Literature DB >> 15664917

Closely related mycobacterial strains demonstrate contrasting levels of efficacy as antitumor vaccines and are processed for major histocompatibility complex class I presentation by multiple routes in dendritic cells.

Eleanor J Cheadle1, Dearbhaile O'Donnell, Peter J Selby, Andrew M Jackson.   

Abstract

Mycobacteria expressing recombinant antigens are already being developed as vaccines against both infections and tumors. Little is known about how dendritic cells might process such antigens. Two different mycobacterial species, the fast-growing Mycobacterium smegmatis and the slow-growing M. bovis M. bovis BCG, were engineered to express a model tumor antigen, the K(b)-restricted dominant cytotoxic T-lymphocyte epitope OVA(257-264). Recombinant M. bovis BCG but not recombinant M. smegmatis conferred protection to mice challenged with the B16-OVA tumor cell line. We went on to investigate whether the contrast in antitumor efficacy could be due to differences in how dendritic cells process antigen from the two mycobacterial strains for class I presentation. Both strains of mycobacteria caused phenotypic maturation of dendritic cells, but recombinant M. smegmatis infection led to a greater degree of dendritic cell maturation than recombinant M. bovis BCG infection. Antigen from recombinant M. smegmatis was processed and presented as OVA(257-264) on K(b) molecules by the dendritic cell line DC2.4 but not by bone marrow-derived dendritic cells (BMDC) or splenic dendritic cells. In contrast, antigen from recombinant M. bovis BCG was presented by all three dendritic cell types as long as the mycobacteria were viable. Such presentation was dependent on proteasome function and nascent major histocompatibility complex (MHC) class I molecules in DC2.4 cells but independent of the proteasome and transporter associated with antigen processings (TAP) in BMDC and splenic dendritic cells. These data demonstrate for the first time that antigen vectored by the slow-growing M. bovis BCG but not that vectored by fast-growing, readily destroyed M. smegmatis is processed and presented on MHC class I by in vitro-generated dendritic cells, which has implications for recombinant microbial vaccine development.

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Year:  2005        PMID: 15664917      PMCID: PMC546964          DOI: 10.1128/IAI.73.2.784-794.2005

Source DB:  PubMed          Journal:  Infect Immun        ISSN: 0019-9567            Impact factor:   3.441


  55 in total

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Journal:  Eur J Immunol       Date:  2000-12       Impact factor: 5.532

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5.  Electroporation of mycobacteria.

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Journal:  Methods Mol Biol       Date:  1998

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Authors:  M Svensson; B Stockinger; M J Wick
Journal:  J Immunol       Date:  1997-05-01       Impact factor: 5.422

7.  Major histocompatibility complex class I presentation of ovalbumin peptide 257-264 from exogenous sources: protein context influences the degree of TAP-independent presentation.

Authors:  M J Wick; J D Pfeifer
Journal:  Eur J Immunol       Date:  1996-11       Impact factor: 5.532

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Authors:  A J Crowle; R Dahl; E Ross; M H May
Journal:  Infect Immun       Date:  1991-05       Impact factor: 3.441

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10.  Effects of cytokines on mycobacterial phagosome maturation.

Authors:  L E Via; R A Fratti; M McFalone; E Pagan-Ramos; D Deretic; V Deretic
Journal:  J Cell Sci       Date:  1998-04       Impact factor: 5.285
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Authors:  Paul Hatfield; Alison E Merrick; Emma West; Dearbhaile O'Donnell; Peter Selby; Richard Vile; Alan A Melcher
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4.  Rapid memory CD8+ T-lymphocyte induction through priming with recombinant Mycobacterium smegmatis.

Authors:  Avi-Hai Hovav; Mark J Cayabyab; Michael W Panas; Sampa Santra; John Greenland; Ralf Geiben; Barton F Haynes; William R Jacobs; Norman L Letvin
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5.  Enhanced priming of adaptive immunity by Mycobacterium smegmatis mutants with high-level protein secretion.

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6.  Anti-tuberculosis immunity induced in mice by vaccination with Mycobacterium smegmatis over-expressing Antigen 85B is due to the increased influx of IFNgamma-positive CD4 T cells into the lungs.

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7.  Activation of anti-tumor immune response and reduction of regulatory T cells with Mycobacterium indicus pranii (MIP) therapy in tumor bearing mice.

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9.  Prime-boost with Mycobacterium smegmatis recombinant vaccine improves protection in mice infected with Mycobacterium tuberculosis.

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10.  Evaluation of specific humoral immune response and cross reactivity against Mycobacterium tuberculosis antigens induced in mice immunized with liposomes composed of total lipids extracted from Mycobacterium smegmatis.

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Journal:  BMC Immunol       Date:  2013-02-25       Impact factor: 3.615
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