Amoeboid cells undergo durotaxis with soft end polarized NMIIA

Author:

Kang Chenlu123,Chen Pengcheng4,Yi Xin123,Li Dong56ORCID,Hu Yiping123,Yang Yihong57,Cai Huaqing57ORCID,Li Bo4ORCID,Wu Congying123ORCID

Affiliation:

1. Institute of Systems Biomedicine, Schol of Basic Medical Sciences, Peking University Health Science Center

2. Beijing Key Laboratory of Tumor Systems Biology, Peking University Health Science Center

3. International Cancer Institute, Peking University

4. Institute of Biomechanics and Medical Engineering, Applied Mechanics Laboratory, Department of Engineering Mechanics, Tsinghua University

5. National Laboratory of Biomacromolecules, Institute of Biophysics, Chinese Academy of Sciences

6. School of Life Sciences and Medicine, University of Science and Technology of China

7. College of Life Sciences, University of Chinese Academy of Sciences

Abstract

Cell migration towards stiff substrates has been coined as durotaxis and implicated in development, wound healing and cancer, where complex interplays between immune and non-immune cells are present. Compared to the emerging mechanisms underlying the strongly adhesive mesenchymal durotaxis, little is known about whether immune cells - migrating in amoeboid mode - could follow mechanical cues. Here we develop an imaging-based confined migration device with stiffness gradient. By tracking live cell trajectory and analyzing the directionality of T cells and neutrophils, we observe that amoeboid cells can durotax. We further delineate the underlying mechanism to involve non-muscle myosin IIA (NMIIA) polarization towards the soft-matrix-side but may not require differential actin flow up-or down-stiffness gradient. Using the protista Dictyostelium , we demonstrate the evolutionary conservation of amoeboid durotaxis. Finally, these experimental phenomena are theoretically captured by an active gel model capable of mechanosensing. Collectively, these results may shed new lights on immune surveillance and recently identified confined migration of cancer cells, within the mechanically inhomogeneous tumor microenvironment or the inflamed fibrotic tissues.

Publisher

eLife Sciences Publications, Ltd

Reference66 articles.

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