Your search keyword '"Rolf Kiessling"' showing total 441 results

1. Trogocytosis and fratricide killing impede MSLN-directed CAR T cell functionality

Author

Esther Schoutrop, Stefanie Renken, Isabella Micallef Nilsson, Paula Hahn, Thomas Poiret, Rolf Kiessling, Stina L Wickström, Jonas Mattsson, and Isabelle Magalhaes

Subjects

CAR T cells, mesothelin, trogocytosis, ovarian cancer, immune escape, fratricide killing, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Successful translation of chimeric antigen receptor (CAR) T cell therapy for the treatment of solid tumors has proved to be troublesome, mainly due to the complex tumor microenvironment promoting T cell dysfunction and antigen heterogeneity. Mesothelin (MSLN) has emerged as an attractive target for CAR T cell therapy of several solid malignancies, including ovarian cancer. To improve clinical response rates with MSLN-CAR T cells, a better understanding of the mechanisms impacting CAR T cell functionality in vitro is crucial. Here, we demonstrated superior cytolytic capacity of CD28-costimulated MSLN-CAR T cells (M28z) relative to 4–1BB-costimulated MSLN-CAR T cells (MBBz). Furthermore, CD28-costimulated MSLN CAR T cells displayed enhanced cytolytic capacity against tumor spheroids with heterogeneous MSLN expression compared to MBBz CAR T cells. In this study, we identified CAR-mediated trogocytosis as a potential impeding factor for successful MSLN-CAR T cell therapy due to fratricide killing and contributing to tumor antigen heterogeneity. Moreover, we link antigen-dependent upregulation of LAG-3 with reduced CAR T cell functionality. Taken together, our study highlights the therapeutic potential and bottlenecks of MSLN-CAR T cells, providing a rationale for combinatorial treatment strategies.

Published

2022

2. Targeting of Nrf2 improves antitumoral responses by human NK cells, TIL and CAR T cells during oxidative stress

Author

Andreas Lundqvist, Rolf Kiessling, Isabelle Magalhaes, Jonas Mattsson, Stefanie Renken, Takahiro Nakajima, Elias S J Arnér, and Stina Linnea Wickström

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Published

2022

3. Generation of Tumor-Specific Cytotoxic T Cells From Blood via In Vitro Expansion Using Autologous Dendritic Cells Pulsed With Neoantigen-Coupled Microbeads

Author

Adela Kiessling, Keerthana Ramanathan, Ola B. Nilsson, Luigi Notari, Stefanie Renken, Rolf Kiessling, Hans Grönlund, and Stina L. Wickström

Subjects

neoantigen, tumor-specific antigens, autologous tumor recognition, dendritic cell-mediated activation, personalized cancer immunotherapy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

For the past decade, adoptive cell therapy including tumor-infiltrating lymphocytes, genetically modified cytotoxic lymphocytes expressing a chimeric antigen receptor, or a novel T-cell receptor has revolutionized the treatment of many cancers. Progress within exome sequencing and neoantigen prediction technologies provides opportunities for further development of personalized immunotherapies. In this study, we present a novel strategy to deliver in silico predicted neoantigens to autologous dendritic cells (DCs) using paramagnetic beads (EpiTCer beads). DCs pulsed with EpiTCer beads are superior in enriching for healthy donor and patient blood-derived tumor-specific CD8+ T cells compared to DC loaded with whole-tumor lysate or 9mer neoantigen peptides. A dose-dependent effect was observed, with higher EpiTCer bead per DC being favorable. We concluded that CD8+ T cells enriched by DC loaded with EpiTCer beads are tumor specific with limited tumor cross-reactivity and low recognition of autologous non-activated monocytes or CD8+ T cells. Furthermore, tumor specificity and recognition were improved and preserved after additional expansion using our Good Manufacturing Process (GMP)-compatible rapid expansion protocol. Phenotypic analysis of patient-derived EpiTCer DC expanded CD8+ T cells revealed efficient maturation, with high frequencies of central memory and effector memory T cells, similar to those observed in autologous expanded tumor-infiltrating lymphocytes. These results indicate that DC pulsed with EpiTCer beads enrich for a T-cell population with high capacity of tumor recognition and elimination, which are features needed for a T-cell product to be used for personalized adoptive cell therapy.

Published

2022

4. Interleukin‐33 is a Novel Immunosuppressor that Protects Cancer Cells from TIL Killing by a Macrophage‐Mediated Shedding Mechanism

Author

Jing Wu, Ziqing Chen, Stina L. Wickström, Juan Gao, Xingkang He, Xu Jing, Jieyu Wu, Qiqiao Du, Muyi Yang, Yi Chen, Dingding Zhang, Xin Yin, Ziheng Guo, Lasse Jensen, Yunlong Yang, Wei Tao, Andreas Lundqvist, Rolf Kiessling, and Yihai Cao

Subjects

cancer cells, cytolytic T cells, interleukin‐33, metalloprotease, T‐cell receptors, Science

Abstract

Abstract Recognition of specific antigens expressed in cancer cells is the initial process of cytolytic T cell‐mediated cancer killing. However, this process can be affected by other non‐cancerous cellular components in the tumor microenvironment. Here, it is shown that interleukin‐33 (IL‐33)‐activated macrophages protect melanoma cells from tumor‐infiltrating lymphocyte‐mediated killing. Mechanistically, IL‐33 markedly upregulates metalloprotease 9 (MMP‐9) expression in macrophages, which acts as a sheddase to trim NKG2D, an activating receptor expressed on the surface of natural killer (NK) cells, CD8+ T cells, subsets of CD4+ T cells, iNKT cells, and γδ T cells. Further, MMP‐9 also cleaves the MHC class I molecule, cell surface antigen‐presenting complex molecules, expressed in melanoma cells. Consequently, IL‐33‐induced macrophage MMP‐9 robustly mitigates the tumor killing‐effect by T cells. Genetic and pharmacological loss‐of‐function of MMP‐9 sheddase restore T cell‐mediated cancer killing. Together, these data provide compelling in vitro and in vivo evidence showing novel mechanisms underlying the IL‐33‐macrophage‐MMP‐9 axis‐mediated immune tolerance against cancer cells. Targeting each of these signaling components, including IL‐33 and MMP‐9 provides a new therapeutic paradigm for improving anticancer efficacy by immune therapy.

Published

2021

5. Predicting anti-PD-1 responders in malignant melanoma from the frequency of S100A9+ monocytes in the blood

Author

David Gomez-Cabrero, Rolf Kiessling, Yago Pico de Coaña, Maria Wolodarski, Johan Hansson, Jesper Tegner, Soudabeh Rad Pour, Xavier Martinez Demorentin, Jeroen Melief, and Manjula Thimma

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background While programmed cell death receptor 1 (PD-1) blockade treatment has revolutionized treatment of patients with melanoma, clinical outcomes are highly variable, and only a fraction of patients show durable responses. Therefore, there is a clear need for predictive biomarkers to select patients who will benefit from the treatment.Method To identify potential predictive markers for response to PD-1 checkpoint blockade immunotherapy, we conducted single-cell RNA sequencing analyses of peripheral blood mononuclear cells (PBMC) (n=8), as well as an in-depth immune monitoring study (n=20) by flow cytometry in patients with advanced melanoma undergoing treatment with nivolumab at Karolinska University Hospital. Blood samples were collected before the start of treatment and at the time of the second dose.Results Unbiased single-cell RNA sequencing of PBMC in patients with melanoma uncovered that a higher frequency of monocytes and a lower ratio of CD4+ T cells to monocyte were inversely associated with overall survival. Similarly, S100A9 expression in the monocytic subset was correlated inversely with overall survival. These results were confirmed by a flow cytometry-based analysis in an independent patient cohort.Conclusion Our results suggest that monocytic cell populations can critically determine the outcome of PD-1 blockade, particularly the subset expressing S100A9, which should be further explored as a possible predictive biomarker. Detailed knowledge of the biological role of S100A9+ monocytes is of high translational relevance.

Published

2021

6. Cisplatin inhibits frequency and suppressive activity of monocytic myeloid-derived suppressor cells in cancer patients

Author

Glenn F. Van Wigcheren, Nienke De Haas, Tom A. Mulder, Sophie K. Horrevorts, Martine Bloemendal, Simone Hins-Debree, Yumeng Mao, Rolf Kiessling, Carla M.L. van Herpen, Georgina Flórez-Grau, Stanleyson V. Hato, and I. Jolanda M. De Vries

Subjects

cancer, mdsc, platinum-based chemotherapy, cisplatin, immunotherapy, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Cancer immunotherapies have induced long-lasting responses in cancer patients including those with melanoma and head and neck squamous cell carcinoma (HNSCC). However, the majority of treated patients does not achieve clinical benefit from immunotherapy because of systemic tumor-induced immunosuppression. Monocytic myeloid-derived suppressor cells (M-MDSCs) are implicated as key players in inhibiting anti-tumor immune responses and their frequencies are closely associated with tumor progression. Tumor-derived signals, including signaling via STAT3-COX-2, induce the transformation of monocytic precursors into suppressive M-MDSCs. In a retrospective assessment, we observed that survival of melanoma patients undergoing dendritic cell vaccination was negatively associated with blood M-MDSC levels. Previously, it was shown that platinum-based chemotherapeutics inhibit STAT signaling. Here, we show that cisplatin and oxaliplatin treatment interfere with the development of M-MDSCs, potentially synergizing with cancer immunotherapy. In vitro, subclinical doses of platinum-based drugs prevented the generation of COX-2+ M-MDSCs induced by tumor cells from melanoma patients. This was confirmed in HNSCC patients where intravenous cisplatin treatment drastically lowered M-MDSC frequency while monocyte levels remained stable. In treated patients, expression of COX-2 and arginase-1 in M-MDSCs was significantly decreased after two rounds of cisplatin, indicating inhibition of STAT3 signaling. In line, the capacity of M-MDSCs to inhibit activated T cell responses ex vivo was significantly decreased after patients received cisplatin. These results show that platinum-based chemotherapeutics inhibit the expansion and suppressive activity of M-MDSCs in vitro and in cancer patients. Therefore, platinum-based drugs have the potential to enhance response rates of immunotherapy by overcoming M-MDSC-mediated immunosuppression.

Published

2021

7. Complete and long-lasting clinical responses in immune checkpoint inhibitor-resistant, metastasized melanoma treated with adoptive T cell transfer combined with DC vaccination

Author

Tanja Lövgren, Maria Wolodarski, Stina Wickström, Ulrika Edbäck, Mette Wallin, Eva Martell, Katrin Markland, Pontus Blomberg, Maria Nyström, Andreas Lundqvist, Hans Jacobsson, Gustav Ullenhag, Per Ljungman, Johan Hansson, Giuseppe Masucci, Roger Tell, Isabel Poschke, Lars Adamson, Jonas Mattsson, and Rolf Kiessling

Subjects

combination immunotherapy, adoptive tumor-infiltrating lymphocyte therapy, tumor lysate, dc vaccination, immune checkpoint inhibitor resistance, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Development of T cell-directed immune checkpoint inhibitors (ICI) has revolutionized metastatic melanoma (MM) therapy, but 36 and >18 months, respectively). In addition, two patients had partial responses (PR), one still ongoing (>42 months) with only a small bone-lesion remaining, and one of short duration (

Published

2020

8. PD-1 checkpoint blockade in advanced melanoma patients: NK cells, monocytic subsets and host PD-L1 expression as predictive biomarker candidates

Author

Yago Pico de Coaña, Maria Wolodarski, Irene van der Haar Àvila, Takahiro Nakajima, Stamatina Rentouli, Andreas Lundqvist, Giuseppe Masucci, Johan Hansson, and Rolf Kiessling

Subjects

melanoma, immune checkpoint inhibitors, mdscs, nk cells, predictive biomarkers, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Blockade of the PD-1 receptor has revolutionized the treatment of metastatic melanoma, with significant increases in overall survival (OS) and a dramatic improvement in patient quality of life. Despite the success of this approach, the number of benefitting patients is limited and there is a need for predictive biomarkers as well as a deeper mechanistic analysis of the cellular populations involved in clinical responses. With the aim to find predictive biomarkers for PD-1 checkpoint blockade, an in-depth immune monitoring study was conducted in 36 advanced melanoma patients receiving pembrolizumab or nivolumab treatment at Karolinska University Hospital. Blood samples were collected before treatment and before administration of the second and fourth doses. Peripheral blood mononuclear cells were isolated and stained for flow cytometric analysis within 2 h of sample collection. Overall survival and progression-free survival (PFS) were inversely correlated with CD69 expression NK cells. In the myeloid compartment, high frequencies of non-classical monocytes and low frequencies of monocytic myeloid derived suppressor cells (MoMDSCs) correlated with response rates and OS. A deeper characterization of monocytic subsets showed that PD-L1 expression in MDSCs, non-classical and intermediate monocytes was significantly increased in patients with shorter PFS in addition to correlating inversely with OS. Our results suggest that cellular populations other than T cells can be critical in the outcome of PD-1 blockade treatment. Specifically, the frequencies of activated NK cells and monocytic subsets are inversely correlated with survival and clinical benefit, suggesting that their role as predictive biomarkers should be further evaluated.

Published

2020

9. Intratumorally injected pro-inflammatory allogeneic dendritic cells as immune enhancers: a first-in-human study in unfavourable risk patients with metastatic renal cell carcinoma

Author

Anna Laurell, Maria Lönnemark, Einar Brekkan, Anders Magnusson, Anna Tolf, Anna Carin Wallgren, Bengt Andersson, Lars Adamson, Rolf Kiessling, and Alex Karlsson-Parra

Subjects

Metastatic renal cell carcinoma, Phase I/II study, Intratumoral administration, Vaccine, Allogeneic dendritic cells, Anti-tumor response, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Accumulating pre-clinical data indicate that the efficient induction of antigen-specific cytotoxic CD8+ T cells characterizing viral infections is caused by cross-priming where initially infected DCs produce an unique set of inflammatory factors that recruit and activate non-infected bystander DCs. Our DC-based immunotherapy concept is guided by such bystander view and accordingly, we have developed a cellular adjuvant consisting of pre-activated allogeneic DCs producing high levels of DC-recruiting and DC-activating factors. This concept doesn’t require MHC-compatibility between injected cells and the patient and therefore introduces the possibility of using pre-produced and freeze-stored DCs from healthy blood donors as an off- the-shelf immune enhancer. The use of MHC-incompatible allogeneic DCs will further induce a local rejection process at the injection site that is expected to further enhance recruitment and maturation of endogenous bystander DCs. Methods Twelve intermediate and poor risk patients with newly diagnosed metastatic renal cell carcinoma (mRCC) where included in a phase I/II study. Pro-inflammatory allogeneic DCs were produced from a leukapheresis product collected from one healthy blood donor and subsequently deep-frozen. A dose of 5–20 × 106 DCs (INTUVAX) was injected into the renal tumor twice with 2 weeks interval before planned nephrectomy and subsequent standard of care. Results No INTUVAX-related severe adverse events were observed. A massive infiltration of CD8+ T cells was found in 5 out of 12 removed kidney tumors. No objective tumor response was observed and 6 out of 11 evaluable patients have subsequently received additional treatment with standard tyrosine kinase inhibitors (TKI). Three of these 6 patients experienced an objective tumor response including one sunitinib-treated patient who responded with a complete and durable regression of 4 brain metastases. Median overall survival (mOS) is still not reached (currently 42.5 months) but has already passed historical mOS in patients with unfavourable risk mRCC on standard TKI therapy. Conclusions Our findings indicate that intratumoral administration of proinflammatory allogeneic DCs induces an anti-tumor immune response that may prolong survival in unfavourable risk mRCC-patients given subsequent standard of care. A randomized, multi-center, phase II mRCC trial (MERECA) with INTUVAX in conjuction with sunitinib has been initiated. Trial registration Clinicaltrials.gov identifier: NCT01525017 .

Published

2017

10. Cancer Neoepitopes for Immunotherapy: Discordance Between Tumor-Infiltrating T Cell Reactivity and Tumor MHC Peptidome Display

Author

Stina L. Wickström, Tanja Lövgren, Michael Volkmar, Bruce Reinhold, Jonathan S. Duke-Cohan, Laura Hartmann, Janina Rebmann, Anja Mueller, Jeroen Melief, Roeltje Maas, Maarten Ligtenberg, Johan Hansson, Rienk Offringa, Barbara Seliger, Isabel Poschke, Ellis L. Reinherz, and Rolf Kiessling

Subjects

TIL, tumor, Immune peptidome, neoepitopes, mass spectrometry, immunotherapy, Immunologic diseases. Allergy, RC581-607

Abstract

Tumor-infiltrating lymphocytes (TIL) are considered enriched for T cells recognizing shared tumor antigens or mutation-derived neoepitopes. We performed exome sequencing and HLA-A*02:01 epitope prediction from tumor cell lines from two HLA-A2-positive melanoma patients whose TIL displayed strong tumor reactivity. The potential neoepitopes were screened for recognition using autologous TIL by immunological assays and presentation on tumor major histocompatibility complex class I (MHC-I) molecules by Poisson detection mass spectrometry (MS). TIL from the patients recognized 5/181 and 3/49 of the predicted neoepitopes, respectively. MS screening detected 3/181 neoepitopes on tumor MHC-I from the first patient but only one was also among those recognized by TIL. Consequently, TIL enriched for neoepitope specificity failed to recognize tumor cells, despite being activated by peptides. For the second patient, only after IFN-γ treatment of the tumor cells was one of 49 predicted neoepitopes detected by MS, and this coincided with recognition by TIL sorted for the same specificity. Importantly, specific T cells could be expanded from patient and donor peripheral blood mononuclear cells (PBMC) for all neoepitopes recognized by TIL and/or detected on tumor MHC-I. In summary, stimulating the appropriate inflammatory environment within tumors may promote neoepitope MHC presentation while expanding T cells in blood may circumvent lack of specific TIL. The discordance in detection between physical and functional methods revealed here can be rationalized and used to improve neoantigen-targeted T cell immunotherapy.

Published

2019

11. IL-15, TIM-3 and NK cells subsets predict responsiveness to anti-CTLA-4 treatment in melanoma patients

Author

Rossana Tallerico, Costanza M. Cristiani, Elina Staaf, Cinzia Garofalo, Rosa Sottile, Mariaelena Capone, Yago Pico de Coaña, Gabriele Madonna, Eleonora Palella, Maria Wolodarski, Valentina Carannante, Domenico Mallardo, Ester Simeone, Antonio M. Grimaldi, Sofia Johansson, Paolo Frumento, Elio Gulletta, Andrea Anichini, Francesco Colucci, Gennaro Ciliberto, Rolf Kiessling, Klas Kärre, Paolo A. Ascierto, and Ennio Carbone

Subjects

anti-ctla-4, il-15, melanoma, nk cells, pd-1, tim-3, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Despite the success of immune checkpoint blockade in melanoma, the majority of patients do not respond. We hypothesized that the T and NK cell subset frequencies and expression levels of their receptors may predict responses and clinical outcome of anti-CTLA-4 treatment. We thus characterized the NK and T cell phenotype, as well as serum levels of several cytokines in 67 melanoma patients recruited in Italy and Sweden, using samples drawn prior to and during treatment. Survival correlated with low expression of the inhibitory receptor TIM-3 on circulating T and NK cells prior to and during treatment and with the increased frequency of mature circulating NK cells (defined as CD3−CD56dim CD16+) during treatment. Survival also correlated with low levels of IL-15 in the serum. Functional experiments in vitro demonstrated that sustained exposure to IL-15 enhanced the expression of PD-1 and TIM-3 on both T and NK cells, indicating a causative link between high IL-15 levels and enhanced expression of TIM-3 on these cells. Receptor blockade of TIM-3 improved NK cell-mediated elimination of melanoma metastasis cell lines in vitro. These observations may lead to the development of novel biomarkers to predict patient response to checkpoint blockade treatment. They also suggest that induction of additional checkpoints is a possibility that needs to be considered when treating melanoma patients with IL-15.

Published

2017

12. Methylcholanthrene-Induced Sarcomas Develop Independently from NOX2-Derived ROS.

Author

Maarten A Ligtenberg, Özcan Çınar, Rikard Holmdahl, Dimitrios Mougiakakos, and Rolf Kiessling

Subjects

Medicine, Science

Abstract

Reactive oxygen species (ROS) produced by the inducible NADPH oxidase type 2 (NOX2) complex are essential for clearing certain infectious organisms but may also have a role in regulating inflammation and immune response. For example, ROS is involved in myeloid derived suppressor cell (MDSC)- and regulatory T cell (T(reg)) mediated T- and NK-cell suppression. However, abundant ROS produced within the tumor microenvironment, or by the tumor itself may also yield oxidative stress, which can blunt anti-tumor immune responses as well as eventually leading to tumor toxicity. In this study we aimed to decipher the role of NOX2-derived ROS in a chemically (by methylcholanthrene (MCA)) induced sarcoma model. Superoxide production by NOX2 requires the p47(phox) (NCF1) subunit to organize the formation of the NOX2 complex on the cell membrane. Homozygous mutant mice (NCF1*/*) have a functional loss of their super oxide burst while heterozygous mice (NCF1*/+) retain this key function. Mice harboring either a homo- or a heterozygous mutation were injected intramuscularly with MCA to induce sarcoma formation. We found that NOX2 functionality does not determine tumor incidence in the tested MCA model. Comprehensive immune monitoring in tumor bearing mice showed that infiltrating immune cells experienced an increase in their oxidative state regardless of the NOX2 functionality. While MCA-induced sarcomas where characterized by a T(reg) and MDSC accumulation, no significant differences could be found between NCF1*/* and NCF1*/+ mice. Furthermore, infiltrating T cells showed an increase in effector-memory cell phenotype markers in both NCF1*/* and NCF1*/+ mice. Tumors established from both NCF1*/* and NCF1*/+ mice were tested for their in vitro proliferative capacity as well as their resistance to cisplatin and radiation therapy, with no differences being recorded. Overall our findings indicate that NOX2 activity does not play a key role in tumor development or immune cell infiltration in the chemically induced MCA sarcoma model.

Published

2015

13. Contrasting Effects of the Cytotoxic Anticancer Drug Gemcitabine and the EGFR Tyrosine Kinase Inhibitor Gefitinib on NK Cell-Mediated Cytotoxicity via Regulation of NKG2D Ligand in Non-Small-Cell Lung Cancer Cells.

Author

Riki Okita, Diana Wolf, Koichiro Yasuda, Ai Maeda, Takuro Yukawa, Shinsuke Saisho, Katsuhiko Shimizu, Yoshiyuki Yamaguchi, Mikio Oka, Eiichi Nakayama, Andreas Lundqvist, Rolf Kiessling, Barbara Seliger, and Masao Nakata

Subjects

Medicine, Science

Abstract

Several cytotoxic anticancer drugs inhibit DNA replication and/or mitosis, while EGFR tyrosine kinase inhibitors inactivate EGFR signalling in cancer cell. Both types of anticancer drugs improve the overall survival of the patients with non-small-cell lung cancer (NSCLC), although tumors often become refractory to this treatment. Despite several mechanisms by which the tumors become resistant having been described the effect of these compounds on anti-tumor immunity remains largely unknown.This study examines the effect of the cytotoxic drug Gemcitabine and the EGFR tyrosine kinase inhibitor Gefitinib on the expression of NK group 2 member D (NKG2D) ligands as well as the sensitivity of NSCLC cells to the NK-mediated lysis.We demonstrate that Gemcitabine treatment leads to an enhanced expression, while Gefitinib downregulated the expression of molecules that act as key ligands for the activating receptor NKG2D and promote NK cell-mediated recognition and cytolysis. Gemcitabine activated ATM and ATM- and Rad-3-related protein kinase (ATR) pathways. The Gemcitabine-induced phosphorylation of ATM as well as the upregulation of the NKG2D ligand expression could be blocked by an ATM-ATR inhibitor. In contrast, Gefitinib attenuated NKG2D ligand expression. Silencing EGFR using siRNA or addition of the PI3K inhibitor resulted in downregulation of NKG2D ligands. The observations suggest that the EGFR/PI3K pathway also regulates the expression of NKG2D ligands. Additionally, we showed that both ATM-ATR and EGFR regulate MICA/B via miR20a.In keeping with the effect on NKG2D expression, Gemcitabine enhanced NK cell-mediated cytotoxicity while Gefitinib attenuated NK cell killing in NSCLC cells.

Published

2015

14. Raume, Grenzen und Identitaten in der Vormoderne - Methodische Uberlegungen und ihre konkretisierung am Beispiel Schwaben

Author

Rolf Kiessling

Subjects

History (General), D1-2009

Published

2005

15. Comparative expression profiling of distinct T cell subsets undergoing oxidative stress.

Author

Rudolf Lichtenfels, Dimitrios Mougiakakos, C Christian Johansson, Sven P Dressler, Christian V Recktenwald, Rolf Kiessling, and Barbara Seliger

Subjects

Medicine, Science

Abstract

The clinical outcome of adoptive T cell transfer-based immunotherapies is often limited due to different escape mechanisms established by tumors in order to evade the hosts' immune system. The establishment of an immunosuppressive micromilieu by tumor cells along with distinct subsets of tumor-infiltrating lymphocytes is often associated with oxidative stress that can affect antigen-specific memory/effector cytotoxic T cells thereby substantially reducing their frequency and functional activation. Therefore, protection of tumor-reactive cytotoxic T lymphocytes from oxidative stress may enhance the anti-tumor-directed immune response. In order to better define the key pathways/proteins involved in the response to oxidative stress a comparative 2-DE-based proteome analysis of naïve CD45RA(+) and their memory/effector CD45RO(+) T cell counterparts in the presence and absence of low dose hydrogen peroxide (H(2)O(2)) was performed in this pilot study. Based on the profiling data of these T cell subpopulations under the various conditions, a series of differentially expressed spots were defined, members thereof identified by mass spectrometry and subsequently classified according to their cellular function and localization. Representative targets responding to oxidative stress including proteins involved in signaling pathways, in regulating the cellular redox status as well as in shaping/maintaining the structural cell integrity were independently verified at the transcript and protein level under the same conditions in both T cell subsets. In conclusion the resulting profiling data describe complex, oxidative stress-induced, but not strictly concordant changes within the respective expression profiles of CD45RA(+) and CD45RO(+) T cells. Some of the differentially expressed genes/proteins might be further exploited as potential targets toward modulating the redox capacity of the distinct lymphocyte subsets thereby providing the basis for further studies aiming at rendering them more resistant to tumor micromilieu-induced oxidative stress.

Published

2012

16. Kleine Geschichte Schwabens

Author

Rolf Kießling

Published

2021

17. Judengemeinden in Schwaben im Kontext des Alten Reiches

Author

Rolf Kießling, Rolf Kießling

Published

2019

18. Landjudentum im deutschen Südwesten während der Frühen Neuzeit

Author

Rolf Kießling, Sabine Ullmann, Rolf Kießling, Sabine Ullmann

Published

2018

19. Konrad Peutinger: Ein Universalgelehrter zwischen Spätmittelalter und Früher Neuzeit: Bestandsaufnahme und Perspektiven

Author

Rolf Kießling, Rolf Kießling

Published

2018

20. Rolf Kießling (25. Juli 1941 – 22. Juni 2020)

Author

Dietmar Schiersner and Rolf Kießling

Published

2023

21. Rezension von: Kießling, Rolf, Jüdische Geschichte in Bayern

Author

Benigna Schönhagen and Rolf Kießling

Abstract

Rolf Kießling, Jüdische Geschichte in Bayern. Von den Anfängen bis zur Gegenwart (Studien zur Jüdischen Geschichte und Kultur in Bayern, Bd. 11), hg. von Michael Brenner. München: De Gruyter Oldenbourg 2019. 681 S. ISBN 978-3486811230. € 79,95

Published

2022

22. Figure S5 from Cripto-1 Plasmid DNA Vaccination Targets Metastasis and Cancer Stem Cells in Murine Mammary Carcinoma

Author

Rolf Kiessling, Federica Cavallo, Andreas Lundqvist, Alvaro Lladser, Charlotte Rolny, Benedict J. Chambers, Helena Tufvesson-Stiller, Tatjana Wallmann, Roberto Ruiu, Stefania Lanzardo, Laura Conti, Maarten A. Ligtenberg, and Kristina Witt

Abstract

Tumor multiplicity in BALB-neuT mice.

Published

2023

23. Data from Cripto-1 Plasmid DNA Vaccination Targets Metastasis and Cancer Stem Cells in Murine Mammary Carcinoma

Author

Rolf Kiessling, Federica Cavallo, Andreas Lundqvist, Alvaro Lladser, Charlotte Rolny, Benedict J. Chambers, Helena Tufvesson-Stiller, Tatjana Wallmann, Roberto Ruiu, Stefania Lanzardo, Laura Conti, Maarten A. Ligtenberg, and Kristina Witt

Abstract

Metastatic breast cancer is a fatal disease that responds poorly to treatment. Cancer vaccines targeting antigens expressed by metastatic breast cancer cells and cancer stem cells could function as anticancer therapies. Cripto-1 is an oncofetal protein overexpressed in invasive breast cancer and cancer-initiating cells. In this study, we explored the potential of a Cripto-1–encoding DNA vaccine to target breast cancer in preclinical mouse models. BALB/c mice and BALB-neuT mice were treated with a DNA vaccine encoding mouse Cripto-1 (mCr-1). BALB/c mice were challenged with murine breast cancer 4T1 cells or TUBO spheres; BALB-neuT mice spontaneously developed breast cancer. Tumor growth was followed in all mouse models and lung metastases were evaluated. In vitro assays were performed to identify the immune response elicited by vaccination. Vaccination against mCr-1 reduced primary tumor growth in the 4T1 metastatic breast cancer model and reduced lung metastatic burden. In BALB-neuT mice, because the primary tumors are Cripto-1 negative, vaccination against mCr-1 did not affect primary tumors but did reduce lung metastatic burden. Spheroid-cultured TUBO cells, derived from a BALB/neuT primary tumor, develop a cancer stem cell–like phenotype and express mCr-1. We observed reduced tumor growth in vaccinated mice after challenge with TUBO spheres. Our data indicate that vaccination against Cripto-1 results in a protective immune response against mCr-1 expressing and metastasizing cells. Targeting Cripto-1 by vaccination holds promise as an immunotherapy for treatment of metastatic breast cancer. Cancer Immunol Res; 6(11); 1417–25. ©2018 AACR.

Published

2023

24. Data from Ipilimumab Treatment Results in an Early Decrease in the Frequency of Circulating Granulocytic Myeloid-Derived Suppressor Cells as well as Their Arginase1 Production

Author

Rolf Kiessling, Giuseppe V. Masucci, Johan Hansson, Maria Nyström, Yumeng Mao, Giusy Gentilcore, Isabel Poschke, and Yago Pico de Coaña

Abstract

Blocking the immune checkpoint molecule CTL antigen-4 (CTLA-4) with ipilimumab has proven to induce long-lasting clinical responses in patients with metastatic melanoma. To study the early response that takes place after CTLA-4 blockade, peripheral blood immune monitoring was conducted in five patients undergoing ipilimumab treatment at baseline, three and nine weeks after administration of the first dose. Along with T-cell population analysis, this work was primarily focused on an in-depth study of the myeloid-derived suppressor cell (MDSC) populations. Ipilimumab treatment resulted in lower frequencies of regulatory T cells along with reduced expression levels of PD-1 at the nine-week time point. Three weeks after the initial ipilimumab dose, the frequency of granulocytic MDSCs was significantly reduced and was followed by a reduction in the frequency of arginase1-producing CD3− cells, indicating an indirect in trans effect that should be taken into account for future evaluations of ipilimumab mechanisms of action. Cancer Immunol Res; 1(3); 158–62. ©2013 AACR.

Published

2023

25. Supplementary Tables 1 and 2 from Ipilimumab Treatment Results in an Early Decrease in the Frequency of Circulating Granulocytic Myeloid-Derived Suppressor Cells as well as Their Arginase1 Production

Author

Rolf Kiessling, Giuseppe V. Masucci, Johan Hansson, Maria Nyström, Yumeng Mao, Giusy Gentilcore, Isabel Poschke, and Yago Pico de Coaña

Abstract

PDF file - 51K, These tables show the additional untreated melanoma patients and the antibodies used in flow cytometry

Published

2023

26. Supplementary Figures 1 and 2 from Ipilimumab Treatment Results in an Early Decrease in the Frequency of Circulating Granulocytic Myeloid-Derived Suppressor Cells as well as Their Arginase1 Production

Author

Rolf Kiessling, Giuseppe V. Masucci, Johan Hansson, Maria Nyström, Yumeng Mao, Giusy Gentilcore, Isabel Poschke, and Yago Pico de Coaña

Abstract

PDF file - 75K, Supplementary figure 1 depicts the absolute lymphocyte counts in patients during ipilimumab treatment. Supplementary figure 2 depicts the correlation analysis of different dellular populations

Published

2023

27. Supplementary Figure 3 from Ipilimumab Treatment Results in an Early Decrease in the Frequency of Circulating Granulocytic Myeloid-Derived Suppressor Cells as well as Their Arginase1 Production

Author

Rolf Kiessling, Giuseppe V. Masucci, Johan Hansson, Maria Nyström, Yumeng Mao, Giusy Gentilcore, Isabel Poschke, and Yago Pico de Coaña

Abstract

PDF file - 213K, This figure shows the gating strategy used for analyzing the arginase staining

Published

2023

28. Table S1 from Cripto-1 Plasmid DNA Vaccination Targets Metastasis and Cancer Stem Cells in Murine Mammary Carcinoma

Author

Rolf Kiessling, Federica Cavallo, Andreas Lundqvist, Alvaro Lladser, Charlotte Rolny, Benedict J. Chambers, Helena Tufvesson-Stiller, Tatjana Wallmann, Roberto Ruiu, Stefania Lanzardo, Laura Conti, Maarten A. Ligtenberg, and Kristina Witt

Abstract

Summary of all antibodies.

Published

2023

29. Precision radiation of immune checkpoint therapy resistant melanoma metastases (PROMMEL study): study protocol for a phase II open-label multicenter trial

Author

Ellen Backlund, Muyi Yang, Vitali Grozman, Giuseppe Masucci, Johan Falkenius, Hanna Eriksson, Braslav Jovanovic, Katarina Hammarlund, Ulf Isacsson, Calin Radu, Edvard Abel, Kristin Karlsson, Ricardo Palanco Zamora, Peter Wersäll, Ulrika Edbäck, Stina Wickström, Eva Darai Ramqvist, Suzanne Egyhazi Brage, Rolf Kiessling, Kristina Viktorsson, Bo Franzén, Rolf Lewensohn, Roger Olofsson Bagge, Gustav J. Ullenhag, Lars Ny, Karin Lindberg, and Hildur Helgadottir

Subjects

Oncology, Radiology, Nuclear Medicine and imaging, Hematology, General Medicine

Published

2022

30. Rezension von: Brakensiek, Stefan; Kießling, Rolf; Troßbach, Werner; Zimmermann, Clemens (Hrsg.), Grundzüge der Agrargeschichte (Band 1–3)

Author

Winfried Schenk, Stefan Brakensiek, Rolf Kießling, Werner Troßbach, and Clemens Zimmermann

Abstract

Grundzüge der Agrargeschichte (Band 1 – 3), hg. von Stefan Brakensiek, Rolf Kießling, Werner Troßbach und Clemens Zimmermann, Köln: Böhlau 2016. 704 S., 123 s/w Abb. ISBN 978-3-412-22225-3. € 70,–

Published

2022

31. Supplemental Tables and Figure Legends from Targeting Suppressive Myeloid Cells Potentiates Checkpoint Inhibitors to Control Spontaneous Neuroblastoma

Author

Rolf Kiessling, Per Kogner, John Inge Johnsen, Katarina Le Blanc, Nina Eissler, and Yumeng Mao

Abstract

Table S1. Statistical comparisons between neurofibroma (NF) and 3 cohorts of human neuroblastoma (NB) tissues. Table S2. Authentication of human neuroblastoma cell lines Table S3. Antibodies and dyes used for flow cytometry. Supplemental Figure Legends

Published

2023

32. Supplementary Figure 3 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplemental Figure 3: Patterns of clonal shifts during early and late phase of in vitro TIL expansion

Published

2023

33. Data from Targeting Suppressive Myeloid Cells Potentiates Checkpoint Inhibitors to Control Spontaneous Neuroblastoma

Author

Rolf Kiessling, Per Kogner, John Inge Johnsen, Katarina Le Blanc, Nina Eissler, and Yumeng Mao

Abstract

Purpose: Neuroblastoma is the most common extracranial solid cancer type in childhood, and high-risk patients have poor prognosis despite aggressive multimodal treatment. Neuroblastoma-driven inflammation contributes to the induction of suppressive myeloid cells that hamper efficient antitumor immune responses. Therefore, we sought to enhance antitumor immunity by removing immunosuppression mediated by myeloid cells.Experimental Design: The prognostic values of myeloid cells are demonstrated by analyzing genomic datasets of neuroblastoma patients. The impact of tumor-derived factors on myelopoiesis and local induction of suppressive myeloid cells is dissected by in vitro culture models using freshly isolated human CD34+ hematopoietic stem cells, primary human monocytes, and murine bone marrow cells. To test the therapeutic efficacy of BLZ945 as a monotherapy or in combination with checkpoint inhibitors, we used a transgenic murine model (TH-MYCN) that develops aggressive spontaneous neuroblastoma.Results: We report that infiltrating CSF-1R+ myeloid cells predict poor clinical outcome in patients with neuroblastoma. In vitro, neuroblastoma-derived factors interfere with early development of myeloid cells and enable suppressive functions on human monocytes through M-CSF/CSF-1R interaction. In a transgenic mouse model (TH-MYCN) resembling high-risk human neuroblastoma, antagonizing CSF-1R with a selective inhibitor (BLZ945) modulates the induction of human and murine suppressive myeloid cells and efficiently limit tumor progression. While checkpoint inhibitors are insufficient in controlling tumor growth, combining BLZ945 with PD-1/PD-L1 blocking antibodies results in superior tumor control.Conclusions: Our results demonstrate the essential role of CSF-1R signaling during the induction of suppressive myeloid cells and emphasize its clinical potential as an immunotherapy for human cancers. Clin Cancer Res; 22(15); 3849–59. ©2016 AACR.

Published

2023

34. Data from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Purpose:During our efforts to develop tumor-infiltrating lymphocyte (TIL) therapy to counter the devastating recurrence rate in patients with primary resectable pancreatic ductal adenocarcinoma (PDA), we found that PDA TILs can readily be expanded in vitro and that the majority of resulting TIL cultures show reactivity against the autologous tumor. However, the fraction of tumor-reactive T cells is low. We investigated to which extent this was related to the in vitro expansion.Experimental Design:We compared the clonal composition of TIL preparations before and after in vitro expansion using T-cell receptor (TCR) deep sequencing. Our findings for PDA were benchmarked to experiments with melanoma TILs.Results:We found that the TIL TCR repertoire changes dramatically during in vitro expansion, leading to loss of tumor- dominant T-cell clones and overgrowth by newly emerging T-cell clones that are barely detectable in the tumor. These changes are primarily driven by differences in the intrinsic in vitro expansion capacity of T-cell clones. Single-cell experiments showed an association between poor proliferative capacity and expression of markers related to antigen experience and dysfunction. Furthermore, we found that spatial heterogeneity of the TIL repertoire resulted in TCR repertoires that are greatly divergent between TIL cultures derived from distant tumor samples of the same patient.Conclusions:Culture-induced changes in clonal composition are likely to affect tumor reactivity of TIL preparations. TCR deep sequencing provides important insights into the factors that govern the outcome of in vitro TIL expansion and thereby a path toward optimization of the production of TIL preparations with high therapeutic efficacy.See related commentary by Lozano-Rabella and Gros, p. 4177

Published

2023

35. Supplementary Figure 5 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplemental Figure 5: Intratumoral and intra-patient heterogeneity of the PDA and melanoma TIL TCR repertoire

Published

2023

36. Supplementary Figure 7 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplemental Figure 7: Schematic representation of TIL repertoire in different tumor samples from the same patient and the result of ex vivo TIL expansion.

Published

2023

37. Supplementary Table 1 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplementary Table 1

Published

2023

38. Supplementary Figure Legends from Inhibition of Tumor-Derived Prostaglandin-E2 Blocks the Induction of Myeloid-Derived Suppressor Cells and Recovers Natural Killer Cell Activity

Author

Andreas Lundqvist, Rolf Kiessling, Barbara Seliger, André Steven, Dhifaf Sarhan, and Yumeng Mao

Abstract

PDF file - 93K

Published

2023

39. Supplementary Tables 1 - 2 from Inhibition of Tumor-Derived Prostaglandin-E2 Blocks the Induction of Myeloid-Derived Suppressor Cells and Recovers Natural Killer Cell Activity

Author

Andreas Lundqvist, Rolf Kiessling, Barbara Seliger, André Steven, Dhifaf Sarhan, and Yumeng Mao

Abstract

PDF file - 207K, Table S1. Cell line authentication. Table S2. Antibodies used for flow cytometry.

Published

2023

40. Data from Inhibition of Tumor-Derived Prostaglandin-E2 Blocks the Induction of Myeloid-Derived Suppressor Cells and Recovers Natural Killer Cell Activity

Author

Andreas Lundqvist, Rolf Kiessling, Barbara Seliger, André Steven, Dhifaf Sarhan, and Yumeng Mao

Abstract

Purpose: Increased frequencies of myeloid-derived suppressor cells (MDSC) correlate with poor prognosis in patients with cancers. Tumor-derived prostaglandin-E2 (PGE2) plays an important role in inducing MDSCs. However, the detailed mechanisms of this induction remain unknown. To develop targeted therapies for MDSCs, we sought to investigate the molecular basis of PGE2-regulated accumulation of MDSCs and their functional consequence on natural killer (NK) cell activity.Experimental Design: The effects of PGE2 in inducing phenotypic, signaling, and functional alternations on monocytes were analyzed in vitro. Suppression of NK-cell activity by PGE2-treated monocytes was compared with that of freshly isolated CD14+HLA-DRlow/− monocytic MDSCs (moMDSC) from patients with melanoma. In addition, to explore the in vivo relevance of targeting PGE2 to reduce MDSC-mediated suppression of NK cells, we established a murine model, where tumor cells were disabled from cyclooxygenase-2 (COX-2) production.Results: Patient-derived moMDSCs inhibited NK-cell activity through the production of TGFβ. In vitro, binding of PGE2 to EP2 and EP4 receptors on monocytes activated the p38MAPK/ERK pathway and resulted in elevated secretion of TGFβ. Similar to moMDSCs, PGE2-treated monocytes potently suppressed NK-cell activity through production of TGFβ. Furthermore, silencing COX-2 in murine 4T1 tumor cells reduced the accumulation of CD11b+Gr1+ MDSCs in the spleen, resulting in concomitant improved in vivo clearance of NK-cell sensitive YAC-1 cells.Conclusions: Our results reveal an indispensable role of tumor-derived PGE2 in inducing MDSCs and suggest a favorable outcome of combining COX-2–targeted therapy and adoptive NK-cell transfer in patients with cancer. Clin Cancer Res; 20(15); 4096–106. ©2014 AACR.

Published

2023

41. Supplementary Figure 2 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplemental Figure 2: Tumor antigen reactivity is associated with CD8 +CCR7 -CD45RA-PD-1high cells

Published

2023

42. Supplementary Figure 4 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplemental Figure 4: TIL expansion is influenced by the use of feeder cells

Published

2023

43. Supplementary Figures 1 - 3 from Inhibition of Tumor-Derived Prostaglandin-E2 Blocks the Induction of Myeloid-Derived Suppressor Cells and Recovers Natural Killer Cell Activity

Author

Andreas Lundqvist, Rolf Kiessling, Barbara Seliger, André Steven, Dhifaf Sarhan, and Yumeng Mao

Abstract

PDF file - 252K, Figure S1. HLA-DR+ cells do not inhibit NK cells. Figure S2. PGE2 induces suppressive functions on monocytes. Figure S3. COX-2 silencing of tumor cells reduces immune suppression in mice.

Published

2023

44. Supplementary Methods from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplementary Methods

Published

2023

45. Supplementary Figure 1 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplemental Figure 1: TIL expansion is reproducible

Published

2023

46. Supplemental figures from Targeting Suppressive Myeloid Cells Potentiates Checkpoint Inhibitors to Control Spontaneous Neuroblastoma

Author

Rolf Kiessling, Per Kogner, John Inge Johnsen, Katarina Le Blanc, Nina Eissler, and Yumeng Mao

Abstract

Figure S1. A) Expression levels of granulocytic marker CD66b, regulatory T cell marker FoxP3 or dendritic cell marker CD83, CD11c Figure S2. A) CD34+ hematopoietic stem cells without cytokine activation lack the capacity to stimulate allogeneic T cells. Figure S3. Analysis of A) M-CSF or B) 27 other soluble factors produced by the three human neuroblastoma cell lines (SK-N-BE(2), SK-N-AS or SK-N-FI). Figure S4. Expression of PD-L1 on A) tumor-educated monocytes Figure S5. Bone marrow cells extracted from naïve mice were cultured in medium, recombinant murine M-CSF (20 ng/ml) or neuroblastoma tumor-conditioned medium (TCM). Figure S6. Mice were sacrificed 10 days after spontaneous tumors were palpable Figure S7. A) BLZ945 treatment scheme in the TH-MYCN mice bearing established spontaneous tumors was summarized. Figure S8. A) Treatment scheme combining PD-1/PD-L1 blockade and CSF-1R inhibition was illustrated.

Published

2023

47. Related Article from Myeloid Suppressors Decrease Melanoma Survival by Abating Tumor-Fighting T Cells

Author

Yago Pico de Coaña, Yumeng Mao, and Rolf Kiessling

Abstract

Related Article from Myeloid Suppressors Decrease Melanoma Survival by Abating Tumor-Fighting T Cells

Published

2023

48. Supplementary Table 2 from The Outcome of Ex Vivo TIL Expansion Is Highly Influenced by Spatial Heterogeneity of the Tumor T-Cell Repertoire and Differences in Intrinsic In Vitro Growth Capacity between T-Cell Clones

Author

Rienk Offringa, Oliver Strobel, Michael Flossdorf, Frank Bergmann, Rolf Kiessling, Joost van den Berg, John B.A.G. Haanen, Anna-Katharina König, Jasmin Roth, Claudia Lauenstein, Stina L. Wickström, Tanja Lövgren, Johanna Lehmann, Lena M. Appel, Ignacio Heras-Murillo, Katharina A.M. Lindner, Aaron Rodriguez-Ehrenfried, Jessica C. Hassel, and Isabel C. Poschke

Abstract

Supplementary Table 2

Published

2023

49. Data from Myeloid Suppressors Decrease Melanoma Survival by Abating Tumor-Fighting T Cells

Author

Yago Pico de Coaña, Yumeng Mao, and Rolf Kiessling

Abstract

Disseminated malignant melanoma has a poor prognosis. Immunotherapy based on cytokines or checkpoint inhibitors has a protracted beneficial effect in a select group of patients. Understanding the mechanisms that inhibit tumor-specific T cells will help the development of biomarkers to formulate therapy for this disease. Clin Cancer Res; 20(6); 1401–3. ©2014 AACR.

Published

2023

50. Data from Immature Immunosuppressive CD14+HLA-DR−/low Cells in Melanoma Patients Are Stat3hi and Overexpress CD80, CD83, and DC-Sign

Author

Rolf Kiessling, Giuseppe V. Masucci, Johan Hansson, Dimitrios Mougiakakos, and Isabel Poschke

Abstract

Myeloid-derived suppressor cells (MDSC) have emerged as key immune modulators in various tumor models and human malignancies, but their characteristics in humans remain to be unequivocally defined. In this study, we have examined circulating CD14+HLA-DR−/low MDSC in 34 advanced malignant melanoma (MM) patients. Their frequency is significantly increased and associated with disease activity. Contrary to the common notion that MDSC are a heterogeneous population of exclusively immature cells, we find the coexpression of markers associated with mature phenotype. We show for the first time the overexpression of CD80, CD83, and DC-Sign in human MDSC. Further, increased levels of signal transducer and activator of transcription 3 (Stat3), an important regulator in MDSC development and function, were noted in MM-MDSC. Stat3 was altered toward an active, phosphorylated state in the HLA-DR− population of CD14+ cells and was more reactive to activating stimuli in patients. Importantly, inhibition of Stat3 abolished their suppressive activity almost completely. The described MM-MDSC use arginase in conjunction with other yet undefined mechanisms to suppress CD4+ and CD8+ T cells. Several observations suggest a redox imbalance in MDSC and indicate an important role of Stat3-dependent oxidative stress in MDSC-mediated T-cell suppression. These results emphasize the diversity of MDSC in human cancer and provide potential targets for therapeutic interventions. Cancer Res; 70(11); 4335–45. ©2010 AACR.

Published

2023