Endothelial paxillin and focal adhesion kinase (FAK) play a critical role in neutrophil transmigration

Parsons, Sean A.; Sharma, Ritu; Roccamatisi, Dawn Louise; Zhang, Hong; Petri, Bjӧrn; Kubes, Paul; Colarusso, Pina; Patel, Kamala D.

doi:10.1002/eji.201041303

Cited by 35 publications

(43 citation statements)

References 45 publications

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“…Since FAK appears to integrate receptor-mediated signals that control actin reorganization in immune cells (33-36), we examined actin polymerization upon TCR induction. Jurkat cells expressing the Luc or FAK-specific miRNAs were stimulated on glass chamber slides treated with anti-TCR and stained to detect actin filaments that form upon T cell spreading (47).…”

Section: Resultsmentioning

confidence: 99%

Focal Adhesion Kinase Negatively Regulates Lck Function Downstream of the T Cell Antigen Receptor

Chapman

Connolly

Reinl

et al. 2013

The Journal of Immunology

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Focal adhesion kinase (FAK) is a critical regulator of signal transduction in multiple cell types. Although this protein is activated upon T cell receptor (TCR) engagement, the cellular function that FAK plays in mature human T cells is unknown. By suppressing the function of FAK, we revealed that FAK inhibits TCR-mediated signaling by recruiting C-terminal Src kinase (Csk) to the membrane and/or receptor complex following TCR activation. Thus, in the absence of FAK, the inhibitory phosphorylation of Lck and/or Fyn is impaired. Together, these data highlight a novel role for FAK as a negative regulator TCR function in human T cells. These results also suggest that changes in FAK expression could modulate sensitivity to TCR stimulation and contribute to the progression of T cell malignancies and autoimmune diseases.

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Section: Resultsmentioning

confidence: 99%

Focal Adhesion Kinase Negatively Regulates Lck Function Downstream of the T Cell Antigen Receptor

Chapman

Connolly

Reinl

et al. 2013

The Journal of Immunology

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“…New findings show that CPT increases PAX expression and appears to do so in a concentration-dependent manner ( Figure 4A). The increase in PAX could be strengthening the focal adhesion contacts [8,50] and cytoskeletal stability as has been observed in epithelial cells [51,52] and migration [9,53], thereby reducing capacity of these cells to move in response to a stimulant. In complement, FAK and Src together act as a signaling nexus to induce phosphorylation of FA proteins including autophosphorylation of FAK itself, PAX and p130Cas [4,6,54].…”

Section: Discussionmentioning

confidence: 99%

Exchange protein activated by cAMP (EPAC) controls migration of vascular smooth muscle cells in concentration- and timedependent manner

Adderley¹,

Martin²,

Tulis³

2015

Arch Physiol

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“…Interactions between eosinophils and endothelial cells were visualized on a Zeiss Axiovert 100 microscope using either a 106/0.25 NA or 406/ 0.60 NA phase-contrast objective and recorded by using a chargecoupled device camera (KP-M1U; Hitachi Denshi, Ltd). The total number of cells accumulated on the monolayer was determined at 5 minutes of perfusion, and the numbers of rolling, firmly adherent and transmigrated cells were determined at 10 minutes as described (Cuvelier and Patel, 2001;Parsons et al, 2012). For each condition, four to ten fields of view were examined.…”

Section: Eosinophil Recruitment Under Flow Conditionsmentioning

confidence: 99%

Focal adhesion kinase-related nonkinase (FRNK) negatively regulates IL-4-mediated inflammation

Sharma

Colarusso

Zhang

et al. 2015

Journal of Cell Science

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Focal adhesion kinase (FAK)-related nonkinase (PTK2 isoform 6 in humans, hereafter referred to as FRNK) is a cytoskeletal regulatory protein that has recently been shown to dampen lung fibrosis, yet its role in inflammation is unknown. Here, we show for the first time that expression of FRNK negatively regulates IL-4-mediated inflammation in a human model of eosinophil recruitment. Mechanistically, FRNK blocks eosinophil accumulation, firm adhesion and transmigration by preventing transcription and protein expression of VCAM-1 and CCL26. IL-4 activates STAT6 to induce VCAM-1 and CCL26 transcription. We now show that IL-4 also increases GATA6 to induce VCAM-1 expression. FRNK blocks IL-4-induced GATA6 transcription but has little effect on GATA6 protein expression and no effect on STAT6 activation. FRNK can block FAK or Pyk2 signaling and we, thus, downregulated these proteins using siRNA to determine whether signaling from either protein is involved in the regulation of VCAM-1 and CCL26. Knockdown of FAK, Pyk2 or both had no effect on VCAM-1 or CCL26 expression, which suggests that FRNK acts independently of FAK and Pyk2 signaling. Finally, we found that IL-4 induces the late expression of endogenous FRNK. In summary, FRNK represents a novel mechanism to negatively regulate IL-4-mediated inflammation.

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Endothelial paxillin and focal adhesion kinase (FAK) play a critical role in neutrophil transmigration

Cited by 35 publications

References 45 publications

Focal Adhesion Kinase Negatively Regulates Lck Function Downstream of the T Cell Antigen Receptor

Focal Adhesion Kinase Negatively Regulates Lck Function Downstream of the T Cell Antigen Receptor

Exchange protein activated by cAMP (EPAC) controls migration of vascular smooth muscle cells in concentration- and timedependent manner

Focal adhesion kinase-related nonkinase (FRNK) negatively regulates IL-4-mediated inflammation

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