RT Journal Article SR Electronic T1 Thalamocortical projections have a K+ channel that is phosphorylated and modulated by cAMP-dependent protein kinase JF The Journal of Neuroscience JO J. Neurosci. FD Society for Neuroscience SP 5486 OP 5501 DO 10.1523/JNEUROSCI.15-08-05486.1995 VO 15 IS 8 A1 Moreno, H A1 Kentros, C A1 Bueno, E A1 Weiser, M A1 Hernandez, A A1 Vega-Saenz de Miera, E A1 Ponce, A A1 Thornhill, W A1 Rudy, B YR 1995 UL http://www.jneurosci.org/content/15/8/5486.abstract AB The finding that some K+ channel mRNAs are restricted to certain populations of neurons in the CNS suggests that there are K+ channels tailored to certain neuronal circuits. One such example are the transcripts from the KV3.2 gene, the majority of which are expressed in thalamic relay neurons. To gain insights into the specific roles of KV3.2 subunits, site specific antibodies were raised to determine their localization in thalamic relay neurons. Immunohistochemical and focal lesioning studies demonstrate that KV3.2 proteins are localized to the terminal fields of thalamocortical projections. It is also shown that KV3.2 channels expressed in vitro are strongly inhibited through phosphorylation by cAMP-dependent protein kinase (PKA). Channels containing KV3.1 subunits, which otherwise exhibit nearly identical electrophysiological properties in heterologous expression systems but have a different and less restricted pattern of expression in the CNS, are not affected by PKA. Therefore, this modulation might be associated with the specific roles of KV3.2 subunits. Furthermore, we demonstrate that KV3.2 proteins can be phosphorylated in situ by intrinsic PKA. KV3.2 subunits display properties and have a localization consistent with a role in the regulation of the efficacy of the thalamocortical synapse, and could thereby participate in the neurotransmitter-mediated control of functional states of the thalamocortical system associated with global states of awareness.