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SP600125

別名: Nsc75890

SP600125 (Nsc75890)是一種廣譜JNK抑制劑,作用于JNK1、JNK2和JNK3,無細胞試驗中IC50分別為40 nM、40 nM和90 nM,比作用于MKK4選擇性高10倍,比作用于MKK3、MKK6、PKB和PKCα選擇性高25倍,比作用于ERK2、p38、Chk1、EGFR等選擇性高100倍。SP600125也是一種廣譜的serine/threonine kinases抑制劑,包括Aurora kinase AFLT3TRKA,對應的IC50值為60?nM、90?nM和70?nM。SP600125可抑制自噬而激活細胞凋亡。

SP600125 Chemical Structure

SP600125 Chemical Structure

CAS: 129-56-6

規(guī)格 價格 庫存 購買數(shù)量
10mM (1mL in DMSO) 647.05 現(xiàn)貨
10mg 573.66 現(xiàn)貨
50mg 1204.13 現(xiàn)貨
100mg 1613.43 現(xiàn)貨
1g 7944.3 現(xiàn)貨
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常與SP600125一起在實驗中被使用的化合物

Adezmapimod (SB203580)

SP600125抑制自噬并激活細胞凋亡,而Adezmapimod則誘導線粒體自噬和自噬。

PD98059

SP600125和PD98059是兩種在TQ誘導的細胞死亡中具有促生存活性的激酶。

El-Najjar N, et al. Apoptosis. 2010 Feb;15(2):183-95.

SCH772984

SP600125和SCH772984在體外顯著增加PMN-MDSC和M-MDSC的凋亡。

Yu J, et al. Front Oncol. 2021 Mar 18;11:647312.

LY294002

SP600125和LY294002抑制SNU-216和NCI-N87細胞的生長。

Choi Y, et al. World J Gastroenterol. 2016 Nov 7; 22(41): 9141–9153.

Bentamapimod (AS602801)

SP600125和Bentamapimod是泛JNK抑制劑,可導致GBM干細胞(GSC)培養(yǎng)物中的細胞活力大幅降低。

MacLeod G, et al. Cell Rep. 2019 Apr 16;27(3):971-986.e9.

SP600125相關產(chǎn)品

相關信號通路圖

JNK Signaling Pathways

JNK信號通路圖

細胞實驗數(shù)據(jù)示例

細胞系 實驗類型 給藥濃度 孵育時間 活性描述 文獻信息
PC12 Function Assay 10 μM 5 h Activation of Nrf2/ARE assessed as HO-1 protein induction pretreated with SB203580 21345685
PC12 Function Assay 10 μM 5 h Activation of Nrf2/ARE assessed as HO-1 protein induction pretreated with SP600125 21345685
PC12 Function Assay 10 μM 5 h Activation of Nrf2/ARE assessed as HO-1 protein induction pretreated with U0126 21345685
PC12 Function Assay 10 μM 5 h Activation of Nrf2/ARE assessed as HO-1 protein induction pretreated with PD98059 21345685
A549 Function Assay 20 μM 1 h Inhibition of TPA-induced MMP-2 and u-PA expression 20492175
HaCaT Function Assay 20 μM 24 h Blocks the phosphorylation of c-Jun protein 19812349
HaCaT Function Assay 20 μM 4 h Blocks the TNF-α-induced?CYP4F11?transcription 19812349
PC3 Function Assay 20 μM 1 h Decreases the MMP2 and MMP9 expression 19633975
RAW264.7 Function Assay 10 μM 12 h Antiinflammatory activity assessed as inhibition of LPS-induced NO production with IC50 of 17μM 19497418
BV-2 Function Assay 2 μM 1 h Inhibits the increase of sBAFF release in Gmix-treated BV-2 cells 19406831
Hep3B Function Assay 10 μM 1 h Blocks autophagy and upregulation of Beclin 1 expression induced by ceramide 19060920
LoVo Function Assay 1 μM 1 h Inhibition of PGE2-induced expression of uPA and MMP-9 significantly 21859479
LoVo Function Assay 1 μM 1 h BlocksPGE2-induced cell migration significantly 21859479
THP-1 Function Assay 90 nM 30 min Inhibition of tissue factor expression 22940059
PC3 Function Assay 25 μM 24 h Inhibition of AP-1 and p21 luciferase activity induced by S179D PRL 23162652
SH-SY5Y Function Assay 10 μM 1 h Neuroprotective activity assessed as reduction of anisomycin-induced cell death 23498914
SH-SY5Y Kinase Assay 10 μM 1 h Inhibition of JNK3 assessed as blockade of anisomycin-induced c-jun phosphorylation at ser73 23498914
RAW264.7 Function Assay 10 μM 24 h Antiinflammatory activity assessed as inhibition of IL-1beta release 23791078
RAW264.7 Function Assay 10 μM 24 h Antiinflammatory activity assessed as inhibition of LPS-induced iNOS expression 23791078
RAW264.7 Function Assay 10 μM 2 h Antiinflammatory activity assessed as inhibition of LPS-induced NO production 23791078
A549 Growth Inhibition Assay 20 μM 72 h Rapid and potent inhibition of cell proliferation 23912840
BMMC Function assay 1 to 20 uM 7 days Inhibition of RANKL/M-CSF-stimulated osteoclastogenesis in ICR mouse BMMC assessed as reduction in TRAP positive multinucleated cells at 1 to 20 uM incubated for 7 days by light microscopy 25397676
Plasmodium falciparum GB4 Antibacterial Assay 72 h Antiplasmodial activity with IC50 of 12.5893μM 19734910
Plasmodium falciparum 3D7 Antibacterial Assay 72 h Antiplasmodial activity with IC50 of 12.5893 μM 19734910
Plasmodium falciparum 7G8 Antibacterial Assay 72 h Antiplasmodial activity with IC50 of 10 μM 19734910
Plasmodium falciparum W2 Antibacterial Assay 72 h Antiplasmodial activity with IC50 of 7.94328 μM 19734910
Plasmodium falciparum HB3 Antibacterial Assay 72 h Antiplasmodial activity with IC50 of 7.94328 μM 19734910
B16-F10 Function Assay 1 h Inhibition of TNF-alpha-induced c-JUN phosphorylation 21815634
RAW264.7 Antiinflammatory assay Antiinflammatory activity in mouse RAW264.7 cells assessed as inhibition of LPS-induced NO production relative to control, IC50 = 17 μM. 22831798
A673 qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for A673 cells 29435139
BT-37 qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for BT-37 cells 29435139
SK-N-SH qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for SK-N-SH cells 29435139
NB1643 qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for NB1643 cells 29435139
OHS-50 qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for OHS-50 cells 29435139
SK-N-MC qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for SK-N-MC cells 29435139
NB-EBc1 qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for NB-EBc1 cells 29435139
LAN-5 qHTS assay qHTS of pediatric cancer cell lines to identify multiple opportunities for drug repurposing: Primary screen for LAN-5 cells 29435139
點擊查看更多細胞系數(shù)據(jù)

生物活性

產(chǎn)品描述 SP600125 (Nsc75890)是一種廣譜JNK抑制劑,作用于JNK1、JNK2和JNK3,無細胞試驗中IC50分別為40 nM、40 nM和90 nM,比作用于MKK4選擇性高10倍,比作用于MKK3、MKK6、PKB和PKCα選擇性高25倍,比作用于ERK2、p38、Chk1、EGFR等選擇性高100倍。SP600125也是一種廣譜的serine/threonine kinases抑制劑,包括Aurora kinase AFLT3TRKA,對應的IC50值為60?nM、90?nM和70?nM。SP600125可抑制自噬而激活細胞凋亡。
特性 SP600125是絲/蘇氨酸激酶廣譜抑制劑,有效抑制c-Jun 氨基末端激酶(JNK)。
靶點
serine/threonine kinase [1] JNK1 [1]
(Cell-free assay)		 JNK2 [1]
(Cell-free assay)		 Aurora A [4]
(Cell-free assay)		 TrkA [4]
(Cell-free assay)		 點擊更多
40 nM 40 nM 60 nM 70 nM
體外研究(In Vitro)
體外研究活性

SP600125是ATP競爭性的c-Jun氨基末端激酶(JNK)選擇性抑制劑,IC50為40 nM 到90 nM。SP600125作用于Jurkat T細胞,抑制c-Jun磷酸化,IC50為5 μM 到10 μM。SP600125作用于CD4+細胞, 如從人臍血或外周血分離的Th0細胞,抑制細胞活化和分化,且抑制炎癥基因 COX-2, IL-2, IL-10, IFN-γ,和TNF-α的表達, IC50為5 μM 到 12 μM。[1]然而,后期研究顯示 SP600125 也抑制香烴受體(AhR)[2] Mps1,[3] 和一系列其他絲/蘇氨酸激酶, 包括Aurora 激酶 A, FLT3, MELK,和 TRKA。[4] 20 μM SP600125作用于小鼠beta 細胞 MIN6, 誘導p38 MAPK 磷酸化,和其下游CREB依賴的 啟動子的激活。[5] 20 μM SP600125 作用于HCT116細胞, 使有絲分裂停在G2期,且誘導核內(nèi)復制。[6]
激酶實驗 體外激酶實驗
根據(jù)測量放射性磷酸轉(zhuǎn)移到底物中的量,而測定SP600125作用于激酶的效果,包括MPS1, JNK, 和 Aurora 激酶 A。使用5 nM MPS1 重組蛋白在50 mM HEPES pH 7.5,2.5 mM MgCl2,1 mM MnCl2,1 mM DTT,3 μM NaVO3, 2 mM β-甘油磷酸,0.2 mg/mL BSA, 200 μM P38-βtide 底物-肽(KRQADEEMTGYVATRWYRAE),和含1.5 nM33P-γ-ATP的8 μM ATP中測量MPS1活性。使用1:3 稀釋的(從30 μM 稀釋成 1.5 nM) SP600125進行實驗,然后測定IC50值。
細胞實驗 細胞系 HCT116, A2780, 和U2OS細胞
濃度 0-5 μM
孵育時間 72小時
方法

細胞接種在384孔板上。實驗第一天,用SP600125處理細胞72小時,然后通過 CellTiter-Glo 實驗處理實驗板。測定與對照組相比,實驗組的抑制活性,計算抑制增殖的IC50值。
實驗圖片 檢測方法 檢測指標 實驗圖片 PMID
Western blot p-JNK p-IGF1R / IGF1R / p-Akt / Akt / p-ERK / ERK p-Src / Src p-c-Jun / c-Jun / pJNK / JNK Survivin / Bcl-2 / PARP p-FADD / FADD / p-c-Jun / c-Jun 25226534
Immunofluorescence AIF / Endo G E-cadherin / β-catenin α-catenin / Actin 21738692
Growth inhibition assay Cell viability (U-87 MG) Cell viability (A549) 27176481
體內(nèi)研究(In Vivo)
體內(nèi)研究活性

SP600125按15 mg/kg或30 mg/kg劑量作用于小鼠,顯著抑制脂多糖(LPS)誘導的TNF-α表達和CD3抗體誘導的CD4+ CD8+胸腺細胞凋亡。[1]
動物實驗 Animal Models 雌性 CD-1小鼠LPS/TNF模型
Dosages 15或30 mg/kg
Administration 靜脈注射或口服處理

化學信息&溶解度

分子量 220.23 分子式

C14H8N2O
CAS號 129-56-6 SDF Download SP600125 SDF
Smiles C1=CC=C2C(=C1)C3=NNC4=CC=CC(=C43)C2=O
儲存條件(自收到貨起)

體外溶解度
批次:

DMSO : 60 mg/mL ( (272.44 mM) ;DMSO吸濕會降低化合物溶解度,請使用新開封DMSO)

Water : Insoluble

Ethanol : Insoluble

摩爾濃度計算器

體內(nèi)溶解度
批次:

現(xiàn)配現(xiàn)用,請按從左到右的順序依次添加,澄清后再加入下一溶劑

 動物體內(nèi)配方計算器

實驗計算

摩爾濃度計算器

質(zhì)量 濃度 體積 分子量

動物體內(nèi)配方計算器(澄清溶液)

第一步:請輸入基本實驗信息(考慮到實驗過程中的損耗,建議多配一只動物的藥量)

mg/kg g μL

第二步:請輸入動物體內(nèi)配方組成(配方適用于不溶于水的藥物;不同批次藥物配方比例不同,請聯(lián)系Selleck為您提供正確的澄清溶液配方)

% DMSO % % Tween 80 % ddH2O
%DMSO %

計算結(jié)果:

工作液濃度: mg/ml;

DMSO母液配制方法: mg 藥物溶于μL DMSO溶液(母液濃度mg/mL,:如該濃度超過該批次藥物DMSO溶解度,請先聯(lián)系Selleck);

體內(nèi)配方配制方法:μL DMSO母液,加入μL PEG300,混勻澄清后加入μL Tween 80,混勻澄清后加入μL ddH2O,混勻澄清。

體內(nèi)配方配制方法:μL DMSO母液,加入μL Corn oil,混勻澄清。

注意:1. 首先保證母液是澄清的;
2.一定要按照順序依次將溶劑加入,進行下一步操作之前必須保證上一步操作得到的是澄清的溶液,可采用渦旋、超聲或水浴加熱等物理方法助溶。

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常見問題及建議解決方法

問題 1:
how to reconstitute the inhibitor for in vivo studies?

回答:
S1460 can be dissolved in 5% DMSO/corn oil at 5 mg/ml as a clear solution for injection. The inhibitor dissolved in vehicle 30% PEG400/0.5% Tween80/5%Propylene glycol, at 30mg/ml is a suspension and can be used for oral administration.

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