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Anti-arthritic activity of hydroxamic acid-based pseudopeptide inhibitors of matrix metalloproteinases and TNF alpha processing

被引:38
作者
DiMartino, M
Wolff, C
High, W
Stroup, G
Hoffman, S
Laydon, J
Lee, JC
Bertolini, D
Galloway, WA
Crimmin, MJ
Davis, M
Davies, S
机构
[1] SMITHKLINE BEECHAM PHARMACEUT,KING OF PRUSSIA,PA 19406
[2] MILES INC,W HAVEN,CT 06516
[3] BRITISH BIOTECH PHARMACEUT LTD,OXFORD OX4 5LY,ENGLAND
来源
INFLAMMATION RESEARCH | 1997年 / 46卷 / 06期
关键词
metalloproteinases; arthritis; TNF alpha;
D O I
10.1007/s000110050175
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Objective and Design: The effects of two hydroxamate inhibitors of metalloproteinase and tumor necrosis factor alpha (TNF alpha) processing on endotoxin-induced plasma TNF alpha and arthritic lesions in adjuvant-induced arthritic (AA) rats were determined. Material and Treatment: BB-1101 and BE-1433 were administered orally twice daily to AA Lewis rats with an established disease (days 13 to 22). AA rats (day 16) or normal rats were injected with bacterial endotoxin and plasma levels of TNF alpha were also determined. Methods: Hindpaw swelling was measured plethysmogra phically. Bone degradation was determined by radiography and bone mineral densitometry. TNF alpha was quantified using a sandwich ELISA. Results: The hydroxamic-acid pseudopeptides inhibited plasma TNF alpha levels in vivo and significantly reduced swelling and bone degradation of the tibiotarsal joints of AA rats in the range of 10-50 mg/kg given orally (p < 0.01 by Student's t-test). Conclusions: Thus, these novel compounds offer a new disease-modifying therapy for arthritis and the results also suggest that inhibition of TNF alpha production may contribute, at least in part, to their anti-arthritic activity.
引用
收藏
页码:211 / 215
页数:5
相关论文
共 15 条
[1]   MATRIX METALLOPROTEINASES - A REVIEW [J].
BIRKEDALHANSEN, H ;
MOORE, WGI ;
BODDEN, MK ;
WINDSOR, LJ ;
BIRKEDALHANSEN, B ;
DECARLO, A ;
ENGLER, JA .
CRITICAL REVIEWS IN ORAL BIOLOGY & MEDICINE, 1993, 4 (02) :197-250
[2]  
BRENNAN FM, 1992, BRIT J RHEUMATOL, V31, P293
[3]   PURIFICATION OF RABBIT BONE INHIBITOR OF COLLAGENASE [J].
CAWSTON, TE ;
GALLOWAY, WA ;
MERCER, E ;
MURPHY, G ;
REYNOLDS, JJ .
BIOCHEMICAL JOURNAL, 1981, 195 (01) :159-165
[4]   RAPID AND REPRODUCIBLE ASSAY FOR COLLAGENASE USING [ACETYLATED-1-C-14 COLLAGEN [J].
CAWSTON, TE ;
BARRETT, AJ .
ANALYTICAL BIOCHEMISTRY, 1979, 99 (02) :340-345
[5]   INHIBITION OF CARTILAGE AND BONE DESTRUCTION IN ADJUVANT ARTHRITIS IN THE RAT BY A MATRIX METALLOPROTEINASE INHIBITOR [J].
CONWAY, JG ;
WAKEFIELD, JA ;
BROWN, RH ;
MARRON, BE ;
SEKUT, L ;
STIMPSON, SA ;
MCELROY, A ;
MENIUS, JA ;
JEFFREYS, JJ ;
CLARK, RL ;
MCGEEHAN, GM ;
CONNOLLY, KM .
JOURNAL OF EXPERIMENTAL MEDICINE, 1995, 182 (02) :449-457
[6]  
DAVIES B, 1993, CANCER RES, V53, P2087
[7]   ADJUVANT ARTHRITIC (AA) RATS EXHIBIT ENHANCED ENDOTOXIN-INDUCED PLASMA TNF (EIPT) LEVELS [J].
DIMARTINO, M ;
SLIVJAK, M ;
ESSER, K ;
WOLFF, C ;
SMITH, E ;
GAGNON, R .
AGENTS AND ACTIONS, 1993, 39 :C58-C60
[8]   PRECLINICAL ANTIARTHRITIC ACTIVITY OF MATRIX METALLOPROTEINASE INHIBITORS [J].
DIMARTINO, MJ ;
HIGH, W ;
GALLOWAY, WA ;
CRIMMIN, MJ .
INHIBITION OF MATRIX METALLOPROTEINASES: THERAPEUTIC POTENTIAL, 1994, 732 :411-413
[9]   RANDOMIZED DOUBLE-BLIND COMPARISON OF CHIMERIC MONOCLONAL-ANTIBODY TO TUMOR-NECROSIS-FACTOR-ALPHA (CA2) VERSUS PLACEBO IN RHEUMATOID-ARTHRITIS [J].
ELLIOTT, MJ ;
MAINI, RN ;
FELDMANN, M ;
KALDEN, JR ;
ANTONI, C ;
SMOLEN, JS ;
LEEB, B ;
BREEDVELD, FC ;
MACFARLANE, JD ;
BIJL, H ;
WOODY, JN .
LANCET, 1994, 344 (8930) :1105-1110
[10]   PROCESSING OF TUMOR-NECROSIS-FACTOR-ALPHA PRECURSOR BY METALLOPROTEINASES [J].
GEARING, AJH ;
BECKETT, P ;
CHRISTODOULOU, M ;
CHURCHILL, M ;
CLEMENTS, J ;
DAVIDSON, AH ;
DRUMMOND, AH ;
GALLOWAY, WA ;
GILBERT, R ;
GORDON, JL ;
LEBER, TM ;
MANGAN, M ;
MILLER, K ;
NAYEE, P ;
OWEN, K ;
PATEL, S ;
THOMAS, W ;
WELLS, G ;
WOOD, LM ;
WOOLLEY, K .
NATURE, 1994, 370 (6490) :555-557
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