Abstract

A fundamental understanding of the pathogenesis of congenital kidney and urinary tract defects is crucial for developing new diagnostic and therapeutic strategies. To extend our research in this area, we propose to study embryonic patterning defects causing concurrent anomalies in the limbs and the urinary system, a phenomenon repeatedly observed in human patients. Luxate (Lx) and X-linked polydactyly (Xpl) are two classical mouse mutants with concurrent limb defects and a range of anomalies in the urinary system. We hypothesize that the Lx and Xpl mutations interrupt embryonic patterning events with pleiotropic effects on, or key regulatory circuits shared by, the development of the urinary system and the development of the limbs. We will first analyze the Lx and Xpl mice for a better understanding of the developmental processes that, when interrupted, cause the concurrent defects. In addition, we will combine the well-established positional cloning methods and the latest genome analysis tools to identify the mutations in the Lx and Xpl mutants. No known genes involved in congenital kidney and urinary tract abnormalities remain as candidates in the chromosomal intervals we have defined for Lx and Xpl. The identification of the mutations will thus reveal novel factors in the regulation of kidney development. The mechanistic studies and the mutation identification efforts are mutually supportive and are aimed at the common goal of illustrating the genetic basis and molecular mechanisms by which genetic mutations cause congenital renal diseases.

Public Health Relevance

Urogenital defects are the second most common birth defects. Congenital kidney and urinary tract malformation is a major cause for renal failure in infants and children. The terminal pathological changes to the affected kidneys can be very similar in patients with very different causes. The hope for cure lies in the understanding of the causes and the correction of the initial cellular lesions. The Lx and Xpl mutant mice have concurrent limb and renal defects that resemble """"""""Acrorenal Syndrome"""""""" in humans. In this application, we propose to identify the genetic mutations in the Lx and Xpl mutants and to reveal the molecular mechanisms by which these mutations cause the concurrent defects. Results from the proposed studies will contribute to the understanding of the genetic determinants and pathogenesis of birth defects in both the urinary system and the limbs. Such knowledge is crucial for developing new diagnostic and therapeutic strategies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
1R01DK081592-01A1
Application #
7654047
Study Section
Urologic and Kidney Development and Genitourinary Diseases Study Section (UKGD)
Program Officer
Hoshizaki, Deborah K
Project Start
2009-04-06
Project End
2013-03-31
Budget Start
2009-04-06
Budget End
2010-03-31
Support Year
1
Fiscal Year
2009
Total Cost
$364,800
Indirect Cost

  Institution

Name
Washington University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Guo, Qiusha; Wang, Yinqiu; Tripathi, Piyush et al. (2015) Adam10 mediates the choice between principal cells and intercalated cells in the kidney. J Am Soc Nephrol 26:149-59
Tripathi, P; Wang, Y; Coussens, M et al. (2014) Activation of NFAT signaling establishes a tumorigenic microenvironment through cell autonomous and non-cell autonomous mechanisms. Oncogene 33:1840-9
Ding, Li; Raphael, Benjamin J; Chen, Feng et al. (2013) Advances for studying clonal evolution in cancer. Cancer Lett 340:212-9
Pan, M-G; Xiong, Y; Chen, F (2013) NFAT gene family in inflammation and cancer. Curr Mol Med 13:543-54
Walker, Kenneth A; Sims-Lucas, Sunder; Di Giovanni, Valeria E et al. (2013) Deletion of fibroblast growth factor receptor 2 from the peri-wolffian duct stroma leads to ureteric induction abnormalities and vesicoureteral reflux. PLoS One 8:e56062
Wang, Yinqiu; Guo, Qiusha; Casey, Adam et al. (2012) A new tool for conditional gene manipulation in a subset of keratin-expressing epithelia. Genesis 50:899-907
Tripathi, Piyush; Wang, Yinqiu; Casey, Adam M et al. (2012) Absence of canonical Smad signaling in ureteral and bladder mesenchyme causes ureteropelvic junction obstruction. J Am Soc Nephrol 23:618-28
Chen, Feng; Ding, Li (2012) Co-survival of the fittest few: mosaic amplification of receptor tyrosine kinases in glioblastoma. Genome Biol 13:141
Guo, Qiusha; Tripathi, Piyush; Poyo, Edward et al. (2011) Cell death serves as a single etiological cause of a wide spectrum of congenital urinary tract defects. J Urol 185:2320-8
Tripathi, Piyush; Guo, Qiusha; Wang, Yinqiu et al. (2010) Midline signaling regulates kidney positioning but not nephrogenesis through Shh. Dev Biol 340:518-27

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