Safety and immunogenicity studies in animal models support clinical development of a bivalent norovirus-like particle vaccine produced in plants

Daniel Tusé; Maria Malm; Kirsi Tamminen; André Diessner; Frank Thieme; Franziska Jarczowski; Vesna Blazevic; Victor Klimyuk

doi:10.1016/j.vaccine.2022.01.009

Safety and immunogenicity studies in animal models support clinical development of a bivalent norovirus-like particle vaccine produced in plants

Vaccine. 2022 Feb 11;40(7):977-987. doi: 10.1016/j.vaccine.2022.01.009. Epub 2022 Jan 19.

Authors

Daniel Tusé¹, Maria Malm², Kirsi Tamminen², André Diessner³, Frank Thieme³, Franziska Jarczowski³, Vesna Blazevic², Victor Klimyuk⁴

Affiliations

¹ DT/Consulting Group, 2695 13(th) Street, Sacramento, CA 95818, USA.
² Vaccine Research Center, University of Tampere, Arvo Ylpön katu 34, 33520 Tampere, Finland.
³ Icon Genetics GmbH, a Denka Company, Weinbergweg 22, D-06120 Halle, Germany.
⁴ Icon Genetics GmbH, a Denka Company, Weinbergweg 22, D-06120 Halle, Germany. Electronic address: klimyuk@icongenetics.de.

PMID: 35063285
DOI: 10.1016/j.vaccine.2022.01.009

Abstract

Noroviruses (NoV) are the leading cause of epidemic acute gastroenteritis in humans worldwide. A safe and effective vaccine that prevents NoV infection or minimizes NoV disease burden is needed, especially for children and the elderly who are particularly susceptible to NoV disease. A plant-based expression system (magnICON®) was used to manufacture two different virus-like particle (VLP) immunogens derived from human NoV genogroups I and II, genotype 4 (GI.4 and GII.4), which were subsequently blended 1:1 (w/w) into a bivalent vaccine composition (rNV-2v). Here, we report on the safety and immunogenicity of rNV-2v from one pilot and two GLP-compliant toxicity studies in New Zealand White rabbits administered the vaccine subcutaneously (SC) or intramuscularly (IM). Strong genogroup-specific immune responses were induced by vaccination without adjuvant at various doses (200 to 400 μg VLP/administration) and administration schedules (Days 1 and 7; or Days 1, 15 and 29). The results showed sporadic local irritation at the injection site, which resolved over time, and was non-adverse and consistent with expected reactogenicity. There were no signs of systemic toxicity related to vaccine administration relative to vehicle-treated controls with respect to clinical chemistry, haematology, organ weights, macroscopic examinations, or histopathology. In a 3-administration regimen (n + 1 the clinical regimen), the NOAEL for rNV-2v via the SC or IM route was initially determined to be 200 μg. An improved GI.4 VLP variant mixed 1:1 (w/w) with the wild-type GII.4 VLP was subsequently evaluated via the IM route at a higher dose in the same 3-administration model, and the NOAEL was raised to 300 µg. Serology performed in samples of both toxicity studies showed significant and substantial anti-VLP-specific antibody titers for rNV-2v vaccines administered via the IM or SC route, as well as relevant NoV blocking antibody responses. These results support initiation of clinical development of the plant-made NoV vaccine.

Keywords: Immunogenicity; Norovirus; Plant; Safety; Virus-like particle (VLP).

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Antibodies, Viral
Caliciviridae Infections*
Models, Animal
Norovirus*
Rabbits
Vaccines, Virus-Like Particle*
Viral Vaccines*

Substances

Antibodies, Viral
Vaccines, Virus-Like Particle
Viral Vaccines