CCT-251236
CAS No. 1693731-40-6
CCT-251236( CCT251236 )
Catalog No. M12581 CAS No. 1693731-40-6
A potent, orally available Pirin ligand (Ki=28 nM), blocks the HSF1-mediated induction of both HSP72 and HSP27.
Purity : >98% (HPLC)
COA
Datasheet
HNMR
HPLC
MSDS
Handing Instructions
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| 100MG | 1053 | Get Quote |
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Biological Information
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Product NameCCT-251236
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NoteResearch use only, not for human use.
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Brief DescriptionA potent, orally available Pirin ligand (Ki=28 nM), blocks the HSF1-mediated induction of both HSP72 and HSP27.
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DescriptionA potent, orally available Pirin ligand (Ki=28 nM), blocks the HSF1-mediated induction of both HSP72 and HSP27; inhibits the induction of HSP72 at the mRNA level, blocks the induction of HSPA1A gene expression with IC50 of 40 nM, inhibits SK-OV-3 cells proliferation with GI50 of 1.1 nM; displays efficacy in a human ovarian carcinoma xenograft model.
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In VitroCCT251236 (0-100 nM; 24hours) displays a desired balance of in vitro properties, while maintaining excellent cellular activity with a pIC50=7.73 ± 0.07 (IC50=19 nM) for inhibition of HSF1-mediated HSP72 induction. The free GI50?is 1.1 nM in SK-OV-3 cells that calculated from the free fraction in the cell assay.CCT251236 (0-100 nM; 24 hours) blocks 17-AAG induced he HSF1-mediated heat-shock proteins, HSP72 and HSP27 expression as a concentration manner in SK-OV-3 cells.CCT251236 (0-100 nM; 24 hours), pre-treated with250 nM 17-AAG for 6h, blocks the induction of HSPA1A mRNA by 17-AAG in a dosedependent manner. Western Blot Analysis Cell Line:SK-OV-3 cells Concentration:0 nM; 10 nM; 100 nM Incubation Time:24 hours Result:Inhibited HSP72 and HSP27 expression at the dose of 10 nM.RT-PCRCell Line:SK-OV-3 cells Concentration:0 nM; 10 nM; 100 nM and 1000 nM Incubation Time:24 hours Result:Decreased HSPA1A mRNA level.
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In VivoCCT251236 (oral adminstation; 5 or 20 mg/kg) in nontumor bearing immunocompetent BALB/c mice exhibits free?Cav0-24h?value of 2.0 nM and 1.2 nM, respectively.CCT251236 (oral adminstation; 20 mg/kg; 33 days)has aclear therapeutic efficacy in mice with a tumor growth inhibition (%TGI) of 70% based on final tumor volumes. After 33 days, the mean tumor weights decreases 64% when compares to control group. In addition, the compound’s basicity and high volume of distribution shows in tumor withtumor concentrations of?CCT251236?as high as 940 nM. Animal Model:Athymic mice with SK-OV-3 cells Dosage:20 mg/kg; 33 days Administration:Oral adminstation Result:Was efficacious in SK-OV-3 cell induced-tumor mice model.
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SynonymsCCT251236
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PathwayCytoskeleton/Cell Adhesion Molecules
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TargetHSP
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RecptorHSP
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Research Area——
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Indication——
Chemical Information
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CAS Number1693731-40-6
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Formula Weight552.631
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Molecular FormulaC32H32N4O5
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Purity>98% (HPLC)
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SolubilityDMSO : ≥ 150 mg/mL 271.43 mM
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SMILESO=C(C1=CC(C=CC(OCCN2CCCC2)=N3)=C3C=C1)NC4=CC(NC(C5=CC(OCCO6)=C6C=C5)=O)=CC=C4C
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Chemical NameN-(5-(2,3-dihydrobenzo[b][1,4]dioxine-6-carboxamido)-2-methylphenyl)-2-(2-(pyrrolidin-1-yl)ethoxy)quinoline-6-carboxamide
Shipping & Storage Information
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Storage(-20℃)
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ShippingWith Ice Pack
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Stability≥ 2 years
Reference
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Hsp70-derived octape...
A group of tetratricopeptide repeat (TPR)-containing proteins has been shown to interact with the C-terminal domain of the 70 kDa heat-shock cognate protein (hsc70). In the present study, the effect of the TPR-containing proteins, including the C-terminus of hsc70-interacting protein (CHIP), TPR1 and human glutamine-rich TPR-containing protein (hSGT), on refolding of luciferase by DnaJ and hsc70 was investigated.
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AT13387
AT13387 is a selective potent Hsp90 inhibitor with IC50 of 18 nM in A375 cells, displays a long duration of anti-tumor activity.
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p5 Ligand for Dnak a...
p5 Ligand for Dnak and DnaJ is a non-apeptide and correspond to the main binding sites of the 23 residues of the mitochondrial aspartate aminotransferase presequence.P5 ligand is a high affinity ligand for Dnak and DnaJ.
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