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1. Five-year follow-up of a phase I trial of donor-derived modified immune cell infusion in kidney transplantation

Author

Matthias Schaier, Christian Morath, Lei Wang, Christian Kleist, Gerhard Opelz, Thuong Hien Tran, Sabine Scherer, Lien Pham, Naruemol Ekpoom, Caner Süsal, Gerald Ponath, Florian Kälble, Claudius Speer, Louise Benning, Christian Nusshag, Christoph F. Mahler, Luiza Pego da Silva, Claudia Sommerer, Angela Hückelhoven-Krauss, David Czock, Arianeb Mehrabi, Constantin Schwab, Rüdiger Waldherr, Paul Schnitzler, Uta Merle, Vedat Schwenger, Markus Krautter, Stephan Kemmner, Michael Fischereder, Manfred Stangl, Ingeborg A. Hauser, Anna-Isabelle Kälsch, Bernhard K. Krämer, Georg A. Böhmig, Carsten Müller-Tidow, Jochen Reiser, Martin Zeier, Michael Schmitt, Peter Terness, Anita Schmitt, and Volker Daniel

Subjects
transplantation - kidney, tolerance, cell therapy, regulatory B (Breg) cells, phase I (drug development), Immunologic diseases. Allergy, RC581-607
Abstract

BackgroundThe administration of modified immune cells (MIC) before kidney transplantation led to specific immunosuppression against the allogeneic donor and a significant increase in regulatory B lymphocytes. We wondered how this approach affected the continued clinical course of these patients.MethodsTen patients from a phase I clinical trial who had received MIC infusions prior to kidney transplantation were retrospectively compared to 15 matched standard-risk recipients. Follow-up was until year five after surgery.ResultsThe 10 MIC patients had an excellent clinical course with stable kidney graft function, no donor-specific human leukocyte antigen antibodies (DSA) or acute rejections, and no opportunistic infections. In comparison, a retrospectively matched control group receiving standard immunosuppressive therapy had a higher frequency of DSA (log rank P = 0.046) and more opportunistic infections (log rank P = 0.033). Importantly, MIC patients, and in particular the four patients who had received the highest cell number 7 days before surgery and received low immunosuppression during follow-up, continued to show a lack of anti-donor T lymphocyte reactivity in vitro and high CD19+CD24hiCD38hi transitional and CD19+CD24hiCD27+ memory B lymphocytes until year five after surgery.ConclusionsMIC infusions together with reduced conventional immunosuppression were associated with good graft function during five years of follow-up, no de novo DSA development and no opportunistic infections. In the future, MIC infusions might contribute to graft protection while reducing the side effects of immunosuppressive therapy. However, this approach needs further validation in direct comparison with prospective controls.Trial registrationhttps://clinicaltrials.gov/, identifier NCT02560220 (for the TOL-1 Study). EudraCT Number: 2014-002086-30.

Published
2023
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2. Individualised immunosuppression with intravenously administered donor-derived modified immune cells compared with standard of care in living donor kidney transplantation (TOL-2 Study): protocol for a multicentre, open-label, phase II, randomised controlled trial

Author

Lei Wang, Arianeb Mehrabi, Maria-Luisa Schubert, Anita Schmitt, Brigitte Neuber, Alexander Kunz, Angela Hückelhoven-Krauss, Carsten Müller-Tidow, Michael Schmitt, Christian Morath, Martin Zeier, Constantin Schwab, Anja Sander, Sabine Scherer, Claudius Speer, Christian Kleist, Claudia Sommerer, Florian Kälble, Christian Nusshag, Matthias Schaier, Louise Benning, Vedat Schwenger, Caner Süsal, Gerhard Opelz, T. Hien Tran, Stephan Kemmner, Michael Fischereder, Manfred Stangl, Ingeborg A. Hauser, Christian Bischofs, Sandra Sauer, Rüdiger Waldherr, Christopher Büsch, David Czock, Georg A Böhmig, Jochen Reiser, Axel Roers, Peter Terness, and Volker Daniel

Subjects
Medicine
Abstract

Introduction Donor-derived modified immune cells (MIC) induced long-term specific immunosuppression against the allogeneic donor in preclinical models of transplantation. In a phase I clinical trial (TOL-1 Study), MIC treatment resulted in a cellular phenotype that was directly and indirectly suppressive to the recipient’s immune system allowing for reduction of conventional immunosuppressive therapy. Here, we describe a protocol for a randomised controlled, multicentre phase-IIb clinical trial of individualised immunosuppression with intravenously administered donor MIC compared with standard-of-care (SoC) in living donor kidney transplantation (TOL-2 Study).Methods and analysis Sixty-three living donor kidney transplant recipients from six German transplant centres are randomised 2:1 to treatment with MIC (MIC group, N=42) or no treatment with MIC (control arm, N=21). MIC are manufactured from donor peripheral blood mononuclear cells under Good Manufacturing Practice conditions. The primary objective of this trial is to determine the efficacy of MIC treatment together with reduced conventional immunosuppressive therapy in terms of achieving an operational tolerance-like phenotype compared with SoC 12 months after MIC administration. Key secondary endpoints are the number of patient-relevant infections as well as a composite of biopsy-proven acute rejection, graft loss, graft dysfunction or death. Immunosuppressive therapy of MIC-treated patients is reduced during follow-up under an extended immunological monitoring including human leucocyte antigen-antibody testing, and determination of lymphocyte subsets, for example, regulatory B lymphocytes (Breg) and antidonor T cell response. A Data Safety Monitoring Board has been established to allow an independent assessment of safety and efficacy.Ethics and dissemination Ethical approval has been provided by the Ethics Committee of the Medical Faculty of the University of Heidelberg, Heidelberg, Germany (AFmu-580/2021, 17 March 2022) and from the Federal Institute for Vaccines and Biomedicines, Paul-Ehrlich-Institute, Langen, Germany (Vorlage-Nr. 4586/02, 21 March 2022). Written informed consent will be obtained from all patients and respective donors prior to enrolment in the study. The results from the TOL-2 Study will be published in peer-reviewed medical journals and will be presented at symposia and scientific meetings.Trial registration number NCT05365672.

Published
2022
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6. Individualised immunosuppression with intravenously administered donor-derived modified immune cells compared with standard of care in living donor kidney transplantation (TOL-2 Study): protocol for a multicentre, open-label, phase II, randomised controlled trial

Author

Süsal, Caner (ORCID 0000-0003-2521-8201 & YÖK ID 351800), Morath, C.; Schmitt, A.; Schmitt, M.; Wang, L.; Kleist, C.; Opelz, G.; Tran, T.H.; Scherer, S.; Schwenger, V.; Kemmner, S.; Fischereder, M.; Stangl, M.; Hauser, I.A.; Sommerer, C.; Nusshag, C.; Kalble, F.; Speer, C.; Benning, L.; Bischofs, C.; Sauer, S.; Schubert, M.L.; Kunz, A.; Hückelhoven-Krauss, A.; Neuber, B.; Mehrabi, A.; Schwab, C.; Waldherr, R.; Sander, A.; Büsch, C.; Czock, D.; Böhmig, G.A.; Reiser, J.; Roers, A.; Müller-Tidow, C.; Terness, P.; Zeier, M.; Daniel, V.; Schaier, M., Koç University Research Center for Translational Medicine (KUTTAM) / Koç Üniversitesi Translasyonel Tıp Araştırma Merkezi (KUTTAM), School of Medicine, Süsal, Caner (ORCID 0000-0003-2521-8201 & YÖK ID 351800), Morath, C.; Schmitt, A.; Schmitt, M.; Wang, L.; Kleist, C.; Opelz, G.; Tran, T.H.; Scherer, S.; Schwenger, V.; Kemmner, S.; Fischereder, M.; Stangl, M.; Hauser, I.A.; Sommerer, C.; Nusshag, C.; Kalble, F.; Speer, C.; Benning, L.; Bischofs, C.; Sauer, S.; Schubert, M.L.; Kunz, A.; Hückelhoven-Krauss, A.; Neuber, B.; Mehrabi, A.; Schwab, C.; Waldherr, R.; Sander, A.; Büsch, C.; Czock, D.; Böhmig, G.A.; Reiser, J.; Roers, A.; Müller-Tidow, C.; Terness, P.; Zeier, M.; Daniel, V.; Schaier, M., Koç University Research Center for Translational Medicine (KUTTAM) / Koç Üniversitesi Translasyonel Tıp Araştırma Merkezi (KUTTAM), and School of Medicine

Abstract

Introduction: donor-derived modified immune cells (MIC) induced long-term specific immunosuppression against the allogeneic donor in preclinical models of transplantation. In a phase I clinical trial (TOL-1 Study), MIC treatment resulted in a cellular phenotype that was directly and indirectly suppressive to the recipient's immune system allowing for reduction of conventional immunosuppressive therapy. Here, we describe a protocol for a randomised controlled, multicentre phase-IIb clinical trial of individualised immunosuppression with intravenously administered donor MIC compared with standard-of-care (SoC) in living donor kidney transplantation (TOL-2 Study). Methods and analysis: sixty-three living donor kidney transplant recipients from six German transplant centres are randomised 2:1 to treatment with MIC (MIC group, N=42) or no treatment with MIC (control arm, N=21). MIC are manufactured from donor peripheral blood mononuclear cells under Good Manufacturing Practice conditions. The primary objective of this trial is to determine the efficacy of MIC treatment together with reduced conventional immunosuppressive therapy in terms of achieving an operational tolerance-like phenotype compared with SoC 12 months after MIC administration. Key secondary endpoints are the number of patient-relevant infections as well as a composite of biopsy-proven acute rejection, graft loss, graft dysfunction or death. Immunosuppressive therapy of MIC-treated patients is reduced during follow-up under an extended immunological monitoring including human leucocyte antigen-antibody testing, and determination of lymphocyte subsets, for example, regulatory B lymphocytes (Breg) and antidonor T cell response. A Data Safety Monitoring Board has been established to allow an independent assessment of safety and efficacy. Ethics and dissemination: ethical approval has been provided by the Ethics Committee of the Medical Faculty of the University of Heidelberg, Heidelberg, Germany (AFmu-580/202, Preparation of the study was funded by the Federal Ministry of Education and Research, Berlin, Germany (FKZ 161B0560A, 161B0560B, and FKZ 031B0560A, 031B0560B), and TolerogenixX GmbH, Heidelberg, Germany (N/A). Conduct of the study is funded by TolerogenixX GmbH (N/A).

Published
2022

7. Einfluss des IDO2 Inhibitors D-1-Methyltryptophan auf die IDO Aktivität humaner Tumore und dendritischer Zellen

Author

Löb, S., Terness, P., Zieker, D., Schäfer, R., Brücher, B., Rammensee, H. -G., Königsrainer, A., Buhr, H. J., editor, Hölscher, A., editor, Izbicki, J. R., editor, Jauch, K. W., editor, Post, S., editor, Allgayer, H., editor, Bartsch, D. K., editor, Fries, H., editor, Ghadimi, B. M., editor, Habermann, J. K., editor, Kalthoff, H., editor, Schackert, H. K., editor, Bruns, C. J., editor, Duda, D. N., editor, Fändrich, F., editor, Heberer, M., editor, Nüssler, A. K., editor, Stark, G. B., editor, Brückner, U. B., editor, Ertel, W., editor, Faist, E., editor, Heidecke, C. D., editor, Kalff, J. C., editor, Menger, M. D., editor, Schade, U. F., editor, Vollmar, B., editor, Bechstein, W. O., editor, Klar, E., editor, Klempnauer, J., editor, Minor, T., editor, Neuhaus, P., editor, Schmidt, J., editor, Langer, S., editor, Laschke, M. W., editor, Machens, H. G., editor, Steinau, H. U., editor, Südkamp, N., editor, Vogt, P., editor, Berger, D., editor, Klinge, U., editor, Schachtrupp, A., editor, Schilling, M. K., editor, Schumpelick, V., editor, Altendorf-Hofmann, A., editor, Bollschweiler, E., editor, Bruch, H. -P., editor, Lehnert, T., editor, Lorenz, W., editor, Neugebauer, E., editor, Ohmann, C., editor, Seiler, C. M., editor, Becker, H., editor, Betzler, M., editor, Bittner, R., editor, Broelsch, C., editor, Büchler, M. W., editor, Bumm, R., editor, Dralle, H., editor, Friess, H., editor, Frilling, A., editor, Germer, C. T., editor, Hopt, U., editor, Jonas, S., editor, Jost, J., editor, Markus, B., editor, Raab, H. R., editor, Reith, H. B., editor, Schlag, P. M., editor, Teichmann, W., editor, Uhl, W., editor, Wenisch, H., editor, and Zornig, C., editor

Published
2009
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17. Induction of Long-Lasting Regulatory B Lymphocytes by Modified Immune Cells in Kidney Transplant Recipients

Author

Morath, Christian, Schaier, Matthias, Ibrahim, Eman, Wang, Lei, Kleist, Christian, Opelz, Gerhard, Süsal, Caner, Ponath, Gerald, Aly, Mostafa, Alvarez, Cristiam M., Kälble, Florian, Speer, Claudius, Benning, Louise, Nusshag, Christian, Pego da Silva, Luiza, Sommerer, Claudia, Hückelhoven-Krauss, Angela, Czock, David, Mehrabi, Arianeb, Schwab, Constantin, Waldherr, Rüdiger, Schnitzler, Paul, Merle, Uta, Tran, Thuong Hien, Scherer, Sabine, Böhmig, Georg A., Müller-Tidow, Carsten, Reiser, Jochen, Zeier, Martin, Schmitt, Michael, Terness, Peter, Schmitt, Anita, and Daniel, Volker

Abstract

In previous work, the authors demonstrated that kidney transplant recipients developed donor-specific unresponsiveness when they were given a pretransplant infusion of modified donor-derived PBMCs. In this study, they provide evidence that the immunosuppressive properties of these cells persist and the donor-specific unresponsiveness is long-lasting. In the four patients who received the highest dose of the modified immune cells, administration of these cells was associated with a striking increase in IL-10–producing regulatory B lymphocytes and evidence of the consensus gene expression signature of operational tolerance. In vitro, donor-specific unresponsiveness was abolished after B lymphocyte depletion, suggesting a direct pathophysiologic role for regulatory B lymphocytes. These findings support the notion that modified donor-derived PBMCs may be useful in kidney transplantation, but this approach requires further validation and rigorous controlled randomized studies.

Published
2023
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30. Mitomycin-C behandelte mononukleäre Zellen des peripheren Blutes in der Composite Tissue Allotransplantation

Author

Kiefer, J, Radu, CA, Horn, D, Kleist, C, Dittmar, L, Sandra, F, Rebel, M, Ryssel, H, Köllensperger, E, Gebhard, MM, Lehnhardt, M, Germann, G, and Terness, P

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Einleitung: Composite Tissue Allotransplantationen (CTA) eröffnen ein neues Feld der Transplantationschirurgie. Das Überleben klinischer CTAs übertrifft das von Organtransplantationen unter standardmäßiger immunsuppressiver Therapie. Hand- und Gesichtstransplantationen, die [for full text, please go to the a.m. URL], 43. Jahrestagung der Deutschen Gesellschaft der Plastischen, Rekonstruktiven und Ästhetischen Chirurgen (DGPRÄC), 17. Jahrestagung der Vereinigung der Deutschen Ästhetisch-Plastischen Chirurgen (VDÄPC)

Published
2012
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32. Einfluss des IDO2-Blockers D-1MT auf die IDO-Aktivität humaner Tumoren und dendritischer Zellen

Author

Löb, S., Terness, P., Zieker, D., Schäfer, R., Brücher, B., Rammensee, H.G., and Königsrainer, A.

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Introduction: Clinical phase-I-trials with cancer patients have been started with the aim of inducing tumor immunity by blocking the immunosuppressive action of indoleamine-2,3-dioxygenase (IDO) with the IDO2-inhibitor dextro-1-methyl-tryptophan (D-1MT). In this study we analyzed IDO2- and IDO1-expression[for full text, please go to the a.m. URL], 126. Kongress der Deutschen Gesellschaft für Chirurgie

Published
2009

41. The Natural Human-igg Anti-f(ab')(2) Antibody Recognizes A Conformational Igg1 Hinge Epitope

Author

Terness, P., Kohl, I., Hübener, G., Battistutta, R., Luis Moroder, Welschof, M., Dufter, C., Finger, M., Hain, C., Jung, M., and Opelz, G.

Subjects
Models, Molecular, Binding Sites, Protein Conformation, ALLOIMMUNIZATION, FLEXIBILITY, Molecular Sequence Data, FULLY SYNTHETIC IMMUNOGENS, NUCLEAR MAGNETIC-RESONANCE, IMMUNOGLOBULIN-G, IDIOTYPIC ANTIBODIES, FRAGMENT 225-232, B-CELLS, REGION, ASSOCIATION, In Vitro Techniques, Binding, Competitive, Antibodies, Anti-Idiotypic, Epitopes, Immunoglobulin Fab Fragments, Antibody Specificity, Immunoglobulin G, Humans, Amino Acid Sequence
Abstract

Natural IgG anti-F(ab')2 Abs are part of the physiologic immune repertoire and have important immunoregulatory functions. Although previous work suggested that some of these Abs recognize epitopes located in the constant region of the F(ab')2 molecule, an exact epitope mapping has not been performed. We found that the anti-F(ab')2 Ab binds strongly to F(ab')2 but only weakly to Fab fragments. Fab fragments are lacking the core and lower hinge region. In our experiments, we show that the IgG anti-F(ab')2 Ab binds strongly to a synthetic double chain peptide (225-237/225'-237') comprising the core and lower hinge region of the human IgG1 molecule. In contrast, it binds only weakly to the same peptide in monomeric form (225-237) or to a short double chain hinge peptide (225-232/225'-232'). The double chain peptides comprise a cyclic region between the two cystine bridges and an exocyclic region. Previous nuclear magnetic resonance analyses showed that the cyclic portion of the short double chain hinge peptide adopts the same conformation as that found in the intact IgG1 molecule. The dichroic properties of the short and long double chain hinge peptides indicate that they have identical conformations in their cyclic regions, but have different conformations in their exocyclic regions. The conformational differences in the exocyclic regions explain the binding of the Ab to the long double chain hinge peptide and the lack of binding to the short one. The circular dichroism spectrum of the monomeric hinge peptide, which is not recognized by the Ab, is consistent with the absence of an ordered peptide structure. These findings lead us to conclude that the IgG anti-F(ab')2 Ab recognizes a conformational IgG1 hinge epitope.

Published
1995

44. Single-Chain Fv-Based Affinity Purification of the Cellular Stress Protein gp96 for Vaccine Development.

Author

Walker, John M., Krauss, Jürgen, Kleist, Christian, Arnold-Schild, Daniéle, Welschof, Martin, Finger, Martina, Opelz, Gerhard, Rammensee, Hans-Georg, Schild, Hansjörg, and Terness, Peter

Abstract

Cellular stress proteins like the classical heat-shock proteins (HSPs) hsp70 (1-3), hsp90 (3) and hsp110 (4); the glucose-regulated proteins gp96/GRP94 (3,5) and grp170 (4); as well as the endoplasmic chaperone calreticulin (6,7) have been shown to induce cytotoxic T-cell responses and protective immunity when isolated from tumor or infected cells and used to vaccinate animals (8-10; reviewed in refs. 11-17). The specificity of the immune responses is owing to antigenic peptides associated with the HSPs (18-26). The HSP-peptide complexes are taken up by professional antigen-presenting cells (APCs) for effective presentation of the peptides to T cells (19,27-33). The extensively studied endoplasmic reticulum-resident chaperone gp96 is most efficient and promising in this regard (34-39); encouraging clinical studies with human cancer patients (40). [ABSTRACT FROM AUTHOR]

Published
2003
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