The 1 H, 15 N, and 13 C resonance assignments of a single-domain antibody against immunoglobulin G

Author:

Leite Vanessa Bezerra Oliveira1,Andrade Rafael Alves1,Almeida Fabio Ceneviva Lacerda1,Nascimento Claudia Jorge2,Araújo Talita Stelling1,Almeida Marcius Silva1

Affiliation:

1. Federal University of Rio de Janeiro

2. Federal University of the State of Rio de Janeiro (UNIRIO)

Abstract

Abstract

Research on camelid-derived single-domain antibodies (sdAbs) has demonstrated their significant utility in diverse biotechnological applications, including therapy and diagnostic. This is largely due to their relative simplicity as monomeric proteins, ranging from 12–15 kDa, in contrast to immunoglobulin G (IgG) antibodies, which are glycosylated heterotetramers of 150–160 kDa. Single-domain antibodies exhibit high conformational stability and adopt the typical immunoglobulin domain fold, consisting of a two-layer sandwich of 7–9 antiparallel beta-strands. They contain three loops, known as complementary-determining regions (CDRs), which are assembled on the sdAb surface and are responsible for antigen recognition. The single-domain antibody examined in this study, sdAb-mrh-IgG, was engineered to recognize IgG from rats, mice, but it also weakly recognizes IgG from humans (Pleiner et al. 2018). A search of the Protein Data Bank revealed only one NMR structure of a single-domain antibody, which is unrelated to sdAb-mrh-IgG. The NMR chemical shift assignments of sdAb-mrh-IgG will be utilized to study its molecular dynamics and interactions with antigens in solution, which is fundamental for the rational design of novel single-domain antibodies.

Publisher

Springer Science and Business Media LLC

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