Development of Risperidone PLGA Microspheres.

Journal of drug delivery Pub Date : 2014-01-01 Epub Date: 2014-01-28 DOI:10.1155/2014/620464
Susan D'Souza, Jabar A Faraj, Stefano Giovagnoli, Patrick P Deluca
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引用次数: 38

Abstract

The aim of this study was to design and evaluate biodegradable PLGA microspheres for sustained delivery of Risperidone, with an eventual goal of avoiding combination therapy for the treatment of schizophrenia. Two PLGA copolymers (50 : 50 and 75 : 25) were used to prepare four microsphere formulations of Risperidone. The microspheres were characterized by several in vitro techniques. In vivo studies in male Sprague-Dawley rats at 20 and 40 mg/kg doses revealed that all formulations exhibited an initial burst followed by sustained release of the active moiety. Additionally, formulations prepared with 50 : 50 PLGA had a shorter duration of action and lower cumulative AUC levels than the 75 : 25 PLGA microspheres. A simulation of multiple dosing at weekly or 15-day regimen revealed pulsatile behavior for all formulations with steady state being achieved by the second dose. Overall, the clinical use of Formulations A, B, C, or D will eliminate the need for combination oral therapy and reduce time to achieve steady state, with a smaller washout period upon cessation of therapy. Results of this study prove the suitability of using PLGA copolymers of varying composition and molecular weight to develop sustained release formulations that can tailor in vivo behavior and enhance pharmacological effectiveness of the drug.

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利培酮PLGA微球的研制。
本研究的目的是设计和评估可生物降解的PLGA微球,用于持续递送利培酮,最终目标是避免联合治疗精神分裂症。采用两种PLGA共聚物(50:50和75:25)制备了四种利培酮微球配方。用几种体外技术对微球进行了表征。在雄性Sprague-Dawley大鼠体内的研究表明,在20和40 mg/kg剂量下,所有配方都表现出最初的爆发,随后持续释放活性部分。此外,与75:25 PLGA微球相比,50:50 PLGA微球的作用时间更短,累积AUC水平更低。一周或15天多次给药的模拟显示,所有配方的脉动行为在第二次给药时达到稳定状态。总体而言,制剂A、B、C或D的临床使用将消除联合口服治疗的需要,减少达到稳定状态的时间,停止治疗后的洗脱期更短。本研究的结果证明了使用不同组成和分子量的PLGA共聚物来开发缓释配方的适用性,该配方可以定制体内行为并增强药物的药理效力。
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Journal of drug delivery
Journal of drug delivery PHARMACOLOGY & PHARMACY-
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