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Abstract Time-series single-cell RNA sequencing (scRNA-seq) datasets provide unprecedented opportunities to learn dynamic processes of cellular systems. Due to the destructive nature of sequencing, it remains challenging to link the scRNA-seq snapshots sampled at different time points. Here we present TIGON, a dynamic, unbalanced optimal transport algorithm that reconstructs dynamic trajectories and population growth simultaneously as well as the underlying gene regulatory network from multiple snapshots. To tackle the high-dimensional optimal transport problem, we introduce a deep learning method using a dimensionless formulation based on the Wasserstein–Fisher–Rao (WFR) distance. TIGON is evaluated on simulated data and compared with existing methods for its robustness and accuracy in predicting cell state transition and cell population growth. Using three scRNA-seq datasets, we show the importance of growth in the temporal inference, TIGON’s capability in reconstructing gene expression at unmeasured time points and its applications to temporal gene regulatory networks and cell–cell communication inference.
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Dissecting crosstalk induced by cell-cell communication using single-cell transcriptomic data
Abstract During cell-cell communication (CCC), pathways activated by different ligand-receptor pairs may have crosstalk with each other. While multiple methods have been developed to infer CCC networks and their downstream response using single-cell RNA-seq data (scRNA-seq), the potential crosstalk between pathways connecting CCC with its downstream targets has been ignored. Here we introduce a machine learning-based method SigXTalk to analyze the crosstalk using scRNA-seq data by quantifying signal fidelity and specificity, two critical quantities measuring the effect of crosstalk. Specifically, a hypergraph learning method is used to encode the higher-order relations among receptors, transcription factors and target genes within regulatory pathways. Benchmarking of SigXTalk using simulation and real-world data shows the effectiveness, robustness, and accuracy in identifying key shared molecules among crosstalk pathways and their roles in transferring shared CCC information. Analysis of disease data shows SigXTalk’s capability in identifying crucial signals, targets, regulatory networks, and CCC patterns that distinguish different disease conditions. Applications to the data with multiple time points reveals SigXTalk’s capability in tracking the evolution of crosstalk pathways over time. Together our studies provide a systematic analysis of CCC-induced regulatory networks from the perspective of crosstalk between pathways.
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- Award ID(s):
- 2134916
- PAR ID:
- 10611764
- Publisher / Repository:
- Nature Publishing Group
- Date Published:
- Journal Name:
- Nature Communications
- Volume:
- 16
- Issue:
- 1
- ISSN:
- 2041-1723
- Format(s):
- Medium: X
- Sponsoring Org:
- National Science Foundation
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