Literature DB >> 9767431

Antigen detection in vivo after immunization with different presentation forms of rabies virus antigen, II. Cellular, but not humoral, systemic immune responses against rabies virus immune-stimulating complexes are macrophage dependent.

I J Claassen1, A D Osterhaus, M Poelen, N Van Rooijen, E Claassen.   

Abstract

In this paper we describe the effect of depletion of splenic macrophages on the uptake, and immune response against, different formulations of rabies virus antigen. Splenic macrophages were removed by intravenous injection with clodronate liposomes. beta-propiolacton inactivated rabies virus (RV-BPL) and immune-stimulating complexes (iscom) containing these antigens were given to macrophage-depleted and control mice. In the absence of phagocytic cells in the spleen, antigen is still trapped in the red pulp and to a lesser extent in the peri-arteriolar lymphocyte sheaths (PALS) for both antigen formulations. The localization pattern in the main area of immune response induction, namely the follicles, was unaltered after macrophage depletion. Functionally, the depletion of splenic and liver macrophages had no influence on the induction of specific antibody responses in both RV-BPL or RV-iscom immunized mice, even though the latter presentation form was clearly associated with specific localization in the marginal metallophillic macrophages. In RV-BPL immunized mice, macrophage depletion had no influence on proliferative T-cell responses. However, macrophage-depleted mice that were immunized with RV-iscom showed a significant decrease in proliferative T-cell responses. These results confirm existing ideas on the spleen as a physical filter rather than an induction site for humoral responses and shed new light on the efficient role of iscoms as antigen-presenting moieties in relation to their specific in vivo localization patterns and partial macrophage dependency.

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Year:  1998        PMID: 9767431      PMCID: PMC1364221          DOI: 10.1046/j.1365-2567.1998.00539.x

Source DB:  PubMed          Journal:  Immunology        ISSN: 0019-2805            Impact factor:   7.397


  23 in total

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5.  Repopulation of macrophages in popliteal lymph nodes of mice after liposome-mediated depletion.

Authors:  F G Delemarre; N Kors; G Kraal; N van Rooijen
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6.  Complement-mediated follicular localization of T-independent type-2 antigens: the role of marginal zone macrophages revisited.

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Authors:  B Morein; B Sundquist; S Höglund; K Dalsgaard; A Osterhaus
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8.  The effect of elimination of macrophages on the tissue distribution of liposomes containing [3H]methotrexate.

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Review 6.  Distinct Immunologic Properties of Soluble Versus Particulate Antigens.

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