4.4 Article

Isotropic myosin-generated tissue tension is required for the dynamic orientation of the mitotic spindle

Journal

MOLECULAR BIOLOGY OF THE CELL
Volume 31, Issue 13, Pages 1370-1379

Publisher

AMER SOC CELL BIOLOGY
DOI: 10.1091/mbc.E19-09-0545

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Funding

  1. Agency for Science, Technology and Research (Singapore)
  2. Wellcome Trust Developmental and Stem Cell Biology PhD program
  3. MRC [MC_CF12266]
  4. Cancer Research UK [C1529/A1734]
  5. Biological Sciences Research Council (BBSRC) [BB/J008532/1, BB/K009001/1]
  6. European Research Council (MolCellTissMech) [647186]
  7. Medical Research Council Fellowship [MR/L009056/1]
  8. UCL Excellence Fellowship
  9. EMBO long-term postdoctoral fellowship [29-2016]
  10. BBSRC [BB/K009001/1, BB/J008532/1, BB/R009732/1] Funding Source: UKRI

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The ability of cells to divide along their longest axis has been proposed to play an important role in maintaining epithelial tissue homeostasis in many systems. Because the division plane is largely set by the position of the anaphase spindle, it is important to understand how spindles become oriented. While several molecules have been identified that play key roles in spindle orientation across systems, most notably Mud/NuMA and cortical dynein, the precise mechanism by which spindles detect and align with the long cell axis remain poorly understood. Here, in exploring the dynamics of spindle orientation in mechanically distinct regions of the fly notum, we find that the ability of cells to properly reorient their divisions depends on local tissue tension. Thus, spindles reorient to align with the long cell axis in regions where isotropic tension is elevated, but fail to do so in elongated cells within the crowded midline, where tension is low, or in regions that have been mechanically isolated from the rest of the tissue via laser ablation. Importantly, these differences in spindle behavior outside and inside the midline can be recapitulated by corresponding changes in tension induced by perturbations that alter nonmuscle myosin II activity. These data lead us to propose that isotropic tension within an epithelium provides cells with a mechanically stable substrate upon which localized cortical motor complexes can act on astral microtubules to orient the spindle.

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