Single-Cell Dna Methylome and 3D Multi-Omic Atlas of the Adult Mouse Brain

Authors

Hanqing Liu
Qiurui Zeng
Jingtian Zhou
Anna Bartlett
Bang-An Wang
Peter Berube
Wei Tian
Mia Kenworthy
Jordan Altshul
Joseph R Nery
Huaming Chen
Rosa G Castanon
Songpeng Zu
Yang Eric Li
Jacinta Lucero
Julia K Osteen
Antonio Pinto-Duarte
Jasper Lee
Jon Rink
Silvia Cho
Nora Emerson
Michael Nunn
Carolyn O'Connor
Zhanghao Wu
Ion Stoica
Zizhen Yao
Kimberly A Smith
Bosiljka Tasic
Chongyuan Luo
Jesse R Dixon
Hongkui Zeng
Bing Ren
M Margarita Behrens
Joseph R Ecker

Publication Date

12-1-2023

Journal

Nature

Abstract

Cytosine DNA methylation is essential in brain development and is implicated in various neurological disorders. Understanding DNA methylation diversity across the entire brain in a spatial context is fundamental for a complete molecular atlas of brain cell types and their gene regulatory landscapes. Here we used single-nucleus methylome sequencing (snmC-seq3) and multi-omic sequencing (snm3C-seq)1 technologies to generate 301,626 methylomes and 176,003 chromatin conformation–methylome joint profiles from 117 dissected regions throughout the adult mouse brain. Using iterative clustering and integrating with companion whole-brain transcriptome and chromatin accessibility datasets, we constructed a methylation-based cell taxonomy with 4,673 cell groups and 274 cross-modality-annotated subclasses. We identified 2.6 million differentially methylated regions across the genome that represent potential gene regulation elements. Notably, we observed spatial cytosine methylation patterns on both genes and regulatory elements in cell types within and across brain regions. Brain-wide spatial transcriptomics data validated the association of spatial epigenetic diversity with transcription and improved the anatomical mapping of our epigenetic datasets. Furthermore, chromatin conformation diversities occurred in important neuronal genes and were highly associated with DNA methylation and transcription changes. Brain-wide cell-type comparisons enabled the construction of regulatory networks that incorporate transcription factors, regulatory elements and their potential downstream gene targets. Finally, intragenic DNA methylation and chromatin conformation patterns predicted alternative gene isoform expression observed in a whole-brain SMART-seq2 dataset. Our study establishes a brain-wide, single-cell DNA methylome and 3D multi-omic atlas and provides a valuable resource for comprehending the cellular–spatial and regulatory genome diversity of the mouse brain.

Keywords

Animals, Mice, Brain, Chromatin, Cytosine, Datasets as Topic, DNA Methylation, Epigenome, Multiomics, Single-Cell Analysis, Transcription Factors, Transcription, Genetic, Epigenetics in the nervous system, Molecular neuroscience, DNA methylation, Chromatin structure

Comments

Supplementary Materials

PMID: 38092913