Author: Kim, Youngâ€Seok; Lim, Jongkwan; Sung, Jemin; Cheong, Yucheol; Lee, Eunâ€Young; Kim, Jihoon; Oh, Hana; Kim, Yeonâ€Sook; Cho, Namâ€Hyuk; Choi, Seongil; Kang, Sangâ€Moo; Nam, Jaeâ€Hwan; Chae, Wonil; Seong, Baik L.
Title: Builtâ€in RNAâ€mediated chaperone (chaperna) for antigen folding tailored to immunized hosts Cord-id: ln2v50b7 Document date: 2020_5_2
ID: ln2v50b7
Snippet: Highâ€quality antibody (Ab) production depends on the availability of immunologically relevant antigens. We present a potentially universal platform for generating soluble antigens from bacterial hosts, tailored to immunized animals for Ab production. A novel RNAâ€dependent chaperone, in which the target antigen is genetically fused with an RNAâ€interacting domain (RID) docking tag derived from the immunized host, promotes the solubility and robust folding of the target antigen. We selected t
Document: Highâ€quality antibody (Ab) production depends on the availability of immunologically relevant antigens. We present a potentially universal platform for generating soluble antigens from bacterial hosts, tailored to immunized animals for Ab production. A novel RNAâ€dependent chaperone, in which the target antigen is genetically fused with an RNAâ€interacting domain (RID) docking tag derived from the immunized host, promotes the solubility and robust folding of the target antigen. We selected the Nâ€terminal tRNAâ€binding domain of lysylâ€tRNA synthetase (LysRS) as the RID for fusion with viral proteins and demonstrated the expression of the RID fusion proteins in their soluble and native conformations; immunization predominantly elicited Ab responses to the target antigen, whereas the “self†RID tag remained nonimmunogenic. Differential immunogenicity of the fusion proteins greatly enriched and simplified the screening of hybridoma clones of monoclonal antibodies (mAbs), enabling specific and sensitive serodiagnosis of MERSâ€CoV infection. Moreover, mAbs against the consensus influenza hemagglutinin stalk domain enabled a novel assay for trivalent seasonal influenza vaccines. The Fcâ€mediated effector function was demonstrated, which could be harnessed for the design of nextâ€generation “universal†influenza vaccines. The nonimmunogenic builtâ€in antigen folding module tailored to a repertoire of immunized animal hosts will drive immunochemical diagnostics, therapeutics, and designer vaccines.
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