Schematic representation of fV and fV short. (A) A1-A2-B-A3-C1-C2 domain organization of fV (2196 residues total) and details of the B domain containing the BR (⁹⁶³KPGKQSGHPKFPRVRHKSLQVRQDGGKSRLKKSQFLIKTRKKKKEK¹⁰⁰⁸) and AR (¹⁴⁹³DYIEIIPKEEVQSSEDDYAEIDYVPYDDPYKTDVRTNINSSRDPD¹⁵³⁷) that interact to keep fV in its inactive state.^1,5-9 The hydrophobic patch ¹⁴⁸¹PLVIVG¹⁴⁸⁶ is highlighted preceding the AR. The sites of thrombin activation (R709, R1018, R1545) and APC inactivation (R306, R506) are indicated. (B) A1-A2-B-A3-C1-C2 domain organization of the splice variant fV short carrying a deletion of 703 residues, from 756 through 1458, in the B domain (1493 residues total). The deletion removes the site of thrombin activation at R1018 and the entire BR, which unmasks the hydrophobic patch ¹⁴⁸¹PLVIVG¹⁴⁸⁶ and the AR region to promote TFPIα binding. The cryo-EM structure of fV short (Figure 2; supplemental Figure 3) reveals all residues of the A1-A2-A3-C1-C2 assembly. Reproduced with modifications,¹⁰ copyright Elsevier (2022).