Oral budesonide is as effective as oral prednisolone in active Crohn's disease

被引:260
作者
Campieri, M
Ferguson, A
Doe, W
Persson, T
Nilsson, LG
Malchow, H
Prantera, C
Mani, V
OMorain, C
Selby, W
Pallone, F
diPietralata, MM
Sjodahl, R
Florin, T
Smith, P
Bianchi, P
Lofberg, R
Rutgeerts, P
Smallwood, R
Lamers, HW
TasmanJones, C
Hunter, JO
Hodgson, H
Danielsson, A
Lee, FI
Piacitelli, G
Giovanni, S
Ellis, A
Weir, DG
机构
[1] UNIV EDINBURGH,DEPT MED,EDINBURGH EH8 9YL,MIDLOTHIAN,SCOTLAND
[2] AUSTRALIAN NATL UNIV,JOHN CURTIN SCH MED RES,DIV MOL MED,CANBERRA,ACT 2601,AUSTRALIA
[3] ASTRO DRACO AB,LUND,SWEDEN
[4] MED KLIN 2,LEVERKUSEN,GERMANY
[5] OSPEDALE NUOVO REGINA MARGHERITA,DEPT GASTROENTEROL,ROME,ITALY
[6] LEIGH INFIRM,LEIGH,ENGLAND
[7] MEATH HOSP,DUBLIN,IRELAND
[8] ROYAL PRINCE ALFRED MED CTR,NEWTOWN,TAS,AUSTRALIA
[9] CLIN MED POLICLIN 2,ROME,ITALY
[10] S EUGENIO HOSP,ROME,ITALY
[11] LINKOPING UNIV HOSP,S-58185 LINKOPING,SWEDEN
[12] MATER ADULT HOSP,BRISBANE,QLD,AUSTRALIA
[13] LLANDOUGH HOSP,PENARTH,S GLAM,WALES
[14] INST CLIN MED 1,MILAN,ITALY
[15] HUDDINGE HOSP,HUDDINGE,SWEDEN
[16] CATHOLIC UNIV LEUVEN,B-3000 LOUVAIN,BELGIUM
[17] REPATRIAT GEN HOSP,HEIDELBERG,VIC,AUSTRALIA
[18] UNIV LEIDEN HOSP,NL-2300 RC LEIDEN,NETHERLANDS
[19] UNIV AUCKLAND,SCH MED,AUCKLAND,NEW ZEALAND
[20] ADDENBROOKES HOSP,CAMBRIDGE,ENGLAND
[21] HAMMERSMITH HOSP,LONDON,ENGLAND
[22] UMEA UNIV HOSP,S-90185 UMEA,SWEDEN
[23] VICTORIA HOSP,BLACKPOOL,ENGLAND
[24] HOSP S GIOVANNI,ROME,ITALY
[25] BROADGREEN HOSP,LIVERPOOL L14 3LB,MERSEYSIDE,ENGLAND
[26] ST JAMES HOSP,DUBLIN 8,IRELAND
来源
GUT | 1997年 / 41卷 / 02期
关键词
adrenal function; CDAI; glucocorticoid; glucocorticoid associated side effects;
D O I
10.1136/gut.41.2.209
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Background-The use of corticosteroids in active Crohn's disease often becomes limited by side effects. Budesonide is a potent corticosteroid with low systemic bioavailability due to an extensive first pass liver metabolism. Aims-To compare the efficacy and safety of two dosage regimens of budesonide and prednisolone in patients with active Crohn's disease affecting the ileum and/or the ascending colon. Patients and methods-One hundred and seventy eight patients were randomised to receive budesonide controlled ileal release (CIR) capsules 9 mg once daily or 4.5 mg twice daily, or prednisolone tablets 40 mg once daily. The treatment period was 12 weeks. The primary efficacy variable was clinical remission, defined as a Crohn's Disease Activity Index (CDAI) of 150 or less. Results-After eight weeks of treatment, remission occurred in 60% of patients receiving budesonide once daily or prednisolone and in 42% of those receiving budesonide twice daily (p=0.062). The presence of glucocorticoid associated side effects was similar in all groups; however, moon face was more common in the prednisolone group (p=0.0005). The highest frequency of impaired adrenal function, as measured by a short ACTH test, was found in the prednisolone group (p=0.0023). Conclusions-Budesonide CIR, administered at 9 mg once daily or 4.5 mg twice daily, is comparable to prednisolone in inducing remission in active Crohn's disease. The single dose administration is as promptly effective as prednisolone and represents a simpler and safer therapeutic approach, with a considerable reduction in side effects.
引用
收藏
页码:209 / 214
页数:6
相关论文
共 21 条
[1]  
BEST WR, 1976, GASTROENTEROLOGY, V70, P439
[2]  
Brattsand R., 1990, Can J Gastroenterol, V4, P407
[3]   BUDESONIDE - AN UPDATED REVIEW OF ITS PHARMACOLOGICAL PROPERTIES, AND THERAPEUTIC EFFICACY IN ASTHMA AND RHINITIS [J].
BROGDEN, RN ;
MCTAVISH, D .
DRUGS, 1992, 44 (03) :375-407
[4]  
*DAN BUD STUD GROU, 1991, SCAND J GASTROENTERO, V26, P1225
[5]   BUDESONIDE CONTROLLED ILEAL RELEASE (CIR) CAPSULES AFFECT PLASMA-CORTISOL LESS-THAN PREDNISOLONE [J].
EDSBACKER, S ;
LARSSON, P ;
NILSSON, M ;
WIREN, JE .
GASTROENTEROLOGY, 1995, 108 (04) :A814-A814
[6]  
EDSBACKER S, 1993, GASTROENTEROLOGY, V104, pA695
[7]   GLUCOCORTICOSTEROID THERAPY - MECHANISMS OF ACTION AND CLINICAL CONSIDERATIONS [J].
FAUCI, AS ;
DALE, DC ;
BALOW, JE .
ANNALS OF INTERNAL MEDICINE, 1976, 84 (03) :304-315
[8]   ORAL BUDESONIDE FOR ACTIVE CROHNS-DISEASE [J].
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 .
NEW ENGLAND JOURNAL OF MEDICINE, 1994, 331 (13) :836-841
[9]   RISK-BENEFIT ASSESSMENT OF DRUGS USED IN THE TREATMENT OF INFLAMMATORY BOWEL-DISEASE [J].
HANAUER, SB ;
STATHOPOULOS, G .
DRUG SAFETY, 1991, 6 (03) :192-219
[10]  
LOFBERG R, 1993, ALIMENT PHARM THERAP, V7, P611
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