Lithium
is an effective mood stabilizer but its use is associated with many side
effects. Electrophysiological recordings of miniature excitatory postsynaptic
currents (mEPSCs) mediated by glutamate receptor AMPA-subtype (AMPARs) in
hippocampal pyramidal neurons revealed that CLi (therapeutic concentration of 1
mM lithium, from days in vitro 4-10) decreased the mean amplitude and mean
rectification index (RI) of AMPAR mEPSCs. Lowered mean RI indicate that
contribution of Ca2+-permeable AMPARs in synaptic events is higher in CLi
neurons (supported by experiments sensitive to Ca2+-permeable AMPAR
modulation). Co-inhibiting PKA, GSK-3β and glutamate reuptake was necessary to
bring about changes in AMPAR mEPSCs similar to that seen in CLi neurons. FM1-43
experiments revealed that recycling pool size was affected in CLi cultures.
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