Kinney William A, McDonnell Mark E, Zhong Hua Marlon, Liu Chaomin, Yang Lanyi, Ling Wei, Qian Tao, Chen Yu, Cai Zhijie, Petkanas Dean, Brenneman Douglas E
KannaLife Sciences , 3805 Old Easton Road, Doylestown, Pennsylvania 18902, United States.
PharmaAdvance, Inc. , 6 Dongsheng West Road, Building D1, Jiangyin, Jiangsu Province, P. R. China.
ACS Med Chem Lett. 2016 Feb 10;7(4):424-8. doi: 10.1021/acsmedchemlett.6b00009. eCollection 2016 Apr 14.
Cannabidiol is the nonpsychoactive natural component of C. sativa that has been shown to be neuroprotective in multiple animal models. Our interest is to advance a therapeutic candidate for the orphan indication hepatic encephalopathy (HE). HE is a serious neurological disorder that occurs in patients with cirrhosis or liver failure. Although cannabidiol is effective in models of HE, it has limitations in terms of safety and oral bioavailability. Herein, we describe a series of side chain modified resorcinols that were designed for greater hydrophilicity and "drug likeness", while varying hydrogen bond donors, acceptors, architecture, basicity, neutrality, acidity, and polar surface area within the pendent group. Our primary screen evaluated the ability of the test agents to prevent damage to hippocampal neurons induced by ammonium acetate and ethanol at clinically relevant concentrations. Notably, KLS-13019 was 50-fold more potent and >400-fold safer than cannabidiol and exhibited an in vitro profile consistent with improved oral bioavailability.
大麻二酚是大麻的非精神活性天然成分,已在多种动物模型中显示出神经保护作用。我们感兴趣的是推进一种针对罕见病肝性脑病(HE)的治疗候选药物。肝性脑病是一种发生在肝硬化或肝衰竭患者身上的严重神经系统疾病。尽管大麻二酚在肝性脑病模型中有效,但在安全性和口服生物利用度方面存在局限性。在此,我们描述了一系列侧链修饰的间苯二酚,其设计目的是提高亲水性和“药物相似性”,同时改变侧链基团内的氢键供体、受体、结构、碱性、中性、酸性和极性表面积。我们的初步筛选评估了测试药物在临床相关浓度下预防乙酸铵和乙醇对海马神经元造成损伤的能力。值得注意的是,KLS-13019的效力比大麻二酚高50倍,安全性比大麻二酚高400倍以上,并且其体外特性表明口服生物利用度有所提高。
