Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector

Bo Liang; Joan O. Ngwuta; Richard Herbert; Joanna Swerczek; David W. Dorward; Emerito Amaro-Carambot; Natalie Mackow; Barbora Kabatova; Matthias Lingemann; Sonja Surman; Lijuan Yang; Man Chen; Syed M. Moin; Azad Kumar; Jason S. McLellan; Peter D. Kwong; Barney S. Graham; Anne Schaap-Nutt; Peter L. Collins; Shirin Munir

doi:10.1128/JVI.01196-16

Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector

Bo Liang
, Joan O. Ngwuta
, Richard Herbert
, Joanna Swerczek
, David W. Dorward
, Emerito Amaro-Carambot
, Natalie Mackow
, Barbora Kabatova
, Matthias Lingemann
, Sonja Surman
, Lijuan Yang
, Man Chen
, Syed M. Moin
, Azad Kumar
, Jason S. McLellan
, Peter D. Kwong
, Barney S. Graham
, Anne Schaap-Nutt
, Peter L. Collins
, Shirin Munir

Infectious Diseases

National Institutes of Health
Dartmouth College

Research output: Contribution to journal › Article › peer-review

36 Scopus citations

Abstract

Human respiratory syncytial virus (RSV) and human parainfluenza virus type 3 (HPIV3) are major pediatric respiratory pathogens that lack vaccines. A chimeric bovine/human PIV3 (rB/HPIV3) virus expressing the unmodified, wild-type (wt) RSV fusion (F) protein from an added gene was previously evaluated in seronegative children as a bivalent intranasal RSV/HPIV3 vaccine, and it was well tolerated but insufficiently immunogenic for RSV F. We recently showed that rB/HPIV3 expressing a partially stabilized prefusion form (pre-F) of RSV F efficiently induced "high-quality" RSV-neutralizing antibodies, defined as antibodies that neutralize RSV in vitro without added complement (B. Liang et al., J Virol 89:9499 -9510, 2015, doi:10.1128/JVI.01373-15). In the present study, we modified RSV F by replacing its cytoplasmic tail (CT) domain or its CT and transmembrane (TM) domains (TMCT) with counterparts from BPIV3 F, with or without pre-F stabilization. This resulted in RSV F being packaged in the rB/HPIV3 particle with an efficiency similar to that of RSV particles. Enhanced packaging was substantially attenuating in hamsters (10- to 100-fold) and rhesus monkeys (100- to 1,000-fold). Nonetheless, TMCT-directed packaging substantially increased the titers of high-quality RSV-neutralizing serum antibodies in hamsters. In rhesus monkeys, a strongly additive immunogenic effect of packaging and pre-F stabilization was observed, as demonstrated by 8- and 30-fold increases of RSV-neutralizing serum antibody titers in the presence and absence of added complement, respectively, compared to pre-F stabilization alone. Analysis of vaccine-induced F-specific antibodies by binding assays indicated that packaging conferred substantial stabilization of RSV F in the pre-F conformation. This provides an improved version of this well-tolerated RSV/HPIV3 vaccine candidate, with potently improved immunogenicity, which can be returned to clinical trials.

Original language	English
Pages (from-to)	10022-10038
Number of pages	17
Journal	Journal of Virology
Volume	90
Issue number	21
DOIs	https://doi.org/10.1128/JVI.01196-16
State	Published - 2016

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Liang, B., Ngwuta, J. O., Herbert, R., Swerczek, J., Dorward, D. W., Amaro-Carambot, E., Mackow, N., Kabatova, B., Lingemann, M., Surman, S., Yang, L., Chen, M., Moin, S. M., Kumar, A., McLellan, J. S., Kwong, P. D., Graham, B. S., Schaap-Nutt, A., Collins, P. L., & Munir, S. (2016). Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector. Journal of Virology, 90(21), 10022-10038. https://doi.org/10.1128/JVI.01196-16

@article{ff7ba09c12e049d39d7bfdfc4a76504c,

title = "Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector",

abstract = "Human respiratory syncytial virus (RSV) and human parainfluenza virus type 3 (HPIV3) are major pediatric respiratory pathogens that lack vaccines. A chimeric bovine/human PIV3 (rB/HPIV3) virus expressing the unmodified, wild-type (wt) RSV fusion (F) protein from an added gene was previously evaluated in seronegative children as a bivalent intranasal RSV/HPIV3 vaccine, and it was well tolerated but insufficiently immunogenic for RSV F. We recently showed that rB/HPIV3 expressing a partially stabilized prefusion form (pre-F) of RSV F efficiently induced {"}high-quality{"} RSV-neutralizing antibodies, defined as antibodies that neutralize RSV in vitro without added complement (B. Liang et al., J Virol 89:9499 -9510, 2015, doi:10.1128/JVI.01373-15). In the present study, we modified RSV F by replacing its cytoplasmic tail (CT) domain or its CT and transmembrane (TM) domains (TMCT) with counterparts from BPIV3 F, with or without pre-F stabilization. This resulted in RSV F being packaged in the rB/HPIV3 particle with an efficiency similar to that of RSV particles. Enhanced packaging was substantially attenuating in hamsters (10- to 100-fold) and rhesus monkeys (100- to 1,000-fold). Nonetheless, TMCT-directed packaging substantially increased the titers of high-quality RSV-neutralizing serum antibodies in hamsters. In rhesus monkeys, a strongly additive immunogenic effect of packaging and pre-F stabilization was observed, as demonstrated by 8- and 30-fold increases of RSV-neutralizing serum antibody titers in the presence and absence of added complement, respectively, compared to pre-F stabilization alone. Analysis of vaccine-induced F-specific antibodies by binding assays indicated that packaging conferred substantial stabilization of RSV F in the pre-F conformation. This provides an improved version of this well-tolerated RSV/HPIV3 vaccine candidate, with potently improved immunogenicity, which can be returned to clinical trials.",

author = "Bo Liang and Ngwuta, \{Joan O.\} and Richard Herbert and Joanna Swerczek and Dorward, \{David W.\} and Emerito Amaro-Carambot and Natalie Mackow and Barbora Kabatova and Matthias Lingemann and Sonja Surman and Lijuan Yang and Man Chen and Moin, \{Syed M.\} and Azad Kumar and McLellan, \{Jason S.\} and Kwong, \{Peter D.\} and Graham, \{Barney S.\} and Anne Schaap-Nutt and Collins, \{Peter L.\} and Shirin Munir",

note = "Publisher Copyright: {\textcopyright} 2016, American Society for Microbiology.",

year = "2016",

doi = "10.1128/JVI.01196-16",

language = "English",

volume = "90",

pages = "10022--10038",

journal = "Journal of Virology",

issn = "0022-538X",

number = "21",

}

Liang, B, Ngwuta, JO, Herbert, R, Swerczek, J, Dorward, DW, Amaro-Carambot, E, Mackow, N, Kabatova, B, Lingemann, M, Surman, S, Yang, L, Chen, M, Moin, SM, Kumar, A, McLellan, JS, Kwong, PD, Graham, BS, Schaap-Nutt, A, Collins, PL & Munir, S 2016, 'Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector', Journal of Virology, vol. 90, no. 21, pp. 10022-10038. https://doi.org/10.1128/JVI.01196-16

Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector. / Liang, Bo; Ngwuta, Joan O.; Herbert, Richard et al.
In: Journal of Virology, Vol. 90, No. 21, 2016, p. 10022-10038.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector

AU - Liang, Bo

AU - Ngwuta, Joan O.

AU - Herbert, Richard

AU - Swerczek, Joanna

AU - Dorward, David W.

AU - Amaro-Carambot, Emerito

AU - Mackow, Natalie

AU - Kabatova, Barbora

AU - Lingemann, Matthias

AU - Surman, Sonja

AU - Yang, Lijuan

AU - Chen, Man

AU - Moin, Syed M.

AU - Kumar, Azad

AU - McLellan, Jason S.

AU - Kwong, Peter D.

AU - Graham, Barney S.

AU - Schaap-Nutt, Anne

AU - Collins, Peter L.

AU - Munir, Shirin

PY - 2016

Y1 - 2016

N2 - Human respiratory syncytial virus (RSV) and human parainfluenza virus type 3 (HPIV3) are major pediatric respiratory pathogens that lack vaccines. A chimeric bovine/human PIV3 (rB/HPIV3) virus expressing the unmodified, wild-type (wt) RSV fusion (F) protein from an added gene was previously evaluated in seronegative children as a bivalent intranasal RSV/HPIV3 vaccine, and it was well tolerated but insufficiently immunogenic for RSV F. We recently showed that rB/HPIV3 expressing a partially stabilized prefusion form (pre-F) of RSV F efficiently induced "high-quality" RSV-neutralizing antibodies, defined as antibodies that neutralize RSV in vitro without added complement (B. Liang et al., J Virol 89:9499 -9510, 2015, doi:10.1128/JVI.01373-15). In the present study, we modified RSV F by replacing its cytoplasmic tail (CT) domain or its CT and transmembrane (TM) domains (TMCT) with counterparts from BPIV3 F, with or without pre-F stabilization. This resulted in RSV F being packaged in the rB/HPIV3 particle with an efficiency similar to that of RSV particles. Enhanced packaging was substantially attenuating in hamsters (10- to 100-fold) and rhesus monkeys (100- to 1,000-fold). Nonetheless, TMCT-directed packaging substantially increased the titers of high-quality RSV-neutralizing serum antibodies in hamsters. In rhesus monkeys, a strongly additive immunogenic effect of packaging and pre-F stabilization was observed, as demonstrated by 8- and 30-fold increases of RSV-neutralizing serum antibody titers in the presence and absence of added complement, respectively, compared to pre-F stabilization alone. Analysis of vaccine-induced F-specific antibodies by binding assays indicated that packaging conferred substantial stabilization of RSV F in the pre-F conformation. This provides an improved version of this well-tolerated RSV/HPIV3 vaccine candidate, with potently improved immunogenicity, which can be returned to clinical trials.

AB - Human respiratory syncytial virus (RSV) and human parainfluenza virus type 3 (HPIV3) are major pediatric respiratory pathogens that lack vaccines. A chimeric bovine/human PIV3 (rB/HPIV3) virus expressing the unmodified, wild-type (wt) RSV fusion (F) protein from an added gene was previously evaluated in seronegative children as a bivalent intranasal RSV/HPIV3 vaccine, and it was well tolerated but insufficiently immunogenic for RSV F. We recently showed that rB/HPIV3 expressing a partially stabilized prefusion form (pre-F) of RSV F efficiently induced "high-quality" RSV-neutralizing antibodies, defined as antibodies that neutralize RSV in vitro without added complement (B. Liang et al., J Virol 89:9499 -9510, 2015, doi:10.1128/JVI.01373-15). In the present study, we modified RSV F by replacing its cytoplasmic tail (CT) domain or its CT and transmembrane (TM) domains (TMCT) with counterparts from BPIV3 F, with or without pre-F stabilization. This resulted in RSV F being packaged in the rB/HPIV3 particle with an efficiency similar to that of RSV particles. Enhanced packaging was substantially attenuating in hamsters (10- to 100-fold) and rhesus monkeys (100- to 1,000-fold). Nonetheless, TMCT-directed packaging substantially increased the titers of high-quality RSV-neutralizing serum antibodies in hamsters. In rhesus monkeys, a strongly additive immunogenic effect of packaging and pre-F stabilization was observed, as demonstrated by 8- and 30-fold increases of RSV-neutralizing serum antibody titers in the presence and absence of added complement, respectively, compared to pre-F stabilization alone. Analysis of vaccine-induced F-specific antibodies by binding assays indicated that packaging conferred substantial stabilization of RSV F in the pre-F conformation. This provides an improved version of this well-tolerated RSV/HPIV3 vaccine candidate, with potently improved immunogenicity, which can be returned to clinical trials.

UR - https://www.scopus.com/pages/publications/84994048510

U2 - 10.1128/JVI.01196-16

DO - 10.1128/JVI.01196-16

M3 - Article

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AN - SCOPUS:84994048510

SN - 0022-538X

VL - 90

SP - 10022

EP - 10038

JO - Journal of Virology

JF - Journal of Virology

IS - 21

ER -

Liang B, Ngwuta JO, Herbert R, Swerczek J, Dorward DW, Amaro-Carambot E et al. Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector. Journal of Virology. 2016;90(21):10022-10038. doi: 10.1128/JVI.01196-16

Packaging and prefusion stabilization separately and additively increase the quantity and quality of respiratory syncytial virus (RSV)-neutralizing antibodies induced by an RSV fusion protein expressed by a parainfluenza virus vector

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