Abstract
Simple SummaryThe estimated survival time for glioblastoma patients is extremely low; only about 5% of patients survive five years post diagnosis. The standard of care for glioblastoma patients involves surgery, radiation therapy, and chemotherapy with temozolomide. However, due to the extremely invasive capability of glioblastoma cells, tumors develop very diffusely, integrating into the healthy brain tissue. Indeed, the separation of healthy brain tissue and the tumor boundaries, by standard surgical microscopy, is very challenging. Therefore, the maximum safe removal of the tumor mass is difficult, leaving some tumor cells behind. Therefore, understanding the molecular mechanisms of tumor cell infiltration and developing anti-invasive approaches are of the utmost priority. Here, we provide a review of the characteristics and molecular mechanisms of glioblastoma invasion, and include a perspective of clinical applications.Glioblastoma is the most common and malignant primary brain tumor, defined by its highly aggressive nature. Despite the advances in diagnostic and surgical techniques, and the development of novel therapies in the last decade, the prognosis for glioblastoma is still extremely poor. One major factor for the failure of existing therapeutic approaches is the highly invasive nature of glioblastomas. The extreme infiltrating capacity of tumor cells into the brain parenchyma makes complete surgical removal difficult; glioblastomas almost inevitably recur in a more therapy-resistant state, sometimes at distant sites in the brain. Therefore, there are major efforts to understand the molecular mechanisms underpinning glioblastoma invasion; however, there is no approved therapy directed against the invasive phenotype as of now. Here, we review the major molecular mechanisms of glioblastoma cell invasion, including the routes followed by glioblastoma cells, the interaction of tumor cells within the brain environment and the extracellular matrix components, and the roles of tumor cell adhesion and extracellular matrix remodeling. We also include a perspective of high-throughput approaches utilized to discover novel players for invasion and clinical targeting of invasive glioblastoma cells.
Highlights
The distant invasion of tumor followed by the Stupp protocol, which is radiotherapy combined with concurrent daily cells to the brain parenchyma, theirbyinfiltration and cooperation with healthy tissue, temozolomide,and followed adjuvant temozolomide treatment
For examthe cores formed more confined tumors with therapy resistance. It was ple, in a recent mouse model established with regionally derived glioblastoma cells, it was uncovered that the core and edge cells exhibited a paracrine crosstalk through soluble demonstrated that cells from thetheir edge formed highly invasive tumors, and cells from thesuch factors to maintain phenotypes
They analyzed the changes in the transcriptional program of glioblastoma cells before and after coculture with iPSC-derived human cerebral organoids, which function as a scaffold for glioblastoma cell invasion [148]
Summary
Taking healthy tissue near theresection tumorisenvironment of decreasing the tumor burden before radiotherapy and chemotherapy, and in reducing during the removal of tumors located in functional areas of the brain or adjacent to the the risk of recurrence. The current treatment for glioblastoma patients is the maximal safe tumor resection nature of glioblastoma cells limits the therapeutic efficacy. The distant invasion of tumor followed by the Stupp protocol, which is radiotherapy combined with concurrent daily cells to the brain parenchyma, theirbyinfiltration and cooperation with healthy tissue, temozolomide,and followed adjuvant temozolomide treatment [4]. Understanding the mechanisms sults for therapy resistance, high recurrence and survival rates, there is no di- of glioblastoma cell invasiveness is of the utmost priority to develop successful therapeutic rected therapy to prevent this invasive behavior [5]. We include a perspective on high-throughput approaches for invasion studies and clinical targeting of invasive cells
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