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Potential applications of polymeric microsphere suspension as subcutaneous depot for insulin.

机译:聚合物微球悬浮液作为胰岛素皮下贮库的潜在应用。

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摘要

The objective of this investigation was to develop an injectable, depot-forming drug delivery system for insulin based on microparticle technology to maintain constant plasma drug concentrations over prolonged period of time for the effective control blood sugar levels. Formulations were optimized with two well-characterized biodegradable polymers namely, poly(DL-lactide-co-glycolide) and poly-epsilon-caprolactone and evaluated in vitro for physicochemical characteristics, drug release in phosphate buffered saline (pH 7.4), and evaluated in vivo in streptozotocin-induced hypoglycemic rats. With a large volume of internal aqueous phase during w/o/w double emulsion solvent evaporation process and high molecular weight of the polymers used, we could not achieve high drug capture and precise control over subsequent release within the study period of 60 days. However, this investigation revealed that upon subcutaneous injection, the biodegradable depot-forming polymeric microspheres controlled the drug release and plasma sugar levels more efficiently than plain insulin injection. Preliminary pharmacokinetic evaluation exhibited steady plasma insulin concentration during the study period. These formulations, with their reduced frequency of administration and better control over drug disposition, may provide an economic benefit to the user compared with products currently available for diabetes control.
机译:这项研究的目的是开发一种基于微粒技术的胰岛素可注射,长效剂形成的药物输送系统,以在长时间内保持恒定的血浆药物浓度,以有效控制血糖水平。用两种良好表征的可生物降解聚合物,即聚(DL-丙交酯-共-乙交酯)和聚ε-己内酯对配方进行优化,并在体外评估其理化特性,在磷酸盐缓冲液(pH 7.4)中的药物释放,并在在链脲佐菌素诱导的降血糖大鼠体内。由于在w / o / w双乳液溶剂蒸发过程中存在大量内部水相,并且所用聚合物的分子量较高,因此在60天的研究期内,我们无法实现较高的药物捕获率和后续释放的精确控制。但是,这项研究表明,皮下注射后,可生物降解的形成贮库的聚合物微球比普通胰岛素注射更有效地控制药物释放和血浆糖水平。在研究期间,初步药代动力学评估显示血浆胰岛素浓度稳定。与目前可用于糖尿病控制的产品相比,这些制剂具有降低的给药频率和更好地控制药物处置的特性,可以为用户带来经济利益。

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