CD4-independent in vivo priming of murine CTL by optimal MHC class I-restricted peptides derived from intracellular pathogens

Rubendra Dyall; Ljiljana V. Vasović; Alberto Molano; Janko Nikolić-žugić

doi:10.1093/intimm/7.8.1205

CD4-independent in vivo priming of murine CTL by optimal MHC class I-restricted peptides derived from intracellular pathogens

Rubendra Dyall, Ljiljana V. Vasović, Alberto Molano, Janko Nikolić-žugić

Research output: Contribution to journal › Article › peer-review

42 Scopus citations

Abstract

CTL combat intracellular pathogens by killing infected cells. The molecular targets of their attack are foreign peptides bound to self MHC encoded class I molecules. Immunization of mice with peptides containing CTL determinants was shown to elicit CD4-dependent CTL. Here, we have achieved in vivo CTL priming with naturally processed 8-10 amino acid long class I-restricted peptides emulsified in an adjuvant. A potent, reproducible and physiologically relevant response was obtained using peptides from an intracellular bacterium and five viruses (including HIV) in two murine MHC haplotypes. This method is suitable for multiple vaccination, since a 'cocktail' of peptides derived from three pathogens elicited effector CTL against each pathogen. Most importantly, peptide-induced CD8⁺CD4^- CTL were CD4⁺-independent These results have implications for CTL induction in situations where CD4 T cells are depleted or compromised, as is the case n HIV infection

Original language	English (US)
Pages (from-to)	1205-1212
Number of pages	8
Journal	International Immunology
Volume	7
Issue number	8
DOIs	https://doi.org/10.1093/intimm/7.8.1205
State	Published - Aug 1995
Externally published	Yes

Keywords

CD4
CTL
Peptide
Vaccine

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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10.1093/intimm/7.8.1205

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title = "CD4-independent in vivo priming of murine CTL by optimal MHC class I-restricted peptides derived from intracellular pathogens",

abstract = "CTL combat intracellular pathogens by killing infected cells. The molecular targets of their attack are foreign peptides bound to self MHC encoded class I molecules. Immunization of mice with peptides containing CTL determinants was shown to elicit CD4-dependent CTL. Here, we have achieved in vivo CTL priming with naturally processed 8-10 amino acid long class I-restricted peptides emulsified in an adjuvant. A potent, reproducible and physiologically relevant response was obtained using peptides from an intracellular bacterium and five viruses (including HIV) in two murine MHC haplotypes. This method is suitable for multiple vaccination, since a 'cocktail' of peptides derived from three pathogens elicited effector CTL against each pathogen. Most importantly, peptide-induced CD8+CD4- CTL were CD4+-independent These results have implications for CTL induction in situations where CD4 T cells are depleted or compromised, as is the case n HIV infection",

keywords = "CD4, CTL, Peptide, Vaccine",

author = "Rubendra Dyall and Vasovi{\'c}, {Ljiljana V.} and Alberto Molano and Janko Nikoli{\'c}-{\v z}ugi{\'c}",

note = "Funding Information: We wish to thank Drs M. J. Bevan, S. Jameson, B. B. Knowtes, J. G. Michael, E. Pamer, J. vasilakos and S. Silverstein for their generous donation of cell lines, peptides and viruses; the MSKCC Microchemistry Core Facility for peptide synthesis; and Ms D. Nikolic-Zugi6 for flow cytometry. This work was supported in part by the Pew Charitable Trust (J. N.-Z. is a PEW Scholar), the NIH NCI Cancer Center Support Grant CA-08748, the African-American Institute (R. D.) and the Michael and Ethel Cohen Fellowship Fund (L. V. V. is a Dana Fellow).",

year = "1995",

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doi = "10.1093/intimm/7.8.1205",

language = "English (US)",

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AU - Dyall, Rubendra

AU - Vasović, Ljiljana V.

AU - Molano, Alberto

AU - Nikolić-žugić, Janko

N1 - Funding Information: We wish to thank Drs M. J. Bevan, S. Jameson, B. B. Knowtes, J. G. Michael, E. Pamer, J. vasilakos and S. Silverstein for their generous donation of cell lines, peptides and viruses; the MSKCC Microchemistry Core Facility for peptide synthesis; and Ms D. Nikolic-Zugi6 for flow cytometry. This work was supported in part by the Pew Charitable Trust (J. N.-Z. is a PEW Scholar), the NIH NCI Cancer Center Support Grant CA-08748, the African-American Institute (R. D.) and the Michael and Ethel Cohen Fellowship Fund (L. V. V. is a Dana Fellow).

PY - 1995/8

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N2 - CTL combat intracellular pathogens by killing infected cells. The molecular targets of their attack are foreign peptides bound to self MHC encoded class I molecules. Immunization of mice with peptides containing CTL determinants was shown to elicit CD4-dependent CTL. Here, we have achieved in vivo CTL priming with naturally processed 8-10 amino acid long class I-restricted peptides emulsified in an adjuvant. A potent, reproducible and physiologically relevant response was obtained using peptides from an intracellular bacterium and five viruses (including HIV) in two murine MHC haplotypes. This method is suitable for multiple vaccination, since a 'cocktail' of peptides derived from three pathogens elicited effector CTL against each pathogen. Most importantly, peptide-induced CD8+CD4- CTL were CD4+-independent These results have implications for CTL induction in situations where CD4 T cells are depleted or compromised, as is the case n HIV infection

AB - CTL combat intracellular pathogens by killing infected cells. The molecular targets of their attack are foreign peptides bound to self MHC encoded class I molecules. Immunization of mice with peptides containing CTL determinants was shown to elicit CD4-dependent CTL. Here, we have achieved in vivo CTL priming with naturally processed 8-10 amino acid long class I-restricted peptides emulsified in an adjuvant. A potent, reproducible and physiologically relevant response was obtained using peptides from an intracellular bacterium and five viruses (including HIV) in two murine MHC haplotypes. This method is suitable for multiple vaccination, since a 'cocktail' of peptides derived from three pathogens elicited effector CTL against each pathogen. Most importantly, peptide-induced CD8+CD4- CTL were CD4+-independent These results have implications for CTL induction in situations where CD4 T cells are depleted or compromised, as is the case n HIV infection

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CD4-independent in vivo priming of murine CTL by optimal MHC class I-restricted peptides derived from intracellular pathogens

Abstract

Keywords

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