Narrowed TCR repertoire and viral escape as a consequence of heterologous immunity
Markus Cornberg, … , Raymond M. Welsh, Liisa K. Selin
Markus Cornberg, … , Raymond M. Welsh, Liisa K. Selin
Published May 1, 2006
Citation Information: J Clin Invest. 2006;116(5):1443-1456. https://doi.org/10.1172/JCI27804.
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Narrowed TCR repertoire and viral escape as a consequence of heterologous immunity

Abstract

Why some virus-specific CD8 TCR repertoires are diverse and others restricted or “oligoclonal” has been unknown. We show here that oligoclonality and extreme clonal dominance can be a consequence of T cell cross-reactivity. Lymphocytic choriomeningitis virus (LCMV) and Pichinde virus (PV) encode NP205–212 epitopes that induce different but highly cross-reactive diverse TCR repertoires. Homologous viral challenge of immune mice only slightly skewed the repertoire and enriched for predictable TCR motifs. However, heterologous viral challenge resulted in a narrow oligoclonal repertoire with dominant clones with unpredictable TCR sequences. This shift in clonal dominance varied with the private, i.e., unique, specificity of the host’s TCR repertoire and was simulated using affinity-based computer models. The skewing differences in TCR repertoire following homologous versus heterologous challenge were observed within the same private immune system in mice adoptively reconstituted with memory CD8 T cell pools from the same donor. Conditions driving oligoclonality resulted in an LCMV epitope escape variant in vivo resembling the natural Lassa virus sequence. Thus, T cell oligoclonality, including extremes in clonal dominance, may be a consequence of heterologous immunity and lead to viral escape. This has implications for the design of peptide-based vaccines, which might unintentionally prime for skewed TCR responses to cross-reactive epitopes.

Authors

Markus Cornberg, Alex T. Chen, Lee A. Wilkinson, Michael A. Brehm, Sung-Kwon Kim, Claudia Calcagno, Dario Ghersi, Roberto Puzone, Franco Celada, Raymond M. Welsh, Liisa K. Selin

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Figure 4

Narrowing of the private LCMV NP205 –specific CD8 T cell Vβ repertoire after heterologous PV infection.

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Narrowing of the private LCMV NP205 ...
(A) PBMCs were isolated from 10 LCMV-immune mice (white bars), and the LCMV NP205-specific CD8 T cells were analyzed either by ICS or by tetramer staining and costaining with Vβ-specific antibodies. The same mice were infected with PV (black bars), and 8 days after infection PBMCs were isolated, and the TCR Vβ repertoire of LCMV NP205 tetramer–positive cells was analyzed. (B and C) The cross-reactive NP205-specific TCR repertoire is oligoclonal after heterologous virus infection. (B) The FACS dot plots show the dominant Vβ usage of the NP205-specific CD8 T cells from 2 representative LCMV+PV–infected mice (mouse 1 [M1] and M8). (C) The LCMV NP205–specific CD8 T cells from M1 and M8 were sorted, and the dominant Vβ family was subcloned and sequenced.