Enhanced Immunogenicity of an HIV-1 DNA Vaccine Delivered with Electroporation via Combined Intramuscular and Intradermal Routes

Mann, J. Adin; McKay, Paul F.; Fiserova, A.; Klein, Katja; Cope, Alethea; Rogers, P. S. Z.; Swales, Julie; Seaman, Michael S.; Combadière, Béhazine; Shattock, Robin J.

doi:10.1128/jvi.00183-14

Cited by 32 publications

(31 citation statements)

References 38 publications

(44 reference statements)

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“…Sera, feces, and vaginal washes were collected on days 0, 14, 28, and 42 and treated as described previously for subsequent ELISA-based analyses (14). Affinity assays were performed by ELISA as described by Mann et al (15). Serum CXCL13 levels were determined in 10-fold diluted samples using a DuoSet ELISA Mouse CXCL13 Kit (R&D Systems).…”

Section: In Vivo Immunogenicity Of Vaccine Formulationsmentioning

confidence: 99%

Cutting Edge: A Dual TLR2 and TLR7 Ligand Induces Highly Potent Humoral and Cell-Mediated Immune Responses

Gutjahr

Papagno

Nicoli

et al. 2017

The Journal of Immunology

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TLR agonists are currently being developed and tested as adjuvants in various formulations to optimize the immunogenicity and efficacy of vaccines. The aim of this study was to evaluate the immunostimulatory properties of a novel compound incorporating covalently linked moieties designed to stimulate both TLR2 and TLR7. This dual TLR2/TLR7 agonist induced the maturation of dendritic cells and primed substantial populations of cytolytic and highly polyfunctional effector CD8 T cells in vitro, and safely potentiated the immunogenic properties of a nanoparticulate Ag in vivo, eliciting humoral responses with a balanced T1/T2 profile in mice. Collectively, these data reveal the potential utility of chimeric adjuvants with synergistic activities mediated via TLRs.

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Section: In Vivo Immunogenicity Of Vaccine Formulationsmentioning

confidence: 99%

Cutting Edge: A Dual TLR2 and TLR7 Ligand Induces Highly Potent Humoral and Cell-Mediated Immune Responses

Gutjahr

Papagno

Nicoli

et al. 2017

The Journal of Immunology

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“…After the addition of 1N H 2 SO 4 to stop the reaction, the optical densities (OD) at 450 nm and 630 nm were measured in a microplate reader. To estimate the avidity of the immunoglobulins, we have tested antibody/antigen binding resistance to 8 M urea using a published method [31]. A prerequisite step was to have serum dilutions giving an OD at 450 nm of between 1 and 1.5.…”

Section: Methodsmentioning

confidence: 99%

“…The plates were then washed three times with PBS/0.05% Tween-20 or PBS/0.05% Tween-20/urea 8 M. The last steps were performed as for the ELISA assays. According to Mann et al [31], the avidity index corresponds to OD450 of urea-treated samples/OD450 of PBS/0.05% Tween-20 samples.…”

Section: Methodsmentioning

confidence: 99%

Poly(Lactic Acid) Nanoparticles Targeting α5β1 Integrin as Vaccine Delivery Vehicle, a Prospective Study

et al. 2016

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Biodegradable polymeric nanoparticles are vehicles of choice for drug delivery and have the ability to encapsulate and present at their surface different molecules of interest. Among these bio-nanocarriers, poly(lactic acid) (PLA) nanoparticles have been used as adjuvant and vehicle for enhanced vaccine efficacy. In order to develop an approach to efficient vaccine delivery, we developed nanoparticles to target α5β1 positive cells. We first overproduced, in bacteria, human fibronectin FNIII9/10 recombinant proteins possessing an integrin α5β1 binding site, the RGDS sequence, or a mutated form of this site. After having confirmed the integrin binding properties of these recombinant proteins in cell culture assays, we were able to formulate PLA nanoparticles with these FNIII9/10 proteins at their surface. We then confirmed, by fluorescence and confocal microscopy, an enhanced cellular uptake by α5β1+ cells of RGDS-FNIII9/10 coated PLA nanoparticles, in comparison to KGES-FNIII9/10 coated or non-coated controls. As a first vaccination approach, we prepared PLA nanoparticles co-coated with p24 (an HIV antigen), and RGDS- or KGES-FNIII9/10 proteins, followed by subcutaneous vaccine administration, in mice. Although we did not detect improvements in the apparent humoral response to p24 antigen in the serum of RGDS/p24 nanoparticle-treated mice, the presence of the FNIII proteins increased significantly the avidity index of anti-p24 antibodies compared to p24-nanoparticle-injected control mice. Future developments of this innovative targeted vaccine are discussed.

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“…125 However, immunogenicity can now be improved with intradermal delivery using electroporation, a technique that applies transient electrical pulses to cells to increase the permeability of the cell membrane and allow the nucleic acid to enter, or administration in conjunction with molecular adjuvants, such as interleukin 12. 126,127 These adjustments encouraged stimulation of both the cellular and humoral arms of the immune system. 127 HVTN 087 was a Phase I trial designed to assess the effect of increasing doses of plasmid DNA IL-12 adjuvant in conjunction with an HIV-1 multiantigen DNA vaccine delivered via electroporation.…”

Section: Dna-based Vaccinesmentioning

confidence: 99%

Innovations in HIV-1 Vaccine Design

Jones

Moody

Thompson

2020

Clinical Therapeutics

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Purpose: The field of HIV-1 vaccinology has evolved during the last 30 years from the first viral vector HIV gene insert constructs to vaccination regimens using a myriad of strategies. These strategies now include germline-targeting, lineagebased, and structure-guided immunogen design. This narrative review outlines the historical context of HIV vaccinology and subsequently highlights the scientific discoveries during the last 6 years that promise to propel the field forward.Methods: We conducted a search of 2 electronic databases, PubMed and EMBASE, for experimental studies that involved new HIV immunogen designs between 2013 and 2019. During the title and abstract reviews, publications were excluded if they were written in language other than English and/or were a letter to the editor, a commentary, or a conference-only presentation. We then used ClinicalTrials.gov to identify completed and ongoing clinical trials using these strategies.Findings: The HIV vaccinology field has undergone periods of significant growth during the last 3 decades. Findings elucidated in preclinical studies have revealed the importance of the interaction between the cellular and humoral immune system. As a result, several new rationally designed vaccine strategies have been developed and explored in the last 6 years, including native-like envelope trimers, nanoparticle, and mRNA vaccine design strategies among others. Several of these strategies have shown enough promise in animal models to progress toward first-inhuman Phase I clinical trials.Implications: Rapid developments in preclinical and early-phase clinical studies suggest that a tolerable and effective HIV vaccine may be on the horizon. (Clin Ther. xxxx;xxx:xxx)

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Enhanced Immunogenicity of an HIV-1 DNA Vaccine Delivered with Electroporation via Combined Intramuscular and Intradermal Routes

Cited by 32 publications

References 38 publications

Cutting Edge: A Dual TLR2 and TLR7 Ligand Induces Highly Potent Humoral and Cell-Mediated Immune Responses

Cutting Edge: A Dual TLR2 and TLR7 Ligand Induces Highly Potent Humoral and Cell-Mediated Immune Responses

Poly(Lactic Acid) Nanoparticles Targeting α5β1 Integrin as Vaccine Delivery Vehicle, a Prospective Study

Innovations in HIV-1 Vaccine Design

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