Interactome analysis of longitudinal pharyngeal infection of cynomolgus macaques by group A
            <i>Streptococcus</i>

Shea, Patrick R.; Virtaneva, Kimmo; Kupko, John J.; Porcella, Stephen F.; Barry, William T.; Wright, Fred A.; Kobayashi, Scott D.; Carmody, Aaron B.; Ireland, Robin; Sturdevant, Daniel E.; Ricklefs, Stacy M.; Babar, Imran; Johnson, Claire; Graham, Morag; Gardner, Donald J.; Bailey, John R.; Parnell, Michael J.; DeLeo, Frank R.; Musser, James M.

doi:10.1073/pnas.0906384107

Cited by 29 publications

(25 citation statements)

References 36 publications

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“…The use of different transactivating ligands and receptors by SMC could provide a means to adapt inflammatory responses to the type of injury. EGFR/ErbB1 sensing could be more important to the binding and clearance of bacteria (31), whereas the initiation of inflammation after acid exposure might require ErbB4 signaling, which is important for surfactant production and proliferation of lung epithelial cells (32). Moreover, we found that IL-1b induced CXCL8 release by htSMC in an ADAM17-NRG1-dependent manner.…”

Section: Discussionmentioning

confidence: 72%

Smooth Muscle Cells Relay Acute Pulmonary Inflammation via Distinct ADAM17/ErbB Axes

Dreymueller¹,

Martin²,

Schumacher³

et al. 2014

The Journal of Immunology

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In acute pulmonary inflammation, danger is first recognized by epithelial cells lining the alveolar lumen and relayed to vascular responses, including leukocyte recruitment and increased endothelial permeability. We supposed that this inflammatory relay critically depends on the immunological function of lung interstitial cells such as smooth muscle cells (SMC). Mice with smooth muscle protein-22α promotor-driven deficiency of the disintegrin and metalloproteinase (ADAM) 17 (SM22-Adam17−/−) were investigated in models of acute pulmonary inflammation (LPS, cytokine, and acid instillation). Underlying signaling mechanisms were identified in cultured tracheal SMC and verified by in vivo reconstitution experiments. SM22-Adam17−/− mice showed considerably decreased cytokine production and vascular responses in LPS- or acid-induced pulmonary inflammation. In vitro, ADAM17 deficiency abrogated cytokine release of primary SMC stimulated with LPS or supernatant of acid-exposed epithelial cells. This was explained by a loss of ADAM17-mediated growth factor shedding. LPS responses required ErbB1/epidermal growth factor receptor transactivation by TGFα, whereas acid responses required ErbB4 transactivation by neuregulins. Finally, LPS-induced pulmonary inflammation in SM22-Adam17−/− mice was restored by exogenous TGFα application, confirming the involvement of transactivation pathways in vivo. This highlights a new decisive immunological role of lung interstitial cells such as SMC in promoting acute pulmonary inflammation by ADAM17-dependent transactivation.

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Section: Discussionmentioning

confidence: 72%

Smooth Muscle Cells Relay Acute Pulmonary Inflammation via Distinct ADAM17/ErbB Axes

Dreymueller¹,

Martin²,

Schumacher³

et al. 2014

The Journal of Immunology

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“…As a consequence, we have extensively used non-human primates, the most human-relevant animal model possible, as the preferred host for testing hypotheses bearing on GAS molecular pathogenesis. 13,14,34,[37][38][39] However, high cost and substantial…”

Section: Discussionmentioning

confidence: 99%

“…A growing body of evidence suggests an increased interest in performing GAS gene expression studies under human-relevant in vitro conditions or during in vivo infections. 14,37,[46][47][48][49] Infected hemolymph is easy to manipulate and enriched in GAS cells relative to host cells. This helps to overcome the challenges associated with extracting a sufficient quantity of high quality GAS RNA from infected animal tissues for TaqMan or expression microarray analyses.…”

Section: ©2 0 1 1 L a N D E S B I O S C I E N C E D O N O T D I S Tmentioning

confidence: 99%

Virulence of serotype M3 Group AStreptococcusstrains in wax worms (Galleria mellonellalarvae)

et al. 2011

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“…Genechip Experiment-RNAs were extracted and DNA microarray targets were prepared as described previously (27). Gene expression was measured using the Affymetrix 430 2.0 Genechip containing the mouse genome and data analysis were carried out as described previously (28) with the following modifications.…”

Section: Rna Isolation and Real Time Pcr (Rt-pcr)mentioning

confidence: 99%

IL-17-induced NF-κB Activation via CIKS/Act1

Sønder

Saret

Tang

et al. 2011

Journal of Biological Chemistry

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124

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Interleukin-17 (IL-17) is essential in host defense against extracellular bacteria and fungi, especially at mucosal sites, but it also contributes significantly to inflammatory and autoimmune disease pathologies. Binding of IL-17 to its receptor leads to recruitment of adaptor protein CIKS/Act1 via heterotypic association of their respective SEFIR domains and activation of transcription factor NF-B; it is not known whether CIKS and/or NF-B are required for all gene induction events. Here we report that CIKS is essential for all IL-17-induced immediate-early genes in primary mouse embryo fibroblasts, whereas NF-B is profoundly involved. We also identify a novel subdomain in the N terminus of CIKS that is essential for IL-17-mediated NF-B activation. This domain is both necessary and sufficient for interaction between CIKS and TRAF6, an adaptor required for NF-B activation. The ability of decoy peptides to block this interaction may provide a new therapeutic strategy for intervention in IL-17-driven autoimmune and inflammatory diseases.

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Interactome analysis of longitudinal pharyngeal infection of cynomolgus macaques by group A Streptococcus

Cited by 29 publications

References 36 publications

Smooth Muscle Cells Relay Acute Pulmonary Inflammation via Distinct ADAM17/ErbB Axes

Smooth Muscle Cells Relay Acute Pulmonary Inflammation via Distinct ADAM17/ErbB Axes

Virulence of serotype M3 Group AStreptococcusstrains in wax worms (Galleria mellonellalarvae)

IL-17-induced NF-κB Activation via CIKS/Act1

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