Mapping recurrent mosaic copy number variation in human neurons
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Published:2024-05-17
Issue:1
Volume:15
Page:
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ISSN:2041-1723
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Container-title:Nature Communications
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language:en
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Short-container-title:Nat Commun
Author:
Sun ChenORCID, Kathuria KunalORCID, Emery Sarah B., Kim ByungJun, Burbulis Ian E.ORCID, Shin Joo HeonORCID, , Gleeson Joseph G., Breuss Martin W., Yang Xiaoxu, Antaki Danny, Chung Changuk, Averbuj Dan, Ball Laurel L., Roy Subhojit, Weinberger Daniel, Jaffe Andrew, Paquola Apua, Erwin Jennifer, Straub Richard, Narurkar Rujuta, Mathern Gary, Walsh Christopher A., Lee Alice, Huang August Yue, D’Gama Alissa, Dias Caroline, Maury Eduardo, Ganz Javier, Lodato Michael, Miller Michael, Li Pengpeng, Rodin Rachel, Borges-Monroy Rebeca, Hill Robert, Bizzotto Sara, Khoshkhoo Sattar, Kim Sonia, Zhou Zinan, Park Peter J., Barton Alison, Galor Alon, Chu Chong, Bohrson Craig, Gulhan Doga, Lim Elaine, Lim Euncheon, Melloni Giorgio, Cortes Isidro, Lee Jake, Luquette Joe, Yang Lixing, Sherman Maxwell, Coulter Michael, Kwon Minseok, Lee Semin, Lee Soo, Viswanadham Vinary, Dou Yanmei, Chess Andrew J., Jones Attila, Rosenbluh Chaggai, Akbarian Schahram, Langmead Ben, Thorpe Jeremy, Cho Sean, Abyzov Alexej, Bae Taejeong, Jang Yeongjun, Wang Yifan, Molitor Cindy, Peters Mette, Gage Fred H., Wang Meiyan, Reed Patrick, Linker Sara, Urban Alexander, Zhou Bo, Pattni Reenal, Zhu Xiaowei, Amero Aitor Serres, Juan David, Povolotskaya Inna, Lobon Irene, Moruno Manuel Solis, Perez Raquel Garcia, Marques-Bonet Tomas, Soriano Eduardo, Moran John V., Flasch Diane A., Frisbie Trenton J., Kopera Huira C., Moldovan John B., Kwan Kenneth Y., Mills Ryan E., Zhou Weichen, Zhao Xuefang, Ratan Aakrosh, Vaccarino Flora M., Cherskov Adriana, Jourdon Alexandre, Fasching Liana, Sestan Nenad, Pochareddy Sirisha, Scuder Soraya, Weinberger Daniel R.ORCID, Moran John V.ORCID, Kidd Jeffrey M.ORCID, Mills Ryan E.ORCID, McConnell Michael J.ORCID
Abstract
AbstractWhen somatic cells acquire complex karyotypes, they often are removed by the immune system. Mutant somatic cells that evade immune surveillance can lead to cancer. Neurons with complex karyotypes arise during neurotypical brain development, but neurons are almost never the origin of brain cancers. Instead, somatic mutations in neurons can bring about neurodevelopmental disorders, and contribute to the polygenic landscape of neuropsychiatric and neurodegenerative disease. A subset of human neurons harbors idiosyncratic copy number variants (CNVs, “CNV neurons”), but previous analyses of CNV neurons are limited by relatively small sample sizes. Here, we develop an allele-based validation approach, SCOVAL, to corroborate or reject read-depth based CNV calls in single human neurons. We apply this approach to 2,125 frontal cortical neurons from a neurotypical human brain. SCOVAL identifies 226 CNV neurons, which include a subclass of 65 CNV neurons with highly aberrant karyotypes containing whole or substantial losses on multiple chromosomes. Moreover, we find that CNV location appears to be nonrandom. Recurrent regions of neuronal genome rearrangement contain fewer, but longer, genes.
Funder
U.S. Department of Health & Human Services | NIH | National Institute of Mental Health
Publisher
Springer Science and Business Media LLC
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