AI Article Synopsis

  • Burkholderia pseudomallei causes melioidosis, leading to severe health issues such as sepsis and pneumonia, mostly in Southeast Asia and Northern Australia, with no approved vaccines available.
  • Researchers developed a potential vaccine candidate using the OmpW protein from the bacteria, which showed promising immunoprotective effects in mice, achieving a 75% survival rate compared to 25% in controls.
  • The OmpW protein is conserved across multiple strains of B. pseudomallei, suggesting it could provide broad protection against melioidosis, indicating its potential as a key component in a future vaccine.

Article Abstract

Burkholderia pseudomallei is the causative agent of melioidosis, which is associated with a range of clinical manifestations, including sepsis and fatal pneumonia and is endemic in Southeast Asia and Northern Australia. Treatment can be challenging and control of infection involves prolonged antibiotic therapy, yet there are no approved vaccines available to prevent infection. Our aim was to develop and assess the potential of a prophylactic vaccine candidate targeted against melioidosis. The identified candidate is the 22kDa outer membrane protein, OmpW. We previously demonstrated that this protein was immunoprotective in mouse models of Burkholderia cepacia complex (Bcc) infections. We cloned Bp_ompW in Escherichia coli, expressed and purified the protein. Endotoxin free protein administered with SAS adjuvant protected Balb/C mice (75% survival) relative to controls (25% survival) (p<0.05). A potent serological response was observed with IgG2a to IgG1 ratio of 6.0. Furthermore C57BL/6 mice were protected for up to 80 days against a lethal dose of B. pseudomallei and surpassed the efficacy of the live attenuated 2D2 positive control. BpompW is homologous across thirteen sequenced B. pseudomallei strains, indicating that it should be broadly protective against B. pseudomallei. In conclusion, we have demonstrated that BpOmpW is able to induce protective immunity against melioidosis and is likely to be an effective vaccine antigen, possibly in combination with other subunit antigens.

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Source
http://dx.doi.org/10.1016/j.vaccine.2016.03.088DOI Listing

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