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Independent Optical Excitation of Distinct Neural Populations

Optogenetic tools enable the causal examination of how specific cell types contribute to brain circuit functions. A long-standing question is whether it is possible to independently activate two distinct neural populations in mammalian brain tissue. Such a capability would enable the examination of...

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Autores principales: Klapoetke, Nathan C, Murata, Yasunobu, Kim, Sung Soo, Pulver, Stefan R., Birdsey-Benson, Amanda, Cho, Yong Ku, Morimoto, Tania K, Chuong, Amy S, Carpenter, Eric J, Tian, Zhijian, Wang, Jun, Xie, Yinlong, Yan, Zhixiang, Zhang, Yong, Chow, Brian Y, Surek, Barbara, Melkonian, Michael, Jayaraman, Vivek, Constantine-Paton, Martha, Wong, Gane Ka-Shu, Boyden, Edward S
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3943671/
https://www.ncbi.nlm.nih.gov/pubmed/24509633
http://dx.doi.org/10.1038/nmeth.2836
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author Klapoetke, Nathan C
Murata, Yasunobu
Kim, Sung Soo
Pulver, Stefan R.
Birdsey-Benson, Amanda
Cho, Yong Ku
Morimoto, Tania K
Chuong, Amy S
Carpenter, Eric J
Tian, Zhijian
Wang, Jun
Xie, Yinlong
Yan, Zhixiang
Zhang, Yong
Chow, Brian Y
Surek, Barbara
Melkonian, Michael
Jayaraman, Vivek
Constantine-Paton, Martha
Wong, Gane Ka-Shu
Boyden, Edward S
author_facet Klapoetke, Nathan C
Murata, Yasunobu
Kim, Sung Soo
Pulver, Stefan R.
Birdsey-Benson, Amanda
Cho, Yong Ku
Morimoto, Tania K
Chuong, Amy S
Carpenter, Eric J
Tian, Zhijian
Wang, Jun
Xie, Yinlong
Yan, Zhixiang
Zhang, Yong
Chow, Brian Y
Surek, Barbara
Melkonian, Michael
Jayaraman, Vivek
Constantine-Paton, Martha
Wong, Gane Ka-Shu
Boyden, Edward S
author_sort Klapoetke, Nathan C
collection PubMed
description Optogenetic tools enable the causal examination of how specific cell types contribute to brain circuit functions. A long-standing question is whether it is possible to independently activate two distinct neural populations in mammalian brain tissue. Such a capability would enable the examination of how different synapses or pathways interact to support computation. Here we report two new channelrhodopsins, Chronos and Chrimson, obtained through the de novo sequencing and physiological characterization of opsins from over 100 species of algae. Chrimson is 45 nm red-shifted relative to any previous channelrhodopsin, important for scenarios where red light would be preferred; we show minimal visual system mediated behavioral artifact in optogenetically stimulated Drosophila. Chronos has faster kinetics than any previous channelrhodopsin, yet is effectively more light-sensitive. Together, these two reagents enable crosstalk-free two-color activation of neural spiking and downstream synaptic transmission in independent neural populations in mouse brain slice.
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spelling pubmed-39436712014-09-01 Independent Optical Excitation of Distinct Neural Populations Klapoetke, Nathan C Murata, Yasunobu Kim, Sung Soo Pulver, Stefan R. Birdsey-Benson, Amanda Cho, Yong Ku Morimoto, Tania K Chuong, Amy S Carpenter, Eric J Tian, Zhijian Wang, Jun Xie, Yinlong Yan, Zhixiang Zhang, Yong Chow, Brian Y Surek, Barbara Melkonian, Michael Jayaraman, Vivek Constantine-Paton, Martha Wong, Gane Ka-Shu Boyden, Edward S Nat Methods Article Optogenetic tools enable the causal examination of how specific cell types contribute to brain circuit functions. A long-standing question is whether it is possible to independently activate two distinct neural populations in mammalian brain tissue. Such a capability would enable the examination of how different synapses or pathways interact to support computation. Here we report two new channelrhodopsins, Chronos and Chrimson, obtained through the de novo sequencing and physiological characterization of opsins from over 100 species of algae. Chrimson is 45 nm red-shifted relative to any previous channelrhodopsin, important for scenarios where red light would be preferred; we show minimal visual system mediated behavioral artifact in optogenetically stimulated Drosophila. Chronos has faster kinetics than any previous channelrhodopsin, yet is effectively more light-sensitive. Together, these two reagents enable crosstalk-free two-color activation of neural spiking and downstream synaptic transmission in independent neural populations in mouse brain slice. 2014-02-09 2014-03 /pmc/articles/PMC3943671/ /pubmed/24509633 http://dx.doi.org/10.1038/nmeth.2836 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Klapoetke, Nathan C
Murata, Yasunobu
Kim, Sung Soo
Pulver, Stefan R.
Birdsey-Benson, Amanda
Cho, Yong Ku
Morimoto, Tania K
Chuong, Amy S
Carpenter, Eric J
Tian, Zhijian
Wang, Jun
Xie, Yinlong
Yan, Zhixiang
Zhang, Yong
Chow, Brian Y
Surek, Barbara
Melkonian, Michael
Jayaraman, Vivek
Constantine-Paton, Martha
Wong, Gane Ka-Shu
Boyden, Edward S
Independent Optical Excitation of Distinct Neural Populations
title Independent Optical Excitation of Distinct Neural Populations
title_full Independent Optical Excitation of Distinct Neural Populations
title_fullStr Independent Optical Excitation of Distinct Neural Populations
title_full_unstemmed Independent Optical Excitation of Distinct Neural Populations
title_short Independent Optical Excitation of Distinct Neural Populations
title_sort independent optical excitation of distinct neural populations
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3943671/
https://www.ncbi.nlm.nih.gov/pubmed/24509633
http://dx.doi.org/10.1038/nmeth.2836
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