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Molecular Pharmacology, Vol 20, 76-82, Copyright © 1981 by the American Society for Pharmacology and Experimental Therapeutics
-Ketoisocaproic Acid is an Appropriate Model Compound to Study
the Role of B-Cell Metabolism
1 Institute of Pharmacology and Toxicology, University of Göttingen, Kreuzbergring 57, D-3400 Göttingen, Germany
-Ketoisocaproic acid released insulin from isolated mouse islets with a threshold concentration at 2-3 mM and a maximal effect at 15-20 mM. Stimulation of insulin secretion
was accompanied by small increases of cyclic AMP accumulation by islets which could be
prevented by omission of Ca2+ from the incubation media. Extramitochondrial metabolites
that could arise from -ketoisocaproic acid released much less insulin than their mother
substance. Accumulation of intramitochondrial CoA compounds typical for degradation
of -ketoisocaproic acid probably did not cause the specific B-cell response to this keto
acid. It is concluded that metabolites do not represent primary signals during -ketoisocaproic acid-induced insulin secretion. The experimental data are compatible with the
view that increase of intramitochondrial production of reducing equivalents is necessary
for recognizing insulin-releasing fuels by B-cells.
Note:
ACKNOWLEDGMENTS
We thank Professor E. Brunner and his colleagues for help with the
statistical testing.
This article has been cited by other articles:
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  H.-P. Bode, B. Moormann, R. Dabew, and B. Göke Glucagon-Like Peptide 1 Elevates Cytosolic Calcium in Pancreatic {beta}-Cells Independently of Protein Kinase A Endocrinology, September 1, 1999; 140(9): 3919 - 3927. [Abstract] [Full Text]
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