![[Feedback]](/icons/banner/feedbackACT.gif){kind=icon}
![[For Subscribers]](/icons/banner/subscriberACT.gif){kind=icon}
![[Archive]](/icons/banner/archiveACT.gif){kind=icon}
![[Search]](/icons/banner/searchACT.gif){kind=icon}
![[Contents]](/icons/banner/tocACT.gif){kind=icon}
|
|
|
|
|
||
Vol. 286, Issue 1, 509-518, July 1998
-Aminobutyric Acid Receptor-Mediated Hyperpolarization
Recorded from the Dorsolateral Septum1
Department of Pharmacology and Toxicology, University of Texas
Medical Branch at Galveston, Galveston, Texas
Previous reports of membrane hyperpolarizations, associated with
acute application of cocaine, have been recorded from brain slice
preparations containing aminergic nuclei and have always been
attributed to cocaine's ability to elevate levels of local biogenic
amines followed by activation of their receptors. The majority of these
studies were conducted with brain slices obtained from rats that had
not received prior chronic in vivo treatment with
cocaine. We observed that cocaine alone, at 3 µM, could induce a
membrane hyperpolarization (COC-HYP) in 100% of rat dorsolateral septal nucleus (DLSN) neurons from brain slices of rats treated chronically with cocaine for either 14 or 28 days in
vivo. The DLSN is a nucleus absent of biogenic amine cell
bodies, but does contain biogenic amine terminals with GABAergic cell
bodies and terminals. Cocaine applied to brain slices from rats not
previously administered cocaine or administered cocaine for up to seven
days in vivo yielded a maximum incidence of COC-HYPs at
only 50%. COC-HYPs recorded from DLSN neurons were not blocked by
previous treatment with amine receptor antagonists or by a TTX and zero
calcium medium. Based on these results, the ability of DLSN neurons to
respond to a cocaine challenge with a COC-HYP did not involve
inhibition of amine reuptake/uptake or action potential release of
neuroactive substances. Rather, the COC-HYP, with an apparent reversal
potential of -80 mV, was reduced by the GABA receptor
antagonists-bicuculline and CGP-55845A. Lowering extracellular
Na+ or Cl
, lowering of
temperature, or previous superfusion with the GABA uptake blocker
NO-711 could block the COC-HYP. In summary, our data suggest that
COC-HYPs, after application of a cocaine challenge to brain slices from
rats treated chronically (14 - 28 days, but not acutely, 7 days) with
cocaine are due to cocaine-induced changes in GABA release and/or
transporter function. The latter changes in transporter function may
involve the reversal of the GABA transporter with release of GABA and
subsequent activation of postsynaptic GABAA and
GABAB receptors.
This article has been cited by other articles:
|
|
 |
|
  C. A. Winstanley, Q. LaPlant, D. E. H. Theobald, T. A. Green, R. K. Bachtell, L. I. Perrotti, R. J. DiLeone, S. J. Russo, W. J. Garth, D. W. Self, et al. {Delta}FosB Induction in Orbitofrontal Cortex Mediates Tolerance to Cocaine-Induced Cognitive Dysfunction J. Neurosci., September 26, 2007; 27(39): 10497 - 10507. [Abstract] [Full Text] [PDF]
|
|
|
|
 |
|
 V. Neugebauer, F. Zinebi, R. Russell, J. P. Gallagher, and P. Shinnick-Gallagher Cocaine and Kindling Alter the Sensitivity of Group II and III Metabotropic Glutamate Receptors in the Central Amygdala J Neurophysiol, August 1, 2000; 84(2): 759 - 770. [Abstract] [Full Text] [PDF]
|
|
 |
 |
 |
|
 |
 |
 |
