Letter Special Issues

Rigidity sensing by blood-borne leukocytes: Is it independent of internal signaling?

  • Received: 10 September 2023 Revised: 19 November 2023 Accepted: 26 November 2023 Published: 10 January 2024
  • Atherosclerosis is a chronic inflammatory disease that results in the formation of lipid-rich lesions and stiffening of arterial walls. An increasing body of evidence suggests that nearly all members of the leukocyte family accumulate within atherosclerosis-prone arteries and participate in various stages of disease progression. Recently, it has been proposed that progressive changes of the elastic modulus of the arterial wall during plaque development may directly influence the kinematics of leukocyte rolling. In the present study, we propose that rigidity sensing of rolling leukocytes may occur spontaneously due to the stiffness-dependent elastic instability of reversible bonds between rolling leukocytes and the arterial walls. This effect is mechanistic in nature and operates independently of cell biochemical signaling. To partially test this hypothesis, we measured the rolling velocities of functionalized microparticles, comparable in size to leukocytes, interacting with E-selectin coated substrates of controlled stiffness. The kinematic analysis of the particles' motion reveals a larger rolling velocity on softer substrates, aligning with previous reports regarding monocytes. A simple kinetic model for a cluster of reversible bonds formed between a cell and the underlying substrate demonstrates that the critical forces needed for bond disassembly decrease as substrate stiffness decreases. Consequently, bonds are more likely to break on softer substrates, resulting in enhanced cell mobility.

    Citation: Alireza Sarvestami, Madeline Smith, Arsha Moorthy, Patrick Kho, Lauren Talbo, Chamaree de Silva. Rigidity sensing by blood-borne leukocytes: Is it independent of internal signaling?[J]. AIMS Biophysics, 2024, 11(1): 18-30. doi: 10.3934/biophy.2024002

    Related Papers:

  • Atherosclerosis is a chronic inflammatory disease that results in the formation of lipid-rich lesions and stiffening of arterial walls. An increasing body of evidence suggests that nearly all members of the leukocyte family accumulate within atherosclerosis-prone arteries and participate in various stages of disease progression. Recently, it has been proposed that progressive changes of the elastic modulus of the arterial wall during plaque development may directly influence the kinematics of leukocyte rolling. In the present study, we propose that rigidity sensing of rolling leukocytes may occur spontaneously due to the stiffness-dependent elastic instability of reversible bonds between rolling leukocytes and the arterial walls. This effect is mechanistic in nature and operates independently of cell biochemical signaling. To partially test this hypothesis, we measured the rolling velocities of functionalized microparticles, comparable in size to leukocytes, interacting with E-selectin coated substrates of controlled stiffness. The kinematic analysis of the particles' motion reveals a larger rolling velocity on softer substrates, aligning with previous reports regarding monocytes. A simple kinetic model for a cluster of reversible bonds formed between a cell and the underlying substrate demonstrates that the critical forces needed for bond disassembly decrease as substrate stiffness decreases. Consequently, bonds are more likely to break on softer substrates, resulting in enhanced cell mobility.



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    Acknowledgments



    This work was supported by the seed grant provided by the Provost's office at Mercer University .

    Conflict of interest



    The authors declare no conflict of interests.

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