Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment

Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment

Abstract Background Treatment of patients with solid tumors and KRAS mutations remains disappointing. One option is the combined inhibition of pathways involved in RAF‐MEK‐ERK and PI3K‐AKT‐mTOR. Methods Patients with relapsed solid tumors were treated with escalating doses of everolimus (E) 2.5‐10.0...

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Main Authors: Lucia Nogova, Christian Mattonet, Matthias Scheffler, Max Taubert, Masyar Gardizi, Martin L. Sos, Sebastian Michels, Rieke N. Fischer, Meike Limburg, Diana S.Y. Abdulla, Thorsten Persigehl, Carsten Kobe, Sabine Merkelbach‐Bruse, Jeremy Franklin, Heiko Backes, Roland Schnell, Dirk Behringer, Britta Kaminsky, Martina Eichstaedt, Christoph Stelzer, Martina Kinzig, Fritz Sörgel, Yingying Tian, Lisa Junge, Ahmed A. Suleiman, Sebastian Frechen, Dennis Rokitta, Dongsheng Ouyang, Uwe Fuhr, Reinhard Buettner, Jürgen Wolf
Format: Article
Language:English
Published: Wiley 2020-07-01
Series:Cancer Medicine
Subjects:
FDG‐PET
KRAS mutation
non‐small‐cell lung cancer
pharmacodynamics
pharmacokinetics
Phase‐I trial
Online Access:https://doi.org/10.1002/cam4.3131
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author Lucia Nogova
Christian Mattonet
Matthias Scheffler
Max Taubert
Masyar Gardizi
Martin L. Sos
Sebastian Michels
Rieke N. Fischer
Meike Limburg
Diana S.Y. Abdulla
Thorsten Persigehl
Carsten Kobe
Sabine Merkelbach‐Bruse
Jeremy Franklin
Heiko Backes
Roland Schnell
Dirk Behringer
Britta Kaminsky
Martina Eichstaedt
Christoph Stelzer
Martina Kinzig
Fritz Sörgel
Yingying Tian
Lisa Junge
Ahmed A. Suleiman
Sebastian Frechen
Dennis Rokitta
Dongsheng Ouyang
Uwe Fuhr
Reinhard Buettner
Jürgen Wolf
spellingShingle Lucia Nogova
Christian Mattonet
Matthias Scheffler
Max Taubert
Masyar Gardizi
Martin L. Sos
Sebastian Michels
Rieke N. Fischer
Meike Limburg
Diana S.Y. Abdulla
Thorsten Persigehl
Carsten Kobe
Sabine Merkelbach‐Bruse
Jeremy Franklin
Heiko Backes
Roland Schnell
Dirk Behringer
Britta Kaminsky
Martina Eichstaedt
Christoph Stelzer
Martina Kinzig
Fritz Sörgel
Yingying Tian
Lisa Junge
Ahmed A. Suleiman
Sebastian Frechen
Dennis Rokitta
Dongsheng Ouyang
Uwe Fuhr
Reinhard Buettner
Jürgen Wolf
Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment
Cancer Medicine
FDG‐PET
KRAS mutation
non‐small‐cell lung cancer
pharmacodynamics
pharmacokinetics
Phase‐I trial
author_facet Lucia Nogova
Christian Mattonet
Matthias Scheffler
Max Taubert
Masyar Gardizi
Martin L. Sos
Sebastian Michels
Rieke N. Fischer
Meike Limburg
Diana S.Y. Abdulla
Thorsten Persigehl
Carsten Kobe
Sabine Merkelbach‐Bruse
Jeremy Franklin
Heiko Backes
Roland Schnell
Dirk Behringer
Britta Kaminsky
Martina Eichstaedt
Christoph Stelzer
Martina Kinzig
Fritz Sörgel
Yingying Tian
Lisa Junge
Ahmed A. Suleiman
Sebastian Frechen
Dennis Rokitta
Dongsheng Ouyang
Uwe Fuhr
Reinhard Buettner
Jürgen Wolf
author_sort Lucia Nogova
title Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment
title_short Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment
title_full Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment
title_fullStr Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment
title_full_unstemmed Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessment
title_sort sorafenib and everolimus in patients with advanced solid tumors and kras‐mutated nsclc: a phase i trial with early pharmacodynamic fdg‐pet assessment
publisher Wiley
series Cancer Medicine
issn 2045-7634
publishDate 2020-07-01
description Abstract Background Treatment of patients with solid tumors and KRAS mutations remains disappointing. One option is the combined inhibition of pathways involved in RAF‐MEK‐ERK and PI3K‐AKT‐mTOR. Methods Patients with relapsed solid tumors were treated with escalating doses of everolimus (E) 2.5‐10.0 mg/d in a 14‐day run‐in phase followed by combination therapy with sorafenib (S) 800 mg/d from day 15. KRAS mutational status was assessed retrospectively in the escalation phase. Extension phase included KRAS‐mutated non–small‐cell lung cancer (NSCLC) only. Pharmacokinetic analyses were accompanied by pharmacodynamics assessment of E by FDG‐PET. Efficacy was assessed by CT scans every 6 weeks of combination. Results Of 31 evaluable patients, 15 had KRAS mutation, 4 patients were negative for KRAS mutation, and the KRAS status remained unknown in 12 patients. Dose‐limiting toxicity (DLT) was not reached. The maximum tolerated dose (MTD) was defined as 7.5 mg/d E + 800 mg/d S due to toxicities at previous dose level (10 mg/d E + 800 mg/d S) including leucopenia/thrombopenia III° and pneumonia III° occurring after the DLT interval. The metabolic response rate in FDG‐PET was 17% on day 5 and 20% on day 14. No patient reached partial response in CT scan. Median progression free survival (PFS) and overall survival (OS) were 3.25 and 5.85 months, respectively. Conclusions Treatment of patients with relapsed solid tumors with 7.5 mg/d E and 800 mg/d S is safe and feasible. Early metabolic response in FDG‐PET was not confirmed in CT scan several weeks later. The combination of S and E is obviously not sufficient to induce durable responses in patients with KRAS‐mutant solid tumors.
topic FDG‐PET
KRAS mutation
non‐small‐cell lung cancer
pharmacodynamics
pharmacokinetics
Phase‐I trial
url https://doi.org/10.1002/cam4.3131
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spelling doaj-04f6918ff70742839866e3f4fa056a572020-11-25T02:35:48ZengWileyCancer Medicine2045-76342020-07-019144991500710.1002/cam4.3131Sorafenib and everolimus in patients with advanced solid tumors and KRAS‐mutated NSCLC: A phase I trial with early pharmacodynamic FDG‐PET assessmentLucia Nogova0Christian Mattonet1Matthias Scheffler2Max Taubert3Masyar Gardizi4Martin L. Sos5Sebastian Michels6Rieke N. Fischer7Meike Limburg8Diana S.Y. Abdulla9Thorsten Persigehl10Carsten Kobe11Sabine Merkelbach‐Bruse12Jeremy Franklin13Heiko Backes14Roland Schnell15Dirk Behringer16Britta Kaminsky17Martina Eichstaedt18Christoph Stelzer19Martina Kinzig20Fritz Sörgel21Yingying Tian22Lisa Junge23Ahmed A. Suleiman24Sebastian Frechen25Dennis Rokitta26Dongsheng Ouyang27Uwe Fuhr28Reinhard Buettner29Jürgen Wolf30Department I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Center for Pharmacology Department I of Pharmacology University of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Institute for Diagnostics und Intervention Radiology University of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Department for Nuclear Medicine University of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Institute for PathologyUniversity of Cologne Cologne GermanyFaculty of Medicine Institute for Medical Statistics and Bioinformatics University of Cologne Cologne GermanyMax Planck Institute for Metabolism Research Cologne GermanyPraxis for Medical Oncology and Haematology (PIOH) Frechen GermanyHeamatology and Oncology Augusta Hospital Bochum GermanyBethanien Hospital Solingen GermanyMedical Oncology and Haematology St. Marien Hospital Düren GermanyInstitute for Biomedical and Pharmaceutical Research (IBMP) Nürnberg GermanyInstitute for Biomedical and Pharmaceutical Research (IBMP) Nürnberg GermanyInstitute for Biomedical and Pharmaceutical Research (IBMP) Nürnberg GermanyFaculty of Medicine and University Hospital Cologne Center for Pharmacology Department I of Pharmacology University of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Center for Pharmacology Department I of Pharmacology University of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Center for Pharmacology Department I of Pharmacology University of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Center for Pharmacology Department I of Pharmacology University of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Center for Pharmacology Department I of Pharmacology University of Cologne Cologne GermanyDepartment of Clinical Pharmacology Xiangya HospitalCentral South University Changsha ChinaFaculty of Medicine and University Hospital Cologne Center for Pharmacology Department I of Pharmacology University of Cologne Cologne GermanyFaculty of Medicine and University Hospital Cologne Institute for PathologyUniversity of Cologne Cologne GermanyDepartment I of Internal Medicine Center for Integrated Oncology Aachen Bonn Cologne Duesseldorf Lung Cancer GroupUniversity of Cologne Cologne GermanyAbstract Background Treatment of patients with solid tumors and KRAS mutations remains disappointing. One option is the combined inhibition of pathways involved in RAF‐MEK‐ERK and PI3K‐AKT‐mTOR. Methods Patients with relapsed solid tumors were treated with escalating doses of everolimus (E) 2.5‐10.0 mg/d in a 14‐day run‐in phase followed by combination therapy with sorafenib (S) 800 mg/d from day 15. KRAS mutational status was assessed retrospectively in the escalation phase. Extension phase included KRAS‐mutated non–small‐cell lung cancer (NSCLC) only. Pharmacokinetic analyses were accompanied by pharmacodynamics assessment of E by FDG‐PET. Efficacy was assessed by CT scans every 6 weeks of combination. Results Of 31 evaluable patients, 15 had KRAS mutation, 4 patients were negative for KRAS mutation, and the KRAS status remained unknown in 12 patients. Dose‐limiting toxicity (DLT) was not reached. The maximum tolerated dose (MTD) was defined as 7.5 mg/d E + 800 mg/d S due to toxicities at previous dose level (10 mg/d E + 800 mg/d S) including leucopenia/thrombopenia III° and pneumonia III° occurring after the DLT interval. The metabolic response rate in FDG‐PET was 17% on day 5 and 20% on day 14. No patient reached partial response in CT scan. Median progression free survival (PFS) and overall survival (OS) were 3.25 and 5.85 months, respectively. Conclusions Treatment of patients with relapsed solid tumors with 7.5 mg/d E and 800 mg/d S is safe and feasible. Early metabolic response in FDG‐PET was not confirmed in CT scan several weeks later. The combination of S and E is obviously not sufficient to induce durable responses in patients with KRAS‐mutant solid tumors.https://doi.org/10.1002/cam4.3131FDG‐PETKRAS mutationnon‐small‐cell lung cancerpharmacodynamicspharmacokineticsPhase‐I trial

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