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Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy

Brain function is mediated by the physiological coordination of a vast, intricately connected network of molecular and cellular components. The physiological properties of neural network components can be quantified with high throughput. The ability to assess many animals per study has been critical...

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Autores principales: Lillvis, Joshua L, Otsuna, Hideo, Ding, Xiaoyu, Pisarev, Igor, Kawase, Takashi, Colonell, Jennifer, Rokicki, Konrad, Goina, Cristian, Gao, Ruixuan, Hu, Amy, Wang, Kaiyu, Bogovic, John, Milkie, Daniel E, Meienberg, Linus, Mensh, Brett D, Boyden, Edward S, Saalfeld, Stephan, Tillberg, Paul W, Dickson, Barry J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: eLife Sciences Publications, Ltd 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9651950/
https://www.ncbi.nlm.nih.gov/pubmed/36286237
http://dx.doi.org/10.7554/eLife.81248
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author Lillvis, Joshua L
Otsuna, Hideo
Ding, Xiaoyu
Pisarev, Igor
Kawase, Takashi
Colonell, Jennifer
Rokicki, Konrad
Goina, Cristian
Gao, Ruixuan
Hu, Amy
Wang, Kaiyu
Bogovic, John
Milkie, Daniel E
Meienberg, Linus
Mensh, Brett D
Boyden, Edward S
Saalfeld, Stephan
Tillberg, Paul W
Dickson, Barry J
author_facet Lillvis, Joshua L
Otsuna, Hideo
Ding, Xiaoyu
Pisarev, Igor
Kawase, Takashi
Colonell, Jennifer
Rokicki, Konrad
Goina, Cristian
Gao, Ruixuan
Hu, Amy
Wang, Kaiyu
Bogovic, John
Milkie, Daniel E
Meienberg, Linus
Mensh, Brett D
Boyden, Edward S
Saalfeld, Stephan
Tillberg, Paul W
Dickson, Barry J
author_sort Lillvis, Joshua L
collection PubMed
description Brain function is mediated by the physiological coordination of a vast, intricately connected network of molecular and cellular components. The physiological properties of neural network components can be quantified with high throughput. The ability to assess many animals per study has been critical in relating physiological properties to behavior. By contrast, the synaptic structure of neural circuits is presently quantifiable only with low throughput. This low throughput hampers efforts to understand how variations in network structure relate to variations in behavior. For neuroanatomical reconstruction, there is a methodological gulf between electron microscopic (EM) methods, which yield dense connectomes at considerable expense and low throughput, and light microscopic (LM) methods, which provide molecular and cell-type specificity at high throughput but without synaptic resolution. To bridge this gulf, we developed a high-throughput analysis pipeline and imaging protocol using tissue expansion and light sheet microscopy (ExLLSM) to rapidly reconstruct selected circuits across many animals with single-synapse resolution and molecular contrast. Using Drosophila to validate this approach, we demonstrate that it yields synaptic counts similar to those obtained by EM, enables synaptic connectivity to be compared across sex and experience, and can be used to correlate structural connectivity, functional connectivity, and behavior. This approach fills a critical methodological gap in studying variability in the structure and function of neural circuits across individuals within and between species.
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spelling pubmed-96519502022-11-15 Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy Lillvis, Joshua L Otsuna, Hideo Ding, Xiaoyu Pisarev, Igor Kawase, Takashi Colonell, Jennifer Rokicki, Konrad Goina, Cristian Gao, Ruixuan Hu, Amy Wang, Kaiyu Bogovic, John Milkie, Daniel E Meienberg, Linus Mensh, Brett D Boyden, Edward S Saalfeld, Stephan Tillberg, Paul W Dickson, Barry J eLife Neuroscience Brain function is mediated by the physiological coordination of a vast, intricately connected network of molecular and cellular components. The physiological properties of neural network components can be quantified with high throughput. The ability to assess many animals per study has been critical in relating physiological properties to behavior. By contrast, the synaptic structure of neural circuits is presently quantifiable only with low throughput. This low throughput hampers efforts to understand how variations in network structure relate to variations in behavior. For neuroanatomical reconstruction, there is a methodological gulf between electron microscopic (EM) methods, which yield dense connectomes at considerable expense and low throughput, and light microscopic (LM) methods, which provide molecular and cell-type specificity at high throughput but without synaptic resolution. To bridge this gulf, we developed a high-throughput analysis pipeline and imaging protocol using tissue expansion and light sheet microscopy (ExLLSM) to rapidly reconstruct selected circuits across many animals with single-synapse resolution and molecular contrast. Using Drosophila to validate this approach, we demonstrate that it yields synaptic counts similar to those obtained by EM, enables synaptic connectivity to be compared across sex and experience, and can be used to correlate structural connectivity, functional connectivity, and behavior. This approach fills a critical methodological gap in studying variability in the structure and function of neural circuits across individuals within and between species. eLife Sciences Publications, Ltd 2022-10-26 /pmc/articles/PMC9651950/ /pubmed/36286237 http://dx.doi.org/10.7554/eLife.81248 Text en © 2022, Lillvis et al https://creativecommons.org/licenses/by/4.0/This article is distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use and redistribution provided that the original author and source are credited.
spellingShingle Neuroscience
Lillvis, Joshua L
Otsuna, Hideo
Ding, Xiaoyu
Pisarev, Igor
Kawase, Takashi
Colonell, Jennifer
Rokicki, Konrad
Goina, Cristian
Gao, Ruixuan
Hu, Amy
Wang, Kaiyu
Bogovic, John
Milkie, Daniel E
Meienberg, Linus
Mensh, Brett D
Boyden, Edward S
Saalfeld, Stephan
Tillberg, Paul W
Dickson, Barry J
Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy
title Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy
title_full Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy
title_fullStr Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy
title_full_unstemmed Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy
title_short Rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy
title_sort rapid reconstruction of neural circuits using tissue expansion and light sheet microscopy
topic Neuroscience
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9651950/
https://www.ncbi.nlm.nih.gov/pubmed/36286237
http://dx.doi.org/10.7554/eLife.81248
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