3D genetic architecture of schizophrenia risk across three neuronal subtypes

Samuel K. Powell; Will Liao; Sadaf Ghorbani; Raymond Rigat; Callan O’Shea; Sarah Kammourh; Rahat Elahi; Dana Infante; PJ Michael Deans; Derek J. Le; Poonam Agarwal; Wei Qiang Seow; Novin Balafkan; Kevin C. Wang; Schahram Akbarian; Kristen J. Brennand

doi:10.1038/s41380-025-03352-y

3D genetic architecture of schizophrenia risk across three neuronal subtypes

Samuel K. Powell
, Will Liao
, Sadaf Ghorbani
, Raymond Rigat
, Callan O’Shea
, Sarah Kammourh
, Rahat Elahi
, Dana Infante
, PJ Michael Deans
, Derek J. Le
, Poonam Agarwal
, Wei Qiang Seow
, Novin Balafkan
, Kevin C. Wang
, Schahram Akbarian
, Kristen J. Brennand

Research output: Contribution to journal › Article › peer-review

Abstract

Common genetic variants associated with schizophrenia risk are concentrated in non-coding regulatory sequences, but their precise target genes are context-dependent and impacted by cell-type-specific three-dimensional spatial chromatin organization. Here, we map long-range chromosomal conformations in human dopaminergic, GABAergic, and glutamatergic neurons to track developmentally programmed shifts in the regulatory activity of schizophrenia risk loci. Large-scale repressive compartmentalization, concomitant with the emergence of hundreds of neuron-specific multi-valent chromatin architectural stripes, occurs during neuronal differentiation, with genes interconnected to genetic risk loci through these long-range chromatin structures differing in their biological roles from genes more proximal to sequences conferring heritable risk. Functional targeting of chromatin loops involving the proximal risk gene SNAP91 and the distal putative risk gene BHLHE22 altered gene expression and neuronal phenotypes. Our findings highlight the large-scale cell-type-specific reorganization of chromosomal conformations at schizophrenia risk loci during neurodevelopment and provide functional validation of selected target genes implicated in the disorder through 3D chromatin looping.

Original language	English
Journal	Molecular Psychiatry
DOIs	https://doi.org/10.1038/s41380-025-03352-y
State	Accepted/In press - 2025

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Powell, S. K., Liao, W., Ghorbani, S., Rigat, R., O’Shea, C., Kammourh, S., Elahi, R., Infante, D., Deans, PJ. M., Le, D. J., Agarwal, P., Qiang Seow, W., Balafkan, N., Wang, K. C., Akbarian, S., & Brennand, K. J. (Accepted/In press). 3D genetic architecture of schizophrenia risk across three neuronal subtypes. Molecular Psychiatry. https://doi.org/10.1038/s41380-025-03352-y

@article{1d490299a43c445aa59afed258f2b3bd,

title = "3D genetic architecture of schizophrenia risk across three neuronal subtypes",

abstract = "Common genetic variants associated with schizophrenia risk are concentrated in non-coding regulatory sequences, but their precise target genes are context-dependent and impacted by cell-type-specific three-dimensional spatial chromatin organization. Here, we map long-range chromosomal conformations in human dopaminergic, GABAergic, and glutamatergic neurons to track developmentally programmed shifts in the regulatory activity of schizophrenia risk loci. Large-scale repressive compartmentalization, concomitant with the emergence of hundreds of neuron-specific multi-valent chromatin architectural stripes, occurs during neuronal differentiation, with genes interconnected to genetic risk loci through these long-range chromatin structures differing in their biological roles from genes more proximal to sequences conferring heritable risk. Functional targeting of chromatin loops involving the proximal risk gene SNAP91 and the distal putative risk gene BHLHE22 altered gene expression and neuronal phenotypes. Our findings highlight the large-scale cell-type-specific reorganization of chromosomal conformations at schizophrenia risk loci during neurodevelopment and provide functional validation of selected target genes implicated in the disorder through 3D chromatin looping.",

author = "Powell, \{Samuel K.\} and Will Liao and Sadaf Ghorbani and Raymond Rigat and Callan O{\textquoteright}Shea and Sarah Kammourh and Rahat Elahi and Dana Infante and Deans, \{PJ Michael\} and Le, \{Derek J.\} and Poonam Agarwal and \{Qiang Seow\}, Wei and Novin Balafkan and Wang, \{Kevin C.\} and Schahram Akbarian and Brennand, \{Kristen J.\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

doi = "10.1038/s41380-025-03352-y",

language = "English",

journal = "Molecular Psychiatry",

issn = "1359-4184",

publisher = "Springer Nature",

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T1 - 3D genetic architecture of schizophrenia risk across three neuronal subtypes

AU - Powell, Samuel K.

AU - Liao, Will

AU - Ghorbani, Sadaf

AU - Rigat, Raymond

AU - O’Shea, Callan

AU - Kammourh, Sarah

AU - Elahi, Rahat

AU - Infante, Dana

AU - Deans, PJ Michael

AU - Le, Derek J.

AU - Agarwal, Poonam

AU - Qiang Seow, Wei

AU - Balafkan, Novin

AU - Wang, Kevin C.

AU - Akbarian, Schahram

AU - Brennand, Kristen J.

PY - 2025

Y1 - 2025

N2 - Common genetic variants associated with schizophrenia risk are concentrated in non-coding regulatory sequences, but their precise target genes are context-dependent and impacted by cell-type-specific three-dimensional spatial chromatin organization. Here, we map long-range chromosomal conformations in human dopaminergic, GABAergic, and glutamatergic neurons to track developmentally programmed shifts in the regulatory activity of schizophrenia risk loci. Large-scale repressive compartmentalization, concomitant with the emergence of hundreds of neuron-specific multi-valent chromatin architectural stripes, occurs during neuronal differentiation, with genes interconnected to genetic risk loci through these long-range chromatin structures differing in their biological roles from genes more proximal to sequences conferring heritable risk. Functional targeting of chromatin loops involving the proximal risk gene SNAP91 and the distal putative risk gene BHLHE22 altered gene expression and neuronal phenotypes. Our findings highlight the large-scale cell-type-specific reorganization of chromosomal conformations at schizophrenia risk loci during neurodevelopment and provide functional validation of selected target genes implicated in the disorder through 3D chromatin looping.

AB - Common genetic variants associated with schizophrenia risk are concentrated in non-coding regulatory sequences, but their precise target genes are context-dependent and impacted by cell-type-specific three-dimensional spatial chromatin organization. Here, we map long-range chromosomal conformations in human dopaminergic, GABAergic, and glutamatergic neurons to track developmentally programmed shifts in the regulatory activity of schizophrenia risk loci. Large-scale repressive compartmentalization, concomitant with the emergence of hundreds of neuron-specific multi-valent chromatin architectural stripes, occurs during neuronal differentiation, with genes interconnected to genetic risk loci through these long-range chromatin structures differing in their biological roles from genes more proximal to sequences conferring heritable risk. Functional targeting of chromatin loops involving the proximal risk gene SNAP91 and the distal putative risk gene BHLHE22 altered gene expression and neuronal phenotypes. Our findings highlight the large-scale cell-type-specific reorganization of chromosomal conformations at schizophrenia risk loci during neurodevelopment and provide functional validation of selected target genes implicated in the disorder through 3D chromatin looping.

UR - https://www.scopus.com/pages/publications/105023180470

U2 - 10.1038/s41380-025-03352-y

DO - 10.1038/s41380-025-03352-y

M3 - Article

AN - SCOPUS:105023180470

SN - 1359-4184

JO - Molecular Psychiatry

JF - Molecular Psychiatry

ER -

3D genetic architecture of schizophrenia risk across three neuronal subtypes

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