Neutralization of Diverse Human Cytomegalovirus Strains Conferred by Antibodies Targeting Viral gH/gL/pUL128-131 Pentameric Complex

Authors

Sha Ha, Merck & Company
Fengsheng Li, Merck & Company
Matthew C. Troutman, Merck & Company
Daniel C. Freed, Merck & Company
Aimin Tang, Merck & Company
John W. Loughney, Merck & Company
Dai Wang, Merck & Company
I-Ming Wang, Merck & Company
Josef Vlasak, Merck & Company
David C. Nickle, Merck & Company
Richard R. Rustandi, Merck & Company
Melissa Hamm, Merck & Company
Pete A. DePhillips, Merck & Company
Ningyan Zhang, University of Texas
Jason S. McLellan, Dartmouth College
Hua Zhu, New Jersey Medical School
Stuart P. Adler, CMV Research Foundation
Michael A. McVoy, Virginia Commonwealth University
Zhiqiang An, University of Texas
Tong-Ming Fu, Merck & Company

Document Type

Article

Original Publication Date

2017

Journal/Book/Conference Title

JOURNAL OF VIROLOGY

Volume

91

Issue

7

First Page

1

Last Page

15

DOI of Original Publication

10.1128/JVI.02033-16

Comments

Originally published at http://doi.org/10.1128/JVI.02033-16

Date of Submission

June 2017

Abstract

Human cytomegalovirus (HCMV) is the leading cause of congenital viral infection, and developing a prophylactic vaccine is of high priority to public health. We recently reported a replication-defective human cytomegalovirus with restored pentameric complex glycoprotein H (gH)/gL/pUL128-131 for prevention of congenital HCMV infection. While the quantity of vaccine-induced antibody responses can be measured in a viral neutralization assay, assessing the quality of such responses, including the ability of vaccine-induced antibodies to cross-neutralize the field strains of HCMV, remains a challenge. In this study, with a panel of neutralizing antibodies from three healthy human donors with natural HCMV infection or a vaccinated animal, we mapped eight sites on the dominant virus-neutralizing antigen-the pentameric complex of glycoprotein H (gH), gL, and pUL128, pUL130, and pUL131. By evaluating the site-specific antibodies in vaccine immune sera, we demonstrated that vaccination elicited functional antiviral antibodies to multiple neutralizing sites in rhesus macaques, with quality attributes comparable to those of CMV hyperimmune globulin. Furthermore, these immune sera showed antiviral activities against a panel of genetically distinct HCMV clinical isolates. These results highlighted the importance of understanding the quality of vaccine-induced antibody responses, which includes not only the neutralizing potency in key cell types but also the ability to protect against the genetically diverse field strains.

IMPORTANCE HCMV is the leading cause of congenital viral infection, and development of a preventive vaccine is a high public health priority. To understand the strain coverage of vaccine-induced immune responses in comparison with natural immunity, we used a panel of broadly neutralizing antibodies to identify the immunogenic sites of a dominant viral antigen-the pentameric complex. We further demonstrated that following vaccination of a replication-defective virus with the restored pentameric complex, rhesus macaques can develop broadly neutralizing antibodies targeting multiple immunogenic sites of the pentameric complex. Such analyses of site-specific antibody responses are imperative to our assessment of the quality of vaccine-induced immunity in clinical studies.

Rights

Copyright © 2017 Ha et al. This is an openaccess article distributed under the terms of the Creative Commons Attribution 4.0 International license.

Is Part Of

VCU Biochemistry and Molecular Biology Publications