Freund B, Gravenstein S, Elliott M, Miller I
Eastern Virginia Medical School, Norfolk, USA.
Drug Saf. 1999 Oct;21(4):267-81. doi: 10.2165/00002018-199921040-00003.
Preclinical and clinical studies have clearly demonstrated that zanamivir, a potent and highly selective inhibitor of the influenza A and B virus neuraminidase, has an impressive safety profile. This report describes the safety and tolerability findings from the clinical studies completed up to the 17 July 1998 involving over 6000 adult and adolescent patients from North America, Europe and the Southern Hemisphere. Serious adverse events from an ongoing Japanese clinical programme are also reported. Zanamivir was administered in various dose forms and frequencies and was found to have a comparable safety profile with placebo when given for both the treatment and prophylaxis of influenza-like illness. These findings were independent of age and underlying medical condition. 4152 patients received zanamivir and the most commonly reported adverse events were consistent with the signs and symptoms of influenza-like illness. Most of the adverse events were mild and did not result in patient withdrawal from the studies. Less than 1% of zanamivir and placebo recipients reported a serious adverse event. In addition, 490 healthy volunteers received zanamivir in clinical pharmacology studies. It was well tolerated and the incidence of adverse events was similar in zanamivir and placebo recipients. In addition, no clinically significant laboratory abnormalities were detected. Results from in vitro and in vivo animal studies suggest that zanamivir has low acute toxicity and no significant systemic toxicity or respiratory tract irritancy at plasma exposures more than 100-fold higher than those anticipated following clinical use. Neither genotoxic nor reproductive types of toxicity have been observed in toxicology studies at doses equal to 17 to 197 times the current therapeutic dose (20 mg/day). The characteristics of the molecule and the low systemic exposure indicate a very low potential for drug interactions with the inhaled route. Furthermore, repeated 600mg intravenous doses were well tolerated in healthy volunteers. The observed safety profile of zanamivir compares favourably with currently available agents with anti-influenza virus activity, such as rimantadine and amantadine, as well as GS4104, a neuraminidase inhibitor currently in phase III development. This may be attributed to the low systemic bioavailability of zanamivir, which is given by oral inhalation, direct to the primary site of viral replication. The potential advantages of this include a reduced risk of drug-drug interactions, other nontarget organ toxicities (e.g. brain) and drug clearance issues from both kidney and liver. Therefore, the safety profile of zanamivir supports its use in the management of influenza.
临床前和临床研究已明确表明,扎那米韦作为一种强效且高度选择性的甲型和乙型流感病毒神经氨酸酶抑制剂,具有令人印象深刻的安全性。本报告描述了截至1998年7月17日完成的临床研究中的安全性和耐受性结果,这些研究涉及来自北美、欧洲和南半球的6000多名成年和青少年患者。还报告了正在进行的日本临床项目中的严重不良事件。扎那米韦以多种剂型和频率给药,在用于治疗和预防流感样疾病时,其安全性与安慰剂相当。这些结果与年龄和潜在疾病无关。4152名患者接受了扎那米韦治疗,最常报告的不良事件与流感样疾病的体征和症状一致。大多数不良事件为轻度,未导致患者退出研究。接受扎那米韦和安慰剂的患者中,报告严重不良事件的比例均不到1%。此外,490名健康志愿者在临床药理学研究中接受了扎那米韦。它耐受性良好,扎那米韦组和安慰剂组的不良事件发生率相似。此外,未检测到具有临床意义的实验室异常。体外和体内动物研究结果表明,扎那米韦急性毒性低,在血浆暴露量比临床使用预期高100倍以上时,无明显全身毒性或呼吸道刺激性。在毒理学研究中,给予相当于当前治疗剂量(20mg/天)17至197倍的剂量时,未观察到遗传毒性或生殖毒性。该分子的特性和低全身暴露表明通过吸入途径发生药物相互作用的可能性非常低。此外,健康志愿者对600mg静脉重复给药耐受性良好。扎那米韦观察到的安全性与目前可用的具有抗流感病毒活性的药物(如金刚乙胺和金刚烷胺)以及目前处于III期开发阶段的神经氨酸酶抑制剂GS4104相比具有优势。这可能归因于扎那米韦口服吸入给药时全身生物利用度低,直接作用于病毒复制的主要部位。其潜在优势包括降低药物相互作用、其他非靶器官毒性(如脑部)以及肾和肝药物清除问题的风险。因此,扎那米韦的安全性支持其用于流感的治疗。
