Design and evaluation of bi- and trispecific antibodies targeting multiple filovirus glycoproteins

Elisabeth K. Nyakatura; Samantha E. Zak; Anna Z. Wec; Daniel Hofmann; Sergey Shulenin; R. R. Bakken; M. Javad Aman; Kartik Chandran; John M. Dye; Jonathan R. Lai

doi:10.1074/jbc.RA117.001627

Design and evaluation of bi- and trispecific antibodies targeting multiple filovirus glycoproteins

Elisabeth K. Nyakatura, Samantha E. Zak, Anna Z. Wec, Daniel Hofmann, Sergey Shulenin, R. R. Bakken, M. Javad Aman, Kartik Chandran, John M. Dye, Jonathan R. Lai

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

7 Scopus citations

Abstract

Filoviruses (family Filoviridae) include five ebolaviruses and Marburg virus. These pathogens cause a rapidly progressing and severe viral disease with high mortality rates (generally 30 -90%). Outbreaks of filovirus disease are sporadic and, until recently, were limited to less than 500 cases. However, the 2013-2016 epidemic in western Africa, caused by Ebola virus (EBOV), illustrated the potential of filovirus outbreaks to escalate to a much larger scale (over 28,000 suspected cases). mAbs against the envelope glycoprotein represent a promising therapeutic platform for managing filovirus infections. However, mAbs that exhibit neutralization or protective properties against multiple filoviruses are rare. Here we examined a panel of engineered bi- and trispecific antibodies, in which variable domains of mAbs that target epitopes from multiple filoviruses were combined, for their capacity to neutralize viral infection across filovirus species. We found that bispecific combinations targeting EBOV and Sudan virus (another ebolavirus), provide potent cross-neutralization and protection in mice. Furthermore, trispecific combinations, targeting EBOV, Sudan virus, and Marburg virus, exhibited strong neutralization potential against all three viruses. These results provide important insights into multispecific antibody engineering against filoviruses and will inform future immunotherapeutic discoveries.

Original language	English (US)
Pages (from-to)	6201-6211
Number of pages	11
Journal	Journal of Biological Chemistry
Volume	293
Issue number	16
DOIs	https://doi.org/10.1074/jbc.RA117.001627
State	Published - Apr 20 2018

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Cell Biology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1074/jbc.RA117.001627

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@article{51dcab50dabf49e4a6d6d3173f0ffc9b,

title = "Design and evaluation of bi- and trispecific antibodies targeting multiple filovirus glycoproteins",

abstract = "Filoviruses (family Filoviridae) include five ebolaviruses and Marburg virus. These pathogens cause a rapidly progressing and severe viral disease with high mortality rates (generally 30 -90%). Outbreaks of filovirus disease are sporadic and, until recently, were limited to less than 500 cases. However, the 2013-2016 epidemic in western Africa, caused by Ebola virus (EBOV), illustrated the potential of filovirus outbreaks to escalate to a much larger scale (over 28,000 suspected cases). mAbs against the envelope glycoprotein represent a promising therapeutic platform for managing filovirus infections. However, mAbs that exhibit neutralization or protective properties against multiple filoviruses are rare. Here we examined a panel of engineered bi- and trispecific antibodies, in which variable domains of mAbs that target epitopes from multiple filoviruses were combined, for their capacity to neutralize viral infection across filovirus species. We found that bispecific combinations targeting EBOV and Sudan virus (another ebolavirus), provide potent cross-neutralization and protection in mice. Furthermore, trispecific combinations, targeting EBOV, Sudan virus, and Marburg virus, exhibited strong neutralization potential against all three viruses. These results provide important insights into multispecific antibody engineering against filoviruses and will inform future immunotherapeutic discoveries.",

author = "Nyakatura, {Elisabeth K.} and Zak, {Samantha E.} and Wec, {Anna Z.} and Daniel Hofmann and Sergey Shulenin and Bakken, {R. R.} and {Javad Aman}, M. and Kartik Chandran and Dye, {John M.} and Lai, {Jonathan R.}",

note = "Funding Information: This work was supported by NIAID, National Institutes of Health Centers of Excellence for Translational Research Grant U19 AI109762 and National Institutes of Health Grants R01-AI125462 (to J. R. L.) and R41-AI122403 (to J. R. L. and M. J. A.). The authors declare that they have no conflicts of inter-est with the contents of this article. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. Opinions, conclusions, interpretations, and recommendations are those of the authors and are not necessarily endorsed by the United States Army. The mention of trade names or com-mercial products does not constitute endorsement or recommendation for use by the Department of the Army or the Department of Defense. Funding Information: Research was conducted under an IACUC-approved protocol in compliance with the Animal Welfare Act, Public Health Service Policy, and other federal statutes and regulations relating to animals and experiments involving animals. The facility where this research was conducted is accredited by the Association for Assessment and Accreditation of Laboratory Animal Care, International and adheres to principles stated in the Guide for the Care and Use of Laboratory Animals, National Research Council, 2011. Funding Information: 1Supported in part by a postdoctoral fellowship from the Deutscher Akade-mischer Austauschdienst (German Academic Exchange Service). Publisher Copyright: {\textcopyright} 2018 American Society for Biochemistry and Molecular Biology Inc. All Rights Reserved.",

year = "2018",

month = apr,

day = "20",

doi = "10.1074/jbc.RA117.001627",

language = "English (US)",

volume = "293",

pages = "6201--6211",

journal = "Journal of Biological Chemistry",

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T1 - Design and evaluation of bi- and trispecific antibodies targeting multiple filovirus glycoproteins

AU - Nyakatura, Elisabeth K.

AU - Zak, Samantha E.

AU - Wec, Anna Z.

AU - Hofmann, Daniel

AU - Shulenin, Sergey

AU - Bakken, R. R.

AU - Javad Aman, M.

AU - Chandran, Kartik

AU - Dye, John M.

AU - Lai, Jonathan R.

N1 - Funding Information: This work was supported by NIAID, National Institutes of Health Centers of Excellence for Translational Research Grant U19 AI109762 and National Institutes of Health Grants R01-AI125462 (to J. R. L.) and R41-AI122403 (to J. R. L. and M. J. A.). The authors declare that they have no conflicts of inter-est with the contents of this article. The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. Opinions, conclusions, interpretations, and recommendations are those of the authors and are not necessarily endorsed by the United States Army. The mention of trade names or com-mercial products does not constitute endorsement or recommendation for use by the Department of the Army or the Department of Defense. Funding Information: Research was conducted under an IACUC-approved protocol in compliance with the Animal Welfare Act, Public Health Service Policy, and other federal statutes and regulations relating to animals and experiments involving animals. The facility where this research was conducted is accredited by the Association for Assessment and Accreditation of Laboratory Animal Care, International and adheres to principles stated in the Guide for the Care and Use of Laboratory Animals, National Research Council, 2011. Funding Information: 1Supported in part by a postdoctoral fellowship from the Deutscher Akade-mischer Austauschdienst (German Academic Exchange Service). Publisher Copyright: © 2018 American Society for Biochemistry and Molecular Biology Inc. All Rights Reserved.

PY - 2018/4/20

Y1 - 2018/4/20

N2 - Filoviruses (family Filoviridae) include five ebolaviruses and Marburg virus. These pathogens cause a rapidly progressing and severe viral disease with high mortality rates (generally 30 -90%). Outbreaks of filovirus disease are sporadic and, until recently, were limited to less than 500 cases. However, the 2013-2016 epidemic in western Africa, caused by Ebola virus (EBOV), illustrated the potential of filovirus outbreaks to escalate to a much larger scale (over 28,000 suspected cases). mAbs against the envelope glycoprotein represent a promising therapeutic platform for managing filovirus infections. However, mAbs that exhibit neutralization or protective properties against multiple filoviruses are rare. Here we examined a panel of engineered bi- and trispecific antibodies, in which variable domains of mAbs that target epitopes from multiple filoviruses were combined, for their capacity to neutralize viral infection across filovirus species. We found that bispecific combinations targeting EBOV and Sudan virus (another ebolavirus), provide potent cross-neutralization and protection in mice. Furthermore, trispecific combinations, targeting EBOV, Sudan virus, and Marburg virus, exhibited strong neutralization potential against all three viruses. These results provide important insights into multispecific antibody engineering against filoviruses and will inform future immunotherapeutic discoveries.

AB - Filoviruses (family Filoviridae) include five ebolaviruses and Marburg virus. These pathogens cause a rapidly progressing and severe viral disease with high mortality rates (generally 30 -90%). Outbreaks of filovirus disease are sporadic and, until recently, were limited to less than 500 cases. However, the 2013-2016 epidemic in western Africa, caused by Ebola virus (EBOV), illustrated the potential of filovirus outbreaks to escalate to a much larger scale (over 28,000 suspected cases). mAbs against the envelope glycoprotein represent a promising therapeutic platform for managing filovirus infections. However, mAbs that exhibit neutralization or protective properties against multiple filoviruses are rare. Here we examined a panel of engineered bi- and trispecific antibodies, in which variable domains of mAbs that target epitopes from multiple filoviruses were combined, for their capacity to neutralize viral infection across filovirus species. We found that bispecific combinations targeting EBOV and Sudan virus (another ebolavirus), provide potent cross-neutralization and protection in mice. Furthermore, trispecific combinations, targeting EBOV, Sudan virus, and Marburg virus, exhibited strong neutralization potential against all three viruses. These results provide important insights into multispecific antibody engineering against filoviruses and will inform future immunotherapeutic discoveries.

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Design and evaluation of bi- and trispecific antibodies targeting multiple filovirus glycoproteins

Abstract

ASJC Scopus subject areas

UN SDGs

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