J-LEAPS vaccines initiate murine Th1 responses by activating dendritic cells

Abstract The Ligand Epitope Antigen Presentation System (LEAPS) converts a peptide containing a T cell epitope as small as 8 amino acids into an immunogen and directs the nature of the subsequent response. Tandem synthesis of the J peptide (a peptide from the beta-2-microglobulin) with peptides of 1...

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Bibliographic Details
Published in:Vaccine 2010-08, Vol.28 (34), p.5533-5542
Main Authors: Taylor, P.R, Koski, G.K, Paustian, C.C, Bailey, E, Cohen, P.A, Moore, F.B.-G, Zimmerman, D.H, Rosenthal, K.S
Format: Article
Language:English
Subjects:
Adoptive Transfer
Allergy and Immunology
Amino acids
Animals
Antigen Presentation
Applied microbiology
Binding sites
Biological and medical sciences
Bone marrow
Cells, Cultured
Dendritic cells
Dendritic Cells - immunology
Epitopes, T-Lymphocyte - immunology
Female
Fundamental and applied biological sciences. Psychology
gag Gene Products, Human Immunodeficiency Virus - immunology
Herpes Simplex - immunology
Herpes Simplex - prevention & control
Herpes simplex virus 1
Herpesvirus 1, Human - immunology
HIV
HSV
Human immunodeficiency virus
IL12
Immune system
Immunization
Interferon-gamma - immunology
Interleukin-12 - immunology
LEAPS
Ligands
Lymphocytes
Mice
Mice, Inbred A
Mice, Inbred C57BL
Microbiology
Miscellaneous
Peptides
Proteins
Studies
T cell receptors
Th1
Th1 Cells - immunology
Vaccines
Vaccines, antisera, therapeutical immunoglobulins and monoclonal antibodies (general aspects)
Viral Envelope Proteins - immunology
Viral Vaccines - immunology
Virology
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Summary:Abstract The Ligand Epitope Antigen Presentation System (LEAPS) converts a peptide containing a T cell epitope as small as 8 amino acids into an immunogen and directs the nature of the subsequent response. Tandem synthesis of the J peptide (a peptide from the beta-2-microglobulin) with peptides of 15 or 30 amino acids from HSV-1 or HIV made them immunogenic and promoted Th1 immune responses. Immunization of A/J or C57BL/6 mice with J-LEAPS heteroconjugates containing an epitope from the HSV-1 glycoprotein D (JgD) or an epitope from the HIV gag protein (JH) emulsified with Seppic ISA51 induced increased levels of IL-12p70 by day 3 and increased levels of interferon gamma (IFN-gamma) on days 10 and 24. Interestingly, levels of IL-10, TNF-alpha, and IL-6 did not change. Neither the H nor the gD peptides alone elicited responses and only weak responses followed immunization with the J peptide. Bone marrow (BM) cells became CD86 and CD11c positive within 48 h of treatment with JgD or JH. JH or JgD treatment promoted IL-12p70 production and expression of CD8 denoting the maturation and activation of a subclass of myeloid DCs. Pure cultures of immature myeloid DCs also responded to JgD treatment, forming clusters, developing dendrites, and producing IL-12p70 within 24 h. The JH or JgD treated bone marrow cells (JgD-DC) were necessary and sufficient to activate splenic T cells to produce IFN-gamma and the JgD-DC provided an antigen specific booster response to T cells from JgD immunized mice. Adoptive transfer of JgD-DC was also sufficient to initiate protective antigen specific immunity from lethal challenge with HSV-1. The J-LEAPS vaccines appear to act as an adjuvant and immunogen on DC precursors in a unique manner to promote activation and maturation into IL-12p70 producing DCs which then can initiate sufficient Th1 immune responses to elicit protection without production of acute phase cytokines.
ISSN:0264-410X
1873-2518
DOI:10.1016/j.vaccine.2010.06.043