The lung vascular filter as a site of immune induction for T cell responses to large embolic antigen

doi:10.1084/jem.20082401

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doi:10.1084/jem.20082401
The Journal of Experimental Medicine
The Rockefeller University Press, 0022-1007 $30.00
© Willart et al.

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Article

The lung vascular filter as a site of immune induction for T cell responses to large embolic antigen

Monique A.M. Willart¹, Hendrik Jan de Heer², Hamida Hammad¹, Thomas Soullié², Kim Deswarte¹, Björn E. Clausen³, Louis Boon⁴, Henk C. Hoogsteden², and Bart N. Lambrecht¹^,2

¹ Laboratory of Immunoregulation and Mucosal Immunology, Department of Pulmonary Medicine, University of Ghent, Ghent B-9000, Belgium
² Department of Pulmonary Medicine and ³ Department of Immunology, Erasmus Medical Center, Rotterdam 3000 CA, Netherlands
⁴ Bioceros B.V., Utrecht 3584 CM, Netherlands

CORRESPONDENCE Bart N. Lambrecht: Bart.lambrecht{at}ugent.be

The bloodstream is an important route of dissemination of invadingpathogens. Most of the small bloodborne pathogens, like bacteriaor viruses, are filtered by the spleen or liver sinusoids andpresented to the immune system by dendritic cells (DCs) thatprobe these filters for the presence of foreign antigen (Ag).However, larger pathogens, like helminths or infectious emboli,that exceed 20 µm are mostly trapped in the vasculatureof the lung. To determine if Ag trapped here can be presentedto cells of the immune system, we used a model of venous embolismof large particulate Ag (in the form of ovalbumin [OVA]-coatedSepharose beads) in the lung vascular bed. We found that largeAgs were presented and cross-presented to CD4 and CD8 T cellsin the mediastinal lymph nodes (LNs) but not in the spleen orliver-draining LNs. Dividing T cells returned to the lungs,and a short-lived infiltrate consisting of T cells and DCs formedaround trapped Ag. This infiltrate was increased when the Toll-likereceptor 4 was stimulated and full DC maturation was inducedby CD40 triggering. Under these conditions, OVA-specific cytotoxicT lymphocyte responses, as well as humoral immunity, were induced.The T cell response to embolic Ag was severely reduced in micedepleted of CD11c^hi cells or Ly6C/G⁺ cells but restored uponadoptive transfer of Ly6C^hi monocytes. We conclude that thelung vascular filter represents a largely unexplored site ofimmune induction that traps large bloodborne Ags for presentationby monocyte-derived DCs.

M.A.M. Willart and H. Jan de Heer contributed equally to thispaper.

Abbreviations used: Ag, antigen; DT, diphtheria toxin; DTR, diphtheria toxin receptor; MCP-1, monocyte chemotactic protein 1; MLN, mediastinal LN; OB, OVA bead; pDC, plasmacytoid DC; PLN, peripheral LN; PPD, purified protein derivate; Tg, transgenic; UB, uncoated bead.

© 2009 Willart et al.
This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.jem.org/misc/terms.shtml). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 3.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/3.0/).

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