Substance P Mediates Excitatory Interactions between Striatal Projection Neurons

doi:10.1523/JNEUROSCI.6020-08.2009

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The Journal of Neuroscience, April 15, 2009, 29(15):4953-4963; doi:10.1523/JNEUROSCI.6020-08.2009

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Cellular/Molecular
Substance P Mediates Excitatory Interactions between Striatal Projection Neurons
Craig P. Blomeley, Laura A. Kehoe, and Enrico Bracci
Faculty of Life Sciences, University of Manchester, Manchester M13 9PT, United Kingdom
Correspondence should be addressed to Enrico Bracci, Faculty of Life Sciences, University of Manchester, AV Hill Building, Manchester M13 9PT, UK. Email: e.bracci{at}manchester.ac.uk
The striatum is the largest nucleus of the basal ganglia, andis crucially involved in motor control. Striatal projectioncells are medium-size spiny neurons (MSNs) and form functionalGABAergic synapses with other MSNs through their axon collaterals.A subpopulation of MSNs also release substance P (SP), but itsrole in MSN–MSN communication is unknown. We studied thisissue in rat brain slices, in the presence of antagonists forGABA, acetylcholine, dopamine, and opioid receptors; under theseconditions, whole-cell paired recordings from MSNs (located<100 µm apart) revealed that, in 31/137 (23%) pairs,a burst of five spikes in a MSN caused significant facilitation(14.2 ± 8.9%) of evoked glutamatergic responses in theother MSN. Reciprocal facilitation of glutamatergic responseswas present in 4 of these pairs. These facilitatory effectswere maximal when spikes preceded glutamatergic responses by100 ms, and were completely blocked by the NK1 receptor antagonistL-732,138. Furthermore, in 31/57 (54%) MSNs, a burst of 5 antidromicstimuli delivered to MSN axons in the globus pallidus significantlypotentiated glutamatergic responses evoked 250 or 500 ms laterby stimulation of the corpus callosum. These effects were largerat 250 than 500 ms intervals, were completely blocked by L-732,138,and facilitated spike generation. These data demonstrate thatMSNs facilitate glutamatergic inputs to neighboring MSNs throughspike-released SP acting on NK1 receptors. The current viewthat MSNs form inhibitory networks characterized by competitivedynamics will have to be updated to incorporate the fact thatgroups of MSNs interact in an excitatory manner.

Received Nov. 24, 2008; revised March 10, 2009; accepted March 24, 2009.

Correspondence should be addressed to Enrico Bracci, Faculty of Life Sciences, University of Manchester, AV Hill Building, Manchester M13 9PT, UK. Email: e.bracci{at}manchester.ac.uk

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