Precise temporal control of neuroblast migration through combined regulation and feedback of a Wnt receptor

Erik S. Schild, Shivam Gupta, Clément Dubois, Euclides E. Fernandes Póvoa, Marie Anne Félix, Andrew Mugler*, Hendrik C. Korswagen*

*Corresponding author for this work

Research output: Contribution to journalArticleAcademicpeer-review

Abstract

Many developmental processes depend on precise temporal control of gene expres-sion. We have previously established a theoretical framework for regulatory strategies that can govern such high temporal precision, but experimental validation of these predictions was still lacking. Here, we use the time-dependent expression of a Wnt receptor that controls neuroblast migration in Caenorhabditis elegans as a tractable system to study a robust, cell-intrinsic timing mechanism in vivo. Single-molecule mRNA quantification showed that the expression of the receptor increases non-linearly, a dynamic that is predicted to enhance timing precision over an unregulated, linear increase in timekeeper abundance. We show that this upregulation depends on transcriptional activation, providing in vivo evidence for a model in which the timing of receptor expression is regulated through an accumulating activator that triggers expression when a specific threshold is reached. This timing mechanism acts across a cell division that occurs in the neuroblast lineage and is influenced by the asymmetry of the division. Finally, we show that positive feedback oreceptor expression through the canonical Wnt pathway enhances temporal precision. We conclude that robust cell-intrinsic timing can be achieved by combining regulation and feedback of the timekeeper gene.

Original languageEnglish
Article numbere82675
JournaleLife
Volume12
DOIs
Publication statusPublished - May 2023

Bibliographical note

Publisher Copyright:
© 2023, eLife Sciences Publications Ltd. All rights reserved.

Funding

We thank the Hubrecht Imaging Center for technical support. This work was funded by the Human Frontier Science Program Grant RGP0030/2016 to AM, MAF, and HCK and grants from the Simons Foundation (376198) and the National Science Foundation (PHY-1945018) to SG and AM. Some strains were provided by the CGC, which is funded by the NIH Office of Research Infrastructure Programs (P40 OD010440). We are grateful to Damien Coudreuse and members of the Korswagen and Galli groups for helpful discussions and critical reading of the manuscript.

FundersFunder number
Damien Coudreuse
National Science FoundationPHY-1945018
National Institutes of HealthP40 OD010440
Simons Foundation376198
Human Frontier Science ProgramRGP0030/2016

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