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The Journal of Neuroscience, July 30, 2003, 23(17):6904-6913
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AII Amacrine Cells Express L-Type Calcium Channels at Their Output Synapses
Christopher J. Habermann,
Brendan J. O'Brien,
Heinz Wässle, and
Dario A. Protti
Department of Neuroanatomy, Max Planck Institute for Brain Research,
D-60528 Frankfurt am Main, Germany
AII amacrine cells play a critical role in the high-fidelity signal
transmission pathways involved with nighttime vision. The temporal properties
of the light responses strongly depend on the transfer function at different
synaptic stages and consequently on presynaptic calcium influx. AII light
responses are complex waveforms generated by graded input, they comprise
Na+-based spikes as well as a sustained component, and they are
transferred to graded cone bipolar cells. It is, therefore, of interest to
determine the properties of AII voltage-dependent calcium channels (VDCCs) to
establish whether these cells express N-type and/or P/Q-type VDCCs,
characteristic of spiking neurons, or whether they are more like graded
neurons, which mostly use L-type VDCCs. We combined electrophysiological,
molecular biological, and imaging techniques to characterize calcium currents
and their sites of origin in mouse AII amacrine cells. Calcium currents
activated at potentials more positive than -60 mV (maximally between -50 and
-20 mV) and inactivated slowly. These currents were blocked by dihydropyridine
(DHP) antagonists and were enhanced by the DHP agonist BayK 8644. Single-cell
RT-PCR analysis of mRNA encoding for different calcium channel
subunits in AIIs revealed a consistent expression of the 1-D subunit.
Calcium imaging of AII cells showed that the greatest change in intracellular
calcium occurred in the lobular appendages, with minor changes being observed
in the arboreal dendrites. Depolarization-induced calcium rises were also
modulated by DHPs, suggesting that a particular kind of L-type VDCC, mainly
localized to the lobular appendages, enables these spiking-capable neurons to
release neurotransmitter in a sustained manner onto OFF-cone bipolar
cells.
Key words: amacrine; rod vision; scotopic pathways; tonic synapses; transmitter release; 1D; CaV1.3 1; mouse retina; dihydropyridine
Received Dec. 17, 2002;
revised Apr. 15, 2003;
accepted Apr. 15, 2003.
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