Glucose stimulation of pancreatic beta-cell lines induces expression and secretion of dynorphin

To investigate adaptive responses of pancreatic beta-cells to hyperglycemia, genes induced by glucose stimulation were identified by subtraction cloning. Among 53 clones representing differentially expressed genes, 20 encoded the endogenous opioid precursor, prodynorphin. The amino acid sequence of...

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Published inEndocrinology (Philadelphia) Vol. 139; no. 10; pp. 4329 - 4336
Main Authors Josefsen, K, Buschard, K, Sørensen, L R, Wøllike, M, Ekman, R, Birkenbach, M
Format Journal Article
LanguageEnglish
Published United States 01.10.1998
Subjects
Amino Acid Sequence
Animals
Base Sequence
Cell Line
Dynorphins - biosynthesis
Dynorphins - secretion
Enkephalins - genetics
Glucose - pharmacology
Islets of Langerhans - drug effects
Islets of Langerhans - metabolism
Male
Molecular Sequence Data
Protein Precursors - genetics
Rats
Rats, Inbred Lew
RNA, Messenger - analysis
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Summary:To investigate adaptive responses of pancreatic beta-cells to hyperglycemia, genes induced by glucose stimulation were identified by subtraction cloning. Among 53 clones representing differentially expressed genes, 20 encoded the endogenous opioid precursor, prodynorphin. The amino acid sequence of murine prodynorphin is identical to the rat protein in sequences comprising the opioid peptides and 86% identical in the remainder of the molecule. Stimulation of MIN6 cells increased prodynorphin RNA levels to more than 20-fold in proportion to physiological glucose concentrations. Similar induction levels were observed in murine betaTC3 and rat Rinm5F beta-cell lines. Prodynorphin RNA expression increased within 1 h of glucose stimulation, achieved maximal levels by 4 h, and remained elevated for at least 24 h. By using RIA, MIN6 cells were shown to contain and secrete increased amounts of dynorphin-A following glucose stimulation. Treatment of MIN6 cells with KCl, forskolin, or isobutyl-methyl-xanthine strongly induced prodynorphin RNA expression, suggesting that induction may be related to secretion-coupled signaling pathways. The induction of prodynorphin in several beta-cell lines is consistent with previous demonstrations of beta-cell synthesis of other endogenous opioids, including beta-endorphin, and suggests that opioids may have a potentially significant role in regulating beta-cell secretion.
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ISSN:0013-7227
1945-7170
DOI:10.1210/en.139.10.4329