Development of orally bioavailable bicyclic pyrazolones as inhibitors of tumor necrosis factor-α production

Michael Philip Clark,Steven K. Laughlin,Matthew J. Laufersweiler,Roger Gunnard Bookland,Todd A. Brugel,Adam Golebiowski,Mark Sabat,Jennifer A. Townes,John C. VanRens,Jane Far-Jine Djung,Michael G. Natchus,Biswanath De,Lily C. Hsieh,Susan C. Xu,Rick L. Walter,Marlene Mekel,S. A. Heitmeyer,Kimberly K. Brown,Karen Juergens,Yetunde Olabisi Taiwo,Michael J. Janusz

Development of orally bioavailable bicyclic pyrazolones as inhibitors of tumor necrosis factor-α production

2004

2-Aryl-3-pyrimidinyl based tumor necrosis factor-α (TNF-α) inhibitors, which contain a novel bicyclic pyrazolone core, are described. Many showed low-nanomolar activity against lipopolysaccharide-induced TNF-α production in monocytic cells. Secondary screening data are presented for the pyrimidinyl bicyclic pyrazolones. Several of these analogues showed good oral bioavailability in rat and efficacy in the rat iodoacetate in vivo model.

Keywords:

Pyrazolones
Tumor necrosis factor alpha
Pyrazolone
Bicyclic molecule
Cytokine
Biochemistry
Organic chemistry
In vivo
In vitro
Enzyme inhibitor
Chemistry

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