated for 30 mins by fluorimetry
    		[PMID: 22112540]
    MDCK-II IC50
    0.276 μM
    Compound: Ko143
    Inhibition of recombinant human GFP-fused ABCG2 expressed in MDCK2 cells assessed as reduction in pheophorbide A efflux preincubated for 30 mins followed by pheophorbide A addition measured after 2 hrs by flow cytometry
    Inhibition of recombinant human GFP-fused ABCG2 expressed in MDCK2 cells assessed as reduction in pheophorbide A efflux preincubated for 30 mins followed by pheophorbide A addition measured after 2 hrs by flow cytometry
    		[PMID: 27676469]
    MDCK-II IC50
    0.33 μM
    Compound: Ko143
    Inhibition of human BCRP expressed in MDCK2 cells assessed as pheophorbide A accumulation treated 30 mins before pheophorbide A addition measured up to 120 mins by flow cytometry
    Inhibition of human BCRP expressed in MDCK2 cells assessed as pheophorbide A accumulation treated 30 mins before pheophorbide A addition measured up to 120 mins by flow cytometry
    		[PMID: 24184213]
    MDCK-II IC50
    0.354 μM
    Compound: Ko143
    Inhibition of human BCRP expressed in MDCK2 cells assessed as accumulation of pheophorbide-A preincubated for 30 mins before pheophorbide-A addition measured after 120 mins by flow cytometry
    Inhibition of human BCRP expressed in MDCK2 cells assessed as accumulation of pheophorbide-A preincubated for 30 mins before pheophorbide-A addition measured after 120 mins by flow cytometry
    		[PMID: 23851114]
    MDCK-II GI50
    10.9 μM
    Compound: Ko143
    Cytotoxicity against wild-type MDCK2 cells assessed as reduction in cell viability after 72 hrs by MTT assay
    Cytotoxicity against wild-type MDCK2 cells assessed as reduction in cell viability after 72 hrs by MTT assay
    		[PMID: 27280693]
    MDCK-II GI50
    10.9 μM
    Compound: Ko143
    Intrinsic cytotoxicity against parental MDCK2 cells incubated for 72 hrs by MTT assay
    Intrinsic cytotoxicity against parental MDCK2 cells incubated for 72 hrs by MTT assay
    		[PMID: 27148793]
    MDCK-II GI50
    10.9 μM
    Compound: Ko143
    Cytotoxicity against MDCK2 cells assessed as reduction in cell viability after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells assessed as reduction in cell viability after 72 hrs by MTT assay
    		[PMID: 27100033]
    MDCK-II GI50
    11.1 μM
    Compound: Ko143
    Cytotoxicity against MDCK2 cells expressing human ABCG2 assessed as reduction in cell viability after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells expressing human ABCG2 assessed as reduction in cell viability after 72 hrs by MTT assay
    		[PMID: 27280693]
    MDCK-II GI50
    11.1 μM
    Compound: Ko143
    Intrinsic cytotoxicity against MDCK2 cells over-expressing human ABCG2 incubated for 72 hrs by MTT assay
    Intrinsic cytotoxicity against MDCK2 cells over-expressing human ABCG2 incubated for 72 hrs by MTT assay
    		[PMID: 27148793]
    MDCK-II GI50
    11.1 μM
    Compound: Ko143
    Cytotoxicity against MDCK2 cells expressing human C-terminal GFP-tagged ABCG2 assessed as reduction in cell viability after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells expressing human C-terminal GFP-tagged ABCG2 assessed as reduction in cell viability after 72 hrs by MTT assay
    		[PMID: 27100033]
    MDCK-II GI50
    12.5 μM
    Compound: Ko143
    Growth inhibition of MDCK2 cells after 72 hrs by MTT assay
    Growth inhibition of MDCK2 cells after 72 hrs by MTT assay
    		[PMID: 30390439]
    MDCK-II GI50
    12.5 μM
    Compound: 59; Ko143
    Intrinsic cytotoxicity in parental MDCK2 cells assessed as inhibition of cell growth incubated for 72 hrs by MTT assay
    Intrinsic cytotoxicity in parental MDCK2 cells assessed as inhibition of cell growth incubated for 72 hrs by MTT assay
    		[PMID: 30075623]
    MDCK-II GI50
    12.5 μM
    Compound: Ko143
    Cytotoxicity against MDCK2 cells assessed as cell growth inhibition after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells assessed as cell growth inhibition after 72 hrs by MTT assay
    		[PMID: 28841513]
    MDCK-II GI50
    12.5 μM
    Compound: 55; Ko143
    Cytotoxicity against MDCK2 cells assessed as cell growth inhibition after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells assessed as cell growth inhibition after 72 hrs by MTT assay
    		[PMID: 28471656]
    MDCK-II GI50
    12.6 μM
    Compound: Ko143
    Growth inhibition of MDCK2 cells harboring GFP-fused human ABCG2 after 72 hrs by MTT assay
    Growth inhibition of MDCK2 cells harboring GFP-fused human ABCG2 after 72 hrs by MTT assay
    		[PMID: 30390439]
    MDCK-II GI50
    12.6 μM
    Compound: 59; Ko143
    Intrinsic cytotoxicity in MDCK2 cells overexpressing BCRP assessed as inhibition of cell growth incubated for 72 hrs by MTT assay
    Intrinsic cytotoxicity in MDCK2 cells overexpressing BCRP assessed as inhibition of cell growth incubated for 72 hrs by MTT assay
    		[PMID: 30075623]
    MDCK-II GI50
    12.6 μM
    Compound: Ko143
    Cytotoxicity against MDCK2 cells harboring human ABCG2 assessed as cell growth inhibition after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells harboring human ABCG2 assessed as cell growth inhibition after 72 hrs by MTT assay
    		[PMID: 28841513]
    MDCK-II GI50
    12.6 μM
    Compound: 55; Ko143
    Cytotoxicity against ABCG2 over-expressing MDCK2 cells assessed as cell growth inhibition after 72 hrs by MTT assay
    Cytotoxicity against ABCG2 over-expressing MDCK2 cells assessed as cell growth inhibition after 72 hrs by MTT assay
    		[PMID: 28471656]
    MDCK-II GI50
    13 μM
    Compound: 56; Ko143
    Cytotoxicity against MDCK2 cells expressing human BCRP assessed as decrease in cell viability after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells expressing human BCRP assessed as decrease in cell viability after 72 hrs by MTT assay
    		[PMID: 29547272]
    MDCK-II GI50
    13 μM
    Compound: 56; Ko143
    Cytotoxicity against MDCK2 cells assessed as decrease in cell viability after 72 hrs by MTT assay
    Cytotoxicity against MDCK2 cells assessed as decrease in cell viability after 72 hrs by MTT assay
    		[PMID: 29547272]
    MDCK-II IC50
    58.26 μM
    Compound: Ko143
    Cytotoxicity against BCRP-overexpressing MDCK-II cells incubated for 48 hrs by MTT assay
    Cytotoxicity against BCRP-overexpressing MDCK-II cells incubated for 48 hrs by MTT assay
    		[PMID: 33938746]
    MDCK-II IC50
    87.19 μM
    Compound: Ko143
    Cytotoxicity against MDCK-II cells incubated for 48 hrs by MTT assay
    Cytotoxicity against MDCK-II cells incubated for 48 hrs by MTT assay
    		[PMID: 33938746]
    NCI-H460 IC50
    0.21 μM
    Compound: Ko143
    Chemo-sensitizing activity against mitoxantrone-selected ABCG2-overexpressing human NCI-H460/MX20 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 4.33 +/-1.18 microM)
    Chemo-sensitizing activity against mitoxantrone-selected ABCG2-overexpressing human NCI-H460/MX20 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 4.33 +/-1.18 microM)
    		[PMID: 34496204]
    NCI-H460 IC50
    102.95 nM
    Compound: Ko143
    Chemo-sensitizing activity against human NCI-H460 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 279.69 +/-31.94 nM)
    Chemo-sensitizing activity against human NCI-H460 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 279.69 +/-31.94 nM)
    		[PMID: 34496204]
    NCI-H460 IC50
    12.27 nM
    Compound: Ko143
    Chemo-sensitizing activity against human NCI-H460 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 20.7 +/-6.32 nM)
    Chemo-sensitizing activity against human NCI-H460 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 20.7 +/-6.32 nM)
    		[PMID: 34496204]
    NCI-H460 IC50
    144.61 nM
    Compound: Ko143
    Chemo-sensitizing activity against mitoxantrone-selected ABCG2-overexpressing human NCI-H460/MX20 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 3262.6 +/-811.81 nM)
    Chemo-sensitizing activity against mitoxantrone-selected ABCG2-overexpressing human NCI-H460/MX20 cells assessed as topotecan IC50 at 1 uM measured after 72 hrs in presence of topotecan by CCK8 assay (Rvb = 3262.6 +/-811.81 nM)
    		[PMID: 34496204]
    NCI-H460 IC50
    42.61 nM
    Compound: Ko143
    Chemo-sensitizing activity against human NCI-H460 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 128.27 +/-22.6 nM)
    Chemo-sensitizing activity against human NCI-H460 cells assessed as SN-38 IC50 at 1 uM measured after 72 hrs in presence of SN-38 by CCK8 assay (Rvb = 128.27 +/-22.6 nM)
    		[PMID: 34496204]
    NCI-H460 IC50
    53.43 nM
    Compound: Ko143
    Chemo-sensitizing activity against mitoxantrone-selected ABCG2-overexpressing human NCI-H460/MX20 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 963.32 +/-120.89 nM)
    Chemo-sensitizing activity against mitoxantrone-selected ABCG2-overexpressing human NCI-H460/MX20 cells assessed as mitoxantrone IC50 at 1 uM measured after 72 hrs in presence of mitoxantrone by CCK8 assay (Rvb = 963.32 +/-120.89 nM)
    		[PMID: 34496204]
    Sf9 IC50
    0.004 μM
    Compound: Ko143
    Inhibition of human ABCG2 expressed in baculovirus infected Sf9 cell membrane assessed as inhibition of vanadate sensitive basal ATPase activity after 20 mins by colorimetric method
    Inhibition of human ABCG2 expressed in baculovirus infected Sf9 cell membrane assessed as inhibition of vanadate sensitive basal ATPase activity after 20 mins by colorimetric method
    		[PMID: 27280693]
    Sf9 IC50
    0.028 μM
    Compound: Ko143
    Inhibition of human ABCG2 expressed in baculovirus infected Sf9 cell membrane assessed as inhibition of vanadate sensitive quercetin-stimulated ATPase activity after 20 mins by colorimetric method
    Inhibition of human ABCG2 expressed in baculovirus infected Sf9 cell membrane assessed as inhibition of vanadate sensitive quercetin-stimulated ATPase activity after 20 mins by colorimetric method
    		[PMID: 27280693]
    Sf9 IC50
    0.17 μM
    Compound: Ko143
    Inhibition of human ABCG2 expressed in Sf9 insect cell membranes assessed as inhibition of quercetin-stimulated ATPase activity after 30 mins by colorimetric analysis in presence of sodium orthovanadate
    Inhibition of human ABCG2 expressed in Sf9 insect cell membranes assessed as inhibition of quercetin-stimulated ATPase activity after 30 mins by colorimetric analysis in presence of sodium orthovanadate
    		[PMID: 24304387]
    體外研究
    (In Vitro)

    Ko143 (10 nM) 顯著降低 (2.5 倍) MTX 對 HEK G2 細(xì)胞和小鼠 G2 細(xì)胞的 IC50。Ko143 (1-100 μM) 代謝物不抑制 ABC 轉(zhuǎn)運蛋白的功能[1]。
    FTC 類似物 Ko143 逆轉(zhuǎn) SKF 104864A 選擇的小鼠 MEF3.8/T6400 細(xì)胞和人 IGROV1/T8 細(xì)胞的耐藥性。Ko143 的應(yīng)用濃度為 EC90 25 nM 的零、一或八倍[2]。
    Ko143 抑制 Madin-Darby 犬腎 (MDCK) 2-BCRP421CC (野生型) 細(xì)胞和 MDCK2-BCRP421AA (突變型) 細(xì)胞中 BCRP 介導(dǎo)的 ZD 4522 轉(zhuǎn)運[3]。

    MCE has not independently confirmed the accuracy of these methods. They are for reference only.
    體內(nèi)研究
    (In Vivo)

    Ko143 (10 mg/kg,口服) 增加小鼠體內(nèi) SKF 104864A 的口服利用度[2]。
    Ko143 顯著影響 ZD 4522 在大鼠體內(nèi)的藥代動力學(xué)[3]。

    MCE has not independently confirmed the accuracy of these methods. They are for reference only.
    分子量

    469.57

    Formula

    C26H35N3O5
    CAS 號
    性狀

    固體

    顏色

    White to off-white

    運輸條件

    Room temperature in continental US; may vary elsewhere.
    儲存方式
    Powder -20°C 3 years
    4°C 2 years
    In solvent -80°C 6 months
    -20°C 1 month
    溶解性數(shù)據(jù)
    細(xì)胞實驗: 

    DMSO 中的溶解度 : 100 mg/mL (212.96 mM; 超聲助溶; 吸濕的 DMSO 對產(chǎn)品的溶解度有顯著影響,請使用新開封的 DMSO)

    配制儲備液
    濃度 溶劑體積 質(zhì)量 1 mg 5 mg 10 mg
    1 mM 2.1296 mL 10.6480 mL 21.2961 mL
    5 mM 0.4259 mL 2.1296 mL 4.2592 mL
    查看完整儲備液配制表

    * 請根據(jù)產(chǎn)品在不同溶劑中的溶解度選擇合適的溶劑配制儲備液;一旦配成溶液,請分裝保存,避免反復(fù)凍融造成的產(chǎn)品失效。
    儲備液的保存方式和期限:-80°C, 6 months; -20°C, 1 month。-80°C儲存時,請在6個月內(nèi)使用,-20°C儲存時,請在1個月內(nèi)使用。

    • 摩爾計算器

    • 稀釋計算器

    Mass (g) = Concentration (mol/L) × Volume (L) × Molecular Weight (g/mol)

    質(zhì)量
    =
    濃度
    ×
    體積
    ×
    分子量 *

    Concentration (start) × Volume (start) = Concentration (final) × Volume (final)

    This equation is commonly abbreviated as: C1V1 = C2V2

    濃度 (start)

    C1

    ×
    體積 (start)

    V1

    =
    濃度 (final)

    C2

    ×
    體積 (final)

    V2

    動物實驗:

    請根據(jù)您的 實驗動物和給藥方式 選擇適當(dāng)?shù)娜芙夥桨浮?

    以下溶解方案都請先按照 In Vitro 方式配制澄清的儲備液,再依次添加助溶劑:
    ——為保證實驗結(jié)果的可靠性,澄清的儲備液可以根據(jù)儲存條件,適當(dāng)保存;體內(nèi)實驗的工作液,建議您現(xiàn)用現(xiàn)配,當(dāng)天使用
    以下溶劑前顯示的百分比是指該溶劑在您配制終溶液中的體積占比;如在配制過程中出現(xiàn)沉淀、析出現(xiàn)象,可以通過加熱和/或超聲的方式助溶

    • 方案 一

      請依序添加每種溶劑: 10% DMSO    40% PEG300    5% Tween-80    45% Saline

      Solubility: ≥ 2.5 mg/mL (5.32 mM); 澄清溶液

      此方案可獲得 ≥ 2.5 mg/mL(飽和度未知)的澄清溶液。

      1 mL 工作液為例,取 100 μL 25.0 mg/mL 的澄清 DMSO 儲備液加到 400 μL PEG300 中,混合均勻;再向上述體系中加入 50 μL Tween-80,混合均勻;然后再繼續(xù)加入 450 μL 生理鹽水 定容至 1 mL。

      生理鹽水的配制:將 0.9 g 氯化鈉,溶解于 ddH?O 并定容至 100 mL,可以得到澄清透明的生理鹽水溶液。
    • 方案 二

      請依序添加每種溶劑: 10% DMSO    90% (20% SBE-β-CD in Saline)

      Solubility: 2.5 mg/mL (5.32 mM); 懸濁液; 超聲助溶 (<50°C)

      此方案可獲得 2.5 mg/mL的均勻懸濁液,懸濁液可用于口服和腹腔注射。

      1 mL 工作液為例,取 100 μL 25.0 mg/mL 的澄清 DMSO 儲備液加到 900 μL 20% 的 SBE-β-CD 生理鹽水水溶液 中,混合均勻。

      2 g SBE-β-CD(磺丁基醚 β-環(huán)糊精)粉末定容于 10 mL 的生理鹽水中,完全溶解至澄清透明。
    動物溶解方案計算器
    請輸入動物實驗的基本信息:

    給藥劑量

    mg/kg

    動物的平均體重

    g

    每只動物的給藥體積

    μL

    動物數(shù)量

    由于實驗過程有損耗,建議您多配一只動物的量
    請輸入您的動物體內(nèi)配方組成:
    %
    DMSO +
    +
    %
    Tween-80 +
    %
    Saline
    如果您的動物是免疫缺陷鼠或者體弱鼠,建議 DMSO 中的在最后工作液體系中的占比盡量不超過 2%。
    方案所需 助溶劑 包括:DMSO, ,均可在 MCE 網(wǎng)站選購。 ,Tween 80,均可在 MCE 網(wǎng)站選購。
    計算結(jié)果
    工作液所需濃度 : mg/mL
    儲備液配制方法 : mg 藥物溶于 μL  DMSO(母液濃度為 mg/mL)。
    您所需的儲備液濃度超過該產(chǎn)品的實測溶解度,以下方案僅供參考,如有需要,請與 MCE 中國技術(shù)支持聯(lián)系。
    動物實驗體內(nèi)工作液的配制方法 : 取 μL DMSO 儲備液,加入 μL 。 μL ,混合均勻至澄清,再加 μL Tween 80,混合均勻至澄清,再加 μL 生理鹽水。
    連續(xù)給藥周期超過半月以上,請謹(jǐn)慎選擇該方案。
    請確保第一步儲備液溶解至澄清狀態(tài),從左到右依次添加助溶劑。您可采用超聲加熱 (超聲清洗儀,建議頻次 20-40 kHz),渦旋吹打等方式輔助溶解。
    純度 & 產(chǎn)品資料

    純度: 99.97%

    參考文獻(xiàn)
    Cell Assay
    [2]

    cells are plated at 400 or 1000/well in 96-well plates the night before addition of drugs. A concentration series of drug is applied along one plate axis and left for the duration of the assay. Plates are harvested after 4-5 days while untreated wells are still subconfluent. Relative cell proliferation is quantified with CyQuant or Sybr Green I fluorescent nucleic acid stains. Assays with human cell lines are performed in the presence of 0.1 μm?PSC833 to inhibit confounding P-gp activity.

    MCE has not independently confirmed the accuracy of these methods. They are for reference only.
    Animal Administration
    [2]

    Oral toxicity of FTC analogues in mice is tested by mixing 50 mg/mL stocks in DMSO 1:1 with Tween 80 (polyoxyethylene sorbitan mono-oleate) and diluting with 5% w/v glucose such that the final volume administered by oral gavage is 10 μL/g of body weight. Pairs of mice are administered oral doses of 50 mg/kg Ko132, Ko134, Ko143, or vehicle under light methoxyflurane anesthesia. Final tests of 50 mg/kg Ko134 or Ko143 are performed on additional pairs of unanesthetized animals to observe any behavioral effects. Further, another pair of mice receive the higher dose of 100 mg/kg Ko134. For i.p. toxicity tests, the FTC analogue stocks in DMSO are dispersed in at least 10 volumes of sterile corn oil such that the injected volume is 5 μL/g of body weight. After pilot tests at lower doses show no adverse effects, mice (4 per group) are administered vehicle or 10 mg/kg i.p. of Ko132, Ko134, or Ko143. The mice are observed continuously during the first hour after administration and then at increasing intervals for 2 weeks, after which they are sacrificed for histological examination of major organs and structures including brain, salivary glands, heart, lungs, liver, adrenal glands, kidneys, urinary tract, spleen, thymus, bone marrow, pancreas, stomach, intestines, cecum, colon, testes, epididymus, skin, head, trunk, and limbs.

    MCE has not independently confirmed the accuracy of these methods. They are for reference only.
    參考文獻(xiàn)

    完整儲備液配制表

    * 請根據(jù)產(chǎn)品在不同溶劑中的溶解度選擇合適的溶劑配制儲備液;一旦配成溶液,請分裝保存,避免反復(fù)凍融造成的產(chǎn)品失效
    儲備液的保存方式和期限:-80°C, 6 months; -20°C, 1 month。-80°C儲存時,請在6個月內(nèi)使用,-20°C儲存時,請在1個月內(nèi)使用。

    可選溶劑 濃度 溶劑體積 質(zhì)量 1 mg 5 mg 10 mg 25 mg
    DMSO 1 mM 2.1296 mL 10.6480 mL 21.2961 mL 53.2402 mL
    5 mM 0.4259 mL 2.1296 mL 4.2592 mL 10.6480 mL
    10 mM 0.2130 mL 1.0648 mL 2.1296 mL 5.3240 mL
    15 mM 0.1420 mL 0.7099 mL 1.4197 mL 3.5493 mL
    20 mM 0.1065 mL 0.5324 mL 1.0648 mL 2.6620 mL
    25 mM 0.0852 mL 0.4259 mL 0.8518 mL 2.1296 mL
    30 mM 0.0710 mL 0.3549 mL 0.7099 mL 1.7747 mL
    40 mM 0.0532 mL 0.2662 mL 0.5324 mL 1.3310 mL
    50 mM 0.0426 mL 0.2130 mL 0.4259 mL 1.0648 mL
    60 mM 0.0355 mL 0.1775 mL 0.3549 mL 0.8873 mL
    80 mM 0.0266 mL 0.1331 mL 0.2662 mL 0.6655 mL
    100 mM 0.0213 mL 0.1065 mL 0.2130 mL 0.5324 mL
    Help & FAQs
    • Do most proteins show cross-species activity?

      Species cross-reactivity must be investigated individually for each product. Many human cytokines will produce a nice response in mouse cell lines, and many mouse proteins will show activity on human cells. Other proteins may have a lower specific activity when used in the opposite species.

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    Inquiry Information

    產(chǎn)品名稱:
    Ko 143
    目錄號:
    HY-10010
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