Literature DB >> 21806925

Traction forces of neutrophils migrating on compliant substrates.

Risat A Jannat1, Micah Dembo, Daniel A Hammer.   

Abstract

Proper functioning of the innate immune response depends on migration of circulating neutrophils into tissues at sites of infection and inflammation. Migration of highly motile, amoeboid cells such as neutrophils has significant physiological relevance, yet the traction forces that drive neutrophil motion in response to chemical cues are not well characterized. To better understand the relationship between chemotactic signals and the organization of forces in motile neutrophils, force measurements were made on hydrogel surfaces under well-defined chemotactic gradients created with a microfluidic device. Two parameters, the mean chemoattractant concentration (C(M)) and the gradient magnitude (Δc/Δx) were varied. Cells experiencing a large gradient with C(M) near the chemotactic receptor K(D) displayed strong punctate centers of uropodial contractile force and strong directional motion on stiff (12 kPa) surfaces. Under conditions of ideal chemotaxis--cells in strong gradients with mean chemoattractant near the receptor K(D) and on stiffer substrates--there is a correlation between the magnitude of force generation and directional motion as measured by the chemotactic index. However, on soft materials or under weaker chemotactic conditions, directional motion is uncorrelated with the magnitude of traction force. Inhibition of either β(2) integrins or Rho-associated kinase, a kinase downstream from RhoA, greatly reduced rearward traction forces and directional motion, although some vestigial lamellipodium-driven motility remained. In summary, neutrophils display a diverse repertoire of methods for organizing their internal machinery to generate directional motion.
Copyright © 2011 Biophysical Society. Published by Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21806925      PMCID: PMC3145281          DOI: 10.1016/j.bpj.2011.05.040

Source DB:  PubMed          Journal:  Biophys J        ISSN: 0006-3495            Impact factor:   4.033


  34 in total

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8.  Neutrophil chemotaxis in linear and complex gradients of interleukin-8 formed in a microfabricated device.

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9.  Ability of polymorphonuclear leukocytes to orient in gradients of chemotactic factors.

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  43 in total

1.  Protrusive and Contractile Forces of Spreading Human Neutrophils.

Authors:  Steven J Henry; Christopher S Chen; John C Crocker; Daniel A Hammer
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2.  Finite element analysis of traction force microscopy: influence of cell mechanics, adhesion, and morphology.

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Review 3.  Toward single cell traction microscopy within 3D collagen matrices.

Authors:  Matthew S Hall; Rong Long; Xinzeng Feng; Yuling Huang; Chung-Yuen Hui; Mingming Wu
Journal:  Exp Cell Res       Date:  2013-06-25       Impact factor: 3.905

4.  Matrix confinement plays a pivotal role in regulating neutrophil-generated tractions, speed, and integrin utilization.

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5.  T cells have a light touch.

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6.  A biomechanical model for fluidization of cells under dynamic strain.

Authors:  Tenghu Wu; James J Feng
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Review 7.  Mechanical forces in the immune system.

Authors:  Morgan Huse
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8.  The RhoA guanine nucleotide exchange factor, LARG, mediates ICAM-1-dependent mechanotransduction in endothelial cells to stimulate transendothelial migration.

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9.  Macrophage motility is driven by frontal-towing with a force magnitude dependent on substrate stiffness.

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Review 10.  Leading from the Back: The Role of the Uropod in Neutrophil Polarization and Migration.

Authors:  Laurel E Hind; William J B Vincent; Anna Huttenlocher
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