BETA-CYCLODEXTRIN DERIVATIVES, SBE4-BETA-CD AND HP-BETA-CD, INCREASE THE ORAL BIOAVAILABILITY OF CINNARIZINE IN BEAGLE DOGS

被引：81

作者：

JARVINEN, T

JARVINEN, K

SCHWARTING, N

STELLA, VJ

机构：

[1] UNIV KANSAS,DEPT PHARMACEUT CHEM,LAWRENCE,KS 66045

[2] UNIV KANSAS,CTR DRUG DELIVERY RES,LAWRENCE,KS 66045

[3] UNIV KANSAS,ANIM CARE UNIT,LAWRENCE,KS 66045

[4] UNIV KUOPIO,DEPT PHARMACEUT TECHNOL,SF-70211 KUOPIO,FINLAND

[5] UNIV KUOPIO,DEPT CHEM,SF-70211 KUOPIO,FINLAND

来源：

JOURNAL OF PHARMACEUTICAL SCIENCES | 1995年 / 84卷 / 03期

关键词：

D O I：

10.1002/jps.2600840306

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

The absolute bioavailabilities (F-abs) of cinnarizine after oral administration as two modified beta-cyclodextrin (SBE4-beta-CD or HP-beta-CD) solutions, an aqueous suspension, and two capsules in fasted beagle dogs were determined. Cinnarizine was administered orally (25.0 mg) and intravenously (12.5 mg) to four dogs. Blood samples were drawn for 24.5 h postdosing, and cinnarizine levels in plasma were determined by HPLC with spectrofluorometric detection. Cinnarizine pharmacokinetics after iv administration as a 1.25 mg/mL SBE4-beta-CD solution followed triexponential behavior (t(1/2) = 12.6 +/- 0.4 h and Cl = 1.4 +/- 0.17 L/h/kg). A very low bioavailability of cinnarizine with a wide interanimal variation was observed after oral administration as a suspension (F-abs = 8 +/- 4%) or capsule containing only cinnarizine (F-abs = 0.8 +/- 0.4%) Administration of cinnarizine as a CD complex either as a solution (F-abs = 55-60%) or in a capsule (F-abs = 38 +/- 12%) significantly enhanced the bioavailability. Since the solutions showed excellent bioavailability, the logical conclusion is that, once presented as a solution, cinnarizine is well absorbed and that cinnarizine rapidly dissociates from its inclusion complexes. Presumably, the elevated bioavailability from the SBE4-beta-CD containing capsule was due to rapid dissolution and release of cinnarizine.

引用

页码：295 / 299

页数：5

共 30 条

[1] CYCLODEXTRINS IN THE PHARMACEUTICAL FIELD
BEKERS, O
UIJTENDAAL, EV
BEIJNEN, JH
BULT, A
UNDERBERG, WJM
[J]. DRUG DEVELOPMENT AND INDUSTRIAL PHARMACY, 1991, 17 (11) : 1503 - 1549
[2] CASTANEDAHERNAN.G, 1993, ARZNEIM FORSCH DRUG, V43, P539
[3] THE EFFECTS OF CYCLODEXTRINS ON DRUG ABSORPTION .2. INVIVO OBSERVATIONS
FRIJLINK, HW
EISSENS, AC
SCHOONEN, AJM
LERK, CF
[J]. INTERNATIONAL JOURNAL OF PHARMACEUTICS, 1990, 64 (2-3) : 195 - 205
[4] Gibaldi M., 1982, PHARMACOKINETICS, Vsecond
[5] GODFRAIND T, 1982, DRUG TODAY, V18, P27
[6] PHYSIOLOGICALLY BASED PHARMACOKINETIC MODEL FOR DIGOXIN DISPOSITION IN DOGS AND ITS PRELIMINARY APPLICATION TO HUMANS
HARRISON, LI
GIBALDI, M
[J]. JOURNAL OF PHARMACEUTICAL SCIENCES, 1977, 66 (12) : 1679 - 1683
[7] Higuchi T., 1965, PHASE SOLUBILITY TEC, V4, P117
[8] DETERMINATION OF CINNARIZINE IN PLASMA BY HIGH-PERFORMANCE LIQUID-CHROMATOGRAPHY
HUNDT, HKL
BROWN, LW
CLARK, EC
[J]. JOURNAL OF CHROMATOGRAPHY, 1980, 183 (03): : 378 - 382
[9] SOLUBILIZATION OF A TRIPEPTIDE HIV PROTEASE INHIBITOR USING A COMBINATION OF IONIZATION AND COMPLEXATION WITH CHEMICALLY-MODIFIED CYCLODEXTRINS
JOHNSON, MD
HOESTEREY, BL
ANDERSON, BD
[J]. JOURNAL OF PHARMACEUTICAL SCIENCES, 1994, 83 (08) : 1142 - 1146
[10] PLASMA CINNARIZINE LEVELS RESULTING FROM ORAL-ADMINISTRATION AS CAPSULE OR TABLET FORMULATION INVESTIGATED BY GAS-LIQUID-CHROMATOGRAPHY
MORRISON, PJ
BRADBROOK, ID
ROGERS, HJ
[J]. BRITISH JOURNAL OF CLINICAL PHARMACOLOGY, 1979, 7 (04) : 349 - 352

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