TCR β-Chain Sharing in Human CD8+ T Cell Responses to Cytomegalovirus and EBV

Venturi, Vanessa; Chin, Hui Yee; Asher, Tedi E.; Ladell, Kristin; Scheinberg, Phillip; Bornstein, Ethan; Bockel, David van; Kelleher, Anthony D.; Douek, Daniel C.; Price, David A.; Davenport, Miles P.

doi:10.4049/jimmunol.181.11.7853

Cited by 105 publications

(159 citation statements)

References 51 publications

(94 reference statements)

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“…The conservation of this N-encoded sequence suggested Ag-driven selection of this clonotype. Of note, two clonotypes found in response to CMV NLVPMVATV were also found by anchored RT-PCR and sequencing of subclones in previous studies (19,20). With regard to EBV-specific CD8 T cells, the same degree of clonotypic diversity was found for two epitopes (Fig.…”

Section: Cdr3 Length Distribution Analysis Of Trbv Transcripts Derivesupporting

confidence: 58%

“…In addition, it has been shown that the TCR repertoire directed against a particular CMV-derived epitope remained quite heterogeneous in healthy individuals (15). Along the same line, direct sequencing of the TCR b-chain by anchored PCR on ex vivo virus-specific sorted CD8 T cells revealed that two epitopes derived from EBV and CMV were recognized by CD8 T cells exhibiting a higher degree (seven to nine clonotypes) of clonotypic diversity (19,20) indicating that the TCR repertoire during viral response might not be as restricted as thought. The variable degree of diversity of the TCR repertoire observed during chronic virus infections might be related to the experimental strategies used in various studies.…”

mentioning

confidence: 77%

“…Conserved CDR3 residues found in the current study are highlighted in yellow. Public clonotypes found in previous studies (19,20) are shown in blue boxes.…”

Section: Cdr3 Length Distribution Analysis Of Trbv Transcripts Derivementioning

confidence: 99%

“…Many studies have analyzed the TCR repertoire in T cell lines and/or clones obtained in vitro from a limited number of subjects (21,22) and/or have been based on the use of an incomplete panel of anti-Vb mAbs (14,15,(21)(22)(23), raising the question of to what extent these data were representative of the in vivo situation. With regard to the direct sequencing of the TCR b-chain by anchored PCR in ex vivo Ag-specific sorted cells (19,20,24), it is possible that the TCR repertoire diversity might be underestimated, as the degree of diversity measured will be dependent upon the extent of sequencing with the potential for preferential detection of dominant CD8 T cell clonotypes.…”

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confidence: 99%

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Large TCR Diversity of Virus-Specific CD8 T Cells Provides the Mechanistic Basis for Massive TCR Renewal after Antigen Exposure

Miconnet

Marrau

Farina

et al. 2011

The Journal of Immunology

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Ex vivo analysis of virus-specific CD8 T cell populations by anchored PCR has shown that the CD8 TCR repertoire was less oligoclonal (seven to nine clonotypes per individual epitope) than previously thought. In the current study, TCR diversity was investigated by assessing both the overall TCR β-chain variable regions usage as well as the CDR3 regions in ex vivo-isolated CMV- and EBV-specific CD8 T cells from 27 healthy donors. The average number of clonotypes specific to most single viral epitopes comprised between 14 and 77. Changes in the CD8 TCR repertoire were also longitudinally assessed under conditions of HIV-1 chronic infection (i.e., in patients with suppressed virus replication and after treatment interruption and Ag re-exposure). The results showed that a large renewal (≤80%) of the TRB repertoire occurred after Ag re-exposure and was eventually associated with an increased T cell recognition functional avidity. These results demonstrate that the global CD8 TCR repertoire is much more diverse (≤9-fold) than previously estimated and provide the mechanistic basis for supporting massive repertoire renewal during chronic virus infection and Ag re-exposure.

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Section: Cdr3 Length Distribution Analysis Of Trbv Transcripts Derivesupporting

confidence: 58%

mentioning

confidence: 77%

“…Conserved CDR3 residues found in the current study are highlighted in yellow. Public clonotypes found in previous studies (19,20) are shown in blue boxes.…”

Section: Cdr3 Length Distribution Analysis Of Trbv Transcripts Derivementioning

confidence: 99%

mentioning

confidence: 99%

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Large TCR Diversity of Virus-Specific CD8 T Cells Provides the Mechanistic Basis for Massive TCR Renewal after Antigen Exposure

Miconnet

Marrau

Farina

et al. 2011

The Journal of Immunology

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“…Furthermore, the high representation of some V-J combinations in humans and in humanized mice suggests a similar mechanism of selection, independently of the donor genotype and/or of the immunological history of the subject. In that regard, it is striking to note that, in the few studies that describe public TCR (T-cell clones conserved in various human afflictions among different patients), most belong to highly conserved hTRBV families that we describe here (the BV19 gene for Influenza infection [24], the BV6 family for HCMV [25] and SIV [26] infections, and the BV20 gene for EBV infection [27,28]. This correlation is not restricted to viral infections since the BV4 and BV12 families are also commonly used in autoimmune anti-phospholipid syndrome [29]).…”

Section: Discussionmentioning

confidence: 91%

Half of the T‐cell repertoire combinatorial diversity is genetically determined in humans and humanized mice

Pham

Manuel²,

Petit

et al. 2011

Eur J Immunol

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In humanized mice, the T-cell repertoire is derived from genetically identical human progenitors in distinct animals. Thus, careful comparison of the T-cell repertoires of humanized mice with those of humans may reveal the contribution of genetic determinism on T-cell repertoire formation. Here, we performed a comprehensive assessment of the distribution of V-J combinations of the human b chain of the T-cell receptor (hTRBV) in NOD.SCID.cc À/À (NSG) humanized mice. We observed that numerous V-J combinations were equally distributed in the thymus and in the periphery of humanized mice compared with human references. A global analysis of the data, comparing repertoire perturbation indices in humanized NSG mice and unrelated human PBMCs, reveals that 50% of the hTRBV families significantly overlapped. Using multivariate ranking and bootstrap analyses, we found that 18% of all possible V-J combinations contributed close to 50% of the expressed diversity, with significant over-representation of BV5-J1.111.2 and BV6-J1.111.2 rearrangements. Finally, comparison of CD3 À and CD3 1 thymocyte repertoires indicated that the observed V-J combination overlap was already present before TCR-MHC selection in the thymus. Altogether, our results show that half of the T-cell repertoire combinatorial diversity in humans is genetically determined.Key words: Humanized mice . ISEApeaks . Multivariate score . T-cell repertoire . V-J rearrangements Supporting Information available online Introduction T-cell repertoire diversity is based upon tightly ordered genetic rearrangements of the T-cell receptor V, D and J genes. The available numbers of these genes in the genome constitutes a first level of diversity: to date, 33 and 65 genes encoding variable elements of the human T-cell receptor b chain (hTRBV) from 30 hTRBV families have been characterized in mice and humans respectively (according to the ImMunoGeneTics (IMGT) database (http://www.imgt.org)). An additional level of diversity comes from the association of single V, (D) and J elements together. The major determinant of repertoire diversity is then random addition of nucleotides at the junction of these V(D)J gene segments, constituting the CDR3 of the TCR. Finally, a fourth level of complexity originates from the association of the rearranged a and b chains of the TCR. In theory, these sequential processes occurring during T-cell differentiation in the thymus could Eur. J. Immunol. 2012. 42: 760-770 760 generate up to 10 15 different TCRs, a number far in excess of the number of T-cells in the body. The 'real' size of the repertoire is probably much lower though, with recent estimations of unique TCR b chains ranging from 10 6 to 4.10 6 in humans [1,2]. Mice reconstituted with a human immune system generated from hematopoietic precursors represent a new animal model for human immunology studies. The extent of the human T-cell repertoire diversity generated in mice may represent an important functional indicator [3], useful for immunological studies in the models. However, a...

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Copy number variations across the blood–brain barrier in multiple sclerosis

Bedri

Evertsson

Khademi

et al. 2022

Ann Clin Transl Neurol

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Objective Multiple sclerosis (MS) is a neuroinflammatory disease where immune cells cross the blood–brain barrier (BBB) into the central nervous system (CNS). What predisposes these immune cells to cross the BBB is still unknown. Here, we examine the possibility that genomic rearrangements could predisposespecific immune cells in the peripheral blood to cross the BBB and form sub‐populations of cells involved in the inflammatory process in the CNS. Methods We compared copy number variations in paired peripheral blood mononuclear cells (PBMCs) and cerebrospinal fluid (CSF) cells from MS patients. Thereafter, using next generation sequencing, we studied the T‐cell receptor beta (TRB) locus rearrangements and profiled the αβ T cell repertoire in peripheral CD4+ and CD8+ T cells and in the CSF. Results We identified deletions in the T‐cell receptor alpha/delta (TRA/D), gamma (TRG), and TRB loci in CSF cells compared to PBMCs. Further characterization revealed diversity of the TRB locus which was used to describe the character and clonal expansion of T cells in the CNS. T‐cell repertoire profiling from either side of the BBB concluded that the most frequent clones in the CSF samples are unique to an individual. Furthermore, we observed a difference in the proportion of expanded T‐cell clones when comparing samples from MS patients in relapse and remission with opposite trends in CSF and peripheral blood. Interpretation This study provides a characterization of the T cells in the CSF and might indicate a role of expanded clones in MS pathogenicity.

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TCR β-Chain Sharing in Human CD8+ T Cell Responses to Cytomegalovirus and EBV

Cited by 105 publications

References 51 publications

Large TCR Diversity of Virus-Specific CD8 T Cells Provides the Mechanistic Basis for Massive TCR Renewal after Antigen Exposure

Large TCR Diversity of Virus-Specific CD8 T Cells Provides the Mechanistic Basis for Massive TCR Renewal after Antigen Exposure

Half of the T‐cell repertoire combinatorial diversity is genetically determined in humans and humanized mice

Copy number variations across the blood–brain barrier in multiple sclerosis

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