(A) Survival of GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f animals (n = 55) is reduced compared with GFAPCre+/VHL^+f/+f mice (n = 45). GFAPCre+/VHL^+f/+f/HIF-2α^+f/+f mice (n = 59) have a normal life span. Data represent mean survival (weeks). (B) At 12 weeks, hematocrits of both GFAPCre+/VHL^+f/+f (n = 7) and GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f mice (n = 11) are significantly elevated (GFAPCre–; n = 20). GFAPCre+/VHL^+f/+f/HIF-2α^+f/+f mice (n = 9) have a normal hematocrit. Data represent mean. (C) Hematocrit development: increased hematocrit in GFAPCre+/VHL^+f/+f mice from the age of 4 weeks and from 3 weeks in GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f mutants compared with WT. Hematocrits of GFAPCre+/VHL^+f/+f/HIF-2α^+f/+f animals are not changed (n > 3 for all genotypes and time points). Data represent mean α SEM. *P < 0.05 vs. WT; ^#P < 0.05 vs. GFAPCre+/VHL^+f/+f. (D) GFAPCre+/VHL^+f/+f (n = 12) and GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f mice (n = 6) have significantly higher plasma EPO concentrations compared with controls (GFAPCre–; n = 30). Plasma EPO levels in GFAPCre+/VHL^+f/+f/HIF-2α^+f/+f animals (n = 9) are not elevated. (E) EPO mRNA is upregulated in brains of GFAPCre+/VHL^+f/+f (n = 10) and GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f mice (n = 6) compared with controls (GFAPCre–; n = 9). (F) Kidney EPO mRNA is suppressed in GFAPCre+/VHL^+f/+f animals (n = 8) relative to controls (GFAPCre–; n = 12) and is not detectable in 4 of 5 kidneys of GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f mice. In kidneys of GFAPCre+/VHL^+f/+f/HIF-2α^+f/+f mice (n = 6), kidney EPO mRNA expression is normal. (G) Hepatic EPO mRNA expression in GFAPCre+/VHL^+f/+f (n = 5) and GFAPCre+/VHL^+f/+f/HIF-2α^+f/+f mice (n = 5) and controls (GFAPCre–; n = 14) does not differ, but is higher in GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f animals (n = 5). Rel, relative. (D–G) Data represent mean + SEM, Mann-Whitney U test. (H) No HIF-α activation in livers of GFAPCre+/VHL^+f/+f/HIF-1α^+f/+f animals. Representative photograph. Scale bars: 100 μm.