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PDBsum entry 1f0r
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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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Crystal structures of human factor xa complexed with potent inhibitors.
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Authors
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S.Maignan,
J.P.Guilloteau,
S.Pouzieux,
Y.M.Choi-Sledeski,
M.R.Becker,
S.I.Klein,
W.R.Ewing,
H.W.Pauls,
A.P.Spada,
V.Mikol.
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Ref.
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J Med Chem, 2000,
43,
3226-3232.
[DOI no: ]
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PubMed id
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Abstract
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Involved in the coagulation cascade, factor Xa (FXa) is a serine protease which
has received great interest as a potential target for the development of new
antithrombotics. Although there is a great wealth of structural data on thrombin
complexes, few structures of ligand/FXa complexes have been reported, presumably
because of the difficulty in growing crystals. Reproducible crystallization
conditions for human des-Gla1-45 coagulation FXa have been found. This has led
to an improvement in the diffraction quality of the crystals (about 2.1 A) when
compared to the previously reported forms (2.3-2.8 A) thus providing a suitable
platform for a structure-based drug design approach. A series of crystal
structures of noncovalent inhibitors complexed with FXa have been determined,
three of which are presented herein. These include compounds containing the
benzamidine moiety and surrogates of the basic group. The benzamidine-containing
compound binds in a canonical fashion typical of synthetic serine protease
inhibitors. On the contrary, molecules that contain surrogates of the
benzamidine group do not make direct hydrogen-bonding interactions with the
carboxylate of Asp189 at the bottom of the S1 pocket. The structural data
provide a likely explanation for the specificity of these inhibitors and a great
aid in the design of bioavailable potent FXa inhibitors.
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