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Mucosal adjuvants and anti-infection and anti-immunopathology vaccines based on cholera toxin, cholera toxin B subunit and CpG DNA
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2005 (English)In: Immunology Letters, ISSN 0165-2478, E-ISSN 1879-0542, Vol. 97, no 2 SPEC. ISS., p. 181-188Article in journal (Refereed) Published
Abstract [en]

Mucosal immunisation may be used both to protect the mucosal surfaces against infections and as a means for immunological treatment of peripheral immunopathological disorders through the induction of systemic antigen-specific tolerance ('oral tolerance'). The development of mucosal vaccines, whether for prevention of infectious diseases or for oral tolerance immunotherapy, requires efficient antigen delivery and adjuvant systems that can help to present the appropriate vaccine or immunotherapy antigens to the mucosal immune system. The most potent (but also toxic) mucosal adjuvants are cholera toxin (CT) and the closely related Escherichia coli heat-labile enterotoxin (LT), and much effort and significant progress have been made recently to generate toxicologically acceptable derivatives of these toxins with retained adjuvant activity. Among these are the non-toxic, recombinantly produced cholera toxin B-subunit (CTB). CTB is a specific protective antigen component of a widely registered oral cholera vaccine as well as a promising vector for either giving rise to mucosal anti-infective immunity or for inducing peripheral anti-inflammatory tolerance to chemically or genetically linked foreign antigens administered mucosally. CT and CTB have also recently been used as combined vectors and adjuvants for markedly promoting ex vivo dendritic cell (DC) vaccination with different antigens and also steering the immune response to the in vivo-reinfused DCs towards either broad Th1 + Th2 + CTL immunity (CT) or Th2 or tolerance (CTB). Another type of mucosal adjuvants is represented by bacterial DNA or synthetic oligodeoxynucleotides containing CpG-motifs, which especially when linked to CTB have been found to effectively stimulate both innate and adaptive mucosal immune responses. The properties and clinical potential of these different classes of adjuvants are being discussed. © 2004 Elsevier B.V. All rights reserved.

Place, publisher, year, edition, pages
Elsevier , 2005. Vol. 97, no 2 SPEC. ISS., p. 181-188
Keywords [en]
Anti-immunopathology, Anti-infection, Mucosal adjuvants, antigen, bacterial DNA, BCG vaccine, cancer antibody, cholera b subunit whole cell cholera vaccine, cholera toxin, cholera toxin a subunit, cholera toxin B subunit, cholera vaccine, CpG DNA, dendritic cell vaccine, enterotoxin, immunostimulating agent, immunosuppressive agent, influenza vaccine, ISCOM, oligodeoxynucleotide derivative, peptide derivative, tetanus toxin, unclassified drug, virus vector, adjuvant therapy, allergic reaction, antigen specificity, autoimmune disease, bacterial infection, Behcet disease, cholera, conference paper, dendritic cell, drug delivery system, drug safety, drug tolerability, Escherichia coli, ex vivo study, genital system, human, Human immunodeficiency virus infection, immune response, immune system, immunization, immunopathogenesis, immunopathology, immunotherapy, in vivo study, infection, influenza, influenza vaccination, innate immunity, mucosal immunity, nonhuman, priority journal, protein motif, side effect, Th1 cell, Th2 cell, tumor, uveitis, vaccination, virus infection
National Category
Natural Sciences
Identifiers
URN: urn:nbn:se:ri:diva-56884DOI: 10.1016/j.imlet.2004.11.009Scopus ID: 2-s2.0-20044365044OAI: oai:DiVA.org:ri-56884DiVA, id: diva2:1612573
Available from: 2021-11-18 Created: 2021-11-18 Last updated: 2021-11-18Bibliographically approved

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Nygren, Erik

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