Literature DB >> 15611257

The functional and structural properties of MD-2 required for lipopolysaccharide binding are absent in MD-1.

Naoko Tsuneyoshi1, Kenji Fukudome, Jun Kohara, Rika Tomimasu, Jean-Francois Gauchat, Hiroshi Nakatake, Masao Kimoto.   

Abstract

MD-1 and MD-2 are secretory glycoproteins that exist on the cell surface in complexes with transmembrane proteins. MD-1 is anchored by radioprotective 105 (RP105), and MD-2 is associated with TLR4. In vivo studies revealed that MD-1 and MD-2 have roles in responses to LPS. Although the direct binding function of MD-2 to LPS has been observed, the physiological function of MD-1 remains unknown. In this study, we compared the LPS-binding functions of MD-1 and MD-2. LPS binding to cell surface complexes was detected for cells transfected with TLR4/MD-2. In contrast, binding was not observed for RP105/MD-1-transfected cells. When rMD-2 protein was expressed in Escherichia coli, it was purified in complexes containing LPS. In contrast, preparations of MD-1 did not contain LPS. When rMD-2 protein was prepared in a mutant strain lacking the lpxM gene, LPS binding disappeared. Therefore, the secondary myristoyl chain attached to the (R)-3-hydroxymyristoyl chain added by LpxM is required for LPS recognition by MD-2, under these conditions. An amphipathic cluster composed of basic and hydrophobic residues in MD-2 has been suggested to be the LPS-binding site. We specifically focused on two Phe residues (119 and 121), which can associate with fatty acids. A mutation at Phe(191) or Phe(121) strongly reduced binding activity, and a double mutation at these residues prevented any binding from occurring. The Phe residues are present in MD-2 and absent in MD-1. Therefore, the LPS recognition mechanism by RP105/MD-1 is distinct from that of TLR4/MD-2.

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Year:  2005        PMID: 15611257     DOI: 10.4049/jimmunol.174.1.340

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  13 in total

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3.  Comparison of lipopolysaccharide-binding functions of CD14 and MD-2.

Authors:  Jun Koraha; Naoko Tsuneyoshi; Masao Kimoto; Jean-Francois Gauchat; Hiroshi Nakatake; Kenji Fukudome
Journal:  Clin Diagn Lab Immunol       Date:  2005-11

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8.  Studies of the TLR4-associated protein MD-2 using yeast-display and mutational analyses.

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9.  RP105 facilitates macrophage activation by Mycobacterium tuberculosis lipoproteins.

Authors:  Antje Blumenthal; Toshihiko Kobayashi; Lynda M Pierini; Niaz Banaei; Joel D Ernst; Kensuke Miyake; Sabine Ehrt
Journal:  Cell Host Microbe       Date:  2009-01-22       Impact factor: 21.023

10.  Drosophila melanogaster NPC2 proteins bind bacterial cell wall components and may function in immune signal pathways.

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