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与聚-L-谷氨酰胺缀合的扎那米韦在小鼠和雪貂体内对流感病毒的活性比药物本身高得多。

Zanamivir conjugated to poly-L-glutamine is much more active against influenza viruses in mice and ferrets than the drug itself.

作者信息

Weight Alisha K, Belser Jessica A, Tumpey Terrence M, Chen Jianzhu, Klibanov Alexander M

机构信息

Department of Chemistry, Massachusetts Institute of Technology, Cambridge, Massachusetts, 02139, USA.

出版信息

Pharm Res. 2014 Feb;31(2):466-74. doi: 10.1007/s11095-013-1175-4. Epub 2013 Sep 25.

Abstract

PURPOSE

Previously, polymer-attached zanamivir had been found to inhibit influenza A viruses in vitro far better than did small-molecule zanamivir (1) itself. The aim of this study was to identify in vitro-using the plaque reduction assay-a highly potent 1-polymer conjugate, and subsequently test its antiviral efficacy in vivo.

METHODS

By examining the structure-activity relationship of 1-polymer conjugates in the plaque assay, we have determined that the most potent inhibitor against several representative influenza virus strains has a neutral high-molecular-weight backbone and a short alkyl linker. We have examined this optimal polymeric inhibitor for efficacy and immunogenicity in the mouse and ferret models of infection.

RESULTS

1 attached to poly-L-glutamine is an effective therapeutic for established influenza infection in ferrets, reducing viral titers up to 30-fold for 6 days. There is also up to a 190-fold reduction in viral load when the drug is used as a combined prophylactic/therapeutic in mice. Additionally, we see no evidence that the drug conjugate stimulates an immune response in mice upon repeat administration.

CONCLUSIONS

1 attached to a neutral high-molecular-weight backbone through a short alkyl linker drastically reduced both in vitro and in vivo titers compared to those observed with 1 itself. Thus, further development of this polymeric zanamivir for the mitigation of influenza infection seems warranted.

摘要

目的

此前已发现,与聚合物相连的扎那米韦在体外对甲型流感病毒的抑制作用远优于小分子扎那米韦(1)本身。本研究的目的是通过蚀斑减少试验在体外鉴定一种高效的1-聚合物缀合物,随后在体内测试其抗病毒功效。

方法

通过在蚀斑试验中研究1-聚合物缀合物的构效关系,我们确定,针对几种代表性流感病毒株的最有效抑制剂具有中性高分子量主链和短烷基连接基。我们在小鼠和雪貂感染模型中研究了这种最佳聚合物抑制剂的功效和免疫原性。

结果

与聚-L-谷氨酰胺相连的1对雪貂已确诊的流感感染是一种有效的治疗方法,可使病毒滴度在6天内降低多达30倍。当该药物在小鼠中用作联合预防/治疗药物时,病毒载量也可降低多达190倍。此外,我们没有发现该药物缀合物在重复给药后会刺激小鼠免疫反应的证据。

结论

与1本身相比,通过短烷基连接基与中性高分子量主链相连的1在体外和体内均能大幅降低病毒滴度。因此,进一步开发这种聚合物扎那米韦以减轻流感感染似乎是有必要的。

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