![In vitro and in vivo effects of an anti-human VWFA1 monoclonal antibody in the H1HA mouse strain. (A) Response to ristocetin (1.5 mg/mL) in PRP from 4 mouse strains; platelet aggregation is evident only in H1HA mice. (B) Dose-response of H1HA PRP to the indicated ristocetin concentrations. (C) The anti-human VWFA1 monoclonal antibody NMC-4 (5 μg/mL; 1 minute incubation), but not 5 μg/mL of nonimmune control immunoglobulin G (IgG), completely blocked ristocetin-induced platelet aggregation in H1HA mouse PRP. (D) Treatment of H1HA mice with NMC-4 (0.8 mg/kg injected IV 7 minutes before the start of the test procedure [n = 6]) prolonged the tail bleeding time to >10 minutes as compared with <3 minutes in mice treated with control IgG (n = 6). (E) The same dose of NMC-4 prevented carotid artery occlusion in H1HA mice after a 9% FeCl3–induced lesion (n = 10 for both treated and control mice). (A-C) Platelet aggregation is shown as a time-dependent increase in light transmittance through PRP. (D-E) Individual data are shown with median and interquartile range. Statistical analysis was performed with the Mann-Whitney nonparametric U test. **P < .01; ***P < .001.](https://ash.silverchair-cdn.com/ash/content_public/journal/bloodadvances/2/19/10.1182_bloodadvances.2018023507/7/advances023507f5.png?Expires=1720282597&Signature=Bm1jzcAyrAq8cc7kGZQM3PHuKntKuW4xh-gAqiCnfoA3uW7Mkd0tlKBAZ0A4q1djbmoxiFBm0lXoiP0yDehiQ6MRJIdPBZcJ1Ni6DmAC593NLndiVkR3r7~k3UtmCn9UH96R2eueaQxExBD0uWzQ63U2-MAe6BU-5tOZFiHcMV71XE7B1~tKz5UihvFM7xzeitcPTDX5q3y3biDvBoTvr9zggyUFzhY2~IuviSwmWKblykiI5mtSKrAK6MyvvoM8y7ERdWfJK-~jWRe4T-7~qFniDvhldKNoOaexLV4KHCp4y~RPqB3HV00TRP0cGpxdepZugZUvMtuhFebih~nujg__&Key-Pair-Id=APKAIE5G5CRDK6RD3PGA)
In vitro and in vivo effects of an anti-human VWFA1 monoclonal antibody in the H1HA mouse strain. (A) Response to ristocetin (1.5 mg/mL) in PRP from 4 mouse strains; platelet aggregation is evident only in H1HA mice. (B) Dose-response of H1HA PRP to the indicated ristocetin concentrations. (C) The anti-human VWFA1 monoclonal antibody NMC-4 (5 μg/mL; 1 minute incubation), but not 5 μg/mL of nonimmune control immunoglobulin G (IgG), completely blocked ristocetin-induced platelet aggregation in H1HA mouse PRP. (D) Treatment of H1HA mice with NMC-4 (0.8 mg/kg injected IV 7 minutes before the start of the test procedure [n = 6]) prolonged the tail bleeding time to >10 minutes as compared with <3 minutes in mice treated with control IgG (n = 6). (E) The same dose of NMC-4 prevented carotid artery occlusion in H1HA mice after a 9% FeCl3–induced lesion (n = 10 for both treated and control mice). (A-C) Platelet aggregation is shown as a time-dependent increase in light transmittance through PRP. (D-E) Individual data are shown with median and interquartile range. Statistical analysis was performed with the Mann-Whitney nonparametric U test. **P < .01; ***P < .001.