Silvia Cellini scite author profile

The proteasome is a multicatalytic proteinase complex which plays a central role in intracellular protein degradation. We report here the synthesis and biological activities of a new class of specific proteasome inhibitors selective for trypsin-like activity. These tripeptide-based compounds bearing a C-terminal vinyl ester are nontoxic, and do not affect cell proliferation, but are able to modulate the generation and presentation of immunogenic peptides presented by MHC class I molecules.

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IFN-α boosts epitope cross-presentation by dendritic cells via modulation of proteasome activity

Lattanzi

Rozera

Marescotti

et al. 2011

Immunobiology

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Identification of new HIV-1 Gag-specific cytotoxic T lymphocyte responses in BALB/c mice

Cellini

Fortini

Gallerani

et al. 2008

Virol J

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Background: As HIV-specific cytotoxic T cells play a key role during acute and chronic HIV-1 infection in humans, the ability of potential anti-HIV vaccines to elicit strong, broad T cell responses is likely to be crucial. The HIV-1 Gag antigen is widely considered a relevant antigen for the development of an anti-HIV vaccine since it is one of the most conserved viral proteins and is also known to induce T cell responses. In the majority of studies reporting Gag-specific cellular immune responses induced by Gag-based vaccines, only a small number of Gag T cell epitopes were tested in preclinical mouse models, thus giving an incomplete picture of the numerous possible cellular immune responses against this antigen. As is, this partial knowledge of epitope-specific T cell responses directed to Gag will unavoidably result in a limited preclinical evaluation of Gag-based vaccines.

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Silvia Cellini

The Tat protein broadens T cell responses directed to the HIV-1 antigens Gag and Env: Implications for the design of new vaccination strategies against AIDS

Peptidyl Vinyl Ester Derivatives: New Class of Selective Inhibitors of Proteasome Trypsin-Like Activity

IFN-α boosts epitope cross-presentation by dendritic cells via modulation of proteasome activity

Identification of new HIV-1 Gag-specific cytotoxic T lymphocyte responses in BALB/c mice

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