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目錄:MedChemExpress LLC>>信號通路>> (+)-JQ-1 | MedChemExpress

(+)-JQ-1 | MedChemExpress
  • (+)-JQ-1 | MedChemExpress
參考價 935
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參考價 935
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更新時間:2023-09-28 14:49:53瀏覽次數:260評價

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CAS 1268524-70-4 純度 99.90%
分子量 456.99 分子式 C??H??ClN?O?S
供貨周期 現貨 規格 10 mM * 1 mL
貨號 HY-13030 應用領域 醫療衛生,化工,生物產業,制藥/生物制藥
(+)-JQ-1 (JQ1) 是一種有效特異性的可逆 <b>BET bromodomain</b> 抑制劑,抑制 <b>BRD4(1/2)</b> 的 <b>IC<sub>50</sub></b> 分別為 77 nM 和 33 nM。(+)-JQ-1 激活自噬 (<b>autophagy</b>)<sup>[2]</sup>。

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(+)-JQ-1

CAS No. : 1268524-70-4

MCE 國際站:(+)-JQ-1

產品活性:(+)-JQ-1 (JQ1) 是一種有效特異性的可逆 BET bromodomain 抑制劑,抑制 BRD4(1/2)IC50 分別為 77 nM 和 33 nM。(+)-JQ-1 激活自噬 (autophagy)。

研究領域:Epigenetics  |  Autophagy  |  PROTAC

作用靶點:Epigenetic Reader Domain  |  Autophagy  |  Ligands for Target Protein for PROTAC

In Vitro: (+)-JQ-1 represents a potent, highly specific and Kac competitive inhibitor for the BET family of bromodomains. (+)-JQ-1 (100 nM, 48 h) prompts squamous differentiation exhibited by cell spindling, flattening and increased expression of keratin. (+)-JQ-1 (250 nM) induces rapid expression of keratin in treated NMC 797 cells compared to (-)-JQ1 (250 nM) and vehicle controls, as determined by quantitative immunohistochemistry.(+)-JQ-1 (250 nM) elicits a time-dependent induction of strong (3+) keratin staining of treated NMC 797 cells, compared to (-)-JQ1 (250 nM). De-repression of autophagy genes is observed almost immediately after (+)-JQ-1 addition. (+)-JQ-1 is a potent thienodiazepine inhibitor (Kd=90 nM) of the BET family coactivator protein BRD4, which is implicated in the pathogenesis of cancer via transcriptional control of the MYC oncogene. Dose-ranging studies of (+)-JQ-1 demonstrates potent inhibition of H4Kac4 binding with a IC50 value of 10 nM for murine BRDT(1) and 11 nM for human BRDT(1).

In Vivo: Matched cohorts of mice with established tumors are randomized to treatment with (+)-JQ1 (50 mg/kg) or vehicle, administered by daily intraperitoneal injection. Prior to randomization, and after four days of therapy, mice are evaluated by FDG-PET imaging. A marked reduction in FDG uptake is observed with (+)-JQ1 treatment. Tumor-volume measurements confirm a reduction in tumor growth with JQ1 treatment. Pharmacokinetic studies of (+)-JQ1 are performed in CD1 mice following intravenous and oral administration. Mean plasma concentration-time profiles of (+)-JQ1 after intravenous dosing (5 mg/kg). The pharmacokinetic parameters for intravenous (+)-JQ1 demonstrate excellent drug exposure (AUC=2090 hr*ng/mL) and an approximately one hour half-life (T1/2). Mean plasma concentration-time profiles of (+)-JQ1 after oral dosing (10 mg/kg). The pharmacokinetic parameters for oral (+)-JQ1 demonstrate excellent oral bioavailability (F=49%), peak plasma concentration (Cmax=1180 ng/mL) and drug exposure (AUC=2090 hr*ng/mL).

相關產品:Bioactive Compound Library Plus  |  Epigenetics Compound Library  |  Histone Modification Research Compound Library  |  Anti-Cancer Compound Library  |  CNS-Penetrant Compound Library  |  Autophagy Compound Library  |  Reprogramming Compound Library  |  Chemical Probe Library  |  Anti-Blood Cancer Compound Library  |  Target Protein Ligand Library  |  Heterocyclic Compound Library  |  Highly Selective Inhibitors Library  |  Highly Selective Activators Library  |  Cell Death Library  |  BRD4 Inhibitor-18  |  ACBI2  |  BI01826025  |  Curcumin  |  GSK6853  |  MI-1  |  GSK 4027  |  ZL0590  |  BRD4 Inhibitor-26  |  Apabetalone  |  PROTAC BRD2/BRD4 degrader-1  |  MS645  |  OF-1  |  I-CBP112  |  BRM/BRG1 ATP Inhibitor-2  |  UMB-32  |  Abemaciclib metabolite M18 hydrochloride  |  PROTAC Bcl-xL ligand-1  |  Ziftomenib  |  GSK761  |  XX-650-23  |  KB02-JQ1  |  CD235  |  I-BET151  |  VZ185  |  BET-IN-6  |  PLK1/BRD4-IN-1  |  MI-136  |  AP1867-2-(carboxymethoxy)

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