In vivo cross-priming of MHC class I-restricted antigens requires the TAP transporter

Alex Y.C. Huang; Allen T. Bruce; Drew M. Pardoll; Hyam I. Levitsky

doi:10.1016/S1074-7613(00)80248-4

In vivo cross-priming of MHC class I-restricted antigens requires the TAP transporter

Alex Y.C. Huang, Allen T. Bruce, Drew M. Pardoll, Hyam I. Levitsky

School of Medicine

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

190 Scopus citations

Abstract

Recent in vitro evidence suggests two alternative mechanisms by which bone marrow-derived APCs may process exogenous antigens for presentation to CTL in vivo, a phenomenon termed cross-priming. Although in vitro studies have suggested that both TAP-dependent and TAP-independent pathways exist, we have now demonstrated an absolute requirement for a functional TAP for cross-priming to occur in vivo. Bone marrow chimeras reconstituted with marrow from TAP-defective donors develop functional CD8⁺ CTL, but have APCs with disrupted TAP function. In such chimeras, in vivo priming of naive CTL was observed when antigen was targeted to the ER in a TAP-independent fashion, but cross-priming could not be demonstrated. These results support the TAP-dependent mechanism of cross-priming.

Original language	English (US)
Pages (from-to)	349-355
Number of pages	7
Journal	Immunity
Volume	4
Issue number	4
DOIs	https://doi.org/10.1016/S1074-7613(00)80248-4
State	Published - Apr 1996

ASJC Scopus subject areas

Immunology and Allergy
Immunology
Infectious Diseases

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title = "In vivo cross-priming of MHC class I-restricted antigens requires the TAP transporter",

abstract = "Recent in vitro evidence suggests two alternative mechanisms by which bone marrow-derived APCs may process exogenous antigens for presentation to CTL in vivo, a phenomenon termed cross-priming. Although in vitro studies have suggested that both TAP-dependent and TAP-independent pathways exist, we have now demonstrated an absolute requirement for a functional TAP for cross-priming to occur in vivo. Bone marrow chimeras reconstituted with marrow from TAP-defective donors develop functional CD8+ CTL, but have APCs with disrupted TAP function. In such chimeras, in vivo priming of naive CTL was observed when antigen was targeted to the ER in a TAP-independent fashion, but cross-priming could not be demonstrated. These results support the TAP-dependent mechanism of cross-priming.",

author = "Huang, {Alex Y.C.} and Bruce, {Allen T.} and Pardoll, {Drew M.} and Levitsky, {Hyam I.}",

note = "Funding Information: The authors wish to thank J. Yewdell, J. Bennink, N. Restifo, L. Van Kaer, and J. Schneck for providing valuable reagents, E. Fuchs for helpful discussions, and L. Van Kaer and T.-C. Wu for critical review of the manuscript. This work was supported by the National Institutes of Health grant 1RO1A137273.",

year = "1996",

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doi = "10.1016/S1074-7613(00)80248-4",

language = "English (US)",

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journal = "Immunity",

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AU - Huang, Alex Y.C.

AU - Bruce, Allen T.

AU - Pardoll, Drew M.

AU - Levitsky, Hyam I.

N1 - Funding Information: The authors wish to thank J. Yewdell, J. Bennink, N. Restifo, L. Van Kaer, and J. Schneck for providing valuable reagents, E. Fuchs for helpful discussions, and L. Van Kaer and T.-C. Wu for critical review of the manuscript. This work was supported by the National Institutes of Health grant 1RO1A137273.

PY - 1996/4

Y1 - 1996/4

N2 - Recent in vitro evidence suggests two alternative mechanisms by which bone marrow-derived APCs may process exogenous antigens for presentation to CTL in vivo, a phenomenon termed cross-priming. Although in vitro studies have suggested that both TAP-dependent and TAP-independent pathways exist, we have now demonstrated an absolute requirement for a functional TAP for cross-priming to occur in vivo. Bone marrow chimeras reconstituted with marrow from TAP-defective donors develop functional CD8+ CTL, but have APCs with disrupted TAP function. In such chimeras, in vivo priming of naive CTL was observed when antigen was targeted to the ER in a TAP-independent fashion, but cross-priming could not be demonstrated. These results support the TAP-dependent mechanism of cross-priming.

AB - Recent in vitro evidence suggests two alternative mechanisms by which bone marrow-derived APCs may process exogenous antigens for presentation to CTL in vivo, a phenomenon termed cross-priming. Although in vitro studies have suggested that both TAP-dependent and TAP-independent pathways exist, we have now demonstrated an absolute requirement for a functional TAP for cross-priming to occur in vivo. Bone marrow chimeras reconstituted with marrow from TAP-defective donors develop functional CD8+ CTL, but have APCs with disrupted TAP function. In such chimeras, in vivo priming of naive CTL was observed when antigen was targeted to the ER in a TAP-independent fashion, but cross-priming could not be demonstrated. These results support the TAP-dependent mechanism of cross-priming.

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ER -

In vivo cross-priming of MHC class I-restricted antigens requires the TAP transporter

Abstract

ASJC Scopus subject areas

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