4.7 Review

Delivery strategies to enhance oral vaccination against enteric infections

Journal

ADVANCED DRUG DELIVERY REVIEWS
Volume 91, Issue -, Pages 52-69

Publisher

ELSEVIER
DOI: 10.1016/j.addr.2015.03.007

Keywords

Delivery system; Adjuvant; Nanoparticle; Mucosal; Gastrointestinal; Oral; Vaccine

Funding

  1. Science Foundation Ireland (SFI) [12/IA/1421]
  2. SFI Research Centre, Advanced Materials and BioEngineering Research (AMBER) [SFI/12/RC/2278]
  3. European Union FP7 programme HELICOVAXOR [FP7-SME-2012-1]
  4. Irish Research Council

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While the majority of human pathogens infect the body through mucosal sites, most licensed vaccines are injectable. In fact the only mucosal vaccine that has been widely used globally for infant and childhood vaccination programs is the oral polio vaccine (OPV) developed by Albert Sabin in the 1950s. While oral vaccines against Cholera, rotavirus and Salmonella typhi have also been licensed, the development of additional non-living oral vaccines against these and other enteric pathogens has been slow and challenging. Mucosal vaccines can elicit protective immunity at the gut mucosa, in part via antigen-specific secretory immunoglobulin A (SIgA). However, despite their advantages over the injectable route, oral vaccines face many hurdles. A key challenge lies in design of delivery strategies that can protect antigens from degradation in the stomach and intestine, incorporate appropriate immune-stimulatory adjuvants and control release at the appropriate gastrointestinal site. A number of systems including micro and nanoparticles, lipid-based strategies and enteric capsules have significant potential either alone or in advanced combined formulations to enhance intestinal immune responses. In this review we will outline the opportunities, challenges and potential delivery solutions to facilitate the development of improved oral vaccines for infectious enteric diseases. (C) 2015 Elsevier B.V. All rights reserved.

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