Differential expression of K(4-AP) currents and Kv3.1 potassium channel transcripts in cortical neurons that develop distinct firing phenotypes

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Abstract

Maturation of electrical excitability during early postnatal development is critical to formation of functional neural circuitry in the mammalian neocortex. Little is known, however, about the changes in gene expression underlying the development of firing properties that characterize different classes of cortical neurons. Here we describe the development of cortical neurons with two distinct firing phenotypes, regular-spiking (RS) and fast- spiking (FS), that appear to emerge from a population of immature multiple- spiking (IMS) neurons during the first two postnatal weeks, both in viva (within layer IV) and in vitro. We report the expression of a slowly inactivating, 4-AP-sensitive potassium current (K(4-AP)) at significantly higher density in FS compared with RS neurons. The same current is expressed at intermediate levels in IMS neurons. The kinetic, voltage-dependent, and pharmacological properties of the K(4-AP) current are similar to those observed by heterologous expression of Kv3.1 potassium channel mRNA. Single- cell RT-PCR analysis demonstrates that PCR products representing Kv3.1 transcripts are amplified more frequently from FS than RS neurons, with an intermediate frequency of Kv3.1 detection in neurons with immature firing properties. Taken together, these data suggest that the Kv3.1 gene encodes the K(4-AP) current and that expression of this gene is regulated in a cell- specific manner during development. Analysis of the effects of 4-AP on firing properties suggests that the K(4-AP) current is important for rapid action potential repolarization, fast after-hyperpolarization, brief refractory period, and high firing frequency characteristic of FS GABAergic interneurons.

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Massengill, J. L., Smith, M. A., Son, D. I., & O’Dowd, D. K. (1997). Differential expression of K(4-AP) currents and Kv3.1 potassium channel transcripts in cortical neurons that develop distinct firing phenotypes. Journal of Neuroscience, 17(9), 3136–3147. https://doi.org/10.1523/jneurosci.17-09-03136.1997

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