Abstract

Our long-term objective is to characterize the mechanism by which CFTR controls membrane recycling and C1- conductance in reabsorptive sweat duct cells and in the heterologous expression systems. A major premise of this proposal is that CFTR regulates membrane recycling which, in turn, influences the cell surface expression of C1- channels and/or proteins that regulate these channels. Optical and electrophysiologic techniques will be used to achieve the following specific aims: 1) to relate alterations in CFTR expression to changes in endocytosis/exocytosis and C1- conductance in these experimental systems; 2) to provide a detailed characterization of the C1- conductance properties of reabsorptive sweat duct cells; 3) to characterize the regulation, ultrastructure and dynamics of the endocytic and exocytic pathways in these systems, and the identities of those vesicles whose movements are CFTR-dependent: 4) to immunolocalize CFTR in these systems and relate the location of this protein to those vesicles whose movements are CFTR-dependent and 5) to characterize the mechanism by which CFTR directs exocytosis in these systems and test the hypothesis that this exocytic process causes the CFTR-dependent upregulation of C1- conductance. Our results should provide significant insights into the mechanism by which the CF gene product controls epithelial C1- transport and membrane turnover; insights that may prove useful for designing treatments for this disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
2P01DK038518-06
Application #
3840072
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
6
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of Alabama Birmingham
Department
Type
DUNS #
004514360
City
Birmingham
State
AL
Country
United States
Zip Code
35294

  Publications

Schultz, B D; Frizzell, R A; Bridges, R J (1999) Rescue of dysfunctional deltaF508-CFTR chloride channel activity by IBMX. J Membr Biol 170:51-66
Dubinsky, W P; Mayorga-Wark, O; Schultz, S G (1998) Colocalization of glycolytic enzyme activity and KATP channels in basolateral membrane of Necturus enterocytes. Am J Physiol 275:C1653-9
Schultz, B D; DeRoos, A D; Venglarik, C J et al. (1996) Glibenclamide blockade of CFTR chloride channels. Am J Physiol 271:L192-200
Mayorga-Wark, O; Dubinsky, W P; Schultz, S G (1996) Reversal of glibenclamide and voltage block of an epithelial KATP channel. Am J Physiol 271:C1122-30
Dong, J Y; Wang, D; Van Ginkel, F W et al. (1996) Systematic analysis of repeated gene delivery into animal lungs with a recombinant adenovirus vector. Hum Gene Ther 7:319-31
Schultz, B D; Bridges, R J; Frizzell, R A (1996) Lack of conventional ATPase properties in CFTR chloride channel gating. J Membr Biol 151:63-75
Howard, M; DuVall, M D; Devor, D C et al. (1995) Epitope tagging permits cell surface detection of functional CFTR. Am J Physiol 269:C1565-76
Frizzell, R A (1995) Functions of the cystic fibrosis transmembrane conductance regulator protein. Am J Respir Crit Care Med 151:S54-8
Mayorga-Wark, O; Dubinsky, W P; Schultz, S G (1995) Reconstitution of a KATP channel from basolateral membranes of Necturus enterocytes. Am J Physiol 269:C464-71
Schultz, B D; Venglarik, C J; Bridges, R J et al. (1995) Regulation of CFTR Cl- channel gating by ADP and ATP analogues. J Gen Physiol 105:329-61

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