X-ray structure of antistasin at 1.9 A resolution and its modelled complex with blood coagulation factor Xa.

نویسندگان

  • R Lapatto
  • U Krengel
  • H A Schreuder
  • A Arkema
  • B de Boer
  • K H Kalk
  • W G Hol
  • P D Grootenhuis
  • J W Mulders
  • R Dijkema
  • H J Theunissen
  • B W Dijkstra
چکیده

The three-dimensional structure of antistasin, a potent inhibitor of blood coagulation factor Xa, from the Mexican leech Haementeria officinalis was determined at 1.9 A resolution by X-ray crystallography. The structure reveals a novel protein fold composed of two homologous domains, each resembling the structure of hirustasin, a related 55-residue protease inhibitor. However, hirustasin has a different overall shape than the individual antistasin domains, it contains four rather than two beta-strands, and does not inhibit factor Xa. The two antistasin domains can be subdivided into two similarly sized subdomains with different relative orientations. Consequently, the domain shapes are different, the N-terminal domain being wedge-shaped and the C-terminal domain flat. Docking studies suggest that differences in domain shape enable the N-terminal, but not C-terminal, domain of antistasin to bind and inhibit factor Xa, even though both have a very similar reactive site. Furthermore, a putative exosite binding region could be defined in the N-terminal domain of antistasin, comprising residues 15-17, which is likely to interact with a cluster of positively charged residues on the factor Xa surface (Arg222/Lys223/Lys224). This exosite binding region explains the specificity and inhibitory potency of antistasin towards factor Xa. In the C-terminal domain of antistasin, these exosite interactions are prevented due to the different overall shape of this domain.

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عنوان ژورنال:
  • The EMBO journal

دوره 16 17  شماره 

صفحات  -

تاریخ انتشار 1997