Brain Tumors Clinical Trial
Official title:
Establishment of a Signature of Circulating microRNA as a Tool to Aid Diagnosis of Primary Brain Tumors in Adults
MIRNA is a prospective multi-center observational study designed to explore 762 plasma microRNAs in patients with malignant CNS tumours: 60 primary glioblastoma (GBM), 20 primary CNS lymphomas and 40 brain metastases in an attempt to establish plasma microRNA signatures specific to GBM capable of distinguishing them from malignant non-glial brain tumours. 20 patients with cerebral stroke and 20 healthy volunteers will also participate in the study, and for each patient, a panel of 762 microRNAs will be screened in plasma.
Neuro-oncology faces two challenges: establishing an accurate, rapid diagnosis and having
early therapeutic response. This applies particularly to glioblastoma (GBM) since the
positive diagnosis is evoked on MRI imaging and the diagnosis of certainty provided by
anatomopathology. There are no perfect techniques and there are problems of differential
diagnosis in imaging. Sometimes the context does not allow biopsy or excision.
This study is a prospective multi-center observational study designed to be conducted in
patients with malignant CNS tumours: primary glioblastoma (60 GBM), primary CNS lymphomas (20
PCNSL), brain metastases (40 BM), in an attempt to establish plasma microRNA signatures
characteristic of a tumour process. Patients with cerebral stroke (20 CS) and healthy
volunteers (20 HV) will also participate in the study. For each patient, a panel of 762
microRNAs will be screened in plasma.
First, the investigators will focus on the potentially diagnostic nature of the signature,
which may prove useful when there are problems of differential diagnosis in imaging or when
the context does not permit biopsy or excision. The main objective of the study is to
establish a plasma microRNA signature specific to GBM, capable of distinguishing them from
malignant non-glial brain tumours (PCNSL and BM). Within the main objective, discrimination
will be established between GBM and malignant non-glial brain tumours.
Secondly, the quantitative approach of plasma miRNoma with 752 microRNAs studied in the
different patient groups will allow for other objectives:1/ Establish plasma microRNA
signatures characteristic of other types of brain tumours; 2/ Identify a plasma microRNA
signature characteristic of the cerebral injury component independently of the tumor
component with the CS and HV groups; 3/ Identify plasma microRNA signatures characteristic of
GBM subtypes in relation to their genomic alterations; 4/ Establish correlations between
plasma microRNA expression levels and data collected through multi-modality MRI imaging and
anatomopathology.
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