7UJ6
Outer Surface Protein C Type K
Summary for 7UJ6
| Entry DOI | 10.2210/pdb7uj6/pdb |
| Descriptor | Outer surface protein C (2 entities in total) |
| Functional Keywords | outer surface protein borrelia burgdorferi, unknown function |
| Biological source | Borreliella burgdorferi |
| Total number of polymer chains | 4 |
| Total formula weight | 70605.30 |
| Authors | Rudolph, M.J.,Mantis, N. (deposition date: 2022-03-30, release date: 2023-04-05, Last modification date: 2023-10-25) |
| Primary citation | Rudolph, M.J.,Davis, S.A.,Haque, H.M.E.,Weis, D.D.,Vance, D.J.,Piazza, C.L.,Ejemel, M.,Cavacini, L.,Wang, Y.,Mbow, M.L.,Gilmore, R.D.,Mantis, N.J. Structural Elucidation of a Protective B Cell Epitope on Outer Surface Protein C (OspC) of the Lyme Disease Spirochete, Borreliella burgdorferi. Mbio, 14:e0298122-e0298122, 2023 Cited by PubMed Abstract: Outer surface protein C (OspC) plays a pivotal role in mediating tick-to-host transmission and infectivity of the Lyme disease spirochete, Borreliella burgdorferi. OspC is a helical-rich homodimer that interacts with tick salivary proteins, as well as components of the mammalian immune system. Several decades ago, it was shown that the OspC-specific monoclonal antibody, B5, was able to passively protect mice from experimental tick-transmitted infection by B. burgdorferi strain B31. However, B5's epitope has never been elucidated, despite widespread interest in OspC as a possible Lyme disease vaccine antigen. Here, we report the crystal structure of B5 antigen-binding fragments (Fabs) in complex with recombinant OspC type A (OspC). Each OspC monomer within the homodimer was bound by a single B5 Fab in a side-on orientation, with contact points along OspC's α-helix 1 and α-helix 6, as well as interactions with the loop between α-helices 5 and 6. In addition, B5's complementarity-determining region (CDR) H3 bridged the OspC-OspC' homodimer interface, revealing the quaternary nature of the protective epitope. To provide insight into the molecular basis of B5 serotype specificity, we solved the crystal structures of recombinant OspC types B and K and compared them to OspC. This study represents the first structure of a protective B cell epitope on OspC and will aid in the rational design of OspC-based vaccines and therapeutics for Lyme disease. The spirochete Borreliella burgdorferi is a causative agent of Lyme disease, the most common tickborne disease in the United States. The spirochete is transmitted to humans during the course of a tick taking a bloodmeal. After B. burgdorferi is deposited into the skin of a human host, it replicates locally and spreads systemically, often resulting in clinical manifestations involving the central nervous system, joints, and/or heart. Antibodies directed against B. burgdorferi's outer surface protein C (OspC) are known to block tick-to-host transmission, as well as dissemination of the spirochete within a mammalian host. In this report, we reveal the first atomic structure of one such antibody in complex with OspC. Our results have implications for the design of a Lyme disease vaccine capable of interfering with multiple stages in B. burgdorferi infection. PubMed: 36976016DOI: 10.1128/mbio.02981-22 PDB entries with the same primary citation |
| Experimental method | X-RAY DIFFRACTION (1.951 Å) |
Structure validation
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