Hypoxia Supports Differentiation of Terminally Exhausted CD8 T Cells

doi:10.3389/fimmu.2021.660944

. 2021 May 7:12:660944.

doi: 10.3389/fimmu.2021.660944. eCollection 2021.

Hypoxia Supports Differentiation of Terminally Exhausted CD8 T Cells

Nadia Bannoud^{1

2}, Tomás Dalotto-Moreno³, Lucía Kindgard¹, Pablo A García¹, Ada G Blidner³, Karina V Mariño⁴, Gabriel A Rabinovich^{3

5}, Diego O Croci^{1

6}

Affiliations

¹ Laboratorio de Inmunopatología, Instituto de Histología y Embriología de Mendoza (IHEM), Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Mendoza, Argentina.
² Facultad de Ciencias Médicas, Universidad Nacional de Cuyo, Mendoza, Argentina.
³ Laboratorio de Inmunopatología, Instituto de Biología y Medicina Experimental (IBYME), Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Buenos Aires, Argentina.
⁴ Laboratorio de Glicómica Funcional y Molecular, Instituto de Biología y Medicina Experimental (IBYME), Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Buenos Aires, Argentina.
⁵ Facultad de Ciencias Exactas y Naturales, Universidad de Buenos Aires, Buenos Aires, Argentina.
⁶ Facultad de Ciencias Exactas y Naturales, Universidad Nacional de Cuyo, Mendoza, Argentina.

PMID: 34025660
PMCID: PMC8137905
DOI: 10.3389/fimmu.2021.660944

Hypoxia Supports Differentiation of Terminally Exhausted CD8 T Cells

Nadia Bannoud et al. Front Immunol. 2021.

. 2021 May 7:12:660944.

doi: 10.3389/fimmu.2021.660944. eCollection 2021.

Authors

Nadia Bannoud^{1

2}, Tomás Dalotto-Moreno³, Lucía Kindgard¹, Pablo A García¹, Ada G Blidner³, Karina V Mariño⁴, Gabriel A Rabinovich^{3

5}, Diego O Croci^{1

6}

Affiliations

¹ Laboratorio de Inmunopatología, Instituto de Histología y Embriología de Mendoza (IHEM), Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Mendoza, Argentina.
² Facultad de Ciencias Médicas, Universidad Nacional de Cuyo, Mendoza, Argentina.
³ Laboratorio de Inmunopatología, Instituto de Biología y Medicina Experimental (IBYME), Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Buenos Aires, Argentina.
⁴ Laboratorio de Glicómica Funcional y Molecular, Instituto de Biología y Medicina Experimental (IBYME), Consejo Nacional de Investigaciones Científicas y Técnicas (CONICET), Buenos Aires, Argentina.
⁵ Facultad de Ciencias Exactas y Naturales, Universidad de Buenos Aires, Buenos Aires, Argentina.
⁶ Facultad de Ciencias Exactas y Naturales, Universidad Nacional de Cuyo, Mendoza, Argentina.

PMID: 34025660
PMCID: PMC8137905
DOI: 10.3389/fimmu.2021.660944

Abstract

Hypoxia, angiogenesis, and immunosuppression have been proposed to be interrelated events that fuel tumor progression and impair the clinical effectiveness of anti-tumor therapies. Here we present new mechanistic data highlighting the role of hypoxia in fine-tuning CD8 T cell exhaustion in vitro, in an attempt to reconcile seemingly opposite evidence regarding the impact of hypoxia on functional features of exhausted CD8 T cells. Focusing on the recently characterized terminally-differentiated and progenitor exhausted CD8 T cells, we found that both hypoxia and its regulated mediator, vascular endothelial growth factor (VEGF)-A, promote the differentiation of PD-1⁺ TIM-3⁺ CXCR5⁺ terminally exhausted-like CD8 T cells at the expense of PD-1⁺ TIM-3^- progenitor-like subsets without affecting tumor necrosis factor (TNF)-α and interferon (IFN)-γ production or granzyme B (GZMB) expression by these subpopulations. Interestingly, hypoxia accentuated the proangiogenic secretory profile in exhausted CD8 T cells. VEGF-A was the main factor differentially secreted by exhausted CD8 T cells under hypoxic conditions. In this sense, we found that VEGF-A contributes to generation of terminally exhausted CD8 T cells during in vitro differentiation. Altogether, our findings highlight the reciprocal regulation between hypoxia, angiogenesis, and immunosuppression, providing a rational basis to optimize synergistic combinations of antiangiogenic and immunotherapeutic strategies, with the overarching goal of improving the efficacy of these treatments.

Keywords: CD8 T cell exhaustion; Hypoxia; VEGF-A; anti cancer agents; immunosuppression.

PubMed Disclaimer

Conflict of interest statement

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Figures

**Figure 1**
Association between CD8 T cell exhaustion and hypoxia. **(A)** Schematic representation of progenitor and terminally exhausted T cell subsets. Although T cell exhaustion comprises a wide range of exhausted states, two major subsets of exhCD8 T cells have been studied in detail: the progenitor and the terminally exhausted T cell population. Whereas progenitor exhausted T cells exhibit proliferative potential, and stemness properties and can be rescued by immune checkpoint blockade (ICB) therapies, terminally exhausted T cells have higher cytotoxic potential but represent a terminal differentiation state and cannot be rescued by ICB. Proposed key molecules which discriminate these subpopulations are listed. **(B)** Modulation of CD8 T cell functions by hypoxia. Through HIF-1α and HIF2α- dependent mechanisms, hypoxic stimuli favor glycolytic anaerobic metabolism promoting T cell receptor (TCR) signaling. These include enhanced perforin and granzyme-B (GzmB) release as well as expression of immune checkpoint molecules (including both activators and inhibitors). Hypoxia inhibits expression of chemokine and cytokine receptors and adhesion molecules.

**Figure 2**
Hypoxia and VEGF-A promote differentiation of terminally exhCD8 T cells. **(A)** Schematic representation of workflow and gating strategy for *in vitro* differentiation of exhCD8 T cells. **(B)** Representative histograms showing intracellular staining of CD107a, Granzyme-B (GzmB), and TNF-α in progenitor (green) or terminally (pink) exhCD8 T cells. **(C)** Representative contour plots showing GzmB and CD107a expression in CD8⁺ PD-1⁺ T cells after 24 h exposure to hypoxia (1% O₂) or normoxia (20% O₂). **(D)** Differentiation of PD-1⁺TIM-3^-CXCR5⁺ progenitor exhCD8 T cells and PD-1⁺TIM-3⁺ terminally exhCD8 T cells under normoxic (blue bars) or hypoxic (red bars) conditions. Left, percentage of each subpopulation. Right, representative density plots showing the subpopulations. Data are the mean ± SEM of five independent experiments. **(E)** Determination of cytokine expression by intracellular flow cytometry in different exhCD8 T cell subpopulations under normoxic or hypoxic conditions. Data are the mean ± SEM of 4 independent experiments. **(F)** Heat map representing normalized row Z-score of semiquantitative cytokine array analysis of angiogenic factors secreted by CD8⁺ T cells during the differentiation process. Data shows densitometric determinations and cluster analysis of pooled supernatants from five independent experiments. **(G)** Representation of the ratio of cytokines secreted by exhCD8 T cells under normoxic or hypoxic conditions. Heat maps represent the ratio of normalized densitometric data for each cytokine in normoxia versus hypoxia. **(H)** VEGF secretion by PD-1⁺TIM-3^-CXCR5⁺ progenitor exhCD8 T cells and PD-1⁺TIM-3⁺ terminally exhCD8 T cells under normoxic (blue bars) or hypoxic (red bars) conditions. Data are the mean ± SEM of four independent experiments. **(I)** Differentiation of PD-1⁺TIM-3^-CXCR5⁺ progenitor exhCD8 T cells and PD-1⁺TIM-3⁺ terminally exhCD8 T cells in the presence (orange bars) or in the absence (blue bars) of VEGF-A (50 ng/ml). Data are the mean ± SEM of five independent experiments. **(J)** Heat map representation of intracellular cytokines determined by flow cytometry in different exhCD8 T cells subpopulations in the presence or the absence of VEGF-A (50 ng/ml). Each row represents the mean ± SEM of the percentage of cells expressing each cytokine in four independent experiments. *p < 0.05, **p < 0.01.

See this image and copyright information in PMC

Cited by

Tumor hypoxia unveiled: insights into microenvironment, detection tools and emerging therapies.
Ciepła J, Smolarczyk R. Ciepła J, et al. Clin Exp Med. 2024 Oct 3;24(1):235. doi: 10.1007/s10238-024-01501-1. Clin Exp Med. 2024. PMID: 39361163 Free PMC article. Review.
Prediction of immunotherapy efficacy and immunomodulatory role of hypoxia in colorectal cancer.
Zheng Z, Bian C, Wang H, Su J, Meng L, Xin Y, Jiang X. Zheng Z, et al. Ther Adv Med Oncol. 2022 Nov 19;14:17588359221138383. doi: 10.1177/17588359221138383. eCollection 2022. Ther Adv Med Oncol. 2022. PMID: 36425871 Free PMC article. Review.
Hypoxia, Metabolic Reprogramming, and Drug Resistance in Liver Cancer.
Bao MH, Wong CC. Bao MH, et al. Cells. 2021 Jul 6;10(7):1715. doi: 10.3390/cells10071715. Cells. 2021. PMID: 34359884 Free PMC article. Review.
Novel targets for immunotherapy associated with exhausted CD8 + T cells in cancer.
Zhang L, Zhang B, Li L, Ye Y, Wu Y, Yuan Q, Xu W, Wen X, Guo X, Nian S. Zhang L, et al. J Cancer Res Clin Oncol. 2023 May;149(5):2243-2258. doi: 10.1007/s00432-022-04326-1. Epub 2022 Sep 15. J Cancer Res Clin Oncol. 2023. PMID: 36107246 Review.
(Im)maturity in Tumor Ecosystem.
Mortezaee K, Majidpoor J. Mortezaee K, et al. Front Oncol. 2022 Jan 25;11:813897. doi: 10.3389/fonc.2021.813897. eCollection 2021. Front Oncol. 2022. PMID: 35145911 Free PMC article. Review.

See all "Cited by" articles

References

1. Coussens LM, Zitvogel L, Palucka AK. Neutralizing Tumor-Promoting Chronic Inflammation: A Magic Bullet? Science (2013) 339:286–91. 10.1126/science.1232227 - DOI - PMC - PubMed
1. Quail DF, Joyce JA. Microenvironmental Regulation of Tumor Progression and Metastasis. Nat Med (2013) 19:1423–37. 10.1038/nm.3394 - DOI - PMC - PubMed
1. Junttila MR, de Sauvage FJ. Influence of Tumour Micro-Environment Heterogeneity on Therapeutic Response. Nature (2013) 501:346–54. 10.1038/nature12626 - DOI - PubMed
1. Petitprez F, Meylan M, de Reynies A, Sautes-Fridman C, Fridman WH. The Tumor Microenvironment in the Response to Immune Checkpoint Blockade Therapies. Front Immunol (2020) 11:784. 10.3389/fimmu.2020.00784 - DOI - PMC - PubMed
1. Pardoll DM. The Blockade of Immune Checkpoints in Cancer Immunotherapy. Nat Rev Cancer (2012) 12:252–64. 10.1038/nrc3239 - DOI - PMC - PubMed

Publication types

Actions
Actions

MeSH terms

Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions
Actions

Substances

Actions

Grants and funding

U54 CA221208/CA/NCI NIH HHS/United States

LinkOut - more resources

Full Text Sources
Other Literature Sources
- scite Smart Citations
Research Materials
- NCI CPTC Antibody Characterization Program

[1] Coussens LM, Zitvogel L, Palucka AK. Neutralizing Tumor-Promoting Chronic Inflammation: A Magic Bullet? Science (2013) 339:286–91. 10.1126/science.1232227 - DOI - PMC - PubMed

[2] Coussens LM, Zitvogel L, Palucka AK. Neutralizing Tumor-Promoting Chronic Inflammation: A Magic Bullet? Science (2013) 339:286–91. 10.1126/science.1232227 - DOI - PMC - PubMed

[3] Quail DF, Joyce JA. Microenvironmental Regulation of Tumor Progression and Metastasis. Nat Med (2013) 19:1423–37. 10.1038/nm.3394 - DOI - PMC - PubMed

[4] Quail DF, Joyce JA. Microenvironmental Regulation of Tumor Progression and Metastasis. Nat Med (2013) 19:1423–37. 10.1038/nm.3394 - DOI - PMC - PubMed

[5] Junttila MR, de Sauvage FJ. Influence of Tumour Micro-Environment Heterogeneity on Therapeutic Response. Nature (2013) 501:346–54. 10.1038/nature12626 - DOI - PubMed

[6] Junttila MR, de Sauvage FJ. Influence of Tumour Micro-Environment Heterogeneity on Therapeutic Response. Nature (2013) 501:346–54. 10.1038/nature12626 - DOI - PubMed

[7] Petitprez F, Meylan M, de Reynies A, Sautes-Fridman C, Fridman WH. The Tumor Microenvironment in the Response to Immune Checkpoint Blockade Therapies. Front Immunol (2020) 11:784. 10.3389/fimmu.2020.00784 - DOI - PMC - PubMed

[8] Petitprez F, Meylan M, de Reynies A, Sautes-Fridman C, Fridman WH. The Tumor Microenvironment in the Response to Immune Checkpoint Blockade Therapies. Front Immunol (2020) 11:784. 10.3389/fimmu.2020.00784 - DOI - PMC - PubMed

[9] Pardoll DM. The Blockade of Immune Checkpoints in Cancer Immunotherapy. Nat Rev Cancer (2012) 12:252–64. 10.1038/nrc3239 - DOI - PMC - PubMed

[10] Pardoll DM. The Blockade of Immune Checkpoints in Cancer Immunotherapy. Nat Rev Cancer (2012) 12:252–64. 10.1038/nrc3239 - DOI - PMC - PubMed

Save citation to file

Email citation

Add to Collections

Add to My Bibliography

Your saved search

Create a file for external citation management software

Your RSS Feed

Hypoxia Supports Differentiation of Terminally Exhausted CD8 T Cells

Affiliations

Hypoxia Supports Differentiation of Terminally Exhausted CD8 T Cells

Authors

Affiliations

Abstract

Conflict of interest statement

Figures

Similar articles

Cited by

References

Publication types

MeSH terms

Substances

Grants and funding

LinkOut - more resources

Full Text Sources

Other Literature Sources

Research Materials

Abstract

Conflict of interest statement

Figures

Similar articles

Cited by

References

Publication types

MeSH terms

Substances

Related information

Grants and funding

LinkOut - more resources

Full Text Sources

Other Literature Sources

Research Materials