Efficacy and breadth of adjuvanted SARS-CoV-2 receptor-binding domain nanoparticle vaccine in macaques (preprint)

Hannah A. D. King; M. Gordon Joyce; Ines Elakhal Naouar; Aslaa Ahmed; Camila Macedo Cincotta; Caroline Subra; Kristina K. Peachman; Holly H. Hack; Rita E. Chen; Paul V. Thomas; Wei-Hung Chen; Rajeshwer S. Sankhala; Agnes Hajduczki; Elizabeth J. Martinez; Caroline E. Peterson; William C. Chang; Misook Choe; Clayton Smith; Jarrett A. Headley; Hanne A. Elyard; Anthony Cook; Alexander Anderson; Kathryn M. Wuertz; Ming Dong; Isabella Swafford; James B. Case; Jeffrey R. Currier; Kerri G. Lal; Mihret F. Amare; Vincent Dussupt; Sebastian Molnar; Sharon P. Daye; Xiankun Zeng; Erica K. Barkei; Kendra Alfson; Hilary M. Staples; Ricardo Carrion; Shelly J. Krebs; Dominic Paquin-Proulx; Nicos Karasavvas; Victoria R. Polonis; Linda L. Jagodzinski; Sandhya Vasan; Paul T. Scott; Yaoxing Huang; Manoj S. Nair; David D. Ho; Natalia de Val; Michael S. Diamond; Mark G. Lewis; Mangala Rao; Gary R. Matyas; Gregory D. Gromowski; Sheila A. Peel; Nelson L. Michael; Kayvon Modjarrad; Diane L. Bolton

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Efficacy and breadth of adjuvanted SARS-CoV-2 receptor-binding domain nanoparticle vaccine in macaques (preprint)

Hannah A. D. King; M. Gordon Joyce; Ines Elakhal Naouar; Aslaa Ahmed; Camila Macedo Cincotta; Caroline Subra; Kristina K. Peachman; Holly H. Hack; Rita E. Chen; Paul V. Thomas; Wei-Hung Chen; Rajeshwer S. Sankhala; Agnes Hajduczki; Elizabeth J. Martinez; Caroline E. Peterson; William C. Chang; Misook Choe; Clayton Smith; Jarrett A. Headley; Hanne A. Elyard; Anthony Cook; Alexander Anderson; Kathryn M. Wuertz; Ming Dong; Isabella Swafford; James B. Case; Jeffrey R. Currier; Kerri G. Lal; Mihret F. Amare; Vincent Dussupt; Sebastian Molnar; Sharon P. Daye; Xiankun Zeng; Erica K. Barkei; Kendra Alfson; Hilary M. Staples; Ricardo Carrion; Shelly J. Krebs; Dominic Paquin-Proulx; Nicos Karasavvas; Victoria R. Polonis; Linda L. Jagodzinski; Sandhya Vasan; Paul T. Scott; Yaoxing Huang; Manoj S. Nair; David D. Ho; Natalia de Val; Michael S. Diamond; Mark G. Lewis; Mangala Rao; Gary R. Matyas; Gregory D. Gromowski; Sheila A. Peel; Nelson L. Michael; Kayvon Modjarrad; Diane L. Bolton.

biorxiv; 2021.

Preprint in English | bioRxiv | ID: ppzbmed-10.1101.2021.04.09.439166

ABSTRACT

ABSTRACT

Emergence of novel variants of the severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) underscores the need for next-generation vaccines able to elicit broad and durable immunity. Here we report the evaluation of a ferritin nanoparticle vaccine displaying the receptor-binding domain of the SARS-CoV-2 spike protein (RFN) adjuvanted with Army Liposomal Formulation QS-21 (ALFQ). RFN vaccination of macaques using a two-dose regimen resulted in robust, predominantly Th1 CD4+ T cell responses and reciprocal peak mean neutralizing antibody titers of 14,000-21,000. Rapid control of viral replication was achieved in the upper and lower airways of animals after high-dose SARS-CoV-2 respiratory challenge, with undetectable replication within four days in 7 of 8 animals receiving 50 {micro}g RFN. Cross-neutralization activity against SARS-CoV-2 variant B.1.351 decreased only [~]2-fold relative to USA-WA1. In addition, neutralizing, effector antibody and cellular responses targeted the heterotypic SARS-CoV-1, highlighting the broad immunogenicity of RFN-ALFQ for SARS-like betacoronavirus vaccine development. Significance StatementThe emergence of SARS-CoV-2 variants of concern (VOC) that reduce the efficacy of current COVID-19 vaccines is a major threat to pandemic control. We evaluate a SARS-CoV-2 Spike receptor-binding domain ferritin nanoparticle protein vaccine (RFN) in a nonhuman primate challenge model that addresses the need for a next-generation, efficacious vaccine with increased pan-SARS breadth of coverage. RFN, adjuvanted with a liposomal-QS21 formulation (ALFQ), elicits humoral and cellular immune responses exceeding those of current vaccines in terms of breadth and potency and protects against high-dose respiratory tract challenge. Neutralization activity against the B.1.351 VOC within two-fold of wild-type virus and against SARS-CoV-1 indicate exceptional breadth. Our results support consideration of RFN for SARS-like betacoronavirus vaccine development.

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COVID-19

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Full text: Available Collection: Preprints Database: bioRxiv Main subject: COVID-19 Language: English Year: 2021 Document Type: Preprint