School of Basic Medical Sciences and the Institutes of Brain Science, Fudan University, Shanghai, 200032, China.
Ginkgopharma Co. Ltd, Suzhou, 215123, China.
Acta Pharmacol Sin. 2018 Nov;39(11):1746-1752. doi: 10.1038/s41401-018-0046-2. Epub 2018 Jun 21.
NS3/4A serine protease is a prime target for direct-acting antiviral therapies against hepatitis C virus (HCV) infection. Several NS3/4A inhibitors have been widely used in clinic, while new inhibitors with better characteristics are still urgently needed. GP205 is a new macrocyclic inhibitor of NS3/4A with low nanomolar activities against HCV replicons of genotypes 1b, 2a, 4a, and 5a, with EC values ranging from 1.5 to 12.8 nmol/L. In resistance selection study in vitro, we found resistance-associated substitutions on D168: The activity of GP205 was significantly attenuated against 1b replicon with D168V or D168A mutation, similar as simeprevir. No cross resistance of GP205 with NS5B or NS5A inhibitor was observed. Combination of GP205 with sofosbuvir or daclatasvir displayed additive or synergistic efficacy. The pharmacokinetic profile of GP205 was characterized in rats and dogs after oral administration, which revealed good drug exposure both in plasma and in liver and long plasma half-life. The in vitro stability test showed ideal microsomal and hepatic cells stability of GP205. The preclinical profiles of GP205 support further research on this NS3/4A inhibitor to expand the existing HCV infection therapies.
NS3/4A 丝氨酸蛋白酶是直接作用抗病毒疗法治疗丙型肝炎病毒 (HCV) 感染的主要靶点。几种 NS3/4A 抑制剂已广泛用于临床,但仍迫切需要具有更好特性的新型抑制剂。GP205 是一种新型 NS3/4A 大环抑制剂,对基因型 1b、2a、4a 和 5a 的 HCV 复制子具有低纳摩尔的活性,EC 值范围为 1.5 至 12.8nmol/L。在体外耐药选择研究中,我们发现 D168 上存在耐药相关取代:GP205 对 1b 复制子的活性明显减弱,与 simeprevir 相似,具有 D168V 或 D168A 突变。未观察到 GP205 与 NS5B 或 NS5A 抑制剂之间的交叉耐药性。GP205 与索非布韦或达卡他韦联合使用显示出相加或协同疗效。GP205 的药代动力学特征在大鼠和狗中进行了口服给药后进行了表征,结果显示在血浆和肝脏中均具有良好的药物暴露量和较长的血浆半衰期。体外稳定性试验表明,GP205 具有理想的微粒体和肝细胞稳定性。GP205 的临床前特征支持对这种 NS3/4A 抑制剂进行进一步研究,以扩大现有的 HCV 感染治疗方法。
