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   <ui>ar1347</ui>
   <ji>ARJ</ji>
   <fm>
      <dochead>Oral presentation</dochead>
      <bibl>
         <title>
            <p>The nonsense allele <it>oblivious </it>reveals a sensor of di-acylglycerides acting in conjunction with TLR2 and TLR6</p>
         </title>
         <aug>
            <au id="A1">
               <snm>Hoebe</snm>
               <fnm>K</fnm>
               <insr iid="I1"/>
            </au>
            <au id="A2">
               <snm>Tabeta</snm>
               <fnm>K</fnm>
               <insr iid="I1"/>
            </au>
            <au id="A3">
               <snm>Georgel</snm>
               <fnm>P</fnm>
               <insr iid="I1"/>
            </au>
            <au id="A4">
               <snm>Du</snm>
               <fnm>X</fnm>
               <insr iid="I1"/>
            </au>
            <au id="A5">
               <snm>Mudd</snm>
               <fnm>S</fnm>
               <insr iid="I1"/>
            </au>
            <au id="A6">
               <snm>Sovath</snm>
               <fnm>S</fnm>
               <insr iid="I1"/>
            </au>
            <au id="A7">
               <snm>Shamel</snm>
               <fnm>L</fnm>
               <insr iid="I1"/>
            </au>
            <au id="A8">
               <snm>Hartung</snm>
               <fnm>T</fnm>
               <insr iid="I2"/>
            </au>
            <au id="A9">
               <snm>Z&#228;hringer</snm>
               <fnm>Ul</fnm>
               <insr iid="I3"/>
            </au>
            <au id="A10">
               <snm>Beutler</snm>
               <fnm>B</fnm>
               <insr iid="I1"/>
            </au>
         </aug>
         <insg>
            <ins id="I1">
               <p>The Scripps Research Institute, La Jolla, California, USA</p>
            </ins>
            <ins id="I2">
               <p>Department of Biochemical Pharmacology, University of Konstanz, Konstanz, Germany</p>
            </ins>
            <ins id="I3">
               <p>Research Center Borstel, Leipniz-center for Medicine and Bioscience, Borstel, Germany</p>
            </ins>
         </insg>
         <source>Arthritis Res Ther</source>
         <supplement>
            <title>
               <p>Global Arthritis Research Network (GARN): 4th World Congress on Arthritis in Montreal</p>
            </title>
            <note>Meeting abstracts</note>
         </supplement>
         <conference>
            <title>
               <p>Global Arthritis Research Network (GARN): 4th World Congress on Arthritis in Montreal</p>
            </title>
            <location>Montreal, Quebec, Canada</location>
            <date-range>20&#8211;22 September 2004</date-range>
         </conference>
         <issn>1478-6354</issn>
         <pubdate>2004</pubdate>
         <volume>6</volume>
         <issue>Suppl 3</issue>
         <fpage>13</fpage>
         <xrefbib>
            <pubid idtype="doi">10.1186/ar1347</pubid>
         </xrefbib>
      </bibl>
      <history>
         <pub>
            <date>
               <day>13</day>
               <month>9</month>
               <year>2004</year>
            </date>
         </pub>
      </history>
   </fm>
   <bdy>
      <sec>
         <st>
            <p/>
         </st>
         <p>The mammalian Toll-like receptors (TLRs) activate cells of the innate immune system when stimulated by diverse ligands of microbial origin. In some instances, these ligands are directly engaged by the TLRs; however, this is not necessarily true in all cases. TLR2 recognizes multiple, structurally disparate microbial ligands, consistent with a requirement for co-receptors in ligand binding. Using <it>N</it>-ethyl-<it>N</it>-nitrosourea, we generated the recessive immunodeficiency phenotype <it>oblivious</it>, in which macrophages show diminished awareness of the S-enantiomer of the di-acylated bacterial lipopeptide MALP-2 and lipoteichoic acid, together with spontaneous ocular colonization by Gram-positive organisms and hypersusceptibility to <it>Staphylococcus aureus </it>infection. <it>Oblivious </it>macrophages readily detect the tri-acylated bacterial lipopeptide PAM<sub>3</sub>CSK<sub>4 </sub>as well as zymosan, revealing that some TLR2 ligands are activated via an <it>Oblivious</it>-independent pathway. The gene responsible for the <it>oblivious </it>phenotype has been positionally cloned. In its ability to carry the lipoteichoic acid and MALP-2 signal to the transmembrane signaling receptors TLR2 and TLR6, <it>Oblivious </it>serves a function analogous to CD14, which concentrates the lipopolysacchardide signal for transduction by TLR4. Besides microbial molecules, <it>oblivious </it>also serves as a receptor for endogenous molecules and may mediate (some) of the inflammatory events involved in the development of atherosclerosis.</p>
      </sec>
   </bdy>
</art>
