Data integration and inference of gene regulation using single-cell temporal multimodal data with scTIE

  1. Y.X. Rachel Wang1,4
  1. 1 The University of Sydney;
  2. 2 Stanford University;
  3. 3 National Yang Ming Chiao Tung University
  • * Corresponding author; email: rachel.wang{at}sydney.edu.au
  • Abstract

    Single-cell technologies offer unprecedented opportunities to dissect gene regulatory mechanisms in context-specific ways. Although there are computational methods for extracting gene regulatory relationships from scRNA-seq and scATAC-seq data, the data integration problem, essential for accurate cell type identification, has been mostly treated as a standalone challenge. Here we present scTIE, a unified method that integrates temporal multimodal data and infers regulatory relationships predictive of cellular state changes. scTIE uses an autoencoder to embed cells from all time points into a common space using iterative optimal transport, followed by extracting interpretable information to predict cell trajectories. Using a variety of synthetic and real temporal multimodal datasets, we demonstrate scTIE achieves effective data integration while preserving more biological signals than existing methods, particularly in the presence of batch effects and noise. Furthermore, on the exemplar multiome dataset we generated from differentiating mouse embryonic stem cells over time, we demonstrate scTIE captures regulatory elements highly predictive of cell transition probabilities, providing new avenues to understand the regulatory landscape driving developmental processes.

    • Received April 6, 2023.
    • Accepted December 13, 2023.

    This manuscript is Open Access.

    This article, published in Genome Research, is available under a Creative Commons License (Attribution-NonCommercial 4.0 International license), as described at http://creativecommons.org/licenses/by-nc/4.0/.

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    1. Genome Res. gr.277960.123 Published by Cold Spring Harbor Laboratory Press

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