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<pubDate>Thu, 21 Aug 2008 15:09:35 BST</pubDate>


	<title>CiteULike: AlfonsoVicenteSuarez's Haury</title>
	<description>CiteULike: AlfonsoVicenteSuarez's Haury</description>


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<item rdf:about="http://www.citeulike.org/user/AlfonsoVicenteSuarez/article/1382216">
    <title>Regulatory T Cells Selectively Express Toll-like Receptors and Are Activated by Lipopolysaccharide</title>
    <link>http://www.citeulike.org/user/AlfonsoVicenteSuarez/article/1382216</link>
    <description>&lt;i&gt;J. Exp. Med., Vol. 197, No. 4. (17 February 2003), pp. 403-411.&lt;/i&gt;&lt;br /&gt;&lt;br /&gt;Regulatory CD4 T cells (Treg) control inflammatory reactions to commensal bacteria and opportunist pathogens. Activation of Treg functions during these processes might be mediated by host-derived proinflammatory molecules or directly by bacterial products. We tested the hypothesis that engagement of germline-encoded receptors expressed by Treg participate in the triggering of their function. We report that the subset of CD4 cells known to exert regulatory functions in vivo (CD45RBlow CD25+) selectively express Toll-like receptors (TLR)-4, -5, -7, and -8. Exposure of CD4+ CD25+ cells to the TLR-4 ligand lipopolysaccharide (LPS) induces up-regulation of several activation markers and enhances their survival/proliferation. This proliferative response does not require antigen-presenting cells and is augmented by T cell receptor triggering and interleukin 2 stimulation. Most importantly, LPS treatment increases CD4+ CD25+ cell suppressor efficiency by 10-fold and reveals suppressive activity in the CD4+ CD45RBlow CD25- subset that when tested ex-vivo, scores negative. Moreover, LPS-activated Treg efficiently control naive CD4 T cell-dependent wasting disease. These findings provide the first evidence that Treg respond directly to proinflammatory bacterial products, a mechanism that likely contributes to the control of inflammatory responses. 10.1084/jem.20021633</description>
    <dc:title>Regulatory T Cells Selectively Express Toll-like Receptors and Are Activated by Lipopolysaccharide</dc:title>

    <dc:creator>Iris Caramalho</dc:creator>
    <dc:creator>Thiago Lopes-Carvalho</dc:creator>
    <dc:creator>Dominique Ostler</dc:creator>
    <dc:creator>Santiago Zelenay</dc:creator>
    <dc:creator>Matthias Haury</dc:creator>
    <dc:creator>Jocelyne Demengeot</dc:creator>
    <dc:identifier>doi:10.1084/jem.20021633</dc:identifier>
    <dc:source>J. Exp. Med., Vol. 197, No. 4. (17 February 2003), pp. 403-411.</dc:source>
    <dc:date>2007-06-12T21:34:17-00:00</dc:date>
    <prism:publicationYear>2003</prism:publicationYear>
    <prism:publicationName>J. Exp. Med.</prism:publicationName>
    <prism:volume>197</prism:volume>
    <prism:number>4</prism:number>
    <prism:startingPage>403</prism:startingPage>
    <prism:endingPage>411</prism:endingPage>
    <prism:category>tlr5-flagellin</prism:category>
    <prism:category>tlrs-lymphocytes</prism:category>
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