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Efficacy and Safety of AP 12009 in Patients With Recurrent or Refractory Anaplastic Astrocytoma or Secondary Glioblastoma (SAPPHIRE)

Primary Purpose

Anaplastic Astrocytoma, Glioblastoma

Status
Terminated
Phase
Phase 3
Locations
International
Study Type
Interventional
Intervention
trabedersen
temozolomide
Drug delivery system for administration of AP 12009
Placement of Drug Delivery System
carmustine
lomustine
Sponsored by
Isarna Therapeutics GmbH
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional treatment trial for Anaplastic Astrocytoma focused on measuring Anaplastic astrocytoma, Glioblastoma, Antisense, Cancer, Transforming Growth Factor beta 2, Targeted therapy, Brain tumor, Glioma, Central Nervous System (CNS), Convection Enhanced Delivery (CED), Intratumoral administration

Eligibility Criteria

18 Years - 70 Years (Adult, Older Adult)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

  • The patient has provided written informed consent prior to any study-related procedure.
  • The patient is at least 18 years of age and equal to or below 70 years.
  • The patient has a present diagnosis of AA or secondary GBM.
  • The patient has a measurable lesion (> 1 ccm in volume, central MRI review).
  • The lesion (or sum of lesions) does not exceed 50 ccm in volume (central MRI review).
  • The tumor is localized supratentorially (central MRI review).
  • All patients have recurrent or refractory disease, i.e. disease has progressed after prior surgery and radiotherapy at any time of the disease course or stage. Secondary GBM patients have progressed after a previous diagnosis of A and/or AA.
  • The patient has not received more than one chemotherapy regimen. Radiation with concomitant chemotherapy, followed by adjuvant chemotherapy, is considered as one chemotherapy regimen.
  • The patient is eligible for chemotherapy.
  • The patient is on a maximum dose of 4 mg/day dexamethasone or equivalent doses for other corticosteroids, which has been stable or decreasing for at least 3 weeks prior to Screening.
  • The patient is male or a non-pregnant, non-lactating female.
  • Females of childbearing potential must have a negative beta-HCG pregnancy test at Screening.
  • Females of childbearing potential and males must practice strict birth control.
  • The patient must have recovered from acute toxicity caused by any previous therapy.
  • The patient has a life expectancy of at least 3 months.
  • The patient has a Karnofsky Performance Status of at least 70%.
  • The patient shows adequate organ functions as assessed by the following screening laboratory values:

    1. Adequate renal function determined by serum creatinine and urea < 2 times the upper limit of normal
    2. Adequate liver function with ALT, AST and AP < 3 times the upper limit of normal, and bilirubin < 2.5 mg/dL
    3. INR < 1.5 and aPTT < 1.5 x ULN
    4. Hemoglobin > 9 g/dL
    5. Platelet count > 100 x 10E9/L
    6. WBC > 3 x 10E9/L
    7. ANC > 1.5 x 10E9/L (or WBC > 3.0 x 10E9/L)

Exclusion Criteria:

  • Patient unable or not willing to comply with the protocol regulations.
  • The investigator deems it necessary to surgically (re-)resect the present tumor (NOTE: the patient might still be eligible for randomization at a later timepoint).
  • Tumor surgery, tumor debulking, or other neurosurgery within 3 months prior to randomization. If a ≤48-hour routine post-surgery MRI (in accordance with study specifications) qualifies the patient for study participation, the patient can be randomized 30 ± 7 days post-surgery.
  • Radiotherapy or stereotactic (gamma knife) radiosurgery within 3 months prior to randomization.
  • Prior interstitial brachytherapy of the brain with permanent implants. Prior interstitial brachytherapy of the brain with removable implants within 3 months prior to randomization.
  • Chemotherapy, hormone therapy, or any other therapy with established or suggested anti-tumor effects within 4 weeks (nitrosoureas: 6 weeks) prior to randomization.
  • Prior anti-TGF-beta 2 targeted therapy.
  • Screening MRI shows a mass effect caused by the tumor defined as significant compression of the ventricular system and/or a midline shift (≥ 3 mm, central MRI review). Compression of the ventricular system and/or a midline shift ≥ 3 mm only due to the presence of (a) cyst(s) or scarring processes does not exclude an individual from the study.
  • Participation in another clinical study with another investigational medicinal product within 30 days prior to randomization.
  • History of a second independent malignant disorder within 5 years, except for carcinoma in situ of the cervix and basal cell carcinoma.
  • Presence of poorly controlled seizures.
  • Clinically relevant cardiovascular abnormalities such as uncontrolled hypertension, congestive heart failure, unstable angina, or poorly controlled arrhythmia. Myocardial infarction within 6 months prior to randomization.
  • Known HIV, HBV or HCV infection.
  • Acute viral, bacterial, or fungal infection.
  • Acute medical problems that may be considered to become an unacceptable risk, or any conditions, which might be contraindications for starting study treatment.
  • Presence of high risk for pulmonary toxicities, defined as:

    1. Lung function: vital capacity ≤ 70%
    2. Status following sequential or concomitant thoracic irradiation
    3. Increased risk for a pulmonary toxicity induced by BCNU (Carmustine) or CCNU (Lomustine). Risk factors include smoking, presence of a respiratory condition, pre-existing radiographic pulmonary abnormalities, exposure to agents that cause lung damage.
  • History of allergies to reagents used in this study, history of celiac disease.
  • Drug abuse or extensive use of alcohol.
  • Clinically relevant psychiatric disorders / legal incapacity or a limited legal capacity.
  • Concomitant treatment with yellow fever vaccine.

Sites / Locations

  • NJ Neuroscience Institute; JFK Medical Center
  • Winthrop University Hospital
  • University of Rochester Medical Center
  • Hospital Británico
  • FLENI
  • Sanatorio Allende
  • Universitätsklinik Innsbruck, Abteilung für Neurologie
  • AKH Wien, Klinik für Neurochirurgie
  • Hospital de Câncer de Barretos
  • Centro Goiano de Oncologia (CGO)
  • Hospital Sao Vicente de Paulo
  • Hospital de Clínicas de Porto Alegre
  • Hospital Sao Lucas da PUCRS
  • Hospital do Servidor Público Estadual
  • ECOGENE-21 Centre d'études cliniques
  • Foothills Medical Centre
  • Montreal Neurological Institute and Hospital
  • La Timone University Hospital
  • Klinik und Poliklinik für Neurochirurgie
  • Universitätsklinikum Freiburg
  • Neurochirurgische Klinik an der Universität Ulm am Bezirkskrankenhaus Günzburg
  • Universitätklinikum Hamburg-Eppendorf, Klinik für Neurochirurgie
  • Medizinische Hochschule Hannover Neurochirurgische Klinik
  • Universitätsklinik Heidelberg Neurologische Klinik
  • Universitätsklinikum Leipzig, Neurochirurgische Klinik
  • Otto-von-Guericke-Universität, Klinik für Neurochirurgie
  • Klinik und Poliklinik für Neurochirurgie
  • Klinik und Poliklinik für Neurologie
  • Szegedi Tudományegyetem Szent-Györgyi Albert Klinikai Központ
  • Manipal Hospital & Manipal Institute for Neurological Disorders
  • NIMHANS
  • BGS Global Hospital
  • Postgraduate Institute of Medical Education & Research (PGIMER)
  • Apollo Speciality Hospitals
  • Amrita Institute of Medical Sciences Research Center
  • Care Hospitals
  • AMRI Hospitals
  • SGPGI of Medical Sciences
  • Advanced Centre for Treatment Research and Education in Cancer (ACTREC)
  • All India Institute of Medical Sciences (AIIMS)
  • SCTIMST, Dept. of Neurosurgery
  • Severance Hospital, Yonsei University College of Medicine
  • Kangnam St. Mary's Hospital
  • Asan Medical Center
  • Hospital San Javier
  • Hospital General de Mexico
  • Medica Sur
  • Wojskowy Szpital Kliniczny, Klinika Neurochirurgii
  • Akademickie Centrum Kliniczne
  • Samodzielny Publiczny Szpital Kliniczny nr 4, Klinika Neurochirurgii i Neurochirurgii Dziecięcej
  • Kliniczny Oddzial Neurochirurgii SUM w Sosnowcu Wojewódzki Szpital Specjalistyczny nr 5
  • Centrum Onkologii - Instytut Im. Marii Sklodowskiej-Curie
  • SP ZOZ Uniwersytecki Szpital Kliniczny nr 1, Klinika Neurochirurgii
  • Chelyabinsk City Hospital #3; Department of Neurosurgery
  • State Institution Russian Oncology Research Center N.N. Blokhin
  • Samara Region Clinical Hospital M.I. Kalinin
  • Russian Scientific Research Neurosurgical Institute A.L. Polenov
  • Military Medical Academy, Neurosurgery Dept
  • Hospital de Cruces
  • Hospital Universitario Vall d'Hebron
  • Hospital Doce de Octubre
  • Hospital Universitario Marqués de Valdecilla
  • Hospital Universitario Virgen del Rocío
  • China Medical University Hospital
  • Taichung Veterans General Hospital
  • Tri-Service General Hospital
  • Edinburgh Centre for Neuro-Oncology, Western General Hospital
  • The National Hospital for Neurology and Neurosurgery

Arms of the Study

Arm 1

Arm 2

Arm Type

Experimental

Active Comparator

Arm Label

trabedersen 10 µM

Chemotherapy

Arm Description

10 µM trabedersen (AP 12009), intratumoral infusion, every other week, 11 cycles, maximum 21 weeks

temozolomide: capsules, up to 200 mg/sqm/day, 5 days per cycle, up to 26 cycles; carmustine: i.v. administration, up to 200 mg/sqm/day, 1 day per cycle, up to 8 cycles; lomustine: capsules, 110 mg/sqm/day, 1 day per cycle, up to 8 cycles. Only 1 of these 3 drugs/interventions is administered per patient in the comparator arm.

Outcomes

Primary Outcome Measures

Survival Rate at 24 Months in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Survival rate was defined as the proportion of participants known to be alive at 24 months from randomization. If a participant's status was unknown and there was no follow-up information available, they were categorized as 'Died' for the purposes of the analysis.
Survival at 24 Months in the Intent-to-treat Population - Number of Participants
Survival status was assessed at 24 months from randomization. Participants with unknown or missing status were considered treatment failures, i.e., assumed to be dead. The category "Lost to / insufficient follow-up" includes participants who were alive at last data collection point but did not yet have enough follow-up time to reach the 24 month time point.

Secondary Outcome Measures

Survival Rate at 12, 18, and 21 Months in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Survival rate was defined as the proportion of participants known to be alive at each time-point from randomization. Participants with unknown or missing status were considered treatment failures, i.e., assumed to be dead.
Survival at 12, 18, and 21 Months in the Intent-to-treat Population - Number of Participants
Survival status was assessed at each time-point from randomization. Participants with unknown or missing status were considered treatment failures, i.e., assumed to be dead. The category "Lost to follow-up" for each time-point includes participants who were alive at the last data collection point but did not yet have enough follow-up time to reach the time point.
Median Overall Survival (Days) From Randomization in the Intent-to-treat Population (Descriptive Analysis, Only)
Median overall survival was defined as the date of randomization to the date of death. If a participant's status was unknown and there was no follow-up information available, they were categorized as 'Died' for the purposes of the analysis. Analysis was by Kaplan-Meier estimation.
Response Category by Independent Review in the Intent-to-treat Population - Number of Participants
Tumor response was classified based on the (neuro-)radiologist's evaluation according to the Macdonald Response Criteria for bidimensionally measurable disease as outlined below: Complete Response (CR): Disappearance of all enhancing tumor on consecutive MRI scans at least 1 month apart, off steroids, neurologically stable or improved. Partial Response (PR): ≥50% reduction in size of enhancing tumor on consecutive MRI scans at least 1 month apart, steroids stable or reduced, neurologically stable or improved. Progressive Disease (PD): ≥25% increase in size of enhancing tumor or any new tumor on MRI scans, steroids stable or increased, neurologically worse. Stable Disease (SD): all other situations. Two qualified neuro-radiologists reviewed scans at each MRI time point, with adjudication of discrepancies by a third reviewer. Their findings and clinical information were independently reviewed by a neuro-oncologist, who made the assessment of overall response.
Overall Response Rate (CR+PR) by Independent Review in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Overall response rate was the proportion of participants with a best response of Complete Response (CR) or Partial Response (PR) observed from the start of treatment until disease progression.
Tumor Control Rate (CR+PR+SD) by Independent Review in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Tumor control rate was defined as the proportion of participants assessed as having Complete Response (CR), Partial Response (PR), or Stable Disease (SD). Participants with unknown or missing response were treated as non-responders.
Median Duration of Response (Days) by Independent Review (Descriptive Analysis, Only)
Duration of response was defined as the time from the first documentation of confirmed response (Complete Response, CR, or Partial Response, PR) to the first signs of Progressive Disease (PD), as assessed by the study neuro-oncologist. Median Duration of Response was calculated by Kaplan-Meier estimate. Censoring rules were: at the date of randomization -- participants without baseline assessments, or for those with no post-baseline timor assessments who were discontinued for other than progressive disease or death. at the date of last tumor assessment -- discontinuation other than PD or death, or if a new treatment was started prior to disease progression at the date of death or last tumor assessment -- death or PD after one missed tumor assessment at the date of last tumor assessment -- death or PD after more than one missed tumor assessment at the date of last tumor assessment -- participants on ongoing treatment at data cut-off
Disease Progression at 10, 12, 14, 16, 18, 21, and 24 Months by Independent Review in the Intent-to-treat Population - Number of Participants
Tumor response was classified based on the (neuro-)radiologist's evaluation: Complete Response (CR): Disappearance of all enhancing tumor on consecutive MRI scans at least 1 month apart, off steroids, neurologically stable or improved. Partial Response (PR): ≥50% reduction in size of enhancing tumor on consecutive MRI scans at least 1 month apart, steroids stable or reduced, neurologically stable or improved. Progressive Disease (PD): ≥25% increase in size of enhancing tumor or any new tumor on MRI scans, steroids stable or increased, neurologically worse. Stable Disease (SD): all other situations. Based on clinical and imaging data, an independent neuro-oncologist made the final assessment of "Progressed" versus "Not Progressed". Participants who had MRI assessment results missing or unknown were "UNK or missing", and were treated as "Progressed" for the purposes of the calculation.
Disease Progression Rate at 10, 12, 14, 16, 18, 21, and 24 Months by Independent Review in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Tumor response was classified based on the (neuro-)radiologist's evaluation: Complete Response (CR): Disappearance of all enhancing tumor on consecutive MRI scans at least 1 month apart, off steroids, neurologically stable or improved. Partial Response (PR): ≥50% reduction in size of enhancing tumor on consecutive MRI scans at least 1 month apart, steroids stable or reduced, neurologically stable or improved. Progressive Disease (PD): ≥25% increase in size of enhancing tumor or any new tumor on MRI scans, steroids stable or increased, neurologically worse. Stable Disease (SD): all other situations. Based on clinical and imaging data, an independent neuro-oncologist made the final assessment of "Progressed" versus "Not Progressed". Participants who had MRI assessment results missing or unknown were "UNK or missing", and were treated as "Progressed" for the purposes of the calculation.
Median Time to Progression (Days) by Independent Review for the Intent-to-treat Population (Descriptive Analysis, Only)
Time to progression was calculated from the date of randomization to the date of the first documented tumor progression. Participants who did not progress or died were censored at the last tumor assessment date or the date of start of a new anti-tumor treatment or death.

Full Information

First Posted
September 26, 2008
Last Updated
November 4, 2014
Sponsor
Isarna Therapeutics GmbH
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1. Study Identification

Unique Protocol Identification Number
NCT00761280
Brief Title
Efficacy and Safety of AP 12009 in Patients With Recurrent or Refractory Anaplastic Astrocytoma or Secondary Glioblastoma
Acronym
SAPPHIRE
Official Title
Efficacy and Safety of AP 12009 in Adult Patients With Recurrent or Refractory Anaplastic Astrocytoma or Secondary Glioblastoma as Compared to Standard Chemotherapy Treatment: A Randomized, Actively Controlled, Open Label Clinical Phase III Study.
Study Type
Interventional

2. Study Status

Record Verification Date
November 2014
Overall Recruitment Status
Terminated
Why Stopped
Unable to recruit the projected patient number. All analyses are descriptive, only.
Study Start Date
December 2008 (undefined)
Primary Completion Date
February 2012 (Actual)
Study Completion Date
June 2012 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor
Name of the Sponsor
Isarna Therapeutics GmbH

4. Oversight

Data Monitoring Committee
Yes

5. Study Description

Brief Summary
In this multinational Phase III study the efficacy and safety of 10 µM AP 12009 is compared to standard chemotherapy (temozolomide or BCNU or CCNU) in adult patients with confirmed recurrent or refractory anaplastic astrocytoma (WHO grade III) or secondary glioblastoma (WHO grade IV).
Detailed Description
The purpose of this study is to compare the safety and efficacy of the 10 µM concentration of AP 12009 and standard chemotherapy (temozolomide, BCNU, CCNU) in adult patients with recurrent or refractory anaplastic astrocytoma (AA, WHO grade III) or secondary glioblastoma (GBM, WHO grade IV). AP 12009 (trabedersen) is a phosphorothioate antisense oligodeoxynucleotide specific for the mRNA of human Transforming Growth Factor beta 2 (TGF-beta-2), which is applied intratumorally. The growth factor TGF-beta plays a key role in malignant progression of various tumors by inducing proliferation, invasion, metastasis, angiogenesis, and escape from immunosurveillance. In patients with high-grade glioma, the TGF-beta-2 overexpression is associated with disease stage, clinical prognosis, and the immunodeficient state of the patients. Main objective of the study is to determine survival (rate) and tumor response. Important note: Due to early trial termination, resulting in limited data availability, all analyses remain descriptive by nature, only. No conclusive endpoint analysis can be performed.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Anaplastic Astrocytoma, Glioblastoma
Keywords
Anaplastic astrocytoma, Glioblastoma, Antisense, Cancer, Transforming Growth Factor beta 2, Targeted therapy, Brain tumor, Glioma, Central Nervous System (CNS), Convection Enhanced Delivery (CED), Intratumoral administration

7. Study Design

Primary Purpose
Treatment
Study Phase
Phase 3
Interventional Study Model
Parallel Assignment
Masking
None (Open Label)
Allocation
Randomized
Enrollment
27 (Actual)

8. Arms, Groups, and Interventions

Arm Title
trabedersen 10 µM
Arm Type
Experimental
Arm Description
10 µM trabedersen (AP 12009), intratumoral infusion, every other week, 11 cycles, maximum 21 weeks
Arm Title
Chemotherapy
Arm Type
Active Comparator
Arm Description
temozolomide: capsules, up to 200 mg/sqm/day, 5 days per cycle, up to 26 cycles; carmustine: i.v. administration, up to 200 mg/sqm/day, 1 day per cycle, up to 8 cycles; lomustine: capsules, 110 mg/sqm/day, 1 day per cycle, up to 8 cycles. Only 1 of these 3 drugs/interventions is administered per patient in the comparator arm.
Intervention Type
Drug
Intervention Name(s)
trabedersen
Other Intervention Name(s)
AP 12009
Intervention Type
Drug
Intervention Name(s)
temozolomide
Other Intervention Name(s)
Temodar, Temodal, TMZ
Intervention Type
Device
Intervention Name(s)
Drug delivery system for administration of AP 12009
Intervention Description
Drug delivery system for Convection Enhanced Delivery consists of a portable pump (Pegasus vario or Pega vario) with drug reservoir (Pega Bag) and infusion line (Pega Line). Main implanted parts are the port access system (PORT-A-CATH) and the intratumoral catheter (Medtronic ventricular catheter).
Intervention Type
Procedure
Intervention Name(s)
Placement of Drug Delivery System
Intervention Description
Surgery for placement of intratumoral catheter and subcutaneous port access system as per routine clinical practice. Stereotactical catheter placement controlled by CT.
Intervention Type
Drug
Intervention Name(s)
carmustine
Other Intervention Name(s)
BCNU, BiCNU, Carmubris
Intervention Type
Drug
Intervention Name(s)
lomustine
Other Intervention Name(s)
CCNU, CeeNU
Primary Outcome Measure Information:
Title
Survival Rate at 24 Months in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Description
Survival rate was defined as the proportion of participants known to be alive at 24 months from randomization. If a participant's status was unknown and there was no follow-up information available, they were categorized as 'Died' for the purposes of the analysis.
Time Frame
24 months
Title
Survival at 24 Months in the Intent-to-treat Population - Number of Participants
Description
Survival status was assessed at 24 months from randomization. Participants with unknown or missing status were considered treatment failures, i.e., assumed to be dead. The category "Lost to / insufficient follow-up" includes participants who were alive at last data collection point but did not yet have enough follow-up time to reach the 24 month time point.
Time Frame
24 months
Secondary Outcome Measure Information:
Title
Survival Rate at 12, 18, and 21 Months in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Description
Survival rate was defined as the proportion of participants known to be alive at each time-point from randomization. Participants with unknown or missing status were considered treatment failures, i.e., assumed to be dead.
Time Frame
12, 18, and 21 months
Title
Survival at 12, 18, and 21 Months in the Intent-to-treat Population - Number of Participants
Description
Survival status was assessed at each time-point from randomization. Participants with unknown or missing status were considered treatment failures, i.e., assumed to be dead. The category "Lost to follow-up" for each time-point includes participants who were alive at the last data collection point but did not yet have enough follow-up time to reach the time point.
Time Frame
12, 18, and 21 months
Title
Median Overall Survival (Days) From Randomization in the Intent-to-treat Population (Descriptive Analysis, Only)
Description
Median overall survival was defined as the date of randomization to the date of death. If a participant's status was unknown and there was no follow-up information available, they were categorized as 'Died' for the purposes of the analysis. Analysis was by Kaplan-Meier estimation.
Time Frame
Up to 24 months
Title
Response Category by Independent Review in the Intent-to-treat Population - Number of Participants
Description
Tumor response was classified based on the (neuro-)radiologist's evaluation according to the Macdonald Response Criteria for bidimensionally measurable disease as outlined below: Complete Response (CR): Disappearance of all enhancing tumor on consecutive MRI scans at least 1 month apart, off steroids, neurologically stable or improved. Partial Response (PR): ≥50% reduction in size of enhancing tumor on consecutive MRI scans at least 1 month apart, steroids stable or reduced, neurologically stable or improved. Progressive Disease (PD): ≥25% increase in size of enhancing tumor or any new tumor on MRI scans, steroids stable or increased, neurologically worse. Stable Disease (SD): all other situations. Two qualified neuro-radiologists reviewed scans at each MRI time point, with adjudication of discrepancies by a third reviewer. Their findings and clinical information were independently reviewed by a neuro-oncologist, who made the assessment of overall response.
Time Frame
Up to 24 months
Title
Overall Response Rate (CR+PR) by Independent Review in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Description
Overall response rate was the proportion of participants with a best response of Complete Response (CR) or Partial Response (PR) observed from the start of treatment until disease progression.
Time Frame
Up to 24 months
Title
Tumor Control Rate (CR+PR+SD) by Independent Review in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Description
Tumor control rate was defined as the proportion of participants assessed as having Complete Response (CR), Partial Response (PR), or Stable Disease (SD). Participants with unknown or missing response were treated as non-responders.
Time Frame
Up to 24 months
Title
Median Duration of Response (Days) by Independent Review (Descriptive Analysis, Only)
Description
Duration of response was defined as the time from the first documentation of confirmed response (Complete Response, CR, or Partial Response, PR) to the first signs of Progressive Disease (PD), as assessed by the study neuro-oncologist. Median Duration of Response was calculated by Kaplan-Meier estimate. Censoring rules were: at the date of randomization -- participants without baseline assessments, or for those with no post-baseline timor assessments who were discontinued for other than progressive disease or death. at the date of last tumor assessment -- discontinuation other than PD or death, or if a new treatment was started prior to disease progression at the date of death or last tumor assessment -- death or PD after one missed tumor assessment at the date of last tumor assessment -- death or PD after more than one missed tumor assessment at the date of last tumor assessment -- participants on ongoing treatment at data cut-off
Time Frame
Up to 24 months
Title
Disease Progression at 10, 12, 14, 16, 18, 21, and 24 Months by Independent Review in the Intent-to-treat Population - Number of Participants
Description
Tumor response was classified based on the (neuro-)radiologist's evaluation: Complete Response (CR): Disappearance of all enhancing tumor on consecutive MRI scans at least 1 month apart, off steroids, neurologically stable or improved. Partial Response (PR): ≥50% reduction in size of enhancing tumor on consecutive MRI scans at least 1 month apart, steroids stable or reduced, neurologically stable or improved. Progressive Disease (PD): ≥25% increase in size of enhancing tumor or any new tumor on MRI scans, steroids stable or increased, neurologically worse. Stable Disease (SD): all other situations. Based on clinical and imaging data, an independent neuro-oncologist made the final assessment of "Progressed" versus "Not Progressed". Participants who had MRI assessment results missing or unknown were "UNK or missing", and were treated as "Progressed" for the purposes of the calculation.
Time Frame
10, 12, 14, 16, 18, 21, and 24 months
Title
Disease Progression Rate at 10, 12, 14, 16, 18, 21, and 24 Months by Independent Review in the Intent-to-treat Population - Percentage of Participants (Descriptive Analysis, Only)
Description
Tumor response was classified based on the (neuro-)radiologist's evaluation: Complete Response (CR): Disappearance of all enhancing tumor on consecutive MRI scans at least 1 month apart, off steroids, neurologically stable or improved. Partial Response (PR): ≥50% reduction in size of enhancing tumor on consecutive MRI scans at least 1 month apart, steroids stable or reduced, neurologically stable or improved. Progressive Disease (PD): ≥25% increase in size of enhancing tumor or any new tumor on MRI scans, steroids stable or increased, neurologically worse. Stable Disease (SD): all other situations. Based on clinical and imaging data, an independent neuro-oncologist made the final assessment of "Progressed" versus "Not Progressed". Participants who had MRI assessment results missing or unknown were "UNK or missing", and were treated as "Progressed" for the purposes of the calculation.
Time Frame
10, 12, 14, 16, 18, 21 and 24 months
Title
Median Time to Progression (Days) by Independent Review for the Intent-to-treat Population (Descriptive Analysis, Only)
Description
Time to progression was calculated from the date of randomization to the date of the first documented tumor progression. Participants who did not progress or died were censored at the last tumor assessment date or the date of start of a new anti-tumor treatment or death.
Time Frame
Up to 24 months

10. Eligibility

Sex
All
Minimum Age & Unit of Time
18 Years
Maximum Age & Unit of Time
70 Years
Accepts Healthy Volunteers
No
Eligibility Criteria
Inclusion Criteria: The patient has provided written informed consent prior to any study-related procedure. The patient is at least 18 years of age and equal to or below 70 years. The patient has a present diagnosis of AA or secondary GBM. The patient has a measurable lesion (> 1 ccm in volume, central MRI review). The lesion (or sum of lesions) does not exceed 50 ccm in volume (central MRI review). The tumor is localized supratentorially (central MRI review). All patients have recurrent or refractory disease, i.e. disease has progressed after prior surgery and radiotherapy at any time of the disease course or stage. Secondary GBM patients have progressed after a previous diagnosis of A and/or AA. The patient has not received more than one chemotherapy regimen. Radiation with concomitant chemotherapy, followed by adjuvant chemotherapy, is considered as one chemotherapy regimen. The patient is eligible for chemotherapy. The patient is on a maximum dose of 4 mg/day dexamethasone or equivalent doses for other corticosteroids, which has been stable or decreasing for at least 3 weeks prior to Screening. The patient is male or a non-pregnant, non-lactating female. Females of childbearing potential must have a negative beta-HCG pregnancy test at Screening. Females of childbearing potential and males must practice strict birth control. The patient must have recovered from acute toxicity caused by any previous therapy. The patient has a life expectancy of at least 3 months. The patient has a Karnofsky Performance Status of at least 70%. The patient shows adequate organ functions as assessed by the following screening laboratory values: Adequate renal function determined by serum creatinine and urea < 2 times the upper limit of normal Adequate liver function with ALT, AST and AP < 3 times the upper limit of normal, and bilirubin < 2.5 mg/dL INR < 1.5 and aPTT < 1.5 x ULN Hemoglobin > 9 g/dL Platelet count > 100 x 10E9/L WBC > 3 x 10E9/L ANC > 1.5 x 10E9/L (or WBC > 3.0 x 10E9/L) Exclusion Criteria: Patient unable or not willing to comply with the protocol regulations. The investigator deems it necessary to surgically (re-)resect the present tumor (NOTE: the patient might still be eligible for randomization at a later timepoint). Tumor surgery, tumor debulking, or other neurosurgery within 3 months prior to randomization. If a ≤48-hour routine post-surgery MRI (in accordance with study specifications) qualifies the patient for study participation, the patient can be randomized 30 ± 7 days post-surgery. Radiotherapy or stereotactic (gamma knife) radiosurgery within 3 months prior to randomization. Prior interstitial brachytherapy of the brain with permanent implants. Prior interstitial brachytherapy of the brain with removable implants within 3 months prior to randomization. Chemotherapy, hormone therapy, or any other therapy with established or suggested anti-tumor effects within 4 weeks (nitrosoureas: 6 weeks) prior to randomization. Prior anti-TGF-beta 2 targeted therapy. Screening MRI shows a mass effect caused by the tumor defined as significant compression of the ventricular system and/or a midline shift (≥ 3 mm, central MRI review). Compression of the ventricular system and/or a midline shift ≥ 3 mm only due to the presence of (a) cyst(s) or scarring processes does not exclude an individual from the study. Participation in another clinical study with another investigational medicinal product within 30 days prior to randomization. History of a second independent malignant disorder within 5 years, except for carcinoma in situ of the cervix and basal cell carcinoma. Presence of poorly controlled seizures. Clinically relevant cardiovascular abnormalities such as uncontrolled hypertension, congestive heart failure, unstable angina, or poorly controlled arrhythmia. Myocardial infarction within 6 months prior to randomization. Known HIV, HBV or HCV infection. Acute viral, bacterial, or fungal infection. Acute medical problems that may be considered to become an unacceptable risk, or any conditions, which might be contraindications for starting study treatment. Presence of high risk for pulmonary toxicities, defined as: Lung function: vital capacity ≤ 70% Status following sequential or concomitant thoracic irradiation Increased risk for a pulmonary toxicity induced by BCNU (Carmustine) or CCNU (Lomustine). Risk factors include smoking, presence of a respiratory condition, pre-existing radiographic pulmonary abnormalities, exposure to agents that cause lung damage. History of allergies to reagents used in this study, history of celiac disease. Drug abuse or extensive use of alcohol. Clinically relevant psychiatric disorders / legal incapacity or a limited legal capacity. Concomitant treatment with yellow fever vaccine.
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Rolando Del Maestro, MD, PhD
Organizational Affiliation
Montreal Neurological Institute and Hospital
Official's Role
Study Chair
Facility Information:
Facility Name
NJ Neuroscience Institute; JFK Medical Center
City
Edison
State/Province
New Jersey
ZIP/Postal Code
08820
Country
United States
Facility Name
Winthrop University Hospital
City
Mineola
State/Province
New York
ZIP/Postal Code
11501
Country
United States
Facility Name
University of Rochester Medical Center
City
Rochester
State/Province
New York
ZIP/Postal Code
14642
Country
United States
Facility Name
Hospital Británico
City
Ciudad Autónoma de Buenos Aires
ZIP/Postal Code
C1280AEB
Country
Argentina
Facility Name
FLENI
City
Ciudad Autónoma de Buenos Aires
ZIP/Postal Code
C1428
Country
Argentina
Facility Name
Sanatorio Allende
City
Córdoba
ZIP/Postal Code
X5000JHQ
Country
Argentina
Facility Name
Universitätsklinik Innsbruck, Abteilung für Neurologie
City
Innsbruck
ZIP/Postal Code
6020
Country
Austria
Facility Name
AKH Wien, Klinik für Neurochirurgie
City
Wien
ZIP/Postal Code
1090
Country
Austria
Facility Name
Hospital de Câncer de Barretos
City
Barretos / SP
ZIP/Postal Code
14784-400
Country
Brazil
Facility Name
Centro Goiano de Oncologia (CGO)
City
Goiania
ZIP/Postal Code
74223-080
Country
Brazil
Facility Name
Hospital Sao Vicente de Paulo
City
Passo Fundo
ZIP/Postal Code
99010-080
Country
Brazil
Facility Name
Hospital de Clínicas de Porto Alegre
City
Porto Alegre
ZIP/Postal Code
90035-903
Country
Brazil
Facility Name
Hospital Sao Lucas da PUCRS
City
Porto Alegre
ZIP/Postal Code
90610-000
Country
Brazil
Facility Name
Hospital do Servidor Público Estadual
City
Sao Paulo
ZIP/Postal Code
04038-034
Country
Brazil
Facility Name
ECOGENE-21 Centre d'études cliniques
City
Chicoutimi
State/Province
Quebec
ZIP/Postal Code
G7H 7P2
Country
Canada
Facility Name
Foothills Medical Centre
City
Calgary
ZIP/Postal Code
AB T2N 2T9
Country
Canada
Facility Name
Montreal Neurological Institute and Hospital
City
Montreal
ZIP/Postal Code
H3A 2B4
Country
Canada
Facility Name
La Timone University Hospital
City
Marseille
ZIP/Postal Code
13385
Country
France
Facility Name
Klinik und Poliklinik für Neurochirurgie
City
Frankfurt/M.
ZIP/Postal Code
60528
Country
Germany
Facility Name
Universitätsklinikum Freiburg
City
Freiburg
ZIP/Postal Code
79106
Country
Germany
Facility Name
Neurochirurgische Klinik an der Universität Ulm am Bezirkskrankenhaus Günzburg
City
Günzburg
ZIP/Postal Code
89312
Country
Germany
Facility Name
Universitätklinikum Hamburg-Eppendorf, Klinik für Neurochirurgie
City
Hamburg
ZIP/Postal Code
20246
Country
Germany
Facility Name
Medizinische Hochschule Hannover Neurochirurgische Klinik
City
Hannover
ZIP/Postal Code
30625
Country
Germany
Facility Name
Universitätsklinik Heidelberg Neurologische Klinik
City
Heidelberg
ZIP/Postal Code
69120
Country
Germany
Facility Name
Universitätsklinikum Leipzig, Neurochirurgische Klinik
City
Leipzig
ZIP/Postal Code
04103
Country
Germany
Facility Name
Otto-von-Guericke-Universität, Klinik für Neurochirurgie
City
Magdeburg
ZIP/Postal Code
39120
Country
Germany
Facility Name
Klinik und Poliklinik für Neurochirurgie
City
Münster
ZIP/Postal Code
48149
Country
Germany
Facility Name
Klinik und Poliklinik für Neurologie
City
Regensburg
ZIP/Postal Code
93053
Country
Germany
Facility Name
Szegedi Tudományegyetem Szent-Györgyi Albert Klinikai Központ
City
Szeged
ZIP/Postal Code
6720
Country
Hungary
Facility Name
Manipal Hospital & Manipal Institute for Neurological Disorders
City
Bangalore
ZIP/Postal Code
560017
Country
India
Facility Name
NIMHANS
City
Bangalore
ZIP/Postal Code
560029
Country
India
Facility Name
BGS Global Hospital
City
Bangalore
ZIP/Postal Code
560060
Country
India
Facility Name
Postgraduate Institute of Medical Education & Research (PGIMER)
City
Chandigarh
ZIP/Postal Code
160012
Country
India
Facility Name
Apollo Speciality Hospitals
City
Chennai
ZIP/Postal Code
600006
Country
India
Facility Name
Amrita Institute of Medical Sciences Research Center
City
Cochin
ZIP/Postal Code
560017
Country
India
Facility Name
Care Hospitals
City
Hyderabaad
ZIP/Postal Code
500034
Country
India
Facility Name
AMRI Hospitals
City
Kolkata
ZIP/Postal Code
700029
Country
India
Facility Name
SGPGI of Medical Sciences
City
Lucknow
ZIP/Postal Code
226014
Country
India
Facility Name
Advanced Centre for Treatment Research and Education in Cancer (ACTREC)
City
Mumbai
ZIP/Postal Code
410210
Country
India
Facility Name
All India Institute of Medical Sciences (AIIMS)
City
New Delhi
ZIP/Postal Code
110029
Country
India
Facility Name
SCTIMST, Dept. of Neurosurgery
City
Thiruvananthapuram
ZIP/Postal Code
695011
Country
India
Facility Name
Severance Hospital, Yonsei University College of Medicine
City
Seoul
ZIP/Postal Code
120-752
Country
Korea, Republic of
Facility Name
Kangnam St. Mary's Hospital
City
Seoul
ZIP/Postal Code
137-701
Country
Korea, Republic of
Facility Name
Asan Medical Center
City
Seoul
ZIP/Postal Code
138-736
Country
Korea, Republic of
Facility Name
Hospital San Javier
City
Guadalajara
ZIP/Postal Code
44670
Country
Mexico
Facility Name
Hospital General de Mexico
City
Mexico City
ZIP/Postal Code
06120
Country
Mexico
Facility Name
Medica Sur
City
Mexico City
ZIP/Postal Code
14050
Country
Mexico
Facility Name
Wojskowy Szpital Kliniczny, Klinika Neurochirurgii
City
Bydgoszcz
ZIP/Postal Code
85-681
Country
Poland
Facility Name
Akademickie Centrum Kliniczne
City
Gdańsk
ZIP/Postal Code
80-952
Country
Poland
Facility Name
Samodzielny Publiczny Szpital Kliniczny nr 4, Klinika Neurochirurgii i Neurochirurgii Dziecięcej
City
Lublin
ZIP/Postal Code
20-090
Country
Poland
Facility Name
Kliniczny Oddzial Neurochirurgii SUM w Sosnowcu Wojewódzki Szpital Specjalistyczny nr 5
City
Sosnowiec
ZIP/Postal Code
41-200
Country
Poland
Facility Name
Centrum Onkologii - Instytut Im. Marii Sklodowskiej-Curie
City
Warszawa
ZIP/Postal Code
02-781
Country
Poland
Facility Name
SP ZOZ Uniwersytecki Szpital Kliniczny nr 1, Klinika Neurochirurgii
City
Łódź
ZIP/Postal Code
91-153
Country
Poland
Facility Name
Chelyabinsk City Hospital #3; Department of Neurosurgery
City
Chelyabinsk
ZIP/Postal Code
454021
Country
Russian Federation
Facility Name
State Institution Russian Oncology Research Center N.N. Blokhin
City
Moscow
ZIP/Postal Code
115478
Country
Russian Federation
Facility Name
Samara Region Clinical Hospital M.I. Kalinin
City
Samara
ZIP/Postal Code
443095
Country
Russian Federation
Facility Name
Russian Scientific Research Neurosurgical Institute A.L. Polenov
City
St. Petersburg
ZIP/Postal Code
191104
Country
Russian Federation
Facility Name
Military Medical Academy, Neurosurgery Dept
City
St. Petersburg
ZIP/Postal Code
194044
Country
Russian Federation
Facility Name
Hospital de Cruces
City
Baracaldo
ZIP/Postal Code
48903
Country
Spain
Facility Name
Hospital Universitario Vall d'Hebron
City
Barcelona
ZIP/Postal Code
08035
Country
Spain
Facility Name
Hospital Doce de Octubre
City
Madrid
ZIP/Postal Code
28041
Country
Spain
Facility Name
Hospital Universitario Marqués de Valdecilla
City
Santander
ZIP/Postal Code
39008
Country
Spain
Facility Name
Hospital Universitario Virgen del Rocío
City
Sevilla
ZIP/Postal Code
41013
Country
Spain
Facility Name
China Medical University Hospital
City
Taichung
ZIP/Postal Code
404
Country
Taiwan
Facility Name
Taichung Veterans General Hospital
City
Taichung
ZIP/Postal Code
407
Country
Taiwan
Facility Name
Tri-Service General Hospital
City
Taipei City
ZIP/Postal Code
114
Country
Taiwan
Facility Name
Edinburgh Centre for Neuro-Oncology, Western General Hospital
City
Edinburgh
ZIP/Postal Code
EH42XU
Country
United Kingdom
Facility Name
The National Hospital for Neurology and Neurosurgery
City
London
ZIP/Postal Code
WC1N 3BG
Country
United Kingdom

12. IPD Sharing Statement

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Efficacy and Safety of AP 12009 in Patients With Recurrent or Refractory Anaplastic Astrocytoma or Secondary Glioblastoma

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