Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:3.4.21.6 (
thromboplastin
)
13,278
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
We have previously shown that residues Tyr-253 and Glu-255 in the serpin antithrombin function as exosites to promote the inhibition of
factor Xa
and factor IXa when the serpin is conformationally activated by heparin. Here we show that functional exosites can be engineered at homologous positions in a P1 Arg variant of the serpin alpha1-proteinase inhibitor (alpha1PI) that does not require heparin for activation. The combined effect of the two exosites increased the association rate constant for the reactions of alpha1PI with factors Xa and IXa 11-14-fold, comparable with their rate-enhancing effects on the reactions of heparin-activated antithrombin with these proteases. The effects of the engineered exosites were specific, alpha1PI inhibitor reactions with trypsin and thrombin being unaffected. Mutation of Arg-150 in
factor Xa
, which interacts with the exosite residues in heparin-activated antithrombin, abrogated the ability of the engineered exosites in alpha1PI to promote
factor Xa
inhibition. Binding studies showed that the exosites enhance the Michaelis complex interaction of alpha1PI with S195A
factor Xa
as they do with the heparin-activated antithrombin interaction. Replacement of the P4-P2
AIP
reactive loop residues in the alpha1PI exosite variant with a preferred IEG substrate sequence for
factor Xa
modestly enhanced the reactivity of the exosite mutant inhibitor with
factor Xa
by approximately 2-fold but greatly increased the selectivity of alpha1PI for inhibiting
factor Xa
over thrombin by approximately 1000-fold. Together, these results show that a specific and selective inhibitor of
factor Xa
can be engineered by incorporating
factor Xa
exosite and reactive site recognition determinants in a serpin.
...
PMID:Engineering functional antithrombin exosites in alpha1-proteinase inhibitor that specifically promote the inhibition of factor Xa and factor IXa. 1901 Jul 76
