Anti-Alpha-Toxin Monoclonal Antibody and Antibiotic Combination Therapy Improves Disease Outcome and Accelerates Healing in a Staphylococcus aureus Dermonecrosis Model

Hilliard, Jamese J.; Datta, Vivekananda; Tkaczyk, Christine; Hamilton, Melissa; Sadowska, Agnieszka; Jones-Nelson, Omari; O’Day, Terrence; Weiss, Jason; Szarka, Szabolcs; Nguyen, Vien; Prókai, László; Suzich, JoAnn; Stover, C. Kendall; Sellman, Bret R.

doi:10.1128/aac.03918-14

Cited by 49 publications

(47 citation statements)

References 44 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…(50). Intranasal challenge of S. aureus leads to lung infection; both the associated disease mortality and the bacterial burden are increased in IL-12p35 Ϫ/Ϫ mice (51). Following intracerebral inoculation of staphylococci, the initial phases of brain abscess formation were not impacted by IL-12 (p35) deficiency; however, IL-12p35 Ϫ/Ϫ mice displayed fewer clinical disease symptoms and healed more rapidly than wild-type mice (52).…”

Section: Discussionmentioning

confidence: 99%

EssE Promotes Staphylococcus aureus ESS-Dependent Protein Secretion To Modify Host Immune Responses during Infection

et al. 2017

View full text Add to dashboard Cite

Staphylococcus aureus, an invasive pathogen of humans and animals, requires a specialized ESS pathway to secrete proteins (EsxA, EsxB, EsxC, and EsxD) during infection. Expression of ess genes is required for S. aureus establishment of persistent abscess lesions following bloodstream infection; however, the mechanisms whereby effectors of the ESS pathway implement their virulence strategies were heretofore not known. Here, we show that EssE forms a complex with other members of the ESS secretion pathway and its substrates, promoting the secretion of EsxA, EsxB, EsxC, EsxD, and EssD. During bloodstream infection of mice, the S. aureus essE mutant displays defects in host cytokine responses, specifically in the production of interleukin-12 (IL-12) (p40/p70) and the suppression of RANTES (CCL5), activators of T H 1 T cell responses and immune cell chemotaxis, respectively. Thus, essE-mediated secretion of protein effectors via the ESS pathway may enable S. aureus to manipulate host immune responses by modifying the production of cytokines.IMPORTANCE Staphylococcus aureus and other firmicutes evolved a specialized ESS (EsxA/ESAT-6-like secretion system) pathway for the secretion of small subsets of proteins lacking canonical signal peptides. The molecular mechanisms for ESSdependent secretion and their functional purpose are still unknown. We demonstrate here that S. aureus EssE functions as a membrane assembly platform for elements of the secretion machinery and their substrates. Furthermore, S. aureus EssEmediated secretion contributes to the production or the suppression of specific cytokines during host infection, thereby modifying immune responses toward this pathogen.

show abstract

Section: Discussionmentioning

confidence: 99%

EssE Promotes Staphylococcus aureus ESS-Dependent Protein Secretion To Modify Host Immune Responses during Infection

et al. 2017

View full text Add to dashboard Cite

show abstract

“…In ongoing efforts to use these as vaccination targets, alpha-toxin toxoid, for example, has proven to represent a very promising vaccination agent in efforts to reduce S. aureus skin and lung infection (21). In addition, we believe that virulence determinants that are found to strongly impact colonization and virulence phenotypes in MRSA strains with considerable epidemiological importance, wide geographical distribution, and likely further spread, such as SasX, should also be analyzed as potential vaccine targets.…”

Section: Discussionmentioning

confidence: 99%

Targeting Surface Protein SasX by Active and Passive Vaccination To Reduce Staphylococcus aureus Colonization and Infection

Liu

Hong

et al. 2015

Infect Immun

View full text Add to dashboard Cite

c SasX is a recently described surface protein of Staphylococcus aureus that is linked to the epidemic success of hospital-associated methicillin-resistant clones, in particular in Asia. It enhances nasal colonization and virulence in skin and lung infection models. Here, we evaluated the potential of SasX as a vaccine component in passive and active immunization efforts using mouse infection models. We found that SasX induced a specific immune response predominantly based on IgG1 antibodies. Active immunization with recombinant SasX or passive immunization with rabbit polyclonal anti-SasX IgG significantly decreased the size of lesions caused by S. aureus in a skin infection model. Furthermore, active immunization reduced acute lung injury in a lung infection model. Moreover, active or passive immunization significantly reduced S. aureus colonization in a nasal colonization model. Finally, anti-SasX IgG enhanced the susceptibility of S. aureus to killing by human neutrophils. We conclude that SasX is a potential target for therapeutics or vaccines designed to moderate colonization and infection by sasX-positive epidemic strains of S. aureus. Staphylococcus aureus is a major global source of morbidity and mortality (1), causing more than 11,000 deaths per year in the United States alone (2). It is particularly notorious as a dangerous hospital-associated pathogen. Treatment of S. aureus infections is severely complicated by antibiotic resistance (3). In particular, resistance to methicillin in methicillin-resistant S. aureus (MRSA), which in many countries occurs in more than half of infectious S. aureus isolates, is a major health care concern. In addition, many S. aureus strains are resistant to a wide variety of other antibiotics, leaving only very limited options for treatment. In an era that has seen a broad withdrawal of pharmaceutical companies from the much-needed development of novel antibiotics, researchers in companies and academia are again beginning to attempt vaccine development against S. aureus. A working vaccine against S. aureus infections is not available, and multiple reasons have been discussed for why an anti-S. aureus vaccine is difficult to find (4, 5). These include first and foremost the large arsenal of immune evasion factors of S. aureus, which target both acquired and innate immune defenses (6). However, there is promising evidence indicating that passive and active vaccination against S. aureus should in principle be possible, notwithstanding the fact that we still do not completely understand the mechanisms the immune system uses for protective immunity against S. aureus (4).Infective S. aureus and MRSA isolates are very diverse regarding geographical origin and time of isolation. Over the years, specific predominant MRSA clones arose and were thereafter replaced by others, in a scenario of epidemic waves (7). Furthermore, infections in different geographic areas are characterized by a divergent and often endemic composition of prevalent S. aureus and MRSA lineages. This situation ...

show abstract

“…Pathogen-specific monoclonal antibodies are either used independently for disease prevention or in combination with antibiotics to treat bacterial infections [18]. Antibodies neutralize the effects of bacterial toxins [19][20][21][22]; they can also be directed against bacterial antigens [23][24][25] and quorum-sensing signals [26,27] inhibiting biofilm formation enhancing the effect of antibioticbased treatment and can be employed for combating persister cells insensitive to antibiotics [28,29].…”

Section: Antibodiesmentioning

confidence: 99%

Alternatives to Antibiotics: Phage Lytic Enzymes and Phage Therapy

Nazarov¹

2018

BRSMU

View full text Add to dashboard Cite

Anti-Alpha-Toxin Monoclonal Antibody and Antibiotic Combination Therapy Improves Disease Outcome and Accelerates Healing in a Staphylococcus aureus Dermonecrosis Model

Cited by 49 publications

References 44 publications

EssE Promotes Staphylococcus aureus ESS-Dependent Protein Secretion To Modify Host Immune Responses during Infection

EssE Promotes Staphylococcus aureus ESS-Dependent Protein Secretion To Modify Host Immune Responses during Infection

Targeting Surface Protein SasX by Active and Passive Vaccination To Reduce Staphylococcus aureus Colonization and Infection

Alternatives to Antibiotics: Phage Lytic Enzymes and Phage Therapy

Contact Info

Product

Resources

About