Abstract:Factor
XIIa (FXIIa) is a promising target for developing new drugs
that prevent thrombosis without causing bleeding complications. A
native cyclotide (MCoTI-II) is gaining interest for engineering FXIIa-targeted
anticoagulants as this peptide inhibits FXIIa but not other coagulation
proteases. Here, we engineered the native biosynthetic cyclization
loop of MCoTI-II (loop 6) to generate improved FXIIa inhibitors. Decreasing
the loop length led to gains in potency up to 7.7-fold, with the most
potent variant hav… Show more
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