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A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring

Drosophila melanogaster Down syndrome cell adhesion molecule 1 (Dscam1) encodes 19,008 diverse ectodomain isoforms via the alternative splicing of exon 4, 6, and 9 clusters. However, whether individual isoforms or exon clusters have specific significance is unclear. Here, using phenotype–diversity c...

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Autores principales: Dong, Haiyang, Yang, Xi, Wu, Lili, Zhang, Shixin, Zhang, Jian, Guo, Pengjuan, Du, Yiwen, Pan, Changkun, Fu, Ying, Li, Lei, Shi, Jilong, Zhu, Yanda, Ma, Hongru, Bian, Lina, Xu, Bingbing, Li, Guo, Shi, Feng, Huang, Jianhua, He, Haihuai, Jin, Yongfeng
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10325099/
https://www.ncbi.nlm.nih.gov/pubmed/37410725
http://dx.doi.org/10.1371/journal.pbio.3002197
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author Dong, Haiyang
Yang, Xi
Wu, Lili
Zhang, Shixin
Zhang, Jian
Guo, Pengjuan
Du, Yiwen
Pan, Changkun
Fu, Ying
Li, Lei
Shi, Jilong
Zhu, Yanda
Ma, Hongru
Bian, Lina
Xu, Bingbing
Li, Guo
Shi, Feng
Huang, Jianhua
He, Haihuai
Jin, Yongfeng
author_facet Dong, Haiyang
Yang, Xi
Wu, Lili
Zhang, Shixin
Zhang, Jian
Guo, Pengjuan
Du, Yiwen
Pan, Changkun
Fu, Ying
Li, Lei
Shi, Jilong
Zhu, Yanda
Ma, Hongru
Bian, Lina
Xu, Bingbing
Li, Guo
Shi, Feng
Huang, Jianhua
He, Haihuai
Jin, Yongfeng
author_sort Dong, Haiyang
collection PubMed
description Drosophila melanogaster Down syndrome cell adhesion molecule 1 (Dscam1) encodes 19,008 diverse ectodomain isoforms via the alternative splicing of exon 4, 6, and 9 clusters. However, whether individual isoforms or exon clusters have specific significance is unclear. Here, using phenotype–diversity correlation analysis, we reveal the redundant and specific roles of Dscam1 diversity in neuronal wiring. A series of deletion mutations were performed from the endogenous locus harboring exon 4, 6, or 9 clusters, reducing to 396 to 18,612 potential ectodomain isoforms. Of the 3 types of neurons assessed, dendrite self/non-self discrimination required a minimum number of isoforms (approximately 2,000), independent of exon clusters or isoforms. In contrast, normal axon patterning in the mushroom body and mechanosensory neurons requires many more isoforms that tend to associate with specific exon clusters or isoforms. We conclude that the role of the Dscam1 diversity in dendrite self/non-self discrimination is nonspecifically mediated by its isoform diversity. In contrast, a separate role requires variable domain- or isoform-related functions and is essential for other neurodevelopmental contexts, such as axonal growth and branching. Our findings shed new light on a general principle for the role of Dscam1 diversity in neuronal wiring.
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spelling pubmed-103250992023-07-07 A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring Dong, Haiyang Yang, Xi Wu, Lili Zhang, Shixin Zhang, Jian Guo, Pengjuan Du, Yiwen Pan, Changkun Fu, Ying Li, Lei Shi, Jilong Zhu, Yanda Ma, Hongru Bian, Lina Xu, Bingbing Li, Guo Shi, Feng Huang, Jianhua He, Haihuai Jin, Yongfeng PLoS Biol Research Article Drosophila melanogaster Down syndrome cell adhesion molecule 1 (Dscam1) encodes 19,008 diverse ectodomain isoforms via the alternative splicing of exon 4, 6, and 9 clusters. However, whether individual isoforms or exon clusters have specific significance is unclear. Here, using phenotype–diversity correlation analysis, we reveal the redundant and specific roles of Dscam1 diversity in neuronal wiring. A series of deletion mutations were performed from the endogenous locus harboring exon 4, 6, or 9 clusters, reducing to 396 to 18,612 potential ectodomain isoforms. Of the 3 types of neurons assessed, dendrite self/non-self discrimination required a minimum number of isoforms (approximately 2,000), independent of exon clusters or isoforms. In contrast, normal axon patterning in the mushroom body and mechanosensory neurons requires many more isoforms that tend to associate with specific exon clusters or isoforms. We conclude that the role of the Dscam1 diversity in dendrite self/non-self discrimination is nonspecifically mediated by its isoform diversity. In contrast, a separate role requires variable domain- or isoform-related functions and is essential for other neurodevelopmental contexts, such as axonal growth and branching. Our findings shed new light on a general principle for the role of Dscam1 diversity in neuronal wiring. Public Library of Science 2023-07-06 /pmc/articles/PMC10325099/ /pubmed/37410725 http://dx.doi.org/10.1371/journal.pbio.3002197 Text en © 2023 Dong et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Dong, Haiyang
Yang, Xi
Wu, Lili
Zhang, Shixin
Zhang, Jian
Guo, Pengjuan
Du, Yiwen
Pan, Changkun
Fu, Ying
Li, Lei
Shi, Jilong
Zhu, Yanda
Ma, Hongru
Bian, Lina
Xu, Bingbing
Li, Guo
Shi, Feng
Huang, Jianhua
He, Haihuai
Jin, Yongfeng
A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring
title A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring
title_full A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring
title_fullStr A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring
title_full_unstemmed A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring
title_short A systematic CRISPR screen reveals redundant and specific roles for Dscam1 isoform diversity in neuronal wiring
title_sort systematic crispr screen reveals redundant and specific roles for dscam1 isoform diversity in neuronal wiring
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10325099/
https://www.ncbi.nlm.nih.gov/pubmed/37410725
http://dx.doi.org/10.1371/journal.pbio.3002197
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