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1. Combination Therapy with Immune Checkpoint Inhibitors and Histone Deacetylase Inhibitors or Alkylating Agents

Author

Joerger M, Koster KL, Janik T, and de Jong FA

Subjects
histone deacetylase inhibitor, checkpoint inhibitor, alkylating agents, synergy, hematological malignancies, solid tumors, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Markus Joerger,1 Kira-Lee Koster,1 Tomas Janik,2 Floris A de Jong3,4 1Department of Medical Oncology and Hematology, Cantonal Hospital St. Gallen, St. Gallen, Switzerland; 2Research & Development Department, Mundipharma Research Limited, Cambridge, UK; 3Global Medical Affairs Department, Mundipharma Research Limited, Cambridge, UK; 4Medical Affairs Department, Exact Sciences International GmbH, Baar, SwitzerlandCorrespondence: Tomas Janik, Mundipharma Research Limited, Cambridge Science Park, Milton Road, Cambridge, UK, Email tomas.janik@mundipharma.czPurpose: Immune checkpoint inhibitors (CPIs) have been widely adopted in a number of early and advanced malignancies. Histone deacetylase inhibitors (HDACis) and alkylating agents (AAs) have been suggested to potentiate the actions of CPIs on tumor cells. We conducted a comprehensive literature review to explore the potential synergistic activity between CPIs, AAs, and HDACis.Patients and Methods: Clinical and non-clinical studies describing outcomes in patients with cancer receiving CPIs and either concomitant or sequential (pre- or post-CPI) AAs or HDACis were identified in PubMed using pre-defined search strings. Manual searches of key oncology congresses were similarly performed. All relevant articles and abstracts were manually screened for relevance, classified according to the specific anticancer agents used (CPIs, AAs, or HDACis), tumor entity, and whether treatment was concomitant or sequential.Results: Overall, 227 unique clinical studies across a range of tumor types, both solid tumors and hematological malignancies, were identified. One hundred and fifty-nine publications on Phase I and II clinical studies together with 41 publications on Phase III studies were examined. The most commonly investigated tumor types were melanoma, triple-negative breast cancer, non-small cell lung cancer, and Hodgkin lymphoma. The randomized clinical studies identified, all of which reported on the combination of a CPI with an AA, demonstrated superior outcomes in the combination arm compared with CPI or AA monotherapy. Similarly, combination therapy with CPIs and HDACis demonstrated promising activity.Conclusion: Sequential or concomitant administration of a CPI with an AA or an HDACi may improve outcomes for patients with a range of tumor types. There is a rationale to support further investigation into the potential for synergy between CPIs, alkylating agents and/or HDACis in both the non-clinical and clinical settings.Plain Language Summary: People being treated for cancer will often receive more than one drug at a time, and the concept of combining cancer drugs is frequently investigated as a potential opportunity to improve outcomes for patients. We reviewed the published literature for clinical trials and work undertaken in laboratories to explore whether combining targeted agents that stop cancer cells from multiplying (known as checkpoint inhibitors) with traditional chemotherapy that kills cancer cells could be a useful approach. We looked at evidence in publications where checkpoint inhibitors were used at the same time as chemotherapy, or given immediately before or after chemotherapy. The most important evidence came from clinical trials where outcomes for patients receiving combinations of treatment were directly compared with those from patients receiving a single treatment. These studies showed superior outcomes for patients who were treated with a combination of cancer drugs compared with patients receiving monotherapy. We also found evidence that adding another class of cancer drug, called histone deacetylase inhibitors, might sensitize tumors to checkpoint inhibitors. These findings provide a rationale for examining alkylating agents and/or histone deacetylase inhibitors combined with checkpoint inhibitors.Keywords: histone deacetylase inhibitor, checkpoint inhibitor, alkylating agents, synergy, hematological malignancies, solid tumors

Published
2024

5. 146P A novel allosteric oral immunotherapy small molecule modulates adenosine 2a receptor signaling and restores anti-tumor immune responses

Author

Pejoski, D., primary, Suess, C., additional, Gouiller, A., additional, Héritier, M., additional, Boujut, M., additional, Tardy, S., additional, De Smedt, T., additional, Galibert, L., additional, Reith, W., additional, Joerger, M., additional, Toso, C., additional, Kössler, T., additional, Hamed, H., additional, and Scapozza, L., additional

Published
2023
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6. 118O Definitive results for NSCLC and bladder cancer cohorts in the phase IIa trial of visugromab (CTL-002) in advanced/metastatic anti-PD/PD-L1 relapsed/refractory solid tumors (GDFATHER-trial)

Author

Melero, I., primary, De Miguel, M.J., additional, Casal, G. Alonso, additional, De Velasco Oria, G.A., additional, Ramelyte, E., additional, Joerger, M., additional, Martin-Liberal, J., additional, König, D., additional, Sayehli, C.M., additional, Gromke, T., additional, RodrÍguez-Ruiz, M.E., additional, Calvo, E., additional, Garralda, E., additional, Soto-Castillo, J.J., additional, Dummer, R., additional, Villarrubia, J. Esteban, additional, Goebeler, M-E., additional, Fettes, P., additional, Klar, K., additional, and Leo, E., additional

Published
2023
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8. Implementation of dihydropyrimidine dehydrogenase deficiency testing in Europe

Author

de With, M, Sadlon, A, Cecchin, E, Haufroid, V, Thomas, F, Joerger, M, van Schaik, R H N, Mathijssen, R H J, Largiadèr, C R, de With, M, Sadlon, A, Cecchin, E, Haufroid, V, Thomas, F, Joerger, M, van Schaik, R H N, Mathijssen, R H J, and Largiadèr, C R

Abstract

BACKGROUND: The main cause for fluoropyrimidine-related toxicity is deficiency of the metabolizing enzyme dihydropyrimidine dehydrogenase (DPD). In 2020, the European Medicines Agency (EMA) recommended two methods for pre-treatment DPD deficiency testing in clinical practice: phenotyping using endogenous uracil concentration or genotyping for DPYD risk variant alleles. This study assessed the DPD testing implementation status in Europe before (2019) and after (2021) the release of the EMA recommendations.METHODS: The survey was conducted from 16 March 2022 to 31 July 2022. An electronic form with seven closed and three open questions was e-mailed to 251 professionals with DPD testing expertise of 34 European countries. A descriptive analysis was conducted.RESULTS: We received 79 responses (31%) from 23 countries. Following publication of the EMA recommendations, 87% and 75% of the countries reported an increase in the amount of genotype and phenotype testing, respectively. Implementation of novel local guidelines was reported by 21 responders (27%). Countries reporting reimbursement of both tests increased in 2021, and only four (18%) countries reported no coverage for any testing type. In 2019, major implementation drivers were 'retrospective assessment of fluoropyrimidine-related toxicity' (39%), and in 2021, testing was driven by 'publication of guidelines' (40%). Although the major hurdles remained the same after EMA recommendations-'lack of reimbursement' (26%; 2019 versus 15%; 2021) and 'lack of recognizing the clinical relevance by medical oncologists' (25%; 2019 versus 8%; 2021)-the percentage of specialists citing these decreased. Following EMA recommendations, 25% of responders reported no hurdles at all in the adoption of the new testing practice in the clinics.CONCLUSIONS: The EMA recommendations have supported the implementation of DPD deficiency testing in Europe. Key factors for successful implementation were test reimbursement

Published
2023

9. Open-label, randomized study of individualized, pharmacokinetically (PK)-guided dosing of paclitaxel combined with carboplatin or cisplatin in patients with advanced non-small-cell lung cancer (NSCLC)

Author

Joerger, M., von Pawel, J., Kraff, S., Fischer, J.R., Eberhardt, W., Gauler, T.C., Mueller, L., Reinmuth, N., Reck, M., Kimmich, M., Mayer, F., Kopp, H.-G., Behringer, D.M., Ko, Y.-D., Hilger, R.A., Roessler, M., Kloft, C., Henrich, A., Moritz, B., Miller, M.C., Salamone, S.J., and Jaehde, U.

Published
2016
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11. 200MO Anti–IL-8 BMS-986253 + nivolumab (NIVO) ± ipilimumab (IPI) in patients (pts) with advanced cancer: Update of initial phase I results

Author

Simonelli, M., primary, Calvo, E., additional, Davar, D., additional, Richards, D., additional, Gutierrez, M., additional, Moreno Garcia, V., additional, Marron, T., additional, Rottey, S., additional, Orcurto, A., additional, Renouf, D.J., additional, Joerger, M., additional, Barriga Falcon, S., additional, Fan, J., additional, Gibson, E., additional, Chakraborty, D., additional, Arora, V., additional, and Melero, I., additional

Published
2022
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12. 19P Effects of CTLA-4 single nucleotide polymorphisms (SNPs) on toxicity of ipilimumab-containing regimens in patients with advanced stage melanoma

Author

Joode, K.D., primary, Rojas Mora, A., additional, Van Schaik, R., additional, Zippelius, A., additional, Van der Veldt, A.A.M., additional, Gerard, C.L., additional, Läubli, H., additional, Michielin, O.A., additional, von Moos, R.A.F., additional, Joerger, M., additional, Levesque, M.P., additional, Aeppli, S., additional, Mangana, J., additional, Mangas, C., additional, Meyer, S., additional, Leoni-Parvex, S., additional, Mathijssen, R.H., additional, and Metaxas, Y., additional

Published
2022
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13. 194P Thermal ablation followed by intratumoral injection of a novel immune stimulant IP-001 in patients with advanced solid tumors: Phase IB part of study SAKK 66/17

Author

Joerger, M., primary, Knüsel, P., additional, Alejandre-Lafont, E., additional, Metaxas, Y., additional, Mark, M.T., additional, von Moos, R.A.F., additional, Gysel, K., additional, Eckhardt, K., additional, Glaus Garzon, J., additional, Koster, K-L., additional, Wittwer, Y., additional, Tissot, S., additional, Flatz, L., additional, Alleruzzo, L., additional, Lam, S.K., additional, Anderson, D., additional, Chen, W., additional, Baskin-Bey, E., additional, and Hode, T., additional

Published
2022
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18. 749P ANV419, a selective IL-2R-beta-gamma targeted antibody-IL-2 fusion protein, in patients with advanced solid tumors, a phase I/II study

Author

Läubli, H., primary, Alonso, G., additional, Lopez, J.S., additional, Calvo, E., additional, Joerger, M., additional, Perez, V., additional, Di Blasi, D., additional, Nair, A., additional, Richter, K., additional, Huber, C., additional, Mouton, J., additional, Costanzo, S., additional, Jethwa, S., additional, Bucher, C.M., additional, and Garralda, E., additional

Published
2022
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19. 1495P SAKK 57/16 nab-paclitaxel and gemcitabine in soft tissue sarcoma (NAPAGE): Final results from the phase Ib/II trial with >2y median follow up

Author

Digklia, A., primary, Kollar, A., additional, Kronig, M-N., additional, Britschgi, C., additional, Rordorf, T., additional, Joerger, M., additional, Krasniqi, F., additional, Metaxas, Y., additional, Colombo, I., additional, Dietrich, D., additional, Chiquet, S., additional, Ribi, K., additional, and Rothermundt, C.A., additional

Published
2022
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20. 431P Neoadjuvant treatment with regorafenib and capecitabine combined with radiotherapy in locally advanced rectal cancer: A multicenter phase Ib trial (RECAP) SAKK 41/16

Author

Bastian, S., primary, Joerger, M., additional, Baertschi, D., additional, Holer, L., additional, Guckenberger, M., additional, Jochum, W., additional, Koeberle, D., additional, Siebenhüner, A.R., additional, Berger, M.D., additional, Winterhalder, R.C., additional, Largiadèr, C.R., additional, Löffler-Baumann, M., additional, Mosna- Firlejczyk, K., additional, Wicki, A., additional, Fischer Maranta, A., additional, and von Moos, R.A.F., additional

Published
2022
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36. 436P Phase (Ph) II study of taminadenant (NIR178) + spartalizumab (PDR001) in patients (pts) with microsatellite stable (MSS) colorectal cancer (CRC)

Author

Saavedra Santa Gadea, O., primary, Greil, R., additional, de Jonge, M.J.A., additional, Tan, D., additional, Jerusalem, G., additional, Damian, S., additional, Grell, P., additional, Wainberg, Z., additional, Wolf, J., additional, Joerger, M., additional, Carlino, M.S., additional, Kasper, S., additional, Yap, T.A., additional, Otero, J., additional, Yang, X., additional, Nesbitt, V., additional, Kim, J., additional, Lee, L. Ho, additional, Choudhury, S., additional, and Leal, T.A., additional

Published
2021
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38. 1570P Outcome and prognostic factors of COVID-19 infection in cancer patients: Final results of SAKK 80/20

Author

Joerger, M., primary, Metaxas, Y., additional, Zaman, K., additional, Michielin, O.A., additional, Mach, N., additional, Betticher, D., additional, Schmitt, A.M., additional, Cantoni, N., additional, Caspar, C.B., additional, Stettler, S., additional, Malval, R., additional, Pless, M., additional, Britschgi, C., additional, Renner, C., additional, Koeberle, D., additional, Schulz, J., additional, Kopp, C., additional, Hayoz, S., additional, Stathis, A., additional, and von Moos, R., additional

Published
2021
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42. LC3A positive “stone like structures” are differentially associated with survival outcomes and CD68 macrophage infiltration in patients with lung adenocarcinoma and squamous cell carcinoma

Author

Gachechiladze, M., primary, Uberall, I., additional, Skanderova, D., additional, Matchavariani, J., additional, Ibrahim, M., additional, Shani, I., additional, Smickova, P., additional, Kolek, V., additional, Cierna, L., additional, Klein, J., additional, Stahel, R., additional, Joerger, M., additional, Soltermann, A., additional, and Skarda, J., additional

Published
2021
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44. Phase (Ph) II study of taminadenant (NIR178) + spartalizumab (PDR001) in patients (pts) with microsatellite stable (MSS) colorectal cancer (CRC)

Author

Gadea, O. Saavedra Santa, Greil, R., De Jonge, M. J. A., Tan, D., Jerusalem, G., Damian, S., Grell, P., Wainberg, Z., Wolf, J., Joerger, M., Carlino, M. S., Kasper, S., Yap, T. A., Otero, J., Yang, X., Nesbitt, V., Kim, J., Lee, L. Ho, Choudhury, S., Leal, T. A., Gadea, O. Saavedra Santa, Greil, R., De Jonge, M. J. A., Tan, D., Jerusalem, G., Damian, S., Grell, P., Wainberg, Z., Wolf, J., Joerger, M., Carlino, M. S., Kasper, S., Yap, T. A., Otero, J., Yang, X., Nesbitt, V., Kim, J., Lee, L. Ho, Choudhury, S., and Leal, T. A.

Published
2021

46. LBA46 SAKK 11/16, a phase IIa trial evaluating overall survival (OS) for recurrent/metastatic Head & neck squamous cell carcinoma (RMHNSCC) patients (pts) progressing after ≥ 1 line of systemic therapy, treated with MVX-ONCO-1, a novel, first in class cell encapsulation-based immunotherapy

Author

Mach, N., Fernandez, E., Vernet, R., O. Vonrohr, Urwyler, M., Charrier, E., Belkouch, M-C., Saingier, V., F. Courtout, C. de Vito, Rubin, O., Ancrenaz, V., Grogg, J.N., Renaux, J., Gysel, K., Müller, G., Brezina, T., Rordorf, T., Joerger, M., and Michielin, O.A.

Published
2023
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