Study of the Tableting Properties of MCR, a Newly Coprocessed Cellulose-based Direct Compression Excipient

S. Aly
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引用次数: 2

Abstract

The current need for strategies to accelerate and optimize the efforts to develop new in-expensive multifunctional direct compression tableting excipients with minimum risk to the products has urged the workers in pharmaceutical industry field to search for a simple and low cost-effective technique to tailor and engineer multi-functional excipients. Developing new pharmaceutically inactive materials serving as excipients, new grades of existing excipients and co-processing of already existing excipients constitute the techniques utilized to develop multifunctional excipients [1-3]. Developing of new tableting excipients is a tedious and time consuming multi-stage process. In addition to that, the regulatory concerns and issues related to safety and toxicity assessment should be strictly followed. The co-processed excipients can be at high cost effective. Therefore, a great deal of attention was directed to co-processing as a means to develop multifunctional excipients [4-7]. This technique has been defined as particle engineering of individual excipients and excipient combinations using co-processing by virtue, of sub-particle modifications [4,5]. The workers in pharmaceutical industry field has accelerated the steps towards developing direct compression tableting excipients of high functionality in terms of flow, compression, good binding, improved lubricating efficiency and improved dilution potential could be developed [5-8]. Co-processed excipients are produced from two or more existing excipients of different chemical nature. Each excipient exerts a special function in formulations as well as in the corresponding tablets. It should be clear in mind that the physico-chemical properties of the co-processed excipient is, to a great extent, affected by the chemical nature of the excipients contributed to co-processing.
新型协同加工纤维素基直接压缩赋形剂MCR的压片性能研究
当前需要的策略是加快和优化开发新的多功能直接压缩片剂的努力,在昂贵的产品风险最小的情况下,促使制药工业领域的工人寻找一种简单和低成本的技术来定制和设计多功能辅料。开发新的非活性赋形剂、现有赋形剂的新品级和现有赋形剂的协同加工构成了开发多功能赋形剂的技术[1-3]。新型片剂辅料的研制是一个繁琐、耗时的多阶段过程。除此之外,还应严格遵守与安全性和毒性评估有关的法规和问题。共加工辅料具有较高的成本效益。因此,协同加工作为开发多功能辅料的一种手段受到了极大的关注[4-7]。该技术被定义为利用亚粒子修饰的协同加工,对单个赋形剂和赋形剂组合进行粒子工程[4,5]。制药工业领域的工作者已经加快了开发流动、压缩、良好结合、提高润滑效率和提高稀释潜力的高功能直接压缩片剂的步伐[5-8]。共加工辅料是由两种或两种以上具有不同化学性质的现有辅料生产而成。每种赋形剂在制剂和相应片剂中都有特殊的作用。应该清楚的是,协同加工辅料的理化性质在很大程度上受到协同加工辅料的化学性质的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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