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Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing

In sensory systems of the brain, mechanisms exist to extract distinct features from stimuli to generate a variety of behavioral repertoires. These often correspond to different cell types at various stages in sensory processing. In the mammalian olfactory system, complex information processing start...

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Autores principales: Koldaeva, Anzhelika, Zhang, Cary, Huang, Yu-Pei, Reinert, Janine Kristin, Mizuno, Seiya, Sugiyama, Fumihiro, Takahashi, Satoru, Soliman, Taha, Matsunami, Hiroaki, Fukunaga, Izumi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Society for Neuroscience 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8318078/
https://www.ncbi.nlm.nih.gov/pubmed/34099512
http://dx.doi.org/10.1523/JNEUROSCI.3076-20.2021
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author Koldaeva, Anzhelika
Zhang, Cary
Huang, Yu-Pei
Reinert, Janine Kristin
Mizuno, Seiya
Sugiyama, Fumihiro
Takahashi, Satoru
Soliman, Taha
Matsunami, Hiroaki
Fukunaga, Izumi
author_facet Koldaeva, Anzhelika
Zhang, Cary
Huang, Yu-Pei
Reinert, Janine Kristin
Mizuno, Seiya
Sugiyama, Fumihiro
Takahashi, Satoru
Soliman, Taha
Matsunami, Hiroaki
Fukunaga, Izumi
author_sort Koldaeva, Anzhelika
collection PubMed
description In sensory systems of the brain, mechanisms exist to extract distinct features from stimuli to generate a variety of behavioral repertoires. These often correspond to different cell types at various stages in sensory processing. In the mammalian olfactory system, complex information processing starts in the olfactory bulb, whose output is conveyed by mitral cells (MCs) and tufted cells (TCs). Despite many differences between them, and despite the crucial position they occupy in the information hierarchy, Cre-driver lines that distinguish them do not yet exist. Here, we sought to identify genes that are differentially expressed between MCs and TCs of the mouse, with an ultimate goal to generate a cell type-specific Cre-driver line, starting from a transcriptome analysis using a large and publicly available single-cell RNA-seq dataset (Zeisel et al., 2018). Many genes were differentially expressed, but only a few showed consistent expressions in MCs and at the specificity required. After further validating these putative markers using ISH, two genes (i.e., Pkib and Lbdh2) remained as promising candidates. Using CRISPR/Cas9-mediated gene editing, we generated Cre-driver lines and analyzed the resulting recombination patterns. This indicated that our new inducible Cre-driver line, Lbhd2-CreERT2, can be used to genetically label MCs in a tamoxifen dose-dependent manner, both in male and female mice, as assessed by soma locations, projection patterns, and sensory-evoked responses in vivo. Hence, this is a promising tool for investigating cell type-specific contributions to olfactory processing and demonstrates the power of publicly accessible data in accelerating science. SIGNIFICANCE STATEMENT In the brain, distinct cell types play unique roles. It is therefore important to have tools for studying unique cell types specifically. For the sense of smell in mammals, information is processed first by circuits of the olfactory bulb, where two types of cells, mitral cells and tufted cells, output different information. We generated a transgenic mouse line that enables mitral cells to be specifically labeled or manipulated. This was achieved by looking for genes that are specific to mitral cells using a large and public gene expression dataset, and creating a transgenic mouse using the gene editing technique, CRISPR/Cas9. This will allow scientists to better investigate parallel information processing underlying the sense of smell.
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spelling pubmed-83180782021-07-29 Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing Koldaeva, Anzhelika Zhang, Cary Huang, Yu-Pei Reinert, Janine Kristin Mizuno, Seiya Sugiyama, Fumihiro Takahashi, Satoru Soliman, Taha Matsunami, Hiroaki Fukunaga, Izumi J Neurosci Research Articles In sensory systems of the brain, mechanisms exist to extract distinct features from stimuli to generate a variety of behavioral repertoires. These often correspond to different cell types at various stages in sensory processing. In the mammalian olfactory system, complex information processing starts in the olfactory bulb, whose output is conveyed by mitral cells (MCs) and tufted cells (TCs). Despite many differences between them, and despite the crucial position they occupy in the information hierarchy, Cre-driver lines that distinguish them do not yet exist. Here, we sought to identify genes that are differentially expressed between MCs and TCs of the mouse, with an ultimate goal to generate a cell type-specific Cre-driver line, starting from a transcriptome analysis using a large and publicly available single-cell RNA-seq dataset (Zeisel et al., 2018). Many genes were differentially expressed, but only a few showed consistent expressions in MCs and at the specificity required. After further validating these putative markers using ISH, two genes (i.e., Pkib and Lbdh2) remained as promising candidates. Using CRISPR/Cas9-mediated gene editing, we generated Cre-driver lines and analyzed the resulting recombination patterns. This indicated that our new inducible Cre-driver line, Lbhd2-CreERT2, can be used to genetically label MCs in a tamoxifen dose-dependent manner, both in male and female mice, as assessed by soma locations, projection patterns, and sensory-evoked responses in vivo. Hence, this is a promising tool for investigating cell type-specific contributions to olfactory processing and demonstrates the power of publicly accessible data in accelerating science. SIGNIFICANCE STATEMENT In the brain, distinct cell types play unique roles. It is therefore important to have tools for studying unique cell types specifically. For the sense of smell in mammals, information is processed first by circuits of the olfactory bulb, where two types of cells, mitral cells and tufted cells, output different information. We generated a transgenic mouse line that enables mitral cells to be specifically labeled or manipulated. This was achieved by looking for genes that are specific to mitral cells using a large and public gene expression dataset, and creating a transgenic mouse using the gene editing technique, CRISPR/Cas9. This will allow scientists to better investigate parallel information processing underlying the sense of smell. Society for Neuroscience 2021-07-28 /pmc/articles/PMC8318078/ /pubmed/34099512 http://dx.doi.org/10.1523/JNEUROSCI.3076-20.2021 Text en Copyright © 2021 Koldaeva et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Articles
Koldaeva, Anzhelika
Zhang, Cary
Huang, Yu-Pei
Reinert, Janine Kristin
Mizuno, Seiya
Sugiyama, Fumihiro
Takahashi, Satoru
Soliman, Taha
Matsunami, Hiroaki
Fukunaga, Izumi
Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing
title Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing
title_full Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing
title_fullStr Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing
title_full_unstemmed Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing
title_short Generation and Characterization of a Cell Type-Specific, Inducible Cre-Driver Line to Study Olfactory Processing
title_sort generation and characterization of a cell type-specific, inducible cre-driver line to study olfactory processing
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8318078/
https://www.ncbi.nlm.nih.gov/pubmed/34099512
http://dx.doi.org/10.1523/JNEUROSCI.3076-20.2021
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