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Design, expression, and characterization of a novel dendritic cell-targeted proteins.
Wang, Yu; Zhu, Xiao Ming; Wang, Fang; Wu, Shuai; Wang, Zi Cheng; Du, Zhi Yan; Yan, Jin Qi; Yu, Ji Yun.
Affiliation
  • Wang Y; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China.
  • Zhu XM; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China.
  • Wang F; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China.
  • Wu S; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China.
  • Wang ZC; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China.
  • Du ZY; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China.
  • Yan JQ; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China. Electronic address: yanjinqi@sohu.com.
  • Yu JY; Beijing Institute of Basic Medical Sciences, 27 Tai Ping Road, Beijing 100850, China. Electronic address: yujyun@126.com.
Biochem Biophys Res Commun ; 460(2): 227-32, 2015 May 01.
Article in En | MEDLINE | ID: mdl-25769955
ABSTRACT
In vivo approaches to inducing an effective immune response focus on targeted antigen (Ag) delivery to dendritic cells (DCs). In this study, we developed a new method of targeting plasmid DNA and/or the antigen (Ag)-antibody (Ab) complex to DCs via the DC receptor DEC-205, also known as cluster of differentiation CD205. We cloned and expressed a recombinant protein composed of mouse DEC-205-specific single-chain fragment variable region (mDEC-205-scFv), the streptococcal protein G (SPG) IgG-binding domain and cationic peptide (CP), which named mDEC205-scFv-SPG-CP (msSC). In vitro, the recombinant protein msSC can specifically bind to DCs through the section of mDEC-205-scFv, and bound the Ag-Ab complex via SPG as well as plasmid DNA through electrostatic bonding with CP in vitro. In addition, msSC functioned in a manner similar to anti-DEC-205 monoclonal Ab and bound to mouse bone marrow-derived DCs. It was demonstrated in vivo that msSC can target plasmid DNA to DCs, resulting in efficient uptake and expression. Moreover, msSC can form a complex with pGL3-CMV and transport it to draining lymph nodes when injected in vivo. These results indicate that msSC can be used as a carrier protein for vaccine delivery to DCs via formation of plasmid DNA-Ag-Ab ternary complexes.
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Full text: 1 Database: MEDLINE Main subject: Dendritic Cells Limits: Animals Language: En Year: 2015 Type: Article

Full text: 1 Database: MEDLINE Main subject: Dendritic Cells Limits: Animals Language: En Year: 2015 Type: Article