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Defining the directionality and quality of influenza virus–specific CD8+ T cell cross-reactivity in individuals infected with hepatitis C virus
Victoria Kasprowicz, … , Georg M. Lauer, Paul Klenerman
Victoria Kasprowicz, … , Georg M. Lauer, Paul Klenerman
Published February 1, 2008
Citation Information: J Clin Invest. 2008;118(3):1143-1153. https://doi.org/10.1172/JCI33082.
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Research Article Immunology Article has an altmetric score of 3

Defining the directionality and quality of influenza virus–specific CD8+ T cell cross-reactivity in individuals infected with hepatitis C virus

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Abstract

Cross-reactivity of murine and recently human CD8+ T cells between different viral peptides, i.e., heterologous immunity, has been well characterized. However, the directionality and quality of these cross-reactions is critical in determining their biological importance. Herein we analyzed the response of human CD8+ T cells that recognize both a hepatitis C virus peptide (HCV-NS3) and a peptide derived from the influenza neuraminidase protein (Flu-NA). To detect the cross-reactive CD8+ T cells, we used peptide-MHC class I complexes (pMHCs) containing a new mutant form of MHC class I able to bind CD8 more strongly than normal MHC class I complexes. T cell responses against HCV-NS3 and Flu-NA peptide were undetectable in normal donors. In contrast, some responses against the Flu-NA peptide were identified in HCV+ donors who showed strong HCV-NS3–specific reactivity. The Flu-NA peptide was a weak agonist for CD8+ T cells in HCV+ individuals on the basis of novel pMHCs and functional assays. These data support the idea of cross-reactivity between the 2 peptides, but indicate that reactivity toward the Flu-NA peptide is highly CD8-dependent and occurs predominantly after priming during HCV infection. Our findings indicate the utility of the novel pMHCs in dissecting cross-reactivity and suggest that cross-reactivity between HCV and influenza is relatively weak. Further studies are needed to relate affinity and functionality of cross-reactive T cells.

Authors

Victoria Kasprowicz, Scott M. Ward, Alison Turner, Alexandros Grammatikos, Brian E. Nolan, Lia Lewis-Ximenez, Charles Sharp, Jenny Woodruff, Vicki M. Fleming, Stuart Sims, Bruce D. Walker, Andrew K. Sewell, Georg M. Lauer, Paul Klenerman

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Figure 1

Staining for HCV-NS3 responses and Flu-NA responses in healthy donors.

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Staining for HCV-NS3 responses and Flu-NA responses in healthy donors.
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Representative density plots of ex vivo pMHC staining (left), ex vivo MHC Class I pMHC and magnetic bead enrichment (middle), and in vitro peptide restimulation of PBMCs followed by pMHC staining (right). Top row shows an individual with positive Flu matrix responses, and the bottom row shows the equivalent result with Flu-NA. The frequency of the pMHC-positive cells in the CD8+ population is shown in the top right portion of each plot.

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