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A single-cell atlas of entorhinal cortex from individuals with Alzheimer’s disease reveals cell-type-specific gene expression regulation

A single-cell atlas of entorhinal cortex from individuals with Alzheimer’s disease reveals cell-type-specific gene expression regulation
A single-cell atlas of entorhinal cortex from individuals with Alzheimer’s disease reveals cell-type-specific gene expression regulation
There is currently little information available about how individual cell types contribute to Alzheimer’s disease. Here we applied single-nucleus RNA sequencing to entorhinal cortex samples from control and Alzheimer’s disease brains (n = 6 per group), yielding a total of 13,214 high-quality nuclei. We detail cell-type-specific gene expression patterns, unveiling how transcriptional changes in specific cell subpopulations are associated with Alzheimer’s disease. We report that the Alzheimer’s disease risk gene APOE is specifically repressed in Alzheimer’s disease oligodendrocyte progenitor cells and astrocyte subpopulations and upregulated in an Alzheimer’s disease-specific microglial subopulation. Integrating transcription factor regulatory modules with Alzheimer’s disease risk loci revealed drivers of cell-type-specific state transitions towards Alzheimer’s disease. For example, transcription factor EB, a master regulator of lysosomal function, regulates multiple disease genes in a specific Alzheimer’s disease astrocyte subpopulation. These results provide insights into the coordinated control of Alzheimer’s disease risk genes and their cell-type-specific contribution to disease susceptibility. These results are available at http://adsn.ddnetbio.com.
1097-6256
2087-2097
Grubman, Alexandra
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Chew, Gabriel
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Ouyang, John F.
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Sun, Guizhi
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Choo, Xin Yi
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Mclean, Catriona
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Simmons, Rebecca K.
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Buckberry, Sam
fe0c626c-699f-4858-9572-5b1af9b18814
Vargas-Landin, Dulce B.
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Poppe, Daniel
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Pflueger, Jahnvi
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Lister, Ryan
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Rackham, Owen J. L.
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Petretto, Enrico
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Polo, Jose M.
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Grubman, Alexandra
f441d27d-645c-4c8f-8cd1-64f5fece12e8
Chew, Gabriel
714c40fe-c98e-401a-adec-0e02fb23e2c5
Ouyang, John F.
ce6f93a5-b40f-4add-8d7b-3ae795c1a4cb
Sun, Guizhi
ee9e9d6a-2b33-41f8-8fd4-f6eb5f4a074f
Choo, Xin Yi
fbedbb3e-1e79-4729-9258-ae909b0425f4
Mclean, Catriona
4b12c940-0c08-4f6f-8859-86f02b99de74
Simmons, Rebecca K.
3430aa3e-0728-43b0-a3ab-21f6ab5de794
Buckberry, Sam
fe0c626c-699f-4858-9572-5b1af9b18814
Vargas-Landin, Dulce B.
1ac45b9f-4720-4537-b55d-a783ecb39afa
Poppe, Daniel
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Pflueger, Jahnvi
f4cfe097-8ed8-4669-952e-2591447c5fca
Lister, Ryan
7044ae6b-cc46-4912-aa85-243f98f45cf7
Rackham, Owen J. L.
8122eb1f-6e9f-4da5-90e1-ce108ccbbcbf
Petretto, Enrico
a8a7d254-ea06-4ab3-ba7e-b653349a29f4
Polo, Jose M.
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Grubman, Alexandra, Chew, Gabriel, Ouyang, John F., Sun, Guizhi, Choo, Xin Yi, Mclean, Catriona, Simmons, Rebecca K., Buckberry, Sam, Vargas-Landin, Dulce B., Poppe, Daniel, Pflueger, Jahnvi, Lister, Ryan, Rackham, Owen J. L., Petretto, Enrico and Polo, Jose M. (2019) A single-cell atlas of entorhinal cortex from individuals with Alzheimer’s disease reveals cell-type-specific gene expression regulation. Nature Neuroscience, 22 (12), 2087-2097. (doi:10.1038/s41593-019-0539-4).

Record type: Article

Abstract

There is currently little information available about how individual cell types contribute to Alzheimer’s disease. Here we applied single-nucleus RNA sequencing to entorhinal cortex samples from control and Alzheimer’s disease brains (n = 6 per group), yielding a total of 13,214 high-quality nuclei. We detail cell-type-specific gene expression patterns, unveiling how transcriptional changes in specific cell subpopulations are associated with Alzheimer’s disease. We report that the Alzheimer’s disease risk gene APOE is specifically repressed in Alzheimer’s disease oligodendrocyte progenitor cells and astrocyte subpopulations and upregulated in an Alzheimer’s disease-specific microglial subopulation. Integrating transcription factor regulatory modules with Alzheimer’s disease risk loci revealed drivers of cell-type-specific state transitions towards Alzheimer’s disease. For example, transcription factor EB, a master regulator of lysosomal function, regulates multiple disease genes in a specific Alzheimer’s disease astrocyte subpopulation. These results provide insights into the coordinated control of Alzheimer’s disease risk genes and their cell-type-specific contribution to disease susceptibility. These results are available at http://adsn.ddnetbio.com.

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More information

Accepted/In Press date: 1 November 2019
e-pub ahead of print date: 25 November 2019
Published date: 1 December 2019

Identifiers

Local EPrints ID: 444311
URI: http://eprints.soton.ac.uk/id/eprint/444311
ISSN: 1097-6256
PURE UUID: 9965e198-8bc2-421d-a885-4613b3a3dab8
ORCID for Owen J. L. Rackham: ORCID iD orcid.org/0000-0002-4390-0872

Catalogue record

Date deposited: 12 Oct 2020 16:31
Last modified: 17 Mar 2024 04:03

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Contributors

Author: Alexandra Grubman
Author: Gabriel Chew
Author: John F. Ouyang
Author: Guizhi Sun
Author: Xin Yi Choo
Author: Catriona Mclean
Author: Rebecca K. Simmons
Author: Sam Buckberry
Author: Dulce B. Vargas-Landin
Author: Daniel Poppe
Author: Jahnvi Pflueger
Author: Ryan Lister
Author: Enrico Petretto
Author: Jose M. Polo

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