| Literature DB >> 30936567 |
David S Fischer1,2, Anna K Fiedler1,3, Eric M Kernfeld4, Ryan M J Genga4, Aimée Bastidas-Ponce5,6,7,8, Mostafa Bakhti5,6,8, Heiko Lickert5,6,7,8, Jan Hasenauer1,3, Rene Maehr4, Fabian J Theis9,10,11.
Abstract
Recent single-cell RNA-sequencing studies have suggested that cells follow continuous transcriptomic trajectories in an asynchronous fashion during development. However, observations of cell flux along trajectories are confounded with population size effects in snapshot experiments and are therefore hard to interpret. In particular, changes in proliferation and death rates can be mistaken for cell flux. Here we present pseudodynamics, a mathematical framework that reconciles population dynamics with the concepts underlying developmental trajectories inferred from time-series single-cell data. Pseudodynamics models population distribution shifts across trajectories to quantify selection pressure, population expansion, and developmental potentials. Applying this model to time-resolved single-cell RNA-sequencing of T-cell and pancreatic beta cell maturation, we characterize proliferation and apoptosis rates and identify key developmental checkpoints, data inaccessible to existing approaches.Entities:
Mesh:
Year: 2019 PMID: 30936567 PMCID: PMC7397487 DOI: 10.1038/s41587-019-0088-0
Source DB: PubMed Journal: Nat Biotechnol ISSN: 1087-0156 Impact factor: 54.908