Your search keyword '"Busselaar, Julia"' showing total 8 results

1. PD-1 or CTLA-4 blockade promotes CD86-driven Treg responses upon radiotherapy of lymphocyte-depleted cancer in mice

Author

Frijlink, Elselien, Bosma, Douwe M.T., Busselaar, Julia, Battaglia, Thomas W., Staal, Mo D., Verbrugge, Inge, and Borst, Jannie

Subjects

T cells -- Analysis, Immune response -- Analysis, Cancer -- Diagnosis -- Care and treatment, Radiotherapy -- Patient outcomes, Health care industry

Abstract

Radiotherapy (RT) is considered immunogenic, but clinical data demonstrating RT-induced T cell priming are scarce. Here, we show in a mouse tumor model representative of human lymphocyte-depleted cancer that RT enhanced spontaneous priming of thymus-derived ([FOXP3.sup.+][Helios.sup.+]) Tregs by the tumor. These Tregs acquired an effector phenotype, populated the tumor, and impeded tumor control by a simultaneous, RT-induced [CD8.sup.+] cytotoxic T cell (CTL) response. Combination of RT with CTLA-4 or PD-1 blockade, which enables CD28 costimulation, further increased this Treg response and failed to improve tumor control. We discovered that upon RT, the CD28 ligands CD86 and CD80 differentially affected the Treg response. CD86, but not CD80, blockade prevented the effector Treg response, enriched the tumor-draining lymph node migratory conventional DCs that were positive for PD-L1 and CD80 ([PD-L1.sup.+][CD80.sup.+]), and promoted CTL priming. Blockade of CD86 alone or in combination with PD-1 enhanced intratumoral CTL accumulation, and the combination significantly increased RT-induced tumor regression and OS. We advise that combining RT with PD-1 and/or CTLA-4 blockade may be counterproductive in lymphocyte-depleted cancers, since these interventions drive Treg responses in this context. However, combining RT with CD86 blockade may promote the control of such tumors by enabling a CTL response., Introduction Immunotherapy by antibody-based immune checkpoint blockade (ICB) is a new treatment modality for multiple cancer types. However, only a minority of patients experience durable clinical responses (1), partly due [...]

Published

2024

2. PD-1 and CTLA-4 blockade promote CD86-driven Treg responses upon radiotherapy of lymphocyte-depleted cancer in mice

Author

Frijlink, Elselien, primary, Bosma, Douwe M.T., additional, Busselaar, Julia, additional, Battaglia, Thomas W., additional, Staal, Mo D., additional, Verbrugge, Inge, additional, and Borst, Jannie, additional

Published

2024

3. CD4+ T cell help creates memory CD8+ T cells with innate and help-independent recall capacities

Author

Ahrends, Tomasz, Busselaar, Julia, Severson, Tesa M., Bąbała, Nikolina, de Vries, Evert, Bovens, Astrid, Wessels, Lodewyk, van Leeuwen, Fred, and Borst, Jannie

Published

2019

4. Mechanism of action of PD‐1 receptor/ligand targeted cancer immunotherapy

Author

Borst, Jannie, primary, Busselaar, Julia, additional, Bosma, Douwe M. T., additional, and Ossendorp, Ferry, additional

Published

2021

5. Helpless Priming Sends CD8+ T Cells on the Road to Exhaustion

Author

Busselaar, Julia, primary, Tian, Sun, additional, van Eenennaam, Hans, additional, and Borst, Jannie, additional

Published

2020

6. Helpless Priming Sends CD8+ T Cells on the Road to Exhaustion.

Author

Busselaar, Julia, Tian, Sun, van Eenennaam, Hans, and Borst, Jannie

Subjects

T cells, CYTOTOXIC T cells, PROGRAMMED cell death 1 receptors

Abstract

Persistent antigen exposure in chronic infection and cancer has been proposed to lead to cytotoxic T lymphocyte (CTL) "exhaustion", i.e., loss of effector function and disease control. Recent work identifies a population of poorly differentiated TCF-1+PD-1+ CD8+ T cells as precursors of the terminally exhausted CTL pool. These "predysfunctional" CTLs are suggested to respond to PD-1 targeted therapy by giving rise to a pool of functional CTLs. Supported by gene expression analyses, we present a model in which lack of CD4+ T cell help during CD8+ T cell priming results in the formation of predysfunctional CTLs. Our model implies that predysfunctional CTLs are formed during priming and that the remedy for CTL dysfunction is to provide "help" signals for generation of optimal CTL effectors. We substantiate that this may be achieved by engaging CD4+ T cells in new CD8+ T cell priming, or by combined PD-1 blocking and CD27 agonism with available immunotherapeutic antibodies. [ABSTRACT FROM AUTHOR]

Published

2020

7. CD4+ T cell help creates memory CD8+ T cells with innate and help-independent recall capacities.

Author

Ahrends, Tomasz, Busselaar, Julia, Severson, Tesa M., Bąbała, Nikolina, de Vries, Evert, Bovens, Astrid, Wessels, Lodewyk, van Leeuwen, Fred, and Borst, Jannie

Abstract

CD4+ T cell help is required for the generation of CD8+ cytotoxic T lymphocyte (CTL) memory. Here, we use genome-wide analyses to show how CD4+ T cell help delivered during priming promotes memory differentiation of CTLs. Help signals enhance IL-15-dependent maintenance of central memory T (TCM) cells. More importantly, help signals regulate the size and function of the effector memory T (TEM) cell pool. Helped TEM cells produce Granzyme B and IFNγ upon antigen-independent, innate-like recall by IL-12 and IL-18. In addition, helped memory CTLs express the effector program characteristic of helped primary CTLs upon recall with MHC class I-restricted antigens, likely due to epigenetic imprinting and sustained mRNA expression of effector genes. Our data thus indicate that during priming, CD4+ T cell help optimizes CTL memory by creating TEM cells with innate and help-independent antigen-specific recall capacities. [ABSTRACT FROM AUTHOR]

Published

2019

8. Helpless Priming Sends CD8 + T Cells on the Road to Exhaustion.

Author

Busselaar J, Tian S, van Eenennaam H, and Borst J

Subjects

Animals, Biomarkers, CD8-Positive T-Lymphocytes metabolism, Computational Biology methods, Gene Expression Profiling, Humans, Lymphocyte Activation genetics, Lymphocyte Count, Mice, Neoplasms etiology, Neoplasms metabolism, Neoplasms pathology, Signal Transduction, T-Cell Antigen Receptor Specificity, T-Lymphocyte Subsets immunology, T-Lymphocyte Subsets metabolism, Transcriptome, CD8-Positive T-Lymphocytes immunology, Lymphocyte Activation immunology

Abstract

Persistent antigen exposure in chronic infection and cancer has been proposed to lead to cytotoxic T lymphocyte (CTL) "exhaustion", i.e., loss of effector function and disease control. Recent work identifies a population of poorly differentiated TCF-1 + PD-1 + CD8 + T cells as precursors of the terminally exhausted CTL pool. These "predysfunctional" CTLs are suggested to respond to PD-1 targeted therapy by giving rise to a pool of functional CTLs. Supported by gene expression analyses, we present a model in which lack of CD4 + T cell help during CD8 + T cell priming results in the formation of predysfunctional CTLs. Our model implies that predysfunctional CTLs are formed during priming and that the remedy for CTL dysfunction is to provide "help" signals for generation of optimal CTL effectors. We substantiate that this may be achieved by engaging CD4 + T cells in new CD8 + T cell priming, or by combined PD-1 blocking and CD27 agonism with available immunotherapeutic antibodies., (Copyright © 2020 Busselaar, Tian, van Eenennaam and Borst.)

Published

2020