Mechanisms underlying short-term modulation of transmitter release by presynaptic depolarization
AUTOR(ES)
Hori, Tetsuya
FONTE
Blackwell Science Inc
RESUMO
Presynaptic terminal depolarization modulates the efficacy of transmitter release. Residual Ca2+ remaining after presynaptic depolarization is thought to play a critical role in facilitation of transmitter release, but its downstream mechanism remains unclear. By making simultaneous pre- and postsynaptic recordings at the rodent calyx of Held synapse, we have investigated mechanisms involved in the facilitation and depression of postsynaptic currents induced by presynaptic depolarization. In voltage-clamp experiments, cancellation of the Ca2+-dependent presynaptic Ca2+ current (IpCa) facilitation revealed that this mechanism can account for 50% of postsynaptic current facilitation, irrespective of intraterminal EGTA concentrations. Intraterminal EGTA, loaded at 10 mm, failed to block postsynaptic current facilitation, but additional BAPTA at 1 mm abolished it. Potassium-induced sustained depolarization of non-dialysed presynaptic terminals caused a facilitation of postsynaptic currents, superimposed on a depression, with the latter resulting from reductions in presynaptic action potential amplitude and number of releasable vesicles. We conclude that presynaptic depolarization bidirectionally modulates transmitter release, and that the residual Ca2+ mechanism for synaptic facilitation operates in the immediate vicinity of voltage-gated Ca2+ channels in the nerve terminal.
ACESSO AO ARTIGO
http://www.pubmedcentral.nih.gov/articlerender.fcgi?artid=2718256Documentos Relacionados
- Short-term storage of Haemophilus influenzae
- SHORT-TERM N215-INCORPORATION BY AZOTOBACTER1
- Short-term regulation of insulin gene transcription by glucose
- Intracellular calcium transients underlying the short-term force-interval relationship in ferret ventricular myocardium.
- Vitreon, a short-term vitreoretinal tamponade.
