EFFECTS OF PLAIN AND CONTROLLED-ILEAL-RELEASE BUDESONIDE FORMULATIONS IN EXPERIMENTAL ILEITIS

被引：10

作者：

BOYD, AJ

SHERMAN, IA

SAIBIL, FG

机构：

[1] SUNNYBROOK HLTH SCI CTR,ARON M RAPPAPORT MICROCIRCULAT LAB,TORONTO,ON M4N 3M5,CANADA

[2] UNIV TORONTO,INST BIOMED ENGN,DEPT PHYSIOL,TORONTO,ON M5S 1A1,CANADA

[3] UNIV TORONTO,INST BIOMED ENGN,DEPT MED,TORONTO,ON M5S 1A1,CANADA

来源：

SCANDINAVIAN JOURNAL OF GASTROENTEROLOGY | 1995年 / 30卷 / 10期

关键词：

BUDESONIDE; CORTISOL; EXPERIMENTAL ILEITIS; HAMSTER; INTESTINAL INFLAMMATION; MAST CELLS; MYELOPEROXIDASE ACTIVITY; TRINITROBENZENE SULFONIC ACID;

D O I：

10.3109/00365529509096341

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

Background: Budesonide combines a topical anti-inflammatory activity with high first-pass hepatic extraction. This study compared the effects of plain and controlled-ileal-release (CIR) formulations of budesonide on intestinal inflammation. Methods: Ileitis was induced in hamsters by an intraluminal injection of trinitrobenzene sulphonic acid. Inflammation was assessed histologically and by measuring mastocytosis and myeloperoxidase activity. Adrenal-pituitary axis suppression was assessed by radioimmunoassay of plasma cortisol. Animals received budesonide (200 or 800 mu g/kg/day), CIR budesonide (200 mu g/kg/day), or placebo. Results: Plain budesonide (200 mu g/kg/day) did not reduce intestinal inflammation despite significantly lowered plasma cortisol levels. Plain budesonide (800 mu g/kg/day), on the other hand, significantly reduced intestinal inflammation but further decreased plasma cortisol levels. CIR budesonide (200 mu g/kg/day) was as effective in reducing inflammation as plain budesonide (800 mu g/kg/day). Conclusions: CIR budesonide was significantly more effective in reducing intestinal inflammation than plain budesonide. These results suggest that the site of delivery influences the effectiveness of budesonide and that local (topical) rather than systemic action of this compound is primarily responsible for its anti-inflammatory effect.

引用

页码：974 / 981

页数：8

共 15 条

[1] BOYD AJ, 1993, GASTROENTEROLOGY, V104, pA1030
[2] BRATTSAND R, 1990, CAN J GASTROENTEROL, V4, P241
[3] A STEROID ENEMA, BUDESONIDE, LACKING SYSTEMIC EFFECTS FOR THE TREATMENT OF DISTAL ULCERATIVE-COLITIS OR PROCTITIS
DANIELSSON, A
LOFBERG, R
PERSSON, T
SALDE, L
SCHIOLER, R
SUHR, O
WILLEN, R
[J]. SCANDINAVIAN JOURNAL OF GASTROENTEROLOGY, 1992, 27 (01) : 9 - 12
[4] DVORAK AM, 1983, PATHOL ANNU, V18, P181
[5] ORAL BUDESONIDE FOR ACTIVE CROHNS-DISEASE
GREENBERG, GR
FEAGAN, BG
MARTIN, F
SUTHERLAND, LR
THOMSON, ABR
WILLIAMS, CR
NILSSON, LG
PERSSON, T
BAIN, V
CHERRY, R
FEDORAK, R
LALOR, E
SHERBANIUK, R
YACYSHYN, B
KIERDEKIS, P
BAILEY, R
MEYER, D
FREEMAN, H
DAWS, P
HOLLAND, S
BUYTENDORP, M
WHITTAKER, S
CHANG, A
SUTHERLAND, L
HERSHFIELD, N
MACCANNELL, K
MEDDING, J
PRICE, L
SHAFFER, E
RACICOT, N
BASS, S
BRIDGES, R
BLUSTEIN, P
LAY, T
VANROSENDAAL, G
WATSON, M
WILLIAMS, CN
VANZANTEN, V
LEDDIN, D
FALKENHAM, J
TANTON, R
HUMAN, P
TURNBALL, G
SCHEP, G
WOOLNOUGH, J
DALLAIRE, C
ROSSEAU, B
BERNARD, F
DUBE, R
PARE, P
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1994, 331 (13) : 836 - 841
[6] IMMUNOSUPPRESSIVE DRUGS IN INFLAMMATORY BOWEL-DISEASE - A REVIEW OF THEIR MECHANISMS OF EFFICACY AND PLACE IN THERAPY
HAWTHORNE, AB
HAWKEY, CJ
[J]. DRUGS, 1989, 38 (02) : 267 - 288
[7] DEPLETION OF MUCOSAL MAST-CELL PROTEASE BY CORTICOSTEROIDS - EFFECT ON INTESTINAL ANAPHYLAXIS IN THE RAT
KING, SJ
MILLER, HRP
NEWLANDS, GFJ
WOODBURY, RG
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1985, 82 (04) : 1214 - 1218
[8] THE JEJUNAL SECRETION OF HISTAMINE IS INCREASED IN ACTIVE CROHNS-DISEASE
KNUTSON, L
AHRENSTEDT, O
ODLIND, B
HALLGREN, R
[J]. GASTROENTEROLOGY, 1990, 98 (04) : 849 - 854
[9] LENNARDJONES JE, 1983, INFLAMMATORY BOWEL D
[10] LOFBERG R, 1993, ALIMENT PHARM THERAP, V7, P611

← 1 2 →