Impact of Crystal Habit on Biopharmaceutical Performance of Celecoxib

被引:79
|
作者
Modi, Sameer R. [1 ]
Dantuluri, Ajar K. R. [1 ]
Puri, Vibha [1 ]
Pawar, Yogesh B. [1 ]
Nandekar, Prajwal [2 ]
Sangamwar, Abhay T. [2 ]
Perumalla, Sathyanarayana R. [3 ]
Sun, Changquan Calvin [3 ]
Bansal, Arvind K. [1 ]
机构
[1] NIPER, Dept Pharmaceut, Sas Nagar 160062, Punjab, India
[2] NIPER, Dept Pharmacoinformat, Sas Nagar 160062, Punjab, India
[3] Univ Minnesota, Coll Pharm, Dept Pharmaceut, Minneapolis, MN 55455 USA
关键词
ANISOTROPIC SURFACE-CHEMISTRY; I PARACETAMOL CRYSTALS; ACETYL SALICYLIC-ACID; PHARMACEUTICAL POWDERS; CONTACT ANGLES; FORM-I; INTRINSIC DISSOLUTION; ASPIRIN CRYSTALS; WETTABILITY; SOLVENT;
D O I
10.1021/cg400140a
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
Poor biopharmaceutical performance of Bio-pharmaceutical Classification System (BCS) class II drug molecules is a major hurdle in the design and development of pharmaceutical formulations. Anisotropic surface chemistry of different facets in crystalline material affects physicochemical properties, such as wettability, of drugs. In the present investigation, a molecule-centered approach is presented toward crystal habit modification of celecoxib (CEL) and its effect on oral bioavailability. Two crystal habits of CEL, acicular crystal habit (CEL-A) and a plate-shaped crystal habit (CEL-P), were obtained by recrystaffization from toluene at 25 and 60 degrees C, respectively. Compared to CEL-A, CEL-P exhibited significantly faster dissolution kinetics in aqueous media significantly higher C-max and shorter T-max in an oral bioavailability study. The significant enhancement in dissolution and biopharmaceutical performance of CEL-P was attributed to its more abundant hydrophilic surfaces compared to CEL-A. This conclusion was supported by wettability and surface free energy determination from contact angle measurements and surface chemistry determination by X-ray photoelectron spectroscopy (XPS), crystal structure modeling, and crystal face indexation.
引用
收藏
页码:2824 / 2832
页数:9
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