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The essentiality of α‐2‐macroglobulin in human salivary innate immunity against new H1N1 swine origin influenza A virus
Authors:Chao‐Hsuan Chen  Xing‐Quan Zhang  Chih‐Wei Lo  Pei‐Feng Liu  Yu‐Tsueng Liu  Richard L. Gallo  Ming‐Fa Hsieh  Robert T. Schooley  Chun‐Ming Huang
Affiliation:1. Division of Dermatology, Department of Medicine, University of California, San Diego, CA, USA;2. VA San Diego Healthcare Center, San Diego, CA, USA;3. Department of Biomedical Engineering and R&D Center for Biomedical Microdevice Technology, Chung Yuan Christian University, Chung Li, Taiwan;4. Division of Infectious Diseases, Department of Medicine, University of California, San Diego, CA, USA;5. Institute of Biotechnology & Department of Life Science, National Tsing Hua University, Hsinchu, Taiwan;6. Moores Cancer Center;7. University of California, San Diego, CA, USA
Abstract:A novel strain of influenza A H1N1 emerged in the spring of 2009 and has spread rapidly throughout the world. Although vaccines have recently been developed that are expected to be protective, their availability was delayed until well into the influenza season. Although anti‐influenza drugs such as neuraminidase inhibitors can be effective, resistance to these drugs has already been reported. Although human saliva was known to inhibit viral infection and may thus prevent viral transmission, the components responsible for this activity on influenza virus, in particular, influenza A swine origin influenza A virus (S‐OIV), have not yet been defined. By using a proteomic approach in conjunction with beads that bind α‐2,6‐sialylated glycoprotein, we determined that an α‐2‐macroglobulin (A2M) and an A2M‐like protein are essential components in salivary innate immunity against hemagglutination mediated by a clinical isolate of S‐OIV (San Diego/01/09 S‐OIV). A model of an A2M‐based “double‐edged sword” on competition of α‐2,6‐sialylated glycoprotein receptors and inactivation of host proteases is proposed. We emphasize that endogenous A2M in human innate immunity functions as a natural inhibitor against S‐OIV.
Keywords:α  ‐2,6‐Sialylated glycoproteins  α  ‐2‐Macroglobulin  H1N1 swine origin influenza A virus  Microbiology  Salivary innate immunity
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