Active nuclear positioning and actomyosin contractility maintain leader cell integrity during gonadogenesis

Priti Agarwal*, Simon Berger, Tom Shemesh, Ronen Zaidel-Bar*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

3 Scopus citations

Abstract

Proper distribution of organelles can play an important role in a moving cell's performance. During C. elegans gonad morphogenesis, the nucleus of the leading distal tip cell (DTC) is always found at the front, yet the significance of this localization is unknown. Here, we identified the molecular mechanism that keeps the nucleus at the front, despite a frictional force that pushes it backward. The Klarsicht/ANC-1/Syne homology (KASH) domain protein UNC-83 links the nucleus to the motor protein kinesin-1 that moves along a polarized acentrosomal microtubule network. Interestingly, disrupting nuclear positioning on its own did not affect gonad morphogenesis. However, reducing actomyosin contractility on top of nuclear mispositioning led to a dramatic phenotype: DTC splitting and gonad bifurcation. Long-term live imaging of the double knockdown revealed that, while the gonad attempted to perform a planned U-turn, the DTC was stretched due to the lagging nucleus until it fragmented into a nucleated cell and an enucleated cytoplast, each leading an independent gonadal arm. Remarkably, the enucleated cytoplast had polarity and invaded, but it could only temporarily support germ cell proliferation. Based on a qualitative biophysical model, we conclude that the leader cell employs two complementary mechanical approaches to preserve its integrity and ensure proper organ morphogenesis while navigating through a complex 3D environment: active nuclear positioning by microtubule motors and actomyosin-driven cortical contractility.

Original languageEnglish
Pages (from-to)2373-2386.e5
JournalCurrent Biology
Volume34
Issue number11
DOIs
StatePublished - 3 Jun 2024

Funding

FundersFunder number
Israel Science Foundation3308/20, 767/20
United States - Israel Binational Science Foundation2021014, 2751/20

    Keywords

    • C. elegans
    • LINC complex
    • cell migration
    • cytoskeleton
    • development
    • gonad
    • mechanobiology
    • microtubules
    • morphogenesis
    • nucleus

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