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      Optogenetic spatial and temporal control of cortical circuits on a columnar scale

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          Abstract

          Many circuits in the mammalian brain are organized in a topographic or columnar manner. These circuits could be activated—in ways that reveal circuit function or restore function after disease—by an artificial stimulation system that is capable of independently driving local groups of neurons. Here we present a simple custom microscope called ProjectorScope 1 that incorporates off-the-shelf parts and a liquid crystal display (LCD) projector to stimulate surface brain regions that express channelrhodopsin-2 (ChR2). In principle, local optogenetic stimulation of the brain surface with optical projection systems might not produce local activation of a highly interconnected network like the cortex, because of potential stimulation of axons of passage or extended dendritic trees. However, here we demonstrate that the combination of virally mediated ChR2 expression levels and the light intensity of ProjectorScope 1 is capable of producing local spatial activation with a resolution of ∼200–300 μm. We use the system to examine the role of cortical activity in the experience-dependent emergence of motion selectivity in immature ferret visual cortex. We find that optogenetic cortical activation alone—without visual stimulation—is sufficient to produce increases in motion selectivity, suggesting the presence of a sharpening mechanism that does not require precise spatiotemporal activation of the visual system. These results demonstrate that optogenetic stimulation can sculpt the developing brain.

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          Author and article information

          Journal
          J Neurophysiol
          J. Neurophysiol
          jn
          jn
          JN
          Journal of Neurophysiology
          American Physiological Society (Bethesda, MD )
          0022-3077
          1522-1598
          2 December 2015
          1 February 2016
          : 115
          : 2
          : 1043-1062
          Affiliations
          [1] 1Department of Biology, Brandeis University, Waltham, Massachusetts;
          [2] 2Volen Center for Complex Systems, Brandeis University, Waltham, Massachusetts;
          [3] 3Sloan-Swartz Center for Theoretical Neurobiology, Brandeis University, Waltham, Massachusetts; and
          [4] 4Department of Cognitive Sciences, Central European University, Budapest, Hungary
          Author notes
          [*]

          A. Roy, J. J. Osik, and N. J. Ritter contributed equally to this work.

          Address for reprint requests and other correspondence: S. D. Van Hooser, Brandeis Univ., 415 South St. MS008, Waltham, MA 02454 (e-mail: vanhooser@ 123456brandeis.edu ).
          Author information
          http://orcid.org/0000-0002-1112-5832
          Article
          PMC4839491 PMC4839491 4839491 JN-00960-2015
          10.1152/jn.00960.2015
          4839491
          26631152
          83241f85-7b0d-4a2a-bd31-a2d361d27eb6
          Copyright © 2016 the American Physiological Society
          History
          : 16 October 2015
          : 28 November 2015
          Funding
          Funded by: 100000053 HHS | NIH | National Eye Institute (NEI)
          Award ID: EY0220122
          Funded by: 100000001 National Science Foundation (NSF)
          Award ID: 1120938
          Categories
          Innovative Methodology

          activity-dependent plasticity,optogenetics,direction selectivity

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