4.7 Article

Identification of Litopenaeus vannamei BiP as a novel cellular attachment protein for white spot syndrome virus by using a biotinylation based affinity chromatography method

期刊

FISH & SHELLFISH IMMUNOLOGY
卷 79, 期 -, 页码 130-139

出版社

ACADEMIC PRESS LTD- ELSEVIER SCIENCE LTD
DOI: 10.1016/j.fsi.2018.05.003

关键词

White spot syndrome virus; Biotinylation; Litopenaeus vannamei; Viral adhesion; Protein-protein interactions

资金

  1. National Natural Science Foundation of China [31402322, 31472299]
  2. National Basic Research Program (973) of China [2012CB114405]
  3. Tianjin Research Program of Application Foundation and Advanced Technology [15JCQNJC46400, 15JCZDJC33800]
  4. Innovation Team of Tianjin Fisheries Research System [ITTFRS2017007]
  5. Innovation team cultivation program for Tianjin institutions of higher education [TD13-5076]
  6. High Level Innovation and Entrepreneurship Team of Tianjin Special Support Program for Talents Development
  7. Tianjin Normal University Doctoral Research Foundation [52XB1412]

向作者/读者索取更多资源

White spot syndrome virus (WSSV) is a dangerous threat to shrimp farming that also attacks a wide range of crustaceans. Knowledge of the surface protein-protein interactions between the pathogen and host is very crucial to unraveling the molecular pathogenesis mechanisms of WSSV. In this study, LvBiP (Litopenaeus vannamei immunoglobulin heavy-chain-binding protein) was identified as a novel WSSV binding protein of L. vannamei by a biotinylation based affinity chromatography method. By using pull-down and ELISA assays, the binding of recombinant LvBiP to WSSV was proved to be specific and ATP- dependent. The interaction was also confirmed by the result of co-immunoprecipitation assay. Immunofluorescence studies revealed the co-localization of LvBiP with WSSV on the cell surface of shrimp haemocytes. Additionally, LvBiP is likely to play an important role in WSSV infection. Treatment of gill cellular membrane proteins (CMPs) with purified rLvBiP and antibody that specifically recognizes LvBiP, led to a significant reduction in the binding of WSSV to gill CMPs. In the in vivo neutralization assay, rLvBiP and anti-LvBiP polyclonal antibody partially blocked the infection of WSSV. Taken together, the results indicate that LvBiP, a molecular chaperon of the HSP70 family, is a novel host factor involved at the step of attachment of the WSSV to the host cells and a potential candidate of therapeutic target.

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