IL-17A Promotes the Exacerbation of IL-33–Induced Airway Hyperresponsiveness by Enhancing Neutrophilic Inflammation via CXCR2 Signaling in Mice

Mizutani, Nobuaki; Nabe, Takeshi; Yoshino, Shigefumi

doi:10.4049/jimmunol.1301538

Cited by 90 publications

(96 citation statements)

References 63 publications

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Section: Discussionsupporting

confidence: 93%

“…Per a 10 acts via PAR-2 receptors [8], which explains the relatively higher levels of IL-17A in the BALF of Per a 10 immunized mice. This, along with the influx of neutrophils in lungs of Per a 10 immunized mice is in accordance with previous studies where IL-17A is shown to increase neutrophilic infiltration [25].Costimulatory molecules on antigen presenting cells along with the cytokine milieu play a critical role in determining the type of T-cell response. OX40L is an important costimulatory molecule expressed on a wide variety of cells including APCs.…”

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confidence: 92%

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Protease activity of Per a 10 potentiates Th2 polarization by increasing IL‐23 and OX40L

2015

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Proteases are implicated in exacerbation of allergic diseases. In this study, the role of proteolytic activity of Per a 10 was evaluated on Th2 polarization. Intranasal administration of Per a 10 in mice led to allergic airway inflammation as seen by higher IgE levels, cellular infiltration, IL-17A, and Th2 cytokines, whereas, inactive ( )Per a 10 showed attenuated response. There was an increased OX40L expression on lung and lymph node dendritic cells in Per a 10 immunized group and on Per a 10 stimulated BMDCs. Reduction in CD40 expression without any change at transcript level in lungs of Per a 10 immunized mice suggested CD40 cleavage. BMDCs pulsed with Per a 10 showed reduced CD40 expression with lower IL-12p70 secretion as compared to heat inactivated Per a 10. IL-23, TNF-α, and IL-6 levels were significantly higher in Per a 10 stimulated BMDCs supernatant. In DC-T cell coculture studies, Per a 10 pulsed BMDCs showed higher levels of IL-4 and IL-13 that were reduced on blocking of either IL-23 or OX40L. In conclusion, the data suggests a critical role of protease activity of Per a 10 in promoting Th2 polarization by increasing IL-23 secretion and OX40L expression on dendritic cells.Keywords: CD40 r Cytokines r Dendritic cell r OX40L r Protease allergen Additional supporting information may be found in the online version of this article at the publisher's web-site IntroductionProteases are known to play an important role in manifestation of diseases like cancer, coagulopathies, respiratory inflammatory diseases, rheumatoid arthritis, and degenerative diseases [1][2][3]. Proteases from sources like house dust mite (Der p 1, Der p 3, Der p 6, Der p 9, Der f 1) and fungi (Asp f 13, Pen c 1, Pen c 13, Epi p 1) have been characterized as potent allergens [4]. Protease allergens act by proteolytic cleavage of an array of cell surface molecules and are known to modulate the functions of a variety of cell types including both immune and structural cells [5]. Proteolytic allergens from house dust mite are known to exacerbate allergic immune responses by selective cleavage of CD23, CD25, DC-SIGN, and DC-SIGNR on surface of immune cells Correspondence: Dr. Naveen Arora e-mail: naveen@igib.res.in; navdelhi@hotmail.com [6,7]. Further, cleavage and subsequent activation of PAR receptors by proteases lead to increased secretion of chemokines, proinflammatory, and pro Th2 cytokines from airway epithelial cells [8,9]. Studies have reported impaired epithelial barrier function as the feature of allergic diseases like asthma and atopic dermatitis [10]. The enzymatic activity of proteases has been reported to compromise epithelial barrier directly by cleaving tight junction proteins ZO-1 and occludin thereby increasing epithelial permeability [11,12]. Proteases can also act as adjuvants to bystander allergens present in the same microenvironment [13,14].Cockroaches have emerged as an important source of indoor allergens worldwide and cockroach extract is shown to be rich in proteases [15]. Previously, Per a 10, a serine protea...

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Section: Discussionsupporting

confidence: 93%

supporting

confidence: 92%

Protease activity of Per a 10 potentiates Th2 polarization by increasing IL‐23 and OX40L

2015

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“…Steroid resistance may be attributed to activation of the STAT5 signaling pathway by TSLP, which cannot be suppressed by corticosteroids in NH cells (26). Similar to this finding, airway inflammation induced by a combined treatment with IL-33 and IL-17 was also found to be resistant to dexamethasone (19).…”

Section: Glucocorticoidssupporting

confidence: 71%

“…These two phenomena may be related to each other. IL-33-mediated airway inflammation augmented by the neutrophil-related cytokine, IL-17, could not be suppressed by dexamethasone (19).…”

Section: Asthmamentioning

confidence: 82%

Interleukin (IL)-33: New Therapeutic Target for Atopic Diseases

Nabe

2014

J Pharmacol Sci

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Abstract. Interleukin (IL)-33, a member of the IL-1 family of cytokines, is produced when epithelial and endothelial cells are exposed to stimuli. Hematopoietic cells such as macrophages also produce IL-33. IL-33 is considered to function as an 'alarmin', activating various immune cells through its receptor ST2, which leads to the production of various molecules. The IL-33-induced production of pro-inflammatory cytokines is a critical event that aggravates atopic diseases such as asthma, atopic dermatitis, and pollenosis and suggests that IL-33-blocking agents could represent new therapeutic drugs. The anti-IL-33 antibody was effective in allergic models, whereas the anti-ST2 antibody has yielded controversial results because soluble ST2 functions as a decoy receptor for IL-33. IL-33-mediated pulmonary inflammation may be glucocorticoidresistant especially when other cytokines act synergistically. Anti-tumor necrosis factor (TNF)-a therapy may also be effective against IL-33-mediated diseases. ERK1/2 inhibitors have also been shown to suppress the production of IL-33. On the other hand, activation of b 2 -receptors enhanced the expression of IL-33 mRNA in dendritic cells by activating protein kinase A (PKA), suggesting that PKA inhibitors may be candidates for IL-33-blocking agents. The effects of IL-33-blocking agents on atopic diseases need to be pharmacologically assessed in experimental and clinical studies.

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“…4C). IL-17A has the capacity to induce both AHR and neutrophil recruitment (28,29,38). We and others have reported that IL-17 contributes to the AHR caused by repeated O 3 exposure in lean mice (43,44).…”

Section: Bodymentioning

confidence: 95%

Innate and ozone-induced airway hyperresponsiveness in obese mice: role of TNF-α

Williams¹,

Mathews²,

Kasahara³

et al. 2015

American Journal of Physiology-Lung Cellular and Molecular Phys

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IL-17A Promotes the Exacerbation of IL-33–Induced Airway Hyperresponsiveness by Enhancing Neutrophilic Inflammation via CXCR2 Signaling in Mice

Cited by 90 publications

References 63 publications

Protease activity of Per a 10 potentiates Th2 polarization by increasing IL‐23 and OX40L

Protease activity of Per a 10 potentiates Th2 polarization by increasing IL‐23 and OX40L

Interleukin (IL)-33: New Therapeutic Target for Atopic Diseases

Innate and ozone-induced airway hyperresponsiveness in obese mice: role of TNF-α

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