1996
DOI: 10.1111/j.1476-5381.1996.tb15306.x
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Pharmacological antagonism of the actions of group II and III mGluR agonists in the lateral perforant path of rat hippocampal slices

Abstract: An understanding of the physiological and pathological roles of metabotropic glutamate receptors (mGluRs) is currently hampered by the lack of selective antagonists. Standard extracellular recording techniques were used to investigate the activity of recently reported mGluR antagonists on agonist‐induced depressions of synaptic transmission in the lateral perforant path of hippocampal slices obtained from 12–16 day‐old rats. The group III specific mGluR agonist, (S)‐2‐amino‐4‐phosphonobutanoate (L‐AP4) depress… Show more

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Cited by 94 publications
(48 citation statements)
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References 31 publications
(43 reference statements)
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“…Consistent with the function of group II mGluRs in other brain regions (Bushell et al, 1996;Macek et al, 1996;Kilbride et al, 1998), we find selective activation of group II mGluRs in the BNST can produce a reversible depression of synaptic transmission. We find that two group II mGluR selective agonists, DCG-IV and LY354740 (Schoepp et al, 1997), inhibited glutamate-dependent field potentials and EPSCs, and that this effect was blocked by LY341495 at concentrations selective for group II mGluRs.…”
Section: Discussionsupporting
confidence: 63%
“…Consistent with the function of group II mGluRs in other brain regions (Bushell et al, 1996;Macek et al, 1996;Kilbride et al, 1998), we find selective activation of group II mGluRs in the BNST can produce a reversible depression of synaptic transmission. We find that two group II mGluR selective agonists, DCG-IV and LY354740 (Schoepp et al, 1997), inhibited glutamate-dependent field potentials and EPSCs, and that this effect was blocked by LY341495 at concentrations selective for group II mGluRs.…”
Section: Discussionsupporting
confidence: 63%
“…These alterations point to an abnormal hippocampal function that, besides a reduced presynaptic control of glutamate release from the lateral perforant path onto granule cells (Bushell et al, 1996;Shigemoto et al, 1997;Zhai et al, 2002), will also result in altered temporal patterns of GABA release from interneurons. Figure 12.…”
Section: The Role Of Group III Mglursmentioning
confidence: 99%
“…The mGluR7 subtype is the most prominent member of the group III mGluR subfamily found on presynaptic terminals in different brain regions (Bradley et al, 1996;Kinoshita et al, 1998). It provides neurons with a negative feedback mechanism which, by inhibiting voltage-dependent Ca 2ϩ channels, reduces glutamate release (Bushell et al, 1996;Perroy et al, 2000;Millan et al, 2002). Because of its low affinity for glutamate, mGluR7 has been proposed to only be activated under conditions of sustained synaptic activity (Okamoto et al, 1994).…”
Section: Introductionmentioning
confidence: 99%