Cicero Predicts cis-Regulatory DNA Interactions from Single-Cell Chromatin Accessibility Data

Hannah A. Pliner; Jonathan S. Packer; José L. McFaline-Figueroa; Darren A. Cusanovich; Riza M. Daza; Delasa Aghamirzaie; Sanjay Srivatsan; Xiaojie Qiu; Dana Jackson; Anna Minkina; Andrew C. Adey; Frank J. Steemers; Jay Shendure; Cole Trapnell

doi:10.1016/j.molcel.2018.06.044

Cicero Predicts cis-Regulatory DNA Interactions from Single-Cell Chromatin Accessibility Data

Hannah A. Pliner, Jonathan S. Packer, José L. McFaline-Figueroa, Darren A. Cusanovich, Riza M. Daza, Delasa Aghamirzaie, Sanjay Srivatsan, Xiaojie Qiu, Dana Jackson, Anna Minkina, Andrew C. Adey, Frank J. Steemers, Jay Shendure, Cole Trapnell

Molecular and Medical Genetics

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

345 Scopus citations

Abstract

Linking regulatory DNA elements to their target genes, which may be located hundreds of kilobases away, remains challenging. Here, we introduce Cicero, an algorithm that identifies co-accessible pairs of DNA elements using single-cell chromatin accessibility data and so connects regulatory elements to their putative target genes. We apply Cicero to investigate how dynamically accessible elements orchestrate gene regulation in differentiating myoblasts. Groups of Cicero-linked regulatory elements meet criteria of “chromatin hubs”—they are enriched for physical proximity, interact with a common set of transcription factors, and undergo coordinated changes in histone marks that are predictive of changes in gene expression. Pseudotemporal analysis revealed that most DNA elements remain in chromatin hubs throughout differentiation. A subset of elements bound by MYOD1 in myoblasts exhibit early opening in a PBX1- and MEIS1-dependent manner. Our strategy can be applied to dissect the architecture, sequence determinants, and mechanisms of cis-regulation on a genome-wide scale. Pliner et al. introduce Cicero, a software program to connect distal regulatory elements with target genes using single-cell ATAC-seq data. They find evidence that groups of co-accessible elements form chromatin hubs and undergo coordinated changes in histone marks that are predictive of changes in gene expression in skeletal muscle development.

Original language	English (US)
Pages (from-to)	858-871.e8
Journal	Molecular Cell
Volume	71
Issue number	5
DOIs	https://doi.org/10.1016/j.molcel.2018.06.044
State	Published - Sep 6 2018

Keywords

ATAC-seq
chromatin accessibility
co-accessibility
gene regulation
machine learning
myoblast differentiation
single-cell

ASJC Scopus subject areas

Molecular Biology
Cell Biology

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10.1016/j.molcel.2018.06.044

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Pliner, H. A., Packer, J. S., McFaline-Figueroa, J. L., Cusanovich, D. A., Daza, R. M., Aghamirzaie, D., Srivatsan, S., Qiu, X., Jackson, D., Minkina, A., Adey, A. C., Steemers, F. J., Shendure, J., & Trapnell, C. (2018). Cicero Predicts cis-Regulatory DNA Interactions from Single-Cell Chromatin Accessibility Data. Molecular Cell, 71(5), 858-871.e8. https://doi.org/10.1016/j.molcel.2018.06.044

Pliner, HA, Packer, JS, McFaline-Figueroa, JL, Cusanovich, DA, Daza, RM, Aghamirzaie, D, Srivatsan, S, Qiu, X, Jackson, D, Minkina, A, Adey, AC, Steemers, FJ, Shendure, J & Trapnell, C 2018, 'Cicero Predicts cis-Regulatory DNA Interactions from Single-Cell Chromatin Accessibility Data', Molecular Cell, vol. 71, no. 5, pp. 858-871.e8. https://doi.org/10.1016/j.molcel.2018.06.044

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abstract = "Linking regulatory DNA elements to their target genes, which may be located hundreds of kilobases away, remains challenging. Here, we introduce Cicero, an algorithm that identifies co-accessible pairs of DNA elements using single-cell chromatin accessibility data and so connects regulatory elements to their putative target genes. We apply Cicero to investigate how dynamically accessible elements orchestrate gene regulation in differentiating myoblasts. Groups of Cicero-linked regulatory elements meet criteria of “chromatin hubs”—they are enriched for physical proximity, interact with a common set of transcription factors, and undergo coordinated changes in histone marks that are predictive of changes in gene expression. Pseudotemporal analysis revealed that most DNA elements remain in chromatin hubs throughout differentiation. A subset of elements bound by MYOD1 in myoblasts exhibit early opening in a PBX1- and MEIS1-dependent manner. Our strategy can be applied to dissect the architecture, sequence determinants, and mechanisms of cis-regulation on a genome-wide scale. Pliner et al. introduce Cicero, a software program to connect distal regulatory elements with target genes using single-cell ATAC-seq data. They find evidence that groups of co-accessible elements form chromatin hubs and undergo coordinated changes in histone marks that are predictive of changes in gene expression in skeletal muscle development.",

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AU - Pliner, Hannah A.

AU - Packer, Jonathan S.

AU - McFaline-Figueroa, José L.

AU - Cusanovich, Darren A.

AU - Daza, Riza M.

AU - Aghamirzaie, Delasa

AU - Srivatsan, Sanjay

AU - Qiu, Xiaojie

AU - Jackson, Dana

AU - Minkina, Anna

AU - Adey, Andrew C.

AU - Steemers, Frank J.

AU - Shendure, Jay

AU - Trapnell, Cole

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AB - Linking regulatory DNA elements to their target genes, which may be located hundreds of kilobases away, remains challenging. Here, we introduce Cicero, an algorithm that identifies co-accessible pairs of DNA elements using single-cell chromatin accessibility data and so connects regulatory elements to their putative target genes. We apply Cicero to investigate how dynamically accessible elements orchestrate gene regulation in differentiating myoblasts. Groups of Cicero-linked regulatory elements meet criteria of “chromatin hubs”—they are enriched for physical proximity, interact with a common set of transcription factors, and undergo coordinated changes in histone marks that are predictive of changes in gene expression. Pseudotemporal analysis revealed that most DNA elements remain in chromatin hubs throughout differentiation. A subset of elements bound by MYOD1 in myoblasts exhibit early opening in a PBX1- and MEIS1-dependent manner. Our strategy can be applied to dissect the architecture, sequence determinants, and mechanisms of cis-regulation on a genome-wide scale. Pliner et al. introduce Cicero, a software program to connect distal regulatory elements with target genes using single-cell ATAC-seq data. They find evidence that groups of co-accessible elements form chromatin hubs and undergo coordinated changes in histone marks that are predictive of changes in gene expression in skeletal muscle development.

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Cicero Predicts cis-Regulatory DNA Interactions from Single-Cell Chromatin Accessibility Data

Abstract

Keywords

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