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KMID : 1146920190490050565
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Journal of Pharmaceutical Investigation
2019 Volume.49 No. 5 p.565 ~ p.573
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Liposomal formulation and pharmacokinetic study of CPD409, a novel sodium channel blocker
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Lee Ga-Hee
Shin Dae-Hwan
Suh Hong-Won
Lee Jae-Yong
Lim Soon-Sung
Kim Jin-Seok
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Abstract
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Purpose: CPD409 is a novel sodium channel blocker for pain control in chemotherapy-induced peripheral neuropathy with a very poor water solubility of less than 10 ¥ìg/mL. The aim of this study is to improve the aqueous solubility of CPD409 by using inclusion complexes with ¥â-cyclodextrin (¥â-CD) and 2-hydroxypropyl-¥â-cyclodextrin (HP-¥â-CD).
Methods: The inclusion complexes were prepared by two different methods; common solvent evaporation (CSE) and freeze-drying (FD) method.
Results: The phase solubility study indicated that HP-¥â-CD showed 3-times higher formation constant with CPD409 than ¥â-CD. Inclusion complexes at a molar ratio of 1:2 increased the solubility of CPD409 by 130 times when compared with pure CPD409. The physicochemical characterization of the prepared formulation confirmed the formation of CPD409/HP-¥â-CD inclusion complexes. In dissolution study, inclusion complexes at a molar ratio of 1:2 released 70% of CPD409 but CSE method showed more rapid dissolution profile than FD method. Pharmacokinetic study also showed an increased bioavailability in 1:2 formulation compared to pure CPD409. In conclusion, inclusion complexes of CSE and FD method at a molar ratio of 1:2 showed increased solubility, dissolution rate, and bioavailability of CPD409.
Conclusion: Therefore, complexation of CPD409 with HP-¥â-CD using CSE and FD method at a molar ratio 1:2 can be promising strategy for effective oral delivery.
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KEYWORD
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CPD409, Solubilization, Pharmacokinetics, Dissolution, ¥â-Cyclodextrin, Oral delivery
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