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The Journal of Neuroscience, October 1, 2001, 21(19):7474-7480
Cocaine- and Amphetamine-Regulated Transcript Peptide Modulation
of Voltage-Gated Ca2+ Signaling in Hippocampal
Neurons
Olena
Yermolaieva1,
Jianguo
Chen1,
Pastor R.
Couceyro2, and
Toshinori
Hoshi1
1 Department of Physiology and Biophysics, University
of Iowa, Iowa City, Iowa 52242, and 2 Department of
Cellular and Molecular Pharmacology, Chicago Medical School, North
Chicago, Illinois 60064
Administration of cocaine and amphetamine increases cocaine- and
amphetamine-regulated transcript (CART) expression in the rat striatum
(Douglass et al., 1995). CART mRNA is highly expressed in different
parts of the human and rat brain, including hippocampus (Douglass et
al., 1995; Couceyro et al., 1997; Kuhar and Yoho, 1999; Hurd and
Fagergren, 2000). The presence of CART peptide 55-102 immunoreactivity
in dense core vesicles of axon terminals suggests that the peptide may
be released and may act as a neuromodulator (Smith et al., 1997)
to induce neurophysiological and behavioral effects. Little is known,
however, about CART peptide-responsive cells, receptor(s), or
intracellular signaling mechanisms that mediate CART peptide action.
Here we show that CART peptide 55-102 inhibits voltage-dependent
intracellular Ca2+ signaling and attenuates cocaine
enhancement of depolarization-induced Ca2+ influx in
rat hippocampal neurons. The inhibitory effect of CART peptide 55-102
on Ca2+ signaling is likely mediated by an
inhibition of L-type voltage-gated Ca2+ channel
activity via a G-protein-dependent pathway. These results indicate that
voltage-gated Ca2+ channels in hippocampal neurons
are targets for CART peptide 55-102 and suggest that CART peptides may
be important in physiology and behavior mediated by the hippocampus,
such as certain forms of learning and memory.
Key words:
hippocampus; neuropeptide; cocaine; CART; calcium; voltage-gated calcium channels
Copyright © 2001 Society for Neuroscience 0270-6474/01/21197474-07$05.00/0
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