Peripheral and systemic antigens elicit an expandable pool of resident memory CD8<sup>+</sup> T cells in the bone marrow

Pascutti, María Fernanda; Geerman, Sulima; Collins, Nicholas; Brasser, Giso; Nota, Benjamin; Stark, Regina; Behr, Felix M.; Oja, Anna E.; Slot, Ed; Panagioti, Eleni; Hickson, Sarah; Wolkers, Monika C.; Heemskerk, Mirjam H.M.; Hombrink, Pleun; Arens, Ramon; Mackay, Laura K.; Gisbergen, Klaas P. J. M. van; Nolte, Martijn A.

doi:10.1002/eji.201848003

Cited by 27 publications

(33 citation statements)

References 65 publications

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“…Improved responses to anti-PD-1 in patients with high densities of tumor CD103 + CD8 + T RM cells, even after having undergone resection of their tumor, may be associated with a pool of cancer-specific CD8 + T cells present in bone marrow, as has been described in infectious diseases. 54 This non-circulating memory CD8 + T cell subset develops in response to a wide variety of antigens, including tumor antigens, and expands upon antigen rechallenge. Thus, CD103 + CD8 + T RM cells appear to be crucial components in immune protection against cancer and in the response of NSCLC to ICB, opening up new avenues in cancer immunotherapy.…”

Section: Discussionmentioning

confidence: 99%

CD103+CD8+ TRM Cells Accumulate in Tumors of Anti-PD-1-Responder Lung Cancer Patients and Are Tumor-Reactive Lymphocytes Enriched with Tc17

Corgnac

Malenica

Mezquita

et al. 2020

Cell Reports Medicine

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Summary Accumulation of CD103 + CD8 + resident memory T (T RM ) cells in human lung tumors has been associated with a favorable prognosis. However, the contribution of T RM to anti-tumor immunity and to the response to immune checkpoint blockade has not been clearly established. Using quantitative multiplex immunofluorescence on cohorts of non-small cell lung cancer patients treated with anti-PD-(L)1, we show that an increased density of CD103 + CD8 + lymphocytes in immunotherapy-naive tumors is associated with greatly improved outcomes. The density of CD103 + CD8 + cells increases during immunotherapy in most responder, but not in non-responder, patients. CD103 + CD8 + cells co-express CD49a and CD69 and display a molecular profile characterized by the expression of PD-1 and CD39. CD103 + CD8 + tumor T RM , but not CD103 − CD8 + tumor-infiltrating counterparts, express Aiolos, phosphorylated STAT-3, and IL-17; demonstrate enhanced proliferation and cytotoxicity toward autologous cancer cells; and frequently display oligoclonal expansion of TCR-β clonotypes. These results explain why CD103 + CD8 + T RM are associated with better outcomes in anti-PD-(L)1-treated patients.

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Section: Discussionmentioning

confidence: 99%

CD103+CD8+ TRM Cells Accumulate in Tumors of Anti-PD-1-Responder Lung Cancer Patients and Are Tumor-Reactive Lymphocytes Enriched with Tc17

Corgnac

Malenica

Mezquita

et al. 2020

Cell Reports Medicine

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“…In addition to the well-studied epidermis and small intestinal epithelium that are constitutively exposed to microbes, T RM lodge to organs that are less subjected to constant microbial challenge and contain few or no E-cadherin-expressing epithelial layers. These organs include CNS, kidney, submandibular salivary glands (SMG), liver, and bone marrow ( 10 , 16 , 75 , 76 ). In contrast to epidermis where CD8 + T RM are embedded between non-vascularized epithelial cells, these complex organs contain extensive blood and lymphatic vascular systems, innervation, fibroblasts, tissue-resident macrophages, and innate immune cells, as well as in some cases arborized secretory epithelium.…”

Section: T Rm Lodging and Surveillance Of “Non-barmentioning

confidence: 99%

Organ-Specific Surveillance and Long-Term Residency Strategies Adapted by Tissue-Resident Memory CD8+ T Cells

2021

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Tissue-resident CD8+ T cells (CD8+ TRM) populate lymphoid and non-lymphoid tissues after infections as first line of defense against re-emerging pathogens. To achieve host protection, CD8+ TRM have developed surveillance strategies that combine dynamic interrogation of pMHC complexes on local stromal and hematopoietic cells with long-term residency. Factors mediating CD8+ TRM residency include CD69, a surface receptor opposing the egress-promoting S1P1, CD49a, a collagen-binding integrin, and CD103, which binds E-cadherin on epithelial cells. Moreover, the topography of the tissues of residency may influence TRM retention and surveillance strategies. Here, we provide a brief summary of these factors to examine how CD8+ TRM reconcile constant migratory behavior with their long-term commitment to local microenvironments, with a focus on epithelial barrier organs and exocrine glands with mixed connective—epithelial tissue composition.

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“…These cells, being dependent on IL-15, reside in BM parenchyma ("chilling in the bone" [76]). They represent a pool of resident MTCs in close contact with the blood circulation and expandable upon peripheral or systemic antigen re-challenge [77].…”

Section: Tissue-resident Memory T Cells (T Mtcs)mentioning

confidence: 99%

New Insights into Mechanisms of Long-term Protective Anti-tumor Immunity Induced by Cancer Vaccines Modified by Virus Infection

Schirrmacher¹

2020

Biomedicines

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The topic is how to achieve long-term protective anti-tumor immunity by anti-cancer vaccination and what are its mechanisms. Cancer vaccines should instruct the immune system regarding relevant cancer targets and contain signals for innate immunity activation. Of central importance is T-cell mediated immunity and thus a detailed understanding of cognate interactions between tumor antigen (TA)-specific T cells and TA-presenting dendritic cells. Microbes and their associated molecular patterns initiate early inflammatory defense reactions that can contribute to the activation of antigen-presenting cells (APCs) and to costimulation of T cells. The concommitant stimulation of naive TA-specific CD4+ and CD8+ T cells with TAs and costimulatory signals occurs in T-APC clusters that generate effectors, such as cytotoxic T lymphocytes and T cell mediated immunological memory. Information about how such memory can be maintained over long times is updated. The role that the bone marrow with its specialized niches plays for the survival of memory T cells is emphasized. Examples are presented that demonstrate long-term protective anti-tumor immunity can be achieved by post-operative vaccination with autologous cancer vaccines that are modified by virus infection.

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Peripheral and systemic antigens elicit an expandable pool of resident memory CD8⁺ T cells in the bone marrow

Cited by 27 publications

References 65 publications

CD103+CD8+ TRM Cells Accumulate in Tumors of Anti-PD-1-Responder Lung Cancer Patients and Are Tumor-Reactive Lymphocytes Enriched with Tc17

CD103+CD8+ TRM Cells Accumulate in Tumors of Anti-PD-1-Responder Lung Cancer Patients and Are Tumor-Reactive Lymphocytes Enriched with Tc17

Organ-Specific Surveillance and Long-Term Residency Strategies Adapted by Tissue-Resident Memory CD8+ T Cells

New Insights into Mechanisms of Long-term Protective Anti-tumor Immunity Induced by Cancer Vaccines Modified by Virus Infection

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Peripheral and systemic antigens elicit an expandable pool of resident memory CD8+ T cells in the bone marrow

Cited by 27 publications

References 65 publications

CD103+CD8+ TRM Cells Accumulate in Tumors of Anti-PD-1-Responder Lung Cancer Patients and Are Tumor-Reactive Lymphocytes Enriched with Tc17

CD103+CD8+ TRM Cells Accumulate in Tumors of Anti-PD-1-Responder Lung Cancer Patients and Are Tumor-Reactive Lymphocytes Enriched with Tc17

Organ-Specific Surveillance and Long-Term Residency Strategies Adapted by Tissue-Resident Memory CD8+ T Cells

New Insights into Mechanisms of Long-term Protective Anti-tumor Immunity Induced by Cancer Vaccines Modified by Virus Infection

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Peripheral and systemic antigens elicit an expandable pool of resident memory CD8⁺ T cells in the bone marrow