Abstract

Contact sensitivity (CS) responses are very common allergic disorders of the skin. Elicitation of the late T cell 24 hr phase of CS in immunized mice requires an early antigen-specific initiating phase. This peaks 2 hr after challenge and depends on local complement activation to elaborate C5a due to antigen binding IgM antibodies produced by B- I cells, leading to vascular activation for local T cell recruitment. We hypothesize that NK T cell derived IL-4 activates the B-1 cells to mediate this CS-initiation.
Aim #1 : Determine the role of IL-4 in the early CS response. CS responses in IL- 4-/- vs. wild type mice will be investigated. If IL-4-/- mice show an impaired early response, the deficient mice will be injected with different doses of IL-4. Activated immune B-1 cells from contact sensitized wild type mice will be transferred into sensitized IL-4 deficient mice and test for elicitation of CS. Mice with defective IL-4 signaling (Stat-6-/-) will also be evaluated similarly.
Aim #2 : Evaluate contact sensitivity in NK T cell- deficient mice. If IL-4 is found involved in CS-initiation, NK T cell deficient mice will be evaluated. Two strains of NK T cell deficient mice will be employed: CDld-/- and Jalpha281-/-. If there is deficient CS, then adoptive cell transfers of FACS purified NK T cells (using CD1d fluorescent tetramers) and B-1 cells (CD 19+ CD5+) will be performed, as well as treatment with different doses of IL-4.
Aim #3 : Analysis of the effects of IL-4 on activation of B-1 cells. The phenotype of the B-1 cells will be analyzed for evidence of activation induced by IL-4. The surface marker Thy-1, expressed in vitro on B cells after IL-4 treatment, and on activated CS-initiating cells, will be analyzed on B-1 cells in CS of wild type mice, as well as in CDld-/- and J281-/- mice. CD23 expression, generally associated with IL-4 activation will be investigated similarly. Further the effect of the NK T cell non-specific activator alpha-GalCer, on activation of B-1 cells also will be evaluated. Summary: The current proposal will investigate the role of IL-4 produced by NK T cells in initiating CS responses. We hypothesize that NK T cellderived IL-4 activates B-1 cells to secrete specific IgM, lading to subsequent Ag- dependent elaboration of C5a to initiate CS. Recognized only a few years ago, NK T cells have not been associated with contact dermatitis, nor with the initiating phase of in vivo T cell mediated immunity, nor with allergies. Furthermore, our studies may have the important result of identifying a physiological ligand for the semi-invariant alpha/beta-TCR on regulatory NK T cells.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Center Core Grants (P30)
Project #
5P30AR041942-09
Application #
6577709
Study Section
Special Emphasis Panel (ZAR1)
Project Start
2002-04-01
Project End
2003-03-31
Budget Start
Budget End
Support Year
9
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
Yale University
Department
Type
DUNS #
082359691
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Dainichi, Teruki; Hayden, Matthew S; Park, Sung-Gyoo et al. (2016) PDK1 Is a Regulator of Epidermal Differentiation that Activates and Organizes Asymmetric Cell Division. Cell Rep 15:1615-23
Askenase, Phillip W; Bryniarski, Krzysztof; Paliwal, Vipin et al. (2015) A subset of AID-dependent B-1a cells initiates hypersensitivity and pneumococcal pneumonia resistance. Ann N Y Acad Sci 1362:200-14
Clark, Paul R; Jensen, Todd J; Kluger, Martin S et al. (2011) MEK5 is activated by shear stress, activates ERK5 and induces KLF4 to modulate TNF responses in human dermal microvascular endothelial cells. Microcirculation 18:102-17
Kwong, Bernice Y; Roberts, Scott J; Silberzahn, Tobias et al. (2010) Molecular analysis of tumor-promoting CD8+ T cells in two-stage cutaneous chemical carcinogenesis. J Invest Dermatol 130:1726-36
Radtke, Christine; Vogt, Peter M; Devor, Marshall et al. (2010) Keratinocytes acting on injured afferents induce extreme neuronal hyperexcitability and chronic pain. Pain 148:94-102
Kirkiles-Smith, Nancy C; Harding, Martha J; Shepherd, Benjamin R et al. (2009) Development of a humanized mouse model to study the role of macrophages in allograft injury. Transplantation 87:189-97
Koga, Yasuo; Pelizzola, Mattia; Cheng, Elaine et al. (2009) Genome-wide screen of promoter methylation identifies novel markers in melanoma. Genome Res 19:1462-70
Yates, Kristin E; Korbel, Gregory A; Shtutman, Michael et al. (2008) Repression of the SUMO-specific protease Senp1 induces p53-dependent premature senescence in normal human fibroblasts. Aging Cell 7:609-21
Pelizzola, Mattia; Koga, Yasuo; Urban, Alexander Eckehart et al. (2008) MEDME: an experimental and analytical methodology for the estimation of DNA methylation levels based on microarray derived MeDIP-enrichment. Genome Res 18:1652-9
Shen, Xiaoyan; Berger, Carole L; Tigelaar, Robert et al. (2008) Development of immunogenic tumor-loaded dendritic cells through physical perturbation and apoptotic cell loading. Immunol Invest 37:798-821

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