Study of Sunitinib Before and During Radiotherapy in Newly Diagnosed Biopsy-only Glioblastoma Patients
NCT ID: NCT01100177
Last Updated: 2013-03-11
Study Results
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Basic Information
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COMPLETED
PHASE2
12 participants
INTERVENTIONAL
2009-06-30
2012-01-31
Brief Summary
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Detailed Description
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Glioblastoma (GB) is the most frequent brain tumour. Standard treatment after surgical resection is radiation therapy with Temozolomide. But patients who can afford only a biopsy of their lesion due to the location in eloquent areas of their tumour or multifocality, don't get benefit from such treatment and their median survival is in the best case of only 9 months. These patients constitute 30% of Glioblastomas. Clinical trials in this setting are required as patients should be treated immediately after the biopsy to prevent neurological deterioration.
These patients are ideal to test new promising therapies. Their survival is similar to recurrent patients. The evaluation of response is easier as it's possible to avoid the confounding post-surgical changes that interfere with the evaluation of treatment efficacy in terms of tumour size reduction.. Furthermore, neo adjuvant treatment before radiotherapy has shown not to worsen their survival.
Glioblastoma is a tumour rich in molecular abnormalities. PDGFRs are important in growth signalling pathways and neoangiogenesis of gliomas. PDGF ligands and PDGFR-alfa are expressed in most human gliomas, while PDGFR-beta is expressed in glioma cells and tumor endothelial cells, PDFGR-α is expressed in most human gliomas. Imatinib mesylate exhibited antiglioma activity in preclinical studies, sensitizes glioma cells to radiation injury, and combined with hydroxyurea has shown promising results in the recurrent setting.
Moreover gliomas are among the most angiogenic cancers. VEGF/VEGFR-2 is the most prominent angiogenic signalling pathway. Its inhibition either by a neutralizing anti-VEGF antibody, anti-sense VEGF constructs, expression of a dominant-negative mutant form of VEGFR-2 (a specific small molecule inhibitor of the VEGFR-2 tyrosine kinase) or neutralizing anti-VEGFR-2 antibody has resulted in suppression of experimental malignant glioma growth. VEGF has been the focus in the development of glioma-targeted therapies. Recently Bevacizumab has shown to be active in phase II studies.
For these reasons, Sunitinib seems to be a promising treatment fo The objective of this proposal is to evaluate the clinical activity of Sunitinib as first line therapy in patients who have measurable disease and to evaluate the safety of Sunitinib with radiation therapy.
Conditions
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Study Design
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NON_RANDOMIZED
SINGLE_GROUP
TREATMENT
NONE
Study Groups
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Sunitinib plus radiothery
* Sunitinib at doses of 37.5mg/m2/daily in a continuous dosing during 8 weeks.
* After evaluation of efficacy, they will receive Sunitinib 37.5 mg/d and treatment with Radiation therapy (total dose 60 Gy).
* After radiation therapy, Sunitinib al 37.5 mg/d will be continued until progression.
Sunitinib
Sunitinib 37.5mg/m2/d
Radiation
Radiation therapy (60Gy) 2 Gy per day during 30 days
Interventions
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Sunitinib
Sunitinib 37.5mg/m2/d
Radiation
Radiation therapy (60Gy) 2 Gy per day during 30 days
Eligibility Criteria
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Inclusion Criteria
2. Measurable disease and with contrast capture of 2cm
3. Stable doses of DXM during the week before the inclusion
4. Performance status 0-1-2
5. Age \< 75 years
6. MMS \> 25/30
7. Barthel index \> 50%
8. Surgical incision must have healed before the inclusion
9. Basal MRI done 3 weeks at the most before the beginning of the treatment which has specified conditions at the protocol.
10. FEVI \> 50%
11. Suitable medullar reserve (neutrophils \_2000x109/L, platelets \_ 100x109/L, Haemoglobin \_ 10 g/dl.)
12. Not previous chemotherapy or radiation treatment.
13. Creatinin \< 1,5 times the superior standard limit of the laboratory in charged of the analysis.
14. Serum Bilirubin \< 1, 5/ULN, SGOT y SGPT \_ 2,5 times the superior standard limit of the laboratory in charged of the analysis. Serum alkaline phosphatases \< 3/ULN.
15. Effective contraception method in patients and their couple.
16. Informed consent.
Exclusion Criteria
2. Less than 5 years time from any previous infiltrant neoplasia
3. Serious Cerebral haemorrhage after biopsy
4. Anticomital treatment inducting / inhibiting the CYP3A4 enzyme: fenitoin, carbamacepzin, phenobarbitone or other drugs that interact with sunitinib metabolism and that could not be replaced by another drug without interactions with Sunitinib.
5. Pregnancy or lactation.
6. Active or not controlled cardiovascular disease such as hypertension, angor instable, cardiac congestive failure IInd degree (NYHA), cardiac arrhythmia, previous myocardium heart attack, up to 1 year before the randomization
7. Currently treatment established with therapeutic doses of derivated anticoagulants of coumarin (coumarin, warfarin) or a week before the beginning of sunitinib. The administration of heparins of low molecular weight for TVP's control is allowed
8. Patient with TVP
9. HTA with higher values than 150/100 and not controllable with antihypertensive standard drugs
10. Not healed scars, sores or bone fractures
11. Hemorrhagic diathesis or coagulate illnesses
18 Years
75 Years
ALL
No
Sponsors
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Grupo Español de Investigación en Neurooncología
OTHER
Responsible Party
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Principal Investigators
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Carmen Balaña, Coordiantor
Role: STUDY_CHAIR
Hospital Germans Trias i Pujol, Badalona, Spain
Locations
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Grupo Español de Investigacion en Neurooncologia
Madrid, Madrid, Spain
Countries
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Related Links
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Related Info
Other Identifiers
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GENOM-008
Identifier Type: -
Identifier Source: org_study_id
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