A Novel Staphylococcus aureus Vaccine: Iron Surface Determinant B Induces Rapid Antibody Responses in Rhesus Macaques and Specific Increased Survival in a Murine S. aureus Sepsis Model

Abstract: Staphylococcus aureus is a major cause of nosocomial infections worldwide, and the rate of resistance to clinically relevant antibiotics, such as methicillin, is increasing; furthermore, there has been an increase in the number of methicillin-resistant S. aureus community-acquired infections. Effective treatment and prevention strategies are urgently needed. We investigated the potential of the S. aureus surface protein iron surface determinant B (IsdB) as a prophylactic vaccine against S. aureus infection. Is… Show more

“…Of the 50 hospital controls, 39 had sera from multiple time-points (median number of samples: 4, range: 2 to 8), and the mean time for final follow-up was 11.6 days post-diagnosis (range: 2 to 34 days). The mean time of followup was slightly longer for the hospital S. aureus cases compared deleted strain, 9,16 confirming the specificity of the vaccine. An observed rise in anti-IsdB titers induced by IsdB formulated on Merck aluminum adjuvant (MAA) correlated with protection against lethal S. aureus challenge, 9 indicating that antibody titers may be used as a nominal biomarker for vaccine efficacy.…”

“…9 The potential use of this antigen as a component of a vaccine for prevention of S. aureus disease has been previously described. 9,15 However, as a stand-alone vaccine (V710), protection was not observed in a clinical efficacy trial among cardiac surgery patients, 21 despite a significant increase in IsdB antibody titers in the V710 vaccinated patients. Although the IsdB specific with the hospital controls (p = 0.05).…”

“…8 The IsdB antigen is highly conserved and expressed on all isolates examined to date. 9 Due to upregulation in iron-limited environments, 9,10 IsdB is theoretically available for immune recognition during infection in the human host, where iron is highly sequestered. 8,11,12 Expression of IsdB was highly upregulated by essentially 100% of strain Becker grown under in vivo conditions in rats.…”

“…8,11,12 Expression of IsdB was highly upregulated by essentially 100% of strain Becker grown under in vivo conditions in rats. 10 Multiple reports have demonstrated IsdB to be a potential vaccine candidate for the prevention of S. aureus infection 9,[13][14][15][16] in rodent challenge models. Importantly, enhanced protection from lethal sepsis in rodent models was mediated by both IsdB-specific CD4+ T cells, 16 and IsdB-specific mAb.…”

“…Importantly, enhanced protection from lethal sepsis in rodent models was mediated by both IsdB-specific CD4+ T cells, 16 and IsdB-specific mAb. 10,13,[17][18][19] The protection afforded by vaccination with IsdB in rodents was lost if the animals were challenged with an IsdB fluid (9), surgical tissue (22), synovial fluid (17), sputum (9), or other sites (5) during routine clinical care. Of the 52 S. aureus isolates, 51 were spa typed; a single isolate failed to grow sufficiently in culture for spa determination.…”

Naturally occurring IgG antibody levels to theStaphylococcus aureusprotein IsdB in humans

“…Of the 50 hospital controls, 39 had sera from multiple time-points (median number of samples: 4, range: 2 to 8), and the mean time for final follow-up was 11.6 days post-diagnosis (range: 2 to 34 days). The mean time of followup was slightly longer for the hospital S. aureus cases compared deleted strain, 9,16 confirming the specificity of the vaccine. An observed rise in anti-IsdB titers induced by IsdB formulated on Merck aluminum adjuvant (MAA) correlated with protection against lethal S. aureus challenge, 9 indicating that antibody titers may be used as a nominal biomarker for vaccine efficacy.…”

“…9 The potential use of this antigen as a component of a vaccine for prevention of S. aureus disease has been previously described. 9,15 However, as a stand-alone vaccine (V710), protection was not observed in a clinical efficacy trial among cardiac surgery patients, 21 despite a significant increase in IsdB antibody titers in the V710 vaccinated patients. Although the IsdB specific with the hospital controls (p = 0.05).…”

“…8 The IsdB antigen is highly conserved and expressed on all isolates examined to date. 9 Due to upregulation in iron-limited environments, 9,10 IsdB is theoretically available for immune recognition during infection in the human host, where iron is highly sequestered. 8,11,12 Expression of IsdB was highly upregulated by essentially 100% of strain Becker grown under in vivo conditions in rats.…”

“…8,11,12 Expression of IsdB was highly upregulated by essentially 100% of strain Becker grown under in vivo conditions in rats. 10 Multiple reports have demonstrated IsdB to be a potential vaccine candidate for the prevention of S. aureus infection 9,[13][14][15][16] in rodent challenge models. Importantly, enhanced protection from lethal sepsis in rodent models was mediated by both IsdB-specific CD4+ T cells, 16 and IsdB-specific mAb.…”

“…Importantly, enhanced protection from lethal sepsis in rodent models was mediated by both IsdB-specific CD4+ T cells, 16 and IsdB-specific mAb. 10,13,[17][18][19] The protection afforded by vaccination with IsdB in rodents was lost if the animals were challenged with an IsdB fluid (9), surgical tissue (22), synovial fluid (17), sputum (9), or other sites (5) during routine clinical care. Of the 52 S. aureus isolates, 51 were spa typed; a single isolate failed to grow sufficiently in culture for spa determination.…”

Naturally occurring IgG antibody levels to theStaphylococcus aureusprotein IsdB in humans

Effect of an Investigational Vaccine for Preventing Staphylococcus aureus Infections After Cardiothoracic Surgery

Staphylococcus