Development of a Novel Controlled-Release Tablet of Pregabalin: Formulation Variation and Pharmacokinetics in Dogs and Humans

被引:14
|
作者
Kim, Kyung Hun [1 ,2 ,3 ]
Lim, Seo Hyun [3 ]
Shim, Cho Rok [3 ]
Park, Junsung [3 ]
Song, Woo Heon [3 ]
Kwon, Min Chang [3 ]
Lee, Jong Hyuk [4 ]
Park, Jun Sang [3 ]
Choi, Han-Gon [1 ,2 ]
机构
[1] Hanyang Univ, Coll Pharm, Ansan, South Korea
[2] Hanyang Univ, Inst Pharmaceut Sci & Technol, Ansan, South Korea
[3] GL PharmTech Corp, Seongnam, South Korea
[4] Hoseo Univ, Coll Life & Hlth Sci, Dept Pharmaceut Engn, Asan, South Korea
来源
关键词
controlled-release; three-layered tablet; polyethylene oxide; high swellable; once-a-day; DRUG-RELEASE; GABAPENTIN NEURONTIN; DOSING FREQUENCY; ADHERENCE; SUBUNIT;
D O I
10.2147/DDDT.S222505
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Background: Novel three-layered (TL) tablet systems were compared with both monolithic matrix (MM) formulations and a commercial immediate-release (IR) capsule to develop once-a-day (OAD) pregabalin tablets. Methods: The physical properties of the TL tablets, including dissolution and swelling rates, were compared with those of the MM tablets and the pharmacokinetic parameters of the TL tablet were compared with those of an IR capsule in beagles and humans. Results: Our results indicated that the same amount of a hydrophilic polymer in the formulations had similar dissolution profiles at 12 h, regardless of the tablet geometry. However, the degree of tablet swelling differed, with larger amounts of polymer in the tablets showing a greater degree of swelling. In addition, TL tablets swelled more rapidly compared with MM tablets. For the pharmacokinetic study of the TL tablet, the beagles demonstrated absorption results similar to those of an IR capsule, whereas the humans demonstrated low total absorption compared with an IR capsule. The time of the peak plasma concentration at 6 h in the fed state of humans coincided with the results of the study on beagles. Conclusion: The novel TL tablet system of pregabalin may prove to be helpful in developing improved formulations with better continuous drug absorption for OAD administration.
引用
收藏
页码:445 / 456
页数:12
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