Reactivation of low avidity tumor-specific CD8+ T cells associates with immunotherapeutic efficacy of anti-PD-1
Reactivation of low avidity tumor-specific CD8+ T cells associates with immunotherapeutic efficacy of anti-PD-1
Background: CD8+ T cells are a highly diverse population of cells with distinct phenotypic functions that can influence immunotherapy outcomes. Further insights on the roles of CD8+ specificities and TCR avidity of naturally arising tumor-specific T cells, where both high and low avidity T cells recognizing the same peptide-major histocompatibility complex (pMHC) coexist in the same tumor, are crucial for understanding T cell exhaustion and resistance to PD-1 immunotherapy.
Methods: CT26 models were treated with anti-PD-1 on days 3, 6 and 9 following subcutaneous tumor implantation generating variable responses during early tumor development. Tetramer staining was performed to determine the frequency and avidity of CD8+ T cells targeting the tumor-specific epitope GSW11 and confirmed with tetramer competition assays. Functional characterization of high and low avidity GSW11-specific CD8+ T cells was conducted using flow cytometry and bulk RNA-seq. In vitro cytotoxicity assays and in vivo adoptive transfer experiments were performed to determine the cytotoxicity of high and low avidity populations.
Results: treatment success with anti-PD-1 was associated with the preferential expansion of low avidity (Tetlo) GSW11-specific CD8+ T cells with Vβ TCR expressing clonotypes. High avidity T cells (Tethi), if present, were only found in progressing PD-1 refractory tumors. Tetlo demonstrated precursor exhausted or progenitor T cell phenotypes marked by higher expression of Tcf-1 and T-bet, and lower expression of the exhaustion markers CD39, PD-1 and Eomes compared with Tethi, whereas Tethi cells were terminally exhausted. Transcriptomics analyses showed pathways related to TCR signaling, cytotoxicity and oxidative phosphorylation were significantly enriched in Tetlo found in both regressing and progressing tumors compared with Tethi, whereas genes related to DNA damage, apoptosis and autophagy were downregulated. In vitro studies showed that Tetlo exhibits higher cytotoxicity than Tethi. Adoptive transfer of Tetlo showed more effective tumor control than Tethi, and curative responses were achieved when Tetlo was combined with two doses of anti-PD-1.
Conclusions: targeting subdominant T cell responses with lower avidity against pMHC affinity neoepitopes showed potential for improving PD-1 immunotherapy. Future interventions may consider expanding low avidity populations via vaccination or adoptive transfer.
Sugiyarto, Gessa
571d4680-798b-45e1-9e8b-9990f6ec53bd
Lau, Doreen
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Hill, Samuel Luke
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Arcia-Anaya, David
ef9e7dfa-1fbc-4580-afba-9f5538bc2663
Boulanger, Denise S.M.
c226ad99-9c9a-485a-b480-42fb8799120f
Parkes, Eileen E.
5f9e5c11-d997-4104-b561-57b0e82e21ac
James, Edd
7dc1afb7-d326-4050-89fc-1f4e2a1a19a4
Elliott, Tim
16670fa8-c2f9-477a-91df-7c9e5b453e0e
11 August 2023
Sugiyarto, Gessa
571d4680-798b-45e1-9e8b-9990f6ec53bd
Lau, Doreen
05cd3a38-07be-4dd2-95b8-cf4e52c58e7c
Hill, Samuel Luke
72d727e6-0e71-4e35-8dc3-7123650800b5
Arcia-Anaya, David
ef9e7dfa-1fbc-4580-afba-9f5538bc2663
Boulanger, Denise S.M.
c226ad99-9c9a-485a-b480-42fb8799120f
Parkes, Eileen E.
5f9e5c11-d997-4104-b561-57b0e82e21ac
James, Edd
7dc1afb7-d326-4050-89fc-1f4e2a1a19a4
Elliott, Tim
16670fa8-c2f9-477a-91df-7c9e5b453e0e
Sugiyarto, Gessa, Lau, Doreen, Hill, Samuel Luke, Arcia-Anaya, David, Boulanger, Denise S.M., Parkes, Eileen E., James, Edd and Elliott, Tim
(2023)
Reactivation of low avidity tumor-specific CD8+ T cells associates with immunotherapeutic efficacy of anti-PD-1.
Journal for Immunotherapy of Cancer, 11 (8).
(doi:10.1136/jitc-2023-007114).
Abstract
Background: CD8+ T cells are a highly diverse population of cells with distinct phenotypic functions that can influence immunotherapy outcomes. Further insights on the roles of CD8+ specificities and TCR avidity of naturally arising tumor-specific T cells, where both high and low avidity T cells recognizing the same peptide-major histocompatibility complex (pMHC) coexist in the same tumor, are crucial for understanding T cell exhaustion and resistance to PD-1 immunotherapy.
Methods: CT26 models were treated with anti-PD-1 on days 3, 6 and 9 following subcutaneous tumor implantation generating variable responses during early tumor development. Tetramer staining was performed to determine the frequency and avidity of CD8+ T cells targeting the tumor-specific epitope GSW11 and confirmed with tetramer competition assays. Functional characterization of high and low avidity GSW11-specific CD8+ T cells was conducted using flow cytometry and bulk RNA-seq. In vitro cytotoxicity assays and in vivo adoptive transfer experiments were performed to determine the cytotoxicity of high and low avidity populations.
Results: treatment success with anti-PD-1 was associated with the preferential expansion of low avidity (Tetlo) GSW11-specific CD8+ T cells with Vβ TCR expressing clonotypes. High avidity T cells (Tethi), if present, were only found in progressing PD-1 refractory tumors. Tetlo demonstrated precursor exhausted or progenitor T cell phenotypes marked by higher expression of Tcf-1 and T-bet, and lower expression of the exhaustion markers CD39, PD-1 and Eomes compared with Tethi, whereas Tethi cells were terminally exhausted. Transcriptomics analyses showed pathways related to TCR signaling, cytotoxicity and oxidative phosphorylation were significantly enriched in Tetlo found in both regressing and progressing tumors compared with Tethi, whereas genes related to DNA damage, apoptosis and autophagy were downregulated. In vitro studies showed that Tetlo exhibits higher cytotoxicity than Tethi. Adoptive transfer of Tetlo showed more effective tumor control than Tethi, and curative responses were achieved when Tetlo was combined with two doses of anti-PD-1.
Conclusions: targeting subdominant T cell responses with lower avidity against pMHC affinity neoepitopes showed potential for improving PD-1 immunotherapy. Future interventions may consider expanding low avidity populations via vaccination or adoptive transfer.
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Accepted/In Press date: 31 July 2023
Published date: 11 August 2023
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Local EPrints ID: 498425
URI: http://eprints.soton.ac.uk/id/eprint/498425
PURE UUID: 2c1e5662-abdb-4a8f-9a1e-c55334a08997
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Date deposited: 18 Feb 2025 17:38
Last modified: 22 Aug 2025 01:56
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Author:
Gessa Sugiyarto
Author:
Doreen Lau
Author:
Samuel Luke Hill
Author:
David Arcia-Anaya
Author:
Denise S.M. Boulanger
Author:
Eileen E. Parkes
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