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• W2754785305 abstract "Abstract The absence of an adequate reversal strategy to prevent and stop potential life-threatening bleeding complications is a major drawback to the clinical use of the direct oral inhibitors of blood coagulation factor Xa. Here we show that specific modifications of the substrate-binding aromatic S4 subpocket within the factor Xa active site disrupt high-affinity engagement of the direct factor Xa inhibitors. These modifications either entail amino-acid substitution of S4 subsite residues Tyr99 and/or Phe174 (chymotrypsinogen numbering), or extension of the 99-loop that borders the S4 subsite. The latter modifications led to the engineering of a factor Xa variant that is able to support coagulation in human plasma spiked with (supra-)physiological concentrations of direct factor Xa inhibitors. As such, this factor Xa variant has the potential to be employed to bypass the direct factor Xa inhibitor-mediated anticoagulation in patients that require restoration of blood coagulation." @default.
• W2754785305 created "2017-09-25" @default.
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• W2754785305 date "2017-09-13" @default.
• W2754785305 modified "2023-09-27" @default.
• W2754785305 title "Engineered factor Xa variants retain procoagulant activity independent of direct factor Xa inhibitors" @default.
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• W2754785305 doi "https://doi.org/10.1038/s41467-017-00647-9" @default.
• W2754785305 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/5597622" @default.
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• W2754785305 hasPublicationYear "2017" @default.
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