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首页> 外文期刊>Journal of pharmaceutical sciences. >Oral delivery system for two-pulse colonic release of protein drugs and protease inhibitor/absorption enhancer compounds.
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Oral delivery system for two-pulse colonic release of protein drugs and protease inhibitor/absorption enhancer compounds.

机译:用于蛋白质药物和蛋白酶抑制剂/吸收增强剂化合物的两脉冲结肠释放的口服递送系统。

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It is well known that the intestinal stability and absorption of protein drugs are improved when enzyme inhibitors/permeation enhancers are coadministered. Recently, it was hypothesized that an increased effectiveness of these adjuvants might be achieved by timing their release prior to that of the protein, so that a more favorable environment would be established in advance. Therefore, an oral system was proposed for two-pulse colonic release of insulin and the protease inhibitor camostat mesilate/absorption enhancer sodium glycocholate. The device consisted of a drug-containing core, an inner swellable/erodible low-viscosity hydroxypropyl methylcellulose (HPMC) coating, an intermediate adjuvant layer, and an additional outer HPMC coating. HPMC coats and camostat mesilate/sodium glycocholate films with differing thicknesses were applied to immediate-release tablet cores by aqueous spray coating. The obtained units were characterized for weight, thickness, breaking force, and release performance. All systems showed satisfactory technological properties and the pursued pulsatile delivery behavior, with programmable delay phases preceding inhibitor/enhancer release and elapsing between inhibitor/enhancer and protein release, respectively. Indeed, both lag times linearly correlated with the relevant HPMC coating level. The system was thus proven suitable for yielding two-pulse release profiles, in which lag phases could be modulated to provide convenient concentration patterns for proteins and adjuvants.
机译:众所周知,当同时使用酶抑制剂/渗透促进剂时,蛋白质药物的肠稳定性和吸收性得到改善。最近,据推测,可以通过在蛋白质之前先释放它们来提高这些佐剂的有效性,从而可以提前建立更有利的环境。因此,提出了口服系统用于胰岛素的两脉冲结肠释放和蛋白酶抑制剂康莫司甲磺酸盐/吸收促进剂甘草酸钠。该装置包括一个含药的药芯,一个内部可溶胀/易蚀的低粘度羟丙基甲基纤维素(HPMC)涂层,一个中间佐剂层和一个额外的HPMC外部涂层。通过水性喷雾包衣将HPMC包衣和具有不同厚度的康莫司特甲磺酸盐/胆甾醇酸钠薄膜涂在速释片芯上。表征获得的单元的重量,厚度,断裂力和释放性能。所有系统均表现出令人满意的技术性能和所追求的脉动递送行为,在抑制剂/增强剂释放之前以及在抑制剂/增强剂和蛋白质释放之间分别经过可编程的延迟阶段。实际上,两个滞后时间都与相关的HPMC涂层水平线性相关。因此,该系统被证明适用于产生两脉冲释放曲线,其中可以调节滞后相,从而为蛋白质和佐剂提供方便的浓度模式。

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