Abstract

The general goals of this work are to understand the membrane mechanisms involved in C1 secretion by oxyntic cells and surface cells of the gastric mucosa as well as the different cellular processes which serve to regulate this transport.
The first aim i s to investigate whether membrane Na-H and C1-HCO3 exchangers may be contributing to this transport. A cytoplasmic-trapped, fluorescent dye (so-called BCECF) will be used to monitor quantitatively the cellular pH (pHc) in isolated gastric glands and in isolated purified oxynthic cells and surface cells from rabbit stomach. Measurements of Phc during a variety of experimental treatments (altered solution concentrations of Na, C1 and HCO3/CO2; use of specific inhibitors like amiloride for Na-H exchange and SITS for C1-HCO3 exchange) will allow us to determine whether such exchangers are operational in gastric mucosa. These data will also provide unique information regarding the ability of gastric cells to regulate their pHc. Further information about the C1-HCO3 exchnager will be obtained by monitoring the flux of the fluorescent dye NBD-taurine, which moves across red cell membranes only through the exchanger. The second goal is to measure rapid, unidirectional uptakes of 22 Na, 36 C1 and 42K (or 86 Rb) in isolated rabbit surface cells and oxynthic cells to determine whether these cells contain other mechanisms (e.g. NaC1 or NaKC12) besides the exchangers for accumulating C1. The final goal is to determine some of the mechanisms by which the oxynthic cells and surface cells regulate the activity of these membrane exchangers and co-transporters. Since [Ca]c has been implicated as a cellular second messenger for many cell types (including the stomach), we will utilize the cytoplasmic-trapped fluroescent, Ca-sensitive dye (so-called Quin 2) for quantitatively measuring [Ca]c during conditions in which C1 transport and the activity of the cells has been altered. Interactions among [Ca]c, pHc and other cellular second messengers (e.g. eyclic nucleotides, C-kinase) will also be investigated. These experiments will yield information about how gastric cells generate and control C1 secretion. Since there are many direct relationships among H, C1 and OH/HCO3 transport by gastric cells, this work will have implications about the ability of: (1) the oxyntic cells to secrete HC1; (ii) the surface cells to secrete OH/HCO3 and thereby maintain the so-called mucus/HCO3 barrier; (iii) both cell types to regulate their cytoplasmic pH in the face of the highly acidic stomach contents.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK019520-11
Application #
3226422
Study Section
Physiology Study Section (PHY)
Project Start
1977-04-01
Project End
1989-11-30
Budget Start
1988-12-01
Budget End
1989-11-30
Support Year
11
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
University of California Berkeley
Department
Type
Schools of Arts and Sciences
DUNS #
094878337
City
Berkeley
State
CA
Country
United States
Zip Code
94704

  Publications

Bischof, G; Serwold, T F; Machen, T E (1997) Does nitric oxide regulate capacitative Ca influx in HEK 293 cells? Cell Calcium 21:135-42
Sammak, P J; Hinman, L E; Tran, P O et al. (1997) How do injured cells communicate with the surviving cell monolayer? J Cell Sci 110 ( Pt 4):465-75
Hofer, A M; Curci, S; Machen, T E et al. (1996) ATP regulates calcium leak from agonist-sensitive internal calcium stores. FASEB J 10:302-8
Illek, B; Fischer, H; Machen, T E (1996) Alternate stimulation of apical CFTR by genistein in epithelia. Am J Physiol 270:C265-75
Hofer, A M; Schlue, W R; Curci, S et al. (1995) Spatial distribution and quantitation of free luminal [Ca] within the InsP3-sensitive internal store of individual BHK-21 cells: ion dependence of InsP3-induced Ca release and reloading. FASEB J 9:788-98
Negulescu, P A; Machen, T E (1995) La3+ and pH sensitivity of Ca2+ entry and intracellular store filling in gastric parietal cells. Am J Physiol 269:G770-8
Illek, B; Fischer, H; Santos, G F et al. (1995) cAMP-independent activation of CFTR Cl channels by the tyrosine kinase inhibitor genistein. Am J Physiol 268:C886-93
Bischof, G; Brenman, J; Bredt, D S et al. (1995) Possible regulation of capacitative Ca2+ entry into colonic epithelial cells by NO and cGMP. Cell Calcium 17:250-62
Bischof, G; Illek, B; Reenstra, W W et al. (1995) Role for tyrosine kinases in carbachol-regulated Ca entry into colonic epithelial cells. Am J Physiol 268:C154-61
Poulsen, J H; Fischer, H; Illek, B et al. (1994) Bicarbonate conductance and pH regulatory capability of cystic fibrosis transmembrane conductance regulator. Proc Natl Acad Sci U S A 91:5340-4

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