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3 research outputs found

High Potency of a Bivalent Human VH Domain in SARS-CoV-2 Animal Models

Author: Baric Ralph S.
Berezuk Alison
Chen Chuan
Chittori Sagar
Dimitrov Dimiter S.
Drelich Aleksandra
Falzarano Darryl
Kulkarni Swarali S.
Leist Sarah R.
Leopold Karoline
Li Wei
Liu Xianglei
Martinez David R.
Schäfer Alexandra
Subramaniam Sriram
Sun Zehua
Ura Marcin L.
Zhang Liyong
Publication venue
Publication date: 01/01/2020
Field of study

Novel COVID-19 therapeutics are urgently needed. We generated a phage-displayed human antibody VH domain library from which we identified a high-affinity VH binder ab8. Bivalent VH, VH-Fc ab8, bound with high avidity to membrane-associated S glycoprotein and to mutants found in patients. It potently neutralized mouse-adapted SARS-CoV-2 in wild-type mice at a dose as low as 2 mg/kg and exhibited high prophylactic and therapeutic efficacy in a hamster model of SARS-CoV-2 infection, possibly enhanced by its relatively small size. Electron microscopy combined with scanning mutagenesis identified ab8 interactions with all three S protomers and showed how ab8 neutralized the virus by directly interfering with ACE2 binding. VHFc ab8 did not aggregate and did not bind to 5,300 human membrane-associated proteins. The potent neutralization activity of VH-Fc ab8 combined with good developability properties and cross-reactivity to SARS-CoV-2 mutants provide a strong rationale for its evaluation as a COVID-19 therapeutic

Carolina Digital Repository

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High Potency of a Bivalent Human V H Domain in SARS-CoV-2 Animal Models

Author: Baric Ralph S
Berezuk Alison
Chen Chuan
Chittori Sagar
Dimitrov Dimiter S
Drelich Aleksandra
Falzarano Darryl
Kulkarni Swarali S
Leist Sarah R
Leopold Karoline
Li Wei
Liu Xianglei
Mannar Dhiraj
Martinez David R
Mellors John W
Peterson Eric C
Schäfer Alexandra
Srivastava Shanti S
Subramaniam Sriram
Sun Zehua
Tseng Chien-Te
Ura Marcin L
Zhang Liyong
Zhu Xing
Publication venue
Publication date: 15/10/2020
Field of study

Novel COVID-19 therapeutics are urgently needed. We generated a phage-displayed human antibody V domain library from which we identified a high-affinity V binder ab8. Bivalent V , V -Fc ab8, bound with high avidity to membrane-associated S glycoprotein and to mutants found in patients. It potently neutralized mouse-adapted SARS-CoV-2 in wild-type mice at a dose as low as 2 mg/kg and exhibited high prophylactic and therapeutic efficacy in a hamster model of SARS-CoV-2 infection, possibly enhanced by its relatively small size. Electron microscopy combined with scanning mutagenesis identified ab8 interactions with all three S protomers and showed how ab8 neutralized the virus by directly interfering with ACE2 binding. V -Fc ab8 did not aggregate and did not bind to 5,300 human membrane-associated proteins. The potent neutralization activity of V -Fc ab8 combined with good developability properties and cross-reactivity to SARS-CoV-2 mutants provide a strong rationale for its evaluation as a COVID-19 therapeutic

University of Miami: Scholarship Miami

High Potency of a Bivalent Human VH Domain in SARS-CoV-2 Animal Models

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