Long Kim Bui scite author profile

Antigen-specific, CD8+, cytolytic T lymphocytes (CTLs) could potentially provide resistance to several infectious and malignant diseases. However, the cellular requirements for the generation of specific CTLs in human lymphocyte cultures are not well defined, and repetitive stimulation with antigen is often required. We find that strong CD8+ CTL responses to influenza virus can be generated from freshly isolated blood T cells, as long as dendritic cells are used as antigen presenting cells (APCs). Small numbers of dendritic cells (APC:T cell ratio of 1:50-1:100) induce these CTL responses from most donors in 7 d of culture, but monocytes are weak or inactive. Whereas both dendritic cells and monocytes are infected with influenza virus, the former serve as effective APCs for the induction of CD8+ T cells while the latter act as targets for the CTLs that are induced. The strong CD8+ response to influenza virus-infected dendritic cells is accompanied by extensive proliferation of the CD8+ T cells, but the response can develop in the apparent absence of CD4+ helpers or exogenous lymphokines. CD4+ influenza virus-specific CTLs can also be induced by dendritic cells, but the cultures initially must be depleted of CD8+ cells. These findings should make it possible to use dendritic cells to generate human, antigen-specific, CD8+ CTLs to other targets. The results illustrate the principle that efficient T cell-mediated responses develop in two stages: an afferent limb in which dendritic cells are specialized APCs and an efferent limb in which the primed T cells carry out an immune response to many types of presenting cells. (J. Clin. Invest. 1994. 94:797-807.)

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Inactivated influenza virus, when presented on dendritic cells, elicits human CD8+ cytolytic T cell responses.

Bender

Bui

Feldman

et al. 1995

145

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SummaryInactivated or subunit virus preparations have been excellent vaccines for inducing antibody responses . Generation of cytolytic T cell responses, however, is thought to require replicating virus, primarily to provide sufficiently large amounts of cytoplasmic proteins for processing and presentation on major histocompatibility complex class I molecules by antigen-presenting cells. Potent human CD8+ cytolytic T cell responses to live replicating influenza A virus are generated when dendritic cells are used as the antigen-presenting cells . Here, we demonstrate that dendritic cells pulsed with poorly replicating, heat-or ultraviolet-inactivated influenza virus, induce equally strong CD8 + cytolytic T lymphocyte responses. The cytotoxic T lymphocytes are generated in the apparent absence ofCD4 + helper cells or exogenous cytokines . Active viral protein synthesis is not required to charge class I molecules on dendritic cells . When pulsed with inactivated virus, G1% of dendritic cells express nonstructural protein 1, which is only synthesized in the infectious cycle. To be optimally effective, however, the inactivated virus must retain its fusogenic activity, and presumably access the cytoplasm of dendritic cells . The data indicate, therefore, that dendritic cells require only small amounts of viral protein to charge class I molecules, most likely via traditional class I processing pathways . These results reopen the potential use of inactivated virus preparations as immunogens for cytotoxic T lymphocyte responses .

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Stimulation of Human Anti-Viral CD8+ Cytolytic T Lymphocytes by Dendritic Cells

Bhardwaj

Bender

González

et al. 1995

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Long Kim Bui

Influenza virus-infected dendritic cells stimulate strong proliferative and cytolytic responses from human CD8+ T cells.

Inactivated influenza virus, when presented on dendritic cells, elicits human CD8+ cytolytic T cell responses.

Stimulation of Human Anti-Viral CD8+ Cytolytic T Lymphocytes by Dendritic Cells

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