Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx

Background<p>The role of CD4 T cells in the control of viral infections beyond their traditional helper activity has been increasingly recognized, and CD4 T cells with cytotoxic capacity have been reported for the nearly ubiquitous betaherpesviruses HCMV (human cytomegalovirus) and HHV-6B (hum...

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Huvudupphovsman: Aniuska Becerra-Artiles (829447) (author)
Övriga upphovsmän: Grant C. Weaver (16699376) (author), Peter O. Oluoch (8737743) (author), Lawrence J. Stern (49046) (author)
Publicerad: 2025
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author Aniuska Becerra-Artiles (829447)
author2 Grant C. Weaver (16699376)
Peter O. Oluoch (8737743)
Lawrence J. Stern (49046)
author2_role author
author
author
author_facet Aniuska Becerra-Artiles (829447)
Grant C. Weaver (16699376)
Peter O. Oluoch (8737743)
Lawrence J. Stern (49046)
author_role author
dc.creator.none.fl_str_mv Aniuska Becerra-Artiles (829447)
Grant C. Weaver (16699376)
Peter O. Oluoch (8737743)
Lawrence J. Stern (49046)
dc.date.none.fl_str_mv 2025-11-25T14:36:24Z
dc.identifier.none.fl_str_mv 10.3389/fimmu.2025.1631558.s006
dc.relation.none.fl_str_mv https://figshare.com/articles/dataset/Table_3_TCR_repertoire_of_human_cytotoxic_CD4_T_cells_responding_to_betaherpesviruses_HHV-6B_and_HCMV_xlsx/30710693
dc.rights.none.fl_str_mv CC BY 4.0
info:eu-repo/semantics/openAccess
dc.subject.none.fl_str_mv Genetic Immunology
cytotoxic CD4 T cells
TCR repertoire
public TCRs
HHV-6B
HCMV
dc.title.none.fl_str_mv Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
dc.type.none.fl_str_mv Dataset
info:eu-repo/semantics/publishedVersion
dataset
description Background<p>The role of CD4 T cells in the control of viral infections beyond their traditional helper activity has been increasingly recognized, and CD4 T cells with cytotoxic capacity have been reported for the nearly ubiquitous betaherpesviruses HCMV (human cytomegalovirus) and HHV-6B (human herpesvirus 6B).</p>Objective<p>We sought to investigate the functional landscape of cytotoxic CD4 T cells responding to HHV-6B and HCMV epitopes presented by DRB1*03:01 and to identify public T-cell receptors (TCRs) (i.e., shared by multiple subjects).</p>Approach<p>We tetramer-sorted epitope-specific CD4 T cells from healthy donors and performed RNA and TCR sequencing to assess functional profiles and identify TCR clonotypes. We evaluated the publicity of the repertoire and tested the functionality, epitope specificity, and sensitivity of selected public clonotypes.</p>Results<p>Differential gene expression analysis comparing T cells expanded with HHV-6B and HCMV epitopes showed differences in their functional profiles, with the HCMV-expanded T cells displaying a more robust cytotoxic gene expression signature. Tens to hundreds of TCR clonotypes responding to HHV-6B or HCMV were identified in each subject. The TCR repertoires were dominated by private clonotypes in all subjects, but 3 public TCRα/β, along with 41 public TCRα and TCRβ clonotypes were identified. Some of these clonotypes and closely related variants were found in a substantial fraction of DRB1*03:01 subjects in datasets of total peripheral blood TCR repertoires. TCRs associated with two HHV-6B epitopes (U11.306–323 and U85.88-104) and one HCMV epitope (pp65.509-523) were cloned for validation and biochemical characterization. Using an in vitro activation assay, the epitope specificity was confirmed for each selected TCRα/β, with half-maximal activation observed at 5–50 nM peptide concentration. With one exception, all TCRs bound tightly to the corresponding peptide-major histocompatibility complex (pMHC) tetramer. Finally, minimal peptide mapping combined with structural modeling of pMHCs identified potential sites of TCR interaction.</p>Conclusions<p>CD4 T cells recognizing HHV-6B or HCMV exhibit cytotoxic signatures and can lyse antigen-pulsed target cells, with the HCMV-specific population exhibiting greater activity. The TCR repertoires of CD4 T cells recognizing HHV-6B or HCMV epitopes presented by DRB1*03:01 are broad but include public TCR clonotypes. These TCRs may be useful to monitor infection, reactivation under immunosuppressive conditions, and response to therapy.</p>
eu_rights_str_mv openAccess
id Manara_3176c45540a6b6c8c1244ee6dce588d1
identifier_str_mv 10.3389/fimmu.2025.1631558.s006
network_acronym_str Manara
network_name_str ManaraRepo
oai_identifier_str oai:figshare.com:article/30710693
publishDate 2025
repository.mail.fl_str_mv
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rights_invalid_str_mv CC BY 4.0
spelling Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsxAniuska Becerra-Artiles (829447)Grant C. Weaver (16699376)Peter O. Oluoch (8737743)Lawrence J. Stern (49046)Genetic Immunologycytotoxic CD4 T cellsTCR repertoirepublic TCRsHHV-6BHCMVBackground<p>The role of CD4 T cells in the control of viral infections beyond their traditional helper activity has been increasingly recognized, and CD4 T cells with cytotoxic capacity have been reported for the nearly ubiquitous betaherpesviruses HCMV (human cytomegalovirus) and HHV-6B (human herpesvirus 6B).</p>Objective<p>We sought to investigate the functional landscape of cytotoxic CD4 T cells responding to HHV-6B and HCMV epitopes presented by DRB1*03:01 and to identify public T-cell receptors (TCRs) (i.e., shared by multiple subjects).</p>Approach<p>We tetramer-sorted epitope-specific CD4 T cells from healthy donors and performed RNA and TCR sequencing to assess functional profiles and identify TCR clonotypes. We evaluated the publicity of the repertoire and tested the functionality, epitope specificity, and sensitivity of selected public clonotypes.</p>Results<p>Differential gene expression analysis comparing T cells expanded with HHV-6B and HCMV epitopes showed differences in their functional profiles, with the HCMV-expanded T cells displaying a more robust cytotoxic gene expression signature. Tens to hundreds of TCR clonotypes responding to HHV-6B or HCMV were identified in each subject. The TCR repertoires were dominated by private clonotypes in all subjects, but 3 public TCRα/β, along with 41 public TCRα and TCRβ clonotypes were identified. Some of these clonotypes and closely related variants were found in a substantial fraction of DRB1*03:01 subjects in datasets of total peripheral blood TCR repertoires. TCRs associated with two HHV-6B epitopes (U11.306–323 and U85.88-104) and one HCMV epitope (pp65.509-523) were cloned for validation and biochemical characterization. Using an in vitro activation assay, the epitope specificity was confirmed for each selected TCRα/β, with half-maximal activation observed at 5–50 nM peptide concentration. With one exception, all TCRs bound tightly to the corresponding peptide-major histocompatibility complex (pMHC) tetramer. Finally, minimal peptide mapping combined with structural modeling of pMHCs identified potential sites of TCR interaction.</p>Conclusions<p>CD4 T cells recognizing HHV-6B or HCMV exhibit cytotoxic signatures and can lyse antigen-pulsed target cells, with the HCMV-specific population exhibiting greater activity. The TCR repertoires of CD4 T cells recognizing HHV-6B or HCMV epitopes presented by DRB1*03:01 are broad but include public TCR clonotypes. These TCRs may be useful to monitor infection, reactivation under immunosuppressive conditions, and response to therapy.</p>2025-11-25T14:36:24ZDatasetinfo:eu-repo/semantics/publishedVersiondataset10.3389/fimmu.2025.1631558.s006https://figshare.com/articles/dataset/Table_3_TCR_repertoire_of_human_cytotoxic_CD4_T_cells_responding_to_betaherpesviruses_HHV-6B_and_HCMV_xlsx/30710693CC BY 4.0info:eu-repo/semantics/openAccessoai:figshare.com:article/307106932025-11-25T14:36:24Z
spellingShingle Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
Aniuska Becerra-Artiles (829447)
Genetic Immunology
cytotoxic CD4 T cells
TCR repertoire
public TCRs
HHV-6B
HCMV
status_str publishedVersion
title Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
title_full Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
title_fullStr Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
title_full_unstemmed Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
title_short Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
title_sort Table 3_TCR repertoire of human cytotoxic CD4 T cells responding to betaherpesviruses HHV-6B and HCMV.xlsx
topic Genetic Immunology
cytotoxic CD4 T cells
TCR repertoire
public TCRs
HHV-6B
HCMV