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Publication : Time Course of Homeostatic Structural Plasticity in Response to Optogenetic Stimulation in Mouse Anterior Cingulate Cortex.

First Author  Lu H Year  2022
Journal  Cereb Cortex Volume  32
Issue  8 Pages  1574-1592
PubMed ID  34607362 Mgi Jnum  J:355091
Mgi Id  MGI:7660899 Doi  10.1093/cercor/bhab281
Citation  Lu H, et al. (2022) Time Course of Homeostatic Structural Plasticity in Response to Optogenetic Stimulation in Mouse Anterior Cingulate Cortex. Cereb Cortex 32(8):1574-1592
abstractText  Plasticity is the mechanistic basis of development, aging, learning, and memory, both in healthy and pathological brains. Structural plasticity is rarely accounted for in computational network models due to a lack of insight into the underlying neuronal mechanisms and processes. Little is known about how the rewiring of networks is dynamically regulated. To inform such models, we characterized the time course of neural activity, the expression of synaptic proteins, and neural morphology employing an in vivo optogenetic mouse model. We stimulated pyramidal neurons in the anterior cingulate cortex of mice and harvested their brains at 1.5 h, 24 h, and $48,mathrmh$ after stimulation. Stimulus-induced cortical hyperactivity persisted up to 1.5 h and decayed to baseline after $24,mathrmh$ indicated by c-Fos expression. The synaptic proteins VGLUT1 and PSD-95, in contrast, were upregulated at $24,mathrmh$ and downregulated at $48,mathrmh$, respectively. Spine density and spine head volume were also increased at $24,mathrmh$ and decreased at $48,mathrmh$. This specific sequence of events reflects a continuous joint evolution of activity and connectivity that is characteristic of the model of homeostatic structural plasticity. Our computer simulations thus corroborate the observed empirical evidence from our animal experiments.
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