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Molecular Pharmacology, Vol 11, 866-873, Copyright © 1975 by the American Society for Pharmacology and Experimental Therapeutics
,
-Diaminocarboxylic Acids
1 Department of Pharmacology and Biochemistry, Nippon Roche Research Center, Kajiwara, Kamakura,
Japan
The accumulation of cyclic 3',5'-AMP elicited by glutamate in incubated slices of guinea
pig cerebral cortex was inhibited by 2,3-diaminopropionate, 2,4-diaminobutyrate, or
ornithine. The inhibitory action of histidine was marginal, and other basic amino acids,
-monoamino acids, and aliphatic diamines were ineffective as inhibitors. 2,3-Diaminopropionate at 2 mM inhibited the stimulatory effect of glutamate more than 50% with
respect to both endogenous and radioactive cyclic AMP; the latter was derived from
intracellular nucleotides labeled during a prior incubation with radioactive adenine.
Such a marked inhibitory action of 2,3-diaminopropionate was not observed toward the
effects of adenosine, histamine, or a histamine-norepinephrine combination. 2'-Deoxyadenosine was found to be capable of inhibiting the adenosine effect, using either the
radioactive labeling assay or the measurement of endogenous levels of cyclic AMP. The
glutamate effect was not inhibited by the nucleoside. The results demonstrate that 2,3-diaminopropionic acid and 2'-deoxyadenosine are specific antagonists of the respective
receptors, the former for acidic amino acids and the latter for adenosine, both of which
mediate accumulation of cyclic AMP in incubated brain slices.
Note:
ACKNOWLEDGMENTS
We acknowledge the technical assistance of Miss
Y. Mizokami and Miss S. Oikawa. We are also grateful to Dr. Y. Yagi and Dr. T. Yamada for their
critical review of this paper.
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