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Directional reorientation of migrating neutrophils is limited by suppression of receptor input signaling at the cell rear through myosin II activity

Author

Listed:
  • Amalia Hadjitheodorou

    (Stanford University
    University of Washington)

  • George R. R. Bell

    (University of California, Davis)

  • Felix Ellett

    (BioMEMS Resource Center, Massachusetts General Hospital, Harvard Medical School)

  • Shashank Shastry

    (University of California, Davis)

  • Daniel Irimia

    (BioMEMS Resource Center, Massachusetts General Hospital, Harvard Medical School)

  • Sean R. Collins

    (University of California, Davis)

  • Julie A. Theriot

    (University of Washington)

Abstract

To migrate efficiently to target locations, cells must integrate receptor inputs while maintaining polarity: a distinct front that leads and a rear that follows. Here we investigate what is necessary to overwrite pre-existing front-rear polarity in neutrophil-like HL60 cells migrating inside straight microfluidic channels. Using subcellular optogenetic receptor activation, we show that receptor inputs can reorient weakly polarized cells, but the rear of strongly polarized cells is refractory to new inputs. Transient stimulation reveals a multi-step repolarization process, confirming that cell rear sensitivity to receptor input is the primary determinant of large-scale directional reversal. We demonstrate that the RhoA/ROCK/myosin II pathway limits the ability of receptor inputs to signal to Cdc42 and reorient migrating neutrophils. We discover that by tuning the phosphorylation of myosin regulatory light chain we can modulate the activity and localization of myosin II and thus the amenability of the cell rear to ‘listen’ to receptor inputs and respond to directional reprogramming.

Suggested Citation

  • Amalia Hadjitheodorou & George R. R. Bell & Felix Ellett & Shashank Shastry & Daniel Irimia & Sean R. Collins & Julie A. Theriot, 2021. "Directional reorientation of migrating neutrophils is limited by suppression of receptor input signaling at the cell rear through myosin II activity," Nature Communications, Nature, vol. 12(1), pages 1-15, December.
  • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-26622-z
    DOI: 10.1038/s41467-021-26622-z
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    References listed on IDEAS

    as
    1. Henry R. Bourne & Orion Weiner, 2002. "Cell polarity: A chemical compass," Nature, Nature, vol. 419(6902), pages 21-21, September.
    2. Tsang, Eric W. K., 2014. "Old and New," Management and Organization Review, Cambridge University Press, vol. 10(03), pages 390-390, November.
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    Cited by:

    1. George R. R. Bell & Esther Rincón & Emel Akdoğan & Sean R. Collins, 2021. "Optogenetic control of receptors reveals distinct roles for actin- and Cdc42-dependent negative signals in chemotactic signal processing," Nature Communications, Nature, vol. 12(1), pages 1-14, December.
    2. Nathan M. Belliveau & Matthew J. Footer & Emel Akdoǧan & Aaron P. Loon & Sean R. Collins & Julie A. Theriot, 2023. "Whole-genome screens reveal regulators of differentiation state and context-dependent migration in human neutrophils," Nature Communications, Nature, vol. 14(1), pages 1-20, December.
    3. Eoin McEvoy & Tal Sneh & Emad Moeendarbary & Yousef Javanmardi & Nadia Efimova & Changsong Yang & Gloria E. Marino-Bravante & Xingyu Chen & Jorge Escribano & Fabian Spill & José Manuel Garcia-Aznar & , 2022. "Feedback between mechanosensitive signaling and active forces governs endothelial junction integrity," Nature Communications, Nature, vol. 13(1), pages 1-14, December.
    4. Tatsat Banerjee & Satomi Matsuoka & Debojyoti Biswas & Yuchuan Miao & Dhiman Sankar Pal & Yoichiro Kamimura & Masahiro Ueda & Peter N. Devreotes & Pablo A. Iglesias, 2023. "A dynamic partitioning mechanism polarizes membrane protein distribution," Nature Communications, Nature, vol. 14(1), pages 1-24, December.

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