ABSORPTION OF DANAZOL AFTER ADMINISTRATION TO DIFFERENT SITES OF THE GASTROINTESTINAL-TRACT AND THE RELATIONSHIP TO SINGLE-PEAK AND DOUBLE-PEAK PHENOMENA IN THE PLASMA PROFILES

被引：43

作者：

CHARMAN, WN

ROGGE, MC

BODDY, AW

BARR, WH

BERGER, BM

机构：

[1] STERLING WINTHROP PHARMACEUT RES DIV,DEPT PHARMACEUT SCI,MALVERN,PA

[2] STERLING WINTHROP PHARMACEUT RES DIV,DEPT BIOMETR,MALVERN,PA

[3] STERLING WINTHROP PHARMACEUT RES DIV,DEPT CLIN RES,MALVERN,PA

[4] VIRGINIA COMMONWEALTH UNIV,SCH PHARM,RICHMOND,VA

[5] STERLING WINTHROP PHARMACEUT RES DIV,DEPT DRUG METAB,MALVERN,PA

来源：

JOURNAL OF CLINICAL PHARMACOLOGY | 1993年 / 33卷 / 12期

关键词：

D O I：

10.1002/j.1552-4604.1993.tb03921.x

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

The absorption of danazol (100 mg) after oral or intraintestinal administration to the proximal jejunum or proximal ileum has been studied in healthy female subjects. The extent of danazol absorption after administration as a solubilized glycerol mono-oleate emulsion formulation was approximately twofold and fourfold greater after oral dosing when compared with jejunal or ileal administration, respectively. Although not statistically significant in this study, the extent of absorption after jejunal administration was generally greater than after ileal administration. After oral dosing, qualitative assessment identified the presence of double peaks or major shouldering characteristics in 14 of the 16 individual danazol plasma concentration-time profiles, whereas only single peaks were present after intraintestinal administration. These data are consistent with the double peaking phenomena after oral administration of the emulsion formulation being stomach-related. The double peaking effect may be explained in terms of a probable combination of gastric emptying regulated absorption (due to the presence of the lipid in the emulsion formulation) and the dependence of danazol solubility on bile salt solubilization within the upper small intestine.

引用

页码：1207 / 1213

页数：7

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