Transduction of a dominant-negative H-Ras into human eosinophils attenuates extracellular signal–regulated kinase activation and interleukin-5–mediated cell viability

Hall, D.; Cui, Jinghua; Bates, Mary Ellen; Stout, Barbara A.; Koenderman, Leo; Coffer, Paul J.; Bertics, Paul J.

doi:10.1182/blood.v98.7.2014

Cited by 66 publications

(57 citation statements)

References 45 publications

(64 reference statements)

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“…7), suggesting that Ras not only is involved in Th2 cytokine production, but also in eosinophil migration induced by Th2 cytokines. Furthermore, Ras-induced ERK activation also is involved in IL-5-induced eosinophil survival (24). The relative contribution of each to the blockade of airway eosinophilic inflammation cannot be determined from this study.…”

Section: Discussionmentioning

confidence: 44%

“…The mechanism of these effects is unknown. Decreased eosinophil infiltration may result from one or more of the following: 1) decreased eosinophil adhesion to vascular endothelial cells (23), 2) decreased Th2 cytokine production, or 3) decreased eosinophil survival (24). We recently have demonstrated that the cytosolic group IV-PLA 2 and its upstream activators, ERK and Ras, regulate ␤ 2 -integrindependent adhesion of eosinophils in vitro (22,23).…”

Section: Discussionmentioning

confidence: 99%

“…Isolated leukocytes were resuspended in calcium-and magnesium-free HBSS (pH 6.8) containing 1% BSA. The pH of the sheath fluid of the flow cytometer was adjusted to 6.8 to quench FITC fluorescence on the outside of the cell (24), and at least 10,000 cells were analyzed on a FACScan (BD Biosciences, Mansfield, MA).…”

Section: Flow Cytometric Analysis Of the Tat Fusion Protein Transductmentioning

confidence: 99%

“…Ras-induced extracellular signal-regulated kinase (ERK) 4 activation is also essential for integrin-mediated eosinophil adhesion caused by cytokine, chemokine, and chemoattractant stimulation (22,23). H-Ras has been reported to play a role in IL-5-mediated survival of eosinophils in vitro (24). Recent investigations have reported that group IV cytosolic phospholipase A 2 (PLA 2 ), which is phosphorylated and activated by ERK (25), plays an essential role in Ag-induced eosinophil migration and airway hyperresponsiveness in immunestimulated mice (26) and guinea pigs (27).…”

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confidence: 99%

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Blockade of Airway Inflammation and Hyperresponsiveness by HIV-TAT-Dominant Negative Ras

Myou

Zhu

Myo

et al. 2003

The Journal of Immunology

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We have reported previously that HIV-TAT-dominant negative (dn) Ras inhibits eosinophil adhesion to ICAM-1 after activation by IL-5 and eotaxin. In this study, we evaluated the role of Ras in Ag-induced airway inflammation and hyperresponsiveness by i.p. administration into mice of dnRas, which was fused to an HIV-TAT protein transduction domain (TAT-dnRas). Uptake of TAT-dnRas (t1/2 = 12 h) was demonstrated in leukocytes after i.p. administration. OVA-sensitization significantly increased eosinophil and lymphocyte numbers in bronchoalveolar lavage fluid 24 h after final challenge. Treatment of animals with 3–10 mg/kg TAT-dnRas blocked the migration of eosinophils from 464 ± 91 × 103/ml to 288 ± 79 × 103/ml with 3 mg/kg of TAT-dnRas (p < 0.05), and further decreased to 116 ± 63 × 103/ml after 10 mg/kg TAT-dnRas (p < 0.01). Histological examination demonstrated that inflammatory cell infiltration (largely eosinophils and mononuclear cells) and mucin production around the airways caused by OVA were blocked by TAT-dnRas. OVA challenge also caused airway hyperresponsiveness to methacholine, which was dose dependently blocked by treatment with TAT-dnRas. TAT-dnRas also blocked Ag-induced IL-4 and IL-5, but not IFN-γ, production in lung tissue. Intranasal administration of IL-5 caused eosinophil migration into the airway lumen, which was attenuated by pretreatment with TAT-dnRas. By contrast, TAT-green fluorescent protein or dnRas lacking the TAT protein transduction domain did not block airway inflammation, cytokine production, or airway hyperresponsiveness. We conclude that Ras mediates Th2 cytokine production, airway inflammation, and airway hyperresponsiveness in immune-sensitized mice.

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Section: Discussionmentioning

confidence: 44%

Section: Discussionmentioning

confidence: 99%

Section: Flow Cytometric Analysis Of the Tat Fusion Protein Transductmentioning

confidence: 99%

mentioning

confidence: 99%

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Blockade of Airway Inflammation and Hyperresponsiveness by HIV-TAT-Dominant Negative Ras

Myou

Zhu

Myo

et al. 2003

The Journal of Immunology

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“…However, the process by which cPLA 2 is activated to cause integrin-mediated adhesion remains unknown. HRas has been reported to cause attenuation of IL-5-mediated survival of eosinophils in vitro at 16 h (14). H-Ras also has been reported to enhance both ␤ 1 -and ␤ 2 -integrin-mediated adhesion in nondifferentiated cell systems (15,16).…”

mentioning

confidence: 99%

Blockade of Focal Clustering and Active Conformation in β2-Integrin-Mediated Adhesion of Eosinophils to Intercellular Adhesion Molecule-1 Caused by Transduction of HIV TAT-Dominant Negative Ras

Myou

Zhu

Boetticher

et al. 2002

The Journal of Immunology

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We transduced dominant negative (dn) HIV TAT-Ras protein into mature human eosinophils to determine the signaling pathways and mechanism involved in integrin-mediated adhesion caused by cytokine, chemokine, and chemoattractant stimulation. Transduction of TAT-dnRas into nondividing eosinophils inhibited endogenous Ras activation and extracellular signal-regulated kinase (ERK) phosphorylation caused by IL-5, eotaxin-1, and fMLP. IL-5, eotaxin-1, or fMLP caused 1) change of Mac-1 to its active conformation and 2) focal clustering of Mac-1 on the eosinophil surface. TAT-dnRas or PD98059, a pharmacological mitogen-activated protein/ERK kinase inhibitor, blocked both focal surface clustering of Mac-1 and the change to active conformational structure of this integrin assessed by the mAb CBRM1/5, which binds the activation epitope. Eosinophil adhesion to the endothelial ligand ICAM-1 was correspondingly blocked by TAT-dnRas and PD98059. As a further control, we used PMA, which activates ERK phosphorylation by postmembrane receptor induction of protein kinase C, a mechanism which bypasses Ras. Neither TAT-dnRas nor PD98059 blocked eosinophil adhesion to ICAM-1, up-regulation of CBRM1/5, or focal surface clustering of Mac-1 caused by PMA. In contrast to β2-integrin adhesion, neither TAT-dnRas nor PD98059 blocked the eosinophil adhesion to VCAM-1. Thus, a substantially different signaling mechanism was identified for β1-integrin adhesion. We conclude that H-Ras-mediated activation of ERK is critical for β2-integrin adhesion and that Ras-protein functions as the common regulator for cytokine-, chemokine-, and G-protein-coupled receptors in human eosinophils.

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Protein Transduction: Generation of Full‐Length Transducible Proteins Using the TAT System

Becker-Hapak

Dowdy

2003

CP Cell Biology

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This unit describes the technology that allows an investigator to transduce full‐length proteins by utilizing a minimal, eleven‐amino acid, HIV‐TAT transduction domain that can be fused to a protein of choice using the pTAT or pTAT‐HA protein expression plasmids. Bacterial expression, followed by solubilization of protein aggregates with a denaturing agent, affords high yields of transducible fusion protein. The fusion protein, once added to the culture medium, can cross the cell membrane and then be degraded or refolded by the cellular machinery. Correct targeting and function of the fusion protein can be easily examined by fluorescent microscopy or immunohistochemistry. This strategy was established and improved to its current state by the purification and transduction of a multitude of fusion proteins. Because the pool of fusion proteins spans many different functions, the protocols cover a wide variety of commonly used protein isolation and characterization methods.

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Transduction of a dominant-negative H-Ras into human eosinophils attenuates extracellular signal–regulated kinase activation and interleukin-5–mediated cell viability

Cited by 66 publications

References 45 publications

Blockade of Airway Inflammation and Hyperresponsiveness by HIV-TAT-Dominant Negative Ras

Blockade of Airway Inflammation and Hyperresponsiveness by HIV-TAT-Dominant Negative Ras

Blockade of Focal Clustering and Active Conformation in β2-Integrin-Mediated Adhesion of Eosinophils to Intercellular Adhesion Molecule-1 Caused by Transduction of HIV TAT-Dominant Negative Ras

Protein Transduction: Generation of Full‐Length Transducible Proteins Using the TAT System

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