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ID
Source
Brief title
Health condition
Glioma
Sponsors and support
Intervention
Outcome measures
Primary outcome
Hypothesis 1: glioma growth and peritumor oscillatory activity
Hypothesis 2: (peritumor) oscillatory activity and NLGN3 expression
Secondary outcome
Not applicable
Background summary
Glioma is a devastating and lethal type of cancer, which has proven difficult to grasp mechanistically and impossible to treat up to now. Most neuro-oncological research into biomarkers and treatment targets focuses on properties of the glioma itself, to no avail. Recent animal studies showed that glioma growth may be determined by the activity of the surrounding tissue. Higher activity of neurons surrounding a glioma in an animal model causes an acceleration of glioma growth through increased neuroligin-3 (NLGN3) expression. In the current study we evaluate two hypotheses: 1) higher oscillatory activity relates to faster subsequent glioma growth and 2) lower global oscillatory activity of the electroencephalography (EEG), besides magnetoencephalography (MEG), also reflects lower NLGN3 expression of the resected tumor tissue. The first hypothesis will be evaluated in retrospective data of ~50 histopathologically confirmed glioma patients. Tumor growth will be quantified as the difference in tumor size on T1 MRI scans acquired around the MEG recording (t0) and clinical follow up (t1). In grade II and III glioma, this clinical follow up is usually six months, while glioblastoma patients undergo radiological assessment every three months. Peritumor oscillatory activity will be extracted from the MEG using the Automated Anatomical Labeling (AAL) atlas and calculated as broadband power (0.5-48 Hz). To evaluate the second hypothesis, 35 patients with glioma will be included and MEG/EEG registration will be performed within 4-8 weeks after (re)resection. Oscillatory activity will be determined as peritumor (as previously described) and global broadband power. Tissue from each resection will be requested from the pathology department and NLGN3 expression will be semi-quantitatively categorized as low, moderate or high NLGN3 expression after treatment with the primary antibody (mouse monoclonal, ab186307, Abcam, Cambridge, UK) against NLGN3. To test our second hypothesis regression analysis with EEG global oscillatory activity as the dependent variable and NLGN3 expression as the independent variable will be performed, including tumor grade, molecular subtype (if available), presence of epilepsy, and tumor volume at t0 as covariates. The results of the current study can be the first step a larger, international study to evaluate the sensitivity and specificity of oscillatory activity as a biomarker for progression of glioma.
Study objective
1) higher oscillatory activity relates to faster subsequent glioma growth and 2) lower global oscillatory activity of the EEG also reflects lower NLGN3 expression of the resected tumor tissue
Study design
MEG/EEG recording will be performed 4-8 weeks after (re)resection
Intervention
Not applicable
Inclusion criteria
Adults (≥ 18 years), glioma confirmed on radiological assessment and/or histopathology
Exclusion criteria
Psychiatric disease or symptoms, other comorbidities of the central nervous system (particularly cerebrovascular accidents, multiple sclerosis, Alzheimer’s disease), insufficient mastery of the Dutch language, inability to communicate adequately
Design
Recruitment
IPD sharing statement
Plan description
Followed up by the following (possibly more current) registration
Other (possibly less up-to-date) registrations in this register
No registrations found.
In other registers
Register | ID |
---|---|
NTR-new | NL7769 |
CCMO | NL49485.029.14 |
OMON | NL-OMON55895 |