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PDBsum entry 1cx2
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Oxidoreductase
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PDB id
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1cx2
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Contents |
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* Residue conservation analysis
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References listed in PDB file
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Key reference
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Title
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Structural basis for selective inhibition of cyclooxygenase-2 by anti-Inflammatory agents.
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Authors
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R.G.Kurumbail,
A.M.Stevens,
J.K.Gierse,
J.J.Mcdonald,
R.A.Stegeman,
J.Y.Pak,
D.Gildehaus,
J.M.Miyashiro,
T.D.Penning,
K.Seibert,
P.C.Isakson,
W.C.Stallings.
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Ref.
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Nature, 1996,
384,
644-648.
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PubMed id
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Abstract
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Prostaglandins and glucocorticoids are potent mediators of inflammation.
Non-steroidal anti-inflammatory drugs (NSAIDs) exert their effects by inhibition
of prostaglandin production. The pharmacological target of NSAIDs is
cyclooxygenase (COX, also known as PGH synthase), which catalyses the first
committed step in arachidonic-acid metabolism. Two isoforms of the membrane
protein COX are known: COX-1, which is constitutively expressed in most tissues,
is responsible for the physiological production of prostaglandins; and COX-2,
which is induced by cytokines, mitogens and endotoxins in inflammatory cells, is
responsible for the elevated production of prostaglandins during inflammation.
The structure of ovine COX-1 complexed with several NSAIDs has been determined.
Here we report the structures of unliganded murine COX-2 and complexes with
flurbiprofen, indomethacin and SC-558, a selective COX-2 inhibitor, determined
at 3.0 to 2.5 A resolution. These structures explain the structural basis for
the selective inhibition of COX-2, and demonstrate some of the conformational
changes associated with time-dependent inhibition.
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Secondary reference #1
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Title
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Erratum. Structural basis for selective inhibition of cyclooxygenase-2 by anti-Inflammatory agents
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Authors
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R.G.Kurumbail,
A.M.Stevens,
J.K.Gierse,
J.J.Mcdonald,
R.A.Stegeman,
J.Y.Pak,
D.Gildehaus,
J.M.Miyashiro,
T.D.Penning,
K.Seibert.
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Ref.
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nature, 1997,
385,
555.
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