Application of Outer Membrane Vesicle of Neisseria meningitidis Serogroup B as a New Adjuvant to Induce Strongly Th1-Oriented Responses Against HIV-1

Aghasadeghi, Mohammad Reza; Salmani, Ali; Sadat, Seyed Mehdi; Javadi, Foozieh; Memarnejadian, Arash; Vahabpour, Rouhoullah; Zabihollahi, Rezvan; Moshiri, Arfa; Siadat, Seyed Davar

doi:10.2174/157016211798998772

Cited by 29 publications

(20 citation statements)

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“…An important consideration in relation to this is the presentation of antigens on NOMV in a more native environment and native conformation, compared to recombinant proteins, so that the epitopes on the NOMV vaccines better resemble those of the bacterium. Moreover, the intrinsic adjuvanticity of outer membrane vesicles is also relevant [44, 45]: the immune response against protective antigens on NOMV is likely to be enhanced due to the stimulation of innate receptors (e.g. TLR2 by PorB, TLR4 by LOS [46, 47]), and may also be affected by a different balance in IgG subtype induced by NOMV OE fHbp, compared to the recombinant protein [48].…”

Section: Discussionmentioning

confidence: 99%

Contribution of factor H-Binding protein sequence to the cross-reactivity of meningococcal native outer membrane vesicle vaccines with over-expressed fHbp variant group 1

et al. 2017

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Factor H-binding protein (fHbp) is an important meningococcal vaccine antigen. Native outer membrane vesicles with over-expressed fHbp (NOMV OE fHbp) have been shown to induce antibodies with broader functional activity than recombinant fHbp (rfHbp). Improved understanding of this broad coverage would facilitate rational vaccine design. We performed a pair-wise analysis of 48 surface-exposed amino acids involved in interacting with factor H, among 383 fHbp variant group 1 sequences. We generated isogenic NOMV-producing meningococcal strains from an African serogroup W isolate, each over-expressing one of four fHbp variant group 1 sequences (ID 1, 5, 9, or 74), including those most common among invasive African meningococcal isolates. Mice were immunised with each NOMV, and sera tested for IgG levels against each of the rfHbp ID and for ability to kill a panel of heterologous meningococcal isolates. At the fH-binding site, ID pairs differed by a maximum of 13 (27%) amino acids. ID 9 shared an amino acid sequence common to 83 ID types. The selected ID types differed by up to 6 amino acids, in the fH-binding site. All NOMV and rfHbp induced high IgG levels against each rfHbp. Serum killing from mice immunised with rfHbp was generally less efficient and more restricted compared to NOMV, which induced antibodies that killed most meningococci tested, with decreased stringency for ID type differences. Breadth of killing was mostly due to anti-fHbp antibodies, with some restriction according to ID type sequence differences. Nevertheless, under our experimental conditions, no relationship between antibody cross-reactivity and variation fH-binding site sequence was identified. NOMV over-expressing different fHbp IDs belonging to variant group 1 induce antibodies with fine specificities against fHbp, and ability to kill broadly meningococci expressing heterologous fHbp IDs. The work reinforces that meningococcal NOMV with OE fHbp is a promising vaccine strategy, and provides a basis for rational selection of antigen sequence types for over-expression on NOMV.

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Section: Discussionmentioning

confidence: 99%

Contribution of factor H-Binding protein sequence to the cross-reactivity of meningococcal native outer membrane vesicle vaccines with over-expressed fHbp variant group 1

et al. 2017

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“…Moreover, bacterial vesicles have been successfully used as vaccines or components of vaccines in pathogenic bacteria, including Vibrio cholerae (30), the oral (36,37). Bacterial vesicle vaccines, however, are not uniformly efficacious in that meningococcal vesicles conjugated with capsular polysaccharide are weak immunogens in infants and neonatal mice (38).…”

Section: Discussionmentioning

confidence: 99%

Proteomic Analysis and Immunogenicity of Mannheimia haemolytica Vesicles

Ayalew

Confer

Shrestha

et al. 2013

Clin Vaccine Immunol

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b Mannheimia haemolytica, a major causative agent in bovine respiratory disease, inflicts extensive losses each year on cattle producers. Commercially available vaccines are only partially efficacious. Immunity to M. haemolytica requires antibodies to secreted toxins and outer membrane proteins (OMPs) of the bacterium. Gram-negative bacteria produce membrane blebs or vesicles, the membrane components of which are primarily derived from OMPs. Accordingly, vesicles have been used as immunogens with various degrees of success. This study characterized components of M. haemolytica vesicles and determined their immunogenicity in mice and cattle. Liquid chromatography-tandem mass spectrometry (LC-MS/MS) analysis of vesicles from this bacterium identified 226 proteins, of which 58 (25.6%) were OMPs and periplasmic and one (0.44%) was extracellular. Vesicles were used to vaccinate dairy calves and BALB/c mice. Analyses of sera from calves and mice by enzyme-linked immunosorbent assay (ELISA) showed that circulating antibodies against M. haemolytica whole cells and leukotoxin were significantly higher on days 21 and 28 (P < 0.05) than on day 0. For control calves and mice, there were no significant differences in serum anti-whole-cell and leukotoxin antibody levels from days 0 and 21 or 28, respectively. Lesion scores of lungs from vaccinated calves (15.95%) were significantly (P < 0.05) lower than those from nonvaccinated calves (42.65%). Sera from mice on day 28 and calves on day 21 showed 100% serum bactericidal activity. Sera from vesicle-vaccinated mice neutralized leukotoxin.

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“…When introduced into the body, OMV antigens are presented by antigenpresenting cells (APCs) to CD4 + T cells 45,70,81,82 , which leads to the generation of antigen-specific B cell responses 45,78,82,83 . OMVs can induce protective immune responses during infection with a variety of pathogens -including V. cholerae 81 , H. pylori 80 , S. Typhimurium 45 and Shigella flexneri 84 -and this decreases bacterial burdens [85][86][87] and protects mice from sepsis or death 25,77,79,84,88 (TABLE 1).…”

Section: Presentation Of Omv Antigens Generation Of Protective Immunementioning

confidence: 99%

“…OMVs are highly stable when exposed to different temperatures and treatments 111 , they are non-replicative and hence safe, and they contain many of the immunogenic surface-associated and membrane-associated components of their parent bacterium 45,90,99,112,113 . Furthermore, the ability of OMVs to activate the innate immune system 14,20,22,24,25,69,114 , together with their particulate nature, provides these nano particles with their own adjuvant activity, as they are able to enhance antibody and T cell responses to antigens 76,83,87,115 . Finally, OMVs are very versatile as they can be bioengineered to express any chosen antigen 77,112,[116][117][118] and they can be manipulated to reduce their endotoxicity [119][120][121] .…”

Section: Development Of Vaccines Using Omvsmentioning

confidence: 99%

Immune modulation by bacterial outer membrane vesicles

2015

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Gram-negative bacteria shed extracellular outer membrane vesicles (OMVs) during their normal growth both in vitro and in vivo. OMVs are spherical, bilayered membrane nanostructures that contain many components found within the parent bacterium. Until recently, OMVs were dismissed as a by-product of bacterial growth; however, findings within the past decade have revealed that both pathogenic and commensal bacteria can use OMVs to manipulate the host immune response. In this Review, we describe the mechanisms through which OMVs induce host pathology or immune tolerance, and we discuss the development of OMVs as innovative nanotechnologies.

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Application of Outer Membrane Vesicle of Neisseria meningitidis Serogroup B as a New Adjuvant to Induce Strongly Th1-Oriented Responses Against HIV-1

Cited by 29 publications

References 0 publications

Contribution of factor H-Binding protein sequence to the cross-reactivity of meningococcal native outer membrane vesicle vaccines with over-expressed fHbp variant group 1

Contribution of factor H-Binding protein sequence to the cross-reactivity of meningococcal native outer membrane vesicle vaccines with over-expressed fHbp variant group 1

Proteomic Analysis and Immunogenicity of Mannheimia haemolytica Vesicles

Immune modulation by bacterial outer membrane vesicles

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