Single-cell transcriptional diversity is a hallmark of developmental potential.
Gunsagar Singh GulatiShaheen S SikandarDaniel J WescheAnoop ManjunathAnjan BharadwajMark J BergerFrancisco IlaganAngera H KuoRobert W HsiehShang CaiMaider ZabalaFerenc A ScheerenNeethan A LoboDalong QianFeiqiao Brian YuFrederick M DirbasMichael F ClarkeAaron M NewmanPublished in: Science (New York, N.Y.) (2020)
Single-cell RNA sequencing (scRNA-seq) is a powerful approach for reconstructing cellular differentiation trajectories. However, inferring both the state and direction of differentiation is challenging. Here, we demonstrate a simple, yet robust, determinant of developmental potential-the number of expressed genes per cell-and leverage this measure of transcriptional diversity to develop a computational framework (CytoTRACE) for predicting differentiation states from scRNA-seq data. When applied to diverse tissue types and organisms, CytoTRACE outperformed previous methods and nearly 19,000 annotated gene sets for resolving 52 experimentally determined developmental trajectories. Additionally, it facilitated the identification of quiescent stem cells and revealed genes that contribute to breast tumorigenesis. This study thus establishes a key RNA-based feature of developmental potential and a platform for delineation of cellular hierarchies.
Keyphrases
- single cell
- rna seq
- high throughput
- genome wide
- stem cells
- gene expression
- depressive symptoms
- human health
- genome wide identification
- electronic health record
- machine learning
- dna methylation
- big data
- deep learning
- cell therapy
- risk assessment
- heat shock
- mesenchymal stem cells
- gram negative
- genome wide analysis
- multidrug resistant