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This volume is focused on the development of vaccines which
generate immune effectors capable of blocking mucosal entry or
peripheral pathogen spread. A critical first step in the design of
mucosal vaccines is the selection of administration route. Not all
mucosal immunization routes are created equally when it comes to
eliciting immune responses in multiple body compartments. This
subject and situations when a mucosal route may not be required for
vaccine delivery are reviewed here with an emphasis on the
sublingual immunization route, which may offer a safer alternative
to the nasal route for induction of broadly disseminated immune
responses. External host defenses that inhibit entry of
microorganisms at mucosal surfaces also pose obstacles to the
efficient internalization of mucosally-applied vaccines.
Transcutaneous immunization with appropriate adjuvants and
permeation enhancers can induce mucosal immune responses and may be
advantageous for bypassing these luminal barriers. Other chapters
describe strategies for enhancing uptake of mucosal vaccines, for
instance through targeted delivery to antigen-sampling M cells,
construction of virus-like particles which mimic natural pathogens,
addition of mucoadhesives or formulation as nanoparticles. Topics
include edible vaccines as well as plant-based production of
subunit or particulate vaccines that could be administered by any
route. Dry powder vaccines that could be insufflated or directly
applied to mucosal surfaces may be particularly ideal for mass
vaccination in developing countries. The manufacture, stability and
efficacy of powder formulations is comprehensively reviewed. We
conclude with chapters on two of the greatest challenges facing
mucosal vaccine development: human immunodeficiency virus and
bioterrorist agents. This monograph highlights progress and
information that should prove invaluable for the development of
contemporary vaccines that prevent infection by these and other
mucosal pathogens.
This volume is focused on the development of vaccines which
generate immune effectors capable of blocking mucosal entry or
peripheral pathogen spread. A critical first step in the design of
mucosal vaccines is the selection of administration route. Not all
mucosal immunization routes are created equally when it comes to
eliciting immune responses in multiple body compartments. This
subject and situations when a mucosal route may not be required for
vaccine delivery are reviewed here with an emphasis on the
sublingual immunization route, which may offer a safer alternative
to the nasal route for induction of broadly disseminated immune
responses. External host defenses that inhibit entry of
microorganisms at mucosal surfaces also pose obstacles to the
efficient internalization of mucosally-applied vaccines.
Transcutaneous immunization with appropriate adjuvants and
permeation enhancers can induce mucosal immune responses and may be
advantageous for bypassing these luminal barriers. Other chapters
describe strategies for enhancing uptake of mucosal vaccines, for
instance through targeted delivery to antigen-sampling M cells,
construction of virus-like particles which mimic natural pathogens,
addition of mucoadhesives or formulation as nanoparticles. Topics
include edible vaccines as well as plant-based production of
subunit or particulate vaccines that could be administered by any
route. Dry powder vaccines that could be insufflated or directly
applied to mucosal surfaces may be particularly ideal for mass
vaccination in developing countries. The manufacture, stability and
efficacy of powder formulations is comprehensively reviewed. We
conclude with chapters on two of the greatest challenges facing
mucosal vaccine development: human immunodeficiency virus and
bioterrorist agents. This monograph highlights progress and
information that should prove invaluable for the development of
contemporary vaccines that prevent infection by these and other
mucosal pathogens.
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