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Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation

Common genetic risk for neuropsychiatric disorders is enriched in regulatory elements active during cortical neurogenesis. However, it remains poorly understood how these variants influence gene regulation. To model the functional impact of common genetic variation on the non-coding genome during hu...

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Autores principales: Liang, Dan, Elwell, Angela L., Aygün, Nil, Krupa, Oleh, Wolter, Justin M., Kyere, Felix A., Lafferty, Michael J., Cheek, Kerry E., Courtney, Kenan P., Yusupova, Marianna, Garrett, Melanie E., Ashley-Koch, Allison, Crawford, Gregory E., Love, Michael I., de la Torre-Ubieta, Luis, Geschwind, Daniel H., Stein, Jason L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8254789/
https://www.ncbi.nlm.nih.gov/pubmed/34017130
http://dx.doi.org/10.1038/s41593-021-00858-w
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author Liang, Dan
Elwell, Angela L.
Aygün, Nil
Krupa, Oleh
Wolter, Justin M.
Kyere, Felix A.
Lafferty, Michael J.
Cheek, Kerry E.
Courtney, Kenan P.
Yusupova, Marianna
Garrett, Melanie E.
Ashley-Koch, Allison
Crawford, Gregory E.
Love, Michael I.
de la Torre-Ubieta, Luis
Geschwind, Daniel H.
Stein, Jason L.
author_facet Liang, Dan
Elwell, Angela L.
Aygün, Nil
Krupa, Oleh
Wolter, Justin M.
Kyere, Felix A.
Lafferty, Michael J.
Cheek, Kerry E.
Courtney, Kenan P.
Yusupova, Marianna
Garrett, Melanie E.
Ashley-Koch, Allison
Crawford, Gregory E.
Love, Michael I.
de la Torre-Ubieta, Luis
Geschwind, Daniel H.
Stein, Jason L.
author_sort Liang, Dan
collection PubMed
description Common genetic risk for neuropsychiatric disorders is enriched in regulatory elements active during cortical neurogenesis. However, it remains poorly understood how these variants influence gene regulation. To model the functional impact of common genetic variation on the non-coding genome during human cortical development, we performed ATAC-seq and analyzed chromatin accessibility quantitative trait loci in cultured human neural progenitor cells and their differentiated neuronal progeny from 92 donors. We identified significant genetic effects on 988/1,839 neuron/progenitor regulatory elements, with highly cell-type and temporally specific effects. A subset (~30%) of caQTLs were also associated with changes in gene expression. Motif-disrupting alleles of transcriptional activators generally led to decreases in chromatin accessibility, whereas motif-disrupting alleles of repressors led to increases in chromatin accessibility. By integrating cell-type specific caQTLs and brain-relevant genome-wide association data, we were able to fine-map and identify regulatory mechanisms underlying non-coding neuropsychiatric disorder risk loci.
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spelling pubmed-82547892021-11-20 Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation Liang, Dan Elwell, Angela L. Aygün, Nil Krupa, Oleh Wolter, Justin M. Kyere, Felix A. Lafferty, Michael J. Cheek, Kerry E. Courtney, Kenan P. Yusupova, Marianna Garrett, Melanie E. Ashley-Koch, Allison Crawford, Gregory E. Love, Michael I. de la Torre-Ubieta, Luis Geschwind, Daniel H. Stein, Jason L. Nat Neurosci Article Common genetic risk for neuropsychiatric disorders is enriched in regulatory elements active during cortical neurogenesis. However, it remains poorly understood how these variants influence gene regulation. To model the functional impact of common genetic variation on the non-coding genome during human cortical development, we performed ATAC-seq and analyzed chromatin accessibility quantitative trait loci in cultured human neural progenitor cells and their differentiated neuronal progeny from 92 donors. We identified significant genetic effects on 988/1,839 neuron/progenitor regulatory elements, with highly cell-type and temporally specific effects. A subset (~30%) of caQTLs were also associated with changes in gene expression. Motif-disrupting alleles of transcriptional activators generally led to decreases in chromatin accessibility, whereas motif-disrupting alleles of repressors led to increases in chromatin accessibility. By integrating cell-type specific caQTLs and brain-relevant genome-wide association data, we were able to fine-map and identify regulatory mechanisms underlying non-coding neuropsychiatric disorder risk loci. 2021-05-20 2021-07 /pmc/articles/PMC8254789/ /pubmed/34017130 http://dx.doi.org/10.1038/s41593-021-00858-w Text en http://www.nature.com/authors/editorial_policies/license.html#termsUsers may view, print, copy, and download 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
Liang, Dan
Elwell, Angela L.
Aygün, Nil
Krupa, Oleh
Wolter, Justin M.
Kyere, Felix A.
Lafferty, Michael J.
Cheek, Kerry E.
Courtney, Kenan P.
Yusupova, Marianna
Garrett, Melanie E.
Ashley-Koch, Allison
Crawford, Gregory E.
Love, Michael I.
de la Torre-Ubieta, Luis
Geschwind, Daniel H.
Stein, Jason L.
Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation
title Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation
title_full Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation
title_fullStr Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation
title_full_unstemmed Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation
title_short Cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation
title_sort cell-type specific effects of genetic variation on chromatin accessibility during human neuronal differentiation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8254789/
https://www.ncbi.nlm.nih.gov/pubmed/34017130
http://dx.doi.org/10.1038/s41593-021-00858-w
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