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Published ahead of print on February 13, 2008
Journal of the American Society of Nephrology
© 2008 American Society of Nephrology
doi: 10.1681/ASN.2006090983
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Received September 10, 2006
Accepted on November 6, 2007

BASIC RESEARCH

Bmp in Podocytes Is Essential for Normal Glomerular Capillary Formation

Hiroyuki Ueda *{dagger}1, Yoichi Miyazaki *, Taiji Matsusaka {ddagger}{sect}, Yasunori Utsunomiya *, Tetsuya Kawamura *, Tatsuo Hosoya *, and Iekuni Ichikawa {ddagger}{sect}

*Division of Kidney and Hypertension, Department of Internal Medicine, Jikei University School of Medicine, Tokyo, and {dagger}Department of Pediatrics, and {ddagger}Institute of Medical Science, Tokai University School of Medicine, Kanagawa, Japan; and {sect}Department of Pediatrics, Vanderbilt University School of Medicine, Nashville, Tennessee


1 To whom correspondence should be addressed. E-mail: hi-ro{at}jikei.ac.jp.


  Abstract

Bone morphogenetic protein (BMP) 4 exerts multiple biological effects on kidney and ureter development. To examine the role of BMP4 in glomerular morphogenesis, we generated transgenic mice with altered BMP4 function in podocytes by conferring tissue-specificity with the nephrin (Nphs1) promoter. At birth, Tg(Nphs1-Nog) mice, which had loss of BMP4 function in podocytes, were found to have glomerular microaneurysms, collapsed glomerular capillary tufts, enlarged Bowman’s capsules, and fewer normal proximal tubules. Conversely, Tg(Nphs1-Bmp4) mice, which had increased BMP4 function in podocytes, demonstrated defects in glomerular capillary formation, but podocytes were not appreciably affected. The Tg(Nphs1-Nog) and Tg(Nphs1-Bmp4) mice shared morphological characteristics with the previously reported podocyte-specific Vegf-A over-expressing and knockout mice, respectively. Consistent with the morphological similarity, in situ hybridization revealed an intense signal for podocyte expression of Vegf in Tg(Nphs1-Nog) mice, whereas the signal was markedly suppressed in Tg(Nphs1-Bmp4) mice. However, in vitro studies with metanephroi failed to demonstrate a direct interaction between BMP4 or Noggin and VEGF in podocytes. Instead, immunostaining showed that phosphorylated Smads, the mediators of BMP signaling, are present in endothelial and/or mesangial cells, but not in podocytes, within the developing glomeruli. Therefore, this study suggests that podocyte-derived BMP plays an important role in glomerular capillary formation, perhaps by acting on non-podocyte glomerular cells in a paracrine fashion.




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