Major Histocompatibility Complex Class II-restricted Presentation of an Internally Synthesized Antigen Displays Cell-type Variability and Segregates from the Exogenous Class II and Endogenous Class I Presentation Pathways

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 1993 Jul 1

PMID 8315396

Citations 27

Authors

G E Loss Jr

C G Elias

P E Fields

R K Ribaudo

M McKisic

A J Sant

Affiliations

Soon will be listed here.

Abstract

Although reported examples of endogenous antigen (Ag) presentation by major histocompatibility complex (MHC) class II molecules have increased, the mechanisms governing this process remain poorly defined. In this communication, we describe an experimental system designed to examine the mechanisms governing class II presentation of internal Ag. Our target peptide is processed from a transmembrane protein constitutively expressed by a variety of nucleated cells (MHC class I, H-2Ld), is naturally displayed by MHC class II molecules in vivo, and is recognized by a class II-restricted, CD4+ T cell hybridoma. Our results indicate that presentation of the Ld target Ag is independent of its plasma membrane expression, may not involve endosomal proteolysis, and thus may be distinct from the classically defined class II presentation pathway. In addition, the observations that Ld presentation does not require a functional TAP-1 complex, is not blocked by invariant chain, and cannot utilize cytoplasmic forms of H-2Ld, suggest that a classical class I pathway is not involved in this presentation event. Finally, our data suggest that different cofactors participate in MHC class II presentation of exogenous and endogenous Ag, and that disparate Ag presenting cells, such as B, T, and pancreatic islet cells, may differentially express these two class II pathways of Ag presentation.

Citing Articles

Toward a Network Model of MHC Class II-Restricted Antigen Processing.

Miller M, Ganesan A, Eisenlohr L Front Immunol. 2014; 4:464.

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Sculpting MHC class II-restricted self and non-self peptidome by the class I Ag-processing machinery and its impact on Th-cell responses.

Spencer C, Dragovic S, Conant S, Gray J, Zheng M, Samir P Eur J Immunol. 2013; 43(5):1162-72.

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The utility and limitations of current Web-available algorithms to predict peptides recognized by CD4 T cells in response to pathogen infection.

Chaves F, Lee A, Nayak J, Richards K, Sant A J Immunol. 2012; 188(9):4235-48.

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Beyond the classical: influenza virus and the elucidation of alternative MHC class II-restricted antigen processing pathways.

Eisenlohr L, Luckashenak N, Apcher S, Miller M, Sinnathamby G Immunol Res. 2011; 51(2-3):237-48.

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Dragovic S, Hill T, Christianson G, Kim S, Elliott T, Scott D J Immunol. 2011; 186(12):6683-92.

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