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仿生胰岛素印迹聚合物纳米颗粒作为一种潜在的口服给药系统。

Biomimetic insulin-imprinted polymer nanoparticles as a potential oral drug delivery system.

作者信息

Paul Pijush Kumar, Treetong Alongkot, Suedee Roongnapa

机构信息

, 90112.

.

出版信息

Acta Pharm. 2017 Jun 27;67(2):149-168. doi: 10.1515/acph-2017-0020.

Abstract

In this study, we investigate molecularly imprinted polymers (MIPs), which form a three-dimensional image of the region at and around the active binding sites of pharmaceutically active insulin or are analogous to b cells bound to insulin. This approach was employed to create a welldefined structure within the nanospace cavities that make up functional monomers by cross-linking. The obtained MIPs exhibited a high adsorption capacity for the target insulin, which showed a significantly higher release of insulin in solution at pH 7.4 than at pH 1.2. In vivo studies on diabetic Wistar rats showed that the fast onset within 2 h is similar to subcutaneous injection with a maximum at 4 h, giving an engaged function responsible for the duration of glucose reduction for up to 24 h. These MIPs, prepared as nanosized material, may open a new horizon for oral insulin delivery.

摘要

在本研究中,我们研究了分子印迹聚合物(MIPs),其形成了药物活性胰岛素活性结合位点及其周围区域的三维图像,或类似于与胰岛素结合的β细胞。该方法用于通过交联在构成功能单体的纳米空间腔内创建明确的结构。所获得的MIPs对目标胰岛素表现出高吸附能力,在pH 7.4的溶液中胰岛素的释放明显高于pH 1.2时。对糖尿病Wistar大鼠的体内研究表明,2小时内快速起效,类似于皮下注射,4小时达到最大值,具有长达24小时的降低血糖持续作用。这些制备成纳米材料的MIPs可能为口服胰岛素递送开辟新的前景。

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