BpOmpW Antigen Stimulates the Necessary Protective T-Cell Responses Against Melioidosis

Tomás-Cortázar, Julen; Bossi, Lorenzo; Quinn, Conor; Reynolds, Catherine J.; Murchú, Maitiú Ó; McMahon, Eve; Singh, Mahavir; Rongkard, Patpong; Anguíta, Juan; Blanco, Alfonso; Boyton, Rosemary J.; Arnold, Johan; Giltaire, Séverine; Dunachie, Susanna; Altmann, Daniel M.

doi:10.3389/fimmu.2021.767359

Cited by 7 publications

(9 citation statements)

References 42 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…A variety of defined proteins and polysaccharides, alone or as conjugates, that elicit varying degrees of protection have been previously assessed as potential vaccine components. These are exemplified by T3SS proteins (such as Bip), T6SS proteins (such as Hcp1), proteases, outer membrane proteins (OMPs, LolC), CPS, and LPS or purified OPS (Harland et al, 2007 ; Chin et al, 2012 ; Scott et al, 2014a , b , 2016 ; Gregory et al, 2015 ; Casey et al, 2016 ; Burtnick et al, 2018 ; Tomas-Cortazar et al, 2021 ). Hcp1 is required for assembly of the secretion apparatus and for the export of the T6SS virulence proteins (Mougous et al, 2006 ; Pukatzki et al, 2007 ; Brunet et al, 2014 ; Lim et al, 2015 ).…”

Section: Discussionmentioning

confidence: 99%

Evaluation of two different vaccine platforms for immunization against melioidosis and glanders

et al. 2022

View full text Add to dashboard Cite

Burkholderia pseudomallei and the closely related species, Burkholderia mallei, produce similar multifaceted diseases which range from rapidly fatal to protracted and chronic, and are a major cause of mortality in endemic regions. Besides causing natural infections, both microbes are Tier 1 potential biothreat agents. Antibiotic treatment is prolonged with variable results, hence effective vaccines are urgently needed. The purpose of our studies was to compare candidate vaccines that target both melioidosis and glanders to identify the most efficacious one(s) and define residual requirements for their transition to the non-human primate aerosol model. Studies were conducted in the C57BL/6 mouse model to evaluate the humoral and cell-mediated immune response and protective efficacy of three Burkholderia vaccine candidates against lethal aerosol challenges with B. pseudomallei K96243, B. pseudomallei MSHR5855, and B. mallei FMH. The recombinant vaccines generated significant immune responses to the vaccine antigens, and the live attenuated vaccine generated a greater immune response to OPS and the whole bacterial cells. Regardless of the candidate vaccine evaluated, the protection of mice was associated with a dampened cytokine response within the lungs after exposure to aerosolized bacteria. Despite being delivered by two different platforms and generating distinct immune responses, two experimental vaccines, a capsule conjugate + Hcp1 subunit vaccine and the live B. pseudomallei 668 ΔilvI strain, provided significant protection and were down-selected for further investigation and advanced development.

show abstract

Section: Discussionmentioning

confidence: 99%

Evaluation of two different vaccine platforms for immunization against melioidosis and glanders

et al. 2022

View full text Add to dashboard Cite

show abstract

“…We have previously developed a proteomic cell blot approach to identify bacterial proteins involved in epithelial cell attachment with a high potential to be effective vaccine antigens [ 34 ]. Using this approach, we have already identified an effective melioidosis vaccine candidate that protected mice for up to 81 days against Burkholderia pseudomallei, and that will be progressing to human studies in the near future [ 35 , 36 ]. Our aim was to extend this platform to identify novel protein adhesins specific to VTEC strains that may be effective vaccine antigens, either on their own or in combination with other antigens, to prevent human colonisation.…”

Section: Introductionmentioning

confidence: 99%

GlnH, a Novel Antigen That Offers Partial Protection against Verocytotoxigenic Escherichia coli Infection

et al. 2023

Self Cite

View full text Add to dashboard Cite

Verotoxin-producing Escherichia coli (VTEC) causes zoonotic infections, with potentially devastating complications, and children under 5 years old are particularly susceptible. Antibiotic treatment is contraindicated, and due to the high proportion of infected children that suffer from severe and life-changing complications, there is an unmet need for a vaccine to prevent VTEC infections. Bacterial adhesins represent promising candidates for the successful development of a vaccine against VTEC. Using a proteomic approach to identify bacterial proteins interacting with human gastrointestinal epithelial Caco-2 and HT-29 cells, we identified eleven proteins by mass spectrometry. These included a glutamine-binding periplasmic protein, GlnH, a member of the ABC transporter family. The glnH gene was identified in 13 of the 15 bovine and all 5 human patient samples tested, suggesting that it is prevalent. We confirmed that GlnH is involved in the host cell attachment of an O157:H7 prototype E. coli strain to gastrointestinal cells in vitro. Recombinant GlnH was expressed and purified prior to the immunisation of mice. When alum was used as an adjuvant, GlnH was highly immunogenic, stimulating strong serological responses in immunised mice, and it resulted in a modest reduction in faecal shedding but did not reduce colonisation. GlnH immunisation with a T-cell-inducing adjuvant (SAS) also showed comparable antibody responses and an IgG1/IgG2a ratio suggestive of a mixed Th1/Th2 response but was partially protective, with a 1.5-log reduction in colonisation of the colon and caecum at 7 days relative to the adjuvant only (p = 0.0280). It is clear that future VTEC vaccine developments should consider the contribution of adjuvants in addition to antigens. Moreover, it is likely that a combined cellular and humoral response may prove more beneficial in providing protective interventions against VTEC.

show abstract

“…model in C57BL/6 mice demonstrated more promising results, with OmpW1 + SAS affording 75% protection on day 80 compared to 12.5% in the adjuvant alone group [ 174 ]. Splenocytes from vaccinated animals secreted significant levels of IFN-γ upon ex vivo stimulation with OmpW1, suggesting a strong Th1 response was mounted [ 175 ]. A notable downside of these experiments is that the study reported significant issues with protein solubility that could only be overcome by solubilizing the protein in urea.…”

Section: General Outer Membrane Proteins: β-Barrelsmentioning

confidence: 99%

Burkholderia pseudomallei Complex Subunit and Glycoconjugate Vaccines and Their Potential to Elicit Cross-Protection to Burkholderia cepacia Complex

Badten,

Torres

2024

Vaccines

View full text Add to dashboard Cite

Burkholderia are a group of Gram-negative bacteria that can cause a variety of diseases in at-risk populations. B. pseudomallei and B. mallei, the etiological agents of melioidosis and glanders, respectively, are the two clinically relevant members of the B. pseudomallei complex (Bpc). The development of vaccines against Bpc species has been accelerated in recent years, resulting in numerous promising subunits and glycoconjugate vaccines incorporating a variety of antigens. However, a second group of pathogenic Burkholderia species exists known as the Burkholderia cepacia complex (Bcc), a group of opportunistic bacteria which tend to affect individuals with weakened immunity or cystic fibrosis. To date, there have been few attempts to develop vaccines to Bcc species. Therefore, the primary goal of this review is to provide a broad overview of the various subunit antigens that have been tested in Bpc species, their protective efficacy, study limitations, and known or suspected mechanisms of protection. Then, we assess the reviewed Bpc antigens for their amino acid sequence conservation to homologous proteins found in Bcc species. We propose that protective Bpc antigens with a high degree of Bpc-to-Bcc sequence conservation could serve as components of a pan-Burkholderia vaccine capable of protecting against both disease-causing groups.

show abstract

BpOmpW Antigen Stimulates the Necessary Protective T-Cell Responses Against Melioidosis

Cited by 7 publications

References 42 publications

Evaluation of two different vaccine platforms for immunization against melioidosis and glanders

Evaluation of two different vaccine platforms for immunization against melioidosis and glanders

GlnH, a Novel Antigen That Offers Partial Protection against Verocytotoxigenic Escherichia coli Infection

Burkholderia pseudomallei Complex Subunit and Glycoconjugate Vaccines and Their Potential to Elicit Cross-Protection to Burkholderia cepacia Complex

Contact Info

Product

Resources

About