Adjuvanting a subunit SARS-CoV-2 nanoparticle vaccine to induce protective immunity in non-human primates
By
Prabhu S Arunachalam,
Alexandra C. Walls,
Nadia Golden,
Caroline Atyeo,
Stephanie Fischinger,
Chunfeng Li,
Pyone Aye,
Mary Jane Navarro,
Lilin Lai,
Venkata Viswanadh Edara,
Katharina Roltgen,
Kenneth Rogers,
Lisa Shirreff,
Douglas E Ferrell,
Samuel Wrenn,
Deleah Pettie,
John C Kraft,
Marcos C. Miranda,
Elizabeth Kepl,
Claire Sydeman,
Natalie Brunette,
Michael Murphy,
Brooke Fiala,
Lauren Carter,
Alexander G. White,
Meera Trisal,
Ching-Lin Hsieh,
Kasi Russell-Lodrigue,
Christopher Monjure,
Jason Dufour,
Lara Doyle-Meyer,
Rudolph B Bohm,
Nicholas J Maness,
Chad Roy,
Jessica A. Plante,
Kenneth S. Plante,
Alex Zhu,
Matthew J Gorman,
Sally Shin,
Xiaoying Shen,
Jane Fontenot,
Shakti Gupta,
Derek T O Hagan,
Robbert Van Der Most,
Rino Rappuoli,
Robert L Coffman,
David Novack,
Jason S McLellan,
Shankar Subramaniam,
David Montefiori,
Scott D. Boyd,
JoAnne L Flynn,
Galit Alter,
Francois Villinger,
Harry Kleanthous,
Jay Rappaport,
Mehul Suthar,
Neil P. King,
David Veesler,
Bali Pulendran
Posted 11 Feb 2021
bioRxiv DOI: 10.1101/2021.02.10.430696
The development of a portfolio of SARS-CoV-2 vaccines to vaccinate the global population remains an urgent public health imperative. Here, we demonstrate the capacity of a subunit vaccine under clinical development, comprising the SARS-CoV-2 Spike protein receptor-binding domain displayed on a two-component protein nanoparticle (RBD-NP), to stimulate robust and durable neutralizing antibody (nAb) responses and protection against SARS-CoV-2 in non-human primates. We evaluated five different adjuvants combined with RBD-NP including Essai O/W 1849101, a squalene-in-water emulsion; AS03, an alpha-tocopherol-containing squalene-based oil-in-water emulsion used in pandemic influenza vaccines; AS37, a TLR-7 agonist adsorbed to Alum; CpG 1018-Alum (CpG-Alum), a TLR-9 agonist formulated in Alum; or Alum, the most widely used adjuvant. All five adjuvants induced substantial nAb and CD4 T cell responses after two consecutive immunizations. Durable nAb responses were evaluated for RBD-NP/AS03 immunization and the live-virus nAb response was durably maintained up to 154 days post-vaccination. AS03, CpG-Alum, AS37 and Alum groups conferred significant protection against SARS-CoV-2 infection in the pharynges, nares and in the bronchoalveolar lavage. The nAb titers were highly correlated with protection against infection. Furthermore, RBD-NP when used in conjunction with AS03 was as potent as the prefusion stabilized Spike immunogen, HexaPro. Taken together, these data highlight the efficacy of the RBD-NP formulated with clinically relevant adjuvants in promoting robust immunity against SARS-CoV-2 in non-human primates.
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