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5. The CALR mutations enhance the expression of the immunosuppressive proteins GARP and LAP on peripheral blood lymphocytes through increased binding of activated platelets.

Author

Holmström, Morten Orebo, Ruders, Josephine Hallundbæk, Riley, Caroline Hasselbalch, Larsen, Morten Kranker, Grauslund, Jacob Handlos, Kjær, Lasse, Skov, Vibe, Ellervik, Christina, Guo, Belinda B., Linden, Matthew, Hasselbalch, Hans Carl, and Andersen, Mads Hald

Subjects
TRANSFORMING growth factors-beta, GENE expression, PLATELET count, MYELOPROLIFERATIVE neoplasms, PEPTIDES
Abstract

Summary: Recently, an antibody which inhibits the glycoprotein A repetitions predominant (GARP)‐mediated release of active transforming growth factor beta (TGFβ) from the TGFβ propeptide latency‐associated peptide (LAP) showed preclinical activity in a murine model of the chronic myeloproliferative neoplasms (MPN). Consequently, we investigated the expression of the immunosuppressive molecules LAP and GARP on peripheral blood lymphocytes from 56 MPN patients and 11 healthy donors (HD). We found that lymphocytes from patients with MPN express higher levels of LAP and GARP with no strong differences found between the different MPN diagnoses. The impact of clinical parameters on the expression of LAP and GARP by lymphocytes showed that patients with calreticulin (CALR)mut MPN have increased expression compared with HD and patients with the Januskinase2 (JAK2) mutation. The fraction of lymphocytes bound to activated platelets (aPLT) strongly correlate to LAP and GARP expression suggesting that it is not the lymphocytes themselves but aPLT, which confer the increased expression of GARP and LAP on MPN patient lymphocytes. Notably, no differences in neither platelet counts nor anti‐thrombotic therapy was identified between patients with JAK2‐ and CALRmut patients. Analysis of platelet gene expression failed to identify differences in expression of relevant genes between JAK2‐ and CALRmut patients. [ABSTRACT FROM AUTHOR]

Published
2024
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6. Increased myeloid‐derived suppressor cell activation in clonal cytopenia of undetermined significance and low‐risk myelodysplastic syndrome.

Author

Bentivegna, Sofia, Côme, Christophe, Porse, Bo, Andersen, Mads Hald, and Grønbæk, Kirsten

Subjects
REGULATORY T cells, MYELOID-derived suppressor cells, SUPPRESSOR cells, IMMUNE checkpoint proteins, IMMUNOLOGIC memory, AZACITIDINE
Abstract

The article discusses the presence of myeloid-derived suppressor cells (MDSCs) in patients with clonal cytopenia of undetermined significance (CCUS) and low-risk myelodysplastic syndrome (LR-MDS). The study found that MDSCs were activated in the bone marrow of these patients, along with an increased proportion of CTLA-4+ T cells and alterations in T-cell memory subsets in peripheral blood. These immune changes suggest an early inflammatory state in CCUS/LR-MDS patients, highlighting the potential role of MDSCs in disease progression. Further research is needed to explore the relationship between immune dysregulation and molecular characteristics in these patients. [Extracted from the article]

Published
2024
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7. A phase 1/2 trial of an immune-modulatory vaccine against IDO/PD-L1 in combination with nivolumab in metastatic melanoma

Author

Kjeldsen, Julie Westerlin, Lorentzen, Cathrine Lund, Martinenaite, Evelina, Ellebaek, Eva, Donia, Marco, Holmstroem, Rikke Boedker, Klausen, Tobias Wirenfeldt, Madsen, Cecilie Oelvang, Ahmed, Shamaila Munir, Weis-Banke, Stine Emilie, Holmström, Morten Orebo, Hendel, Helle Westergren, Ehrnrooth, Eva, Zocca, Mai-Britt, Pedersen, Ayako Wakatsuki, Andersen, Mads Hald, and Svane, Inge Marie

Published
2021
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8. 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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12. Survivin

Author

Andersen, Mads Hald, Becker, Jürgen, and Marshall, John L., editor

Published
2017
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13. Author Correction: A phase 1/2 trial of an immune-modulatory vaccine against IDO/PD-L1 in combination with nivolumab in metastatic melanoma

Author

Kjeldsen, Julie Westerlin, Lorentzen, Cathrine Lund, Martinenaite, Evelina, Ellebaek, Eva, Donia, Marco, Holmstroem, Rikke Boedker, Klausen, Tobias Wirenfeldt, Madsen, Cecilie Oelvang, Ahmed, Shamaila Munir, Weis-Banke, Stine Emilie, Holmström, Morten Orebo, Hendel, Helle Westergren, Ehrnrooth, Eva, Zocca, Mai-Britt, Pedersen, Ayako Wakatsuki, Andersen, Mads Hald, and Svane, Inge Marie

Published
2022
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17. Revisiting Circulating Extracellular Matrix Fragments as Disease Markers in Myelofibrosis and Related Neoplasms

Author

Hasselbalch, Hans Carl, primary, Junker, Peter, additional, Skov, Vibe, additional, Kjær, Lasse, additional, Knudsen, Trine A., additional, Larsen, Morten Kranker, additional, Holmström, Morten Orebo, additional, Andersen, Mads Hald, additional, Jensen, Christina, additional, Karsdal, Morten A., additional, and Willumsen, Nicholas, additional

Published
2023
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18. Therapeutic cancer vaccination against mutant calreticulin in myeloproliferative neoplasms induces expansion of specific T cells in the periphery but specific T cells fail to enrich in the bone marrow

Author

Holmström, Morten Orebo, primary, Andersen, Morten, additional, Traynor, Sofie, additional, Ahmad, Shamaila Munir, additional, Lisle, Thomas Landkildehus, additional, Handlos Grauslund, Jacob, additional, Skov, Vibe, additional, Kjær, Lasse, additional, Ottesen, Johnny T., additional, Gjerstorff, Morten Frier, additional, Hasselbalch, Hans Carl, additional, and Andersen, Mads Hald, additional

Published
2023
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19. 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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20. Staphylococcus aureus enterotoxins induce FOXP3 in neoplastic T cells in Sézary syndrome

Author

Willerslev-Olsen, Andreas, Buus, Terkild B., Nastasi, Claudia, Blümel, Edda, Gluud, Maria, Bonefeld, Charlotte M., Geisler, Carsten, Lindahl, Lise M., Vermeer, Maarten, Wasik, Mariusz A., Iversen, Lars, Becker, Jürgen C., Andersen, Mads Hald, Gjerdrum, Lise M. R., Litvinov, Ivan V., Litman, Thomas, Krejsgaard, Thorbjørn, Woetmann, Anders, and Ødum, Niels

Published
2020
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23. Supplementary Figure from IDO Vaccine Ablates Immune-Suppressive Myeloid Populations and Enhances Antitumor Effects Independent of Tumor Cell IDO Status

Author

Nandre, Rahul, primary, Verma, Vivek, primary, Gaur, Pankaj, primary, Patil, Veerupaxagouda, primary, Yang, Xingdong, primary, Ramlaoui, Zainab, primary, Shobaki, Nour, primary, Andersen, Mads Hald, primary, Pedersen, Ayako Wakatsuki, primary, Zocca, Mai-Britt, primary, Mkrtichyan, Mikayel, primary, Gupta, Seema, primary, and Khleif, Samir N., primary

Published
2023
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24. 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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25. Data from Arginase 1–Based Immune Modulatory Vaccines Induce Anticancer Immunity and Synergize with Anti–PD-1 Checkpoint Blockade

Author

Aaboe Jørgensen, Mia, primary, Ugel, Stefano, primary, Linder Hübbe, Mie, primary, Carretta, Marco, primary, Perez-Penco, Maria, primary, Weis-Banke, Stine Emilie, primary, Martinenaite, Evelina, primary, Kopp, Katharina, primary, Chapellier, Marion, primary, Adamo, Annalisa, primary, De Sanctis, Francesco, primary, Frusteri, Cristina, primary, Iezzi, Manuela, primary, Zocca, Mai-Britt, primary, Hargbøll Madsen, Daniel, primary, Wakatsuki Pedersen, Ayako, primary, Bronte, Vincenzo, primary, and Andersen, Mads Hald, primary

Published
2023
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26. 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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27. Data from IDO Vaccine Ablates Immune-Suppressive Myeloid Populations and Enhances Antitumor Effects Independent of Tumor Cell IDO Status

Author

Nandre, Rahul, primary, Verma, Vivek, primary, Gaur, Pankaj, primary, Patil, Veerupaxagouda, primary, Yang, Xingdong, primary, Ramlaoui, Zainab, primary, Shobaki, Nour, primary, Andersen, Mads Hald, primary, Pedersen, Ayako Wakatsuki, primary, Zocca, Mai-Britt, primary, Mkrtichyan, Mikayel, primary, Gupta, Seema, primary, and Khleif, Samir N., primary

Published
2023
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28. 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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29. Supplementary Data from Arginase 1–Based Immune Modulatory Vaccines Induce Anticancer Immunity and Synergize with Anti–PD-1 Checkpoint Blockade

Author

Aaboe Jørgensen, Mia, primary, Ugel, Stefano, primary, Linder Hübbe, Mie, primary, Carretta, Marco, primary, Perez-Penco, Maria, primary, Weis-Banke, Stine Emilie, primary, Martinenaite, Evelina, primary, Kopp, Katharina, primary, Chapellier, Marion, primary, Adamo, Annalisa, primary, De Sanctis, Francesco, primary, Frusteri, Cristina, primary, Iezzi, Manuela, primary, Zocca, Mai-Britt, primary, Hargbøll Madsen, Daniel, primary, Wakatsuki Pedersen, Ayako, primary, Bronte, Vincenzo, primary, and Andersen, Mads Hald, primary

Published
2023
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30. Data from Acquired Immune Resistance Follows Complete Tumor Regression without Loss of Target Antigens or IFNγ Signaling

Author

Donia, Marco, primary, Harbst, Katja, primary, van Buuren, Marit, primary, Kvistborg, Pia, primary, Lindberg, Mattias F., primary, Andersen, Rikke, primary, Idorn, Manja, primary, Munir Ahmad, Shamaila, primary, Ellebæk, Eva, primary, Mueller, Anja, primary, Fagone, Paolo, primary, Nicoletti, Ferdinando, primary, Libra, Massimo, primary, Lauss, Martin, primary, Hadrup, Sine Reker, primary, Schmidt, Henrik, primary, Andersen, Mads Hald, primary, thor Straten, Per, primary, Nilsson, Jonas A., primary, Schumacher, Ton N., primary, Seliger, Barbara, primary, Jönsson, Göran, primary, and Svane, Inge Marie, primary

Published
2023
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31. Supplementary Figure S1-S5 from Acquired Immune Resistance Follows Complete Tumor Regression without Loss of Target Antigens or IFNγ Signaling

Author

Donia, Marco, primary, Harbst, Katja, primary, van Buuren, Marit, primary, Kvistborg, Pia, primary, Lindberg, Mattias F., primary, Andersen, Rikke, primary, Idorn, Manja, primary, Munir Ahmad, Shamaila, primary, Ellebæk, Eva, primary, Mueller, Anja, primary, Fagone, Paolo, primary, Nicoletti, Ferdinando, primary, Libra, Massimo, primary, Lauss, Martin, primary, Hadrup, Sine Reker, primary, Schmidt, Henrik, primary, Andersen, Mads Hald, primary, thor Straten, Per, primary, Nilsson, Jonas A., primary, Schumacher, Ton N., primary, Seliger, Barbara, primary, Jönsson, Göran, primary, and Svane, Inge Marie, primary

Published
2023
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32. Supplementary figure from Long-lasting Disease Stabilization in the Absence of Toxicity in Metastatic Lung Cancer Patients Vaccinated with an Epitope Derived from Indoleamine 2,3 Dioxygenase

Author

Iversen, Trine Zeeberg, primary, Engell-Noerregaard, Lotte, primary, Ellebaek, Eva, primary, Andersen, Rikke, primary, Larsen, Stine Kiaer, primary, Bjoern, Jon, primary, Zeyher, Claus, primary, Gouttefangeas, Cécile, primary, Thomsen, Birthe Moerk, primary, Holm, Bente, primary, thor Straten, Per, primary, Mellemgaard, Anders, primary, Andersen, Mads Hald, primary, and Svane, Inge Marie, primary

Published
2023
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33. 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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34. Supplementary Methods from Acquired Immune Resistance Follows Complete Tumor Regression without Loss of Target Antigens or IFNγ Signaling

Author

Donia, Marco, primary, Harbst, Katja, primary, van Buuren, Marit, primary, Kvistborg, Pia, primary, Lindberg, Mattias F., primary, Andersen, Rikke, primary, Idorn, Manja, primary, Munir Ahmad, Shamaila, primary, Ellebæk, Eva, primary, Mueller, Anja, primary, Fagone, Paolo, primary, Nicoletti, Ferdinando, primary, Libra, Massimo, primary, Lauss, Martin, primary, Hadrup, Sine Reker, primary, Schmidt, Henrik, primary, Andersen, Mads Hald, primary, thor Straten, Per, primary, Nilsson, Jonas A., primary, Schumacher, Ton N., primary, Seliger, Barbara, primary, Jönsson, Göran, primary, and Svane, Inge Marie, primary

Published
2023
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41. First in man study: Bcl-Xl_42-CAF®09b vaccines in patients with locally advanced prostate cancer

Author

Mørk, Sofie Kirial, primary, Kongsted, Per, additional, Westergaard, Marie Christine Wulff, additional, Albieri, Benedetta, additional, Granhøj, Joachim Stoltenborg, additional, Donia, Marco, additional, Martinenaite, Evelina, additional, Holmström, Morten Orebo, additional, Madsen, Kasper, additional, Kverneland, Anders H., additional, Kjeldsen, Julie Westerlin, additional, Holmstroem, Rikke Boedker, additional, Lorentzen, Cathrine Lund, additional, Nørgaard, Nis, additional, Andreasen, Lars Vibe, additional, Wood, Grith Krøyer, additional, Christensen, Dennis, additional, Klausen, Michael Schantz, additional, Hadrup, Sine Reker, additional, thor Straten, Per, additional, Andersen, Mads Hald, additional, and Svane, Inge Marie, additional

Published
2023
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42. 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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43. 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

44. Therapeutic cancer vaccination against mutant calreticulin in myeloproliferative neoplasms induces expansion of specific T cells in the periphery but specific T cells fail to enrich in the bone marrow

Author

Holmström, Morten Orebo, Andersen, Morten, Traynor, Sofie, Ahmad, Shamaila Munir, Lisle, Thomas Landkildehus, Handlos Grauslund, Jacob, Skov, Vibe, Kjær, Lasse, Ottesen, Johnny T., Gjerstorff, Morten Frier, Hasselbalch, Hans Carl, Andersen, Mads Hald, Holmström, Morten Orebo, Andersen, Morten, Traynor, Sofie, Ahmad, Shamaila Munir, Lisle, Thomas Landkildehus, Handlos Grauslund, Jacob, Skov, Vibe, Kjær, Lasse, Ottesen, Johnny T., Gjerstorff, Morten Frier, Hasselbalch, Hans Carl, and Andersen, Mads Hald

Abstract

Background: Therapeutic cancer vaccination against mutant calreticulin (CALR) in patients with CALR-mutant (CALRmut) myeloproliferative neoplasms (MPN) induces strong T-cell responses against mutant CALR yet fails to demonstrate clinical activity. Infiltration of tumor specific T cells into the tumor microenvironment is needed to attain a clinical response to therapeutic cancer vaccination. Aim: Determine if CALRmut specific T cells isolated from vaccinated patients enrich in the bone marrow upon completion of vaccination and explore possible explanations for the lack of enrichment. Methods: CALRmut specific T cells from four of ten vaccinated patients were expanded, enriched, and analyzed by T-cell receptor sequencing (TCRSeq). The TCRs identified were used as fingerprints of CALRmut specific T cells. Bone marrow aspirations from the four patients were acquired at baseline and at the end of trial. T cells were enriched from the bone marrow aspirations and analyzed by TCRSeq to identify the presence and fraction of CALRmut specific T cells at the two different time points. In silico calculations were performed to calculate the ratio between transformed cells and effector cells in patients with CALRmut MPN. Results: The fraction of CALRmut specific T cells in the bone marrow did not increase upon completion of the vaccination trial. In general, the T cell repertoire in the bone marrow remains relatively constant through the vaccination trial. The enriched and expanded CALRmut specific T cells recognize peripheral blood autologous CALRmut cells. In silico analyses demonstrate a high imbalance in the fraction of CALRmut cells and CALRmut specific effector T-cells in peripheral blood. Conclusion: CALRmut specific T cells do not enrich in the bone marrow after therapeutic cancer peptide vaccination against mutant CALR. The specific T cells recognize autologous peripheral blood derived CALRmut cells. In silico analyses demonstrate a high imbalance between the number of

Published
2023

45. Long-term follow-up of anti-PD-1 naïve patients with metastatic melanoma treated with IDO/PD-L1 targeting peptide vaccine and nivolumab

Author

Lorentzen, Cathrine Lund, Kjeldsen, Julie Westerlin, Ehrnrooth, Eva, Andersen, Mads Hald, Marie Svane, Inge, Lorentzen, Cathrine Lund, Kjeldsen, Julie Westerlin, Ehrnrooth, Eva, Andersen, Mads Hald, and Marie Svane, Inge

Abstract

Background We have previously published initial efficacy of the indoleamine 2,3-dioxygenase (IDO)/anti-programmed death ligand 1 (PD-L1) vaccine in combination with nivolumab in 30 anti-PD-1 therapy naïve patients with metastatic melanoma (cohort A). We now report long-term follow-up of patients in cohort A. Further, we report results from cohort B, where the peptide vaccine was added to anti-PD-1 therapy for patients with progressive disease during anti-PD-1 treatment. Methods All patients were treated with a therapeutic peptide vaccine in Montanide targeting IDO and PD-L1 combined with nivolumab (NCT03047928). A long-term follow-up of safety, response rates, and survival rates were performed in cohort A including patient subgroup analyses. Safety and clinical responses were analyzed for cohort B. Results Cohort A: At data cut-off, January 5, 2023, the overall response rate (ORR) was 80%, and 50% of the 30 patients obtained a complete response (CR). The median progression-free survival (mPFS) was 25.5 months (95% CI 8.8 to 39), and median overall survival (mOS) was not reached (NR) (95% CI 36.4 to NR). The minimum follow-up time was 29.8 months, and the median follow-up was 45.3 months (IQR 34.8-59.2). A subgroup evaluation further revealed that cohort A patients with unfavorable baseline characteristics, including either PD-L1 negative tumors (n=13), elevated lactate dehydrogenase (LDH) levels (n=11), or M1c (n=17) obtained both favorable response rates and durable responses. The ORR was 61.5%, 79%, and 88% for patients with PD-L1 - tumors, elevated LDH, and M1c, respectively. The mPFS was 7.1 months for patients with PD-L1 - tumors, 30.9 months for patients with elevated LDH, and 27.9 months for M1c patients. Cohort B: At data cut-off, the best overall response was stable disease for 2 of the 10 evaluable patients. The mPFS was 2.4 months (95% CI 1.38 to 2.52), and the mOS was 16.7 months (95% CI 4.13 to NR). Conclusion This long-term follow-up confirms the pr

Published
2023

46. Revisiting Circulating Extracellular Matrix Fragments as Disease Markers in Myelofibrosis and Related Neoplasms

Author

Hasselbalch, Hans Carl, Junker, Peter, Skov, Vibe, Kjær, Lasse, Knudsen, Trine A., Larsen, Morten Kranker, Holmström, Morten Orebo, Andersen, Mads Hald, Jensen, Christina, Karsdal, Morten A., Willumsen, Nicholas, Hasselbalch, Hans Carl, Junker, Peter, Skov, Vibe, Kjær, Lasse, Knudsen, Trine A., Larsen, Morten Kranker, Holmström, Morten Orebo, Andersen, Mads Hald, Jensen, Christina, Karsdal, Morten A., and Willumsen, Nicholas

Abstract

Philadelphia chromosome-negative chronic myeloproliferative neoplasms (MPNs) arise due to acquired somatic driver mutations in stem cells and develop over 10–30 years from the earliest cancer stages (essential thrombocythemia, polycythemia vera) towards the advanced myelofibrosis stage with bone marrow failure. The JAK2V617F mutation is the most prevalent driver mutation. Chronic inflammation is considered to be a major pathogenetic player, both as a trigger of MPN development and as a driver of disease progression. Chronic inflammation in MPNs is characterized by persistent connective tissue remodeling, which leads to organ dysfunction and ultimately, organ failure, due to excessive accumulation of extracellular matrix (ECM). Considering that MPNs are acquired clonal stem cell diseases developing in an inflammatory microenvironment in which the hematopoietic cell populations are progressively replaced by stromal proliferation—“a wound that never heals”—we herein aim to provide a comprehensive review of previous promising research in the field of circulating ECM fragments in the diagnosis, treatment and monitoring of MPNs. We address the rationales and highlight new perspectives for the use of circulating ECM protein fragments as biologically plausible, noninvasive disease markers in the management of MPNs.

Published
2023

47. 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

48. First in man study:Bcl-Xl_42-CAF®09b vaccines in patients with locally advanced prostate cancer

Author

Mørk, Sofie Kirial, Kongsted, Per, Westergaard, Marie Christine Wulff, Albieri, Benedetta, Granhøj, Joachim Stoltenborg, Donia, Marco, Martinenaite, Evelina, Holmström, Morten Orebo, Madsen, Kasper, Kverneland, Anders H., Kjeldsen, Julie Westerlin, Holmstroem, Rikke Boedker, Lorentzen, Cathrine Lund, Nørgaard, Nis, Andreasen, Lars Vibe, Wood, Grith Krøyer, Christensen, Dennis, Klausen, Michael Schantz, Hadrup, Sine Reker, thor Straten, Per, Andersen, Mads Hald, Svane, Inge Marie, Mørk, Sofie Kirial, Kongsted, Per, Westergaard, Marie Christine Wulff, Albieri, Benedetta, Granhøj, Joachim Stoltenborg, Donia, Marco, Martinenaite, Evelina, Holmström, Morten Orebo, Madsen, Kasper, Kverneland, Anders H., Kjeldsen, Julie Westerlin, Holmstroem, Rikke Boedker, Lorentzen, Cathrine Lund, Nørgaard, Nis, Andreasen, Lars Vibe, Wood, Grith Krøyer, Christensen, Dennis, Klausen, Michael Schantz, Hadrup, Sine Reker, thor Straten, Per, Andersen, Mads Hald, and Svane, Inge Marie

Abstract

Background: The B-cell lymphoma-extra-large (Bcl-XL) protein plays an important role in cancer cells’ resistance to apoptosis. Pre-clinical studies have shown that vaccination with Bcl-XL-derived peptides can induce tumor-specific T cell responses that may lead to the elimination of cancer cells. Furthermore, pre-clinical studies of the novel adjuvant CAF®09b have shown that intraperitoneal (IP) injections of this adjuvant can improve the activation of the immune system. In this study, patients with hormone-sensitive prostate cancer (PC) received a vaccine consisting of Bcl-XL-peptide with CAF®09b as an adjuvant. The primary aim was to evaluate the tolerability and safety of IP and intramuscular (IM) administration, determine the optimal route of administration, and characterize vaccine immunogenicity. Patients and methods: Twenty patients were included. A total of six vaccinations were scheduled: in Group A (IM to IP injections), ten patients received three vaccines IM biweekly; after a three-week pause, patients then received three vaccines IP biweekly. In Group B (IP to IM injections), ten patients received IP vaccines first, followed by IM under a similar vaccination schedule. Safety was assessed by logging and evaluating adverse events (AE) according to Common Terminology Criteria for Adverse Events (CTCAE v. 4.0). Vaccines-induced immune responses were analyzed by Enzyme-Linked Immunospot and flow cytometry. Results: No serious AEs were reported. Although an increase in T cell response against the Bcl-XL-peptide was found in all patients, a larger proportion of patients in group B demonstrated earlier and stronger immune responses to the vaccine compared to patients in group A. Further, we demonstrated vaccine-induced immunity towards patient-specific CD4, and CD8 T cell epitopes embedded in Bcl-XL-peptide and an increase in CD4 and CD8 T cell activation markers CD107a and CD137 following vaccination.

Published
2023

50. Antibodies to calnexin and mutated calreticulin are common in human sera

Author

Kyllesbech, Cecilie, Trier, Nicole Hartwig, Mughal, Farah Perveen, Hansen, Paul Robert, Holmström, Morten Orebo, el Fassi, Daniel, Hasselbalch, Hans, Skov, Vibe, Kjær, Lasse, Andersen, Mads Hald, Ciplys, Evaldas, Slibinskas, Rimantas, Fredriksen, Jette Lautrup, Højrup, Peter, Houen, Gunnar, Kyllesbech, Cecilie, Trier, Nicole Hartwig, Mughal, Farah Perveen, Hansen, Paul Robert, Holmström, Morten Orebo, el Fassi, Daniel, Hasselbalch, Hans, Skov, Vibe, Kjær, Lasse, Andersen, Mads Hald, Ciplys, Evaldas, Slibinskas, Rimantas, Fredriksen, Jette Lautrup, Højrup, Peter, and Houen, Gunnar

Abstract

Purpose of the study Calreticulin is an endoplasmic reticulum chaperone protein, which is involved in protein folding and in peptide loading of major histocompatibility complex class I molecules together with its homolog calnexin. Mutated calreticulin is associated with a group of hemopoietic disorders, especially myeloproliferative neoplasms. Currently only the cellular immune response to mutated calreticulin has been described, although preliminary findings have indicated that antibodies to mutated calreticulin are not specific for myeloproliferative disorders. These findings have prompted us to characterize the humoral immune response to mutated calreticulin and its chaperone homologue calnexin. Patients and methods We analyzed sera from myeloproliferative neoplasm patients, healthy donors and relapsing-remitting multiple sclerosis patients for the occurrence of autoantibodies to wild type and mutated calreticulin forms and to calnexin by enzyme-linked immunosorbent assay. Results Antibodies to mutated calreticulin and calnexin were present at similar levels in serum samples of myeloproliferative neoplasm and multiple sclerosis patients as well as healthy donors. Moreover, a high correlation between antibodies to mutated calreticulin and calnexin was seen for all patient and control groups. Epitope binding studies indicated that cross-reactive antibodies bound to a three-dimensional epitope encompassing a short linear sequence in the C-terminal of mutated calreticulin and calnexin. Conclusion Collectively, these findings indicate that calreticulin mutations may be common and not necessarily lead to onset of myeloproliferative neoplasm, possibly due to elimination of cells with mutations. This, in turn, may suggest that additional molecular changes may be required for development of myeloproliferative neoplasm.

Published
2023

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