Sequential Cleavage by Metallopeptidases and Proteasomes Is Involved in Processing HIV-1 ENV Epitope for Endogenous MHC Class I Antigen Presentation

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Sequential Cleavage by Metallopeptidases and Proteasomes Is Involved in Processing HIV-1 ENV Epitope for Endogenous MHC Class I Antigen Presentation¹

Daniel López^*, Beatriz C. Gil-Torregrosa²^,*, Cornelia Bergmann and Margarita Del Val³^,*

^* Centro Nacional de Biología Fundamental, Instituto de Salud Carlos III, Madrid, Spain; and Departments of Neurology and Microbiology, University of Southern California School of Medicine, Los Angeles, CA 90033

Antigenic peptides derived from viral proteins by multiple proteolyticcleavages are bound by MHC class I molecules and recognized byCTL. Processing predominantly takes place in the cytosol ofinfected cells by the action of proteasomes. To identify otherproteases involved in the endogenous generation of viral epitopes,specifically those derived from proteins routed to the secretorypathway, we investigated presentation of the HIV-1 ENV 10-merepitope ³¹⁸RGPGRAFVTI³²⁷ (p18) to specific CTL in the presenceof diverse protease inhibitors. Both metalloproteinase and proteasomeinhibitors decreased CTL recognition of the p18 epitope expressedfrom either native gp160 or from a chimera based on the hepatitisB virus secretory core protein as carrier protein. Processing ofthis epitope from both native ENV and the hepatitis B virus secretorycore chimeric protein appeared to proceed by a TAP-dependent pathwaythat involved sequential cleavage by proteasomes and metallo-endopeptidases;however, other protease activities could replace the functionof the lactacystin-sensitive proteasomes. By contrast, in asecond TAP-independent pathway we detected no contribution ofmetallopeptidases for processing the ENV epitope from the chimericprotein. These results show that, in the classical TAP-dependentMHC class I pathway, endogenous Ag processing of viral proteinsto yield the p18 10-mer epitope requires metallo-endopeptidasesin addition to proteasomes.

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Sequential Cleavage by Metallopeptidases and Proteasomes Is Involved in Processing HIV-1 ENV Epitope for Endogenous MHC Class I Antigen Presentation1

Sequential Cleavage by Metallopeptidases and Proteasomes Is Involved in Processing HIV-1 ENV Epitope for Endogenous MHC Class I Antigen Presentation¹