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NSC228155

Catalog No.GC14103

NSC228155 est un activateur de l'EGFR, se lie à la région extracellulaire de l'EGFR et améliore la phosphorylation de la tyrosine de l'EGFR. NSC228155 est également un puissant inhibiteur de l'interaction KIX-KID, inhibe le domaine inductible par la kinase (KID) de CREB et le domaine interagissant avec le KID (KIX) de CBP, avec une IC50 de 0,36 μM.

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NSC228155 Chemical Structure

Cas No.: 113104-25-9

Taille Prix Stock Qté
10mg
65,00 $US
En stock
50mg
260,00 $US
En stock
100mg
454,00 $US
En stock
500mg
824,00 $US
En stock
1g
1 236,00 $US
En stock

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Sample solution is provided at 25 µL, 10mM.

Description Chemical Properties Product Documents Related Products

IC50: 0.36 μM for KIX-KID interaction

NSC228155 is a potent inhibitor of KIX-KID interaction.

Cyclic-AMP response-element binding protein (CREB) is identified as a stimulus-activated transcription factor. Its transcription activity needs its binding with CREB-binding protein (CBP) after CREB is phosphorylated at Ser133. The domains involved for CREB-CBP interaction are kinase-inducible domain (KID) from CREB and KID-interacting domain (KIX) from CBP.

In vitro: Previous study found that NSC228155 could dose-dependently inhibit KIX–KID interaction as measured by the split RLuc assay. In living HEK 293T cells, NSC228155 could inhibit CREB-mediated gene transcription with an IC50 of 2.09 μM. NSC228155 also inhibited VP16-CREB-mediated gene transcription with an IC50 of 6.14 μM. Though this was around 3-fold higher than the IC50 of CREB-mediated gene transcription, such results indicated that NSC228155 was not particularly selective in inhibiting KIX–KID interaction inside these living cells. Therefore, although NSC228155 was a potent inhibitor of KIX-KID interaction, it was not selective against CREB-mediated gene transcription, and further SAR studies identified a 4-aniline substituted analog displaying a higher selectivity index [1].

In vivo: So far, there is no animal in vivo data reported.

Clinical trial: Up to now, NSC228155 is still in the preclinical development stage.

Reference:
[1] Xie F, Li BX, Broussard C, Xiao X.  Identification, synthesis and evaluation of substituted benzofurazans as inhibitors of CREB-mediated gene transcription. Bioorg Med Chem Lett. 2013 Oct 1;23(19):5371-5.

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