Role of group-II and -III metabotropic glutamate receptors in the modulation of miniature synaptic activity in frog spinal-cord motoneurons
| Autor: | I. S. Masalov, N. M. Chmykhova, Nikolai P. Vesselkin, O. A. Karamian, V. M. Kozhanov |
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| Rok vydání: | 2008 |
| Předmět: |
musculoskeletal
neural and ocular physiology Metabotropic glutamate receptor 7 Cell Biology Anatomy Biology GABAB receptor Inhibitory postsynaptic potential Miniature Postsynaptic Potentials chemistry.chemical_compound Phaclofen Metabotropic receptor nervous system chemistry Metabotropic glutamate receptor Biophysics Metabotropic glutamate receptor 1 |
| Zdroj: | Cell and Tissue Biology. 2:493-503 |
| ISSN: | 1990-5203 1990-519X |
| DOI: | 10.1134/s1990519x08050076 |
| Popis: | Results of the present work demonstrate the pronounced modulating effects mediated by group-II and-III metabotropic glutamate receptors (mGluRs) on miniature postsynaptic potentials (mPSPs) of frog spinal motoneurons. The character of the effects of the group-II and-III mGluRs ligands, i.e., changes in the mPSPs frequency and the absence of significant changes in their amplitude, indicates the presynaptic mechanism of the modulation due to a change of the process of transmitter release. The application of ethylglutamate (EGLU) and methylaminophosphobutyrate (MAP4), which are selective antagonists of group-II and-III mGluRs, increased frequency of mPSPs by an average of 52.8 ± 30.2% (in four out of six motoneurons) and by 54.7 ± 23.7% (in all 7 motoneurons), respectively. The application of group-III mGluRs agonist L-aminophosphobutyrate (L-AP4) decreased the mPSP frequency by 21.8 ± 5.2% in three out of five motoneurons. The efficiency of the use of an antagonist and the comparatively low efficiency of the agonist suggest that presynaptic mGluRs are tonically activated during motoneuronal synapses. The absence of a group-II mGluR antagonist effect in some motoneurons appears to be explained by the specific localization of group-II mGluRs in the preterminal area distant from the transmitter release site. The modulation of pharmacologically isolated inhibitory miniature activity and its glycine and GABAergic fractions due to the group-III mGluRs-mediated heteroreceptor was investigated. The MAP4 application was shown to increase the glycine-mediated mIPSPs frequency to a greater degree than the GABA-mediated mIPSPs frequency, as their modulations were equal to an average of 97.6 ± 20.7% (n = 7) and 54.6 ± 20.8% (n = 5), respectively. This difference might possibly be due to the segregation of the postsynaptic glycine and GABAA receptors. The study of the convergence of the modulating effects of the presynaptic mGluRs and metabotropic GABAB receptors has shown that, under the condition of the blockage of the tonically active GABAB receptor by phaclofen, the application of the group-III mGluR agonist L-AP4 produces the typical effect, which was completely eliminated by subsequent application of the group-III mGluRs antagonist MAP4. This result agrees with the point of view regarding the independence of effects mediated by GABAB receptors and group-III mGluRse. |
| Databáze: | OpenAIRE |
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