| Literature DB >> 34163074 |
Daniela J Di Bella1,2, Ehsan Habibi1,3, Robert R Stickels2, Gabriele Scalia3, Juliana Brown1,2, Payman Yadollahpour3, Sung Min Yang1,2, Catherine Abbate1,2, Tommaso Biancalani3,4, Evan Z Macosko2, Fei Chen1,2, Aviv Regev5,6,7, Paola Arlotta8,9.
Abstract
The mammalian cerebral cortex has an unparalleled diversity of cell types, which are generated during development through a series of temporally orchestrated events that are under tight evolutionary constraint and are critical for proper cortical assembly and function1,2. However, the molecular logic that governs the establishment and organization of cortical cell types remains unknown, largely due to the large number of cell classes that undergo dynamic cell-state transitions over extended developmental timelines. Here we generate a comprehensive atlas of the developing mouse neocortex, using single-cell RNA sequencing and single-cell assay for transposase-accessible chromatin using sequencing. We sampled the neocortex every day throughout embryonic corticogenesis and at early postnatal ages, and complemented the sequencing data with a spatial transcriptomics time course. We computationally reconstruct developmental trajectories across the diversity of cortical cell classes, and infer their spatial organization and the gene regulatory programs that accompany their lineage bifurcation decisions and differentiation trajectories. Finally, we demonstrate how this developmental map pinpoints the origin of lineage-specific developmental abnormalities that are linked to aberrant corticogenesis in mutant mice. The data provide a global picture of the regulatory mechanisms that govern cellular diversification in the neocortex.Entities:
Mesh:
Substances:
Year: 2021 PMID: 34163074 PMCID: PMC9006333 DOI: 10.1038/s41586-021-03670-5
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962