Norovirus Vaccine against Experimental Human Norwalk Virus Illness

Atmar, Robert L.; Bernstein, David I.; Harro, Clayton; Al-Ibrahim, Mohamed S.; Chen, Wilbur H.; Ferreira, Jennifer; Estes, Mary K.; Graham, David Y.; Opekun, Antone R.; Richardson, Charles C.; Mendelman, Paul M.

doi:10.1056/nejmoa1101245

Cited by 433 publications

(428 citation statements)

References 37 publications

(42 reference statements)

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“…7 The VP1 protein can self-assemble into viruslike particles (VLPs) that are structurally similar to native virions. Clinical trials testing the efficacy of HuNoV VLPs as vaccine candidates administered intranasally or intramuscularly have demonstrated modest short-term (up to 1 month) protection from developing severe disease, 8,9 results that are encouraging but do not address the critical questions of immunity duration or cross-reactive protective immunity. Development of potentially more effective live attenuated viral vaccines has long been hindered by an inability to culture HuNoVs.…”

Section: Introductionmentioning

confidence: 99%

Identification of a novel cellular target and a co-factor for norovirus infection – B cells & commensal bacteria

Karst

2015

Gut Microbes

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Section: Introductionmentioning

confidence: 99%

Identification of a novel cellular target and a co-factor for norovirus infection – B cells & commensal bacteria

Karst

2015

Gut Microbes

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“…125 Two doses of vaccine or placebo were administered intranasally to healthy 18-50 y adults followed by homologous inoculation with HuNoV. The participants enrolled in this study were likely to develop NoV -associated gastroenteritis due to the expression of O or A blood groups and a functional FUT2 gene.…”

Section: Human Trialsmentioning

confidence: 99%

“…This study confirmed HuNoV infection however at a lower rate than those previously reported in other human challenge studies. 125,127 The most recent published data are the results of the phase I clinical trial using VLPs containing GI.1 and GII.4 administered intramuscularly to 18-49 y healthy adults. 130 The results show the ability of this bivalent vaccine to induce serum antibody responses to GI.1 and GII.4 antigens albeit higher in the former.…”

Section: Human Trialsmentioning

confidence: 99%

“…Both oral and intranasal modes of immunization elicited ab responses post vaccination (Table 2). 80,104,[123][124][125] Moreover, the intramuscular administration of candidate vaccines containing GI and GII strains stimulated strong immune responses against the vaccine genotype. 129,130 Human challenge studies 77,96 as well as vaccine studies (Table 2) tested the ability of different vaccine formulas to generate cross-reactive immune responses to account for the diversity of the circulating HuNoV strains.…”

Section: Human Trialsmentioning

confidence: 99%

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Norovirus vaccines: Correlates of protection, challenges and limitations

Melhem

2016

Human Vaccines & Immunotherapeutics

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Norovirus (NoV) is responsible for at least 50% of all gastroenteritis outbreaks worldwide. NoVs are classified into 6 different genogroups (GGI-GGVI) based on the viral capsid protein with NoV genogroup II genotype 4 (GII.4) being the predominant strain causing human diseases. Supportive therapy involving reversal of dehydration and electrolyte deficiency is the main treatment of NoV gastroenteritis. However, the worldwide increased recognition of NoV as an important agent of diarrheal gastroenteritis prompted researchers to focus on establishing preventive strategies conferring long-lasting immunity. This review describes the current status of animal and human vaccine models/studies targeting NoV and addresses the factors hampering the development of a broadly effective vaccine.

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“…A monovalent GI.1VLP vaccine administered via the intranasal (IN) route was shown to provide good protection in a clinical trial. 7 To overcome the epidemiological differences of GI.1 and GII.4 genotypes, a bivalent VLP vaccine carrying GI.1 and GII.4 genotypes was proposed for IN administration and shown to be immunogenic without the use of adjuvant in a guinea pig model. 8 However, intramuscular administration of monovalent GI.1VLPs has been shown to achieve better antigen delivery and antibody responses in adults at a lower dosage than IN immunization.…”

Section: Introductionmentioning

confidence: 99%

More robust gut immune responses induced by combining intranasal and sublingual routes for prime-boost immunization

Hwang

Puth

Tan

et al. 2018

Human Vaccines & Immunotherapeutics

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Norovirus causes acute and debilitating gastroenteritis, characterized by vomiting and diarrhea. We recently reported a recombinant GII. 4 P domain particle (Pd) vaccine adjuvanted with a flagellin, Vibrio vulnificus FlaB, effectively promoting both humoral and cell-mediated immune responses. In the previous study, we found that sublingual (SL) immunization induced higher fecal secretory IgA (SIgA) responses while intranasal (IN) route provided higher amplitude of humoral and cellular immune responses in the systemic compartment. We hypothesized that the combination of IN and SL routes should induce more potent and sustained SIgA responses in the gut. In this study, we have tried combinatorial prime-boost immunization employing both IN and SL routes. The IN priming and SL boosting with the Pd+FlaB vaccine enhanced highest SIgA responses in feces, accompanying increased Pd-specific memory B cells and plasma cells in spleen and bone marrow, respectively. Notably, the strongest long-lasting SIgA response in feces was induced by combined IN prime and SL boost vaccination, which was sustained for more than 3 months. Significantly enhanced gut-homing B cell and follicular helper T cell responses in mesenteric lymph nodes (mLNs) were observed in the IN prime and SL boost combination. IN priming was a requisite for the robust induction of Pd-specific IFNγ, IL-2, IL-4 and IL-5 cytokine responses in the systemic immune compartment. Collectively, the IN prime and SL boost combination was the best option for inducing balanced long-lasting immune responses against the norovirus antigen in both enteric and systemic compartments. These results suggest that immune responses in specific mucosal compartments may be programmed by employing different prime-boost immunization routes.

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Norovirus Vaccine against Experimental Human Norwalk Virus Illness

Cited by 433 publications

References 37 publications

Identification of a novel cellular target and a co-factor for norovirus infection – B cells & commensal bacteria

Identification of a novel cellular target and a co-factor for norovirus infection – B cells & commensal bacteria

Norovirus vaccines: Correlates of protection, challenges and limitations

More robust gut immune responses induced by combining intranasal and sublingual routes for prime-boost immunization

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