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Development of Action Potential‐dependent and Independent Spontaneous GABA A Receptor‐mediated Currents in Granule Cells of Postnatal Rat Cerebellum
Author(s) -
Wall Mark J.,
Usowicz Maria M.
Publication year - 1997
Publication title -
european journal of neuroscience
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.346
H-Index - 206
eISSN - 1460-9568
pISSN - 0953-816X
DOI - 10.1111/j.1460-9568.1997.tb01630.x
Subject(s) - bicuculline , inhibitory postsynaptic potential , gabaa receptor , neuroscience , postsynaptic current , tetrodotoxin , neurotransmission , granule cell , gabaergic , tonic (physiology) , chemistry , postsynaptic potential , biophysics , cerebellum , biology , patch clamp , excitatory postsynaptic potential , microbiology and biotechnology , receptor , electrophysiology , central nervous system , biochemistry , dentate gyrus
The postnatal development of spontaneous GABAergic transmission between cerebellar Golgi cells and granule cells was investigated with voltage‐clamp recording from rat cerebellar slices, in symmetrical Cl ‐ conditions. Between postnatal days 7 and 14 (P7–14), bicuculline‐and TTX (tetrodotoxin)‐sensitive spontaneous inhibitory postsynaptic currents (sIPSCs), occurred at high frequency in 56% of granule cells. Between P10 and P14, sIPSCs were superimposed on tonic current of‐12 ± 1.8 pA at ‐70 mV, that was accompanied by noise with variance of 17 ± 3 pA 2 . Both the current and noise were inhibited by bicuculline. TTX blocked the bicuculline‐sensitive current and noise by˜60%. Between P18 and P25, sIPSCs were less frequent; all cells showed tonic, bicuculline‐sensitive currents, but these were partially inhibited by TTX (˜35%). Between P40 and P53, slPSCs were rare; tonic, bicuculline‐sensitive currents and noise were greater in amplitude, with mean values of‐17 pA and 22 pA 2 at‐70 mV, they were present in all cells but they were not inhibited by TTX. Glycine receptor channels that were expressed in immature, but not adult cells, did not mediate spontaneous currents. Our results indicate that spontaneous transmission onto cerebellar granule cells in immature animals consists primarily of action potential‐dependent, phasic release of vesicular GABA. This generates GABA A receptor‐mediated slPSCs. The effects of GABA transporter blockers suggest that it also produces the TTX‐sensitive current‐noise, as GABA spills out of synapses to activate extrasynaptic receptors or receptors in neighbouring synapses. In older animals, action potential‐independent release of transmitter is predominant and results in tonic activation of GABA A receptors. This does not appear to be spontaneous vesicular release of GABA. Neither does it appear to be reversed uptake of GABA, although further work is required to rule out these possibilities.