Interaction of matrix with integrin receptors is required for optimal LPS-induced MAP kinase activation

Monick, Martha M.; Powers, Linda S.; Butler, Noah S.; Yarovinsky, Timur O.; Hunninghake, Gary W.

doi:10.1152/ajplung.00437.2001

Cited by 42 publications

(47 citation statements)

References 46 publications

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“…Furthermore, FAK-expressing cells transfected with the FAK inhibitor FRNK produced significantly lower amounts of IL-6 upon LPS challenge. This is in line with previous results showing that LPS induced FAK phosphorylation in a murine monocytic cell line (18). We further demonstrated that other TLR ligands may also induce FAK phosphorylation at Tyr 397 and require FAK for cytokine release because comparable results have been obtained with the TLR2 ligand Pam 3 CSK 4 (data not shown).…”

Section: Discussionsupporting

confidence: 93%

Cross Talk between MyD88 and Focal Adhesion Kinase Pathways

Zeisel

Druet

Sibilia

et al. 2005

The Journal of Immunology

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Focal adhesion kinase (FAK) is a nonreceptor protein tyrosine kinase involved in signaling downstream of integrins, linking bacterial detection, cell entry, and initiation of proinflammatory response through MAPKs and NF-κB activation. In this study, using protein I/II from Streptococcus mutans as a model activator of FAK, we investigated the potential link between FAK and TLR pathways. Using macrophages from TLR- or MyD88-deficient mice, we report that MyD88 plays a major role in FAK-dependent protein I/II-induced cytokine release. However, response to protein I/II stimulation was independent of TLR4, TLR2, and TLR6. The data suggest that there is a cross talk between FAK and MyD88 signaling pathways. Moreover, MyD88-dependent, LPS-induced IL-6 secretion by human and murine fibroblasts required the presence of FAK, confirming that MyD88 and FAK pathways are interlinked.

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Section: Discussionsupporting

confidence: 93%

Cross Talk between MyD88 and Focal Adhesion Kinase Pathways

Zeisel

Druet

Sibilia

et al. 2005

The Journal of Immunology

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“…These findings suggest that LPS activates integrins, increasing integrin ligation and clustering, and thus triggering an "outside-in" signaling that amplifies the action of LPS. Consistent with our in vivo data, Monick et al (14) proposed the hypothesis that in vitro treatment of macrophages with LPS results in "insideout" integrin activation, and increased cellular adherence, providing integrin "outside-in" signaling to MAP kinases. Indeed, signals from integrin receptors seem to be required for optimal LPS signaling in macrophages.…”

Section: Discussionsupporting

confidence: 90%

“…Moreover, the Arg-GlyAsp (RGD) motif of ECM entities that associate with integrin ␣ v ␤ 3 signaling appears to be involved in NF-B activation (12). Furthermore, in macrophages, integrins play a complementary role in LPS signaling, i.e., in the activations of MAP kinases (such as ERK and JNK), and in TNF-␣ production (13,14). These relations suggest that integrin signaling in macrophages mediates or amplifies inflammation.…”

Section: N Uclear Factor B (Nf-b) Is Transcriptional Regulatorymentioning

confidence: 99%

Src Tyrosine Kinases Mediate Activations of NF-κB and Integrin Signal during Lipopolysaccharide-Induced Acute Lung Injury

Lee

Moon

Lee

et al. 2007

The Journal of Immunology

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Src tyrosine kinases (TKs) are signaling proteins involved in cell signaling pathways toward cytoskeletal, membrane and nuclear targets. In the present study, using a selective Src TK inhibitor, PP1, we investigated the roles of Src TKs in the key pulmonary responses, NF-κB activation, and integrin signaling during acute lung injury in BALB/C mice intratracheally treated with LPS. LPS resulted in c-Src phosphorylation in lung tissue and the phospho-c-Src was predominantly localized in recruited neutrophils and alveolar macrophages. PP1 inhibited LPS-induced increases in total protein content in bronchoalveolar lavage fluid, neutrophil recruitment, and increases in the production or activity of TNF-α and matrix metalloproteinase-9. PP1 also blocked LPS-induced NF-κB activation, and phosphorylation and degradation of IκB-α. The inhibition of NF-κB activation by PP1 correlated with a depression of LPS-induced integrin signaling, which included increases in the phosphorylations of integrin β3, and of the focal adhesion kinase (FAK) family members, FAK and Pyk2, in lung tissue, and reductions in the fibrinogen-binding activity of alveolar macrophages. Moreover, treatment with anti-αv, anti-β3, or Arg-Gly-Asp-Ser (RGDS), inhibited LPS-induced NF-κB activation. Taken together, our findings suggest that Src TKs play a critical role in LPS-induced activations of NF-κB and integrin (αvβ3) signaling during acute lung injury. Therefore, Src TK inhibition may provide a potential means of ameliorating inflammatory cascade-associated lung injury.

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“…Previously, we reported that cell adhesion (integrin signaling) was required for lipopolysaccharide-induced activation of the mitogen-activated kinase (MAPK), extracellular regulated kinase (ERK), and optimal tumor necrosis factor-␣ production (31). In this study, we evaluated the role of adhesion (tissue culture plates and extracellular matrix-coated plates with collagen type I, collagen type IV, or fibronectin) on hyperoxia-induced growth arrest in macrophages.…”

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confidence: 99%

Hyperoxia Induces Macrophage Cell Cycle Arrest by Adhesion-dependent Induction of p21Cip1 and Activation of the Retinoblastoma Protein

Nyunoya

Powers

Yarovinsky

et al. 2003

Journal of Biological Chemistry

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Hyperoxia induces growth arrest, apoptosis, necrosis, and morphological changes (spreading and adhesion) in various types of cells. The mechanism of hyperoxia-induced cell growth arrest has not been well elucidated, especially in macrophages. One possible mechanism is a role of cell adhesion in hyperoxia-induced cell cycle arrest. To evaluate this finding, macrophages were cultured in normoxia (21% O 2 ) or hyperoxia (95% O 2 ) in adhesion or low adhesion conditions. Incubation of macrophages in hyperoxia induced cell cycle arrest. The hyperoxia-induced cell cycle arrest was prevented by low adhesion conditions. To evaluate pathways potentially involved in hyperoxia-induced growth arrest, we measured extracellular regulated kinase and retinoblastoma protein activation and p21Cip1 and p53 accumulation. Hyperoxia strongly induced activation of extracellular regulated kinase and retinoblastoma protein as well as up-regulation of p21Cip1 . These effects of hyperoxia were attenuated under low adhesion conditions, suggesting a role for integrin-dependent signaling. The induction of p21 Cip1 and activation of retinoblastoma protein occurred via a p53-independent mechanism. These results suggest that adhesiondependent pathways are required for hyperoxia-induced cell cycle arrest in macrophages.

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Interaction of matrix with integrin receptors is required for optimal LPS-induced MAP kinase activation

Cited by 42 publications

References 46 publications

Cross Talk between MyD88 and Focal Adhesion Kinase Pathways

Cross Talk between MyD88 and Focal Adhesion Kinase Pathways

Src Tyrosine Kinases Mediate Activations of NF-κB and Integrin Signal during Lipopolysaccharide-Induced Acute Lung Injury

Hyperoxia Induces Macrophage Cell Cycle Arrest by Adhesion-dependent Induction of p21Cip1 and Activation of the Retinoblastoma Protein

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