Figure 6.
Figure 6. Disease phenotype in FH W1206R mutant mice is mediated by AP complement. (A) FHR/R mice with C3 or FD deficiency survived normally, whereas their FHR/R littermates with normal C3 and FD had high mortality (FHR/RC3−/− n = 64, FHR/RC3+/+ n = 38, FHR/RFD−/− n = 60, and FHR/RFD+/+ n = 36). (B) BUN of FHR/R mice (n = 10) was significantly increased between 5 and 10 weeks of age, whereas BUN in FHR/RC3−/− (n = 6) and FHR/RFD−/− (n = 7) mice remained the same at 5 and 10 weeks of age. (C) CBC analysis showed that FHR/RC3−/− (n = 9) and FHR/RFD−/− (n = 9) mice had normal blood platelet counts and Hb levels, whereas their FHR/R littermates (n = 13) had thrombocytopenia and anemia compared with FHW/W mice (n = 13). (D) Representative pictures of kidney (PAS staining) and liver (hematoxylin and eosin staining) histology, retinal funduscopy, and fluorescence angiography showing that there was no glomerular injury in the kidney or thrombosis in the liver and eye of FHR/RC3−/− and FHR/RFD−/− mice and no retinopathy. Scale bars in panel D represent 25 μm (kidney), 50 μm (liver), and 200 μm (eye). Data in panel B represent mean ± SD. Horizontal bars across scatterplots in panel C represent average values. *P < .05; **P < .01; and ***P < .001 (Mantel-Haenszel log-rank test for panel A; 1-way ANOVA and Student t test for other panels).

Disease phenotype in FH W1206R mutant mice is mediated by AP complement. (A) FHR/R mice with C3 or FD deficiency survived normally, whereas their FHR/R littermates with normal C3 and FD had high mortality (FHR/RC3−/− n = 64, FHR/RC3+/+ n = 38, FHR/RFD−/− n = 60, and FHR/RFD+/+ n = 36). (B) BUN of FHR/R mice (n = 10) was significantly increased between 5 and 10 weeks of age, whereas BUN in FHR/RC3−/− (n = 6) and FHR/RFD−/− (n = 7) mice remained the same at 5 and 10 weeks of age. (C) CBC analysis showed that FHR/RC3−/− (n = 9) and FHR/RFD−/− (n = 9) mice had normal blood platelet counts and Hb levels, whereas their FHR/R littermates (n = 13) had thrombocytopenia and anemia compared with FHW/W mice (n = 13). (D) Representative pictures of kidney (PAS staining) and liver (hematoxylin and eosin staining) histology, retinal funduscopy, and fluorescence angiography showing that there was no glomerular injury in the kidney or thrombosis in the liver and eye of FHR/RC3−/− and FHR/RFD−/− mice and no retinopathy. Scale bars in panel D represent 25 μm (kidney), 50 μm (liver), and 200 μm (eye). Data in panel B represent mean ± SD. Horizontal bars across scatterplots in panel C represent average values. *P < .05; **P < .01; and ***P < .001 (Mantel-Haenszel log-rank test for panel A; 1-way ANOVA and Student t test for other panels).

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