Abstract

IL-13 is a Th2 cytokine that has been shown to be critical for the development of allergic inflammation. IL-13 mediates its effects via a complex receptor system that includes IL-4Ralpha and two other cell surface proteins, IL-13Ralpha1 and IL-13Ralpha2. IL-13Ralpha1 binds IL-13 with low affinity by itself, but when paired with IL-14Ralpha, it binds IL-13 with high affinity and forms a functional IL-13 receptor that signals. Expression of IL-13Ralpha2 in vitro was insufficient to render cells responsive to IL-13, despite high affinity binding even in the presence of IL-4Ralpha. IL-13Ralpha2 has a short cytoplasmic tail, which contains no box 1 or box 2 signaling motifs, supporting that it has no signaling function. The inability of IL-13Ralpha2 expression to confer IL-13 responsiveness despite high affinity binding, along with the finding of soluble IL-13Ralpha2 in vivo, has led to speculation that IL-13Ralpha2 is a decoy receptor. This theory was further supported by the recent characterization of the IL-13Ralpha2-deficient mice that were found to have elevated IgE levels. Although IL-13Ralpha indeed may act as a decoy receptor under some circumstances, it may have other yet unrecognized functions. Recently, we have observed that allergen-induced airway hyperreactivity (AHR) is enhanced in mice that overexpress IL-13Ralpha2 in the lungs. Furthermore, our collaborator, Marsha Wills-Karp, has observed that allergen-induced AHR is decreased in mice that are deficient in IL-13Ralpha2 when compared with wild-type mice. In contrast to the allergen sensitization and challenge model, we observed no change in AHR in mice that overexpress IL-13Ralpha2 in the lungs following IL-13 treatment intratracheally for 3 days. These observations support that under some circumstances IL-13Ralpha2 may contribute to IL-13 responses and that the contribution of IL-13Ralpha2 may be distinct under conditions of chronic vs. acute inflammation. The studies proposed herein will examine this possibility by testing the 2 following hypotheses: (1) IL-13Ralpha2 is not a simple decoy receptor, but can contribute to the allergic response during chronic inflammation; and (2) the subcellular localization of IL-13Ralpha2, as well as the level and timing of IL-13Ralpha2 expression, may be critical in determining its final contribution to the IL-13 response.
In Aim #1, we will determine the effect of IL-13Ralpha2 overexpression in 3 different models of chronic allergic inflammation.
In Aims #2 -3, we will elucidate the mechanism by which IL-13Ralpha2 influences IL-13 responses. We will examine how the level, subcellular location, and cell type of IL-13Ralpha2 expression relates to its function. By providing information about how responses to IL-13 are regulated at the receptor level, our results will complement proposals in this program project that study regulation of IL-13 production and evaluate genes important for asthma that are activated by both IL-4 and IL-13 or by IL-13 alone.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL076383-05
Application #
7637822
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
Project End
Budget Start
2008-07-01
Budget End
2009-06-30
Support Year
5
Fiscal Year
2008
Total Cost
$426,314
Indirect Cost

  Institution

Name
Cincinnati Children's Hospital Medical Center
Department
Type
DUNS #
071284913
City
Cincinnati
State
OH
Country
United States
Zip Code
45229

  Publications

Mehta, Minesh; Hetta, Helal F; Abdel-Hameed, Enass A et al. (2016) Association between IL28B rs12979860 single nucleotide polymorphism and the frequency of colonic Treg in chronically HCV-infected patients. Arch Virol 161:3161-9
Hetta, Helal F; Mekky, Mohamed A; Khalil, Nasr K et al. (2015) Association of colonic regulatory T cells with hepatitis C virus pathogenesis and liver pathology. J Gastroenterol Hepatol 30:1543-51
Lajoie, S; Lewkowich, I; Herman, N S et al. (2014) IL-21 receptor signalling partially mediates Th2-mediated allergic airway responses. Clin Exp Allergy 44:976-85
Abdel-Hameed, Enass A; Ji, Hong; Sherman, Kenneth E et al. (2014) Epigenetic modification of FOXP3 in patients with chronic HIV infection. J Acquir Immune Defic Syndr 65:19-26
Kinker, Kayla G; Gibson, Aaron M; Bass, Stacey A et al. (2014) Overexpression of dimethylarginine dimethylaminohydrolase 1 attenuates airway inflammation in a mouse model of asthma. PLoS One 9:e85148
Fulkerson, Patricia C; Rothenberg, Marc E (2013) Targeting eosinophils in allergy, inflammation and beyond. Nat Rev Drug Discov 12:117-29
Chen, Weiguo; Sivaprasad, Umasundari; Gibson, Aaron M et al. (2013) IL-13 receptor ?2 contributes to development of experimental allergic asthma. J Allergy Clin Immunol 132:951-8.e1-6
Sivaprasad, Umasundari; Askew, David J; Ericksen, Mark B et al. (2011) A nonredundant role for mouse Serpinb3a in the induction of mucus production in asthma. J Allergy Clin Immunol 127:254-61, 261.e1-6
Perkins, Charles; Yanase, Noriko; Smulian, George et al. (2011) Selective stimulation of IL-4 receptor on smooth muscle induces airway hyperresponsiveness in mice. J Exp Med 208:853-67
Zhu, Hongyan; Perkins, Charles; Mingler, Melissa K et al. (2011) The role of neuropeptide S and neuropeptide S receptor 1 in regulation of respiratory function in mice. Peptides 32:818-25

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