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DOI: 10.1016/j.cell.2014.04.005
¤ OpenAccess: Hybrid
This work has “Hybrid” OA status. This means it is free under an open license in a toll-access journal.

Single-Cell Trajectory Detection Uncovers Progression and Regulatory Coordination in Human B Cell Development

Sean C. Bendall,Kara L. Davis,El-ad David Amir,Michelle D. Tadmor,Erin F. Simonds,Tiffany J. Chen,Daniel K. Shenfeld,Garry P. Nolan,Dana Pe’er

Biology
Lymphopoiesis
Mass cytometry
2014
<h2>Summary</h2> Tissue regeneration is an orchestrated progression of cells from an immature state to a mature one, conventionally represented as distinctive cell subsets. A continuum of transitional cell states exists between these discrete stages. We combine the depth of single-cell mass cytometry and an algorithm developed to leverage this continuum by aligning single cells of a given lineage onto a unified trajectory that accurately predicts the developmental path de novo. Applied to human B cell lymphopoiesis, the algorithm (termed Wanderlust) constructed trajectories spanning from hematopoietic stem cells through to naive B cells. This trajectory revealed nascent fractions of B cell progenitors and aligned them with developmentally cued regulatory signaling including IL-7/STAT5 and cellular events such as immunoglobulin rearrangement, highlighting checkpoints across which regulatory signals are rewired paralleling changes in cellular state. This study provides a comprehensive analysis of human B lymphopoiesis, laying a foundation to apply this approach to other tissues and "corrupted" developmental processes including cancer.
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    Single-Cell Trajectory Detection Uncovers Progression and Regulatory Coordination in Human B Cell Development” is a paper by Sean C. Bendall Kara L. Davis El-ad David Amir Michelle D. Tadmor Erin F. Simonds Tiffany J. Chen Daniel K. Shenfeld Garry P. Nolan Dana Pe’er published in 2014. It has an Open Access status of “hybrid”. You can read and download a PDF Full Text of this paper here.