Optimization, Production, and Characterization of a CpG-Oligonucleotide-Ficoll Conjugate Nanoparticle Adjuvant for Enhanced Immunogenicity of Anthrax Protective Antigen

Milley, Bob; Kiwan, Radwan; Ott, Gary; Calacsan, Carlo; Kachura, Melissa A.; Campbell, John D.; Kanzler, Holger; Coffman, Robert L.

doi:10.1021/acs.bioconjchem.6b00107

Cited by 9 publications

(10 citation statements)

References 34 publications

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“…After combining FUC-HTCC nanoparticles with the approved anthrax vaccine AVA, the novel anthrax nanovaccine significantly increased the IgG antibody titers and provided complete protection compared with CpG plus AVA (75%) or AVA alone (50%) in mice exposed to anthrax lethal toxin challenge [162] . However, some other polymer particles (e.g., sucrose polymer, chitosan or its derivative, and others) need an addition of an adjuvant (e.g., CpG, mast cell activator compound 48/80 (C48/80), Poly I:C) to elicit an enhanced immune response [163] , [164] , [231] . Although mice immunized with these liposomes or polymer-based vaccines can achieve a high protection rate after challenge, the use of adjuvants reduces their competitiveness compared with viral vectors.…”

Section: Bacterial Infectious Diseases and Advanced Delivery Systemsmentioning

confidence: 99%

Prophylactic vaccine delivery systems against epidemic infectious diseases

Pan¹,

Yue

Zhu³

et al. 2021

Advanced Drug Delivery Reviews

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Prophylactic vaccines have evolved from traditional whole-cell vaccines to safer subunit vaccines. However, subunit vaccines still face problems, such as poor immunogenicity and low efficiency, while traditional adjuvants are usually unable to meet specific response needs. Advanced delivery vectors are important to overcome these barriers; they have favorable safety and effectiveness, tunable properties, precise location, and immunomodulatory capabilities. Nevertheless, there has been no systematic summary of the delivery systems to cover a wide range of infectious pathogens. We herein summarized and compared the delivery systems for major or epidemic infectious diseases caused by bacteria, viruses, fungi, and parasites. We also included the newly licensed vaccines (e.g., COVID-19 vaccines) and those close to licensure. Furthermore, we highlighted advanced delivery systems with high efficiency, cross-protection, or long-term protection against epidemic pathogens, and we put forward prospects and thoughts on the development of future prophylactic vaccines.

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Section: Bacterial Infectious Diseases and Advanced Delivery Systemsmentioning

confidence: 99%

Prophylactic vaccine delivery systems against epidemic infectious diseases

Pan¹,

Yue

Zhu³

et al. 2021

Advanced Drug Delivery Reviews

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“…In a maleimide-thiol reaction, the nucleophilic thiolate anion attacks the π-bond of maleimide, forming the enolate intermediate and yielding the desired conjugate. This technique has been widely used to assemble nanoparticle vaccines [184][185][186]. In a study on refining a liposomal formulation of HIV vaccine, thiol chemistry was exploited to control the physiological conformation and density of the target antigen to modulate immune responses [186].…”

Section: Chemical Conjugationmentioning

confidence: 99%

Nanoparticle Vaccines Adopting Virus-like Features for Enhanced Immune Potentiation

et al. 2017

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Synthetic nanoparticles play an increasingly significant role in vaccine design and development as many nanoparticle vaccines show improved safety and efficacy over conventional formulations. These nanoformulations are structurally similar to viruses, which are nanoscale pathogenic organisms that have served as a key selective pressure driving the evolution of our immune system. As a result, mechanisms behind the benefits of nanoparticle vaccines can often find analogue to the interaction dynamics between the immune system and viruses. This review covers the advances in vaccine nanotechnology with a perspective on the advantages of virus mimicry towards immune potentiation. It provides an overview to the different types of nanomaterials utilized for nanoparticle vaccine development, including functionalization strategies that bestow nanoparticles with virus-like features. As understanding of human immunity and vaccine mechanisms continue to evolve, recognizing the fundamental semblance between synthetic nanoparticles and viruses may offer an explanation for the superiority of nanoparticle vaccines over conventional vaccines and may spur new design rationales for future vaccine research. These nanoformulations are poised to provide solutions towards pressing and emerging human diseases.

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confidence: 99%

“…We estimated a conjugation ratio of 16 ± 5 CpG/E2 nanoparticle (Supporting Information), within the range achieved for a synthetic nanoparticle system, when adjusting for the difference in particle diameter. 24 Depending on the conformation of the PEG (i.e., brush or mushroom), the polymer may not be fully extended and the maleimide may not be easily accessible to react with the thiol-terminated CpG. 25 Dynamic light scattering (DLS) revealed no significant changes in average particle sizes (Figure 1), demonstrating that conjugation of PEG and ssDNA to E2 did not cause large increases in particle size or aggregation.…”

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confidence: 99%

Display of DNA on Nanoparticles for Targeting Antigen Presenting Cells

Molino

Neek

Tucker

et al. 2017

ACS Biomater. Sci. Eng.

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Efficient delivery of antigens is of paramount concern in immunotherapies. We aimed to target antigen presenting cells (APCs) by conjugating CpG oligonucleotides to an E2 protein nanoparticle surface (CpG-PEG-E2). Compared to E2 alone, we observed ~4-fold increase of in vitro APC uptake of both CpG-PEG-E2 and E2 conjugated to non-CpG DNA. Furthermore, compared to E2-alone or E2 functionalized solely with polyethylene glycol (PEG), the CpG-PEG-E2 showed enhanced lymph node retention up to at least 48 hr and 2-fold increase in APC uptake in vivo, parameters which are advantageous for vaccine success. This suggests that enhanced APC uptake of nanoparticles mediated by oligonucleotide display may help overcome delivery barriers in vaccine development.

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Optimization, Production, and Characterization of a CpG-Oligonucleotide-Ficoll Conjugate Nanoparticle Adjuvant for Enhanced Immunogenicity of Anthrax Protective Antigen

Cited by 9 publications

References 34 publications

Prophylactic vaccine delivery systems against epidemic infectious diseases

Prophylactic vaccine delivery systems against epidemic infectious diseases

Nanoparticle Vaccines Adopting Virus-like Features for Enhanced Immune Potentiation

Display of DNA on Nanoparticles for Targeting Antigen Presenting Cells

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