Fabrication of Polyisobutene Based Matrix Patches for Transdermal Delivery of Atenolol

耐折性 透皮 乙基纤维素 阿替洛尔 渗透 极限抗拉强度 材料科学 透皮贴片 生物医学工程 聚合物 色谱法 复合材料 药理学 化学 医学 血压 内科学 生物化学
作者
Archana S. Patil,Shriraj S. Kamat,Shraja U. Birkodi,Umashri A Kokatanur,Rajashree Masareddy,Panchaxari Mallappa Dandagi
出处
期刊:Research journal of pharmacy and technology [Diva Enterprises Private Limited]
卷期号:: 2085-2090 被引量:1
标识
DOI:10.52711/0974-360x.2023.00342
摘要

One of the possible routes for local and systemic delivery of hypertensive drugs has been identified as transdermal administration. Monolithic drugs in adhesive patches have the advantages of being relatively simple to manufacture and having limited dimensions of both thickness and surface area. Polyisobutene is a pressure-sensitive adhesive polymer often used in transdermal patch preparation. Polyisobutenes with varying molecular weight distributions have differing viscosities, which can affect drug release. In the current study, Atenolol transdermal patches were made with different proportions of low and high molecular weight polyisobutene and ethyl cellulose as a thickening agent. Prepared patches were evaluated for their physicochemical properties like thickness, weight variation, folding endurance, tensile strength, moisture content, drug content and in- vitro permeation rate. Based on tensile strength (1.92kg/mm2), folding endurance (343) and in-vitro permeation rate (85.79%) at the end of 30th hour, F1 formulation was found to be optimum. Ex vivo permeation study was carried out using rat skin and 67.09% drug permeated at the end of 30th hour. Formulations were subjected to stability studies for 60 days and were found to be stable. Thus, an ideal combination of polyisobutenes in the ratio 3:1 (High Molecular Weight: Low Molecular Weight) and ethyl cellulose (200mg) would serve as the best choice for fabrication of Atenolol patches for its sustained effect.

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