4.7 Article

Role of protein kinase C-δ in the age-dependent secretagogue action of bile acids in mammalian colon

Journal

AMERICAN JOURNAL OF PHYSIOLOGY-CELL PHYSIOLOGY
Volume 293, Issue 6, Pages C1851-C1861

Publisher

AMER PHYSIOLOGICAL SOC
DOI: 10.1152/ajpcell.00194.2007

Keywords

epithelial chloride transport; taurodeoxycholate; signal transduction

Funding

  1. NIDDK NIH HHS [DK58135] Funding Source: Medline

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Role of protein kinase C-delta in the age-dependent secretagogue action of bile acids in mammalian colon. Am J Physiol Cell Physiol 293: C1851-C1861, 2007. First published September 26, 2007; doi: 10.1152/ajpcell.00194.2007. - The role of specific PKC isoforms in the regulation of epithelial Cl (-) secretion by Ca2+-dependent secretagogues remains controversial. In the developing rabbit distal colon, the bile acid taurodeoxycholate (TDC) acts via intracellular calcium to stimulate Cl- transport in adult, but not in young, animals, whereas the PKC activator phorbol dibutyrate (PDB) stimulates Cl(-)transport at all ages. We tested the hypothesis that specific PKC isoforms account for the age-specific effects of TDC. The effects of conventional (cPKC) and novel ( nPKC) PKC-specific inhibitors on TDC- and PDB-stimulated Cl (-) transport in adult and weanling colonocytes were assessed by using 6-methoxy-quinolyl acetoethyl ester. In adult colonocytes, the cPKC inhibitor Go-6976 inhibited PDB action but not TDC action, whereas the cPKC and nPKC inhibitor Go r-6850 blocked both TDC and PDB actions. Additionally, rottlerin and the PKC-delta-specific inhibitor peptide (delta V1-1) inhibited TDC- and PDB-stimulated Cl- transport in adult colonocytes. Rottlerin also decreased TDC-stimulated short- circuit current in intact colonic epithelia. Only Go r-6976, but neither rottlerin nor delta V1-1, inhibited PDB-stimulated transport in weanling colonocytes. Colonic lysates express PKC-alpha, -lambda, and -iota protein equally at all ages, but they do not express PKC-gamma or -theta at any age. Expression of PKC-beta and PKC-epsilon protein was newborn > adult > weanling, whereas PKC- delta was expressed in adult but not in weanling or newborn colonocytes. TDC ( 1.6- fold) and PDB (2.0-fold) stimulated PKC-delta enzymatic activity in adult colonocytes but failed to do so in weanling colonocytes. PKC-delta mRNA expression showed age dependence. Thus PKC-delta appears critical for the action of TDC in the adult colon, and its low expression in young animals may account for their inability to secrete in response to bile acids.

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