RSV A2-Based Prefusion F Vaccine Candidates Induce RSV A and RSV B Cross Binding and Neutralizing Antibodies and Provide Protection against RSV A and RSV B Challenge in Preclinical Models

被引:9
作者
Cox, Freek [1 ]
Saeland, Eirikur [1 ]
Thoma, Anne [1 ]
van den Hoogen, Ward [1 ]
Tettero, Lisanne [1 ]
Drijver, Joke [1 ]
Vaneman, Cornelis [1 ]
van Polanen, Yolinda [1 ]
Ritschel, Tina [1 ]
Bastian, Arangassery Rosemary [1 ]
Callendret, Benoit [1 ]
Zahn, Roland [1 ]
van der Fits, Leslie [1 ]
机构
[1] Janssen Vaccines & Prevent BV, Archimedesweg 4 6, NL-2333 CN Leiden, Netherlands
关键词
Adenoviral vector 26; cotton rat model; respiratory syncytial virus; RSV prefusion protein; RSV subtypes; VIRUS FUSION PROTEIN; POSTFUSION F; DESIGN;
D O I
10.3390/vaccines11030672
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
RSV is divided into two antigenic subtypes, RSV A and RSV B, which is largely based on the variation in the G protein, while the fusion protein F is more conserved and a target for antibody-mediated neutralization. Here we evaluate the breadth of the protective immune responses across RSV A and RSV B subtypes, induced by vaccines based on the RSV A-based fusion protein, stabilized in the prefusion conformation (preF) in preclinical models. Immunization of naive cotton rats with preF subunit or preF encoded by a replication incompetent Adenoviral 26, induced antibodies capable of neutralizing recent RSV A and RSV B clinical isolates, as well as protective efficacy against a challenge with RSV A and RSV B strains. Similarly, induction of cross-neutralizing antibodies was observed after immunization with Ad26-encoded preF, preF protein or a mix of both (Ad26/preF protein) in RSV pre-exposed mice and African Green Monkeys. Transfer of serum of human subjects immunized with Ad26/preF protein into cotton rats provide protection against challenges with both RSV A and RSV B, with complete protection against both strains observed in the lower respiratory tract. In contrast, almost no protection against RSV A and B infection was observed after the transfer of a human serum pool isolated pre-vaccination. These results collectively show that the RSV A-based monovalent Ad26/preF protein vaccine induced neutralizing antibodies, as well as protection against both RSV A and RSV B subtypes in animals, including by passive transfer of human antibodies alone, suggesting that clinical efficacy against both subtypes can be achieved.
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页数:14
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