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Comparative Study
. 2024 Nov 4;59(21):2912-2930.e7.
doi: 10.1016/j.devcel.2024.07.013. Epub 2024 Aug 8.

Comparative single-cell analyses identify shared and divergent features of human and mouse kidney development

Affiliations
Comparative Study

Comparative single-cell analyses identify shared and divergent features of human and mouse kidney development

Sunghyun Kim et al. Dev Cell. .

Abstract

The mammalian kidney maintains fluid homeostasis through diverse epithelial cell types generated from nephron and ureteric progenitor cells. To extend a developmental understanding of the kidney's epithelial networks, we compared chromatin organization (single-nuclear assay for transposase-accessible chromatin sequencing [ATAC-seq]; 112,864 nuclei) and gene expression (single-cell/nuclear RNA sequencing [RNA-seq]; 109,477 cells/nuclei) in the developing human (10.6-17.6 weeks; n = 10) and mouse (post-natal day [P]0; n = 10) kidney, supplementing analysis with published mouse datasets from earlier stages. Single-cell/nuclear datasets were analyzed at a species level, and then nephron and ureteric cellular lineages were extracted and integrated into a common, cross-species, multimodal dataset. Comparative computational analyses identified conserved and divergent features of chromatin organization and linked gene activity, identifying species-specific and cell-type-specific regulatory programs. In situ validation of human-enriched gene activity points to human-specific signaling interactions in kidney development. Further, human-specific enhancer regions were linked to kidney diseases through genome-wide association studies (GWASs), highlighting the potential for clinical insight from developmental modeling.

Keywords: ATAC-seq; RNA-seq; enhancers; human; kidney development; mouse; multiomic; single cell; species specific.

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Conflict of interest statement

Declaration of interests A.P.M. is a consultant or scientific advisor to Novartis, eGENESIS, Trestle Biotherapeutics, GentiBio, and IVIVA Medical.

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