Abstract

Cysts derive from renal tubules and may progressively expand to several centimeters in diameter; in a sense they are benign neoplastic tumors. The long-term objective of this application is to determine the aberrant mechanisms responsible for directing epithelial cells of normal and genetically abnormal kidney tubules to become cysts rather than terminally differentiated renal tubules. The applicants will test the general hypothesis that renal cysts of acquired and hereditary etiologies share a developmental abnormality in common, that of being locked in an altered state of differentiation and perpetual radial proliferation in which the cells are morphologically and functionally less mature than those of terminally differentiated tubular epithelium; the immature cyst phenotype is unable to respond to exogenous differentiating agents and fails to down-regulate cyclic-AMP dependent transepithelial chloride secretion through the cystic fibrosis transmembrane conductance regulator (CFTR). There are six Specific Aims: 1) use an in vitro culture method to observe the differentiation of cysts grown in collagen matrix into tubule-like structures, and determine the effect and mechanism of action of fibroblast-conditioned medium and fibroblast co-culture on embedded cells obtained from the walls of established cysts in hereditary and acquired human cystic disorders, in comparison to normal tubule epithelial cells; 2) determine the effect of fibroblast-conditioned medium and fibroblast co-culture on renal epithelial cells cultured from mice and rats with heritable forms of recessive (C57BL/6J-cpk, DBA-pcy) and dominant (HAN:SPRD-cy) renal disease; 3) identify by subtraction cloning the genes uniquely expressed in response to fibroblast-dependent differentiation of MDCK cysts into a tubular phenotype; examine the expression of these genes in spontaneous renal cystic disorders and in in vitro models of cysts derived from human renal cells; 4) determine with polarized cultures of human autosomal dominant PKD, autosomal recessive PKD, acquired cystic kidney disease and human kidney cortex cells, and polarized primary cultures of C57BL/6J-cpk, DBA-pcy, and HAN:SPRD-cy kidney cells the magnitude of chloride secretion in response to secretogogues, and correlate these with contemporaneous changes in the level of intracellular cyclic AMP; 5) determine with in situ and Northern hybridization and immunohistochemistry the extent of CFTR expression: a) in human adult intact kidneys and cells cultured from ADPKD, ARPKD, ACKD, HKC; and b) in fetal, neonatal and adult intact kidneys and cultured cells from C57BL/6J- cpk, DBA-pcy, HAN:SPRD-cy and normal animals of the same strains; and 6) determine in cultured cells grown as cysts in collagen matrix the extent to which CFTR and SGP-2 expression is downregulated in response to soluble fibroblast differentiating factors. Successful completion of this research will determine the extent to which extrinsic signalling mechanisms direct normal human kidney cells to form renal tubules, and will identify specific cellular elements that are developmentally misregulated in aberrant tubulogenesis that leads to cyst formation and expansion.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK045614-02
Application #
3247104
Study Section
General Medicine B Study Section (GMB)
Project Start
1992-09-30
Project End
1995-09-29
Budget Start
1993-09-30
Budget End
1994-09-29
Support Year
2
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
University of Kansas
Department
Type
Schools of Medicine
DUNS #
016060860
City
Kansas City
State
KS
Country
United States
Zip Code
66160

  Publications

Wallace, D P; Tomich, J M; Eppler, J W et al. (2000) A synthetic channel-forming peptide induces Cl(-) secretion: modulation by Ca(2+)-dependent K(+) channels. Biochim Biophys Acta 1464:69-82
Sullivan, L P; Wallace, D P; Grantham, J J (1998) Epithelial transport in polycystic kidney disease. Physiol Rev 78:1165-91
Tomich, J M; Wallace, D; Henderson, K et al. (1998) Aqueous solubilization of transmembrane peptide sequences with retention of membrane insertion and function. Biophys J 74:256-67
Sullivan, L P; Wallace, D P; Grantham, J J (1998) Chloride and fluid secretion in polycystic kidney disease. J Am Soc Nephrol 9:903-16
Wallace, D P; Tomich, J M; Iwamoto, T et al. (1997) A synthetic peptide derived from glycine-gated Cl- channel induces transepithelial Cl- and fluid secretion. Am J Physiol 272:C1672-9
Grantham, J J (1997) Mechanisms of progression in autosomal dominant polycystic kidney disease. Kidney Int Suppl 63:S93-7
Holleran, A L; Fiskum, G; Kelleher, J K (1997) Quantitative analysis of acetoacetate metabolism in AS-30D hepatoma cells with 13C and 14C isotopic techniques. Am J Physiol 272:E945-51
Grantham, J J; Schreiner, G F; Rome, L et al. (1997) Evidence for inflammatory and secretagogue lipids in cyst fluids from patients with autosomal dominant polycystic kidney disease. Proc Assoc Am Physicians 109:397-408
Wallace, D P; Grantham, J J; Sullivan, L P (1996) Chloride and fluid secretion by cultured human polycystic kidney cells. Kidney Int 50:1327-36
Rankin, C A; Suzuki, K; Itoh, Y et al. (1996) Matrix metalloproteinases and TIMPS in cultured C57BL/6J-cpk kidney tubules. Kidney Int 50:835-44

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