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基于药代动力学参数设计沙丁胺醇迟释片。

Design of salbutamol EOP tablets from pharmacokinetics parameters.

作者信息

Sinchaipanid Nuttanan, Pongwai Sansanee, Limsuwan Pichet, Mitrevej Ampol

机构信息

Department of Industrial Pharmacy, Faculty of Pharmacy, Mahidol University, Bangkok, Thailand.

出版信息

Pharm Dev Technol. 2003;8(2):135-42. doi: 10.1081/pdt-120018479.

Abstract

Salbutamol elementary osmotic pump (EOP) tablets were developed, and fundamental variables affecting their release characteristics were evaluated. The effects of film thickness and compression force on drug release from the tablets containing fixed amount of sodium chloride used as osmogent were evaluated. The core tablets were directly compressed at four compression forces and coated with 3% wt/vol cellulose acetate in acetone to levels of 2%, 3%, and 4% wt/wt. Coated tablets were drilled with CO2 laser beam to form drug delivery orifice of approximately 400 microm in diameter. The drug release was found to follow zero order fashion. The release rate decreased with the increased film thickness and was not affected by the compression force or porosity. The tablets coated to 3% and 4% levels exhibited the release rates within the range calculated from pharmacokinetic data. To illustrate the effect of osmogent content, the tablets were prepared at four osmogent levels and compressed at a constant compression force. The core tablets were coated to a level of 3% wt/wt. The release rate was initially increased with osmogent content and then decreased. At higher osmogent contents, the drug fraction in soluble component was decreased and resulted in the reduction of drug release. In conclusion, film thickness and osmogents played important roles in drug release from EOP tablets.

摘要

研发了沙丁胺醇基本渗透泵(EOP)片,并评估了影响其释放特性的基本变量。评估了膜厚度和压片力对含有固定量用作渗透促进剂的氯化钠的片剂药物释放的影响。核心片剂在四种压片力下直接压片,并用3%(重量/体积)的醋酸纤维素丙酮溶液包衣至2%、3%和4%(重量/重量)的水平。用二氧化碳激光束在包衣片剂上打孔,形成直径约400微米的药物释放孔。发现药物释放呈零级方式。释放速率随膜厚度增加而降低,不受压片力或孔隙率影响。包衣至3%和4%水平的片剂释放速率在根据药代动力学数据计算的范围内。为了说明渗透促进剂含量的影响,在四种渗透促进剂水平下制备片剂,并在恒定压片力下压片。核心片剂包衣至3%(重量/重量)的水平。释放速率最初随渗透促进剂含量增加,然后降低。在较高的渗透促进剂含量下,可溶成分中的药物分数降低,导致药物释放减少。总之,膜厚度和渗透促进剂在EOP片的药物释放中起重要作用。

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