Jean A. Wakefield scite author profile

SummaryConsiderable evidence has associated the expression of matrix metalloproteinases (MMPs) with the degradation of cartilage and bone in chronic conditions such as arthritis. Direct evaluation of MMPs' role in vivo has awaited the development of MMP inhibitors with appropriate pharmacological properties. We have identified butanediamide, N4-hydroxy-2-(2-methylpropyl)-as a potent MMP inhibitor with sufficient solubility and stability to permit evaluation in an experimental model of chronic destructive arthritis (adjuvant-induced arthritis) in rats. In this model, pronounced acute and chronic synovial inflammation, distal tibia and metatarsal marrow hyperplasia associated with osteoclasia, severe bone and cartilage destruction, and ectopic new bone growth are well developed by 3 wk after adjuvant injection. Rats were injected with Freund's adjuvant on day 0. GI168 was was administered systemically from days 8 to 21 by osmotic minipumps implanted subcutaneously. GI168 at 6, 12, and 25 mg/kg per d reduced ankle swelling in a dose-related fashion. Radiologicai and histological ankle joint evaluation on day 22 revealed a profound dose related inhibition of bone and cartilage destruction in treated rats relative to rats receiving vehicle alone. A significant reduction in edema, pannus formation, periosteal new bone growth and the numbers of adherent marrow osteoclasts was also noted. However, no significant decrease in polymorphonuclear and mononuclear leukocyte infiltration of synovium and marrow hematopoietic cellularity was seen. This unique profile of antiarthritic activity indicates that GI168 is osteo-and chondro-protective, and it supports a direct role for MMP in cartilage and bone damage and pannus formation in adjuvant-induced arthritis.

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Synthesis and pharmacological characterization of a potent, orally active p38 kinase inhibitor

Dumas¹,

Hatoum‐Mokdad²,

Sibley³

et al. 2002

Bioorganic & Medicinal Chemistry Letters

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Effect of matrix metalloproteinase inhibitors on tumor growth and spontaneous metastasis

et al. 1996

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Four potent, synthetic inhibitors of matrix metalloproteinases (MMPs) were assessed as inhibitors of tumor growth and spontaneous metastasis to the lung. Mat Ly Lu rat prostate tumor, LOX human melanoma and M27 murine Lewis lung tumor were implanted subcutaneously (s.c.) in mice and allowed to grow for 3-12 days. The lungs of the tumor-bearing mice were then removed and implanted s.c. into untreated mice, and the outgrowth of secondary tumors from the implanted lungs measured. The incidence and rate of outgrowth of secondary tumors increased with the length of primary tumor growth, validating these measurements as indices of spontaneous metastasis to the lung. Compounds were tested by s.c. implantation of minipumps which delivered compound throughout the period of primary tumor growth and spontaneous metastasis to the lung at steady-state drug concentrations orders of magnitude greater than the concentrations needed to either inhibit collagenase, gelatinase or stromelysin in vitro. Inhibitor treatment slowed the growth of primary s.c. Mat Ly Lu and LOX tumors by 40-60% but had no significant effect on the growth of primary M27 tumors. Surprisingly, inhibitor treatment had no significant effect on the ability of the lung to generate secondary tumors when reimplanted s.c. in untreated mice. Because of the possible importance of cathepsins B, H and L in tumor growth and metastasis, the irreversible inhibitor E-64 was also infused by s.c. minipump. E-64 had no effect on the growth or spontaneous metastasis of Mat Ly Lu or M27 tumors.

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Utilization of 3H from deoxyuridine and thymidine for synthesis of DNA and other macromolecules in various organs of the rat

Hopkins

Wakefield

1977

Biochemical Pharmacology

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Sonography of Experimental Acute Renal Vein Occlusion

Paling

Wakefield

Watson

1985

J of Clinical Ultrasound

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Complete occlusion of the renal vein in five rabbits with the kidney in its normal position was followed by high‐resolution ultrasound. Early changes consisted of moderate renal enlargement and a diffuse increase in renal echogenicity with a fine echo pattern. On the average, renal length increased by only 13%. Delayed changes were a gradual reduction in renal echogenicity, falling to below baseline, with blurring of the corticomedullary boundary. Intrarenal hemorrhage alone occurred in only one kidney. Perirenal hematomata were seen in two other cases associated with localized intrarenal hemorrhage adjacent to the point of capsular rupture (overall renal morphology was preserved). The relative subtlety of the changes observed contrasts with previously reported data and is felt to preclude a specific diagnosis.

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A Comparative Study of the Response to Radiation by Experimental Tumors with Markedly Different Growth Characteristics

Kovacs¹,

Evans²,

Wakefield³

et al. 1977

Radiation Research

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The Sonographic Evaluation of Hydronephrosis with Progressive Ureteric Obstruction An Experimental Model

Paling¹,

Wakefield²,

Watson³

1985

Investigative Radiology

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Inhibition of cartilage and bone destruction in adjuvant arthritis in the rat by a matrix metalloproteinase inhibitor

Conway¹,

Wakefield²,

Brown³

et al. 1995

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Jean A. Wakefield

Inhibition of cartilage and bone destruction in adjuvant arthritis in the rat by a matrix metalloproteinase inhibitor.

Synthesis and pharmacological characterization of a potent, orally active p38 kinase inhibitor

Effect of matrix metalloproteinase inhibitors on tumor growth and spontaneous metastasis

Utilization of 3H from deoxyuridine and thymidine for synthesis of DNA and other macromolecules in various organs of the rat

Sonography of Experimental Acute Renal Vein Occlusion

A Comparative Study of the Response to Radiation by Experimental Tumors with Markedly Different Growth Characteristics

The Sonographic Evaluation of Hydronephrosis with Progressive Ureteric Obstruction An Experimental Model

Inhibition of cartilage and bone destruction in adjuvant arthritis in the rat by a matrix metalloproteinase inhibitor

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