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一种用于通过滚压造粒和干法制粒工艺支持片剂配方设计的可压性变化分类系统。

A tabletability change classification system in supporting the tablet formulation design via the roll compaction and dry granulation process.

作者信息

Su Junhui, Zhang Kunfeng, Qi Feiyu, Cao Junjie, Miao Yuhua, Zhang Zhiqiang, Qiao Yanjiang, Xu Bing

机构信息

Department of Chinese Medicine Informatics, Beijing University of Chinese Medicine, Beijing 100029, PR China.

Beijing Key Laboratory of Chinese Medicine Manufacturing Process Control and Quality Evaluation, Beijing 100029, PR China.

出版信息

Int J Pharm X. 2023 Jul 28;6:100204. doi: 10.1016/j.ijpx.2023.100204. eCollection 2023 Dec 15.

Abstract

In this paper, the material library approach was used to uncover the pattern of tabletability change and related risk for tablet formulation design under the roll compaction and dry granulation (RCDG) process. 31 materials were fully characterized using 18 physical parameters and 9 compression behavior classification system (CBCS) parameters. Then, each material was dry granulated and sieved into small granules (125-250 μm) and large granules (630-850 μm), respectively. The compression behavior of granules was characterized by the CBCS descriptors, and were compared with that of ungranulated powders. The relative change of tabletability () index was used to establish the tabletability change classification system (TCCS), and all materials were classified into three types, i.e. loss of tabletability (LoT, Type I), unchanged tabletability (Type II) and increase of tabletability (Type III). Results showed that approximately 65% of materials presented LoT, and as the granules size increased, 84% of the materials exhibited LoT. A risk decision tree was innovatively proposed by joint application of the CBCS tabletability categories and the TCCS tabletability change types. It was found that the LoT posed little risk to the tensile strength of the final tablet, when Category 1 or 2A materials, or Category 2B materials with Type II or Type III change of tabletability were used. Formulation risk happened to Category 2C or 3 materials, or Category 2B materials with Type I change of tabletability, particularly when high proportions of these materials were involved in tablet formulation. In addition, the risk assessment results were verified in the material property design space developed from a latent variable model in prediction of tablet tensile strength. Overall, results suggested that a combinational use of CBCS and TCCS could aid the decision making in selecting materials for tablet formulation design via RCDG.

摘要

在本文中,采用材料库方法来揭示在滚压造粒和干法制粒(RCDG)工艺下片剂可压性变化模式及片剂配方设计的相关风险。使用18个物理参数和9个压缩行为分类系统(CBCS)参数对31种材料进行了全面表征。然后,将每种材料进行干法制粒,并分别筛分为小颗粒(125 - 250μm)和大颗粒(630 - 850μm)。颗粒的压缩行为通过CBCS描述符进行表征,并与未制粒粉末的压缩行为进行比较。使用可压性()指数的相对变化建立可压性变化分类系统(TCCS),所有材料被分为三种类型,即可压性损失(LoT,I型)、可压性不变(II型)和可压性增加(III型)。结果表明,约65%的材料表现出可压性损失,并且随着颗粒尺寸的增加,84%的材料表现出可压性损失。通过联合应用CBCS可压性类别和TCCS可压性变化类型,创新性地提出了一个风险决策树。结果发现,当使用1类或2A类材料,或可压性发生II型或III型变化的2B类材料时,可压性损失对最终片剂的拉伸强度几乎没有风险。配方风险发生在2C类或3类材料,或可压性发生I型变化的2B类材料上,特别是当这些材料在片剂配方中占比很高时。此外,在由预测片剂拉伸强度的潜变量模型开发的材料性能设计空间中验证了风险评估结果。总体而言,结果表明CBCS和TCCS的组合使用有助于通过RCDG为片剂配方设计选择材料时的决策制定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b83/10407897/f3f5961fb021/ga1.jpg

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