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Alexander Weidemann, Yann M. Kerdiles, Karl X. Knaup, Christopher A. Rafie, Adam T. Boutin, Christian Stockmann, Norihiko Takeda, Miriam Scadeng, Andy Y. Shih, Volker H. Haase, M. Celeste Simon, David Kleinfeld, Randall S. Johnson
Published in Volume 119, Issue 11
J Clin Invest. 2009; 119(11):3373–3383 doi:10.1172/JCI39378
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Figure 2
Knockout of VHL in astrocytes reduces survival, induces hydrocephalus, and leads to severe erythrocytosis in mice.

(A) The weight of 6-week-old GFAPCre+/VHL+f/+f animals (n = 8) is significantly less than that of control (GFAPCre–; n = 23), GFAPCre+/HIF-1α+f/+f (n = 9), and GFAPCre+/HIF-2α+f/+f (n = 8) animals. Data represent median and interquartile ranges. (B) Survival is significantly reduced to 18.4 weeks in GFAPCre+/VHL+f/+f (n = 45) compared with control animals (GFAPCre–; n = 46). It is normal in GFAPCre+/HIF-1α+f/+f (n = 25) and in GFAPCre+/HIF-2α+f/+f mice (n = 57). Data represent median survival (weeks). (C) GFAPCre+/VHL+f/+f mice (lower panel) develop severe hydrocephaly (representative T2 weighed fMRI photographs; cerebrospinal fluid appears white). (D) Hematocrits at the age of 10 weeks are not different in control (GFAPCre–; n = 19), GFAPCre+/HIF-1α+f/+f (n = 10), and GFAPCre+/HIF-2α+f/+f animals (n = 8). In contrast, GFAPCre+/VHL+f/+f mice (n = 7) exhibit a striking elevation of the hematocrit. (E) Plasma EPO levels in GFAPCre+/VHL+f/+f animals (n = 12) are significantly increased compared with those in control mice (GFAPCre–; n = 34). No difference from WT plasma EPO levels is detected in GFAPCre+/HIF-1α+f/+f (n = 10) and GFAPCre+/HIF-2α+f/+f mice (n = 6). Data represent mean + SEM. (F) Red blood cell count (upper panel) and hemoglobin concentration (lower panel) are both significantly higher in GFAPCre+/VHL+f/+f (n = 6) than in control animals (GFAPCre–; n = 5), which indicates pathological erythrocytosis. Data represent mean + SEM.