Your search keyword '"Maja J.A. de Jonge"' showing total 112 results

1. Data Supplement from Phase I Study of RGB-286638, A Novel, Multitargeted Cyclin-Dependent Kinase Inhibitor in Patients with Solid Tumors

Author

Maja J.A. de Jonge, Ron H.J. Mathijssen, Erik A.C. Wiemer, Hannes Loferer, Nicole Naus, Cor H.J. Lamers, Peter de Bruijn, Herman Burger, and Diane A.J. van der Biessen

Abstract

Supplementary Figure S2: Relationship between area under the curves (AUC) and the administered dose on day 1 of drug intake.

Published

2023

2. Table S2 from Pharmacokinetics, Safety, and Antitumor Effect of Apalutamide with Abiraterone Acetate plus Prednisone in Metastatic Castration-Resistant Prostate Cancer: Phase Ib Study

Author

Fred Saad, Juhui J. Jiao, Charlene Abrams, Caly Chien, Peter Hellemans, Margaret K. Yu, Terence W. Friedlander, Gerhardt Attard, Maja J.A. de Jonge, Ronald de Wit, Kim N. Chi, and Edwin M. Posadas

Abstract

Duration of treatment exposure and PSA response since start of therapy for patients receiving systemic therapy with an AR signaling inhibitor prior to study entry

Published

2023

3. Data from Pharmacokinetics, Safety, and Antitumor Effect of Apalutamide with Abiraterone Acetate plus Prednisone in Metastatic Castration-Resistant Prostate Cancer: Phase Ib Study

Author

Fred Saad, Juhui J. Jiao, Charlene Abrams, Caly Chien, Peter Hellemans, Margaret K. Yu, Terence W. Friedlander, Gerhardt Attard, Maja J.A. de Jonge, Ronald de Wit, Kim N. Chi, and Edwin M. Posadas

Abstract

Purpose:Apalutamide is a next-generation androgen receptor (AR) inhibitor approved for patients with nonmetastatic castration-resistant prostate cancer (CRPC) and metastatic castration-sensitive prostate cancer. We evaluated the pharmacokinetics, safety, and antitumor activity of apalutamide combined with abiraterone acetate plus prednisone (AA-P) in patients with metastatic CRPC (mCRPC).Patients and Methods:Multicenter, open-label, phase Ib drug–drug interaction study conducted in 57 patients with mCRPC treated with 1,000 mg abiraterone acetate plus 10 mg prednisone daily beginning on cycle 1 day 1 (C1D1) and 240 mg apalutamide daily starting on C1D8 in 28-day cycles. Serial blood samples for pharmacokinetic analysis were collected on C1D7 and C2D8.Results:Systemic exposure to abiraterone, prednisone, and prednisolone decreased 14%, 61%, and 42%, respectively, when apalutamide was coadministered with AA-P. No increase in mineralocorticoid excess–related adverse events was observed. Patients without prior exposure to AR signaling inhibitors had longer median treatment duration and greater mean decrease in prostate-specific antigen (PSA) from baseline compared with those who had received prior therapy. Confirmed PSA reductions of ≥50% from baseline at any time were observed in 80% (12/15) of AR signaling inhibitor–naïve patients and 14% (6/42) of AR signaling inhibitor–treated patients.Conclusions:Treatment with apalutamide plus AA-P was well tolerated and showed evidence of antitumor activity in patients with mCRPC, including those with disease progression on AR signaling inhibitors. No clinically significant pharmacokinetic interaction was observed between abiraterone and apalutamide; however, apalutamide decreased exposure to prednisone. These data support development of 1,000 mg abiraterone acetate plus 10 mg prednisone daily with 240 mg apalutamide daily in patients with mCRPC.

Published

2023

4. Data from The c-Met Tyrosine Kinase Inhibitor JNJ-38877605 Causes Renal Toxicity through Species-Specific Insoluble Metabolite Formation

Author

Ferry A.L.M. Eskens, Johann S. de Bono, Peter Hellemans, Leni van Doorn, Maja J.A. de Jonge, Erio Barale, Ann Lampo, Hendrik-Tobias Arkenau, Hilde H. Bohets, and Martijn P. Lolkema

Abstract

Purpose: The receptor tyrosine kinase c-Met plays an important role in tumorigenesis and is a novel target for anticancer treatment. This phase I, first-in-human trial, explored safety, pharmacokinetics, pharmacodynamics, and initial antitumor activity of JNJ-38877605, a potent and selective c-Met inhibitor.Experimental Design: We performed a phase I dose-escalation study according to the standard 3+3 design.Results: Even at subtherapeutic doses, mild though recurrent renal toxicity was observed in virtually all patients. Renal toxicity had not been observed in preclinical studies in rats and dogs. Additional preclinical studies pointed toward the rabbit as a suitable toxicology model, as the formation of the M10 metabolite of JNJ-38877605 specifically occurred in rabbits and humans. Additional toxicology studies in rabbits clearly demonstrated that JNJ-38877605 induced species-specific renal toxicity. Histopathological evaluation in rabbits revealed renal crystal formation with degenerative and inflammatory changes. Identification of the components of these renal crystals revealed M1/3 and M5/6 metabolites. Accordingly, it was found that humans and rabbits showed significantly increased systemic exposure to these metabolites relative to other species. These main culprit insoluble metabolites were generated by aldehyde oxidase activity. Alternative dosing schedules of JNJ-3877605 and concomitant probenecid administration in rabbits failed to prevent renal toxicity at dose levels that could be pharmacologically active.Conclusions: Combined clinical and correlative preclinical studies suggest that renal toxicity of JNJ-38877605 is caused by the formation of species-specific insoluble metabolites. These observations preclude further clinical development of JNJ-38877605. Clin Cancer Res; 21(10); 2297–304. ©2015 AACR.

Published

2023

5. Supplementary Figure 1B from Biologic and Clinical Activity of Tivozanib (AV-951, KRN-951), a Selective Inhibitor of VEGF Receptor-1, -2, and -3 Tyrosine Kinases, in a 4-Week-On, 2-Week-Off Schedule in Patients with Advanced Solid Tumors

Author

Jaap Verweij, Leni van Doorn, Maarten Thomeer, Herman Burger, Kunihiko Hayashi, Brooke Esteves, Monette M. Cotreau, Toshiyuki Isoe, Pankaj Bhargava, Maja J.A. de Jonge, and Ferry A.L.M. Eskens

Abstract

PDF file - 100K

Published

2023

6. Data from Phase I Study of RGB-286638, A Novel, Multitargeted Cyclin-Dependent Kinase Inhibitor in Patients with Solid Tumors

Author

Maja J.A. de Jonge, Ron H.J. Mathijssen, Erik A.C. Wiemer, Hannes Loferer, Nicole Naus, Cor H.J. Lamers, Peter de Bruijn, Herman Burger, and Diane A.J. van der Biessen

Abstract

Purpose: RGB-286638 is a multitargeted inhibitor with targets comprising the family of cyclin-dependent kinases (CDK) and a range of other cancer-relevant tyrosine and serine/threonine kinases. The objectives of this first in human trial of RGB-286638, given i.v. on days 1 to 5 every 28 days, were to determine the maximum tolerated dose (MTD) and to evaluate the pharmacokinetic (PK) and pharmacodynamic (PD) profiles of this new drug.Experimental Design: Sequential cohorts of 3 to 6 patients were treated per dose level. Blood, urine samples, and skin biopsies for full PK and/or PD analyses were collected.Results: Twenty-six patients were enrolled in 6-dose levels from 10 to 160 mg/d. Four dose-limiting toxicities were observed in 2 of the 6 patients enrolled at the highest dose level. These toxicities were AST/ALT elevations in 1 patient, paroxysmal supraventricular tachycardias (SVTs), hypotension, and an increase in troponin T in another patient. The plasma PK of RGB-286638 was shown to be linear over the studied doses. The interpatient variability in clearance was moderate (variation coefficient 7%–36%). The PD analyses in peripheral blood mononuclear cells, serum (apoptosis induction) and skin biopsies (Rb, p-Rb, Ki-67, and p27KIP1 expression) did not demonstrate a consistent modulation of mechanism-related biomarkers with the exception of lowered Ki-67 levels at the MTD level. The recommended MTD for phase II studies is 120 mg/d.Conclusions: RGB-286638 is tolerated when administered at 120 mg/d for 5 days every 28 days. Prolonged disease stabilization (range, 2–14 months) was seen across different dose levels. Clin Cancer Res; 20(18); 4776–83. ©2014 AACR.

Published

2023

7. CCR Translation for This Article from Phase I Pharmacokinetic and Pharmacodynamic Study of the First-in-Class Spliceosome Inhibitor E7107 in Patients with Advanced Solid Tumors

Author

Josep Tabernero, José Baselga, Maria Josepa Carreras, Erik A.C. Wiemer, Yoshiharu Mizui, Maja J.A. de Jonge, Adelaida Piera, James P. O'Brien, Herman Burger, Francisco J. Ramos, and Ferry A.L.M. Eskens

Abstract

CCR Translation for This Article from Phase I Pharmacokinetic and Pharmacodynamic Study of the First-in-Class Spliceosome Inhibitor E7107 in Patients with Advanced Solid Tumors

Published

2023

8. Supplementary Figure 1 from Biologic and Clinical Activity of Tivozanib (AV-951, KRN-951), a Selective Inhibitor of VEGF Receptor-1, -2, and -3 Tyrosine Kinases, in a 4-Week-On, 2-Week-Off Schedule in Patients with Advanced Solid Tumors

Author

Jaap Verweij, Leni van Doorn, Maarten Thomeer, Herman Burger, Kunihiko Hayashi, Brooke Esteves, Monette M. Cotreau, Toshiyuki Isoe, Pankaj Bhargava, Maja J.A. de Jonge, and Ferry A.L.M. Eskens

Abstract

PDF file - 357K

Published

2023

9. Table S1 from Pharmacokinetics, Safety, and Antitumor Effect of Apalutamide with Abiraterone Acetate plus Prednisone in Metastatic Castration-Resistant Prostate Cancer: Phase Ib Study

Author

Fred Saad, Juhui J. Jiao, Charlene Abrams, Caly Chien, Peter Hellemans, Margaret K. Yu, Terence W. Friedlander, Gerhardt Attard, Maja J.A. de Jonge, Ronald de Wit, Kim N. Chi, and Edwin M. Posadas

Abstract

Plasma pharmacokinetic parameters of abiraterone, APA, N-desmethyl APA, prednisone, and prednisolone following oral administration of AA-P on C1D7 and APA plus AA-P on C2D8

Published

2023

10. Supplemental methods from The c-Met Tyrosine Kinase Inhibitor JNJ-38877605 Causes Renal Toxicity through Species-Specific Insoluble Metabolite Formation

Author

Ferry A.L.M. Eskens, Johann S. de Bono, Peter Hellemans, Leni van Doorn, Maja J.A. de Jonge, Erio Barale, Ann Lampo, Hendrik-Tobias Arkenau, Hilde H. Bohets, and Martijn P. Lolkema

Abstract

Supplemental methods. additional description of methods

Published

2023

11. Figure Legends from Pharmacokinetics, Safety, and Antitumor Effect of Apalutamide with Abiraterone Acetate plus Prednisone in Metastatic Castration-Resistant Prostate Cancer: Phase Ib Study

Author

Fred Saad, Juhui J. Jiao, Charlene Abrams, Caly Chien, Peter Hellemans, Margaret K. Yu, Terence W. Friedlander, Gerhardt Attard, Maja J.A. de Jonge, Ronald de Wit, Kim N. Chi, and Edwin M. Posadas

Abstract

Figure legends for Figure S1 and Figure S2

Published

2023

12. Figure S2 from Pharmacokinetics, Safety, and Antitumor Effect of Apalutamide with Abiraterone Acetate plus Prednisone in Metastatic Castration-Resistant Prostate Cancer: Phase Ib Study

Author

Fred Saad, Juhui J. Jiao, Charlene Abrams, Caly Chien, Peter Hellemans, Margaret K. Yu, Terence W. Friedlander, Gerhardt Attard, Maja J.A. de Jonge, Ronald de Wit, Kim N. Chi, and Edwin M. Posadas

Abstract

Confirmed PSA response (as change from baseline) at any time for patients who received no prior therapy with AA-P or ENZ and patients who received therapy with AA-P only, ENZ only, or both AA-P and ENZ prior to study entry. Postbaseline PSA measurements were not available from two patients.

Published

2023

13. Supplemental tables 1-6 from The c-Met Tyrosine Kinase Inhibitor JNJ-38877605 Causes Renal Toxicity through Species-Specific Insoluble Metabolite Formation

Author

Ferry A.L.M. Eskens, Johann S. de Bono, Peter Hellemans, Leni van Doorn, Maja J.A. de Jonge, Erio Barale, Ann Lampo, Hendrik-Tobias Arkenau, Hilde H. Bohets, and Martijn P. Lolkema

Abstract

Supplemental tables 1-6. Supplemental table 1: Patient Demographics and Baseline Characteristics. Supplemental table 2. Plasma Pharmacokinetic parameters. Supplemental table 3. Identification of metabolites of JNJ-38877605. Supplemental table 3. Identification of metabolites of JNJ-38877605. Supplementary table 5: noteworthy post-mortem changes – 1-month recovery phase. Supplementary table 6: noteworthy microscopic changes (Probenecid study.

Published

2023

14. Data from Biologic and Clinical Activity of Tivozanib (AV-951, KRN-951), a Selective Inhibitor of VEGF Receptor-1, -2, and -3 Tyrosine Kinases, in a 4-Week-On, 2-Week-Off Schedule in Patients with Advanced Solid Tumors

Author

Jaap Verweij, Leni van Doorn, Maarten Thomeer, Herman Burger, Kunihiko Hayashi, Brooke Esteves, Monette M. Cotreau, Toshiyuki Isoe, Pankaj Bhargava, Maja J.A. de Jonge, and Ferry A.L.M. Eskens

Abstract

Purpose: To assess the maximum tolerated dose (MTD)/dose-limiting toxicities (DLT), safety, pharmacokinetics, and pharmacodynamics of tivozanib, a potent and selective oral VEGF receptor (VEGFR) tyrosine kinase inhibitor.Experimental Design: Dose levels of 1.0, 1.5, and 2.0 mg/d tivozanib for 28 days followed by 14 days of medication were explored in patients with advanced solid tumors.Results: Forty-one patients were enrolled. Animal data incorrectly predicted toxicity, resulting in DLTs at the starting dose (2.0 mg) consisting of grade 3 proteinuria and hypertension and grade 3 ataxia. At 1.0 mg, no DLT was observed. At an intermediate dose (1.5 mg), 1 patient experienced DLT consisting of grade 3 hypertension. This dose was determined as the MTD. Of 10 additional patients treated at 1.5 mg, 1 patient each experienced grade 3 hypertension and grade 3 fatigue, and 2 patients experienced grade 3 and 4 transaminase elevation. In 12 additional patients treated at 1.0 mg, no DLT was observed. Pharmacokinetics displayed long absorption time, dose proportional exposure, and a half-life of 4.7 days. Plasma levels of VEGF-A and soluble VEGFR-2 showed dose-dependent increases and decreases, respectively. Dynamic contrast-enhanced MRI indicated reduction in tumor perfusion. Clinical activity was observed in renal cell cancer, colorectal cancer, and other tumors.Conclusion: Tivozanib was well tolerated with manageable side effects. The pharmacokinetics profile revealed that tivozanib was suitable for once-daily dosing. Encouraging and durable clinical activity was observed. The recommended daily dose of tivozanib in a 4-week-on and 2-week-off dosing regimen is 1.5 mg. Clin Cancer Res; 17(22); 7156–63. ©2011 AACR.

Published

2023

15. Supplementary Data from Phase I Pharmacokinetic and Pharmacodynamic Study of the First-in-Class Spliceosome Inhibitor E7107 in Patients with Advanced Solid Tumors

Author

Josep Tabernero, José Baselga, Maria Josepa Carreras, Erik A.C. Wiemer, Yoshiharu Mizui, Maja J.A. de Jonge, Adelaida Piera, James P. O'Brien, Herman Burger, Francisco J. Ramos, and Ferry A.L.M. Eskens

Abstract

Supplementary Data - PDF file 104K, Supplementary Data: Eligibility criteria and Pharmacodynamic analysis: methodology sections

Published

2023

16. Figure S1 from Pharmacokinetics, Safety, and Antitumor Effect of Apalutamide with Abiraterone Acetate plus Prednisone in Metastatic Castration-Resistant Prostate Cancer: Phase Ib Study

Author

Fred Saad, Juhui J. Jiao, Charlene Abrams, Caly Chien, Peter Hellemans, Margaret K. Yu, Terence W. Friedlander, Gerhardt Attard, Maja J.A. de Jonge, Ronald de Wit, Kim N. Chi, and Edwin M. Posadas

Abstract

Study design for NCT02123758, a multicenter, open-label phase Ib study in patients with mCRPC to assess potential pharmacokinetic drug-drug interaction, safety, and antitumor activity when APA is given in combination with AA-P.

Published

2023

17. Data from Phase I Pharmacokinetic and Pharmacodynamic Study of the First-in-Class Spliceosome Inhibitor E7107 in Patients with Advanced Solid Tumors

Author

Josep Tabernero, José Baselga, Maria Josepa Carreras, Erik A.C. Wiemer, Yoshiharu Mizui, Maja J.A. de Jonge, Adelaida Piera, James P. O'Brien, Herman Burger, Francisco J. Ramos, and Ferry A.L.M. Eskens

Abstract

Purpose: To assess the safety, tolerability, pharmacokinetics, pharmacodynamics, and clinical activity of E7107 administered as 5-minute bolus infusions on days 1, 8, and 15 in a 28-day schedule.Experimental Design: Patients with solid tumors refractory to standard therapies or with no standard treatment available were enrolled. Dose levels of 0.6 to 4.5 mg/m2 were explored.Results: Forty patients [24M/16F, median age 61 years (45–79)] were enrolled. At 4.5 mg/m2, dose-limiting toxicity (DLT) consisted of grade 3 diarrhea, nausea, and vomiting and grade 4 diarrhea, respectively, in two patients. At 4.0 mg/m2, DLT (grade 3 nausea, vomiting, and abdominal cramps) was observed in one patient. Frequently occurring side effects were mainly gastrointestinal. After drug discontinuation at 4.0 mg/m2, one patient experienced reversible grade 4 blurred vision. The maximum tolerated dose (MTD) is 4.0 mg/m2. No complete or partial responses during treatment were observed; one patient at 4.0 mg/m2 had a confirmed partial response after drug discontinuation. Pharmacokinetic analysis revealed a large volume of distribution, high systemic clearance, and a plasma elimination half-life of 5.3 to 15.1 hours. Overall drug exposure increased in a dose-dependent manner. At the MTD, mRNA levels of selected target genes monitored in peripheral blood mononuclear cells showed a reversible 15- to 25-fold decrease, whereas unspliced pre-mRNA levels of DNAJB1 and EIF4A1 showed a reversible 10- to 25-fold increase.Conclusion: The MTD for E7107 using this schedule is 4.0 mg/m2. Pharmacokinetics is dose-dependent and reproducible within patients. Pharmacodynamic analysis revealed dose-dependent reversible inhibition of pre-mRNA processing of target genes, confirming proof-of-principle activity of E7107. Clin Cancer Res; 19(22); 6296–304. ©2013 AACR.

Published

2023

18. A first-in-man phase 1 study of the DNA-dependent protein kinase inhibitor peposertib (formerly M3814) in patients with advanced solid tumours

Author

Mirjam Kuipers, Ivan Diaz-Padilla, Morten Mau-Sørensen, Barbara Sarholz, Maja J.A. de Jonge, Dorte Nielsen, Ahmad Awada, Henk M.W. Verheul, Karin Berghoff, Jan H.M. Schellens, Lars Damstrup, Samer El Bawab, Patrick Schöffski, and Mark T. J. van Bussel

Subjects

Adult, Male, PK, Cancer Research, medicine.medical_specialty, Nausea, Drug development, DNA-Activated Protein Kinase, Gastroenterology, Article, Tumours of the digestive tract Radboud Institute for Health Sciences [Radboudumc 14], 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Phase I trials, Neoplasms, Internal medicine, Maculopapular rash, Humans, Medicine, DAMAGE RESPONSE, Adverse effect, Protein Kinase Inhibitors, Aged, 030304 developmental biology, 0303 health sciences, Science & Technology, Dose-Response Relationship, Drug, business.industry, Middle Aged, CANCER, Pyridazines, Cancérologie, Oncology, Tolerability, 030220 oncology & carcinogenesis, Pharmacodynamics, Toxicity, Quinazolines, Vomiting, Female, medicine.symptom, business, Life Sciences & Biomedicine

Abstract

Background: This open-label, phase 1 trial (NCT02316197) aimed to determine the maximum-tolerated dose (MTD) and/or recommended phase 2 dose (RP2D) of peposertib (formerly M3814), a DNA-dependent protein kinase (DNA-PK) inhibitor in patients with advanced solid tumours. Secondary/exploratory objectives included safety/tolerability, pharmacokinetic/pharmacodynamic profiles and clinical activity. Methods: Adult patients with advanced solid tumours received peposertib 100–200 mg once daily or 150–400 mg twice daily (BID) in 21-day cycles. Results: Thirty-one patients were included (median age 66 years, 61% male). One dose-limiting toxicity, consisting of mainly gastrointestinal, non-serious adverse events (AEs) and long recovery duration, was reported at 300 mg BID. The most common peposertib-related AEs were nausea, vomiting, fatigue and pyrexia. The most common peposertib-related Grade 3 AEs were maculopapular rash and nausea. Peposertib was quickly absorbed systemically (median Tmax 1.1–2.5 h). The p-DNA-PK/t-DNA-PK ratio decreased consistently in peripheral blood mononuclear cells 3–6 h after doses ≥100 mg. The best overall response was stable disease (12 patients), lasting for ≥12 weeks in seven patients. Conclusions: Peposertib was well-tolerated and demonstrated modest efficacy in unselected tumours. The MTD was not reached; the RP2D was declared as 400 mg BID. Further studies, mainly with peposertib/chemo-radiation, are ongoing. Clinical trial registration: NCT02316197, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2021

19. Pharmacokinetics, Safety, and Antitumor Effect of Apalutamide with Abiraterone Acetate plus Prednisone in Metastatic Castration-Resistant Prostate Cancer: Phase Ib Study

Author

Juhui J. Jiao, Peter Hellemans, Gerhardt Attard, Kim N. Chi, Fred Saad, Caly Chien, Margaret K. Yu, Maja J.A. de Jonge, Terence W. Friedlander, Charlene Connelly Abrams, Edwin M. Posadas, Ronald de Wit, and Medical Oncology

Subjects

Male, Cancer Research, medicine.medical_specialty, Urology, Abiraterone Acetate, Drug Administration Schedule, 03 medical and health sciences, chemistry.chemical_compound, Prostate cancer, 0302 clinical medicine, Pharmacokinetics, SDG 3 - Good Health and Well-being, Prednisone, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Drug Interactions, 030212 general & internal medicine, Adverse effect, Aged, Aged, 80 and over, Cross-Over Studies, business.industry, Apalutamide, Abiraterone acetate, Middle Aged, Prostate-Specific Antigen, medicine.disease, Androgen receptor, Prostatic Neoplasms, Castration-Resistant, Treatment Outcome, Oncology, chemistry, Thiohydantoins, 030220 oncology & carcinogenesis, Prednisolone, Kallikreins, business, medicine.drug

Abstract

Purpose: Apalutamide is a next-generation androgen receptor (AR) inhibitor approved for patients with nonmetastatic castration-resistant prostate cancer (CRPC) and metastatic castration-sensitive prostate cancer. We evaluated the pharmacokinetics, safety, and antitumor activity of apalutamide combined with abiraterone acetate plus prednisone (AA-P) in patients with metastatic CRPC (mCRPC). Patients and Methods: Multicenter, open-label, phase Ib drug–drug interaction study conducted in 57 patients with mCRPC treated with 1,000 mg abiraterone acetate plus 10 mg prednisone daily beginning on cycle 1 day 1 (C1D1) and 240 mg apalutamide daily starting on C1D8 in 28-day cycles. Serial blood samples for pharmacokinetic analysis were collected on C1D7 and C2D8. Results: Systemic exposure to abiraterone, prednisone, and prednisolone decreased 14%, 61%, and 42%, respectively, when apalutamide was coadministered with AA-P. No increase in mineralocorticoid excess–related adverse events was observed. Patients without prior exposure to AR signaling inhibitors had longer median treatment duration and greater mean decrease in prostate-specific antigen (PSA) from baseline compared with those who had received prior therapy. Confirmed PSA reductions of ≥50% from baseline at any time were observed in 80% (12/15) of AR signaling inhibitor–naïve patients and 14% (6/42) of AR signaling inhibitor–treated patients. Conclusions: Treatment with apalutamide plus AA-P was well tolerated and showed evidence of antitumor activity in patients with mCRPC, including those with disease progression on AR signaling inhibitors. No clinically significant pharmacokinetic interaction was observed between abiraterone and apalutamide; however, apalutamide decreased exposure to prednisone. These data support development of 1,000 mg abiraterone acetate plus 10 mg prednisone daily with 240 mg apalutamide daily in patients with mCRPC.

Published

2020

20. Phase I study of intermittent olaparib capsule or tablet dosing in combination with carboplatin and paclitaxel (part 2)

Author

Maja J.A. de Jonge, Jan H.M. Schellens, Diane A.J. van der Biessen, Andre T. Brunetto, Agnes Jager, Johann S. de Bono, Joo Ern Ang, Martijn P. Lolkema, Jacques De Greve, Hendrik-Tobias Arkenau, Ruud van der Noll, Ilian Tchakov, Jos H. Beijnen, Marja Mergui-Roelvink, Serena Marchetti, Afd Pharmacoepi & Clinical Pharmacology, Pharmacoepidemiology and Clinical Pharmacology, Clinical sciences, Medical Genetics, Medical Oncology, and Laboratory for Medical and Molecular Oncology

Subjects

0301 basic medicine, Oncology, Adult, Male, medicine.medical_specialty, Neutropenia, Paclitaxel, Antineoplastic Agents, Capsules, Piperazines, Olaparib, Carboplatin, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Phase I, SDG 3 - Good Health and Well-being, Internal medicine, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Medicine, Humans, Pharmacology (medical), Pharmacokinetics, Dosing, Fatigue, Aged, Pharmacology, business.industry, Area under the curve, Alopecia, Middle Aged, medicine.disease, Thrombocytopenia, 030104 developmental biology, PARP inhibitor, Tolerability, chemistry, 030220 oncology & carcinogenesis, Phthalazines, Female, business, Ovarian cancer, Tablets

Abstract

Background In the first part of this extensive phase I study (NCT00516724), continuous olaparib twice daily (bid) with carboplatin and/or paclitaxel resulted in myelosuppression and dose modifications. Here, we report the safety, tolerability, and efficacy of intermittent olaparib dosing combined with carboplatin and paclitaxel. Methods Patients with advanced solid tumors (part D) and enriched for ovarian and breast cancer (part E) received olaparib (capsule and tablet formulations) using intermittent schedules (2 to 10 days of a 21-day cycle) combined with carboplatin/paclitaxel. Safety assessments included evaluation of dose-limiting toxicities (DLTs; cycle 1 only), adverse events (AEs), and physical examinations. Pharmacokinetic assessments of olaparib capsule and tablet combined with carboplatin/paclitaxel were performed. Tumor responses (RECIST) were assessed every 2 cycles. Results In total, 132 heavily pre-treated patients were included. One DLT of grade 3 elevated alanine aminotransferase lasting for 8 days was reported (olaparib tablet 100 mg bid days 3–12, carboplatin area under the curve 4 and paclitaxel 175 mg/m2). The most common hematological AEs were neutropenia (47%) and thrombocytopenia (39%), which frequently led to dose modifications. Non-hematological AEs were predominantly grade 1–2, including alopecia (89%) and fatigue (84%). Overall objective response rate was 46%. Conclusions Discontinuous dosing of olaparib resulted in significant myelosuppression leading to dose interruptions and/or delays. Anti-tumor activity was encouraging in patients enriched with BRCA-mutated breast and ovarian cancer. The most appropriate olaparib tablet dose for use in further studies evaluating olaparib in combination with carboplatin and paclitaxel is 50 mg bid (days 1–5).

Published

2019

21. Identifying patient values impacting the decision whether to participate in early phase clinical cancer trials: A systematic review

Author

Liza G. G. van Lent, Carin C.D. van der Rijt, Maja J.A. de Jonge, Martijn P. Lolkema, Lea J. Jabbarian, Julia C.M. van Weert, Jeroen Hasselaar, Jelle van Gurp, Persuasive Communication (ASCoR, FMG), Medical Oncology, and Psychiatry

Subjects

0301 basic medicine, Health Knowledge, Attitudes, Practice, medicine.medical_specialty, Decision Making, Psychological intervention, Decisional conflict, Choice Behavior, Healthcare improvement science Radboud Institute for Health Sciences [Radboudumc 18], 03 medical and health sciences, 0302 clinical medicine, Quality of life (healthcare), SDG 3 - Good Health and Well-being, Informed consent, Neoplasms, medicine, Humans, Radiology, Nuclear Medicine and imaging, Clinical Trials as Topic, business.industry, General Medicine, Clinical trial, Identified patient, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Family medicine, Value of life, Patient Participation, business, Qualitative research

Abstract

Contains fulltext : 235017.pdf (Publisher’s version ) (Open Access) BACKGROUND: For many patients with advanced cancer, the decision whether to participate in early phase clinical trials or not is complex. The decision-making process requires an in-depth discussion of patient values. We therefore aimed to synthesize and describe patient values that may affect early phase clinical trial participation. METHODS: We conducted a systematic search in seven electronic databases on patient values in relation to patients' decisions to participate in early phase clinical cancer trials. RESULTS: From 3072 retrieved articles, eleven quantitative and five qualitative studies fulfilled our inclusion criteria. We extracted ten patient values that can contribute to patients' decisions. Overall, patients who seek trial participation usually report hope, trust, quantity of life, altruism, perseverance, faith and/or risk tolerance as important values. Quality of life and humanity are main values of patients who refuse trial participation. Autonomy and social adherence can be reported by both trial seekers or refusers, dependent upon how they are manifested in a patient. CONCLUSIONS: We identified patient values that frequently play a role in the decision-making process. In the setting of discussing early phase clinical trial participation with patients, healthcare professionals need to be aware of these values. This analysis supports the importance of individual exploration of values. Patients that become aware of their values, e.g. by means of interventions focused on clarifying their values, could feel more empowered to choose. Subsequently, healthcare professionals could improve their support in a patients' decision-making process and reduce the chance of decisional conflict.

Published

2021

22. Understanding how coping strategies and quality of life maintain hope in patients deliberating phase I trial participation

Author

Maja J.A. de Jonge, Peer van der Helm, Ron H.J. Mathijssen, Dennis Klein, Simone van der Burg, Diane A.J. van der Biessen, Martijn P. Lolkema, and Medical Oncology

Subjects

Adult, Male, Coping (psychology), Experimental and Cognitive Psychology, Structural equation modeling, Healthcare improvement science Radboud Institute for Health Sciences [Radboudumc 18], 03 medical and health sciences, Hope, 0302 clinical medicine, All institutes and research themes of the Radboud University Medical Center, Quality of life, Informed consent, Neoplasms, Surveys and Questionnaires, Adaptation, Psychological, Cognitive dissonance, Humans, 030212 general & internal medicine, Patient participation, Internal-External Control, Aged, Motivation, Clinical Trials, Phase I as Topic, Social environment, Middle Aged, Psychiatry and Mental health, Locus of control, Cross-Sectional Studies, Oncology, 030220 oncology & carcinogenesis, Quality of Life, Female, Patient Participation, Psychology, Comprehension, Clinical psychology

Abstract

Objective This study aimed to understand how hope and motivation of patients considering phase I trial participation are affected by psychological factors such as coping strategies and locus of control (LoC) and general well-being as measured by the quality of life (QoL). Methods An exploratory cross-sectional study was performed in patients with incurable cancer (N = 135) referred to our phase I unit for the first time. Patients were potentially eligible for phase I trial participation and participated in our study while deliberating phase I trial participation. We used questionnaires on hope, motivation to participate, coping, LoC, and QoL. To investigate the nature and magnitude of the relationships between the scales, a structural equation modeling (SEM) was fitted to the data. Results Hope significantly predicted the motivation to participate in phase I trials. Predictors of hope were a combination of flexible and tenacious goal pursuit (both P

Published

2018

23. A phase I study of SAR405838, a novel human double minute 2 (HDM2) antagonist, in patients with solid tumours

Author

Mark A. Dickson, Wei Zheng, Koruth Thomas, Vincent A. de Weger, Axel Le Cesne, Jan H.M. Schellens, Sandrine Macé, Karl Hsu, Maja J.A. de Jonge, Gilles Tuffal, Andrew J. Wagner, Marlies H.G. Langenberg, and Medical Oncology

Subjects

Male, 0301 basic medicine, Oncology, Cancer Research, Indoles, Lung Neoplasms, Skin Neoplasms, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Neoplasms, Melanoma, Fatigue, Gastrointestinal Neoplasms, Aged, 80 and over, Nausea, Proto-Oncogene Proteins c-mdm2, Liposarcoma, Middle Aged, Anorexia, 030220 oncology & carcinogenesis, Toxicity, Cohort, Female, medicine.symptom, Adult, medicine.medical_specialty, Maximum Tolerated Dose, Vomiting, Antineoplastic Agents, Young Adult, 03 medical and health sciences, Pharmacokinetics, Internal medicine, medicine, Humans, Spiro Compounds, In patient, neoplasms, Aged, Dose-Response Relationship, Drug, business.industry, Antagonist, medicine.disease, Thrombocytopenia, Surgery, 030104 developmental biology, Pharmacodynamics, business

Abstract

Purpose In tumours with wild-type TP53, the tumour-suppressive function of p53 is frequently inhibited by HDM2. This phase I, dose-escalating study investigated the maximum tolerated dose (MTD), safety, pharmacokinetics and pharmacodynamics of SAR405838, an HDM2 inhibitor, in patients with advanced solid tumours ( NCT01636479 ). Methods In dose escalation, patients with any locally advanced/metastatic solid tumour with TP53 mutation prevalence below 40%, or documented as TP53 wild-type, were eligible. In the MTD expansion cohort, only patients with de-differentiated liposarcoma were included. Primary end-points were MTD and efficacy in the MTD expansion cohort. Secondary end-points included safety, pharmacokinetics and pharmacodynamics biomarkers. Results Seventy-four patients were treated with SAR405838 (50–800 mg once daily [QD], 800–1800 mg weekly and 1800 mg twice weekly). Two patients treated with SAR405838 400 mg QD had thrombocytopaenia as a dose-limiting toxicity (DLT). The MTD for the QD schedule of SAR405838 was 300 mg QD. No DLTs were observed with the weekly schedule; one patient had a DLT of nausea with the 1800 mg twice-weekly dose. Treatment with SAR405838 was associated with increased plasma MIC-1, reflecting p53 pathway activation. In the de-differentiated liposarcoma MTD cohort, 89% of the patients had HDM2 amplification at baseline and no TP53 mutations were observed; best response was stable disease in 56% and progression-free rate at 3 months was 32%. Conclusion SAR405838 had an acceptable safety profile with limited activity in patients with advanced solid tumours. The MTD of SAR405838 was 300 mg QD; MTD was not reached with the weekly schedule.

Published

2017

24. Implementation of a Multicenter Biobanking Collaboration for Next-Generation Sequencing-Based Biomarker Discovery Based on Fresh Frozen Pretreatment Tumor Tissue Biopsies

Author

Fleur Weeber, Christa G Gadellaa-van Hooijdonk, Stefan Sleijfer, Marco J. Koudijs, Edwin Cuppen, Neeltje Steeghs, Paul J. van Diest, Michel M. van den Heuvel, Ron H.J. Mathijssen, Wouter B. Veldhuis, Annette H. Bruggink, Isaac J. Numan, Maja J.A. de Jonge, Jan H.M. Schellens, Sander Bins, Emile E. Voest, Geert A. Cirkel, Erik van Werkhoven, Rob J. de Knegt, Stefan M. Willems, Marlies H.G. Langenberg, Martijn P. Lolkema, Medical Oncology, and Gastroenterology & Hepatology

Subjects

0301 basic medicine, Adult, Image-Guided Biopsy, Male, Cancer Research, medicine.medical_specialty, Percutaneous, Cancer Diagnostics and Molecular Pathology, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], DNA sequencing, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Biopsy, medicine, Biomarkers, Tumor, Humans, Biomarker discovery, Aged, Biological Specimen Banks, Netherlands, medicine.diagnostic_test, business.industry, Cancer, High-Throughput Nucleotide Sequencing, Middle Aged, medicine.disease, Biobank, Surgery, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Fresh frozen, Macrodissection, Female, Radiology, business, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

Background The discovery of novel biomarkers that predict treatment response in advanced cancer patients requires acquisition of high-quality tumor samples. As cancer evolves over time, tissue is ideally obtained before the start of each treatment. Preferably, samples are freshly frozen to allow analysis by next-generation DNA/RNA sequencing (NGS) but also for making other emerging systematic techniques such as proteomics and metabolomics possible. Here, we describe the first 469 image-guided biopsies collected in a large collaboration in The Netherlands (Center for Personalized Cancer Treatment) and show the utility of these specimens for NGS analysis. Patients and Methods Image-guided tumor biopsies were performed in advanced cancer patients. Samples were fresh frozen, vital tumor cellularity was estimated, and DNA was isolated after macrodissection of tumor-rich areas. Safety of the image-guided biopsy procedures was assessed by reporting of serious adverse events within 14 days after the biopsy procedure. Results Biopsy procedures were generally well tolerated. Major complications occurred in 2.1%, most frequently consisting of pain. In 7.3% of the percutaneous lung biopsies, pneumothorax requiring drainage occurred. The majority of samples (81%) contained a vital tumor percentage of at least 30%, from which at least 500 ng DNA could be isolated in 91%. Given our preset criteria, 74% of samples were of sufficient quality for biomarker discovery. The NGS results in this cohort were in line with those in other groups. Conclusion Image-guided biopsy procedures for biomarker discovery to enable personalized cancer treatment are safe and feasible and yield a highly valuable biobank.

Published

2017

25. CMET-22. CAPMATINIB (INC280) IN METΔEX14-MUTATED ADVANCED NON-SMALL CELL LUNG CANCER (NSCLC): EFFICACY DATA FROM THE PHASE 2 GEOMETRY MONO-1 STUDY

Author

Egbert F. Smit, Rebecca S. Heist, M. Waldron-Lynch, Monica Giovannini, Edward B. Garon, Ji-Youn Han, Daniel Shao-Weng Tan, Harry J.M. Groen, Toyoaki Hida, Sylvie Le Mouhaer, Noemi Reguart, Johan Vansteenkiste, Pierre-Jean Souquet, Juergen Wolf, Maja J.A. de Jonge, Takashi Seto, Anna Robeva, and Sergey Orlov

Subjects

Cancer Research, CNS Metastasis, Capmatinib, business.industry, non-small cell lung cancer (NSCLC), medicine.disease, Therapy naive, Oncology, Response Evaluation Criteria in Solid Tumors, medicine, Radiology Specialty, Cancer research, Brain lesions, Neurology (clinical), Progression-free survival, business

Abstract

BACKGROUND Capmatinib is a highly potent, selective MET-inhibitor known to cross the BBB, and intracranial activity with capmatinib has been previously reported. Updated results for overall response rate (ORR), duration of response (DOR), progression-free survival (PFS), and brain metastases (BM) activity from the GEOMETRY mono-1 study are presented here. METHODS GEOMETRY mono-1 is a phase 2, multi-cohort, multicenter study evaluating capmatinib in METΔex14-mutated or MET-amplified NSCLC patients. Patients (≥18 years) with ECOG PS 0–1, ALK-/EGFR-wt, and stage IIIB/IV NSCLC were eligible. Patients with asymptomatic BM were allowed. METΔex14-mutated patients were assigned to Cohorts 4 (1–2 prior lines of treatment) and 5b (treatment-naive) and received capmatinib 400mg BID. Endpoints by BIRC: ORR (primary, RECIST v1.1), DOR, and PFS. Ad hoc BIRC neuro-radiologic assessments of all Cohort 4 and 5b patients with baseline BM were performed. RESULTS As of April 15, 2019, 97 patients (Cohort 4: 69 patients; Cohort 5b: 28 patients) were evaluable for efficacy. BIRC assessments: ORR (95%CI): 40.6% (28.9–53.1) in Cohort 4; 67.9% (47.6–84.1) in Cohort 5b. Median DOR (95%CI): 9.7 (5.55–12.98) and 11.1 (5.55-NE) months and median PFS (95%CI): 5.4 (4.17–6.97) and 9.7 (5.52–13.86) months for Cohorts 4 and 5b, respectively. Of 13 evaluable patients with BM at baseline, 7 (54%) had intracranial response by BIRC, including 4 patients with complete resolution of brain lesions, and 12/13 had intracranial disease control. Responses in the brain were as fast as systemic responses. Most common treatment-related AEs (≥15%, all grades) across all cohorts (N=334): peripheral edema (41.6%), nausea (33.2%), increased blood creatinine (19.5%), and vomiting (18.9%); most AEs were grade 1/2. CONCLUSION These data confirm capmatinib to be a promising new treatment option for patients with METΔex14-mutated advanced NSCLC regardless of line of therapy, with deep and durable responses including in patients with brain metastases, and a manageable toxicity profile.

Published

2019

26. Phase I Study of BI 853520, an Inhibitor of Focal Adhesion Kinase, in Patients with Advanced or Metastatic Nonhematologic Malignancies

Author

Lillian L. Siu, David Schnell, Remy B. Verheijen, Albiruni Ryan Abdul Razak, Martijn P. Lolkema, Linda C Pronk, Diane A.J. van der Biessen, Filip de Vos, Monique Jansen, Hal W. Hirte, Maja J.A. de Jonge, Sebastien J. Hotte, and Neeltje Steeghs

Subjects

0301 basic medicine, Male, Cancer Research, Peripheral edema, Gastroenterology, 0302 clinical medicine, Neoplasms, 80 and over, Tissue Distribution, Pharmacology (medical), Original Research Article, Neoplasm Metastasis, Non-U.S. Gov't, Aged, 80 and over, Proteinuria, Research Support, Non-U.S. Gov't, Protein Kinase Inhibitors/pharmacokinetics, Middle Aged, Prognosis, Clinical Trial, 3. Good health, Oncology, 030220 oncology & carcinogenesis, Vomiting, Female, medicine.symptom, Focal Adhesion Kinase 1/antagonists & inhibitors, Adult, medicine.medical_specialty, Maximum Tolerated Dose, Nausea, Research Support, Clinical Trial, Phase I, 03 medical and health sciences, Young Adult, Phase I, Pharmacokinetics, Internal medicine, medicine, Journal Article, Humans, Adverse effect, Protein Kinase Inhibitors, Aged, business.industry, medicine.disease, Neoplasms/drug therapy, 030104 developmental biology, Focal Adhesion Kinase 1, Pharmacodynamics, business, Progressive disease, Follow-Up Studies

Abstract

Background Overexpression/activation of focal adhesion kinase (FAK) in human malignancies has led to its evaluation as a therapeutic target. We report the first-in-human phase I study of BI 853520, a novel, potent, highly selective FAK inhibitor. Objective Our objectives were to identify the maximum tolerated dose (MTD), and to evaluate safety, pharmacokinetics (PK), pharmacodynamics (PD), biomarker expression, and preliminary activity. Patients and Methods The study comprised a standard 3 + 3 dose-escalation phase followed by an expansion phase in patients with selected advanced, nonhematologic malignancies. Results Thirty-three patients received BI 853520 in the dose-escalation phase; the MTD was 200 mg once daily (QD). Dose-limiting toxicities included proteinuria and fatigue, both of which were grade 3. Preliminary PK data supported QD dosing. In the expansion cohort, 63 patients received BI 853520 200 mg QD. Drug-related adverse events (AEs) in > 10% of patients included proteinuria (57%), nausea (57%), fatigue (51%), diarrhea (48%), vomiting (40%), decreased appetite (19%), and peripheral edema (16%). Most AEs were grade 1–2; grade 3 proteinuria, reported in 13 patients (21%), was generally reversible upon treatment interruption. Nineteen patients underwent dose reduction due to AEs, and three drug-related serious AEs were reported, none of which were fatal. Preliminary PD analysis indicated target engagement. Of 63 patients, 49 were evaluable; 17 (27%) achieved a best response of stable disease (4 with 150 + days), and 32 (51%) patients had progressive disease. Conclusions BI 853520 has a manageable and acceptable safety profile, favorable PK, and modest antitumor activity at an MTD of 200 mg QD in patients with selected advanced nonhematologic malignancies. ClinicalTrials.gov identifier NCT01335269. Electronic supplementary material The online version of this article (10.1007/s11523-018-00617-1) contains supplementary material, which is available to authorized users.

Published

2019

27. 53BP1 as a potential predictor of response in PARP inhibitor-treated homologous recombination-deficient ovarian cancer

Author

Peter Ansell, Andrea E. Wahner Hendrickson, Rutger H. T. Koornstra, Scott H. Kaufmann, Matthew W. Dudley, Jourik A. Gietema, Krista M. Goergen, X. Wei Meng, Matthew J. Maurer, Karen S. Flatten, Carla D. Van Herpen, Martha W. den Hollander, Ann L. Oberg, Rachel M. Hurley, Agnes Jager, Maja J.A. de Jonge, Maria I. Harrell, Jill M. Wagner, Elizabeth M. Swisher, Stacie Peacock Shepherd, Daniel W. Visscher, Vivian Negron, Damage and Repair in Cancer Development and Cancer Treatment (DARE), Guided Treatment in Optimal Selected Cancer Patients (GUTS), and Medical Oncology

Subjects

0301 basic medicine, DNA Repair, Genes, BRCA2, Genes, BRCA1, Poly (ADP-Ribose) Polymerase-1, RAD51, MULTICENTER, Cancer development and immune defence Radboud Institute for Health Sciences [Radboudumc 2], 0302 clinical medicine, PARP1, Medicine, Homologous Recombination, PARP inhibitors, Ovarian Neoplasms, Sulfonamides, Obstetrics and Gynecology, HR-deficiency, OPEN-LABEL, 53BP1, POLYMERASE INHIBITORS, Oncology, NIRAPARIB, 030220 oncology & carcinogenesis, Benzamides, PARP inhibitor, Female, Tumor Suppressor p53-Binding Protein 1, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], CARCINOMA, DNA repair, Poly(ADP-ribose) Polymerase Inhibitors, Article, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Ovarian cancer, Cell Line, Tumor, Carcinoma, Humans, Clonogenic assay, REPAIR, business.industry, MUTATIONS, DNA Repair Pathway, medicine.disease, PROFICIENT, 030104 developmental biology, Drug Resistance, Neoplasm, CELLS, Cancer research, DNA damage, business, RESISTANCE

Abstract

Contains fulltext : 202591.pdf (Publisher’s version ) (Closed access) OBJECTIVE: Poly(ADP-ribose) polymerase (PARP) inhibitors have shown substantial activity in homologous recombination- (HR-) deficient ovarian cancer and are undergoing testing in other HR-deficient tumors. For reasons that are incompletely understood, not all patients with HR-deficient cancers respond to these agents. Preclinical studies have demonstrated that changes in alternative DNA repair pathways affect PARP inhibitor (PARPi) sensitivity in ovarian cancer models. This has not previously been assessed in the clinical setting. METHODS: Clonogenic and plasmid-based HR repair assays were performed to compare BRCA1-mutant COV362 ovarian cancer cells with or without 53BP1 gene deletion. Archival biopsies from ovarian cancer patients in the phase I, open-label clinical trial of PARPi ABT-767 were stained for PARP1, RAD51, 53BP1 and multiple components of the nonhomologous end-joining (NHEJ) DNA repair pathway. Modified histochemistry- (H-) scores were determined for each repair protein in each sample. HRD score was determined from tumor DNA. RESULTS: 53BP1 deletion increased HR in BRCA1-mutant COV362 cells and decreased PARPi sensitivity in vitro. In 36 women with relapsed ovarian cancer, responses to the PARPi ABT-767 were observed exclusively in cancers with HR deficiency. In this subset, 7 of 18 patients (39%) had objective responses. The actual HRD score did not further correlate with change from baseline tumor volume (r=0.050; p=0.87). However, in the HR-deficient subset, decreased 53BP1 H-score was associated with decreased antitumor efficacy of ABT-767 (r=-0.69, p=0.004). CONCLUSION: Differences in complementary repair pathways, particularly 53BP1, correlate with PARPi response of HR-deficient ovarian cancers.

Published

2019

28. Realizing better doctor-patient dialogue about choices in palliative care and early phase clinical trial participation: towards an online value clarification tool (OnVaCT)

Author

Maja J.A. de Jonge, Esther Oomen-de Hoop, Saskia M. Pulleman, Liza G. G. van Lent, Jelle van Gurp, Nicole Stoel, Martijn P. Lolkema, Eelke H. Gort, Julia C.M. van Weert, Carin C.D. van der Rijt, Jeroen Hasselaar, Medical Oncology, and Persuasive Communication (ASCoR, FMG)

Subjects

Early phase clinical trial, Palliative care, Referral, lcsh:Special situations and conditions, Patient-centred care, Decisional conflict, Choice Behavior, Healthcare improvement science Radboud Institute for Health Sciences [Radboudumc 18], Interviews as Topic, 03 medical and health sciences, Study Protocol, All institutes and research themes of the Radboud University Medical Center, 0302 clinical medicine, Nursing, eHealth, Humans, 030212 general & internal medicine, Decision-making, Think aloud protocol, Shared decision making, Qualitative Research, Netherlands, Ethics, Clinical Trials as Topic, Physician-Patient Relations, lcsh:RC952-1245, Patient Selection, Value clarification tool, Palliative Care, General Medicine, Focus Groups, Focus group, Patient-physician communication, 3. Good health, Clinical trial, 030220 oncology & carcinogenesis, Psychology

Abstract

Background Patients with advanced cancer for whom standard systemic treatment is no longer available may be offered participation in early phase clinical trials. In the decision making process, both medical-technical information and patient values and preferences are important. Since patients report decisional conflict after deciding on participation in these trials, improving the decision making process is essential. We aim to develop and evaluate an Online Value Clarification Tool (OnVaCT) to assist patients in clarifying their values around this end-of-life decision. This improved sharing of values is hypothesized to support medical oncologists in tailoring their information to individual patients’ needs and, consequently, to support patients in taking decisions in line with their values and reduce decisional conflict. Methods In the first part, patients’ values and preferences and medical oncologists’ views hereupon will be explored in interviews and focus groups to build a first prototype OnVaCT using digital communication (serious gaming). Next, we will test feasibility during think aloud sessions, to deliver a ready-to-implement OnVaCT. In the second part, the OnVaCT, with accompanied training module, will be evaluated in a pre-test (12–18 months before implementation) post-test (12–18 months after implementation) study in three major Dutch cancer centres. We will include 276 patients (> 18 years) with advanced cancer for whom standard systemic therapy is no longer available, and who are referred for participation in early phase clinical trials. The first consultation will be recorded to analyse patient-physician communication regarding the discussion of patients’ values and the decision making process. Three weeks afterwards, decisional conflict will be measured. Discussion This project aims to support the discussion of patient values when considering participation in early phase clinical trials. By including patients before their first appointment with the medical oncologist and recording that consultation, we are able to link decisional conflict to the decision making process, e.g. the communication during consultation. The study faces challenges such as timely including patients within the short period between referral and first consultation. Furthermore, with new treatments being developed rapidly, molecular stratification may affect the patient populations included in the pre-test and post-test periods. Trial registration Netherlands Trial Registry number: NTR7551 (prospective; July 17, 2018).

Published

2019

29. A phase I pharmacokinetic and safety study of cabazitaxel in adult cancer patients with normal and impaired renal function

Author

Sylvie Rottey, Silvia Damian, Jordi Rodon, Ron H. J. Mathijssen, Richard D. Baird, Claudine Wack, Javier Garcia-Corbacho, Analia Azaro, Maja J.A. de Jonge, Pierre-François Clot, Jean-Pascal Machiels, Liji Shen, UCL - SSS/IREC/MIRO - Pôle d'imagerie moléculaire, radiothérapie et oncologie, UCL - (SLuc) Unité d'oncologie médicale, Medical Oncology, Baird, Richard [0000-0001-7071-6483], and Apollo - University of Cambridge Repository

Subjects

Male, tumors, 0301 basic medicine, Cancer Research, Pharmacology, urologic and male genital diseases, Toxicology, Impaired renal function, 0302 clinical medicine, INSUFFICIENCY, Neoplasms, Medicine and Health Sciences, Pharmacology (medical), Renal Insufficiency, DRUG, Renal impairment, EVERY 3 WEEKS, Advanced solid, media_common, Cabazitaxel, Middle Aged, OPEN-LABEL, PREVALENCE, Oncology, 030220 oncology & carcinogenesis, Female, Taxoids, Original Article, advanced solid tumors, pharmacokinetics, medicine.drug, Adult, renal impairment, Drug, medicine.medical_specialty, media_common.quotation_subject, Urology, Antineoplastic Agents, CISPLATIN, 03 medical and health sciences, Phase I, SDG 3 - Good Health and Well-being, Pharmacokinetics, MANAGEMENT, medicine, Humans, In patient, Aged, Cisplatin, DYSFUNCTION WORKING GROUP, Taxane, business.industry, cabazitaxel, Cancer, phase I, medicine.disease, 030104 developmental biology, Advanced solid tumors, business, TAXANE

Abstract

$\textbf{PURPOSE}$ Limited data are available on cabazitaxel pharmacokinetics in patients with renal impairment. This open-label, multicenter study assessed cabazitaxel in patients with advanced solid tumors and normal or impaired renal function. $\textbf{METHODS}$ Cohorts A (normal renal function: creatinine clearance [CrCL] >80 mL/min/1.73 m$^{2}$), B (moderate renal impairment: CrCL 30 to

Published

2016

30. Abstract CT034: Phase I study of WNT974 + spartalizumab in patients (pts) with advanced solid tumors

Author

Rebecca Kan, Filip Janku, Aitano Calvo, Ana Arance, Maja J.A. de Jonge, Maria P. De Miguel, Jiachang Gong, Marios Giannakis, Antoni Ribas, Filip De Vos, Maritza Melendez, Patrick M. Forde, Misako Nagasaka, Guillem Argiles, Sebastian Szpakowski, and Susan Moody

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, business.industry, Melanoma, medicine.medical_treatment, Cancer, Immunotherapy, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Refractory, Pharmacokinetics, 030220 oncology & carcinogenesis, Internal medicine, Pharmacodynamics, medicine, Maculopapular rash, medicine.symptom, business, Progressive disease

Abstract

Background: WNT974, a Porcupine inhibitor, has shown evidence of Wnt pathway inhibition in clinical trials. Dysregulated Wnt signaling has been linked to immunotherapy resistance, suggesting WNT974 may act synergistically with checkpoint inhibitors. Spartalizumab is an αPD-1 mAb with demonstrated clinical activity in solid tumors. Methods: In this Phase I, open-label trial (NCT01351103) adult pts received WNT974 ± spartalizumab; here we report on the dose escalation of the combination. Eligible pts had melanoma (including uveal), lung SCC, HNSCC, esophageal SCC, cervical SCC, or TNBC. Pts with melanoma, lung SCC, or HNSCC must have had a best response of progressive disease (primary refractory) to prior αPD-1 therapy; other pts were naïve or primary refractory to prior αPD-1. WNT974 was dosed orally QD in 28-day cycles (2.5-10 mg, Days 1-8 or 1-15 of Cycles 1 or 1-4); spartalizumab was dosed IV at 400 mg Q4W. Objectives were to determine the maximum tolerated dose (MTD)/recommended dose for expansion (RDE), safety, pharmacokinetics (PK), pharmacodynamics, and activity of WNT974 + spartalizumab. Pre- and on-treatment pt samples were collected: skin samples for RT-PCR analysis of AXIN2, a marker of Wnt pathway activity; tumor samples for RNAseq of AXIN2 and immune cell markers. Results: As of Sept 2, 2019, 27 pts were enrolled: 24 discontinued (18 due to disease progression; 67%), 3 were ongoing. Most common tumor types were non-uveal melanoma (n=8), TNBC (n=7), and uveal melanoma (n=5); 63% had received prior αPD-1. PK parameters for WNT974 + spartalizumab were consistent with prior single agent data. Dose-limiting toxicities were reported in 2 pts: Grade (G) 2 spinal compression fracture that occurred in the setting of trauma and G3 arthralgia. 78% of pts experienced a treatment-related AE, the most common being hypothyroidism (19%); 4 pts (15%) had 7 suspected-related G3/4 AEs (arthralgia, atrial fibrillation, diabetes mellitus, diabetic ketoacidosis, hyperglycemia, hyponatremia, and maculopapular rash). One pt (4%) with TNBC had a partial response, 11 pts (41%) had stable disease (SD), 13 pts (48%) had progressive disease; response was unknown in 2 pts. SD was reported in 9/17 pts (53%) who were primary refractory to prior αPD-1; 4 remained on study >24 wks. All pts with uveal melanoma (n=5) had SD. Evidence of Porcupine inhibition, assessed by skin AXIN2 suppression, was detected at all dose levels studied. Pts with the largest reductions in tumor size had on-treatment increases in immune marker mRNA in tumor samples, including a pt with αPD-1 primary refractory melanoma with high baseline AXIN2 expression and 42% reduction in the sum of target lesion diameters; this pt remained on study at 48 wks at the cutoff date. Conclusions: WNT974 + spartalizumab was well tolerated; MTD/RDE have not been determined. Preliminary data suggest blocking Wnt signaling may enable response to checkpoint inhibition in some pts. Citation Format: Filip Janku, Filip de Vos, Maria de Miguel, Patrick Forde, Antoni Ribas, Misako Nagasaka, Guillem Argiles, Ana Maria Arance, Aitano Calvo, Marios Giannakis, Maritza Melendez, Jiachang Gong, Sebastian Szpakowski, Rebecca Kan, Susan E. Moody, Maja De Jonge. Phase I study of WNT974 + spartalizumab in patients (pts) with advanced solid tumors [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr CT034.

Published

2020

31. Pharmacodynamic effects in blood and tumor tissue of eftozanermin alfa, a tumor necrosis factor-related apoptosis-inducing ligand receptor agonist

Author

Joann P. Palma, Emiliano Calvo, Sudhir Penugonda, Dimple A. Modi, Alexis Cunningham, Monica Motwani, Maja J.A. de Jonge, Patricia LoRusso, and Chun Zhang

Subjects

Agonist, Cancer Research, business.industry, medicine.drug_class, Ligand (biochemistry), Tumor tissue, Oncology, Apoptosis, Pharmacodynamics, Cancer research, Medicine, Tumor necrosis factor alpha, business, Receptor

Abstract

e15668 Background: Eftozanermin alfa (eftoza; formerly known as ABBV-621), a 2nd-generation tumor necrosis factor-related apoptosis-inducing ligand receptor agonist, is being evaluated in previously treated solid and hematologic malignancies (NCT03082209). In a dose-expansion cohort, patients (pts) with KRAS-mutant colorectal cancer (n = 24) and pancreatic cancer (n = 24) were evaluated at 3 dose levels with 12 mandatory paired biopsies per tumor type (pretreatment [Tx] and on-Tx collection). Following eftoza dosing, RNA and protein expression including posttranslational modifications were assessed in tumor biopsies to understand the target engagement and downstream pathway activation. Plasma was evaluated for changes in somatic mutant allele frequency and M30, M65 (circulating apoptotic markers). Methods: Biopsies were collected anytime during the screening period (pre-Tx) and 24±4 h following 2nd or 3rd infusion (on-Tx). Of the requested 4–6 fresh biopsy cores, 1–2 cores were collected as formalin fixed paraffin embedded (FFPE) and the rest were frozen tissue. FFPE tissue was analyzed by multiplex immunohistochemistry (IHC) and RNAseq; reverse phase protein array was used for frozen cores. Plasma was collected at cycle 1 predose and 2, 8, 24, 48, and 168 h postdose and analyzed for M30, M65 (by ELISA) and circulating tumor DNA (64-gene PlasmaSELECT assay). Results: Twenty-five pts consented to biopsies; paired biopsies were obtained from 16 pts at a 64% success rate: FFPE (n = 15) and frozen cores (n = 12). Tumor cells were detected in 11/15 (73%) FFPE and 4/12 (33%) frozen cores. Increase in M30, activated caspases, and cleaved PARP levels was observed in on-Tx biopsy samples compared with pre-Tx, thus serving as evidence for apoptosis induction in tumors following eftoza dosing. Changes in the tumor microenvironment were observed post-Tx by RNAseq and multiplex IHC (eg, CD68 level). Downregulation of prosurvival signaling pathways (eg, AKT/MEK) was also observed following eftoza dosing. Thirteen out of 16 pts showed transient increase in mutant allele fractions post eftoza Tx that correlated with increased plasma circulating tumor markers M30 and M65 at similar time points, suggesting activation of apoptosis pathway. Increase in M30, M65 levels also preceded increase in liver enzymes (ALT/AST) at 2, 48 hr post-Tx. Conclusions: Pharmacodynamic effect of eftoza was successfully demonstrated in blood and tumor tissue, including induction of apoptosis and modulation of PI3K and MEK signaling pathways. Clinical trial information: NCT03082209.

Published

2020

32. Immune activation in first-in-human anti-macrophage antibody (anti-Clever-1 mAb; FP-1305) phase I/II MATINS trial: Part I dose-escalation, safety, and efficacy results

Author

Felix Vaura, Debbie Robbrecht, J. Mandelin, Panu Jaakkola, Matti K Karvonen, Yuk Ting Ma, Tanja Skyttä, Maija Hollmén, Maja J.A. de Jonge, Reetta Virtakoivu, Anna Minchom, Shishir Shetty, Romillie Cruz, Annika Pasanen, Petri Bono, Jussi Koivunen, Christina Yap, Alain Thibault, Markku Jalkanen, and Sirpa Jalkanen

Subjects

Cancer Research, business.industry, medicine.drug_class, First in human, Monoclonal antibody, 3. Good health, Macrophage antibody, 03 medical and health sciences, 0302 clinical medicine, Phase i ii, Oncology, 030220 oncology & carcinogenesis, Cancer research, Dose escalation, Medicine, Scavenger receptor, business, 030215 immunology, Immune activation

Abstract

3097 Background: The scavenger receptor CLEVER-1 mediates the clearance of “unwanted” self-components and is highly expressed on tumor associated macrophages (TAMs). CLEVER-1 expression is associated with immunotherapy resistance and poor survival in several cancers. Pre-clinical studies demonstrate that CLEVER-1 inhibition increases TAM pro-inflammatory cytokine secretion and antigen presentation reactivating CD8 T cell responses with robust anti-tumor activity. Targeting CLEVER-1 could therefore overcome the immunosuppressive tumor microenvironment and has led to the development of FP-1305, a humanized anti-CLEVER-1 IgG4-antibody. Methods: The MATINS (Macrophage Antibody To INhibit immune Suppression) trial is a multicenter first-in-human phase I/II study (NCT03733990) to assess the tolerability, safety and preliminary efficacy of FP-1305 in patients (pts) with advanced cancers including immunotherapy-refractory melanoma, cholangiocarcinoma, hepatocellular carcinoma, ovarian cancer, colorectal (CRC), and pancreatic ductal adenocarcinoma. Part 1 consisted of a dose escalation phase; 30 pts (median age 65, range 30-81) were enrolled to examine 5 dose levels (0.1, 0.3, 1.0, 3.0, 10 mg/kg), to determine the optimal dose of FP-1305 for Parts 2 and 3. Two-stage time-to-event continual reassessment method (TITE-CRM) was utilized for the dose escalation in Part 1. Pts received 1-8 cycles (median 3) of FP-1305 Q3w. FP-1305 was well tolerated without dose-limiting toxicities. A consistent increase in blood NK cells, CD8/CD4 T cell ratio, B cells and a decrease in regulatory T cells was demonstrated. FP-1305 dosing led to the activation (CD25+) and Th1 skewing (CXCR3+) of T cell populations including increase in effector CD8 T-cells with downregulation of several inhibitory immune checkpoint molecules (PD-1, PD-L1, CTLA-4, and LAG3). Increased circulating IFNɣ levels were detected, with the highest levels in a heavily pretreated metastatic, microsatellite stable (MSS) colorectal cancer patient leading to a partial tumor response (-52%). FP-1305 is the first macrophage checkpoint inhibitor candidate promoting immune switch with promising tolerability and clinical anti-tumor activity. FP-1305 represents a novel treatment option to provoke immune response especially in non-inflamed tumors. Full safety, pharmacokinetic and efficacy results of MATINS trial (Part 1) will be presented for the first time in a final late breaking abstract. Clinical trial information: 2018-002732-24 .

Published

2020

33. Self-reported quality of life and hope in phase-I trial participants: An observational prospective cohort study

Author

Esther Oomen-de Hoop, Diane A.J. van der Biessen, Peer van der Helm, Martijn P. Lolkema, Wendy H. Oldenmenger, Dennis Klein, Ron H.J. Mathijssen, Maja J.A. de Jonge, and Medical Oncology

Subjects

Adult, Male, Coping (psychology), medicine.medical_specialty, Research Subjects, Health Status, Appetite, Logistic regression, Cohort Studies, 03 medical and health sciences, Hope, 0302 clinical medicine, SDG 3 - Good Health and Well-being, Neoplasms, Global health, Medicine, Humans, 030212 general & internal medicine, Prospective Studies, Prospective cohort study, Aged, Aged, 80 and over, Clinical Trials, Phase I as Topic, business.industry, Role, Middle Aged, Social Participation, Clinical trial, Oncology, 030220 oncology & carcinogenesis, Mann–Whitney U test, Physical therapy, Quality of Life, Observational study, Female, Analysis of variance, Self Report, business

Abstract

For advanced cancer patients deliberating early clinical trial participation, adequate information about expected effect on quality of life (HRQoL) and hope, may support decision making. The aim was to assess the potential relation of HRQoL to eligibility for phase-I trial participation, and to observe the variations in patient-reported outcomes. Patients completed questionnaires at preconsent (n = 124), baseline (n = 96), and after first evaluation of a phase-I trial (n = 76). The Mann–Whitney U test was used to test differences between eligible and ineligible patients. Univariate logistic regression was performed for eligibility. Factorial repeated-measures ANOVA compared the outcomes of patients continuing vs. stopping participation after first evaluation over time. Eligibility is associated with significant better global health OR = 0.946, 95% CI [0.918, 0.975], p = 0.001, physical functioning OR = 0.959, 95% CI [0.933, 0.985], p = 0.002, role functioning OR = 0.974, 95% CI [0.957, 0.991] and better appetite OR = 1.114 95% CI [1.035, 1.192]. HRQoL outcomes like global health, social functioning and appetite decline in all patients and differ between patients continuing or having to end participation. Over time, hope and tenacity decline in all patients and coping strategies alter in patients stopping participation. Trial participation influences patient-reported outcomes. Global health may predict for eligibility and trial continuation. Informing patients could affect patients’ decision making.

Published

2018

34. A phase 1 study of PARP-inhibitor ABT-767 in advanced solid tumors with BRCA1/2 mutations and high-grade serous ovarian, fallopian tube, or primary peritoneal cancer

Author

Camille Serpenti, Peter Ansell, Kirsten Timms, Ingrid M.E. Desar, Martin Dunbar, Hao Xiong, Diane A.J. van der Biessen, Stacie Peacock Shepherd, Christine K. Ratajczak, Maja J.A. de Jonge, Rajendar K. Mittapalli, Martha W. den Hollander, Matthew W. Dudley, Carla M.L. van Herpen, Jourik A. Gietema, Robert Hetman, Damage and Repair in Cancer Development and Cancer Treatment (DARE), Guided Treatment in Optimal Selected Cancer Patients (GUTS), and Medical Oncology

Subjects

Male, 0301 basic medicine, Oncology, endocrine system diseases, BRCA, Food-Drug Interactions, 0302 clinical medicine, Phase I Studies, Pharmacology (medical), Fatigue, Peritoneal Neoplasms, Aged, 80 and over, Ovarian Neoplasms, Sulfonamides, Solid tumor, BRCA1 Protein, Anemia, Nausea, Middle Aged, CARRIERS, 3. Good health, Serous fluid, Treatment Outcome, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Benzamides, PARP inhibitor, Female, medicine.symptom, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Adult, EPITHELIAL OVARIAN, medicine.medical_specialty, Maximum Tolerated Dose, Antineoplastic Agents, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, Pharmacokinetics, SDG 3 - Good Health and Well-being, Ovarian cancer, Internal medicine, medicine, Fallopian Tube Neoplasms, Humans, Adverse effect, Aged, BRCA2 Protein, Pharmacology, business.industry, medicine.disease, 030104 developmental biology, POLY(ADP-RIBOSE) POLYMERASE INHIBITORS, Mutation, Homologous recombination deficiency, business, Fallopian tube

Abstract

Summary Purpose This phase 1 study examined safety, pharmacokinetics (PK), and efficacy of the poly(ADP-ribose) polymerase (PARP) inhibitor ABT-767 in patients with advanced solid tumors and BRCA1/2 mutations or with high-grade serous ovarian, fallopian tube, or primary peritoneal cancer. Methods Patients received ABT-767 monotherapy orally until disease progression or unacceptable toxicity. Dose was escalated from 20 mg once daily to 500 mg twice daily (BID). Dose-limiting toxicities, recommended phase 2 dose (RP2D), food effect, objective response rate, and biomarkers predicting response were determined. Results Ninety-three patients were treated with ABT-767; 80 had a primary diagnosis of ovarian cancer. ABT-767 demonstrated dose-proportional PK up to 500 mg BID and half-life of ~2 h. Food had no effect on ABT-767 bioavailability. Most common grade 3/4 treatment-related adverse events were nausea, fatigue, decreased appetite, and anemia. Anemia showed dose-dependent increase. RP2D was 400 mg BID. Objective response rate by RECIST 1.1 was 21% (17/80) in all evaluable patients and 20% (14/71) in evaluable patients with ovarian cancer. Response rate by RECIST 1.1 and/or CA-125 was 30% (24/80) in patients with ovarian cancer. Mutations in BRCA1 or BRCA2, homologous recombination deficiency (HRD), and platinum sensitivity were associated with tumor response. Median progression-free survival was longer for HRD positive (6.7 months) versus HRD negative patients (1.8 months) with ovarian cancer. Conclusions ABT-767 had an acceptable safety profile up to the established RP2D of 400 mg BID and dose-proportional PK. Patients with BRCA1 or BRCA2 mutation, HRD positivity, and platinum sensitivity were more sensitive to ABT-767.

Published

2018

35. Phase Ib Study of Lumretuzumab Plus Cetuximab or Erlotinib in Solid Tumor Patients and Evaluation of HER3 and Heregulin as Potential Biomarkers of Clinical Activity

Author

Francesca Michielin, Jan H.M. Schellens, Emile E. Voest, Maitram Nguyen, Álvaro Taus, T. Fleitas, Ji-Youn Han, Georgina Meneses-Lorente, Martin Weisser, Didier Meulendijks, Maja J.A. de Jonge, Marlies H.G. Langenberg, Birgit Bossenmaier, Suzana Vega-Harring, Lori Steiner, Ulrik Lassen, Morten Mau-Sørensen, Stefan Sleijfer, Celine Adessi, Martijn P. Lolkema, Sabine Wilson, Wolfgang Jacob, Marlene Thomas, Andrés Cervantes, Rajiv Dua, Maria Martinez-Garcia, Sang-We Kim, Maurizio Ceppi, Enriqueta Felip, Antonio Calles, Ian James, and Medical Oncology

Subjects

0301 basic medicine, Oncology, Male, Cancer Research, medicine.medical_specialty, Receptor, ErbB-3, Neuregulin-1, Cetuximab, Pharmacology, Antibodies, Monoclonal, Humanized, 03 medical and health sciences, Erlotinib Hydrochloride, 0302 clinical medicine, Internal medicine, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, Medicine, Humans, Adverse effect, neoplasms, Survival analysis, business.industry, Cancer, Lumretuzumab, medicine.disease, Survival Analysis, respiratory tract diseases, Clinical trial, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Treatment Outcome, 030220 oncology & carcinogenesis, Monoclonal, Female, Erlotinib, business, medicine.drug

Abstract

Purpose: This study investigated the safety, clinical activity, and target-associated biomarkers of lumretuzumab, a humanized, glycoengineered, anti-HER3 monoclonal antibody (mAb), in combination with the EGFR-blocking agents erlotinib or cetuximab in patients with advanced HER3-positive carcinomas.Experimental Design: The study included two parts: dose escalation and dose extension phases with lumretuzumab in combination with either cetuximab or erlotinib, respectively. In both parts, patients received lumretuzumab doses from 400 to 2,000 mg plus cetuximab or erlotinib according to standard posology, respectively. The effect of HRG mRNA and HER3 mRNA and protein expression were investigated in a dedicated extension cohort of squamous non–small cell lung cancer (sqNSCLC) patients treated with lumretuzumab and erlotinib.Results: Altogether, 120 patients were treated. One dose-limiting toxicity (DLT) in the cetuximab part and two DLTs in the erlotinib part were reported. The most frequent adverse events were gastrointestinal and skin toxicities, which were manageable. The objective response rate (ORR) was 6.1% in the cetuximab part and 4.2% in the erlotinib part. In the sqNSCLC extension cohort of the erlotinib part, higher tumor HRG and HER3 mRNA levels were associated with a numerically higher disease control rate but not ORR.Conclusions: The toxicity profile of lumretuzumab in combination with cetuximab and erlotinib was manageable, but only modest clinical activity was observed across tumor types. In the sqNSCLC cohort, there was no evidence of meaningful clinical benefit despite enriching for tumors with higher HRG mRNA expression levels. Clin Cancer Res; 23(18); 5406–15. ©2017 AACR.

Published

2017

36. First-in-Human Study of Abbv-621, a TRAIL Receptor Agonist Fusion Protein, in Patients (Pts) with Relapsed/Refractory (RR) Acute Myeloid Leukemia (AML) and Diffuse Large B-Cell Lymphoma (DLBCL)

Author

Sudhir Penugonda, Toshihiko Doi, Yu-Wei Chang, Emiliano Calvo, Monica Motwani, Maja J.A. de Jonge, Dimple A. Modi, Silpa Nuthalapati, Lot A. Devriese, Benedito A. Carneiro, Adam M. Petrich, and Victor Moreno

Subjects

Oncology, medicine.medical_specialty, biology, Combination therapy, business.industry, Venetoclax, Immunology, Cancer, Cell Biology, Hematology, medicine.disease, Biochemistry, chemistry.chemical_compound, chemistry, Tolerability, Alanine transaminase, Internal medicine, biology.protein, Clinical endpoint, Medicine, business, Diffuse large B-cell lymphoma, Progressive disease

Abstract

Background: Apoptotic cell death can be triggered by activation of extrinsic and intrinsic signaling pathways. Tumor necrosis factor (TNF)-related apoptosis-inducing ligand (TRAIL), a member of the TNF superfamily, binds to its death receptors TRAIL-R1 (DR4) and TRAIL-R2 (DR5) to selectively activate the extrinsic apoptotic pathway in cancer cells. ABBV-621 is a second-generation TRAIL receptor agonist with antitumor activity as monotherapy (621-mono) in preclinical models of AML and DLBCL. The intrinsic apoptotic pathway is regulated by the BCL2 protein family, commonly overexpressed in hematologic malignancies. Venetoclax (VEN), a highly selective small-molecule BCL2 inhibitor, has shown antitumor activity in combination therapy in AML and DLBCL. In preclinical and xenograft models of AML and DLBCL, the ABBV-621 and VEN combination (621-VEN) had antitumor activity superior to either agent alone. This first-in-human study evaluated ABBV-621 as single agent and in combination in pts with advanced solid tumors and hematologic malignancies (NCT03082209). Safety and tolerability of ABBV-621 in advanced solid tumors have previously been presented (Ratain et al. J Clin Oncol 2019;37[suppl]: abstr 3013). Here, we report preliminary data for 621-mono in pts with RR AML and for 621-VEN in pts with RR AML and DLBCL. Methods: Adult pts with RR AML or DLBCL (ECOG 0-2) were enrolled. Pts with AML received ABBV-621 at 1.25-, 3.75-, 7.5-mg/kg doses in the 621-mono and at 3.75-mg/kg dose in the 621-VEN arms. Pts in the DLBCL 621-VEN arm received ABBV-621 at 3.75- and 7.5-mg/kg doses. ABBV-621 was administered intravenously on D1, 8, and 15 of a 21-D cycle; in 621-VEN cohorts pts received 400 mg oral VEN daily, and could be escalated to 800 mg. The primary endpoint was safety. In addition, preliminary antitumor efficacy and ABBV-621 binding to decoy receptors on neutrophils from peripheral blood were assessed. Results: As of Jun 2019, 17 pts were enrolled. Pts in AML 621-mono arm (1.25 [1], 3.75 [1], 7.5 [2] mg/kg): 1 male; median (med) age, 75 yr (range 71-82); med prior treatments, 2.5 (range 1-4); med time on treatment, 15 D (range 1-70). Pts in AML 621-VEN arm (3.75 mg/kg [7]): 5 male; med age, 71 yr (60-79); med prior treatments, 2 (1-2); med time on treatment, 26 D (1-77). Pts in DLBCL 621-VEN arm (3.75 [3], 7.5 [3] mg/kg): 4 male; med age, 57 yr (40-75); stage 4 (3); med prior treatments, 2.5 (1 to ≥5); med time on treatment, 26 D (8-36). One pt in the AML 621-VEN 3.75-mg/kg dose cohort had increases in alanine aminotransferase, aspartate aminotransferase and bilirubin as dose-limiting toxicities. Sixteen pts experienced adverse events (AEs) irrespective of causality. A summary of AEs is shown in Table. One pt in the AML 621-mono 7.5-mg/kg dose cohort died due to AML progression, unrelated to ABBV-621. Antitumor activity was observed in 1 pt in the AML 621-VEN arm (with complex cytogenetics and TP53 mutation) who reached complete remission (CR). One pt in the DLBCL 621-VEN 3.75-mg/kg cohort had stable disease, 2 with AML had resistant disease (1 in 621-mono [7.5 mg/kg] and 1 in 621-VEN), and 7 had progressive disease (PD; 1 in AML 621-mono [1.25 mg/kg], 2 in AML 621-VEN, and 4 in DLBCL 621-VEN [2 each in 3.75- and 7.5-mg/kg] cohorts). Using flow cytometry, saturation of ABBV-621 binding to decoy receptors on neutrophils was observed at 2 h postdosing, followed by dose-dependent desaturation of receptors in pts with DLBCL at 48-168 h. In AML 621-VEN pts, ABBV-621 remained bound to decoy receptors for up to 168 h; in DLBCL 621-VEN pts, the duration of binding was higher at ABBV-621 7.5 mg/kg compared with 3.75 mg/kg. In AML, the baseline frequency of myeloblasts was higher in pts with PD than CR, while that of myelomonocytes was higher in the pt with CR. The frequency of myeloblasts and myelomonocytes expressing DR4 and DR5 at baseline was highest in the pt with CR (Figure). Conclusions: ABBV-621 was tolerated and showed antitumor activity in combination with VEN in pts with RR AML. Disclosures de Jonge: Faron Pharmaceuticals Ltd.: Consultancy. Carneiro:Actuate Therapeutics: Research Funding; Bayer: Research Funding; Pfizer: Research Funding; AstraZeneca: Research Funding; Medimmune: Research Funding; Astellas: Research Funding; AbbVie: Research Funding. Devriese:MSD: Consultancy. Penugonda:AbbVie: Employment, Other: Stock/stock options. Petrich:Abbvie: Employment, Equity Ownership. Nuthalapati:AbbVie: Employment, Other: Stock/stock options. Motwani:AbbVie: Employment, Other: Stock/stock options. Modi:AbbVie: Employment, Other: Stock/stock options. Chang:AbbVie: Employment, Other: Stock/stock options. Calvo:Celgene: Consultancy; Roche/Genentech: Consultancy, Other: travel/accommodations/expenses; Seattle Genetics: Consultancy; AstraZeneca: Consultancy, Research Funding; PsiOxus: Consultancy; Amcure: Consultancy; START: Other: stock/ownership interests, Research Funding; Janssen-Cilag: Consultancy; EUSA Pharma: Consultancy; Novartis: Consultancy, Research Funding, Speakers Bureau; Oncoart Associated: Other: stock/ownership interests; Guidepoint Global: Consultancy; Nanobiotix: Consultancy; HM Hospitales Group: Honoraria; AbbVie: Consultancy; BeiGene: Research Funding; Servier: Consultancy; International Cancer Consultants: Other: stock/ownership interests; Foundation INTHEOS: Other: president and founder; Gerson Lehrman Group: Consultancy; Pfizer: Consultancy. Moreno:Puma Biotechnology: Consultancy; Sanofi/Regeneron: Other: travel/accommodations/expenses.

Published

2019

37. OA01.07 Capmatinib (INC280) in METΔEX14-Mutated Advanced NSCLC: Efficacy Data from the Phase 2 Geometry MONO-1 Study

Author

E.F. Smit, Sylvie Le Mouhaer, Takashi Seto, Rebecca S. Heist, M. Waldron-Lynch, Juergen Wolf, P.J. Souquet, Maja J.A. de Jonge, D.S.W. Tan, Toyoaki Hida, Noemí Reguart, Anna Robeva, Sergey Orlov, Johan Vansteenkiste, J-Y. Han, Monica Giovannini, Edward B. Garon, and H. Groen

Subjects

Pulmonary and Respiratory Medicine, Capmatinib, Nuclear magnetic resonance, Oncology, business.industry, Phase (matter), Medicine, business

Published

2019

38. Phase 1, first-in-human study of TRAIL receptor agonist fusion protein ABBV-621

Author

Mark J. Ratain, Emiliano Calvo, Martin Dunbar, Drew W. Rasco, Maja J.A. de Jonge, Adam M. Petrich, Patricia LoRusso, Manoj Chiney, Toshihiko Doi, Jaimee Glasgow, and Monica Motwani

Subjects

Agonist, Cancer Research, medicine.drug_class, business.industry, First in human, Ligand (biochemistry), Fusion protein, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Phase (matter), Apoptotic cell death, medicine, Receptor, business, 030215 immunology

Abstract

3013 Background: ABBV-621 is a potent tumor-necrosis factor-related apoptosis-inducing ligand (TRAIL) receptor agonist fusion protein that induces apoptotic cell death, particularly in DR4/5 expressing tumor models. Methods: Patients (pts) with previously treated solid tumors and ECOG 0–2 were administered ABBV-621 (2.5–15 mg/kg IV) on day (D) 1 (dose level [DL] 1) or D1D8 (DL2 and beyond) of each 21-day cycle. Dose escalation (DE) was guided by a Bayesian continual reassessment method. In addition to PK studies, blood-based PD markers of apoptosis (M30, M65) and drug binding were assessed. Results: As of 14 December 2018, 57 pts were enrolled in the DE portion, of which 30% had pancreatic, 23% colorectal cancer, and 47% other tumor types; 13 were KRAS mutant. Median age was 61 yrs. 60% were male; pts had a median of 4 prior regimens (range 1–10). Pts per DL: 2.5 (5 on D1, 16 on D1D8), 3.75 (12), 5 (6), 6.5 (6), 8.5 (4), 11 (4), and 15 mg/kg (4). Median duration of ABBV-621 exposure was 2 cycles (range 1–11). Seven pts had dose-limiting toxicities: respiratory failure (5 mg/kg; Grade 5, the only treatment-related death), blood bilirubin increased (3.75, 6.5 mg/kg), nausea (3.75 mg/kg), fatigue (3.75 mg/kg), increased ALT (2.5, 3.75, 6.5, 15 mg/kg), and increased AST (6.5 mg/kg). Summary of AEs is shown in Table. Clinical trial information: NCT03082209. A partial response (duration 20 weeks) was observed in a pt with pancreatic cancer (2.5 mg/kg D1D8). 27 pts had stable disease (6 pts for > 12 weeks). ABBV-621 PK was linear (mean ± SD clearance was 1.79 mL/h/kg ± 0.44) with a terminal half-life of 36.7 ± 5.55 h (n = 49). ABBV-621 bound to decoy receptors on neutrophils for up to 168 h; the duration of binding was dose-dependent. M30 and M65 increased at 8, 24, and 48 h following ABBV-621, but effect was independent of dose. Conclusions: ABBV-621 shows evidence of antitumor activity and effect on blood-based markers of apoptosis, with acceptable toxicity (MTD not reached). NCT03082209.[Table: see text]

Published

2019

39. Capmatinib (INC280) in METΔex14-mutated advanced non-small cell lung cancer (NSCLC): Efficacy data from the phase II GEOMETRY mono-1 study

Author

Daniel Shao-Weng Tan, Egbert F. Smit, Harry J.M. Groen, Rebecca S. Heist, Toyoaki Hida, Pierre Jean Souquet, Juergen Wolf, Sylvie Le Mouhaer, Monica Giovannini, Edward B. Garon, Anna Robeva, Sergey Orlov, Maja J.A. de Jonge, M. Waldron-Lynch, Ji-Youn Han, Takashi Seto, Noemí Reguart, and Johan Vansteenkiste

Subjects

Cancer Research, Capmatinib, business.industry, non-small cell lung cancer (NSCLC), Geometry, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Overall response rate, Oncology, 030220 oncology & carcinogenesis, Phase (matter), Toxicity, Medicine, business, 030215 immunology

Abstract

9004 Background: Capmatinib is a highly potent and selective MET inhibitor. Previous data of GEOMETRY mono-1 study showed a clinically meaningful overall response rate (ORR) and manageable toxicity profile in patients (pts) with METΔex14–mutated NSCLC who received 1–2 prior lines of treatment (tx) (Cohort 4) and in particular a high ORR in tx-naïve pts (Cohort 5b). Here we report the results in METΔex14–mutated NSCLC for duration of response (DOR) and progression-free survival (PFS) as well as the updated results for ORR. Methods: GEOMETRY mono-1 is a phase 2, multi-cohort, multicenter study evaluating capmatinib in pts with METΔex14-mutated or MET-amplified advanced NSCLC across 6 cohorts. Pts (≥18 yrs) with ECOG PS 0–1, ALK and EGFR wt, and stage IIIB/IV NSCLC were eligible. Pts with METΔex14 mutation (centrally confirmed) were assigned (regardless of MET amplification status/gene copy number) to Cohorts 4 and 5b and received capmatinib tablets 400 mg BID. Primary endpoint was ORR by Blinded Independent Review Committee (BIRC) per RECIST v1.1. Key secondary endpoint was DOR by BIRC. Results: As of Nov 08, 2018, 97 pts with METΔex14-mutated NSCLC (Cohort 4: 69 pts; Cohort 5b: 28 pts) were evaluable for efficacy. ORR (95% CI) by BIRC was 39.1% (27.6-51.6) in Cohort 4 and 71.4% (51.3-86.8) in Cohort 5b. While still immature at the time of this analysis, data on durability are promising: median DOR (95% CI) by BIRC was 9.72 (4.27-11.14) and 8.41 (5.55-NE) mo for Cohorts 4 and 5b, respectively; median PFS (95% CI) by BIRC was 5.42 (4.17-6.97) and 9.13 (5.52-13.86) mo for Cohorts 4 and 5b, respectively. Safety profile remains favourable and unchanged. Most common AEs (≥25% all grades) across all cohorts (n = 315), were peripheral edema (49.2%), nausea (43.2%), and vomiting (28.3%); majority of the AEs were grade 1/2. Final efficacy analysis (12-mo f-u on DOR) including biomarker data will be presented during meeting. Conclusions: These data confirm capmatinib to be a promising new treatment option for pts with METΔex14-mutated advanced NSCLC regardless of the line of therapy with deep and durable responses and manageable toxicity profile. Clinical trial information: NCT02414139.

Published

2019

40. Randomized, Open-Label, Crossover Studies Evaluating the Effect of Food and Liquid Formulation on the Pharmacokinetics of the Novel Focal Adhesion Kinase (FAK) Inhibitor BI 853520

Author

Neeltje Steeghs, Hal W. Hirte, Lillian L. Siu, Linda C Pronk, David Schnell, Sebastien J. Hotte, Martijn P. Lolkema, Maja J.A. de Jonge, Diane A.J. van der Biessen, Anna Spreafico, Filip de Vos, and Remy B. Verheijen

Subjects

0301 basic medicine, Male, Cancer Research, Analytical chemistry, Administration, Oral, Food-Drug Interactions, 0302 clinical medicine, Treatment compliance, Neoplasms, 80 and over, Medicine, Tissue Distribution, Pharmacology (medical), Original Research Article, Neoplasm Metastasis, Non-U.S. Gov't, Aged, 80 and over, Cross-Over Studies, Research Support, Non-U.S. Gov't, Protein Kinase Inhibitors/pharmacokinetics, Middle Aged, Prognosis, Clinical Trial, Oncology, 030220 oncology & carcinogenesis, Area Under Curve, Administration, Randomized Controlled Trial, Female, Open label, Focal Adhesion Kinase 1/antagonists & inhibitors, Tablets, Oral, Adult, Maximum Tolerated Dose, Cmax, Capsules, Bioequivalence, Research Support, Clinical Trial, Phase I, 03 medical and health sciences, Phase I, Pharmacokinetics, Journal Article, Humans, Protein Kinase Inhibitors, Aged, business.industry, Order (ring theory), Crossover study, Neoplasms/drug therapy, 030104 developmental biology, Therapeutic Equivalency, Focal Adhesion Kinase 1, Tablets/administration & dosage, Geometric mean, business

Abstract

Background BI 853520 is a potent inhibitor of focal adhesion kinase and is currently under clinical development for the treatment of non-hematological malignancies. Objective The objective of this study was to evaluate the effect of food and liquid dispersion on the pharmacokinetics of BI 853520 in two open-label, crossover substudies. Patients and Methods Sixteen patients with advanced solid tumors were enrolled in each substudy. The order of administration was randomized, and pharmacokinetic samples were collected for 48 h after administration of a 200 mg dose of BI 853520. Lack of effect would be demonstrated if the 90% confidence interval (CI) of the ratio of the adjusted geometric mean (GMR) of the area under the plasma curve (area under the plasma concentration–time curve from time zero to the last quantifiable concentration at tz [\documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{AUC}}_{{0{-}t_{\text{z}} }}$$\end{document}AUC0-tz] and observed area under the plasma concentration–time curve extrapolated from time zero to infinity [AUC0–∞,obs]) and maximum plasma concentration (Cmax) did not cross the 80–125% (bioequivalence) boundaries. Results Adjusted GMRs (90% CIs) for the fed versus fasted state were 92.46% (74.24–115.16), 98.17% (78.53–122.74), and 87.34% (71.04–107.38) for \documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{AUC}}_{{0{-}t_{\text{z}} }}$$\end{document}AUC0-tz, AUC0–∞,obs, and Cmax, respectively. Although the 90% CIs were not within bioequivalence limits for the food-effect study, the limited reductions in these pharmacokinetic parameters after administration with a high-fat meal are unlikely to be clinically relevant. Compared with a tablet, administration of BI 853520 as a liquid dispersion did not strongly affect \documentclass[12pt]{minimal} \usepackage{amsmath} \usepackage{wasysym} \usepackage{amsfonts} \usepackage{amssymb} \usepackage{amsbsy} \usepackage{mathrsfs} \usepackage{upgreek} \setlength{\oddsidemargin}{-69pt} \begin{document}$${\text{AUC}}_{{0{-}t_{\text{z}} }}$$\end{document}AUC0-tz, AUC0–∞,obs, or Cmax, resulting in adjusted GMRs (90% CIs) of 1.00 (0.92–1.09), 0.98 (0.90–1.07), and 0.93 (0.86–1.01), respectively. Conclusions These studies demonstrate that BI 853520 can be given with no food restrictions, and as a liquid dispersion, without strongly impacting pharmacokinetics. These pharmacokinetic properties may help make BI 853520 dosing more convenient and flexible, improving treatment compliance. Clinical trials registration ClinicalTrials.gov identifier: NCT01335269. Electronic supplementary material The online version of this article (10.1007/s11523-018-00618-0) contains supplementary material, which is available to authorized users.

Published

2019

41. Moving the Frontiers of Cancer Chemotherapy for Solid Tumors by Changing the Scope of Drug Development

Author

Maja J.A. de Jonge and Jaap Verweij

Subjects

Cancer chemotherapy, Scope (project management), business.industry, Cancer, Hematology, Pharmacology, medicine.disease, Gemcitabine, Drug treatment, Drug development, Cancer cell, Cancer research, Medicine, business, medicine.drug

Abstract

Our increasing knowledge on the pathogenetic mechanisms involved in the growth of cancer cells and on the molecular basis of cancer has influenced the development of anticancer agents. The realization that new targets should be evaluated for anti-cancer drug treatment has a.o. led to the introduction of the taxoids and topoisomerase I inhibitors. Attacking the known targets in a more sophisticated way led to the development of drugs with increased target specificity like Tomudex and Gemcitabine. Finally, using old drugs more efficiently by using pharmacokinetic and pharmacodynamic ananlysis hold a promise for the near future.

Published

2016

42. Targeted Next Generation Sequencing as a Reliable Diagnostic Assay for the Detection of Somatic Mutations in Tumours Using Minimal DNA Amounts from Formalin Fixed Paraffin Embedded Material

Author

Stefan Sleijfer, Christa G Gadellaa-van Hooijdonk, Marco J. Koudijs, Emile E. Voest, Stefan M. Willems, John W. J. Hinrichs, Edwin Cuppen, Wendy W.J. de Leng, Robert D. Loberg, Neeltje Steeghs, Ies J Nijman, Marlies H.G. Langenberg, Martijn P. Lolkema, Roel A. de Weger, Stef van Lieshout, Françoise A. S. Barendregt-Smouter, Maja J.A. de Jonge, and Medical Oncology

Subjects

0301 basic medicine, Tissue Fixation, Molecular biology, Somatic cell, Mutagenesis and Gene Deletion Techniques, DNA Mutational Analysis, Gene Identification and Analysis, Gene Sequencing, lcsh:Medicine, Biochemistry, chemistry.chemical_compound, Sequencing techniques, 0302 clinical medicine, Neoplasms, Medicine and Health Sciences, DNA sequencing, lcsh:Science, Non-U.S. Gov't, Genetics, Medicine(all), Paraffin Embedding, Multidisciplinary, Agricultural and Biological Sciences(all), Research Support, Non-U.S. Gov't, High-Throughput Nucleotide Sequencing, Genomics, Cancer treatment, Oncology, 030220 oncology & carcinogenesis, Transcriptome Analysis, Research Article, Next-Generation Sequencing, Formalin fixed paraffin embedded, Biology, Biomolecular isolation, Research Support, 03 medical and health sciences, Diagnostic Medicine, Formaldehyde, Cancer Detection and Diagnosis, Journal Article, Humans, Mutation Detection, Biology and life sciences, Biochemistry, Genetics and Molecular Biology(all), lcsh:R, Computational Biology, Reproducibility of Results, Ion semiconductor sequencing, Genome Analysis, DNA isolation, DNA extraction, Research and analysis methods, Molecular biology techniques, Mutational Analysis, 030104 developmental biology, chemistry, Mutation, lcsh:Q, DNA, Genetics and Molecular Biology(all)

Abstract

textabstractBackground Targeted Next Generation Sequencing (NGS) offers a way to implement testing of multiple genetic aberrations in diagnostic pathology practice, which is necessary for personalized cancer treatment. However, no standards regarding input material have been defined. This study therefore aimed to determine the effect of the type of input material (e.g. formalin fixed paraffin embedded (FFPE) versus fresh frozen (FF) tissue) on NGS derived results. Moreover, this study aimed to explore a standardized analysis pipeline to support consistent clinical decision-making. Method We used the Ion Torrent PGM sequencing platform in combination with the Ion AmpliSeq Cancer Hotspot Panel v2 to sequence frequently mutated regions in 50 cancer related genes, and validated the NGS detected variants in 250 FFPE samples using standard diagnostic assays. Next, 386 tumour samples were sequenced to explore the effect of input material on variant detection variables. For variant calling, Ion Torrent analysis software was supplemented with additional variant annotation and filtering. Results Both FFPE and FF tissue could be sequenced reliably with a sensitivity of 99.1%. Validation showed a 98.5%concordance between NGS and conventional sequencing techniques, where NGS provided both the advantage of low input DNA concentration and the detection of low-frequency variants. The reliability of mutation analysis could be further improved with manual inspection of sequence data. Conclusion Targeted NGS can be reliably implemented in cancer diagnostics using both FFPE and FF tissue when using appropriate analysis settings, even with low input DNA.

Published

2016

43. First-in-Human Phase I Study of Lumretuzumab, a Glycoengineered Humanized Anti-HER3 Monoclonal Antibody, in Patients with Metastatic or Advanced HER3-Positive Solid Tumors

Author

Morten Mau Soerensen, Andrés Cervantes, Maria Martinez-Garcia, Stefan Sleijfer, Tania Fleitas Kanonnikoff, Didier Meulendijks, Maja J.A. de Jonge, Keelara Abiraj, Álvaro Taus, Marlene Thomas, Maurizio Ceppi, Ulrik Lassen, Birgit Bossenmaier, Emile E. Voest, Jan H.M. Schellens, Celine Adessi, Martin Weisser, Wolfgang Jacob, Georgina Meneses-Lorente, Marlies H.G. Langenberg, Martijn P. Lolkema, Francesca Michielin, Ian James, and Medical Oncology

Subjects

Adult, Male, 0301 basic medicine, Cancer Research, medicine.medical_specialty, Pathology, Maximum Tolerated Dose, Receptor, ErbB-3, Cmax, Antibodies, Monoclonal, Humanized, Research Support, Gastroenterology, Clinical Trial, Phase I, 03 medical and health sciences, Phase I, 0302 clinical medicine, Pharmacokinetics, Internal medicine, Journal Article, medicine, Humans, Non-U.S. Gov't, Adverse effect, Aged, Analgesics, business.industry, Research Support, Non-U.S. Gov't, Cancer, Middle Aged, Lumretuzumab, medicine.disease, Clinical Trial, Multicenter Study, Treatment Outcome, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Pharmacodynamics, Monoclonal, Female, Colorectal Neoplasms, business, Ex vivo

Abstract

Purpose: A first-in-human phase I study was conducted to characterize safety, efficacy, and pharmacokinetic (PK) and pharmacodynamic (PD) properties of lumretuzumab, a humanized and glycoengineered anti-HER3 monoclonal antibody, in patients with advanced cancer. Experimental Design: Twenty-five patients with histologically confirmed HER3-expressing tumors received lumretuzumab (100, 200, 400, 800, 1,600, and 2,000 mg) every two weeks (q2w) in 3+3 dose-escalation phase. In addition, 22 patients were enrolled into an extension cohort at 2,000 mg q2w. Results: There were no dose-limiting toxicities. Common adverse events (any grade) included diarrhea (22 patients, 46.8%), fatigue (21 patients, 44.7%), decreased appetite (15 patients, 31.9%), infusion-related reactions (13 patients, 27.7%), and constipation (10 patients, 21.3%). The peak concentration (Cmax) and area under the concentration–time curve up to the last measurable concentration (AUClast) of lumretuzumab increased more than dose proportionally from 100 mg up to 400 mg. Linear PK was observed with doses ≥400 mg q2w indicating target-mediated drug disposition saturation. Downregulation of HER3 membranous protein was observed in on-treatment tumor biopsies from 200 mg, and was maximal at and above 400 mg. An ex vivo assay demonstrated increased activation potential of peripheral NK lymphocytes with lumretuzumab compared with a non-glycoengineered anti-HER3 antibody. Ten patients (21.3%) had stable disease and remained on study at a median of 111 days (range, 80–225 days). Conclusions: Lumretuzumab was well tolerated and showed evidence of clinical activity. Linear serum PK properties and plateauing of PD effects in serial tumor biopsies indicate optimal biologically active doses of lumretuzumab from 400 mg onwards. Clin Cancer Res; 22(4); 877–85. ©2015 AACR.

Published

2016

44. TP53 mutations emerge with HDM2 inhibitor SAR405838 treatment in de-differentiated liposarcoma

Author

Axel Le Cesne, Mark A. Dickson, Andrea Varga, Madelyn Light, James Watters, Maja J.A. de Jonge, Steve Rowley, Gary K. Schwartz, Andrew J. Wagner, Edwin Choy, Rastilav Bahleda, Sandrine Macé, Joon Sang Lee, Joonil Jung, and Medical Oncology

Subjects

0301 basic medicine, Adult, Indoles, Time Factors, Cellular differentiation, Science, Biopsy, Mutant, DNA Mutational Analysis, General Physics and Astronomy, Antineoplastic Agents, Drug resistance, Biology, Liposarcoma, medicine.disease_cause, Bioinformatics, General Biochemistry, Genetics and Molecular Biology, Article, Circulating Tumor DNA, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Spiro Compounds, neoplasms, Response Evaluation Criteria in Solid Tumors, Mutation, Multidisciplinary, medicine.diagnostic_test, Antagonist, Cell Differentiation, Proto-Oncogene Proteins c-mdm2, General Chemistry, medicine.disease, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Mdm2, Tumor Suppressor Protein p53

Abstract

In tumours that harbour wild-type p53, p53 protein function is frequently disabled by the mouse double minute 2 protein (MDM2, or HDM2 in humans). Multiple HDM2 antagonists are currently in clinical development. Preclinical data indicate that TP53 mutations are a possible mechanism of acquired resistance to HDM2 inhibition; however, this resistance mechanism has not been reported in patients. Utilizing liquid biopsies, here we demonstrate that TP53 mutations appear in circulating cell-free DNA obtained from patients with de-differentiated liposarcoma being treated with an inhibitor of the HDM2–p53 interaction (SAR405838). TP53 mutation burden increases over time and correlates with change in tumour size, likely representing selection of TP53 mutant clones resistant to HDM2 inhibition. These results provide the first clinical demonstration of the emergence of TP53 mutations in response to an HDM2 antagonist and have significant implications for the clinical development of this class of molecules., Pre-clinical studies have shown that TP53 mutations can account for acquired resistance to HDM2 antagonists. This study provides clinical evidence for the emergence of TP53 mutations in circulating cell-free DNA, seen in 5 out of 20 de-differentiated liposarcoma patients treated with an HDM2 antagonist.

Published

2016

45. Moving molecular targeted drug therapy towards personalized medicine: Issues related to clinical trial design

Author

Stefan Sleijfer, Maja J.A. de Jonge, Jaap Verweij, Ferry A.L.M. Eskens, and Medical Oncology

Subjects

Clinical Trials as Topic, Cancer Research, Molecular targeted drug, medicine.medical_specialty, business.industry, Event (computing), Clinical study design, Reviews, Antineoplastic Agents, General Medicine, Pharmacology, Oncology, Research Design, Neoplasms, Genetics, Molecular targets, Humans, Molecular Medicine, Medicine, Medical physics, Personalized medicine, Precision Medicine, business

Abstract

With the event of new Molecular targets, clinical trial design requirements to perform these trials are changing. This paper discusses some of the considerations that need to be taken into account when designing a trial, including those trials that assess combinations of targets. (C) 2012 Federation of European Biochemical Societies. Published by Elsevier B.V. All rights reserved.

Published

2012

46. Biologic and Clinical Activity of Tivozanib (AV-951, KRN-951), a Selective Inhibitor of VEGF Receptor-1,-2, and -3 Tyrosine Kinases, in a 4-Week-On, 2-Week-Off Schedule in Patients with Advanced Solid Tumors

Author

Pankaj Bhargava, Brooke Esteves, Maja J.A. de Jonge, Monette M. Cotreau, Kunihiko Hayashi, Ferry A.L.M. Eskens, Jaap Verweij, Herman Burger, Toshiyuki Isoe, Maarten Thomeer, Leni van Doorn, Medical Oncology, and Radiology & Nuclear Medicine

Subjects

Adult, Male, Cancer Research, medicine.medical_specialty, Tivozanib, Maximum Tolerated Dose, medicine.drug_class, Colorectal cancer, Urology, Antineoplastic Agents, Pharmacology, Tyrosine-kinase inhibitor, Drug Administration Schedule, Animal data, Pharmacokinetics, SDG 3 - Good Health and Well-being, Neoplasms, medicine, Humans, Protein Kinase Inhibitors, Aged, business.industry, Phenylurea Compounds, Cancer, Middle Aged, medicine.disease, Vascular Endothelial Growth Factor Receptor-3, Vascular Endothelial Growth Factor Receptor-2, Receptors, Vascular Endothelial Growth Factor, Oncology, Pharmacodynamics, Toxicity, Quinolines, Female, business, medicine.drug

Abstract

Purpose: To assess the maximum tolerated dose (MTD)/dose-limiting toxicities (DLT), safety, pharmacokinetics, and pharmacodynamics of tivozanib, a potent and selective oral VEGF receptor (VEGFR) tyrosine kinase inhibitor. Experimental Design: Dose levels of 1.0, 1.5, and 2.0 mg/d tivozanib for 28 days followed by 14 days of medication were explored in patients with advanced solid tumors. Results: Forty-one patients were enrolled. Animal data incorrectly predicted toxicity, resulting in DLTs at the starting dose (2.0 mg) consisting of grade 3 proteinuria and hypertension and grade 3 ataxia. At 1.0 mg, no DLT was observed. At an intermediate dose (1.5 mg), 1 patient experienced DLT consisting of grade 3 hypertension. This dose was determined as the MTD. Of 10 additional patients treated at 1.5 mg, 1 patient each experienced grade 3 hypertension and grade 3 fatigue, and 2 patients experienced grade 3 and 4 transaminase elevation. In 12 additional patients treated at 1.0 mg, no DLT was observed. Pharmacokinetics displayed long absorption time, dose proportional exposure, and a half-life of 4.7 days. Plasma levels of VEGF-A and soluble VEGFR-2 showed dose-dependent increases and decreases, respectively. Dynamic contrast-enhanced MRI indicated reduction in tumor perfusion. Clinical activity was observed in renal cell cancer, colorectal cancer, and other tumors. Conclusion: Tivozanib was well tolerated with manageable side effects. The pharmacokinetics profile revealed that tivozanib was suitable for once-daily dosing. Encouraging and durable clinical activity was observed. The recommended daily dose of tivozanib in a 4-week-on and 2-week-off dosing regimen is 1.5 mg. Clin Cancer Res; 17(22); 7156–63. ©2011 AACR.

Published

2011

47. Treatment with Combination of Dabrafenib and Trametinib in Patients with Recurrent/Refractory BRAF V600E-Mutated Hairy Cell Leukemia (HCL)

Author

Robert J. Kreitman, Vivek Subbiah, Sascha Dietrich, Paul Burgess, Maja J.A. de Jonge, Alexander Stein, Anas Gazzah, Fatima Rangwala, Jean-Yves Blay, Bijoyesh Mookerjee, Farhad Ravandi, Wolfgang Willenbacher, Jacques De Greve, Martin Hutchings, Philippe Moreau, Evgeny Arons, and Zev A. Wainberg

Subjects

Trametinib, medicine.medical_specialty, business.industry, Immunology, Dabrafenib, Cell Biology, Hematology, Neutropenia, medicine.disease, Biochemistry, Minimal residual disease, 03 medical and health sciences, Moxetumomab pasudotox, 0302 clinical medicine, 030220 oncology & carcinogenesis, Internal medicine, Clinical endpoint, Medicine, Chills, Rituximab, medicine.symptom, business, 030215 immunology, medicine.drug

Abstract

BACKGROUND: Hairy cell leukemia is a rare, indolent, B-cell lymphoproliferative disease characterized by the BRAF V600E mutation in 90% to 100% of patients. Few treatment options are available for patients who progress on first-line therapy with a purine analogue and/or rituximab. The efficacy of combined BRAF and MEK inhibition is well established in BRAF V600-mutated melanoma, non-small cell lung cancer, and anaplastic thyroid cancer. Here we report interim results of treatment with the combination of dabrafenib (BRAF inhibitor) and trametinib (MEK inhibitor) in patients with recurrent/refractory BRAF V600E-mutated HCL. METHODS: In this phase 2, open-label trial (ROAR; NCT02034110), patients with BRAF V600E mutations in 9 rare tumor types, including HCL, received continuous dabrafenib (150 mg twice daily) and trametinib (2 mg once daily) until unacceptable toxicity, disease progression, or death. For the HCL cohort, eligible patients had histologically confirmed HCL (according to WHO classification) that was refractory to first-line treatment with a purine analogue or relapsed after ≥ 2 prior lines of treatment. The presence of a BRAF V600E mutation was assessed locally and confirmed by a central laboratory. The primary endpoint was investigator-assessed overall response rate (ORR) based on criteria adapted from NCCN guidelines. Secondary endpoints were duration of response (DOR), progression-free survival (PFS), overall survival (OS), and safety. Minimal residual disease (MRD) status was assessed by flow cytometry in both peripheral blood and bone marrow aspirates. For complete response (CR) without MRD, both peripheral blood and bone marrow aspirate samples had to be negative. RESULTS: At the data cutoff (January 3, 2018), 43 patients with HCL had enrolled. Median age was 67 years (range, 40-81) and 38 (88%) were male. Twenty-one patients (49%) had received ≥ 4 prior treatments. At the time of data cutoff, 35 patients (81%) remained on study treatment, 5 (12%) in follow-up; 2 (5%) had withdrawn from study (loss to follow-up and consent withdrawal [n = 1 each]), and 1 (2%) had died. Eight patients had discontinued therapy due to adverse events (AEs; 5 [12%]), study withdrawal (2 [5%]), or disease progression (1 [2%]). Median time on study treatment was 17 months (range, 1-39). Among 41 patients evaluable for response, the investigator-assessed confirmed ORR was 78% (32/41; 95% CI, 62%-89%) with 20 (49%) having CR, (6 [15%] CR without MRD and 14 [34%] CR with MRD), and 12 (29%) partial response. All responses were ongoing at the data cutoff; 16 (50%) responses were lasting ≥ 18 months. PFS and OS rates at 12 months were both 97.6% (95% CI, 83.9%-99.7%). The most common AEs in patients with HCL were pyrexia (67%), chills (51%), hyperglycemia (44%), nausea (44%), peripheral edema (42%), cough (40%), and fatigue (40%). Grade 3/4 AEs were reported in 49% of patients, with the most common (> 5%) being hyperglycemia (9%), anemia (7%), and neutropenia (7%). AEs led to dose reduction and treatment interruption in 42% and 56% of patients, respectively. AEs led to permanent discontinuation in 5 patients (12%; headache and malaise [n = 1]; pyrexia, chills and palmar-plantar erythrodysesthesia syndrome [n = 1]; fat necrosis [n = 1]; hyperglycemia and pancreatic adenocarcinoma [n = 1]; Hodgkin lymphoma [n = 1]). CONCLUSIONS: Dabrafenib + trametinib was well tolerated and demonstrated a high rate of durable responses in patients with heavily pretreated recurrent/refractory BRAF V600E-mutated HCL. Disclosures Kreitman: NIH: Patents & Royalties: Co-inventor on the NIH patent for Moxetumomab Pasudotox. Moreau:Janssen: Honoraria, Membership on an entity's Board of Directors or advisory committees; Amgen: Honoraria, Membership on an entity's Board of Directors or advisory committees; Abbvie: Honoraria, Membership on an entity's Board of Directors or advisory committees; Celgene: Honoraria, Membership on an entity's Board of Directors or advisory committees; Takeda: Honoraria, Membership on an entity's Board of Directors or advisory committees. Blay:Roche: Honoraria, Other: Non-financial support, Research Funding; Novartis: Honoraria, Other: Non-financial support, Research Funding. Wainberg:Merck: Consultancy; EMD Serono: Consultancy; Lilly: Consultancy; Five Prime: Consultancy; Novartis: Consultancy. Stein:Novartis: Other: Patient documentation fees; GSK: Other: Patient documentation fees. Willenbacher:Merck: Honoraria; Celgene: Honoraria, Research Funding; Roche: Honoraria, Research Funding; Janssen: Honoraria, Research Funding; BMS: Honoraria; Novartis: Honoraria, Research Funding; Takeda: Honoraria, Research Funding; Amgen: Honoraria, Other: Steering board, Research Funding. Ravandi:Macrogenix: Honoraria, Research Funding; Abbvie: Research Funding; Xencor: Research Funding; Astellas Pharmaceuticals: Consultancy, Honoraria; Sunesis: Honoraria; Seattle Genetics: Research Funding; Bristol-Myers Squibb: Research Funding; Xencor: Research Funding; Abbvie: Research Funding; Amgen: Honoraria, Research Funding, Speakers Bureau; Bristol-Myers Squibb: Research Funding; Orsenix: Honoraria; Seattle Genetics: Research Funding; Macrogenix: Honoraria, Research Funding; Orsenix: Honoraria; Jazz: Honoraria; Jazz: Honoraria; Sunesis: Honoraria; Astellas Pharmaceuticals: Consultancy, Honoraria; Amgen: Honoraria, Research Funding, Speakers Bureau. Burgess:Novartis: Employment. Mookerjee:Novartis: Employment. Subbiah:Roche/Genentech: Research Funding; LOXO: Research Funding; Blueprint Medicine: Research Funding; Novartis: Research Funding; Abbvie: Research Funding; Bayer: Research Funding.

Published

2018

48. Early cessation of the clinical development of LiPlaCis, a liposomal cisplatin formulation

Author

Jaap Verweij, Judith R. Kroep, Marije Slingerland, Diane A.J. van der Biessen, Margret den Hollander, Erik A.C. Wiemer, Mei-Ho Lam, Walter J. Loos, Ron H.J. Mathijssen, Hans Gelderblom, Maja J.A. de Jonge, Herman Burger, and Medical Oncology

Subjects

Adult, Male, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, Urology, Phases of clinical research, Antineoplastic Agents, Neutropenia, Pharmacology, Nephrotoxicity, Pharmacokinetics, Neoplasms, Injection site reaction, Humans, Medicine, Infusions, Intravenous, Aged, Dose-Response Relationship, Drug, business.industry, Area under the curve, Middle Aged, medicine.disease, Oncology, Tolerability, Area Under Curve, Liposomes, Toxicity, Female, Cisplatin, business

Abstract

PURPOSE: To evaluate the safety and tolerability of LiPlaCis, a liposomal formulated platinum compound, in patients with solid tumours and to determine the maximum tolerated dose (MTD) of intravenous (i.v.) LiPlaCis. and to assess plasma and urine pharmacokinetics and plasma biomarkers.PATIENTS AND METHODS: Patients with solid tumours without standard therapeutic options were enrolled to receive LiPlaCis administered as a 1 h infusion without additional hydration every 3weeks until RECIST progression or unacceptable toxicity. Cohorts of 3-6 patients were treated at each dose level until MTD was reached.RESULTS: Eighteen patients were enrolled and 64 cycles were delivered. At the first dose level 3 patients experienced an infusion reaction. Despite prophylactic pre-medication and prolongation of the infusion to 2 h in further patients, three other patients had mild acute infusion reactions. Toxicity at the fifth dose level of 120 mg consisted of grade 2 renal toxicity reversible after hydration in 2 patients and grade 4 thrombocytopaenia in one of these patients. Peak plasma concentrations and AUC were dose proportional. The interpatient variability in the clearance of total LiPlaCis-derived platinum was 41%. Platinum was excreted via the urine mainly during the first 24 h after administration. Investigated plasma biomarkers sPLA(2) and SC5b-9 were related to, but not predictive for, acute infusion reactions.CONCLUSION: The observed safety profile suggests no benefit over standard cisplatin formulations and LiPlaCis will require reformulation to enable further development.

Published

2010

49. Abstract CT175: Biomarker analyses from a phase I study of WNT974, a first-in-class Porcupine inhibitor, in patients (pts) with advanced solid tumors

Author

Abdelkader Seroutou, Yan Ji, Marios Giannakis, Margaret E. McLaughlin, David Smith, Elena Garralda, Filip Janku, Jennifer Morawiak, Ulka N. Vaishampayan, Roisin M. Connolly, Jason R. Dobson, Sinead Dolan, Guillem Argiles, Jordi Rodon, Susan Moody, and Maja J.A. de Jonge

Subjects

0301 basic medicine, Cancer Research, Colorectal cancer, business.industry, Melanoma, Wnt signaling pathway, Cancer, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Breast cancer, Oncology, 030220 oncology & carcinogenesis, Pancreatic cancer, Cancer research, medicine, AXIN2, business, Triple-negative breast cancer

Abstract

Background: Dysregulated Wnt/β-catenin signaling has been linked to several cancers, including pancreatic cancer (PC) and colorectal cancer (CRC). WNT974 (formerly LGK974) - a first-in-class, selective, oral inhibitor of Porcupine (an O-acyltransferase required for Wnt activation and secretion) - has shown preclinical activity in tumor models with mutations upstream in the Wnt pathway. Furthermore, dysregulated Wnt signaling has been linked to T-cell exclusion in tumor tissue and resistance to immunotherapy, suggesting WNT974 may act synergistically with checkpoint inhibitors. Methods: This ongoing Phase I, open-label, dose-escalation and -expansion study (NCT01351103) is designed to determine the maximum tolerated dose and/or recommended dose for expansion, characterize the safety and tolerability, and assess preliminary antitumor activity, pharmacokinetic (PK), and pharmacodynamic properties of WNT974, alone or combined with PDR001 (spartalizumab, an anti-PD-1 antibody) in advanced/metastatic solid tumors. Here, we focus on preliminary biomarker analyses from the single-agent part of the study. The study initially enrolled pts with lobular breast cancer and melanoma and was later amended to enroll pts with triple negative breast cancer (TNBC), PC, and CRC, and those with tumors with genetic alterations upstream in the Wnt pathway. Pre and on-treatment skin and tumor tissue specimens were collected for RT-PCR analysis of AXIN2, a marker of Wnt pathway activity. NanoString gene expression was measured in a subset of pts using remnant RNA from the tumor samples, and chemokine and dendritic cell signatures were analyzed pre and on-treatment. Results: At the data cut-off date, March 2, 2017, 94 pts were enrolled. Median age was 58.5 years (range, 28-77), 43% were male, and the most common cancer types were PC (30%), melanoma (26%), and breast cancer (21%). Patients received single-agent WNT974 orally at doses of 5, 7.5, 10, 15, 20, 22.5, or 30 mg daily, 30 or 45 mg intermittently (4 days on, 3 days off), or 5 mg twice daily. Median duration of exposure was 4.9 weeks (range, 0.1-27.7). Safety, tolerability, and PK have previously been reported. AXIN2 expression in paired samples from skin and tumor showed evidence of Wnt pathway inhibition in all indications; this was not dose-dependent in the dose range studied. Immune signature analyses of a paired tumor sample subset (n=8) revealed an inverse association between change in AXIN2 expression and change in chemokine and activated dendritic cell signatures. Conclusions: Biomarker analyses show that WNT974 can potently inhibit Wnt pathway activity in skin and tumors. Immune signature data suggest that WNT974 treatment may promote T-cell recruitment into tumors, and support investigation of the combination of WNT974 with immunotherapy. The combination part of this study evaluating WNT974 combined with PDR001 (spartalizumab) is ongoing. Citation Format: Jordi Rodon, Guillem Argilés, Roisin M. Connolly, Ulka Vaishampayan, Maja de Jonge, Elena Garralda, Marios Giannakis, David C. Smith, Jason R. Dobson, Margaret McLaughlin, Abdelkader Seroutou, Yan Ji, Sinead Dolan, Jennifer Morawiak, Susan Moody, Filip Janku. Biomarker analyses from a phase I study of WNT974, a first-in-class Porcupine inhibitor, in patients (pts) with advanced solid tumors [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr CT175.

Published

2018

50. A phase I study of LXH254 in patients (pts) with advanced solid tumors harboring MAPK pathway alterations

Author

A. Mais, Filip Janku, Harry J.M. Groen, Heidi Nauwelaerts, Annie St-Pierre, Frederik Marmé, Noboru Yamamoto, Elena Elez, Maja J.A. de Jonge, Reinhard Dummer, Anna Spreafico, Maritza Melendez, Uz M. Stammberger, Gopa Iyer, Kathrin Gollmer, and Yung-Jue Bang

Subjects

0301 basic medicine, MAPK/ERK pathway, Cancer Research, endocrine system diseases, business.industry, digestive system diseases, Phase i study, enzymes and coenzymes (carbohydrates), 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Mediator, Oncology, 030220 oncology & carcinogenesis, Cancer research, Medicine, In patient, skin and connective tissue diseases, Protein kinase A, business, neoplasms

Abstract

2586Background: CRAF is a key mediator of oncogenic mitogen-activated protein kinase (MAPK) pathway reactivation following MEK or BRAF inhibition. LXH254 is a BRAF and CRAF inhibitor with antitumor...

Published

2018