Abstract
The expansion of the neocortex, a hallmark of mammalian evolution1,2, was accompanied by an increase in cerebellar neuron numbers3. However, little is known about the evolution of the cellular programs underlying cerebellum development in mammals. In this study, we generated single-nucleus RNA-sequencing data for ~400,000 cells to trace cerebellum development from early neurogenesis to adulthood in human, mouse, and the marsupial opossum. We established a consensus classification of the cellular diversity in the developing mammalian cerebellum and validated it by spatial mapping in the fetal human cerebellum. Our cross-species analyses revealed a largely conserved developmental dynamics of cell type generation, except for Purkinje cells, where we observed an expansion of early-born subtypes in the human lineage. Global transcriptome profiles, conserved cell state markers, and gene expression trajectories across neuronal differentiation show that cerebellar cell type-defining programs have been overall preserved for at least ~160 million years. However, we also identified many orthologous genes that gained or lost expression in cerebellar neural cell types in one of the species, or evolved new expression trajectories during neuronal differentiation, indicating widespread gene repurposing at the cell type level. Altogether, our study unveils shared and lineage-specific gene expression programs governing the development of cerebellar cells, and expands our understanding of mammalian brain evolution.
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Supplementary information
Supplementary Information
This file contains Supplementary Methods and additional references.
Reporting Summary
Supplementary Tables
This file contains Supplementary Tables 1-4, 6 and 14. Supplementary Table 1: Samples and libraries. Supplementary Table 2-4: Clustering and annotation of the mouse dataset (2), human dataset (3) and opossum dataset (4). Supplementary Table 6: List of genes analysed by multiplexed single molecule fluorescence in situ hybridisation. Supplementary Table 14. List of genes that gained expression in human astroglia and are enriched in the rhombic lip and posterior ventricular zone progenitors. P-values are from one-sided hypergeometric tests with Benjamini-Hochberg adjustment.
Supplementary Table 5
Cell numbers by sequencing library and annotation categories. Libraries are described as Stage | Tissue ID | batch; and annotations as cell type | state | subtype.
Supplementary Table 7
Gene loadings on principal components 1-15 for the global (PC) and neurons-only (nPC) principal components analyses.
Supplementary Table 8
Conserved cell state marker genes.
Supplementary Table 9
Gene ontology terms associated with the conserved cell state marker genes. P-values are from one-sided hypergeometric tests with Benjamini-Hochberg adjustment for each functional database (source).
Supplementary Table 10
Standardised transcription factor regulon activity scores across cell states in mouse and human.
Supplementary Table 11
Characterization of orthologous genes for expression trajectories during Purkinje and granule cell differentiation.
Supplementary Table 12
Gene ontology terms associated with genes that exhibit trajectory changes or presence/absence (P/A) expression differences. P-values are from one-sided hypergeometric tests with Benjamini-Hochberg adjustment for each functional database (source).
Supplementary Table 13
Presence/absence (P/A) expression differences in cerebellar neural cell types across species.
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Sepp, M., Leiss, K., Murat, F. et al. Cellular development and evolution of the mammalian cerebellum.
Nature (2023). https://doi.org/10.1038/s41586-023-06884-x
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Received: 28 November 2021
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Accepted: 21 November 2023
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Published: 29 November 2023
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DOI: https://doi.org/10.1038/s41586-023-06884-x
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