Figure 2
Figure 2. Thrombocytopenia was not detected in FcRn-deficient neonates delivered from immunized female β3−/−FcRn−/− mice bred with β3+/+FcRn−/− males. (A) Anti-β3 integrin antibodies were generated in β3−/−FcRn−/− mice after 2 immunizations with β3+/+FcRn−/− platelets. Antibodies were detected after immunization (black line), during pregnancy (gray line), and immediately after delivery (dotted line). This figure is representative of at least 3 individual experiments. (B) Thrombocytopenia was not detected in heterozygous pups delivered from immunized β3−/−FcRn−/− mothers (transfused twice with β3+/+FcRn−/− platelets) bred with β3+/+FcRn−/− males. FNIT was induced in pups delivered from mothers immunized twice with β3−/−FcRn+/+ platelets and bred with β3+/+FcRn+/+ males. Pups delivered from naive β3−/−FcRn+/+ female mice bred with male β3+/+FcRn+/+ mice were used as controls. n = 8-21 for each group. (C) Circulating anti-β3 integrin and platelet-associated IgG were undetectable in β3−/+FcRn−/− pups delivered from immunized β3−/−FcRn−/− mothers, but detected in β3−/+FcRn+/+ pups delivered from immunized β3−/−FcRn+/+ mothers. (D) Various IgG isotypes only crossed the FcRn-positive placenta. Mouse anti–mouse β3 integrin mAbs (50 μg; isotypes: JAN DI/IgG1, PSI EI/IgG2b, and DEC AI/IgG3) were injected intraperitoneally into pregnant β3−/−FcRn+/+ and β3−/−FcRn−/− mice, respectively. After delivery, sera from pups were incubated with β3+/+ platelets at a 1:5 dilution and stained with goat anti–mouse FITC-conjugated IgG1, IgG2b, and IgG3. n = 6-14 for each group.

Thrombocytopenia was not detected in FcRn-deficient neonates delivered from immunized female β3−/−FcRn−/− mice bred with β3+/+FcRn−/− males. (A) Anti-β3 integrin antibodies were generated in β3−/−FcRn−/− mice after 2 immunizations with β3+/+FcRn−/− platelets. Antibodies were detected after immunization (black line), during pregnancy (gray line), and immediately after delivery (dotted line). This figure is representative of at least 3 individual experiments. (B) Thrombocytopenia was not detected in heterozygous pups delivered from immunized β3−/−FcRn−/− mothers (transfused twice with β3+/+FcRn−/− platelets) bred with β3+/+FcRn−/− males. FNIT was induced in pups delivered from mothers immunized twice with β3−/−FcRn+/+ platelets and bred with β3+/+FcRn+/+ males. Pups delivered from naive β3−/−FcRn+/+ female mice bred with male β3+/+FcRn+/+ mice were used as controls. n = 8-21 for each group. (C) Circulating anti-β3 integrin and platelet-associated IgG were undetectable in β3−/+FcRn−/− pups delivered from immunized β3−/−FcRn−/− mothers, but detected in β3−/+FcRn+/+ pups delivered from immunized β3−/−FcRn+/+ mothers. (D) Various IgG isotypes only crossed the FcRn-positive placenta. Mouse anti–mouse β3 integrin mAbs (50 μg; isotypes: JAN DI/IgG1, PSI EI/IgG2b, and DEC AI/IgG3) were injected intraperitoneally into pregnant β3−/−FcRn+/+ and β3−/−FcRn−/− mice, respectively. After delivery, sera from pups were incubated with β3+/+ platelets at a 1:5 dilution and stained with goat anti–mouse FITC-conjugated IgG1, IgG2b, and IgG3. n = 6-14 for each group.

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