B cell repertoire analysis identifies new antigenic domains on glycoprotein B of human cytomegalovirus which are target of neutralizing antibodies

Pötzsch S, Spindler N, Wiegers AK, Fisch T, Ruecker P, Sticht H, Grieb N, Baroti T, Weisel F, Stamminger T, Martin-Parras L, Mach M, Winkler T (2011)

Publication Type: Journal article, Original article

Publication year: 2011

Journal

PLoS Pathogens Public Library of Science

Book Volume: 7

Article Number: e1002172

Journal Issue: 8

DOI: 10.1371/journal.ppat.1002172

Abstract

Human cytomegalovirus (HCMV), a herpesvirus, is a ubiquitously distributed pathogen that causes severe disease in immunosuppressed patients and infected newborns. Efforts are underway to prepare effective subunit vaccines and therapies including antiviral antibodies. However, current vaccine efforts are hampered by the lack of information on protective immune responses against HCMV. Characterizing the B-cell response in healthy infected individuals could aid in the design of optimal vaccines and therapeutic antibodies. To address this problem, we determined, for the first time, the B-cell repertoire against glycoprotein B (gB) of HCMV in different healthy HCMV seropositive individuals in an unbiased fashion. HCMV gB represents a dominant viral antigenic determinant for induction of neutralizing antibodies during infection and is also a component in several experimental HCMV vaccines currently being tested in humans. Our findings have revealed that the vast majority (>90%) of gB-specific antibodies secreted from B-cell clones do not have virus neutralizing activity. Most neutralizing antibodies were found to bind to epitopes not located within the previously characterized antigenic domains (AD) of gB. To map the target structures of these neutralizing antibodies, we generated a 3D model of HCMV gB and used it to identify surface exposed protein domains. Two protein domains were found to be targeted by the majority of neutralizing antibodies. Domain I, located between amino acids (aa) 133-343 of gB and domain II, a discontinuous domain, built from residues 121-132 and 344-438. Analysis of a larger panel of human sera from HCMV seropositive individuals revealed positivity rates of >50% against domain I and >90% against domain II, respectively. In accordance with previous nomenclature the domains were designated AD-4 (Dom II) and AD-5 (Dom I), respectively. Collectively, these data will contribute to optimal vaccine design and development of antibodies effective in passive immunization. © 2011 Pötzsch et al.

Authors with CRIS profile

Sonja Pötzsch Institute of Microbiology – Clinical Microbiology, Immunology and Hygiene Nadja Spindler Medizinische Fakultät Anna-Katharina Wiegers Medizinische Fakultät Heinrich Sticht Professur für Bioinformatik Thomas Stamminger Professur für Virologie Michael Mach Medizinische Fakultät Thomas Winkler Professur für Genetik

Involved external institutions

4-Antibody AG

Switzerland (CH)

How to cite

APA:

Pötzsch, S., Spindler, N., Wiegers, A.-K., Fisch, T., Ruecker, P., Sticht, H.,... Winkler, T. (2011). B cell repertoire analysis identifies new antigenic domains on glycoprotein B of human cytomegalovirus which are target of neutralizing antibodies. PLoS Pathogens, 7(8). https://doi.org/10.1371/journal.ppat.1002172

MLA:

Pötzsch, Sonja, et al. "B cell repertoire analysis identifies new antigenic domains on glycoprotein B of human cytomegalovirus which are target of neutralizing antibodies." PLoS Pathogens 7.8 (2011).

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