Expression of BMP-7 and USAG-1 (a BMP antagonist) in kidney development and injury
Author(s) -
Mari Tanaka,
S. Endo,
Tomohiko Okuda,
Aris N. Economides,
David M. Valenzuela,
Andrew Murphy,
Elizabeth J. Robertson,
Takeshi Sakurai,
A Fukatsu,
George D. Yancopoulos,
Tomoko Kita,
Motoko Yanagita
Publication year - 2007
Publication title -
kidney international
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.499
H-Index - 276
eISSN - 1523-1755
pISSN - 0085-2538
DOI - 10.1038/sj.ki.5002626
Subject(s) - bone morphogenetic protein 2 , antagonist , bone morphogenetic protein 7 , kidney development , bone morphogenetic protein , medicine , kidney , endocrinology , biology , receptor , genetics , gene , embryonic stem cell , in vitro
Once developed, end-stage renal disease cannot be reversed by any current therapy. Bone morphogenetic protein-7 (BMP-7), however, is a possible treatment for reversing end-stage renal disease. Previously, we showed that the BMP antagonist uterine sensitization-associated gene-1 (USAG-1, also known as ectodin and sclerostin domain-containing 1) negatively regulates the renoprotective action of BMP-7. Here, we show that the ratio between USAG-1 and BMP-7 expression increased dramatically in the later stage of kidney development, with USAG-1 expression overlapping BMP-7 only in differentiated distal tubules. Examination of USAG-1 expression in developing kidney indicated that a mosaic of proximal and distal tubule marker-positive cells reside side by side in the immature nephron. This suggests that each cell controls its own fate for becoming a proximal or distal tubule cell. In kidney injury models, the ratio of USAG-1 to BMP-7 expression decreased with kidney damage but increased after subsequent kidney regeneration. Our study suggests that USAG-1 expression in a kidney biopsy could be useful in predicting outcome.
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