Literature DB >> 27183642

Immunodominant West Nile Virus T Cell Epitopes Are Fewer in Number and Fashionably Late.

Saghar Kaabinejadian1, Curtis P McMurtrey1, Sojung Kim2, Rinki Jain3, Wilfried Bardet1, Fredda B Schafer1, Jason L Davenport4, Aaron D Martin4, Michael S Diamond5, Jon A Weidanz3, Ted H Hansen2, William H Hildebrand6.   

Abstract

Class I HLA molecules mark infected cells for immune targeting by presenting pathogen-encoded peptides on the cell surface. Characterization of viral peptides unique to infected cells is important for understanding CD8(+) T cell responses and for the development of T cell-based immunotherapies. Having previously reported a series of West Nile virus (WNV) epitopes that are naturally presented by HLA-A*02:01, in this study we generated TCR mimic (TCRm) mAbs to three of these peptide/HLA complexes-the immunodominant SVG9 (E protein), the subdominant SLF9 (NS4B protein), and the immunorecessive YTM9 (NS3 protein)-and used these TCRm mAbs to stain WNV-infected cell lines and primary APCs. TCRm staining of WNV-infected cells demonstrated that the immunorecessive YTM9 appeared several hours earlier and at 5- to 10-fold greater density than the more immunogenic SLF9 and SVG9 ligands, respectively. Moreover, staining following inhibition of the TAP demonstrated that all three viral ligands were presented in a TAP-dependent manner despite originating from different cellular compartments. To our knowledge, this study represents the first use of TCRm mAbs to define the kinetics and magnitude of HLA presentation for a series of epitopes encoded by one virus, and the results depict a pattern whereby individual epitopes differ considerably in abundance and availability. The observations that immunodominant ligands can be found at lower levels and at later time points after infection suggest that a reevaluation of the factors that combine to shape T cell reactivity may be warranted.
Copyright © 2016 by The American Association of Immunologists, Inc.

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Year:  2016        PMID: 27183642      PMCID: PMC4874531          DOI: 10.4049/jimmunol.1501821

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  63 in total

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4.  West Nile Virus Vaccine Design by T Cell Epitope Selection: In Silico Analysis of Conservation, Functional Cross-Reactivity with the Human Genome, and Population Coverage.

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5.  Single-cell RNA transcriptome analysis of CNS immune cells reveals CXCL16/CXCR6 as maintenance factors for tissue-resident T cells that drive synapse elimination.

Authors:  Sarah F Rosen; Allison L Soung; Wei Yang; Shenjian Ai; Marlene Kanmogne; Veronica A Davé; Maxim Artyomov; Jeffrey A Magee; Robyn S Klein
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