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Wiskott-Aldrich Syndrome Protein Is Required for Homeostasis and Function of Invariant NKT Cells¹

Alexander Astrakhan^*, Hans D. Ochs and David J. Rawlings^2,*,

^* Department of Immunology and Department of Pediatrics, University of Washington School of Medicine and Seattle Children’s Research Institute, Seattle, WA 98101

NKT cells comprise a separate T lineage expressing semi-invariant T cell receptors. Canonical invariant NKT (iNKT) cells specifically recognize lipid Ags presented by CD1d, a MHC class I-like molecule. iNKT cells function, in part, as initial responders to bacterial infection and play a role in immune surveillance and tumor rejection. The Wiskott-Aldrich Syndrome protein (WASp) serves as a crucial link between cellular stimuli and cytoskeletal rearrangements. Although we and others have identified a key role for WASp in homeostasis of T-regulatory and marginal zone B cells, little data exist regarding the role for WASp within the iNKT lineage. Analysis of WASp-expressing cell populations in heterozygous female WASp mice revealed a substantial selective advantage for WASp⁺ vs WASp^– iNKT cells. Although adult WASp-deficient (WASp^–/–) mice had normal thymic and bone marrow iNKT numbers, we observed 2- to 3-fold reduction in the numbers of iNKT cells in the spleen and liver. This peripheral iNKT deficit is manifested, in part, due to defective iNKT homeostasis. WASp^–/– iNKT cells exhibited reduced levels of integrin surface expression and decreased homing and/or retention within peripheral tissues in a competitive repopulation model. In addition, analysis of young mice showed that WASp is important for both maturation and egress of thymic iNKT cells. WASp^–/– iNKT cells also exhibited a marked reduction in Ag-induced proliferation and cytokine production. Our findings highlight the crucial role for WASp in iNKT development, homeostasis, and activation, and identify iNKT dysfunction as an additional factor likely to contribute to the clinical features observed in WAS patients.

The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked advertisement in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

¹ This work was supported by a grant from the National Institutes of Health (AI071163; DJR). A.A. is supported by the Cell and Molecular Biology Training Grant (T32GM007270) and the Molecular Medicine fellowship.

² Address correspondence and reprint requests to Dr. David J. Rawlings, Seattle Children’s Research Institute, 1900 Ninth Avenue, Seattle, WA 98101. E-mail address: drawling{at}u.washington.edu

³ Abbreviations used in this paper: MZ, marginal zone; WASp, Wiskott-Aldrich Syndrome protein; iNKT, invariant NKT; GalCer, -galactosylceramide; Treg, regulatory T cell; WT, wild type; HSC, hematopoietic stem cell; S1P, sphingosine-1-phosphate; LN, lymph node; DC, dendritic cell; MFI, median fluorescence intensity.

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The JI 2009 182: 7329-7330. [Full Text]