Scholars@Duke publication: Differential activity-dependent, homeostatic plasticity of two neocortical inhibitory circuits.

Differential activity-dependent, homeostatic plasticity of two neocortical inhibitory circuits.

Publication , Journal Article

Bartley, AF; Huang, ZJ; Huber, KM; Gibson, JR

Published in: J Neurophysiol

October 2008

Chronic changes in neuronal activity homeostatically regulate excitatory circuitry. However, little is known about how activity regulates inhibitory circuits or specific inhibitory neuron types. Here, we examined the activity-dependent regulation of two neocortical inhibitory circuits--parvalbumin-positive (Parv+) and somatostatin-positive (Som+)--using paired recordings of synaptically coupled neurons. Action potentials were blocked for 5 days in slice culture, and unitary synaptic connections among inhibitory/excitatory neuron pairs were examined. Chronic activity blockade caused similar and distinct changes between the two inhibitory circuits. First, increases in intrinsic membrane excitability and excitatory synaptic drive in both inhibitory subtypes were consistent with the homeostatic regulation of firing rate of these neurons. On the other hand, inhibitory synapses originating from these two subtypes were differentially regulated by activity blockade. Parv+ unitary inhibitory postsynaptic current (uIPSC) strength was decreased while Som+ uIPSC strength was unchanged. Using short-duration stimulus trains, short-term plasticity for both unitary excitatory postsynaptic current (uEPSCs) and uIPSCs was unchanged in Parv+ circuitry while distinctively altered in Som+ circuitry--uEPSCs became less facilitating and uIPSCs became more depressing. In the context of recurrent inhibition, these changes would result in a frequency-dependent shift in the relative influence of each circuit. The functional changes at both types of inhibitory connections appear to be mediated by increases in presynaptic release probability and decreases in synapse number. Interestingly, these opposing changes result in decreased Parv+-mediated uIPSCs but balance out to maintain normal Som+-mediated uIPSCs. In summary, these results reveal that inhibitory circuitry is not uniformly regulated by activity levels and may provide insight into the mechanisms of both normal and pathological neocortical plasticity.

Duke Scholars

Author Josh Huang Neurobiology

Published In

J Neurophysiol

DOI

10.1152/jn.90635.2008

ISSN

0022-3077

Publication Date

October 2008

Volume

100

Issue

Start / End Page

1983 / 1994

Location

United States

Related Subject Headings

Synapses
Strontium
Somatostatin
Receptors, Presynaptic
Presynaptic Terminals
Parvalbumins
Neurons
Neuronal Plasticity
Neurology & Neurosurgery
Neural Pathways

Citation

APA

Chicago

ICMJE

MLA

NLM

Bartley, A. F., Huang, Z. J., Huber, K. M., & Gibson, J. R. (2008). Differential activity-dependent, homeostatic plasticity of two neocortical inhibitory circuits. J Neurophysiol, 100(4), 1983–1994. https://doi.org/10.1152/jn.90635.2008

Bartley, Aundrea F., Z Josh Huang, Kimberly M. Huber, and Jay R. Gibson. “Differential activity-dependent, homeostatic plasticity of two neocortical inhibitory circuits.” J Neurophysiol 100, no. 4 (October 2008): 1983–94. https://doi.org/10.1152/jn.90635.2008.

Bartley AF, Huang ZJ, Huber KM, Gibson JR. Differential activity-dependent, homeostatic plasticity of two neocortical inhibitory circuits. J Neurophysiol. 2008 Oct;100(4):1983–94.

Bartley, Aundrea F., et al. “Differential activity-dependent, homeostatic plasticity of two neocortical inhibitory circuits.” J Neurophysiol, vol. 100, no. 4, Oct. 2008, pp. 1983–94. Pubmed, doi:10.1152/jn.90635.2008.

Bartley AF, Huang ZJ, Huber KM, Gibson JR. Differential activity-dependent, homeostatic plasticity of two neocortical inhibitory circuits. J Neurophysiol. 2008 Oct;100(4):1983–1994.