High Grade Glioma Clinical Trial
Official title:
A Phase II Open-Label, Randomized, Multi-Centre Comparative Study Of Bevacizumab-Based Therapy In Paediatric Patients With Newly Diagnosed Supratentorial, Infratentorial Cerebellar, or Peduncular High-Grade Glioma
| Verified date | July 2020 |
| Source | Hoffmann-La Roche |
| Contact | n/a |
| Is FDA regulated | No |
| Health authority | |
| Study type | Interventional |
This randomized, open-label, multicenter, 2-arm study will investigate the efficacy, safety,
tolerability and pharmacokinetics of bevacizumab when added to postoperative radiotherapy
with concomitant and adjuvant TMZ as compared to postoperative radiotherapy with concomitant
and adjuvant TMZ alone in paediatric participants with newly diagnosed histologically
confirmed World Health Organization (WHO) Grade III or IV localized supratentorial or
infratentorial cerebellar or peduncular high grade glioma (HGG). Participants will be
randomly assigned to one of two treatment arms.
Upon approval by the Health Authorities/Ethics Committees in the participating countries, an
additional young participant cohort (YPC) (children >/= 6 months and < 3 years of age with
progressive or relapsed metastatic or localized, supra- or infratentorial, non-brain stem WHO
Grade III or IV HGG) was included in the study. Children in the YPC will receive bevacizumab
and TMZ without radiation therapy. The anticipated time on study treatment is over 1 year.
| Status | Completed |
| Enrollment | 124 |
| Est. completion date | January 29, 2020 |
| Est. primary completion date | February 5, 2016 |
| Accepts healthy volunteers | No |
| Gender | All |
| Age group | 6 Months to 18 Years |
| Eligibility |
Inclusion Criteria - Main cohort : - Paediatric participants, aged >= 3 years and < 18 years - Written informed consent obtained from the participant/parents or legally acceptable representative - Newly diagnosed localised, supratentorial or infratentorial cerebellar or peduncular, WHO Grade III or IV gliomas - Local histological diagnosis confirmed by a designated central reference neuropathologist - Availability of the baseline magnetic resonance imaging (MRI) performed according to imaging guidelines - Able to commence trial treatment not before 4 weeks after cranial surgery and no later than 6 weeks following the last major surgery - Adequate bone marrow, coagulation, liver, and renal function Young Participant Cohort - Written informed consent obtained from parents or legal representative - Age at enrollment: from >= 6 months to < 3 years of age - Progressive or relapsed metastatic or localised, supra- or infratentorial, non-brain stem WHO Grade III or IV glioma (local pathology confirmation made either at initial diagnosis or at relapse) - Availability of a baseline MRI performed according to imaging guidelines - Adequate organ function (bone marrow, coagulation, liver, kidney) Exclusion Criteria - Main cohort: - Metastatic HGG defined as evidence of neuraxis dissemination by MRI or positive cerebrospinal fluid (CSF) cytology - WHO-defined Gliomatosis cerebri (multifocal HGG) - Any disease or condition that contraindicates the use of the study medication/treatment or places the patient at an unacceptable risk of experiencing treatment-related complications - Radiological evidence of surgically related intracranial bleeding - Prior diagnosis of a malignancy and disease-free for 5 years - Prior systemic anti-cancer therapy - Previous cranial irradiation Young Participant Cohort - WHO-defined Gliomatosis cerebri (multifocal HGG) - Newly diagnosed HGG below the age of 3 years - Relapsed HGG below the age of 6 months or above the age of 3 years regardless of the age at first onset - Indication for concomitant cranial irradiation, regardless of age - Any disease or condition that contraindicates the use of the study medication/treatment or places the child at an unacceptable risk of experiencing treatment-related complications - Any specific contraindication to MRI |
| Country | Name | City | State |
|---|---|---|---|
| Australia | Lady Cilento Children's Hospital; Oncology Services Group, Level 12b | South Brisbane | Queensland |
| Australia | The Children's Hospital at Westmead | Westmead | New South Wales |
| Austria | Kepler Universitätskliniken GmbH - Med Campus IV. | Linz | |
| Austria | Medizinische Universität Wien | Wien | |
| Belgium | UZ Leuven Gasthuisberg | Leuven | |
| Canada | Alberta Children'S Hospital | Calgary | Alberta |
| Canada | Hospital For Sick Children | Toronto | Ontario |
| Czechia | Fakultni nemocnice Brno; 2. detska klinika, pracoviste Detska nemocnice | Brno | |
| Czechia | Fakultni Nemocnice V Motole, S.P. | Prague | |
| Denmark | Skejby Sygehus - Aarhus University Hospital; CF Center, Børneafdeling A | Aarhus N | |
| Denmark | Rigshospitalet; Onkologisk Klinik | København Ø | |
| France | Centre Hospitalier d'Angers; Service de cancérologie pédiatrique | Angers | |
| France | CHU ESTAING; Centre Regional de Cancérologie et Thérapie Cellulaire Pédiatrique (CRCTCP) | Clermont Ferrand | |
| France | Centre Oscar Lambret; Service de Pediatrie | Lille | |
| France | Centre Leon Berard | Lyon | |
| France | Hopital Timone Enfants; Onco Pediatrie | Marseille | |
| France | Hopital Lenval; Service Hématologie Infantile | Nice | |
| France | Institut Curie - Centre de Lutte Contre le Cancer (CLCC) de Paris; Service d Oncologie Pediatrique | Paris | |
| France | CHRU de Rennes - Hôpital Sud- Service d'Hématologie Pédiatrique | Rennes | |
| France | Hopital Nord;Consult Pediatrie | St Priest En Jarez | |
| France | Hôpital Hautepierre | Strasbourg | |
| France | Hopital Des Enfants; Service d Hemato-Oncologie | Toulouse | |
| France | CHRU de Tours - Centre de Pédiatrie Clocheville; Service d'Oncopédiatrie | Tours | |
| France | Hopital Brabois Enfants | Vandoeuvre-les-Nancy cedex | |
| France | Institut Gustave Roussy; Service Pediatrique | Villejuif | |
| Hungary | Semmelweis University, 2nd Dept of Pediatrics Neurooncology Unit | Budapest | |
| Italy | Azienda Ospedaliera Universitaria Policlinico Sant'Orsola Malpigh | Bologna | Emilia-Romagna |
| Italy | Istituto Giannina Gaslini-Ospedale Pediatrico IRCCS; U.O.S. Neuroncologia | Genova | Liguria |
| Italy | Fondazione IRCCS Istituto Nazionale dei Tumori | Milano | Lombardia |
| Italy | Azienda Ospedaliera di Padova | Padova | Veneto |
| Netherlands | UMC St Radboud | Nijmegen | |
| Netherlands | Erasmus Mc/Sophia's Childrens Hospital; Dept. of Pediatric Oncology | Rotterdam | |
| Poland | Instytut Pomnik-Centrum Zdrowia Dziecka; Klinika Onkologii | Warsaw | |
| Spain | Hospital Universitari Vall d'Hebron | Barcelona | |
| Spain | Hospital Sant Joan De Deu | Esplugues De Llobregas | Barcelona |
| Spain | Hospital Universitario La Fe | Valencia | |
| Sweden | Sahlgrenska Universitetssjukhuset, Östra Sjukhus; Drottning Silvias Barnsjukhus | Göteborg | |
| Sweden | Universitetssjukhuset Linköping; Barn och Ungdomskliniken | Linkoeping | |
| Sweden | Skånes Universitetssjukhus | Lund | |
| Sweden | Karolinska Universitetssjukhuset, Solna; Astrid Lindgrens Barnsjukhus, Barcanceravdelningen | Solna | |
| United Kingdom | Birmingham Childrens Hospital; Oncology Dept | Birmingham | |
| United Kingdom | Bristol Royal Hospital for Children; Paediatric Haematology, Oncology, BMT | Bristol | |
| United Kingdom | Addenbrookes Hospital; Paediatric Oncology Ward C2 | Cambridge | |
| United Kingdom | Royal Hospital for Sick Children | Edinburgh | |
| United Kingdom | Leeds General Infirmary; Ward 35 | Leeds | |
| United Kingdom | Alder Hey Children's NHS Foundation Trust | Liverpool | |
| United Kingdom | Great Ormond Street Hospital; Dept. Of Pediatric Oncology | London | |
| United Kingdom | University College London NHS Foundation Trust | London | |
| United Kingdom | Royal Manchester Childrens Hospital | Manchester | |
| United Kingdom | Newcastle University & The Newcastle upon Tyne Hospitals NHS Foundation Trust | Newcastle upon Tyne | |
| United Kingdom | Queens Medical Centre | Nottingham | |
| United Kingdom | Southampton General Hospital | Southampton | |
| United Kingdom | Royal Marsden Hospital; Pediatric Unit | Surrey |
| Lead Sponsor | Collaborator |
|---|---|
| Hoffmann-La Roche |
Australia, Austria, Belgium, Canada, Czechia, Denmark, France, Hungary, Italy, Netherlands, Poland, Spain, Sweden, United Kingdom,
| Type | Measure | Description | Time frame | Safety issue |
|---|---|---|---|---|
| Primary | Event-Free Survival (EFS) as Assessed by the Central Radiology Review Committee (CRRC) | EFS was defined as the time from randomisation to the earliest occurrence of any of the following: tumor progression, tumor recurrence, second primary non- HGG malignancy or death attributable to any cause. Tumor assessments were conducted using magnetic resonance imaging (MRI) and reviewed by the site-independent CRRC using Response Assessment in Neuro-Oncology (RANO) criteria. Tumor progression was defined as clear clinical progression or >/= 25% increase in the sum of the products of perpendicular diameters of the contrast enhancing lesions compared with the smallest tumor measurement obtained either at baseline (if no decrease was observed) or best response and with the subject on stable or increasing doses of corticosteroids. Tumor recurrence was defined as recurrence after tumor was completely resected (no disease present at baseline). EFS was estimated using the Kaplan-Meier method. | From the time of randomization to the date of any defined event (up to 12 months) | |
| Secondary | Overall Survival | Overall Survival was defined as the time of diagnosis to the date of death due to any cause. Overall Survival was estimated using the Kaplan-Meier method. | From the time of randomization to the date of death (up to approximately 60 months) | |
| Secondary | Percentage of Participants With 1-Year Survival | 1-year survival was estimated using the Kaplan-Meier method. | 1 year after end of treatment | |
| Secondary | Percentage of Participants With EFS as Determined by the CRRC at 6 Months | EFS was defined as the time from randomisation to the earliest occurrence of any of the following: tumor progression, tumor recurrence, second primary non- HGG malignancy or death attributable to any cause. Tumor assessments were conducted using MRI and reviewed by the site-independent CRRC using RANO criteria. Tumor progression was defined as clear clinical progression or >/= 25% increase in the sum of the products of perpendicular diameters of the contrast enhancing lesions compared with the smallest tumor measurement obtained either at baseline (if no decrease was observed) or best response and with the subject on stable or increasing doses of corticosteroids. Tumor recurrence was defined as recurrence after tumor was completely resected (no disease present at baseline). EFS was estimated using the Kaplan-Meier method. | 6 months | |
| Secondary | Percentage of Participants With EFS as Determined by the CRRC at 1 Year | EFS was defined as the time from randomisation to the earliest occurrence of any of the following: tumor progression, tumor recurrence, second primary non- HGG malignancy or death attributable to any cause. Tumor assessments were conducted using MRI and reviewed by the site-independent CRRC using RANO criteria. Tumor progression was defined as clear clinical progression or >/= 25% increase in the sum of the products of perpendicular diameters of the contrast enhancing lesions compared with the smallest tumor measurement obtained either at baseline (if no decrease was observed) or best response and with the subject on stable or increasing doses of corticosteroids. Tumor recurrence was defined as recurrence after tumor was completely resected (no disease present at baseline). EFS was estimated using the Kaplan-Meier method. | 1 year | |
| Secondary | EFS as Assessed by the Investigator | EFS was defined as the time from randomisation to the earliest occurrence of any of the following: tumor progression, tumor recurrence, second primary non-HGG malignancy or death attributable to any cause. Tumor assessments were conducted using MRI and reviewed by the investigator using RANO criteria. Tumor progression was defined as clear clinical progression or >/= 25% increase in the sum of the products of perpendicular diameters of the contrast enhancing lesions compared with the smallest tumor measurement obtained either at baseline (if no decrease was observed) or best response and with the participant on stable or increasing doses of corticosteroids. Tumor recurrence was defined as recurrence after tumor was completely resected (no disease present at baseline). EFS was estimated using the Kaplan-Meier method. | From the time of randomization to the date of any defined event (up to 12 months) | |
| Secondary | Objective Response Rate (ORR) | ORR was defined as the percentage of participants with a complete response (CR) or partial response (PR) determined on two consecutive occasions >/= 4 weeks apart. Tumor assessments were conducted using MRI and reviewed by the site-independent CRRC using RANO criteria. The following were needed to qualify as CR: complete disappearance of all measurable enhancing lesions sustained for at least 4 weeks by MRI, no steroids above physiological levels, clinical status stable or improved compared to baseline. The following were needed to qualify as PR: = 50% decrease from baseline in the sum of products of perpendicular diameters of all measurable enhancing lesions sustained for at least 4 weeks by MRI, steroid dose not increased compared to baseline, clinical status stable or improved compared to baseline. | From the time of randomization to the date of any defined event (up to 12 months) | |
| Secondary | Concordance Between Structural Versus Multimodal Imaging for CRRC-Assessed Event-Free Survival | Concordance is presented as the percentage of participants with concordance between assessments. EFS concordance was defined as event Structural assessment and Diffusion Perfusion assessment occurs within 28 days or no event Structural and no Diffusion Perfusion. | Up to 12 months | |
| Secondary | Health Status as Measured by the Health Utility Index (HUI) | HUI is a preference-based, multi-attitude, health-related instrument specifically developed for use with children. HUI consists of eight attributes of health status: vision, hearing, speech, ambulation, dexterity, emotion, cognition and pain. Each attribute had 5 or 6 levels varying from highly impaired to normal. Each of the eight health dimensions was tested separately and a composite score ranging between 1 (perfect health) and 0 (death) was obtained for participants aged 5 years or older. | Baseline, Cycle 6 of the adjuvant phase, end of treatment (approximately 58 weeks post-baseline), and yearly during the follow-up period (maximum 5 years in follow-up) | |
| Secondary | Neurological Psychological Function as Measured by the Wechsler Scale | The Wechsler Intelligence Scale for Children version IV (WISC-IV) was used to generate a full scale intelligence quotient (IQ) which represents a child's general intellectual ability. The average IQ score is 100, with lower scores representing lower intellectual ability. | End of treatment (approximately 58 weeks post-baseline) | |
| Secondary | Percentage of Participants Who Completed >/= 90% of Planned Radiotherapy and TMZ Administrations | From the time of randomization of the first participant to the date of clinical cutoff (approximately 60 months) | ||
| Secondary | Percentage of Participants With a Treatment Delay or Discontinuation | From the time of randomization of the first participant to the date of clinical cutoff (approximately 60 months) | ||
| Secondary | Number of Radiotherapy Dose Administrations in the Concurrent Phase | Number of doses were assessed for the concurrent phase, which is the treatment period after the initial treatment phase and including the subsequent treatment break of approximately 4 weeks. | Beginning of the concurrent phase to end of treatment break (10 weeks) | |
| Secondary | Number of Dose Administrations of TMZ and Bevacizumab in the Concurrent Phase | Number of doses were assessed for the concurrent phase, which is the treatment period after the initial treatment phase and including the subsequent treatment break of approximately 4 weeks. | Beginning of the concurrent phase to end of treatment break (10 weeks) | |
| Secondary | Percentage of Participants With an Adverse Event (AE) | An AE was defined as any unfavorable and unintended sign (including an abnormal laboratory finding), symptom, or disease temporally associated with the use of a medicinal product, whether or not considered related to the medicinal product. | From the time of randomization of the first participant to the date of clinical cutoff (approximately 60 months) |
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