Abstract

Our goals are to characterize basolateral C1- channels from medullary thick ascending limbs of Henle (mTAL). Antidiuretic hormone (ADH) increases NaC1 absorption in microperfused mouse mTAL segments. One exploration for this effect is that ADH changes the stoichiometry of apical salt entry from Na: C1 to Na:K:2C1; and ADH increases the functional number of apical K+ channels. ADH also augments basolateral C1 conductance in mouse mTAL segments. One proposed mechanism for this effect is that ADH, via the adenylate cyclase cascade, may directly affect basolateral C1 channels analogs to cAMP effects on C1 channel activity of apical membranes in trachea and small intestine. We have proposed that increases in mTAL C1 concentrations may activate basolateral C1 channels directly, so that intracellular C1 -the substrate for basolateral C1 channels- may be the key determinant of basolateral C1-channel activity. In this regard, work in our laboratory on single C1-channels fused into planar bilayers for basolaterally-enriched vesicles prepared either from rabbit outer medulla or from highly enriched (97%) suspensions of mouse mTAL segments indicates that the open time probability Po in such channels was augmented by increasing progressively the KC1 concentrations facing the intracellular surfaces on these channels form 2 mM to 50 mM (within the physiologic range of intracellular mTAL C1-concentrations). The catalytic subunit of protein kinase A plus ATP (C-PKA + ATP) augmented Po when 2 mM KC1 bathed intracellular faces of these C1- channels, but (c-PKA + ATP) had no effect on Po when 50 mM KC1 bathed intracellular C1- channel faces. Thus so long as intracellular mTAL C1- concentrations are not depleted, cAMP may be a biologically redundant modifier of basolateral mTAL C1-channels. These finding relating Po, (cAMP + ATP) and KC1 concentrations bathing intracellular C1-channel faces are unique among epithelial C1-channels, and may account for the fact that, in vivo, the mTAL is spared in cystic fibrosis. Our key goals are: 1) To verify identify between C1- channels in bilayers and basolateral C1-channels of intact mTAL cells; ii) To define further the biophysical properties of these C1-channels; iii) to purify basolateral mTAL C1-channels to and to reconstitute activity of purified channels in liposomes; iv) To clone the cDNA for basolateral C1-channels of the mTAL.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK025540-11
Application #
2137746
Study Section
General Medicine B Study Section (GMB)
Project Start
1994-04-01
Project End
1998-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
11
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of Arkansas for Medical Sciences
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
City
Little Rock
State
AR
Country
United States
Zip Code
72205

  Publications

Winters, C J; Mikhailova, M V; Andreoli, T E (2003) Cl- channels in basolateral TAL membranes. XIX. Cytosolic Cl- regulates mmCIC-Ka and mcCIC-Ka channels. J Membr Biol 195:73-84
Winters, C J; Andreoli, T E (2003) Chloride channels in basolateral TAL membranes. XVIII. Phenylglyoxal induces functional mcCIC-Ka activity in basolateral MTAL membranes. J Membr Biol 195:63-71
Winters, C J; Andreoli, T E (2002) Cl channels in basolateral TAL membranes. XVII. Kinetic properties of mcClC-Ka, a basolateral CTAL Cl- channel. J Membr Biol 186:159-64
Mikhailova, Marina V; Winters, Christopher J; Andreoli, Thomas E (2002) Cl- channels in basolateral TAL membranes. XVI. MTAL and CTAL cells each contain the mRNAs encoding mmClC-Ka and mcClC-Ka. Kidney Int 61:1003-10
Winters, C J; Zimniak, L; Mikhailova, M V et al. (2000) Cl(-) channels in basolateral TAL membranes XV. Molecular heterogeneity between cortical and medullary channels. J Membr Biol 177:221-30
Winters, C J; Reeves, W B; Andreoli, T E (1999) Cl- channels in basolateral TAL membranes: XIII. Heterogeneity between basolateral MTAL and CTAL Cl- channels. Kidney Int 55:593-601
Winters, C J; Reeves, W B; Andreoli, T E (1999) Cl- channels in basolateral TAL membranes. XIV. Kinetic properties of a basolateral MTAL Cl- channel. Kidney Int 55:1444-9
Winters, C J; Zimniak, L; Reeves, W B et al. (1997) Cl- channels in basolateral renal medullary membranes. XII. Anti-rbClC-Ka antibody blocks MTAL Cl- channels. Am J Physiol 273:F1030-8
Zimniak, L; Winters, C J; Reeves, W B et al. (1996) Cl- channels in basolateral renal medullary vesicles XI. rbClC-Ka cDNA encodes basolateral MTAL Cl- channels. Am J Physiol 270:F1066-72
Reeves, W B; Winters, C J; Filipovic, D M et al. (1995) Cl- channels in basolateral renal medullary vesicles. IX. Channels from mouse MTAL cell patches and medullary vesicles. Am J Physiol 269:F621-7

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