Author: Sangesland, Maya; Yousif, Ashraf S.; Ronsard, Larance; Kazer, Samuel W.; Zhu, Alex Lee; Gatter, G. James; Hayward, Matthew R.; Barnes, Ralston M.; Quirindongo-Crespo, Maricel; Rohrer, Daniel; Lonberg, Nils; Kwon, Douglas; Shalek, Alex K.; Lingwood, Daniel
Title: A Single Human V(H)-gene Allows for a Broad-Spectrum Antibody Response Targeting Bacterial Lipopolysaccharides in the Blood Cord-id: jh39yygg Document date: 2020_8_25
ID: jh39yygg
Snippet: B cell receptors (BCRs) display a combination of variable (V)-gene-encoded complementarity determining regions (CDRs) and adaptive/hypervariable CDR3 loops to engage antigens. It has long been proposed that the former tune for recognition of pathogens or groups of pathogens. To experimentally evaluate this within the human antibody repertoire, we perform immune challenges in transgenic mice that bear diverse human CDR3 and light chains but are constrained to different human V(H)(-)genes. We find
Document: B cell receptors (BCRs) display a combination of variable (V)-gene-encoded complementarity determining regions (CDRs) and adaptive/hypervariable CDR3 loops to engage antigens. It has long been proposed that the former tune for recognition of pathogens or groups of pathogens. To experimentally evaluate this within the human antibody repertoire, we perform immune challenges in transgenic mice that bear diverse human CDR3 and light chains but are constrained to different human V(H)(-)genes. We find that, of six commonly deployed V(H) sequences, only those CDRs encoded by IGHV1-2(∗)02 enable polyclonal antibody responses against bacterial lipopolysaccharide (LPS) when introduced to the bloodstream. The LPS is from diverse strains of gram-negative bacteria, and the V(H)-gene-dependent responses are directed against the non-variable and universal saccrolipid substructure of this antigen. This reveals a broad-spectrum anti-LPS response in which germline-encoded CDRs naturally hardwire the human antibody repertoire for recognition of a conserved microbial target.
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