Enhanced Preprints

The Geometric Basis of Epithelial Convergent Extension

  1. Fridtjof Brauns author has email address
  2. Nikolas H. Claussen
  3. Eric F. Wieschaus
  4. Boris I. Shraiman author has email address
  1. Kavli Institute for Theoretical Physics, University of California Santa Barbara, Santa Barbara, California 93106, USA
  2. Department of Physics, University of California Santa Barbara, Santa Barbara, California 93106, USA
  3. Department of Molecular Biology, Princeton University, Princeton, NJ, USA; The Lewis-Sigler Institute for Integrative Genomics, Princeton University, Princeton, NJ, USA

Editors

  • Reviewing Editor
    Michel Bagnat
    Duke University, Durham, United States of America
  • Senior Editor
    Felix Campelo
    Institute of Photonic Sciences, Barcelona, Spain

Joint Public Review:

Summary:

Brauns et al. work to decipher the respective contribution of active versus passive contributions to cell shape changes during germ band elongation. Using a novel quantification tool of local tension, their results suggest that epithelial convergent extension results from internal forces.

Strengths:

The approach developed here, tension isogonal decomposition, is original and the authors made the demonstration that we can extract comprehensive data on tissue mechanics from this type of analysis.

They present an elegant diagram that quantifies how active and passive forces interact to drive cell intercalations.

The model qualitatively recapitulates the features of passive and active intercalation for a T1 event.

Regions of high isogonal strains are consistent with the proximity of known active regions.

They define a parameter (the LTC parameter) which encompasses the geometry of the tension triangles and allows the authors to define a criterium for T1s to occur.

The data are clearly presented, going from cellular scale to tissue scale, and integrating modeling approach to complement the thoughtful description of tension patterns.

Weaknesses:

The modeling is interesting, with the integration of tension through tension triangulation around vertices and thus integrating force inference directly in the vertex model. However, the authors are not using it to test their hypothesis and support their analysis at the tissue level. Thus, although interesting, the analysis at the tissue level stays mainly descriptive.

Major points:

(1) The authors mention that from their analysis, they can predict what is the tension threshold required for intercalations in different conditions and predict that in Snail and Twist mutants the T1 tension threshold would be around √2. Since movies of these mutants are most probably available, it would be nice to confirm these predictions.

(2) While the formalism is very elegant and convincing, and also convincingly allows making sense of the data presented in the paper, it is not all that clear whether the claims are compatible with previous experimental observations. In particular, it has been reported in different papers (including Collinet et al NCB 2015, Clement et al Curr Biol 2017) that affecting the initial Myosin polarity or the rate of T1s does not affect tissue-scale convergent extension. Analysis/discussion of the Tor phenotype (no extension with myosin anisotropy) and the Eve/Runt phenotype (extension without Myosin anisotropy), which seem in contradiction with an extension mostly driven by myosin anisotropy.

  1. Howard Hughes Medical Institute
  2. Wellcome Trust
  3. Max-Planck-Gesellschaft
  4. Knut and Alice Wallenberg Foundation