Modulation of Cyclic Nucleotide-independent Protein Kinase from Chick Intestine by Naturally Occurring Polyamines and Mucopolysaccharides

Overview

Journal Mol Cell Biochem

Publisher Springer

Specialty Biochemistry

Date 1986 May 1

PMID 2941678

Citations 2

Authors

G Mezzetti

M Moruzzi

G Piccinini

M G Monti

B Barbiroli

Affiliations

Soon will be listed here.

Abstract

Chick duodenal mucosa contains an endogenous factor which is capable to inhibit selectively a homologous polyamine-sensitive protein kinase. The inhibitor was partially purified and characterized, and it was found to contain typical mucopolysaccharidic components. Glycosidases digestion studies, selective degradation analysis and spectrophotometric titrations with metachromatic dyes indicated that the inhibitor preparation contained two major moieties identified as heparin-like and heparan sulfate-like structures. In chick intestine the inhibitor was specific for polyamine-sensitive protein kinase since selectively interacted with it and was inert towards other cAMP-independent and cAMP-dependent protein kinases. The inhibitory effect of the endogenous factor was counteracted by naturally occurring polyamines such as spermine. The order of potency of various polyamines was: spermine greater than thermine much greater than spermidine much greater than diamines. The release of inhibition by addition of physiological concentrations of spermine was also apparent when using cytosolic proteins as endogenous phosphate acceptors. These results suggest that a possible role of polyamine in the regulation of polyamine-sensitive protein kinase in the intestine is to protect the enzyme from the inhibitory action of endogenous heparinoids.

Citing Articles

Inhibitory action of polyamines on protein kinase C association to membranes.

Moruzzi M, Barbiroli B, Monti M, Tadolini B, Hakim G, Mezzetti G Biochem J. 1987; 247(1):175-80.

PMID: 3479981 PMC: 1148385. DOI: 10.1042/bj2470175.

Differential distribution of protein kinases along the crypt-to-lumen regions of rat colonic epithelium.

Schwartz B, FRASER G, Levy J, Sharoni Y, Guberman R, Krawiec J Gut. 1988; 29(9):1213-21.

PMID: 2848753 PMC: 1434355. DOI: 10.1136/gut.29.9.1213.

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