氯氮平Niosomal透皮贴剂的制备与评价

K. Nagasree, K. Pallavi, R. Sri. S
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引用次数: 0

摘要

乳小体是合成的非离子表面活性剂水化后得到的非离子表面活性剂囊泡。这些是有效的经皮给药的有前途的载体。本研究的目的是开发一种稳定的氯氮平透皮贴剂。采用溶剂铸造法制备了乳质体。对所有配方进行了囊泡大小、zeta电位和包封率的评价。然后对所有贴片进行厚度、折叠耐力、药物含量测定、平整度和体外渗透研究。优选出最佳粒径为2.6m、zeta电位最高(-32.56mV)、包封率最高(98.09%)的F3配方。以优化后的纳米体配方F3为原料,采用溶剂铸造法制备透皮贴剂。将制备的优化后的纳米体F3制剂装入贴片制剂中。载膜小体(F3NT3)贴片的累积药物渗透率为95.78%。优化后的配方(F3NT3)符合一级释放动力学。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Preparation and Evaluation of Niosomal Transdermal Patch of Clozapine
Niosomes are the non-ionic surfactant vesicles obtained on hydration of synthetic non-ionic surfactants. These are the promising vehicles for effective transdermal drug delivery. The present research work was aimed to develop niosomal-based transdermal Clozapine patch containing a stable formulation with improved drug permeation. Niosomes were prepared by solvent casting method. All the formulations were evaluated for vesicle size, zeta potential and percent entrapment efficiency. All the patches were then characterized for thickness, folding endurance, drug content determination, Flatness, and in vitro permeation studies. F3 formulation having optimum vesicle size (2.6m), highest zeta potential (-32.56mV) and maximum percent entrapment efficiency (98.09%) was selected as optimized formulation. The transdermal patch was prepared using solvent casting method from the optimised niosomes formulation F3 formulation. The prepared optimised niosomes F3 formulation were loaded into the patch formulation. Patches loaded with niosomes (F3NT3) showed 95.78 % cumulative amount of drug permeated. The optimized formulation (F3NT3) followed first order release kinetics.
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