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Hyun-Woo Jeong, Un Sil Jeon, Bon-Kyoung Koo, Wan-Young Kim, Sun-Kyoung Im, Juhee Shin, Yunje Cho, Jin Kim, Young-Yun Kong
Published in Volume 119, Issue 11
J Clin Invest. 2009; 119(11):3290–3300 doi:10.1172/JCI38416
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Figure 2
Progressive hydronephrosis, urinary concentrating defect, and sodium-wasting phenotype of Hoxb7-CreMib1f/f mice.

(AH) Urinary systems (A, B, E, and F) and H&E staining of kidneys (C, D, G, and H) from Mib1f/f (A, C, E, and G) and Hoxb7-CreMib1f/f (B, D, F, and H) littermates at P0 (AD) or P17 (EH). Scale bars: 2 mm (A, B, E, and F); 300 μm (C and D); 1 mm (G and H). High-magnification images of glomeruli are shown in insets in G and H (scale bars: 40 μm). (I and J) Kidneys of 1-month-old (P30) Mib1f/f (I) and Hoxb7-CreMib1f/f (J) littermates. Scale bars: 2 mm. (K) Urine output for 24 hours of 7-week-old Mib1f/f control and Hoxb7-CreMib1f/f mice. Error bars represent mean ± SD. *P < 0.05. (L) Urine osmolality of 7-week-old Mib1f/f control and Hoxb7-CreMib1f/f mice. Error bars represent mean ± SD. *P < 0.05. (M) Three-hour water deprivation test of 7-week-old Mib1f/f control and Hoxb7-CreMib1f/f mice. F.W., free access to water; 3 hr. D., 3-hour dehydration. *P < 0.05 (paired t test). (N) Relative urinary excretion levels of indicated ions normalized to creatinine in 7-week-old Mib1f/f control and Hoxb7-CreMib1f/f mice. Error bars represent mean ± SD. *P < 0.05.