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目錄:MedChemExpress LLC>>生化試劑>> Aticaprant | MCE

Aticaprant | MCE
  • Aticaprant | MCE
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更新時(shí)間:2023-06-16 17:12:51瀏覽次數(shù):212評價(jià)

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CAS 1174130-61-0 純度 99.87%
分子量 418.5 分子式 C??H??FN?O?
供貨周期 現(xiàn)貨 規(guī)格 5 mg
貨號 HY-101718 應(yīng)用領(lǐng)域 醫(yī)療衛(wèi)生,化工,生物產(chǎn)業(yè),制藥
Aticaprant | MCEAticaprant (CERC-501) is a potent and centrally-penetrant <b>kappa opioid</b> receptor antagonist with a <b>K<sub>i</sub></b> of 0.807 nM.

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Aticaprant

CAS No. : 1174130-61-0

產(chǎn)品活性:Aticaprant (CERC-501) is a potent and centrally-penetrant kappa opioid receptor antagonist with a Ki of 0.807 nM.

研究領(lǐng)域:GPCR/G Protein  |  Neuronal Signaling

作用靶點(diǎn):Opioid Receptor

In Vitro: Aticaprant (CERC-501) binds with high affinity to the human kappa opioid receptor with a 30-fold higher affinity over the human mu opioid receptor and 190-fold higher affinity over the human delta opioid receptor. Aticaprant (CERC-501) shows no appreciable affinity for several non-opioid cell surface G-protein-coupled receptor targets, including monoaminergic, muscarinic, cholinergic, and adrenergic receptors or ion channel/transporter binding targets or the central benzodiazepine binding site.

In Vivo: Aticaprant (CERC-501) has a rapid absorption (tmax=1-2 h) and good oral bioavailability (F=25%). Oral Aticaprant (CERC-501) administration selectively and potently occupies central kappa opioid receptors (ED50=0.33 mg/kg), without evidence of mu or delta receptor occupancy. LY2456302 potently blocks kappa-agonist-mediated analgesia and disruption of prepulse inhibition, without affecting mu-agonist-mediated effects at doses >30-fold higher. Aticaprant (CERC-501) produces antidepressant-like effects in the mouse forced swim test and enhances the effects of imipramine and citalopram. Aticaprant (CERC-501) reduces ethanol self-administration in alcohol-preferring rats. Aticaprant (CERC-501) alleviates the nicotine withdrawal syndrome, as evidenced by decreased expression of nicotine withdrawal induced anxiety-related behavior, somatic signs, and CPA, and increased hotplate latency in nicotine withdrawn mice following pre-treatment.

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