Brain Tumor Clinical Trial
Official title:
Analysis of Disease Progression and Treatment-Induced Alterations in Glioblastoma - an Integrative Morphological and Molecular Approach
Summary of scientific evidence and rationale of this project:
Integrative molecular-genetic approaches have provided important insights in the biology of
glioblastoma. It has meanwhile become clear, that glioblastoma is not a single tumor entity
but comprises different molecular subtypes, which are associated with a distinct
genetic/epigenetic signature and prognosis. Multimodal treatment approaches combining radio-
and chemotherapy as well as the recent introduction of novel antiangiogenic agents have
resulted in increasing survival times and improved quality-of-life of glioblastoma patients.
Yet, despite these intense treatment efforts the therapeutic efficacy in glioblastoma
patients is limited, leading in virtually all cases to tumor recurrence and death of the
patients.
As only a limited fraction of glioblastoma patients undergo second neurosurgery at tumor
recurrence (< 10%), post-therapeutic samples are rare and no systematic, large-scale studies
exist, which address post-therapeutic morphological and molecular alterations in
glioblastoma tumor tissue. Yet, these data would help to improve the understanding of
mechanisms involved in therapy-resistance and tumor progression, to develop new therapeutic
approaches and could pave the way for personalized treatment strategies.
Objectives of the project:
The aim of this study is to analyze systematically morphological and molecular changes
associated with glioblastoma progression and therapy-resistance in matched pre- and
post-therapeutic glioblastoma samples.
The following primary aims will be addressed:
1. Morphological characterisation of changes in a large series of matched glioblastoma
tissues pertaining to i. Vascularization and hypoxia-mediated factors ii. Tumor
necrosis and chemoradiation-induced necrosis iii. Inflammatory response iv. Tumor
cellularity and proliferation v. Tumor cell phenotype after treatment e.g.
glial-mesenchymal transition
2. Molecular analyses
i. Transcriptomic, DNA methylation and genomic profiling will be performed to detect
changes in gene expression, methylation and copy number aberrations in post-therapeutic
as compared to pre-therapeutic tumor tissue. ii. The relationship between the
transcriptomic, DNA methylation and genomic profiles will be analyzed.
3. Exploratory analysis of associations between morphological and molecular changes in a
screening set of 30 glioblastoma cases (with available fresh frozen tissues at first
and second surgery) and subsequent validation of relevant findings in a larger
glioblastoma cohort (150 cases with matched formalin-fixed paraffin-embedded tissues)
by appropriate methods including immunohistochemistry,
fluorescence-in-situ-hybridization, and sequencing.
4. Special attention will be paid to gender-specific patterns of therapy-related changes
and tumor progression.
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