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Intermolecular interactions and characterization of the novel factor Xa exosite involved in macromolecular recognition and inhibition: crystal structure of human Gla-domainless factor Xa complexed with the anticoagulant protein NAPc2 from the hematophagous nematode Ancylostoma caninum
Authors:Murakami M T  Rios-Steiner J  Weaver S E  Tulinsky A  Geiger J H  Arni R K
Affiliation:Department of Physics, IBILCE/UNESP, S?o José do Rio Preto, SP 15054-000, Brazil.
Abstract:NAPc2, an anticoagulant protein from the hematophagous nematode Ancylostoma caninum evaluated in phase-II/IIa clinical trials, inhibits the extrinsic blood coagulation pathway by a two step mechanism, initially interacting with the hitherto uncharacterized factor Xa exosite involved in macromolecular recognition and subsequently inhibiting factor VIIa (K(i)=8.4 pM) of the factor VIIa/tissue factor complex. NAPc2 is highly flexible, becoming partially ordered and undergoing significant structural changes in the C terminus upon binding to the factor Xa exosite. In the crystal structure of the ternary factor Xa/NAPc2/selectide complex, the binding interface consists of an intermolecular antiparallel beta-sheet formed by the segment of the polypeptide chain consisting of residues 74-80 of NAPc2 with the residues 86-93 of factor Xa that is additional maintained by contacts between the short helical segment (residues 67-73) and a turn (residues 26-29) of NAPc2 with the short C-terminal helix of factor Xa (residues 233-243). This exosite is physiologically highly relevant for the recognition and inhibition of factor X/Xa by macromolecular substrates and provides a structural motif for the development of a new class of inhibitors for the treatment of deep vein thrombosis and angioplasty.
Keywords:fXa, activated factor X   Gla, γ-carboxyglutamic acid   EGF, epidermal growth factor   NAPs, nematode anticoagulant proteins   fVIIa, activated factor VII   TAP, tick anticoagulant protein   TF, tissue factor   des-fXa, fXa less its γ-carboxyglumatic domain   r.m.s.d., root mean square deviations
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