NSC228155 can enhance the tyrosine phosphorylation of EGFR via binding to the dimerization domain II. It blocks KIX-KID interaction as well (IC50 = 0.36 μM).
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产品名称 | EGFR/ErbB1 ↓ ↑ | ErbB3 ↓ ↑ | ErbB4 ↓ ↑ | HER2/ErbB2 ↓ ↑ | mutant EGFR ↓ ↑ | 其他靶点 | 纯度 | ||||||||||||
---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
WZ-3146 |
++++
EGFR (E746_A750/T790M), IC50: 14 nM EGFR (E746_A750), IC50: 2 nM |
99%+ | |||||||||||||||||
Daphnetin |
+
EGFR, IC50: 7.67 μM |
PKA,PKC | 95% | ||||||||||||||||
Lifirafenib |
++
EGFR, IC50: 29 nM |
+
EGFR(T790M/L858R), IC50: 495 nM |
98% | ||||||||||||||||
PD168393 |
++++
EGFR, IC50: 0.70 nM |
99%+ | |||||||||||||||||
Nazartinib |
++
mutant EGFR, Ki: 0.031 μM |
++
mutant EGFR, Ki: 0.031 μM |
98% | ||||||||||||||||
Norcantharidin | ✔ | 98% | |||||||||||||||||
CL-387785 |
++++
EGFR, IC50: 370 pM |
98% | |||||||||||||||||
WHI-P154 |
+++
EGFR, IC50: 4 nM |
Src,VEGFR | 98% | ||||||||||||||||
Tyrphostin A9 |
+
EGFR, IC50: 460 μM |
PDGFR | 98% | ||||||||||||||||
AG 555 |
+
EGFR, IC50: 0.7 μM |
98% | |||||||||||||||||
AG 494 |
+
EGFR, IC50: 1.2 μM |
99%+ | |||||||||||||||||
AG-556 |
+
EGFR, IC50: 5 μM |
98% | |||||||||||||||||
RG13022 |
+
EGFR, IC50: 4 μM |
99%+ | |||||||||||||||||
Tyrphostin RG 14620 | ✔ | 99%+ | |||||||||||||||||
Vandetanib |
+
EGFR, IC50: 500 nM |
98% | |||||||||||||||||
CNX-2006 |
++
mutant EGFR, IC50: <20 nM |
++
mutant EGFR, IC50: <20 nM |
98% | ||||||||||||||||
AZD3759 |
++++
EGFR (WT), IC50: 0.3 nM EGFR (L858R), IC50: 0.2 nM |
98% | |||||||||||||||||
Erlotinib |
++++
EGFR, IC50: 2 nM |
95% | |||||||||||||||||
Saracatinib |
+++
EGFR, IC50: 5 nM EGFR (L861Q), IC50: 4 nM |
99%+ | |||||||||||||||||
AG1557 | ✔ | 98% | |||||||||||||||||
Rociletinib |
++
EGFR (wt), Ki: 303.3 nM EGFR (L858R/T790M), Ki: 21.5 nM |
98% | |||||||||||||||||
AG490 |
+
EGFR, IC50: 0.1 μM |
98% | |||||||||||||||||
Cetuximab |
++++
EGFR, Kd: 0.39 nM |
98% | |||||||||||||||||
Osimertinib |
++
L858R/T790M EGFR, IC50: 11.44 nM WT EGFR, IC50: 12.92 nM |
99% | |||||||||||||||||
Osimertinib mesylate | ✔ | 98% (Content MsOH 15.2-18.2%) | |||||||||||||||||
Chrysophanol | ✔ | mTOR | 98% | ||||||||||||||||
PD153035 |
++++
EGFR, Ki: 5.2 pM |
99%+ | |||||||||||||||||
Olmutinib | ✔ | BTK | 99%+ | ||||||||||||||||
WZ4002 |
++++
EGFR (L858R/T790M), IC50: 8 nM EGFR (L858R), IC50: 2 nM |
99%+ | |||||||||||||||||
Icotinib |
+++
EGFR, IC50: 5 nM |
98+% | |||||||||||||||||
Desmethyl Erlotinib HCl |
++++
EGFR, IC50: 2 nM |
98% | |||||||||||||||||
Cyasterone | ✔ | 99%+ | |||||||||||||||||
PP 3 |
+
EGFR tyrosine kinase, IC50: 2.7 μM |
98% | |||||||||||||||||
WZ8040 | ✔ | 99%+ | |||||||||||||||||
(-)-Epigallocatechin Gallate | ✔ | 99% | |||||||||||||||||
AG 18 |
+
EGFR, IC50: 35 μM |
99%+ | |||||||||||||||||
O-Desmethyl gefitinib |
++
EGFR, IC50: 36 nM |
98% | |||||||||||||||||
Falnidamol | ✔ | 99%+ | |||||||||||||||||
AZ-5104 |
++++
EGFR (L861Q) , IC50: <1 nM EGFR (L858R), IC50: 6 nM |
+++
ErbB4, IC50: 7 nM |
BRK | 99%+ | |||||||||||||||
Butein | ✔ | 95% | |||||||||||||||||
Genistein | ✔ | 98% | |||||||||||||||||
SU5214 |
+
EGFR, IC50: 36.7 μM |
99%+ | |||||||||||||||||
Naquotinib | ✔ | 99%+ | |||||||||||||||||
Gefitinib |
++
EGFR, IC50: 15.5 nM |
+
EGFR (858R/T790M), IC50: 823.3 nM |
98% | ||||||||||||||||
Theliatinib |
+++
WT EGFR, IC50: 3 nM |
++
EGFR T790M/L858R, IC50: 22 nM |
98+% | ||||||||||||||||
Lazertinib |
++++
L858R/T790M EGFR, IC50: 2 nM WT EGFR, IC50: 76 nM |
++++
Del19/T790M, IC50: 1.7 nM |
99%+ | ||||||||||||||||
Gefitinib-based PROTAC 3 |
++
EGFR, DC50: 22.3 nM |
99%+ | |||||||||||||||||
MTX-211 | ✔ | PI3K | 98% | ||||||||||||||||
(E)-AG 99 | ✔ | 99%+ | |||||||||||||||||
Licochalcone D | ✔ | Caspase,PARP | 97% | ||||||||||||||||
Zipalertinib |
+++
EGFR WT, IC50: 8 nM EGFR (L861Q), IC50: 4.1 nM |
+++
HER4, IC50: 4 nM |
++++
EGFR(d746-750), IC50: 1.4 nM EGFR L858R, IC50: 2 nM |
97% | |||||||||||||||
JND3229 |
+++
EGFR WT, IC50: 6.8 nM |
++
EGFR L858R/T790M, IC50: 30.5 nM |
99%+ | ||||||||||||||||
Firmonertinib mesylate | ✔ | 99%+ | |||||||||||||||||
Tyrphostin AG30 | ✔ | 99%+ | |||||||||||||||||
EGFR-IN-12 |
++
EGFR, IC50: 21 nM |
99%+ | |||||||||||||||||
Mobocertinib | ✔ | 98% | |||||||||||||||||
(Rac)-JBJ-04-125-02 | ✔ | 99% | |||||||||||||||||
(S)-Sunvozertinib | ✔ | 98% | |||||||||||||||||
BLU-945 | ✔ | 95% | |||||||||||||||||
Poziotinib |
+++
HER1, IC50: 3.2 nM |
++
HER4, IC50: 23.5 nM |
+++
HER2, IC50: 5.3 nM |
98% | |||||||||||||||
TAK-285 |
++
EGFR/HER1, IC50: 23 nM |
+
HER4, IC50: 260 nM |
++
HER2, IC50: 17 nM |
99%+ | |||||||||||||||
ARRY-380 analog | ✔ | 98% | |||||||||||||||||
Canertinib |
++++
EGFR, IC50: 1.5 nM |
+++
ErbB2, IC50: 9.0 nM |
99%+ | ||||||||||||||||
Dacomitinib |
+++
EGFR, IC50: 6.0 nM |
+
ErbB4, IC50: 73.7 nM |
+
ErbB2, IC50: 45.7 nM |
98% | |||||||||||||||
EGFR/ErbB-2/ErbB-4 inhibitor-2 |
+
ErbB4, IC50: 1.91 μM |
+
ErbB2, IC50: 0.08 μM |
99%+ | ||||||||||||||||
(E/Z)-CP-724714 |
++
HER2/ErbB2, IC50: 10 nM |
98+% | |||||||||||||||||
Lapatinib |
++
EGFR, IC50: 10.8 nM |
+
ErbB4, IC50: 367 nM |
+++
ErbB2, IC50: 9.2 nM |
98% | |||||||||||||||
AEE788 |
++++
EGFR, IC50: 2 nM |
+
HER4/ErbB4, IC50: 160 nM |
+++
HER2/ErbB2, IC50: 6 nM |
c-Fms | 98+% | ||||||||||||||
AV-412 free base |
++++
EGFR, IC50: 0.75 nM |
++
ErbB2, IC50: 19 nM |
++++
EGFRT790M, IC50: 0.79 nM EGFRL858R/T790M, IC50: 0.51 nM |
98+% | |||||||||||||||
Neratinib |
+
EGFR, IC50: 92 nM |
+
HER2, IC50: 59 nM |
Src | 98% | |||||||||||||||
BMS-599626 |
++
HER1, IC50: 20 nM |
+
HER4, IC50: 190 nM |
++
HER2, IC50: 30 nM |
99+% | |||||||||||||||
Tucatinib |
+++
ErbB2, IC50: 8 nM |
98% | |||||||||||||||||
Allitinib |
++++
EGFR, IC50: 0.5 nM |
++++
ErbB4, IC50: 0.8 nM |
+++
ErbB2, IC50: 3.0 nM |
99% | |||||||||||||||
Pelitinib |
+
EGFR, IC50: 38.5 nM |
+
ErbB2, IC50: 1.255 μM |
Src,Raf | 99%+ | |||||||||||||||
Sapitinib |
+++
EGFR, IC50: 4 nM |
+++
ErbB3, IC50: 4 nM |
+++
ErbB2, IC50: 3 nM |
99%+ | |||||||||||||||
CUDC-101 |
+++
EGFR, IC50: 2.4 nM |
++
HER2, IC50: 15.7 nM |
HDAC | 99%+ | |||||||||||||||
Varlitinib |
+++
ErbB1, IC50: 7 nM |
++++
ErbB2, IC50: 2 nM |
99%+ | ||||||||||||||||
Afatinib dimaleate |
++++
EGFR (L858R/T790M), IC50: 0.4 nM EGFR (wt), IC50: 0.5 nM |
++
HER2, IC50: 14 nM |
98% | ||||||||||||||||
Canertinib dihydrochloride |
+++
EGFR, IC50: 7.4 nM |
+++
ErbB2, IC50: 9 nM |
98% | ||||||||||||||||
Allitinib tosylate |
++++
EGFR, IC50: 0.5 nM EGFR (T790M/L858R), IC50: 12 nM |
++++
ErbB4, IC50: 0.8 nM |
+++
ErbB2, IC50: 3.0 nM |
99% | |||||||||||||||
Tyrphostin AG 528 |
+
EGFR, IC50: 4.9 μM |
+
HER2, IC50: 2.1 μM |
98% | ||||||||||||||||
Afatinib |
++++
EGFR (wt), IC50: 0.5 nM EGFR (L858R), IC50: 10 nM |
++++
ErbB4, IC50: 1 nM |
++
HER2, IC50: 14 nM |
99% | |||||||||||||||
Pyrotinib dimaleate |
++
EGFR, IC50: 0.013 μM |
++
HER2, IC50: 0.038 μM |
98% | ||||||||||||||||
Epertinib HCl |
++++
EGFR, IC50: 1.48 nM |
+++
HER4, IC50: 2.49 nM |
+++
HER2, IC50: 7.15 nM |
98% | |||||||||||||||
Tuxobertinib |
++++
EGFR, Kd: 0.2 nM |
++++
HER2, Kd: 0.76 nM |
98% | ||||||||||||||||
ALK-IN-1 |
++
EGFR(del19), IC50: 36.8 nM EGFR(C797S/del19), IC50: 138.6 nM |
ALK | 98+% | ||||||||||||||||
Brigatinib |
+
EGFR(C797S/T790M/del19), IC50: 67.2 nM EGFR(del19), IC50: 39.9 nM |
FLT3,ALK | 98% | ||||||||||||||||
Avitinib |
++++
EGFR L858R/T790M, IC50: 0.18 nM |
BTK | 99%+ | ||||||||||||||||
EAI045 | ✔ | 97% | |||||||||||||||||
Almonertinib | ✔ | 98% | |||||||||||||||||
BI-4020 |
++++
EGFRdel19 T790M C797S, IC50: 0.2 nM |
99%+ | |||||||||||||||||
EGFR-IN-7 |
++++
EGFRd746-750/T790M/C797S, IC50: 0.26 nM EGFRL858R/T790M, IC50: 0.19 nM |
98% | |||||||||||||||||
1. 鼠标悬停在“+”上可以显示相关IC50的具体数值。"+"越多,抑制作用越强。2. "✔"表示该化合物对相应的亚型有抑制作用,但抑制强度暂时没有相关数据。 |
描述 | Ligand-dependent activation of epidermal growth factor receptor (EGFR) is an essential process governing signal transduction during cell growth, differentiation, survival, and proliferation in physiological conditions. Mutations resulting in overexpression or deregulation of the receptor impair signal transduction, leading to tumor growth. NSC-228155 is an activator of EGFR, which has a positive log P and could enter cells and enhance EGFR tyrosine phosphorylation [1]. It also dose-dependently inhibits KIX-KID interaction with an IC50 of 0.36 μM [2]. The increase in the fluorescence curve at 665 nm was moderately suppressed in the cells exposed to NSC-228155 indicating the generation of H2O2 in redox cycling, which could activate EGFR. NSC-228155 provided high yields of stable SOD1 (superoxide dismutase 1) dimer at concentration of 100 μM for 15 min in MDA MB468 cells, suggesting specific action of NSC-228155 on SOD1. Further studies showed that EGFR tyrosine phosphorylation was enhanced through the action of SOD1 dimer shortly after exposure of cells to 100 μM NSC-228155 for 10 min. Taken together, NSC-228155 primarily induced the formation of a stable SOD1 dimer that was functionally active and led to the accumulation of intracellular H2O2, which in turn activates EGFR [1]. |
计算器 | ||||
存储液制备 | 1mg | 5mg | 10mg | |
1 mM 5 mM 10 mM |
3.45mL 0.69mL 0.34mL |
17.23mL 3.45mL 1.72mL |
34.45mL 6.89mL 3.45mL |
CAS号 | 113104-25-9 |
分子式 | C11H6N4O4S |
分子量 | 290.255 |
别名 | |
运输 | 蓝冰 |
存储条件 |
液体 -20°C:3-6个月-80°C:12个月 粉末 Keep in dark place,Sealed in dry,2-8°C |
溶解度 |
DMSO: 15 mg/mL(51.68 mM),配合低频超声助溶,注意:DMSO长时间开封后,会吸水并导致溶解能力下降,请避免使用长期开封的DMSO |
动物实验配方 |