Antigen depot is not required for alum adjuvanticity

Hutchison, Sharon; Benson, Robert A.; Gibson, Vivienne B.; Pollock, Abigail H.; Garside, Paul; Brewer, James M.

doi:10.1096/fj.11-184556

Cited by 209 publications

(175 citation statements)

References 34 publications

(51 reference statements)

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“…This observation reinforces that a short period of local sterile inflammation is enough to "educate" DCs in bridging an innate to adaptive immune response as we previously demonstrated (5). This important notion is strongly supported by the investigation showing that surgical removal of the inoculation site containing alum 2 h after vaccination did not compromise the adjuvant effect of alum (26). The study, along with our observations, argues strongly the dispensability of prolonged inflammation at the inoculation site for effective vaccination.…”

Section: Discussionsupporting

confidence: 90%

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Effective and lesion-free cutaneous influenza vaccination

Wang

2015

Proc. Natl. Acad. Sci. U.S.A.

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The current study details efficient lesion-free cutaneous vaccination via vaccine delivery into an array of micropores in the skin, instead of bolus injection at a single site. Such delivery effectively segregated vaccine-induced inflammation, resulting in rapid resolution of the inflammation, provided that distances between any two micropores were sufficient. When the inoculation site was treated by FDA-approved nonablative fractional laser (NAFL) before insertion of a PR8 model influenza vaccine-packaged, biodegradable microneedle array (MNs), mice displayed vigorous antigenuptake, eliciting strong Th1-biased immunity. These animals were completely protected from homologous viral challenges, and fully or partially protected from heterologous H1N1 and H3N2 viral challenges, whereas mice receiving MNs alone suffered from severe illnesses or died of similar viral challenges. NAFL-mediated adjuvanicity was ascribed primarily to dsDNA and other "danger" signals released from laser-damaged skin cells. Thus, mice deficient in dsDNA-sensing pathway, but not Toll like receptor (TLR) or inflammasome pathways, showed poor responses to NAFL. Importantly, with this novel approach both mice and swine exhibited strong protective immunity without incurring any appreciable skin irritation, in sharp contrast to the overt skin irritation caused by intradermal injections. The effective lesion-free cutaneous vaccination merits further clinical studies.biodegradable microneedle | nonablative fractional laser | dsDNA S ubstantial evidence has shown that skin is a more potent site for vaccination than muscle because the former contains a large number of antigen presenting cells (APCs) and abundant network of lymphatic vessels. Moreover, skin offers potential for painless, needle-free, and self-applicable immunization, which would particularly benefit annual influenza vaccination of large populations (1, 2). However, skin immunization has not been broadly adopted to date, due to lack of safe adjuvants and technical difficulties in injecting vaccines into the ultrathin (<2 mm) skin tissue (3,4). We have demonstrated that controllable skin injury can serve as safe "adjuvant" for cutaneous vaccination and similar observations have been also made by other investigators (5-7). Treatment of the inoculation site with nonablative fractional laser (NAFL) generates an array of microthermal zones (MTZs) beneath the stratum corneum (8). The dying cells in the MTZs release "danger" signals that provoke sterile inflammation that is however constrained within individual MTZs. This array of microsterile inflammatory zones is resolved quickly, effectively averting skin lesion, provided that affected and unaffected areas of the skin are adequately balanced (8). Importantly, despite fast resolution, the microinflammation zones prove sufficient in augmentation of adaptive immune responses against the vaccine (5). In addition, this standalone adjuvant does not affect the volume of administration or formulation of the vaccine, which are serious hurdles for...

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Section: Discussionsupporting

confidence: 90%

“…All experiments were repeated twice with similar results. inoculation site was not necessary for effective immunization (5,26). Moreover, in comparison with vaccination of MNs alone, NAFL treatment significantly enhanced the immune responses, without incurring any adverse events.…”

Section: Nafl Significantly Broadens Immunity Induced By Influenza Vamentioning

confidence: 93%

Effective and lesion-free cutaneous influenza vaccination

Wang

2015

Proc. Natl. Acad. Sci. U.S.A.

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“…Alum appears to form a depot with some antigens (12) but not others (115) and likely undergoes desorption of some antigens under in vivo conditions (116). Recent studies have further demonstrated that, following alum immunization, the injection site can be surgically removed 2 hours after injection with no effect on the humoral immune response, suggesting that depot formation is not a critical part of alum's mechanism of action (117,118).…”

Section: Programming Vaccine Kineticsmentioning

confidence: 99%

Beyond antigens and adjuvants: formulating future vaccines

Moyer¹,

Zmolek²,

Irvine³

2016

Journal of Clinical Investigation

326

292

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“…Hutchison et al demonstrated that removing the injection site 2 h after immunization did not result in compromised immune responses, indicating that the antigen deposit e®ect may not be important for the adjuvant e®ect of Alum. 30 Meanwhile, a number of studies suggested the underlying mechanism owing to toxicity of Alum 31 : Alum kills host cells, and dead cells in turn release danger signals, including uric acid, genomic DNAs, etc. [31][32][33] These danger signals are designated as damage-associated molecular patterns (DAMPs).…”

Section: Laser Induced Micro-sterile In°ammation Array As Vaccine Adjmentioning

confidence: 99%

Laser facilitates vaccination

Wang

Chen

et al. 2016

J. Innov. Opt. Health Sci.

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Development of novel vaccine deliveries and vaccine adjuvants is of great importance to address the dilemma that the vaccine¯eld faces: to improve vaccine e±cacy without compromising safety. Harnessing the speci¯c e®ects of laser on biological systems, a number of novel concepts have been proposed and proved in recent years to facilitate vaccination in a safer and more e±cient way. The key advantage of using laser technology in vaccine delivery and adjuvantation is that all processes are initiated by physical e®ects with no foreign chemicals administered into the body. Here, we review the recent advances in using laser technology to facilitate vaccine delivery and augment vaccine e±cacy as well as the underlying mechanisms.

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Antigen depot is not required for alum adjuvanticity

Cited by 209 publications

References 34 publications

Effective and lesion-free cutaneous influenza vaccination

Effective and lesion-free cutaneous influenza vaccination

Beyond antigens and adjuvants: formulating future vaccines

Laser facilitates vaccination

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