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开发新型制剂,以增强腺病毒介导的基因在体外和体内肺中的表达。

Development of novel formulations that enhance adenoviral-mediated gene expression in the lung in vitro and in vivo.

作者信息

Croyle M A, Cheng X, Sandhu A, Wilson J M

机构信息

Division of Pharmaceutics, The University of Texas at Austin College of Pharmacy, Austin, TX 78712, USA.

出版信息

Mol Ther. 2001 Jul;4(1):22-8. doi: 10.1006/mthe.2001.0411.

Abstract

Despite remarkable progress in the development of both viral and non-viral gene delivery vectors for cystic fibrosis therapy, low efficiency of gene transfer to the airway epithelium is a major obstacle to clinical application. Here we develop formulations that enhance cellular absorption of adenoviral vectors. We selected excipients from a panel of pharmaceutically acceptable com-pounds known to enhance drug absorption. Transduction efficiency of the virus in the presence of each ingredient was assessed in vitro and in vivo. Mannitol and chitosan substantially enhanced transduction efficiency in vitro and augmented expression in vivo by 4 and 8 log units, respectively. The most successful formulation (a blend of sucrose, mannitol, and Pluronic F68) transduced 100% of an A549 cell population in vitro and produced areas of intense gene expression in both large and small airways in vivo with minimal toxicity. Dose response studies also indicate that when placed in this formulation, the viral dose can be lowered by 1/2 log while maintaining superior levels of transgene expression. This formulation also enhanced the physical stability of the virus. No significant loss in titer was detected from a lyophilized formulation after storage at 25 degrees C for 30 days.

摘要

尽管在用于囊性纤维化治疗的病毒和非病毒基因递送载体的开发方面取得了显著进展,但基因向气道上皮细胞转移的低效率仍是临床应用的主要障碍。在此,我们开发了可增强腺病毒载体细胞吸收的制剂。我们从一组已知可增强药物吸收的药学上可接受的化合物中选择辅料。在体外和体内评估了每种成分存在下病毒的转导效率。甘露醇和壳聚糖在体外显著提高了转导效率,在体内分别使表达增加了4个和8个对数单位。最成功的制剂(蔗糖、甘露醇和普朗尼克F68的混合物)在体外转导了100%的A549细胞群体,并在体内大小气道中产生了强烈的基因表达区域,且毒性最小。剂量反应研究还表明,当置于该制剂中时,病毒剂量可降低1/2对数,同时保持转基因表达的优异水平。该制剂还增强了病毒的物理稳定性。冻干制剂在25℃储存30天后未检测到效价有显著损失。

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