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1. LTX-315 and adoptive cell therapy using tumor-infiltrating lymphocytes generate tumor specific T cells in patients with metastatic soft tissue sarcoma

Author

Nielsen, Morten, Monberg, Tine, Sundvold, Vibeke, Albieri, Benedetta, Hovgaard, Dorrit, Petersen, Michael Mørk, Krarup-Hansen, Anders, Met, Özcan, Camilio, Ketil, Clancy, Trevor, Stratford, Richard, Sveinbjornsson, Baldur, Rekdal, Øystein, Junker, Niels, Svane, Inge Marie, Nielsen, Morten, Monberg, Tine, Sundvold, Vibeke, Albieri, Benedetta, Hovgaard, Dorrit, Petersen, Michael Mørk, Krarup-Hansen, Anders, Met, Özcan, Camilio, Ketil, Clancy, Trevor, Stratford, Richard, Sveinbjornsson, Baldur, Rekdal, Øystein, Junker, Niels, and Svane, Inge Marie

Abstract

LTX-315 is an oncolytic peptide that elicits both local and systemic immune responses upon intratumoral injection. In the present pilot trial, we treated patients with metastatic soft tissue sarcoma with the combination of LTX-315 and adoptive T-cell therapy using in vitro expanded tumor-infiltrating lymphocytes. Six heavily pretreated patients were included in the trial and treated with LTX-315 of which four patients proceeded to adoptive T-cell therapy. Overall, the treatment was considered safe with only expected and manageable toxicity. The best overall clinical response was stable disease for 208 days, and in this patient, we detected tumor-reactive T cells in the blood that lasted until disease progression. In three patients T-cell reactivity against in silico predicted neoantigens was demonstrated. Additionally, de novo T-cell clones were generated and expanded in the blood following LTX-315 injections. In conclusion, this pilot study provides proof that it is feasible to combine LTX-315 and adoptive T-cell therapy, and that this treatment can induce systemic immune responses that resulted in stabilization of the disease in sarcoma patients with otherwise progressive disease. Further optimization of the treatment protocol is warranted to increase clinical activity. ClinicalTrials.gov Identifier: NCT03725605.

Published
2024

2. Reduced mitochondrial respiration in peripheral T cells after paediatric heamatopoietic stem cell transplantation

Author

Mølgaard, Kasper, Kielsen, Katrine, Ifversen, Marianne, Met, Özcan, Svane, Inge Marie, Müller, Klaus, Mølgaard, Kasper, Kielsen, Katrine, Ifversen, Marianne, Met, Özcan, Svane, Inge Marie, and Müller, Klaus

Abstract

Background: Recovery and functional differentiation of T-cell subsets are central for the development of immune function and complications after allogeneic hematopoietic stem cell transplantation (HSCT), but little is known about the cellular respiration and factors influencing T-cell metabolic fitness during immune maturation after HSCT. Method: We included 20 HSCT patients and analysed mitochondrial oxidative phosphorylation and mitochondrial fitness in peripheral blood mononuclear cell samples collected at days +90 and +180 after HSCT. Results: Phenotypic analysis revealed lower overall T-cell counts, lower CD4+/CD8+ ratio and a skewed distribution of early T-cell subsets at day +90, gradually recovering by day +180. Although ATP turnover in HSCT patients was similar to healthy controls, the spare respiratory capacity (SRC) of T cells, reflecting the available energy reserve, was significantly reduced at day +90 and +180 compared to healthy controls. This reduction in SRC was not correlated with the occurrence of acute graft-versus-host disease (aGVHD), the intensity of conditioning regimens and markers of T-cell exhaustion. Conclusion: We found significantly depressed SRC until six months post-HSCT, but we were not able to identify transplant-related risk factors or associations with the clinical outcome.

Published
2024

3. Arginase-1 specific CD8+ T cells react toward malignant and regulatory myeloid cells

Author

Glöckner, Hannah Jorinde, Martinenaite, Evelina, Landkildehus Lisle, Thomas, Grauslund, Jacob, Ahmad, Shamaila, Met, Özcan, Thor Straten, Per, Hald Andersen, Mads, Glöckner, Hannah Jorinde, Martinenaite, Evelina, Landkildehus Lisle, Thomas, Grauslund, Jacob, Ahmad, Shamaila, Met, Özcan, Thor Straten, Per, and Hald Andersen, Mads

Abstract

Arginase-1 (Arg1) is expressed by regulatory myeloid cells in the tumor microenvironment (TME), where they play a pro-tumorigenic and T-cell suppressive role. Arg1-specific CD4+ and CD8+ memory T cells have been observed in both healthy individuals and cancer patients. However, while the function of anti-regulatory Arg1-specific CD4+ T cells has been characterized, our knowledge of CD8+ Arg1-specific T cells is only scarce. In the current study, we describe the immune-modulatory capabilities of CD8+ Arg1-specific T cells. We generated CD8+ Arg1-specific T cell clones to target Arg1-expressing myeloid cells. Our results demonstrate that these T cells recognize both malignant and nonmalignant regulatory myeloid cells in an Arg1-expression-dependent manner. Notably, Arg1-specific CD8+ T cells possess cytolytic effector capabilities. Immune modulatory vaccines (IMVs) represent a novel treatment modality for cancer. The activation of Arg1-specific CD8+ T cells through Arg1-based IMVs can contribute to the modulatory effects of this treatment strategy.

Published
2024

4. Ex vivo modulation of intact tumor fragments with anti-PD-1 and anti-CTLA-4 influences the expansion and specificity of tumor-infiltrating lymphocytes.

Author

Hulen, Thomas Morgan, Friese, Christina, Kristensen, Nikolaj Pagh, Granhøj, Joachim Stoltenborg, Borch, Troels Holz, Peeters, Marlies J. W., Donia, Marco, Andersen, Mads Hald, Hadrup, Sine Reker, Svane, Inge Marie, and Met, Özcan

Subjects
TUMOR antigens, TUMOR-infiltrating immune cells, DEATH receptors, GENETIC barcoding, CELLULAR therapy
Abstract

Checkpoint inhibition (CPI) therapy and adoptive cell therapy with autologous tumor-infiltrating lymphocytes (TIL-based ACT) are the two most effective immunotherapies for the treatment of metastatic melanoma. While CPI has been the dominating therapy in the past decade, TIL-based ACT is beneficial for individuals even after progression on previous immunotherapies. Given that notable differences in response have been made when used as a subsequent treatment, we investigated how the qualities of TILs changed when the ex vivo microenvironment of intact tumor fragments were modulated with checkpoint inhibitors targeting programmed death receptor 1 (PD-1) and cytotoxic Tlymphocyte-associated protein 4 (CTLA-4). Initially, we show that unmodified TILs from CPI-resistant individuals can be produced, are overwhelmingly terminally differentiated, and are capable of responding to tumor. We then investigate these properties in ex vivo checkpoint modulated TILs finding that that they retain these qualities. Lastly, we confirmed the specificity of the TILs to the highest responding tumor antigens, and identified this reactivity resides largely in CD39+CD69+ terminally differentiated populations. Overall, we found that anti-PD-1 will alter the proliferative capacity while anti-CTLA4 will influence breadth of antigen specificity. [ABSTRACT FROM AUTHOR]

Published
2024
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7. LTX-315 and adoptive cell therapy using tumor-infiltrating lymphocytes generate tumor specific T cells in patients with metastatic soft tissue sarcoma

Author

Nielsen, Morten, primary, Monberg, Tine, additional, Sundvold, Vibeke, additional, Albieri, Benedetta, additional, Hovgaard, Dorrit, additional, Petersen, Michael Mørk, additional, Krarup-Hansen, Anders, additional, Met, Özcan, additional, Camilio, Ketil, additional, Clancy, Trevor, additional, Stratford, Richard, additional, Sveinbjornsson, Baldur, additional, Rekdal, Øystein, additional, Junker, Niels, additional, and Svane, Inge Marie, additional

Published
2023
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10. TCR-engaging scaffolds selectively expand antigen-specific T-cells with a favorable phenotype for adoptive cell therapy

Author

Tvingsholm, Siri Amanda, primary, Frej, Marcus Svensson, additional, Rafa, Vibeke Mindahl, additional, Hansen, Ulla Kring, additional, Ormhøj, Maria, additional, Tyron, Alexander, additional, Jensen, Agnete W P, additional, Kadivar, Mohammad, additional, Bentzen, Amalie Kai, additional, Munk, Kamilla K, additional, Aasbjerg, Gitte N, additional, Ternander, Jeppe S H, additional, Heeke, Christina, additional, Tamhane, Tripti, additional, Schmess, Christian, additional, Funt, Samuel A., additional, Kjeldsen, Julie Westerlin, additional, Kverneland, Anders Handrup, additional, Met, Özcan, additional, Draghi, Arianna, additional, Jakobsen, Søren Nyboe, additional, Donia, Marco, additional, Marie Svane, Inge, additional, and Hadrup, Sine Reker, additional

Published
2023
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11. Restoring tumor immunogenicity with dendritic cell reprogramming

Author

Zimmermannova, Olga, primary, Ferreira, Alexandra G., additional, Ascic, Ervin, additional, Velasco Santiago, Marta, additional, Kurochkin, Ilia, additional, Hansen, Morten, additional, Met, Özcan, additional, Caiado, Inês, additional, Shapiro, Ilja E., additional, Michaux, Justine, additional, Humbert, Marion, additional, Soto-Cabrera, Diego, additional, Benonisson, Hreinn, additional, Silvério-Alves, Rita, additional, Gomez-Jimenez, David, additional, Bernardo, Carina, additional, Bauden, Monika, additional, Andersson, Roland, additional, Höglund, Mattias, additional, Miharada, Kenichi, additional, Nakamura, Yukio, additional, Hugues, Stephanie, additional, Greiff, Lennart, additional, Lindstedt, Malin, additional, Rosa, Fábio F., additional, Pires, Cristiana F., additional, Bassani-Sternberg, Michal, additional, Svane, Inge Marie, additional, and Pereira, Carlos-Filipe, additional

Published
2023
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12. Ex vivo modulation of intact tumor fragments with anti-PD-1 and anti-CTLA-4 influences the expansion and specificity of tumor-infiltrating lymphocytes

Author

Hulen, Thomas Morgan, primary, Friese, Christina, additional, Kristensen, Nikolaj Pagh, additional, Granhøj, Joachim Stoltenborg, additional, Borch, Troels Holz, additional, Peeters, Marlies J. W., additional, Donia, Marco, additional, Andersen, Mads Hald, additional, Hadrup, Sine Reker, additional, Svane, Inge Marie, additional, and Met, Özcan, additional

Published
2023
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13. Data from MERTK Acts as a Costimulatory Receptor on Human CD8+ T Cells

Author

Peeters, Marlies J.W., primary, Dulkeviciute, Donata, primary, Draghi, Arianna, primary, Ritter, Cathrin, primary, Rahbech, Anne, primary, Skadborg, Signe K., primary, Seremet, Tina, primary, Carnaz Simões, Ana Micaela, primary, Martinenaite, Evelina, primary, Halldórsdóttir, Hólmfridur R., primary, Andersen, Mads Hald, primary, Olofsson, Gitte Holmen, primary, Svane, Inge Marie, primary, Rasmussen, Lene Juel, primary, Met, Özcan, primary, Becker, Jürgen C., primary, Donia, Marco, primary, Desler, Claus, primary, and thor Straten, Per, primary

Published
2023
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14. Table S2 from MERTK Acts as a Costimulatory Receptor on Human CD8+ T Cells

Author

Peeters, Marlies J.W., primary, Dulkeviciute, Donata, primary, Draghi, Arianna, primary, Ritter, Cathrin, primary, Rahbech, Anne, primary, Skadborg, Signe K., primary, Seremet, Tina, primary, Carnaz Simões, Ana Micaela, primary, Martinenaite, Evelina, primary, Halldórsdóttir, Hólmfridur R., primary, Andersen, Mads Hald, primary, Olofsson, Gitte Holmen, primary, Svane, Inge Marie, primary, Rasmussen, Lene Juel, primary, Met, Özcan, primary, Becker, Jürgen C., primary, Donia, Marco, primary, Desler, Claus, primary, and thor Straten, Per, primary

Published
2023
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15. Supplementary Data from MERTK Acts as a Costimulatory Receptor on Human CD8+ T Cells

Author

Peeters, Marlies J.W., primary, Dulkeviciute, Donata, primary, Draghi, Arianna, primary, Ritter, Cathrin, primary, Rahbech, Anne, primary, Skadborg, Signe K., primary, Seremet, Tina, primary, Carnaz Simões, Ana Micaela, primary, Martinenaite, Evelina, primary, Halldórsdóttir, Hólmfridur R., primary, Andersen, Mads Hald, primary, Olofsson, Gitte Holmen, primary, Svane, Inge Marie, primary, Rasmussen, Lene Juel, primary, Met, Özcan, primary, Becker, Jürgen C., primary, Donia, Marco, primary, Desler, Claus, primary, and thor Straten, Per, primary

Published
2023
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16. Supplementary Tables and Legends from T-cell Responses in the Microenvironment of Primary Renal Cell Carcinoma—Implications for Adoptive Cell Therapy

Author

Andersen, Rikke, primary, Westergaard, Marie Christine Wulff, primary, Kjeldsen, Julie Westerlin, primary, Müller, Anja, primary, Pedersen, Natasja Wulff, primary, Hadrup, Sine Reker, primary, Met, Özcan, primary, Seliger, Barbara, primary, Kromann-Andersen, Bjarne, primary, Hasselager, Thomas, primary, Donia, Marco, primary, and Svane, Inge Marie, primary

Published
2023
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17. Supplementary Figures 1-16 and Legends from T-cell Responses in the Microenvironment of Primary Renal Cell Carcinoma—Implications for Adoptive Cell Therapy

Author

Andersen, Rikke, primary, Westergaard, Marie Christine Wulff, primary, Kjeldsen, Julie Westerlin, primary, Müller, Anja, primary, Pedersen, Natasja Wulff, primary, Hadrup, Sine Reker, primary, Met, Özcan, primary, Seliger, Barbara, primary, Kromann-Andersen, Bjarne, primary, Hasselager, Thomas, primary, Donia, Marco, primary, and Svane, Inge Marie, primary

Published
2023
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18. Data from T-cell Responses in the Microenvironment of Primary Renal Cell Carcinoma—Implications for Adoptive Cell Therapy

Author

Andersen, Rikke, primary, Westergaard, Marie Christine Wulff, primary, Kjeldsen, Julie Westerlin, primary, Müller, Anja, primary, Pedersen, Natasja Wulff, primary, Hadrup, Sine Reker, primary, Met, Özcan, primary, Seliger, Barbara, primary, Kromann-Andersen, Bjarne, primary, Hasselager, Thomas, primary, Donia, Marco, primary, and Svane, Inge Marie, primary

Published
2023
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22. Supplementary Figures 1-6 and Supplementary Table 1 from Long-Lasting Complete Responses in Patients with Metastatic Melanoma after Adoptive Cell Therapy with Tumor-Infiltrating Lymphocytes and an Attenuated IL2 Regimen

Author

Andersen, Rikke, primary, Donia, Marco, primary, Ellebaek, Eva, primary, Borch, Troels Holz, primary, Kongsted, Per, primary, Iversen, Trine Zeeberg, primary, Hölmich, Lisbet Rosenkrantz, primary, Hendel, Helle Westergren, primary, Met, Özcan, primary, Andersen, Mads Hald, primary, thor Straten, Per, primary, and Svane, Inge Marie, primary

Published
2023
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26. Pre-existing TGF-β-specific T-cell immunity in patients with pancreatic cancer predicts survival after checkpoint inhibitors combined with radiotherapy

Author

Mortensen, Rasmus Erik Johansson, primary, Holmström, Morten Orebo, additional, Lisle, Thomas Landkildehus, additional, Hasselby, Jane P, additional, Willemoe, Gro L, additional, Met, Özcan, additional, Marie Svane, Inge, additional, Johansen, Julia, additional, Nielsen, Dorte L, additional, Chen, Inna M, additional, and Andersen, Mads Hald, additional

Published
2023
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27. TCR-engaging scaffolds selectively expand antigen-specific T-cells with a favorable phenotype for adoptive cell therapy

Author

Tvingsholm, Siri Amanda, Frej, Marcus Svensson, Rafa, Vibeke Mindahl, Hansen, Ulla Kring, Ormhøj, Maria, Tyron, Alexander, Jensen, Agnete W.P., Kadivar, Mohammad, Bentzen, Amalie Kai, Munk, Kamilla K., Aasbjerg, Gitte N., Ternander, Jeppe S.H., Heeke, Christina, Tamhane, Tripti, Schmess, Christian, Funt, Samuel A., Kjeldsen, Julie Westerlin, Kverneland, Anders Handrup, Met, Özcan, Draghi, Arianna, Jakobsen, Søren Nyboe, Donia, Marco, Marie Svane, Inge, Hadrup, Sine Reker, Tvingsholm, Siri Amanda, Frej, Marcus Svensson, Rafa, Vibeke Mindahl, Hansen, Ulla Kring, Ormhøj, Maria, Tyron, Alexander, Jensen, Agnete W.P., Kadivar, Mohammad, Bentzen, Amalie Kai, Munk, Kamilla K., Aasbjerg, Gitte N., Ternander, Jeppe S.H., Heeke, Christina, Tamhane, Tripti, Schmess, Christian, Funt, Samuel A., Kjeldsen, Julie Westerlin, Kverneland, Anders Handrup, Met, Özcan, Draghi, Arianna, Jakobsen, Søren Nyboe, Donia, Marco, Marie Svane, Inge, and Hadrup, Sine Reker

Abstract

Background Adoptive cell therapy (ACT) has shown promising results for the treatment of cancer and viral infections. Successful ACT relies on ex vivo expansion of large numbers of desired T-cells with strong cytotoxic capacity and in vivo persistence, which constitutes the greatest challenge to current ACT strategies. Here, in this study, we present a novel technology for ex vivo expansion of antigen-specific T-cells; artificial antigen-presenting scaffolds (Ag-scaffolds) consisting of a dextran-polysaccharide backbone, decorated with combinations of peptide-Major Histocompatibility Complex (pMHC), cytokines and co-stimulatory molecules, enabling coordinated stimulation of antigen-specific T-cells. Methods The capacity of Ag-scaffolds to expand antigen-specific T-cells was explored in ex vivo cultures with peripheral blood mononuclear cells from healthy donors and patients with metastatic melanoma. The resulting T-cell products were assessed for phenotypic and functional characteristics. Results We identified an optimal Ag-scaffold for expansion of T-cells for ACT, carrying pMHC and interleukin-2 (IL-2) and IL-21, with which we efficiently expanded both virus-specific and tumor-specific CD8+ T cells from peripheral blood of healthy donors and patients, respectively. The resulting T-cell products were characterized by a high frequency of antigen-specific cells with high self-renewal capacity, low exhaustion, a multifunctional cytokine profile upon antigen-challenge and superior tumor killing capacity. This demonstrates that the coordinated stimuli provided by an optimized stoichiometry of TCR engaging (pMHC) and stimulatory (cytokine) moieties is essential to obtain desired T-cell characteristics. To generate an 'off-the-shelf' multitargeting Ag-scaffold product of relevance to patients with metastatic melanoma, we identified the 30 most frequently recognized shared HLA-A0201-restricted melanoma epitopes in a cohort of 87 patients. By combining these in an Ag-scaf

Published
2023

28. Ex vivo modulation of intact tumor fragments with anti-PD-1 and anti-CTLA-4 influences the expansion and specificity of tumor-infiltrating lymphocytes

Author

Hulen, Thomas Morgan, Friese, Christina, Kristensen, Nikolaj Pagh, Granhøj, Joachim Stoltenborg, Borch, Troels Holz, Peeters, Marlies J.W., Donia, Marco, Andersen, Mads Hald, Hadrup, Sine Reker, Svane, Inge Marie, Met, Özcan, Hulen, Thomas Morgan, Friese, Christina, Kristensen, Nikolaj Pagh, Granhøj, Joachim Stoltenborg, Borch, Troels Holz, Peeters, Marlies J.W., Donia, Marco, Andersen, Mads Hald, Hadrup, Sine Reker, Svane, Inge Marie, and Met, Özcan

Abstract

Checkpoint inhibition (CPI) therapy and adoptive cell therapy with autologous tumor-infiltrating lymphocytes (TIL-based ACT) are the two most effective immunotherapies for the treatment of metastatic melanoma. While CPI has been the dominating therapy in the past decade, TIL-based ACT is beneficial for individuals even after progression on previous immunotherapies. Given that notable differences in response have been made when used as a subsequent treatment, we investigated how the qualities of TILs changed when the ex vivo microenvironment of intact tumor fragments were modulated with checkpoint inhibitors targeting programmed death receptor 1 (PD-1) and cytotoxic T-lymphocyte-associated protein 4 (CTLA-4). Initially, we show that unmodified TILs from CPI-resistant individuals can be produced, are overwhelmingly terminally differentiated, and are capable of responding to tumor. We then investigate these properties in ex vivo checkpoint modulated TILs finding that that they retain these qualities. Lastly, we confirmed the specificity of the TILs to the highest responding tumor antigens, and identified this reactivity resides largely in CD39+CD69+ terminally differentiated populations. Overall, we found that anti-PD-1 will alter the proliferative capacity while anti-CTLA4 will influence breadth of antigen specificity.

Published
2023

29. of intact tumor fragments with anti-PD-1 and anti-CTLA-4 influences the expansion and specificity of tumor-infiltrating lymphocytes

Author

Hulen, Thomas Morgan, Friese, Christina, Kristensen, Nikolaj Pagh, Granhøj, Joachim Stoltenborg, Borch, Troels Holz, Peeters, Marlies J.W., Donia, Marco, Andersen, Mads Hald, Hadrup, Sine Reker, Svane, Inge Marie, Met, Özcan, Hulen, Thomas Morgan, Friese, Christina, Kristensen, Nikolaj Pagh, Granhøj, Joachim Stoltenborg, Borch, Troels Holz, Peeters, Marlies J.W., Donia, Marco, Andersen, Mads Hald, Hadrup, Sine Reker, Svane, Inge Marie, and Met, Özcan

Abstract

Checkpoint inhibition (CPI) therapy and adoptive cell therapy with autologous tumor-infiltrating lymphocytes (TIL-based ACT) are the two most effective immunotherapies for the treatment of metastatic melanoma. While CPI has been the dominating therapy in the past decade, TIL-based ACT is beneficial for individuals even after progression on previous immunotherapies. Given that notable differences in response have been made when used as a subsequent treatment, we investigated how the qualities of TILs changed when the ex vivo microenvironment of intact tumor fragments were modulated with checkpoint inhibitors targeting programmed death receptor 1 (PD-1) and cytotoxic T-lymphocyte-associated protein 4 (CTLA-4). Initially, we show that unmodified TILs from CPI-resistant individuals can be produced, are overwhelmingly terminally differentiated, and are capable of responding to tumor. We then investigate these properties in ex vivo checkpoint modulated TILs finding that that they retain these qualities. Lastly, we confirmed the specificity of the TILs to the highest responding tumor antigens, and identified this reactivity resides largely in CD39+CD69+ terminally differentiated populations. Overall, we found that anti-PD-1 will alter the proliferative capacity while anti-CTLA4 will influence breadth of antigen specificity.

Published
2023

30. Restoring tumor immunogenicity with dendritic cell reprogramming

Author

Zimmermannova, Olga, Ferreira, Alexandra G., Ascic, Ervin, Santiago, Marta Velasco, Kurochkin, Ilia, Hansen, Morten, Met, Özcan, Caiado, Inês, Shapiro, Ilja E., Michaux, Justine, Humbert, Marion, Soto-Cabrera, Diego, Benonisson, Hreinn, Silvério-Alves, Rita, Gomez-Jimenez, David, Bernardo, Carina, Bauden, Monika, Andersson, Roland, Höglund, Mattias, Miharada, Kenichi, Nakamura, Yukio, Hugues, Stephanie, Greiff, Lennart, Lindstedt, Malin, Rosa, Fábio F., Pires, Cristiana F., Bassani-Sternberg, Michal, Svane, Inge Marie, Pereira, Carlos Filipe, Zimmermannova, Olga, Ferreira, Alexandra G., Ascic, Ervin, Santiago, Marta Velasco, Kurochkin, Ilia, Hansen, Morten, Met, Özcan, Caiado, Inês, Shapiro, Ilja E., Michaux, Justine, Humbert, Marion, Soto-Cabrera, Diego, Benonisson, Hreinn, Silvério-Alves, Rita, Gomez-Jimenez, David, Bernardo, Carina, Bauden, Monika, Andersson, Roland, Höglund, Mattias, Miharada, Kenichi, Nakamura, Yukio, Hugues, Stephanie, Greiff, Lennart, Lindstedt, Malin, Rosa, Fábio F., Pires, Cristiana F., Bassani-Sternberg, Michal, Svane, Inge Marie, and Pereira, Carlos Filipe

Abstract

Decreased antigen presentation contributes to the ability of cancer cells to evade the immune system. We used the minimal gene regulatory network of type 1 conventional dendritic cells (cDC1) to reprogram cancer cells into professional antigen-presenting cells (tumor-APCs). Enforced expression of the transcription factors PU.1, IRF8, and BATF3 (PIB) was sufficient to induce the cDC1 phenotype in 36 cell lines derived from human and mouse hematological and solid tumors.Within 9 days of reprogramming, tumor-APCs acquired transcriptional and epigenetic programs associated with cDC1 cells. Reprogramming restored the expression of antigen presentation complexes and costimulatory molecules on the surfaces of tumor cells, allowing the presentation of endogenous tumor antigens on MHC-I and facilitating targeted killing by CD8+ T cells. Functionally, tumor-APCs engulfed and processed proteins and dead cells, secreted inflammatory cytokines, and cross-presented antigens to naïve CD8+ T cells. Human primary tumor cells could also be reprogrammed to increase their capability to present antigen and to activate patient-specific tumor-infiltrating lymphocytes. In addition to acquiring improved antigen presentation, tumor-APCs had impaired tumorigenicity in vitro and in vivo. Injection of in vitro generated melanoma-derived tumor-APCs into subcutaneous melanoma tumors delayed tumor growth and increased survival in mice. Antitumor immunity elicited by tumor-APCs was synergistic with immune checkpoint inhibitors. Our approach serves as a platform for the development of immunotherapies that endow cancer cells with the capability to process and present endogenous tumor antigens.

Published
2023

32. Tumor-Infiltrating Lymphocyte Therapy or Ipilimumab in Advanced Melanoma

Author

Rohaan, Maartje W., primary, Borch, Troels H., additional, van den Berg, Joost H., additional, Met, Özcan, additional, Kessels, Rob, additional, Geukes Foppen, Marnix H., additional, Stoltenborg Granhøj, Joachim, additional, Nuijen, Bastiaan, additional, Nijenhuis, Cynthia, additional, Jedema, Inge, additional, van Zon, Maaike, additional, Scheij, Saskia, additional, Beijnen, Jos H., additional, Hansen, Marten, additional, Voermans, Carlijn, additional, Noringriis, Inge M., additional, Monberg, Tine J., additional, Holmstroem, Rikke B., additional, Wever, Lidwina D.V., additional, van Dijk, Marloes, additional, Grijpink-Ongering, Lindsay G., additional, Valkenet, Ludy H.M., additional, Torres Acosta, Alejandro, additional, Karger, Matthias, additional, Borgers, Jessica S.W., additional, ten Ham, Renske M.T., additional, Retèl, Valesca P., additional, van Harten, Wim H., additional, Lalezari, Ferry, additional, van Tinteren, Harm, additional, van der Veldt, Astrid A.M., additional, Hospers, Geke A.P., additional, Stevense-den Boer, Marion A.M., additional, Suijkerbuijk, Karijn P.M., additional, Aarts, Maureen J.B., additional, Piersma, Djura, additional, van den Eertwegh, Alfons J.M., additional, de Groot, Jan-Willem B., additional, Vreugdenhil, Gerard, additional, Kapiteijn, Ellen, additional, Boers-Sonderen, Marye J., additional, Fiets, W. Edward, additional, van den Berkmortel, Franchette W.P.J., additional, Ellebaek, Eva, additional, Hölmich, Lisbet R., additional, van Akkooi, Alexander C.J., additional, van Houdt, Winan J., additional, Wouters, Michel W.J.M., additional, van Thienen, Johannes V., additional, Blank, Christian U., additional, Meerveld-Eggink, Aafke, additional, Klobuch, Sebastian, additional, Wilgenhof, Sofie, additional, Schumacher, Ton N., additional, Donia, Marco, additional, Svane, Inge Marie, additional, and Haanen, John B.A.G., additional

Published
2022
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33. Anti-PD-L1/PD-L2 therapeutic vaccination in untreated chronic lymphocytic leukemia patients with unmutated IgHV

Author

Klausen, Uffe, primary, Grauslund, Jacob Handlos, additional, Jørgensen, Nicolai Grønne Dahlager, additional, Ahmad, Shamaila Munir, additional, Jonassen, Merete, additional, Weis-Banke, Stine Emilie, additional, Martinenaite, Evelina, additional, Pedersen, Lone Bredo, additional, Lisle, Thomas Landkildehus, additional, Gang, Anne Ortved, additional, Enggaard, Lisbeth, additional, Hansen, Morten, additional, Holmström, Morten Orebo, additional, Met, Özcan, additional, Svane, Inge Marie, additional, Niemann, Carsten Utoft, additional, Pedersen, Lars Møller, additional, and Andersen, Mads Hald, additional

Published
2022
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35. 343 Identification of tumor-reactive T cells targeting melanoma Dark Antigens™ validates this novel class of targets for development of immunotherapies

Author

Abbott, Rachel, primary, Hofland, Tom, additional, Hulen, Thomas, additional, Verdegaal, Elizabeth (Els), additional, Crowther, Michael, additional, Dukes, Joseph, additional, Khan, Shawez, additional, Kok, Pita de, additional, Masi, Giulia, additional, Met, Özcan, additional, Schina, Aimilia, additional, Selvadurai, Hayden, additional, Visser, Marten, additional, Ward, Katarzyna, additional, Abbott, Rachel, additional, Burg, Sjoerd van der, additional, Kassiotis, George, additional, and Svane, Inge, additional

Published
2022
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37. Arginase-2-specific cytotoxic T cells specifically recognize functional regulatory T cells

Author

Weis-Banke, Stine Emilie, primary, Lisle, Thomas Landkildehus, additional, Perez-Penco, Maria, additional, Schina, Aimilia, additional, Hübbe, Mie Linder, additional, Siersbæk, Majken, additional, Holmström, Morten Orebo, additional, Jørgensen, Mia Aaboe, additional, Marie Svane, Inge, additional, Met, Özcan, additional, Ødum, Niels, additional, Madsen, Daniel Hargbøl, additional, Donia, Marco, additional, Grøntved, Lars, additional, and Andersen, Mads Hald, additional

Published
2022
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38. Calreticulin mutant myeloproliferative neoplasms induce MHC-I skewing, which can be overcome by an optimized peptide cancer vaccine

Author

Gigoux, Mathieu, primary, Holmström, Morten O., additional, Zappasodi, Roberta, additional, Park, Joseph J., additional, Pourpe, Stephane, additional, Bozkus, Cansu Cimen, additional, Mangarin, Levi M. B., additional, Redmond, David, additional, Verma, Svena, additional, Schad, Sara, additional, George, Mariam M., additional, Venkatesh, Divya, additional, Ghosh, Arnab, additional, Hoyos, David, additional, Molvi, Zaki, additional, Kamaz, Baransel, additional, Marneth, Anna E., additional, Duke, William, additional, Leventhal, Matthew J., additional, Jan, Max, additional, Ho, Vincent T., additional, Hobbs, Gabriela S., additional, Knudsen, Trine Alma, additional, Skov, Vibe, additional, Kjær, Lasse, additional, Larsen, Thomas Stauffer, additional, Hansen, Dennis Lund, additional, Lindsley, R. Coleman, additional, Hasselbalch, Hans, additional, Grauslund, Jacob H., additional, Lisle, Thomas L., additional, Met, Özcan, additional, Wilkinson, Patrick, additional, Greenbaum, Benjamin, additional, Sepulveda, Manuel A., additional, Chan, Timothy, additional, Rampal, Raajit, additional, Andersen, Mads H., additional, Abdel-Wahab, Omar, additional, Bhardwaj, Nina, additional, Wolchok, Jedd D., additional, Mullally, Ann, additional, and Merghoub, Taha, additional

Published
2022
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39. Met, Özcan

Author

Met, Özcan and Met, Özcan

Published
2022

40. Tumor-Infiltrating Lymphocyte Therapy or Ipilimumab in Advanced Melanoma

Author

Rohaan, Maartje W, Borch, Troels H, van den Berg, Joost H, Met, Özcan, Kessels, Rob, Geukes Foppen, Marnix H, Stoltenborg Granhøj, Joachim, Nuijen, Bastiaan, Nijenhuis, Cynthia, Jedema, Inge, van Zon, Maaike, Scheij, Saskia, Beijnen, Jos H, Hansen, Marten, Voermans, Carlijn, Noringriis, Inge M, Monberg, Tine J, Holmstroem, Rikke B, Wever, Lidwina D V, van Dijk, Marloes, Grijpink-Ongering, Lindsay G, Valkenet, Ludy H M, Torres Acosta, Alejandro, Karger, Matthias, Borgers, Jessica S W, Ten Ham, Renske M T, Retèl, Valesca P, van Harten, Wim H, Lalezari, Ferry, van Tinteren, Harm, van der Veldt, Astrid A M, Hospers, Geke A P, Stevense-den Boer, Marion A M, Suijkerbuijk, Karijn P M, Aarts, Maureen J B, Piersma, Djura, van den Eertwegh, Alfons J M, de Groot, Jan-Willem B, Vreugdenhil, Gerard, Kapiteijn, Ellen, Boers-Sonderen, Marye J, Fiets, W Edward, van den Berkmortel, Franchette W P J, Ellebaek, Eva, Hölmich, Lisbet R, van Akkooi, Alexander C J, van Houdt, Winan J, Wouters, Michel W J M, van Thienen, Johannes V, Blank, Christian U, Meerveld-Eggink, Aafke, Klobuch, Sebastian, Wilgenhof, Sofie, Schumacher, Ton N, Donia, Marco, Svane, Inge Marie, Haanen, John B A G, Rohaan, Maartje W, Borch, Troels H, van den Berg, Joost H, Met, Özcan, Kessels, Rob, Geukes Foppen, Marnix H, Stoltenborg Granhøj, Joachim, Nuijen, Bastiaan, Nijenhuis, Cynthia, Jedema, Inge, van Zon, Maaike, Scheij, Saskia, Beijnen, Jos H, Hansen, Marten, Voermans, Carlijn, Noringriis, Inge M, Monberg, Tine J, Holmstroem, Rikke B, Wever, Lidwina D V, van Dijk, Marloes, Grijpink-Ongering, Lindsay G, Valkenet, Ludy H M, Torres Acosta, Alejandro, Karger, Matthias, Borgers, Jessica S W, Ten Ham, Renske M T, Retèl, Valesca P, van Harten, Wim H, Lalezari, Ferry, van Tinteren, Harm, van der Veldt, Astrid A M, Hospers, Geke A P, Stevense-den Boer, Marion A M, Suijkerbuijk, Karijn P M, Aarts, Maureen J B, Piersma, Djura, van den Eertwegh, Alfons J M, de Groot, Jan-Willem B, Vreugdenhil, Gerard, Kapiteijn, Ellen, Boers-Sonderen, Marye J, Fiets, W Edward, van den Berkmortel, Franchette W P J, Ellebaek, Eva, Hölmich, Lisbet R, van Akkooi, Alexander C J, van Houdt, Winan J, Wouters, Michel W J M, van Thienen, Johannes V, Blank, Christian U, Meerveld-Eggink, Aafke, Klobuch, Sebastian, Wilgenhof, Sofie, Schumacher, Ton N, Donia, Marco, Svane, Inge Marie, and Haanen, John B A G

Abstract

Background Immune checkpoint inhibitors and targeted therapies have dramatically improved outcomes in patients with advanced melanoma, but approximately half these patients will not have a durable benefit. Phase 1-2 trials of adoptive cell therapy with tumor-infiltrating lymphocytes (TILs) have shown promising responses, but data from phase 3 trials are lacking to determine the role of TILs in treating advanced melanoma. Methods In this phase 3, multicenter, open-label trial, we randomly assigned patients with unresectable stage IIIC or IV melanoma in a 1:1 ratio to receive TIL or anti-cytotoxic T-lymphocyte antigen 4 therapy (ipilimumab at 3 mg per kilogram of body weight). Infusion of at least 5×109 TILs was preceded by nonmyeloablative, lymphodepleting chemotherapy (cyclophosphamide plus fludarabine) and followed by high-dose interleukin-2. The primary end point was progression-free survival. Results A total of 168 patients (86% with disease refractory to anti-programmed death 1 treatment) were assigned to receive TILs (84 patients) or ipilimumab (84 patients). In the intention-to-treat population, median progression-free survival was 7.2 months (95% confidence interval [CI], 4.2 to 13.1) in the TIL group and 3.1 months (95% CI, 3.0 to 4.3) in the ipilimumab group (hazard ratio for progression or death, 0.50; 95% CI, 0.35 to 0.72; P<0.001); 49% (95% CI, 38 to 60) and 21% (95% CI, 13 to 32) of the patients, respectively, had an objective response. Median overall survival was 25.8 months (95% CI, 18.2 to not reached) in the TIL group and 18.9 months (95% CI, 13.8 to 32.6) in the ipilimumab group. Treatment-related adverse events of grade 3 or higher occurred in all patients who received TILs and in 57% of those who received ipilimumab; in the TIL group, these events were mainly chemotherapy-related myelosuppression. Conclusions In patients with advanced melanoma, progression-free survival was significantly longer among those who received TIL therapy than amon

Published
2022

41. Tumor-Infiltrating Lymphocyte Therapy or Ipilimumab in Advanced Melanoma.

Author

Rohaan, Maartje W., Borch, Troels H., Van Den Berg, Joost H., Met, Özcan, Kessels, Rob, Geukes Foppen, Marnix H., Stoltenborg Granhøj, Joachim, Nuijen, Bastiaan, Nijenhuis, Cynthia, Jedema, Inge, Van Zon, Maaike, Scheij, Saskia, Beijnen, Jos H., Hansen, Marten, Voermans, Carlijn, Noringriis, Inge M., Monberg, Tine J., Holmstroem, Rikke B., Wever, Lidwina D.V., Van Dijk, Marloes, Grijpink-Ongering, Lindsay G., Valkenet, Ludy H.M., Torres Acosta, Alejandro, Karger, Matthias, Borgers, Jessica S.W., Ten Ham, Renske M.T., Retèl, Valesca P., Van Harten, Wim H., Lalezari, Ferry, Van Tinteren, Harm, Van Der Veldt, Astrid A.M., Hospers, Geke A.P., Stevense-Den Boer, Marion A.M., Suijkerbuijk, Karijn P.M., Aarts, Maureen J.B., Piersma, Djura, Van Den Eertwegh, Alfons J.M., De Groot, Jan Willem B., Vreugdenhil, Gerard, Kapiteijn, Ellen, Boers-Sonderen, Marye J., Fiets, W. Edward, Van Den Berkmortel, Franchette W.P.J., Ellebaek, Eva, Hölmich, Lisbet R., Van Akkooi, Alexander C.J., Van Houdt, Winan J., Wouters, Michel W.J.M., Van Thienen, Johannes V., Blank, Christian U., Meerveld-Eggink, Aafke, Klobuch, Sebastian, Wilgenhof, Sofie, Schumacher, Ton N., Donia, Marco, Svane, Inge Marie, Haanen, John B.A.G., Rohaan, Maartje W., Borch, Troels H., Van Den Berg, Joost H., Met, Özcan, Kessels, Rob, Geukes Foppen, Marnix H., Stoltenborg Granhøj, Joachim, Nuijen, Bastiaan, Nijenhuis, Cynthia, Jedema, Inge, Van Zon, Maaike, Scheij, Saskia, Beijnen, Jos H., Hansen, Marten, Voermans, Carlijn, Noringriis, Inge M., Monberg, Tine J., Holmstroem, Rikke B., Wever, Lidwina D.V., Van Dijk, Marloes, Grijpink-Ongering, Lindsay G., Valkenet, Ludy H.M., Torres Acosta, Alejandro, Karger, Matthias, Borgers, Jessica S.W., Ten Ham, Renske M.T., Retèl, Valesca P., Van Harten, Wim H., Lalezari, Ferry, Van Tinteren, Harm, Van Der Veldt, Astrid A.M., Hospers, Geke A.P., Stevense-Den Boer, Marion A.M., Suijkerbuijk, Karijn P.M., Aarts, Maureen J.B., Piersma, Djura, Van Den Eertwegh, Alfons J.M., De Groot, Jan Willem B., Vreugdenhil, Gerard, Kapiteijn, Ellen, Boers-Sonderen, Marye J., Fiets, W. Edward, Van Den Berkmortel, Franchette W.P.J., Ellebaek, Eva, Hölmich, Lisbet R., Van Akkooi, Alexander C.J., Van Houdt, Winan J., Wouters, Michel W.J.M., Van Thienen, Johannes V., Blank, Christian U., Meerveld-Eggink, Aafke, Klobuch, Sebastian, Wilgenhof, Sofie, Schumacher, Ton N., Donia, Marco, Svane, Inge Marie, and Haanen, John B.A.G.

Abstract

Background Immune checkpoint inhibitors and targeted therapies have dramatically improved outcomes in patients with advanced melanoma, but approximately half these patients will not have a durable benefit. Phase 1-2 trials of adoptive cell therapy with tumor-infiltrating lymphocytes (TILs) have shown promising responses, but data from phase 3 trials are lacking to determine the role of TILs in treating advanced melanoma. Methods In this phase 3, multicenter, open-label trial, we randomly assigned patients with unresectable stage IIIC or IV melanoma in a 1:1 ratio to receive TIL or anti-cytotoxic T-lymphocyte antigen 4 therapy (ipilimumab at 3 mg per kilogram of body weight). Infusion of at least 5×109 TILs was preceded by nonmyeloablative, lymphodepleting chemotherapy (cyclophosphamide plus fludarabine) and followed by high-dose interleukin-2. The primary end point was progression-free survival. Results A total of 168 patients (86% with disease refractory to anti-programmed death 1 treatment) were assigned to receive TILs (84 patients) or ipilimumab (84 patients). In the intention-to-treat population, median progression-free survival was 7.2 months (95% confidence interval [CI], 4.2 to 13.1) in the TIL group and 3.1 months (95% CI, 3.0 to 4.3) in the ipilimumab group (hazard ratio for progression or death, 0.50; 95% CI, 0.35 to 0.72; P<0.001); 49% (95% CI, 38 to 60) and 21% (95% CI, 13 to 32) of the patients, respectively, had an objective response. Median overall survival was 25.8 months (95% CI, 18.2 to not reached) in the TIL group and 18.9 months (95% CI, 13.8 to 32.6) in the ipilimumab group. Treatment-related adverse events of grade 3 or higher occurred in all patients who received TILs and in 57% of those who received ipilimumab; in the TIL group, these events were mainly chemotherapy-related myelosuppression. Conclusions In patients with advanced melanoma, progression-free survival was significantly longer among those who received TIL therapy than amon

Published
2022

42. Clinical advances and ongoing trials on mRNA vaccines for cancer treatment

Author

Lorentzen, Cathrine Lund, Haanen, John B., Met, Özcan, Svane, Inge Marie, Lorentzen, Cathrine Lund, Haanen, John B., Met, Özcan, and Svane, Inge Marie

Abstract

Years of research exploring mRNA vaccines for cancer treatment in preclinical and clinical trials have set the stage for the rapid development of mRNA vaccines during the COVID-19 pandemic. Therapeutic cancer vaccines based on mRNA are well tolerated, and the inherent advantage in ease of production, which rivals the best available conventional vaccine manufacture methods, renders mRNA vaccines a promising option for cancer immunotherapy. Technological advances have optimised mRNA-based vaccine stability, structure, and delivery methods, and multiple clinical trials investigating mRNA vaccine therapy are now enrolling patients with various cancer diagnoses. Although therapeutic mRNA-based cancer vaccines have not yet been approved for standard treatment, encouraging results from early clinical trials with mRNA vaccines as monotherapy and in combination with checkpoint inhibitors have been obtained. This Review summarises the latest clinical advances in mRNA-based vaccines for cancer treatment and reflects on future perspectives and challenges for this new and promising treatment approach.

Published
2022

43. Anti-PD-L1/PD-L2 therapeutic vaccination in untreated chronic lymphocytic leukemia patients with unmutated IgHV

Author

Klausen, Uffe, Grauslund, Jacob Handlos, Jørgensen, Nicolai Grønne Dahlager, Ahmad, Shamaila Munir, Jonassen, Merete, Weis-Banke, Stine Emilie, Martinenaite, Evelina, Pedersen, Lone Bredo, Lisle, Thomas Landkildehus, Gang, Anne Ortved, Enggaard, Lisbeth, Hansen, Morten, Holmström, Morten Orebo, Met, Özcan, Svane, Inge Marie, Niemann, Carsten Utoft, Pedersen, Lars Møller, Andersen, Mads Hald, Klausen, Uffe, Grauslund, Jacob Handlos, Jørgensen, Nicolai Grønne Dahlager, Ahmad, Shamaila Munir, Jonassen, Merete, Weis-Banke, Stine Emilie, Martinenaite, Evelina, Pedersen, Lone Bredo, Lisle, Thomas Landkildehus, Gang, Anne Ortved, Enggaard, Lisbeth, Hansen, Morten, Holmström, Morten Orebo, Met, Özcan, Svane, Inge Marie, Niemann, Carsten Utoft, Pedersen, Lars Møller, and Andersen, Mads Hald

Abstract

Chronic lymphocytic leukemia (CLL) patients with unmutated immunoglobulin heavy chain (IgHV) are at risk of early disease progression compared to patients with mutated IgHV. As a preventive strategy, we treated 19 previously untreated CLL patients with unmutated IgHV in a phase 1/2 trial (clinicaltrials.gov, NCT03939234) exploring the efficacy and toxicity of a therapeutic cancer vaccine containing peptides derived from programmed death ligand 1 (PD-L1) and ligand 2 (PD-L2), hoping to restore immunological control of the disease. According to the International Workshop on Chronic lymphocytic Leukemia (iwCLL) response criteria, no patients obtained a response; however, during follow-up, one patient had complete normalization of the peripheral lymphocyte count and remained in biochemical remission after a follow-up time of 15 months. At the end of treatment, one patient had progressed, and 17 patients had stable disease. During follow-up with a median time of 23.5 months since inclusion, seven patients had progressed, and eight patients had stable disease. The median time to first treatment (TTFT) from diagnosis was 90.3 months with a median follow-up time of 50.1 months. This apparent favorable outcome in TTFT needs to be investigated in a randomized setting, as our population may have been biased. More than 80% of patients obtained vaccine-specific immune responses, confirming the immunogenicity of the vaccine. The vaccine was generally well tolerated with only grade I–II adverse events. Although there were some signs of clinical effects, the vaccine seems to be insufficient as monotherapy in CLL, possibly due to a high tumor burden. The efficacy of the vaccine should preferably be tested in combination with novel targeted therapies or as a consolidating treatment.

Published
2022

44. Calreticulin mutant myeloproliferative neoplasms induce MHC-I skewing, which can be overcome by an optimized peptide cancer vaccine

Author

Gigoux, Mathieu, Holmström, Morten O., Zappasodi, Roberta, Park, Joseph J., Pourpe, Stephane, Bozkus, Cansu Cimen, Mangarin, Levi M.B., Redmond, David, Verma, Svena, Schad, Sara, George, Mariam M., Venkatesh, Divya, Ghosh, Arnab, Hoyos, David, Molvi, Zaki, Kamaz, Baransel, Marneth, Anna E., Duke, William, Leventhal, Matthew J., Jan, Max, Ho, Vincent T., Hobbs, Gabriela S., Knudsen, Trine Alma, Skov, Vibe, Kjær, Lasse, Larsen, Thomas Stauffer, Hansen, Dennis Lund, Lindsley, R. Coleman, Hasselbalch, Hans, Grauslund, Jacob H., Lisle, Thomas L., Met, Özcan, Wilkinson, Patrick, Greenbaum, Benjamin, Sepulveda, Manuel A., Chan, Timothy, Rampal, Raajit, Andersen, Mads H., Abdel-Wahab, Omar, Bhardwaj, Nina, Wolchok, Jedd D., Mullally, Ann, Merghoub, Taha, Gigoux, Mathieu, Holmström, Morten O., Zappasodi, Roberta, Park, Joseph J., Pourpe, Stephane, Bozkus, Cansu Cimen, Mangarin, Levi M.B., Redmond, David, Verma, Svena, Schad, Sara, George, Mariam M., Venkatesh, Divya, Ghosh, Arnab, Hoyos, David, Molvi, Zaki, Kamaz, Baransel, Marneth, Anna E., Duke, William, Leventhal, Matthew J., Jan, Max, Ho, Vincent T., Hobbs, Gabriela S., Knudsen, Trine Alma, Skov, Vibe, Kjær, Lasse, Larsen, Thomas Stauffer, Hansen, Dennis Lund, Lindsley, R. Coleman, Hasselbalch, Hans, Grauslund, Jacob H., Lisle, Thomas L., Met, Özcan, Wilkinson, Patrick, Greenbaum, Benjamin, Sepulveda, Manuel A., Chan, Timothy, Rampal, Raajit, Andersen, Mads H., Abdel-Wahab, Omar, Bhardwaj, Nina, Wolchok, Jedd D., Mullally, Ann, and Merghoub, Taha

Abstract

The majority of JAK2V617F-negative myeloproliferative neoplasms (MPNs) have disease-initiating frameshift mutations in calreticulin (CALR), resulting in a common carboxyl-terminal mutant fragment (CALRMUT), representing an attractive source of neoantigens for cancer vaccines. However, studies have shown that CALRMUT-specific T cells are rare in patients with CALRMUT MPN for unknown reasons. We examined class I major histocompatibility complex (MHC-I) allele frequencies in patients with CALRMUT MPN from two independent cohorts. We observed that MHC-I alleles that present CALRMUT neoepitopes with high affinity are underrepresented in patients with CALRMUT MPN. We speculated that this was due to an increased chance of immune-mediated tumor rejection by individuals expressing one of these MHC-I alleles such that the disease never clinically manifested. As a consequence of this MHC-I allele restriction, we reasoned that patients with CALRMUT MPN would not efficiently respond to a CALRMUT fragment cancer vaccine but would when immunized with a modified CALRMUT heteroclitic peptide vaccine approach. We found that heteroclitic CALRMUT peptides specifically designed for the MHC-I alleles of patients with CALRMUT MPN efficiently elicited a CALRMUT cross-reactive CD8+ T cell response in human peripheral blood samples but not to the matched weakly immunogenic CALRMUT native peptides. We corroborated this effect in vivo in mice and observed that C57BL/6J mice can mount a CD8+ T cell response to the CALRMUT fragment upon immunization with a CALRMUT heteroclitic, but not native, peptide. Together, our data emphasize the therapeutic potential of heteroclitic peptide–based cancer vaccines in patients with CALRMUT MPN.

Published
2022

45. Tumor-infiltrating lymphocytes for adoptive cell therapy:recent advances, challenges, and future directions

Author

Granhøj, Joachim Stoltenborg, Witness Præst Jensen, Agnete, Presti, Mario, Met, Özcan, Svane, Inge Marie, Donia, Marco, Granhøj, Joachim Stoltenborg, Witness Præst Jensen, Agnete, Presti, Mario, Met, Özcan, Svane, Inge Marie, and Donia, Marco

Abstract

Introduction: Adoptive cell therapy (ACT) with tumor-infiltrating lymphocytes (TILs) is a highly personalized type of cancer immunotherapy. TIL-based ACT exploits naturally occurring TILs, derived from the patients’ tumor. This treatment has shown consistent clinical responses in melanoma, and recent results point toward a potential use in multiple cancer diagnoses. However, several limitations have restricted the clinical development and adaptation of TIL-based ACT. Areas covered: In this review, we present the principles of TIL-based ACT and discuss the most significant limitations for therapeutic efficacy and its widespread application. The topics of therapeutic resistance (both innate and acquired), treatment-related toxicity, and the novel research topic of metabolic barriers in the tumor microenvironment (TME) are covered. Expert opinion: There are many ongoing areas of research focusing on improving clinical efficacy and optimizing TIL-based ACT. Many strategies have shown a great potential, particularly strategies advancing TIL efficacy (such as increasing and harnessing ex vivo the sub-population of tumor-reactive TILs) and manufacturing processes. Novel approaches can help overcome current limitations and potentially result in TIL-based ACT entering the mainstream of cancer therapy across tumor types.

Published
2022

46. Highly efficient PD-1-targeted CRISPR-Cas9 for tumor-infiltrating lymphocyte-based adoptive T cell therapy

Author

Chamberlain, Christopher Aled, Bennett, Eric Paul, Kverneland, Anders Handrup, Svane, Inge Marie, Donia, Marco, Met, Özcan, Chamberlain, Christopher Aled, Bennett, Eric Paul, Kverneland, Anders Handrup, Svane, Inge Marie, Donia, Marco, and Met, Özcan

Abstract

Adoptive T cell therapy (ACT) with expanded tumor-infiltrating lymphocytes (TIL) can induce durable responses in cancer patients from multiple histologies, with response rates of up to 50%. Antibodies blocking the engagement of the inhibitory receptor programmed cell death protein 1 (PD-1) have been successful across a variety of cancer diagnoses. We hypothesized that these approaches could be combined by using CRISPR-Cas9 gene editing to knock out PD-1 in TILs from metastatic melanoma and head-and-neck, thyroid, and colorectal cancer. Non-viral, non-plasmid-based PD-1 knockout was carried out immediately prior to the traditional 14-day TIL-based ACT rapid-expansion protocol. A median 87.53% reduction in cell surface PD-1 expression was observed post-expansion and confirmed at the genomic level. No off-target editing was detected, and PD-1 knockout had no effect on final fold expansion. Edited cells exhibited few phenotypic differences and matched control functionality. Pre-clinical-scale results were confirmed at a clinical scale by generating a PD-1-deficient TIL product using the good manufacturing practice facilities, equipment, procedures, and starting material used for standard patient treatment. Our results demonstrate that simple, non-viral, non-plasmid-based CRISPR-Cas9 methods can be feasibly adopted into a TIL-based ACT protocol to produce treatment products deficient in molecules such as PD-1, without any evident negative effects.

Published
2022

47. Peptide vaccination activating Galectin-3-specific T cells offers a novel means to target Galectin-3-expressing cells in the tumor microenvironment

Author

Bendtsen, Simone Kloch, Perez-Penco, Maria, Hübbe, Mie Linder, Martinenaite, Evelina, Orebo Holmström, Morten, Weis-Banke, Stine Emilie, Grønne Dahlager Jørgensen, Nicolai, Jørgensen, Mia Aaboe, Munir Ahmad, Shamaila, Jensen, Kasper Mølgaard, Friese, Christina, Lundsager, Mia Thorup, Johansen, Astrid Zedlitz, Carretta, Marco, Ødum, Niels, Met, Özcan, Svane, Inge Marie, Madsen, Daniel Hargbøl, Andersen, Mads Hald, Bendtsen, Simone Kloch, Perez-Penco, Maria, Hübbe, Mie Linder, Martinenaite, Evelina, Orebo Holmström, Morten, Weis-Banke, Stine Emilie, Grønne Dahlager Jørgensen, Nicolai, Jørgensen, Mia Aaboe, Munir Ahmad, Shamaila, Jensen, Kasper Mølgaard, Friese, Christina, Lundsager, Mia Thorup, Johansen, Astrid Zedlitz, Carretta, Marco, Ødum, Niels, Met, Özcan, Svane, Inge Marie, Madsen, Daniel Hargbøl, and Andersen, Mads Hald

Abstract

Galectin-3 (Gal3) can be expressed by many cells in the tumor microenvironment (TME), including cancer cells, cancer-associated fibroblasts, tumor-associated macrophages, and regulatory T cells (Tregs). In addition to immunosuppression, Gal3 expression has been connected to malignant cell transformation, tumor progression, and metastasis. In the present study, we found spontaneous T-cell responses against Gal3-derived peptides in PBMCs from both healthy donors and cancer patients. We isolated and expanded these Gal3-specific T cells in vitro and showed that they could directly recognize target cells that expressed Gal3. Finally, therapeutic vaccination with a long Gal3-derived peptide epitope, which induced the expansion of Gal3-specific CD8+ T cells in vivo, showed a significant tumor-growth delay in mice inoculated with EO771.LMB metastatic mammary tumor cells. This was associated with a significantly lower percentage of both Tregs and tumor-infiltrating Gal3+ cells in the non-myeloid CD45+CD11b− compartment and with an alteration of the T-cell memory populations in the spleens of Gal3-vaccinated mice. These results suggest that by activating Gal3-specific T cells by an immune-modulatory vaccination, we can target Gal3-producing cells in the TME, and thereby induce a more immune permissive TME. This indicates that Gal3 could be a novel target for therapeutic cancer vaccines.

Published
2022

48. Tumor-Infiltrating Lymphocyte Therapy or Ipilimumab in Advanced Melanoma

Author

HEE, MS Medische Oncologie, Cancer, Infection & Immunity, Rohaan, Maartje W, Borch, Troels H, van den Berg, Joost H, Met, Özcan, Kessels, Rob, Geukes Foppen, Marnix H, Stoltenborg Granhøj, Joachim, Nuijen, Bastiaan, Nijenhuis, Cynthia, Jedema, Inge, van Zon, Maaike, Scheij, Saskia, Beijnen, Jos H, Hansen, Marten, Voermans, Carlijn, Noringriis, Inge M, Monberg, Tine J, Holmstroem, Rikke B, Wever, Lidwina D V, van Dijk, Marloes, Grijpink-Ongering, Lindsay G, Valkenet, Ludy H M, Torres Acosta, Alejandro, Karger, Matthias, Borgers, Jessica S W, Ten Ham, Renske M T, Retèl, Valesca P, van Harten, Wim H, Lalezari, Ferry, van Tinteren, Harm, van der Veldt, Astrid A M, Hospers, Geke A P, Stevense-den Boer, Marion A M, Suijkerbuijk, Karijn P M, Aarts, Maureen J B, Piersma, Djura, van den Eertwegh, Alfons J M, de Groot, Jan-Willem B, Vreugdenhil, Gerard, Kapiteijn, Ellen, Boers-Sonderen, Marye J, Fiets, W Edward, van den Berkmortel, Franchette W P J, Ellebaek, Eva, Hölmich, Lisbet R, van Akkooi, Alexander C J, van Houdt, Winan J, Wouters, Michel W J M, van Thienen, Johannes V, Blank, Christian U, Meerveld-Eggink, Aafke, Klobuch, Sebastian, Wilgenhof, Sofie, Schumacher, Ton N, Donia, Marco, Svane, Inge Marie, Haanen, John B A G, HEE, MS Medische Oncologie, Cancer, Infection & Immunity, Rohaan, Maartje W, Borch, Troels H, van den Berg, Joost H, Met, Özcan, Kessels, Rob, Geukes Foppen, Marnix H, Stoltenborg Granhøj, Joachim, Nuijen, Bastiaan, Nijenhuis, Cynthia, Jedema, Inge, van Zon, Maaike, Scheij, Saskia, Beijnen, Jos H, Hansen, Marten, Voermans, Carlijn, Noringriis, Inge M, Monberg, Tine J, Holmstroem, Rikke B, Wever, Lidwina D V, van Dijk, Marloes, Grijpink-Ongering, Lindsay G, Valkenet, Ludy H M, Torres Acosta, Alejandro, Karger, Matthias, Borgers, Jessica S W, Ten Ham, Renske M T, Retèl, Valesca P, van Harten, Wim H, Lalezari, Ferry, van Tinteren, Harm, van der Veldt, Astrid A M, Hospers, Geke A P, Stevense-den Boer, Marion A M, Suijkerbuijk, Karijn P M, Aarts, Maureen J B, Piersma, Djura, van den Eertwegh, Alfons J M, de Groot, Jan-Willem B, Vreugdenhil, Gerard, Kapiteijn, Ellen, Boers-Sonderen, Marye J, Fiets, W Edward, van den Berkmortel, Franchette W P J, Ellebaek, Eva, Hölmich, Lisbet R, van Akkooi, Alexander C J, van Houdt, Winan J, Wouters, Michel W J M, van Thienen, Johannes V, Blank, Christian U, Meerveld-Eggink, Aafke, Klobuch, Sebastian, Wilgenhof, Sofie, Schumacher, Ton N, Donia, Marco, Svane, Inge Marie, and Haanen, John B A G

Published
2022

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