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| ID | Type | Description | Link |
|---|---|---|---|
| 2018-000515-24 | EudraCT Number | ||
| 45535982 | Registry Identifier | ISRCTN |
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FaR-RMS is an over-arching study for children and adults with newly diagnosed and relapsed rhabdomyosarcoma (RMS)
FaR-RMS is an over-arching study for children and adults with newly diagnosed and relapsed rhabdomyosarcoma (RMS). It is a multi-arm, multi-stage format, involving several different trial questions. FaR-RMS is intended to be a rolling programme of research with new treatment arms being introduced dependant on emerging data and innovation. This study has multiple aims. It aims to evaluate the impact of new agent regimens in both newly diagnosed and relapsed RMS; whether changing the duration of maintenance therapy affects outcome; and whether changes to dose, extent (in metastatic disease) and timing of radiotherapy improve outcome and quality of life. In addition the study will evaluate risk stratification through the use of PAX-FOXO1 fusion gene status instead of histological subtyping and explore the use of FDG PET-CT response assessment as a prognostic biomarker for outcome following induction chemotherapy.
Newly diagnosed patients should, where possible, be entered into the FaR-RMS study at the time of first diagnosis prior to receiving any chemotherapy. However, patients can enter at the point of radiotherapy or maintenance, and those with relapsed disease can enter the study even if not previously entered at initial diagnosis. Patients may be entered into more than one randomisation/registration, dependant on patient risk group and disease status.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Phase 1b Dose finding: VHR induction - IRIVA | Experimental | Irinotecan: an i.v. infusion over 1 hour on days 8,9,10,11 and 12 . For the phase 1b registration, starting dose of 20 mg/m2. Ifosfamide: 3g/m2 as an i.v. infusion over 3 hours on days 1 and 2 Vincristine: 1.5 mg/m2 as an As per local practice: recommended as a short infusion (maximum dose 2mg). Administered days 1,8,15 on cycles 1-2 and on days 1 and 8 on cycles 3-9. Actinomycin: 1.5 mg/m2 as an i.v. bolus injection (maximum dose 2mg) on day 1. |
|
| CT1A: VHR induction - IVADO | Active Comparator | Ifosfamide: 3g/m2 as an i.v. infusion over 3 hours on days 1 and 2 Vincristine: 1.5 mg/m2 As per local practice: recommended as a short infusion (maximum dose 2mg). Administered days 1,8,15 on cycles 1-2 and on day 1 on cycles 3-9. Actinomycin: 1.5 mg/m2 as an i.v. bolus injection (maximum dose 2mg) on day 1. Doxorubicin: 30 mg/m2 as an i.v infusion over 1 hour on days 1 and 2 on cycles 1-4 |
|
| CT1A: VHR Induction IRIVA | Experimental | Irinotecan: an i.v. infusion over 1 hour on days 8,9,10,11 and 12 . Phase 2 recommended dose as determined by IRIVA dose finding arm Ifosfamide: 3g/m2 as an i.v. infusion over 3 hours on days 1 and 2 Vincristine: 1.5 mg/m2 As per local practice: recommended as a short infusion (maximum dose 2mg). Administered days 1,8,15 on cycles 1-2 and on days 1 and 8 on cycles 3-9. Actinomycin: 1.5 mg/m2 as an i.v. bolus injection (maximum dose 2mg) on day 1. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| Irinotecan | Drug | antineoplastic enzyme inhibitor |
|
| Measure | Description | Time Frame |
|---|---|---|
| Event Free Survival (RT2) | Failure events are:
| From randomisation to first failure event, timeframe 36 months |
| Event Free Survival (CT1A) | Failure events are:
| From randomisation to first failure event, timeframe 36 months |
| Event Free Survival (CT1B) | Failure events are:
| From randomisation to first failure event, timeframe 36 months |
| Event Free Survival (CT2A) | Failure events are:
| From randomisation to first failure event, timeframe 36 months |
| Event Free Survival (CT2B) | Failure events are:
| Time from randomisation to first failure event, timeframe 36 months |
| Event Free Survival (CT3) | To determine whether new systemic therapy regimens improve event free survival in relapsed RMS compared to standard therapy (VIRT) (CT3): Initial new systemic therapy combination to be tested: o Regorafenib (R) added to vincristine and irinotecan (VIR) (VIRR) |
| Measure | Description | Time Frame |
|---|---|---|
| Recommended Phase II Dose (Phase 1b) | Based on tolerability, where tolerability is evaluated through the occurrence of dose limiting toxicity (DLT). | From first patient first visit in dose finding study until appropriate dose level found, estimated 9 months |
| Maximum Tolerated Dose (Phase 1b) |
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Inclusion Criteria for study entry - Mandatory at first point of study entry
Phase 1b Dose Finding - IRIVA Inclusion
Entered in to the FaR-RMS study at diagnosis
Very High Risk disease
Age >12 months and ≤25 years
No prior treatment for RMS other than surgery
Medically fit to receive treatment
Adequate hepatic function:
Absolute neutrophil count ≥1.0x 109/L
Platelets ≥ 80 x 109/L
Adequate renal function: estimated or measured creatinine clearance ≥60 ml/min/1.73 m2
Documented negative pregnancy test for female patients of childbearing potential
Patient agrees to use contraception during therapy and for 12 months after last trial treatment (females) or 6 months after last trial treatment (males), where patient is sexually active
Written informed consent from the patient and/or the parent/legal guardian
Exclusion
Frontline chemotherapy randomisation Very High Risk - CT1a Inclusion
Entered in to the FaR-RMS study at diagnosis
Very High Risk disease
Age ≥ 6 months
Available for randomisation ≤60 days after diagnostic biopsy/surgery
No prior treatment for RMS other than surgery
Medically fit to receive treatment
Adequate hepatic function :
a. Total bilirubin ≤ 1.5 times upper limit of normal (ULN) for age, unless the patient is known to have Gilbert's syndrome
Absolute neutrophil count ≥1.0x 109/L (except in patients with documented bone marrow disease)
Platelets ≥ 80 x 109/L (except in patients with documented bone marrow disease)
Fractional Shortening ≥ 28%
Documented negative pregnancy test for female patients of childbearing potential
Patient agrees to use contraception during therapy and for 12 months after last trial treatment (females) or 6 months after last trial treatment (males), where patient is sexually active
Written informed consent from the patient and/or the parent/legal guardian
Exclusion
Frontline chemotherapy randomisation High Risk - CT1b Inclusion
Entered in to the FaR-RMS study at diagnosis
High Risk disease
Age ≥ 6 months
Available for randomisation ≤60 days after diagnostic biopsy/surgery
No prior treatment for RMS other than surgery
Medically fit to receive treatment
Adequate hepatic function :
a. Total bilirubin ≤ 1.5 times upper limit of normal (ULN) for age, except if the patient is known to have Gilbert's syndrome
Absolute neutrophil count ≥1.0x 109/L
Platelets ≥ 80 x 109/L
Documented negative pregnancy test for female patients of childbearing potential
Patient agrees to use contraception during therapy and for 12 months after last trial treatment (females) or 6 months after last trial treatment (males), where patient is sexually active
Written informed consent from the patient and/or the parent/legal guardian
Exclusion
Frontline Radiotherapy Note: eligible patients may enter multiple radiotherapy randomisations.
Radiotherapy Inclusion - for all radiotherapy randomisations
Radiotherapy Exclusion - for all radiotherapy randomisations
RT1a Specific Inclusion
RT1b Specific Inclusion
Primary tumour deemed resectable (predicted R0/R1 resection) after 3 cycles of induction chemotherapy (6 cycles for metastatic disease).
Adjuvant radiotherapy required in addition to surgical resection (local decision)
Higher Local Failure Risk (HLFR) based on presence of either of the following criteria:
Available for randomisation after cycle 3 and prior to the start of cycle 6 of induction chemotherapy for localised disease, or after cycle 6 and prior to the start of cycle 9 for metastatic disease
RT1c Specific Inclusion
Primary radiotherapy indicated (local decision)
Higher Local Failure Risk (HLFR) based on either of the following criteria:
Available for randomisation after cycle 3 and prior to the start of cycle 6 of induction chemotherapy for localised disease, or after cycle 6 and prior to the start of cycle 9 for metastatic disease
RT2
Available for randomisation after cycle 6 and before the start of cycle 9 of induction chemotherapy.
Unfavourable metastatic disease, defined as Modified Oberlin Prognostic Score 2-4
Modified Oberlin Prognostic Score (1 point for each adverse factor):
Unfavourable metastatic disease: 2- 4 adverse factors Favourable metastatic disease: 0-1 adverse factors
Maintenance chemotherapy (Very High Risk) - CT2a Inclusion Randomisation must take place during the 12th cycle of maintenance chemotherapy.
Entered in to the FaR-RMS study (at diagnosis or at any subsequent time point)
Very High Risk disease
Received frontline induction chemotherapy as part of the FaR-RMS trial or with a IVA/IVADo based chemotherapy regimen
a. Patients for whom ifosfamide has been replaced with cyclophosphamide will be eligible
Completed 11 cycles of VnC maintenance treatment (either oral or IV regimens)
No evidence of progressive disease
Absence of severe vincristine neuropathy - i.e requiring discontinuation of vincristine treatment)
Medically fit to continue to receive treatment
Patient agrees to use contraception during therapy and for 12 months after last trial treatment (females) or 6 months after last trial treatment (males), where patient is sexually active
Written informed consent from the patient and/or the parent/legal guardian
Exclusion
Maintenance chemotherapy (High Risk) - CT2b Randomisation must take place during the 6th cycle of maintenance chemotherapy. Inclusion
Exclusion
CT3 Relapsed Chemotherapy
Inclusion:
Exclusion:
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| Name | Role | Phone | Extension | |
|---|---|---|---|---|
| Bridget Shaw | Contact | 0121 414 2996 | farrms@trials.bham.ac.uk | |
| Emma Gray | Contact | 0121 414 3799 | farrms@trials.bham.ac.uk |
| Name | Affiliation | Role |
|---|---|---|
| Meriel Jenney | Chief Investigator | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Queensland Children's Hospital | Recruiting | Brisbane | 4101 | Australia |
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| CT1B: HR Induction IVA | Active Comparator | Ifosfamide: 3g/m2 as an i.v. infusion over 3 hours on days 1 and 2 Vincristine: 1.5 mg/m2 As per local practice: recommended as a short infusion (maximum dose 2mg). Administered days 1,8,15 on cycles 1-2 and on day 1 on cycles 3-9. Actinomycin: 1.5 mg/m2 as an i.v. bolus injection (maximum dose 2mg) on day 1. |
|
| CT1B: HR Induction IRIVA | Experimental | Irinotecan: an i.v. infusion over 1 hour on days 8,9,10,11 and 12 . Phase 2 recommended dose as determined by IRIVA dose finding arm Ifosfamide: 3g/m2 as an i.v. infusion over 3 hours on days 1 and 2 Vincristine: 1.5 mg/m2 As per local practice: recommended as a short infusion (maximum dose 2mg). Administered days 1,8,15 on cycles 1-2 and on days 1 and 8 on cycles 3-9. Actinomycin: 1.5 mg/m2 as an i.v. bolus injection (maximum dose 2mg) on day 1. |
|
| RT1A: Preoperative Radiotherapy | Experimental | To be given either 41.4 Gy or 50.4 Gy prior to surgery |
|
| RT1A: Post operative radiotherapy | Active Comparator | To be given either 41.4 Gy or 50.4 Gy following surgery |
|
| RT1B: Radiotherapy for resectable disease: dose escalated | Experimental | To receive 50.4 Gy |
|
| RT1B: Radiotherapy for resectable disease: standard dose | Active Comparator | To receive 41.4 Gy |
|
| RT1C: Radiotherapy for unresectable disease: dose escalated | Experimental | To receive 59.4 Gy |
|
| RT1C: Radiotherapy for unresectable disease: standard dose | Active Comparator | To receive 50.4 Gy |
|
| RT2: Radiotherapy to primary tumour and involved lymph nodes | Experimental | Radiotherapy to the primary tumour and involved regional lymph nodes only |
|
| RT2: Radiotherapy to all metastatic sites | Experimental | Radiotherapy given to all metastatic sites |
|
| CT2A: VHR Maintenance - VC | Experimental | Vinorelbine: 25 mg/m2 i.v. or 60 mg/m2 orally on days 1,8 and 15 Cyclophosphamide 25 mg/m2 orally daily for 28 days |
|
| CT2A: Maintenance -Stop treatment | No Intervention | To stop treatment at the point of randomisation |
| CT2B: HR Maintenance - VC | Experimental | Vinorelbine: 25 mg/m2 i.v. on days 1,8 and 15 Cyclophosphamide 25 mg/m2 orally daily for 28 days |
|
| CT2B: HR Maintenance - Stop Treatment | No Intervention | To stop treatment at the point of randomisation |
| CT3: Relpased Chemotherapy - VIRT | Active Comparator | Vincristine: 1.5 mg/m2 As per local practice: recommended as a short infusion (maximum dose 2mg) on days 1 and 8 Irinotecan: 50 mg/m2 as an i.v. infusion over 1 hour on days 1-5 Temozolomide: 125 mg/m2 (Escalate to 150mg/m2/day in Cycle 2 if no toxicity > grade 3) as an oral tablets prior to vincristine and irinotecan on days 1-5 |
|
| CT3: Relapsed Chemotherapy - VIRR | Experimental | Vincristine: 1.5 mg/m2 As per local practice: recommended as a short infusion (maximum dose 2mg) on days 1 and 8 Irinotecan: 50 mg/m2 as an i.v. infusion over 1 hour on days 1-5 Regorafenib: Children between 6 and 24 months = 65 mg/m2, children less than 12 and/or less than 40kg dose = 82 mg/m2 Maximum 120 mg, Fixed dose of 120 mg for patients over 12 years of age AND ≥ 40 kg, as an oral tablets on days 8 to 21. |
|
| Actinomycin D | Drug | Antineoplastic agent that is a polypeptide antibiotic |
|
|
| Doxorubicin | Drug | An anthracycline topoisomerase inhibitor isolated from streptpmyces peucetius var. casesius |
|
| Ifosfamide | Drug | chemotherapeutic agent chemically related to the nitrogen mustards and is a synthetic analog of cyclophosphamide |
|
| Vincristine | Drug | anti neoplastic vinca alkaloid agent |
|
| Vinorelbine | Drug | vinca alkaloid with a role as an antineoplastic agent |
|
| Cyclophosphamide | Drug | Precursor of an alkylating nitrogen mustard antineoplastic and immunosuppressive agent |
|
| Temozolomide | Drug | oral antineoplastic alkylating agent |
|
| radiotherapy | Radiation | Ionising radiation |
|
| Regorafenib | Drug | Oral multi-kinase inhibitor that targets a broad range of angiogenic, stromal and oncogenic kinases, including vascular endothelial growth factor receptors (VEFGR) 1, 2 and 3, tyrosine kinase with immunoglobulin and epidermal growth factor homology domain 2 (TIE2), platelet-derived growth factor receptor (PDGFR), fibroblast growth factor receptors (FGFR), c-KIT, RET, RAF-1 and BRAF (wild-type and V600E mutant). |
|
| Patients will be followed up for a minimum of 6 years from trial entry (or 5 years from end of relapsed trial treatment, whichever comes later). Patients will be followed up for progression and death until the end of trial definition has been met. |
| Local Failure Free Survival (RT1A and RT1B) | A local failure event is relapse or progression of tumour at the primary site at any time even if there has been a prior /concurrent, regional or distant failure | Time from randomisation to first local failure event, timeframe 36 months |
| Local Failure Free Survival (RT1C) | A local failure event is relapse or progression of tumour at the primary site at any time even if there has been a prior /concurrent, regional or distant failure | Time from randomisation to first local failure event, timeframe 36 months |
Dose level at which no or one participant experiences a DLT when at least two of three to six participants experience a DLT at the next highest dose. |
| From first patient first visit in dose finding study until appropriate dose level |
| Toxicity (All chemotherapy randomisations) | Categorised and graded using Common Terminology Criteria for Adverse Events | From date of protocol defined treatment until 30 days after the administration of the last treatment |
| Dose Limiting Toxicity (Phase 1b) | Diarrhoea: Grade 3 for >3 days despite loperamide therapy Diarrhoea: Grade 4 despite loperamide therapy. Enterocolitis: Grade 3 or above Ileus: Grade 3 or above for more than 3 days Oral mucositis: Grade 3 above for >3 days despite optimal supportive care Persistent neutropenia or thrombocytopenia leading to delay of start of next course by >7 days; i.e. starting > day 28 Any grade 3 or 4 toxicity resulting in discontinuation of the new combination Any grade 5 toxicity | From commencement of treatment until 21 days after the start of cycle 2 (each cycle is 21 days) |
| Response (Phase 1b, CT1A, CT1B) | defined as complete (CR) or partial response (PR) and is clinically defined. Patients who are not assessable for response - e.g. because of early stopping of treatment or death - will be assumed to be non-responders. | Response assessed after course 3 (63 days) and 6 (126 days) |
| Tolerability (CT3) | To determine the tolerability of the regimens. | From registration/randomisation until death/study endpoint |
| Overall Survival (CT1A) | Death from any cause | From randomisation to death from any cause, assessed for 36 months |
| Overall Survival (CT1B) | Death from any cause | From randomisation to death from any cause, assessed for 36 months |
| Overall Survival (CT2A) | Death from any cause | From randomisation to death from any cause, assessed for 36 months |
| Overall Survival (CT2B) | Death from any cause | From randomisation to death from any cause, assessed for 36 months |
| Overall Survival (RT1A and RT1B) | Death from any cause | From randomisation to death from any cause, assessed for 36 months |
| Overall Survival (RT1C) | Death from any cause | From RT1C randomisation to death from any cause, assessed for 36 months |
| Overall Survival (RT2) | Death from any cause | From RT2 randomisation to death from any cause, as assessed for 36 months |
| Overall Survival (CT3) | To evaluate the anti-tumour activity and effect on overall survival of VIRR when compared to standard therapy | Patients will be followed up for a minimum of 6 years from trial entry (or 5 years from end of relapsed trial treatment, whichever comes later). Patients will be followed up for progression and death until the end of trial definition has been met. |
| Overall Survival (all patients) | Death from any cause | From randomisation/registration to death from any cause, assessed for 36 months |
| Acute wound complications and post-operative complications (RT1A and RT1B) | specific grade 3 and above complications according to CTCAE v 4 and Clavien Dindo scale. Specific wound complications within the same time frame will also be collected | Within 120 days from surgery |
| Acute post-radiotherapy complications (All radiotherapy randomisations) | any grade 3 and above event according to CTCAE v 4 | Within 120 days from start of radiotherapy |
| Late complications (RT1A, RT1B. RT1C) | specific grade 3 and above events according to CTCAE and Clavien-Dindo scale | After 120 days from last local therapy |
| Loco-regional failure-free survival (All radiotherapy randomisations) | A local failure event is relapse or progression of tumour at the primary site at any time even if there has been a prior concurrent local, regional or distant failure. A regional event is relapse or progression of tumour at regional lymph nodes at any time even if there has been a prior distant failure. | From randomisation to first local and/or regional failure event, assessed for 36 months |
| Health related quality of life (RT1A and RT2) self-reported questionnaire completed by patient | will be assessed using Pediatric quality of life questionnaire (PedsQL) for the paediatric population (under 18 years). The minimum score is 0 where quality of life is completely unaffected by the intervention to 4 where quality of life is severely affected. | 4 timepoints: 1) 1 day of start of radiotherapy, 2) at completion of radiotherapy, average 5 weeks after start of radiotherapy, 3) 3 months and 4) 24 months following radiotherapy |
| Health related quality of life (RT1A and RT2) self-reported questionnaire completed by the patient | will be assessed using European Organisation for Research and Treatment of Cancer, Quality of Life Questionnaire 30 (EORTC QLQ-C30) for patients 18 years of age and over. The minimum score is 0 where quality of life is completely unaffected by the intervention to 4 where quality of life is severely affected. | 4 timepoints: 1) 1 day of start of radiotherapy, 2) at completion of radiotherapy, average 5 weeks after start of radiotherapy, 3) 3 months and 4) 24 months following radiotherapy |
| Health related quality of life (CT3) self-reported questionnaire completed by the patient | will be assessed using Pediatric quality of life questionnaire (PedsQL) for the paediatric population (under 18 years). The minimum score is 0 where quality of life is completely unaffected by the intervention to 4 where quality of life is severely affected. | 3 timepoints: Each Cycle is 28 days. Timepoint 1: Day 0 of cycle 1 (prior to starting treatment), Timepoint 2 day 0 cycle 3, Timepoint 3) day 0 cycle 5 |
| Health related quality of life (CT3) self-reported questionnaire completed by the patient | will be assessed using European Organisation for Research and Treatment of Cancer, Quality of Life Questionnaire 30 (EORTC QLQ-C30) for patients 18 years of age and over. The minimum score is 0 where quality of life is completely unaffected by the intervention to 4 where quality of life is severely affected. | 3 timepoints: Each Cycle is 28 days. Timepoint 1: Day 0 of cycle 1 (prior to starting treatment), Timepoint 2 day 0 cycle 3, Timepoint 3) day 0 cycle 5 |
| Acceptability and Palatability of Regorafenib (CT3) | "Acceptability and Palatability Questionnaire" To evaluate the acceptability and palatability of regorafenib formulations | 1 timepoint: Day 8 of cycle 1 (Each Cycle is 28 days) |
| PET Response (if participating in PET Sub-study) | assessed by PERCIST criteria and visual 'Deauville like' criteria | After three cycles of chemotherapy (each cycle is 21 days) |
| Event Free Survival (all patients) | Failure events are:
| From date of randomisation/registration to death from any cause, assessed for 36 months |
| Event Free Survival (if participating in PET Sub-study) | Failure events are:
| From date of randomisation/registration to death from any cause, assessed for 36 months |
| Local Failure Free Survival (if participating in PET Sub-study) | A local failure event is relapse or progression of tumour at the primary site at any time even if there has been a prior /concurrent, regional or distant failure | From date of randomisation/registration to first local failure event, assessed for 36 months |
| Chris O'brien Lifehouse | Recruiting | Camperdown | Australia |
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| Monash Children's Hospital | Recruiting | Clayton | Australia |
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| Peter Maccallum Cancer Centre | Recruiting | Melbourne | Australia |
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| Royal Childrens Hospital Melbourne | Recruiting | Melbourne | Australia |
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| John Hunter Children's Hospital | Recruiting | New Lambton Heights | 2310 | Australia |
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| Perth Children's Hospital | Recruiting | Perth | Australia |
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| Sydney Children's Hospital | Recruiting | Sydney | Australia |
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| The Childrens Hospital At Westmead | Recruiting | Sydney | Australia |
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| Westmead Hospital | Recruiting | Westmead | Australia |
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| Princess Alexandra Hospital | Recruiting | Woolloongabba | Australia |
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| Kepler University Clinic Linz | Recruiting | Linz | Austria |
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| St Anna Childrens Hospital | Recruiting | Vienna | Austria |
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| Cliniques Universitaires Saint Luc | Recruiting | Brussels | Belgium |
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| Hopital Universitaire Des Enfants Reine Fabiola | Recruiting | Brussels | Belgium |
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| Universitair Ziekenhuis Gent | Recruiting | Ghent | Belgium |
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| Uz Leuven Campus Gasthuisberg | Recruiting | Leuven | Belgium |
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| Centre Hospitalier Regional De La Citadelle | Recruiting | Liège | Belgium |
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| Clinique Chc Montlegia | Recruiting | Liège | Belgium |
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| Masaryk University Hospital Brno | Recruiting | Brno | 625 00 | Czechia |
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| Aarhus University Hospital | Recruiting | Aarhus | Denmark |
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| University Hospital Rigshospitalet | Recruiting | Copenhagen | Denmark |
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| Centre Hospitalier Universitaire D'angers | Recruiting | Angers | France |
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| Centre Hospitalier Regional Universitaire Besancon - Hopital Jean Minjoz | Recruiting | Besançon | France |
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| Centre Hospitalier Universitaire De Bordeaux - Hopital Pellegrin | Recruiting | Bordeaux | France |
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| Centre Hospitalier Regional Universitaire Brest - Hopital Morvan | Recruiting | Brest | France |
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| Centre Francois Baclesse | Recruiting | Caen | France |
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| Centre Hospitalier Universitaire De Caen | Recruiting | Caen | France |
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| Centre Hospitalier Universitaire Dijon Bourgogne - Hopital D'enfants | Recruiting | Dijon | France |
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| Centre Hospitalier Universitaire De Grenoble | Recruiting | Grenoble | France |
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| Centre Hospitalier Universitaire La Reunion | Recruiting | La Réunion | France |
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| Centre Oscar Lambret | Recruiting | Lille | France |
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| Centre Leon Berard | Recruiting | Lyon | France |
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| Hopital De La Timone (ap-hm) | Recruiting | Marseille | France |
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| Centre Hospitalier Universitaire De Nancy | Recruiting | Nancy | France |
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| Centre Hospitalier Universitaire De Nantes | Recruiting | Nantes | France |
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| Hopital Armand Trousseau | Recruiting | Paris | France |
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| Institut Curie | Recruiting | Paris | France |
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| Centre Hospitalier Universitaire Haut Levque | Recruiting | Pessac | France |
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| Centre Hospitalier Universitaire De Poitiers | Recruiting | Poitiers | France |
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| Chu De Reims | Recruiting | Reims | France |
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| Centre Eugne Marquis De Rennes | Recruiting | Rennes | France |
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| Centre Hospitalier Universitaire De Rennes - Hopital Pontchaillou | Recruiting | Rennes | France |
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| Centre Hospitalier Universitaire De Rouen | Recruiting | Rouen | France |
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| Centre Hospitalier Universitaire Saint-etienne | Recruiting | Saint-Etienne | France |
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| Strasbourg Hautepierre | Recruiting | Strasbourg | France |
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| Centre Hospitalier Universitaire De Toulouse - Hopital Des Enfants | Recruiting | Toulouse | France |
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| Centre Hospitalier Regional Universitaire De Tours - Hopital Clocheville | Recruiting | Tours | France |
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| Gustave Roussy | Recruiting | Villejuif | 94805 | France |
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| Children's General Hospital P and A Kyriakou | Recruiting | Athens | 115 27 | Greece |
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| Department of Pediatric Hematology-oncology - Aghia Sophia Children's Hospital | Recruiting | Athens | Greece |
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| Hellenic Society of Pediatric Hematology- Oncology | Recruiting | Athens | Greece |
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| University Unit of Pediatric Oncology-hematology - Children's Hospital Agia Sophia | Recruiting | Athens | Greece |
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| Children's and Adolescent's Oncology Clinic, "MITERA" Children's Hospital | Recruiting | Attiki | 151 23 | Greece |
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| Hematology-oncology Children's Clinic, University General Hospital of Heraklion | Recruiting | Heraklion | 715 00 | Greece |
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| Ahepa University General Hospital of Thessaloniki | Recruiting | Thessaloniki | Greece |
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| Ippokratio General Hospital of Thessaloniki | Recruiting | Thessaloniki | Greece |
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| Our Lady's Children's Hospital | Not yet recruiting | Crumlin | Ireland |
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| Rambam Health Care Campus | Recruiting | Haifa | Israel |
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| Hadassah University Medical Centre | Recruiting | Jerusalem | Israel |
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| Schneider Medical Centre | Recruiting | Petah Tikva | Israel |
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| Dana Children's Hospital, Tel Aviv Sourasky Medical Center | Recruiting | Tel Aviv | Israel |
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| Chaim Sheba Medical Centre | Recruiting | Tel Litwinsky | Israel |
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| University Hospital of Padova (azienda Ospedaliera of Padua) | Not yet recruiting | Padova | Italy |
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| University Medical Centre Groningen | Recruiting | Groningen | Netherlands |
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| Prinses Maxima Centrum Voor Kinderoncologie | Recruiting | Utrecht | Netherlands |
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| Starship Children's Health | Recruiting | Auckland | New Zealand |
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| Christchurch Hospital | Recruiting | Christchurch | New Zealand |
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| Haukeland University Hospital - Paediatric | Recruiting | Bergen | Norway |
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| Oslo University Hospital - Paediatrics | Recruiting | Oslo | Norway |
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| Oslo University Hospital - Radiumhospitalet | Recruiting | Oslo | Norway |
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| University Hospital of North Norway - Paediatric | Recruiting | Tromsø | Norway |
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| St Olavs Hospital - Paediatric | Recruiting | Trondheim | Norway |
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| Instituto Portugues De Oncologia De Losbona Francisco Gentil, Epe | Not yet recruiting | Lisbon | Portugal |
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| Bratislava, National Institute for Children's Diseases | Not yet recruiting | Bratislava | Slovakia |
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| University Childrens Hospital Ljubljana | Recruiting | Ljubljana | Slovenia |
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| University Medical Centre Ljubjlana | Recruiting | Ljubljana | Slovenia |
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| Hospital Sant Joan De Deu | Recruiting | Barcelona | Spain |
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| Hospital Universitari Vall D'hebron | Recruiting | Barcelona | Spain |
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| Hospital De Cruces | Recruiting | Bilbao | 48903 | Spain |
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| Hospital Del Nino Jesus | Recruiting | Madrid | 28009 | Spain |
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| Hospital Universitario Gregorio Maranon | Recruiting | Madrid | 28009 | Spain |
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| Hospital Universitario La Paz | Recruiting | Madrid | Spain |
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| Hospital Regional Universitario De Malaga | Recruiting | Málaga | Spain |
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| Hospital Virgen Del Rocio | Recruiting | Seville | Spain |
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| Hospital Politecnico U La Fe | Recruiting | Valencia | 46026 | Spain |
|
| Hospital Universitario Miguel Servet Materno - infantil | Recruiting | Zaragoza | Spain |
|
| Uppsala University Childrens Hospital | Recruiting | Uppsala | Sweden |
|
| Kantonsspital Aarau | Recruiting | Aarau | Switzerland |
|
| Universitats-kinderspital Bieder Basel (UKBB) | Recruiting | Basel | Switzerland |
|
| Ospedale San Giovanni | Recruiting | Bellinzona | Switzerland |
|
| Inselspital Bern | Recruiting | Bern | Switzerland |
|
| Hug Hopitaux Universitaires De Geneve | Recruiting | Geneva | Switzerland |
|
| Centre Hospitalier Universitaire Vaudois (CHUV), Lausanne | Recruiting | Lausanne | Switzerland |
|
| Luzerner Kantonspital - Kinderspital Luzern | Recruiting | Lucerne | Switzerland |
|
| Ostschweizer Kinderspital | Recruiting | Sankt Gallen | Switzerland |
|
| Universitaetsspital Zurich | Recruiting | Zurich | Switzerland |
|
| Royal Marsden Hospital | Recruiting | Sutton | Surrey | SM2 5PT | United Kingdom |
|
| Royal Aberdeen Children's Hospital | Recruiting | Aberdeen | United Kingdom |
|
| Belfast City Hospital | Not yet recruiting | Belfast | United Kingdom |
|
| Royal Belfast Hospital for Sick Children | Not yet recruiting | Belfast | United Kingdom |
|
| Birmingham Children's Hospital | Recruiting | Birmingham | United Kingdom |
|
| The Queen Elizabeth Hospital | Not yet recruiting | Birmingham | United Kingdom |
|
| Bristol Haematology And Oncology Centre | Recruiting | Bristol | United Kingdom |
|
| Bristol Royal Hospital for Children | Recruiting | Bristol | United Kingdom |
|
| Addenbrooke's Hospital | Recruiting | Cambridge | United Kingdom |
|
| Noah's Ark Children's Hospital for Wales | Recruiting | Cardiff | United Kingdom |
|
| Velindre Hospital | Recruiting | Cardiff | United Kingdom |
|
| Royal Hospital for Children and Young People | Recruiting | Edinburgh | United Kingdom |
|
| Beatson West of Scotland Cancer Centre | Recruiting | Glasgow | United Kingdom |
|
| Royal Hospital for Children Glasgow | Recruiting | Glasgow | United Kingdom |
|
| Leeds General Infirmary | Recruiting | Leeds | United Kingdom |
|
| St James's University Hospital | Recruiting | Leeds | United Kingdom |
|
| Leicester Royal Infirmary | Recruiting | Leicester | United Kingdom |
|
| Alder Hey Children's Hospital | Recruiting | Liverpool | United Kingdom |
|
| Great Ormond Street Hospital for Children | Recruiting | London | United Kingdom |
|
| Royal Marsden Hospital London | Recruiting | London | United Kingdom |
|
| University College London Hospital | Recruiting | London | United Kingdom |
|
| Royal Manchester Children's Hospital | Recruiting | Manchester | M13 9WL | United Kingdom |
|
| Christie Hospital | Recruiting | Manchester | United Kingdom |
|
| Clatterbridge Cancer Centre | Recruiting | Metropolitan Borough of Wirral | United Kingdom |
|
| Royal Victoria Infirmary | Recruiting | Newcastle upon Tyne | United Kingdom |
|
| Nottingham City Hospital | Recruiting | Nottingham | United Kingdom |
|
| Queen's Medical Centre, Nottingham | Recruiting | Nottingham | United Kingdom |
|
| John Radcliffe Hospital | Recruiting | Oxford | United Kingdom |
|
| Sheffield Children's Hospital | Recruiting | Sheffield | United Kingdom |
|
| Weston Park Hospital | Not yet recruiting | Sheffield | United Kingdom |
|
| Southampton General Hospital | Recruiting | Southampton | United Kingdom |
|
| ID | Term |
|---|---|
| D012208 | Rhabdomyosarcoma |
| ID | Term |
|---|---|
| D009217 | Myosarcoma |
| D009379 | Neoplasms, Muscle Tissue |
| D018204 | Neoplasms, Connective and Soft Tissue |
| D009370 | Neoplasms by Histologic Type |
| D009369 | Neoplasms |
| D012509 | Sarcoma |
Not provided
Not provided
| ID | Term |
|---|---|
| D000077146 | Irinotecan |
| D003609 | Dactinomycin |
| D004317 | Doxorubicin |
| D007069 | Ifosfamide |
| D014750 | Vincristine |
| D000077235 | Vinorelbine |
| D003520 | Cyclophosphamide |
| D000077204 | Temozolomide |
| D011878 | Radiotherapy |
| C559147 | regorafenib |
| ID | Term |
|---|---|
| D002166 | Camptothecin |
| D000470 | Alkaloids |
| D006571 | Heterocyclic Compounds |
| D006575 | Heterocyclic Compounds, 3-Ring |
| D000072471 | Heterocyclic Compounds, Fused-Ring |
| D010456 | Peptides, Cyclic |
| D047028 | Macrocyclic Compounds |
| D011083 | Polycyclic Compounds |
| D010455 | Peptides |
| D000602 | Amino Acids, Peptides, and Proteins |
| D003630 | Daunorubicin |
| D018943 | Anthracyclines |
| D009279 | Naphthacenes |
| D011084 | Polycyclic Aromatic Hydrocarbons |
| D006841 | Hydrocarbons, Aromatic |
| D006844 | Hydrocarbons, Cyclic |
| D006838 | Hydrocarbons |
| D009930 | Organic Chemicals |
| D000617 | Aminoglycosides |
| D006027 | Glycosides |
| D002241 | Carbohydrates |
| D010752 | Phosphoramide Mustards |
| D009588 | Nitrogen Mustard Compounds |
| D009150 | Mustard Compounds |
| D006846 | Hydrocarbons, Halogenated |
| D063088 | Phosphoramides |
| D009943 | Organophosphorus Compounds |
| D010078 | Oxazines |
| D006573 | Heterocyclic Compounds, 1-Ring |
| D014748 | Vinca Alkaloids |
| D046948 | Secologanin Tryptamine Alkaloids |
| D026121 | Indole Alkaloids |
| D007211 | Indoles |
| D006574 | Heterocyclic Compounds, 2-Ring |
| D054836 | Indolizidines |
| D007212 | Indolizines |
| D003606 | Dacarbazine |
| D014226 | Triazenes |
| D007093 | Imidazoles |
| D001393 | Azoles |
| D013812 | Therapeutics |
Not provided
Not provided