Literature DB >> 31553872

Mucosal Immunization with a pH-Responsive Nanoparticle Vaccine Induces Protective CD8+ Lung-Resident Memory T Cells.

Frances C Knight1, Pavlo Gilchuk2,3,4, Amrendra Kumar2,4, Kyle W Becker5, Sema Sevimli5, Max E Jacobson5, Naveenchandra Suryadevara2,4, Lihong Wang-Bishop5, Kelli L Boyd2,6, James E Crowe2,3,6,7,8,9,10, Sebastian Joyce2,4,6,10, John T Wilson1,5,6,10,11.   

Abstract

Tissue-resident memory T cells (TRM) patrol nonlymphoid organs and provide superior protection against pathogens that commonly infect mucosal and barrier tissues, such as the lungs, intestine, liver, and skin. Thus, there is a need for vaccine technologies that can induce a robust, protective TRM response in these tissues. Nanoparticle (NP) vaccines offer important advantages over conventional vaccines; however, there has been minimal investigation into the design of NP-based vaccines for eliciting TRM responses. Here, we describe a pH-responsive polymeric nanoparticle vaccine for generating antigen-specific CD8+ TRM cells in the lungs. With a single intranasal dose, the NP vaccine elicited airway- and lung-resident CD8+ TRM cells and protected against respiratory virus challenge in both sublethal (vaccinia) and lethal (influenza) infection models for up to 9 weeks after immunization. In elucidating the contribution of material properties to the resulting TRM response, we found that the pH-responsive activity of the carrier was important, as a structurally analogous non-pH-responsive control carrier elicited significantly fewer lung-resident CD8+ T cells. We also demonstrated that dual-delivery of protein antigen and nucleic acid adjuvant on the same NP substantially enhanced the magnitude, functionality, and longevity of the antigen-specific CD8+ TRM response in the lungs. Compared to administration of soluble antigen and adjuvant, the NP also mediated retention of vaccine cargo in pulmonary antigen-presenting cells (APCs), enhanced APC activation, and increased production of TRM-related cytokines. Overall, these data suggest a promising vaccine platform technology for rapid generation of protective CD8+ TRM cells in the lungs.

Entities:  

Keywords:  influenza; intranasal; lungs; nanoparticle; nucleic acid adjuvant; subunit vaccine; tissue-resident memory T cells

Mesh:

Substances:

Year:  2019        PMID: 31553872      PMCID: PMC6832804          DOI: 10.1021/acsnano.9b00326

Source DB:  PubMed          Journal:  ACS Nano        ISSN: 1936-0851            Impact factor:   15.881


  101 in total

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Journal:  ACS Nano       Date:  2020-07-31       Impact factor: 15.881

2.  Engineered Nanoparticulate Vaccines to Combat Recurring and Pandemic Influenza Threats.

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