Approximated gene expression trajectories for gene regulatory network inference on cell tracks

Kay Spiess; Shannon E. Taylor; Timothy Fulton; Kane Toh; Dillan Saunders; Seongwon Hwang; Yuxuan Wang; Brooks Paige; Benjamin Steventon; Berta Verd

iScience (Sep 2024)

Approximated gene expression trajectories for gene regulatory network inference on cell tracks

Kay Spiess,
Shannon E. Taylor,
Timothy Fulton,
Kane Toh,
Dillan Saunders,
Seongwon Hwang,
Yuxuan Wang,
Brooks Paige,
Benjamin Steventon,
Berta Verd

Affiliations

Kay Spiess: Department of Genetics, University of Cambridge, Cambridge, UK; The Alan Turing Institute, London, UK
Shannon E. Taylor: Department of Biology, University of Oxford, Oxford, UK
Timothy Fulton: Department of Genetics, University of Cambridge, Cambridge, UK
Kane Toh: Department of Genetics, University of Cambridge, Cambridge, UK
Dillan Saunders: Department of Genetics, University of Cambridge, Cambridge, UK
Seongwon Hwang: Department of Genetics, University of Cambridge, Cambridge, UK
Yuxuan Wang: Department of Genetics, University of Cambridge, Cambridge, UK
Brooks Paige: The Alan Turing Institute, London, UK; Centre for Artificial Intelligence, University College London, London, UK; Corresponding author
Benjamin Steventon: Department of Genetics, University of Cambridge, Cambridge, UK; Corresponding author
Berta Verd: Department of Genetics, University of Cambridge, Cambridge, UK; Department of Biology, University of Oxford, Oxford, UK; Corresponding author

Journal volume & issue: Vol. 27, no. 9
p. 110840

Abstract

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Summary: The study of pattern formation has benefited from our ability to reverse-engineer gene regulatory network (GRN) structure from spatiotemporal quantitative gene expression data. Traditional approaches have focused on systems where the timescales of pattern formation and morphogenesis can be separated. Unfortunately, this is not the case in most animal patterning systems, where pattern formation and morphogenesis are co-occurring and tightly linked. To elucidate patterning mechanisms in such systems we need to adapt our GRN inference methodologies to include cell movements. In this work, we fill this gap by integrating quantitative data from live and fixed embryos to approximate gene expression trajectories (AGETs) in single cells and use these to reverse-engineer GRNs. This framework generates candidate GRNs that recapitulate pattern at the tissue level, gene expression dynamics at the single cell level, recover known genetic interactions and recapitulate experimental perturbations while incorporating cell movements explicitly for the first time.

Published in iScience

ISSN: 2589-0042 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Science
Website: http://www.cell.com/iscience/home

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