Molecular players in neutrophil chemotaxis—focus on PI3K and small GTPases

Gambardella, Laure; Vermeren, Sonja

doi:10.1189/jlb.1112564

Cited by 81 publications

(86 citation statements)

References 120 publications

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“…Chemoattractant concentration gradient directed immune cell migration (chemotaxis) critically orchestrates the trafficking and homing of various immune cell types in tissues (Cahalan and Parker, 2008;Jin et al, 2008;Gambardella and Vermeren, 2013;Heuzé et al, 2013). T lymphocytes are the key players in adaptive immunity (Garside et al, 1998;Miller et al, 2002;Bromley et al, 2008;John et al, 2009).…”

Section: Introductionmentioning

confidence: 99%

Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator

et al. 2015

Journal of Immunological Methods

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a b s t r a c t T lymphocyte migration is crucial for adaptive immunity. Manipulation of signaling molecules controlling cell migration combined with in vitro cell migration analysis provides a powerful research approach. Microfluidic devices, which can precisely configure chemoattractant gradients and allow quantitative single cell analysis, have been increasingly applied to cell migration and chemotaxis studies. However, there are a very limited number of published studies involving microfluidic migration analysis of genetically manipulated immune cells. In this study, we describe a simple microfluidic method for quantitative analysis of T cells expressing transfected chemokine receptors and other cell migration signaling probes. Using this method, we demonstrated chemotaxis of Jurkat transfectants expressing wild type or C terminus mutated CCR7 within a gradient of chemokine CCL19, and characterized the difference in transfectant migration mediated by wild type and mutant CCR7. The EGFP tagged CCR7 allows identification of CCR7 expressing transfectants in cell migration analysis and microscopy assessment of CCR7 dynamics. Collectively, our study demonstrated the effective use of the microfluidic method for studying CCR7 mediated T cell transfectant migration. We envision this developed method will provide a useful platform to functionally test various signaling mechanisms at the cell migration level.

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Section: Introductionmentioning

confidence: 99%

Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator

et al. 2015

Journal of Immunological Methods

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“…Ultimately, neutrophils will dissociate from the intermediary chemoattractants and migrate toward the end-target chemoattractants of bacterial origin (119,125). Although the chemoattractants vary significantly in their structure, the receptors for these molecules are all members of the seven-transmembrane helix receptor family which operate through to heterotrimeric G proteins, which further activate downstream pathways responsible for cytoskeletal arrangements and chemotactic functions (119,120,123).…”

Section: Fusobacterium Nucleatum (F Nucleatum) and Aggregatibacter mentioning

confidence: 99%

“…Since neutrophils are exposed to many chemoattractants that are released at various locations including the vascular endothelium, interstitial cells and the site of infection, it is necessary for them to assimilate and prioritize their response (120,123,124). They can respond to signals from both intermediary chemoattractants (IL-8, platelet activated factor, chemotactic cytokines, leukotriene B 4 (LTB4)) and end target cellular chemoattractants (formyl-methionylleucyl phenylalanine (fMLF), complement fragment C5a, C3a, plasminogen activator), which guide them to a generalized region and then further to a more specific site, where they will encounter their target (118)(119)(120)123).…”

Section: Fusobacterium Nucleatum (F Nucleatum) and Aggregatibacter mentioning

confidence: 99%

“…They can respond to signals from both intermediary chemoattractants (IL-8, platelet activated factor, chemotactic cytokines, leukotriene B 4 (LTB4)) and end target cellular chemoattractants (formyl-methionylleucyl phenylalanine (fMLF), complement fragment C5a, C3a, plasminogen activator), which guide them to a generalized region and then further to a more specific site, where they will encounter their target (118)(119)(120)123). Ultimately, neutrophils will dissociate from the intermediary chemoattractants and migrate toward the end-target chemoattractants of bacterial origin (119,125).…”

Section: Fusobacterium Nucleatum (F Nucleatum) and Aggregatibacter mentioning

confidence: 99%

“…Directional movement of leukocytes is necessary for a functional response to a variety of inflammatory signals (117). Leukocytes participate in directional movement toward sites of injury and inflammation by deciphering a chemoattractant gradient, a process referred to as chemotaxis (114,(117)(118)(119)(120).…”

Section: Fusobacterium Nucleatum (F Nucleatum) and Aggregatibacter mentioning

confidence: 99%

See 2 more Smart Citations

Characterization of Filifactor alocis and its immune evasion strategies employed against human neutrophils.

Armstrong¹

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The RacGAP protein FilGAP is a negative regulator of chemokine‐promoted lymphocyte migration

et al. 2016

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Rho family small GTPases regulate lymphocyte migration induced by chemokines. However, how lymphocyte migration is regulated by Rho GTPases remains to be elucidated. Here, we identified FilGAP, a Rac‐specific GAP, as a negative regulator of lymphocyte polarization and migration. Depletion of FilGAP in mouse pro‐B BAF cells increased cellular elongation and membrane protrusion after stimulation of the cells with SDF‐1α, which caused increased migration speed. Although FilGAP is detectable both at the front and rear of polarized cells, FilGAP appears to be concentrated at the tip of retracting lamellae of moving lymphocytes. Moreover, depletion of FilGAP increased activation of Rac at the front of polarized cells. Thus, FilGAP may inhibit lamellae extension at the front of moving lymphocytes.

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Molecular players in neutrophil chemotaxis—focus on PI3K and small GTPases

Cited by 81 publications

References 120 publications

Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator

Analysis of CCR7 mediated T cell transfectant migration using a microfluidic gradient generator

Characterization of Filifactor alocis and its immune evasion strategies employed against human neutrophils.

The RacGAP protein FilGAP is a negative regulator of chemokine‐promoted lymphocyte migration

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