Figure 6.
Efficacy of BIVV001 in HemA mice. (A,B) Acute hemostatic efficacies of BIVV001 (37.5, 75, and 150 IU/kg; all IV and n = 14 for each dose), equivalent doses of rFVIII (n = 14 for each dose), and vehicle (n = 14) were evaluated in HemA mice in an acute-blood-loss, tail-clip model. C57BL/6 mice (n = 15) served as the positive control. (A) Individual median blood loss over 30 minutes was quantified gravimetrically and compared between groups with the Kolmogorov-Smirnov t test. Horizontal bars are medians. (B) The state of being “protected” was granted if blood loss was less than or equal to the mean volume of blood lost by C57BL/6 mice in the tail-clip model. The ED50 was the dose of each treatment that achieved protection from acute bleeding in 50% of treated animals. ED50 values were 81 IU/kg for BIVV001 and 105 IU/kg for rFVIII. (C) The effect of prophylactic single-dose BIVV001 (1.2-120 IU/kg; IV), equivalent doses of rFVIII, and vehicle on 24-hour survival rates of HemA mice (n = 15-20 per dose group) after tail vein transection were assessed. BIVV001 and rFVIII were administered at 96 and 24 hours, respectively, before tail vein transection. (D) Twenty-four-hour survival rates after BIVV001 and rFVIII administration were compared with those obtained with vehicle (log-rank Mantel-Cox test). FVIII led to significantly higher survival rates at 24 hours after TVT (P < .05) compared with vehicle. Direct survival comparison showed no significant difference between BIVV001 and rFVIII, indicating that BIVV001 is comparable to rFVIII; n = 15 to 20 mice per group. Similar survival protection ED50 values for BIVV001 and rFVIII were calculated by the nonlinear fit equation.

Efficacy of BIVV001 in HemA mice. (A,B) Acute hemostatic efficacies of BIVV001 (37.5, 75, and 150 IU/kg; all IV and n = 14 for each dose), equivalent doses of rFVIII (n = 14 for each dose), and vehicle (n = 14) were evaluated in HemA mice in an acute-blood-loss, tail-clip model. C57BL/6 mice (n = 15) served as the positive control. (A) Individual median blood loss over 30 minutes was quantified gravimetrically and compared between groups with the Kolmogorov-Smirnov t test. Horizontal bars are medians. (B) The state of being “protected” was granted if blood loss was less than or equal to the mean volume of blood lost by C57BL/6 mice in the tail-clip model. The ED50 was the dose of each treatment that achieved protection from acute bleeding in 50% of treated animals. ED50 values were 81 IU/kg for BIVV001 and 105 IU/kg for rFVIII. (C) The effect of prophylactic single-dose BIVV001 (1.2-120 IU/kg; IV), equivalent doses of rFVIII, and vehicle on 24-hour survival rates of HemA mice (n = 15-20 per dose group) after tail vein transection were assessed. BIVV001 and rFVIII were administered at 96 and 24 hours, respectively, before tail vein transection. (D) Twenty-four-hour survival rates after BIVV001 and rFVIII administration were compared with those obtained with vehicle (log-rank Mantel-Cox test). FVIII led to significantly higher survival rates at 24 hours after TVT (P < .05) compared with vehicle. Direct survival comparison showed no significant difference between BIVV001 and rFVIII, indicating that BIVV001 is comparable to rFVIII; n = 15 to 20 mice per group. Similar survival protection ED50 values for BIVV001 and rFVIII were calculated by the nonlinear fit equation.

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