Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia

BACKGROUND: Until today, adult and pediatric clinical trials investigating single-agent or combinatorial HDAC inhibitors including vorinostat in solid tumors have largely failed to demonstrate efficacy. These results may in part be explained by data from preclinical models showing significant activi...

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Autores principales: van Tilburg, Cornelis M., Milde, Till, Witt, Ruth, Ecker, Jonas, Hielscher, Thomas, Seitz, Angelika, Schenk, Jens-Peter, Buhl, Juliane L., Riehl, Dennis, Frühwald, Michael C., Pekrun, Arnulf, Rossig, Claudia, Wieland, Regina, Flotho, Christian, Kordes, Uwe, Gruhn, Bernd, Simon, Thorsten, Linderkamp, Christin, Sahm, Felix, Taylor, Lenka, Freitag, Angelika, Burhenne, Jürgen, Foerster, Kathrin I., Meid, Andreas D., Pfister, Stefan M., Karapanagiotou-Schenkel, Irini, Witt, Olaf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2019
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6902473/
https://www.ncbi.nlm.nih.gov/pubmed/31823832
http://dx.doi.org/10.1186/s13148-019-0775-1
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author van Tilburg, Cornelis M.
Milde, Till
Witt, Ruth
Ecker, Jonas
Hielscher, Thomas
Seitz, Angelika
Schenk, Jens-Peter
Buhl, Juliane L.
Riehl, Dennis
Frühwald, Michael C.
Pekrun, Arnulf
Rossig, Claudia
Wieland, Regina
Flotho, Christian
Kordes, Uwe
Gruhn, Bernd
Simon, Thorsten
Linderkamp, Christin
Sahm, Felix
Taylor, Lenka
Freitag, Angelika
Burhenne, Jürgen
Foerster, Kathrin I.
Meid, Andreas D.
Pfister, Stefan M.
Karapanagiotou-Schenkel, Irini
Witt, Olaf
author_facet van Tilburg, Cornelis M.
Milde, Till
Witt, Ruth
Ecker, Jonas
Hielscher, Thomas
Seitz, Angelika
Schenk, Jens-Peter
Buhl, Juliane L.
Riehl, Dennis
Frühwald, Michael C.
Pekrun, Arnulf
Rossig, Claudia
Wieland, Regina
Flotho, Christian
Kordes, Uwe
Gruhn, Bernd
Simon, Thorsten
Linderkamp, Christin
Sahm, Felix
Taylor, Lenka
Freitag, Angelika
Burhenne, Jürgen
Foerster, Kathrin I.
Meid, Andreas D.
Pfister, Stefan M.
Karapanagiotou-Schenkel, Irini
Witt, Olaf
author_sort van Tilburg, Cornelis M.
collection PubMed
description BACKGROUND: Until today, adult and pediatric clinical trials investigating single-agent or combinatorial HDAC inhibitors including vorinostat in solid tumors have largely failed to demonstrate efficacy. These results may in part be explained by data from preclinical models showing significant activity only at higher concentrations compared to those achieved with current dosing regimens. In the current pediatric trial, we applied an intra-patient dose escalation design. The purpose of this trial was to determine a safe dose recommendation (SDR) of single-agent vorinostat for intra-patient dose escalation, pharmacokinetic analyses (PK), and activity evaluation in children (3–18 years) with relapsed or therapy-refractory malignancies. RESULTS: A phase I intra-patient dose (de)escalation was performed until individual maximum tolerated dose (MTD). The starting dose was 180 mg/m(2)/day with weekly dose escalations of 50 mg/m(2) until DLT/maximum dose. After MTD determination, patients seamlessly continued in phase II with disease assessments every 3 months. PK and plasma cytokine profiles were determined. Fifty of 52 patients received treatment. n = 27/50 (54%) completed the intra-patient (de)escalation and entered phase II. An SDR of 130 mg/m(2)/day was determined (maximum, 580 mg/m(2)/day). n = 46/50 (92%) patients experienced treatment-related AEs which were mostly reversible and included thrombocytopenia, fatigue, nausea, diarrhea, anemia, and vomiting. n = 6/50 (12%) had treatment-related SAEs. No treatment-related deaths occurred. Higher dose levels resulted in higher C(max). Five patients achieved prolonged disease control (> 12 months) and showed a higher C(max) (> 270 ng/mL) and MTDs. Best overall response (combining PR and SD, no CR observed) rate in phase II was 6/27 (22%) with a median PFS and OS of 5.3 and 22.4 months. Low levels of baseline cytokine expression were significantly correlated with favorable outcome. CONCLUSION: An SDR of 130 mg/m(2)/day for individual dose escalation was determined. Higher drug exposure was associated with responses and long-term disease stabilization with manageable toxicity. Patients with low expression of plasma cytokine levels at baseline were able to tolerate higher doses of vorinostat and benefited from treatment. Baseline cytokine profile is a promising potential predictive biomarker. TRIAL REGISTRATION: ClinicalTrials.gov, NCT01422499. Registered 24 August 2011,
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spelling pubmed-69024732019-12-11 Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia van Tilburg, Cornelis M. Milde, Till Witt, Ruth Ecker, Jonas Hielscher, Thomas Seitz, Angelika Schenk, Jens-Peter Buhl, Juliane L. Riehl, Dennis Frühwald, Michael C. Pekrun, Arnulf Rossig, Claudia Wieland, Regina Flotho, Christian Kordes, Uwe Gruhn, Bernd Simon, Thorsten Linderkamp, Christin Sahm, Felix Taylor, Lenka Freitag, Angelika Burhenne, Jürgen Foerster, Kathrin I. Meid, Andreas D. Pfister, Stefan M. Karapanagiotou-Schenkel, Irini Witt, Olaf Clin Epigenetics Research BACKGROUND: Until today, adult and pediatric clinical trials investigating single-agent or combinatorial HDAC inhibitors including vorinostat in solid tumors have largely failed to demonstrate efficacy. These results may in part be explained by data from preclinical models showing significant activity only at higher concentrations compared to those achieved with current dosing regimens. In the current pediatric trial, we applied an intra-patient dose escalation design. The purpose of this trial was to determine a safe dose recommendation (SDR) of single-agent vorinostat for intra-patient dose escalation, pharmacokinetic analyses (PK), and activity evaluation in children (3–18 years) with relapsed or therapy-refractory malignancies. RESULTS: A phase I intra-patient dose (de)escalation was performed until individual maximum tolerated dose (MTD). The starting dose was 180 mg/m(2)/day with weekly dose escalations of 50 mg/m(2) until DLT/maximum dose. After MTD determination, patients seamlessly continued in phase II with disease assessments every 3 months. PK and plasma cytokine profiles were determined. Fifty of 52 patients received treatment. n = 27/50 (54%) completed the intra-patient (de)escalation and entered phase II. An SDR of 130 mg/m(2)/day was determined (maximum, 580 mg/m(2)/day). n = 46/50 (92%) patients experienced treatment-related AEs which were mostly reversible and included thrombocytopenia, fatigue, nausea, diarrhea, anemia, and vomiting. n = 6/50 (12%) had treatment-related SAEs. No treatment-related deaths occurred. Higher dose levels resulted in higher C(max). Five patients achieved prolonged disease control (> 12 months) and showed a higher C(max) (> 270 ng/mL) and MTDs. Best overall response (combining PR and SD, no CR observed) rate in phase II was 6/27 (22%) with a median PFS and OS of 5.3 and 22.4 months. Low levels of baseline cytokine expression were significantly correlated with favorable outcome. CONCLUSION: An SDR of 130 mg/m(2)/day for individual dose escalation was determined. Higher drug exposure was associated with responses and long-term disease stabilization with manageable toxicity. Patients with low expression of plasma cytokine levels at baseline were able to tolerate higher doses of vorinostat and benefited from treatment. Baseline cytokine profile is a promising potential predictive biomarker. TRIAL REGISTRATION: ClinicalTrials.gov, NCT01422499. Registered 24 August 2011, BioMed Central 2019-12-10 /pmc/articles/PMC6902473/ /pubmed/31823832 http://dx.doi.org/10.1186/s13148-019-0775-1 Text en © The Author(s). 2019 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
van Tilburg, Cornelis M.
Milde, Till
Witt, Ruth
Ecker, Jonas
Hielscher, Thomas
Seitz, Angelika
Schenk, Jens-Peter
Buhl, Juliane L.
Riehl, Dennis
Frühwald, Michael C.
Pekrun, Arnulf
Rossig, Claudia
Wieland, Regina
Flotho, Christian
Kordes, Uwe
Gruhn, Bernd
Simon, Thorsten
Linderkamp, Christin
Sahm, Felix
Taylor, Lenka
Freitag, Angelika
Burhenne, Jürgen
Foerster, Kathrin I.
Meid, Andreas D.
Pfister, Stefan M.
Karapanagiotou-Schenkel, Irini
Witt, Olaf
Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia
title Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia
title_full Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia
title_fullStr Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia
title_full_unstemmed Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia
title_short Phase I/II intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia
title_sort phase i/ii intra-patient dose escalation study of vorinostat in children with relapsed solid tumor, lymphoma, or leukemia
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6902473/
https://www.ncbi.nlm.nih.gov/pubmed/31823832
http://dx.doi.org/10.1186/s13148-019-0775-1
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