4.8 Article

Somatostatin Interneurons Promote Neuronal Synchrony in the Neonatal Hippocampus

Journal

CELL REPORTS
Volume 26, Issue 12, Pages 3173-+

Publisher

CELL PRESS
DOI: 10.1016/j.celrep.2019.02.061

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Funding

  1. Priority Program 1665 of the German Research Foundation [HO 2156/3-1/2, KI 1816/1-1/2, KI 1638/3-2]
  2. Collaborative Research Center of the German Research Foundation [Transregio 166]
  3. Research Unit 1738 of the German Research Foundation [WI 830/10-2]
  4. Bernstein Focus of the Federal Ministry of Education and Research [01GQ0923]
  5. Interdisciplinary Centre for Clinical Research Jena

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Synchronized activity is a universal characteristic of immature neural circuits that is essential for their developmental refinement and strongly depends on GABAergic neurotransmission. A major subpopulation of GABA-releasing interneurons (INs) expresses somatostatin (SOM) and proved critical for rhythm generation in adulthood. Here, we report a mechanism whereby SOM INs promote neuronal synchrony in the neonatal CA1 region. Combining imaging and electrophysiological approaches, we demonstrate that SOM INs and pyramidal cells (PCs) coactivate during spontaneous activity. Bidirectional optogenetic manipulations reveal excitatory GABAergic outputs to PCs that evoke correlated network events in an NKCC1-dependent manner and contribute to spontaneous synchrony. Using a dynamic systems modeling approach, we show that SOM INs affect network dynamics through a modulation of network instability and amplification threshold. Our study identifies a network function of SOM INs with implications for the activity-dependent construction of developing brain circuits.

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