Examining Cellular Interactions and Response to Chemotherapy in The Glioblastoma Perivascular Niche

Hatlen, Rosalyn Rae

17 January 2023

Glioblastoma multiforme (GBM) is the most deadly and common form of brain cancer and is responsible for over 50% of adult brain tumors. A specific region within the GBM environment is known as the perivascular niche (PVN). We have designed a 3D in vitro model of the PVN comprised of either collagen Type 1 or HyStem-C®, human umbilical vein endothelial cells (HUVECs) or human brain microvascular endothelial cells (HBMECs), and LN229 (GBM) cells. A synergistic response between HUVECs and LN229 cells was observed in co-culture, including 10 – 16-fold increased cell proliferation, a decrease in the height of hydrogels of up to 68%, as well as elevated secretion of TGF-β and CXCL12 up to 2.6-fold from Day 8 to 14. These trends correlated with cell colocalization, indicating a chemotactic role for CXCL12 in enabling the migration of LN229 cells towards HUVECs in co-cultures. Von Willebrand factor (vWF) was co-expressed with glial fibrillary acidic protein (GFAP) in up to 40% of LN229 cells after 14 days in co-culture in collagen (2.2 mg/mL) and HyStem-C® gels. The expression of vWF indicates the early stages of trans-differentiation of LN229 cells to an endothelial cell phenotype. We then investigated the effect of chemotherapeutic drugs temozolomide (TMZ) and Avastin® on EC networks, LN229 cell morphology and alignment, cytotoxicity, colocalization, and trans-differentiation. TMZ was observed to primarily affect LN229 cells, with treatment at high concentrations resulting in up to 2.3-fold reduced alignment as well as an increase in cell circularity. Cytotoxicity of up to 94% was also observed up to in LN229 monocultures, and was significantly higher in collagen (1.1 mg/mL) gels. Avastin® treatment resulted in changes to ECs. Network features were significantly reduced and EC cellular proliferation decreased up to 69% with Avastin® treatment. Significant increases in percentages of colocalized and GFAP+/vWF+ cells were also observed when treated with 8 µg/mL Avastin®. This suggests that chemotactic signaling may have been altered. TGF-β secretion was reduced in co-cultures when 150 µM TMZ or 8 µg/mL Avastin® were administered. / Doctor of Philosophy / Glioblastoma (GBM) is the most common and deadly form of brain cancer and is responsible for over 50% of adult brain tumors. A specific region within the GBM environment of particular interest is located near the vasculature, known as the perivascular niche (PVN). We have designed a 3D in vitro model of the PVN consisting of either collagen type 1 or HyStem-C®, a material made of primarily hyaluronic acid. Human umbilical vein endothelial cells (HUVECs), an immortalized cell line, or primary human brain microvascular endothelial cells (HBMECs) as well as LN229 (GBM) cells were used. A synergistic response was observed between HUVECs and LN229 cells in co-culture, including changes to the extracellular matrix, and signaling factor secretion. Further supporting this data, colocalization between LN229 cells and HUVECs was observed. Colocalization is a phenomenon where two cell types come into physical contact after one moves toward another. This indicated preferential migration, specifically in response to CXCL12. Endothelial cell marker von Willebrand factor (vWF) was co-expressed with glial fibrillary acidic protein (GFAP), commonly used to identify GBM cells. This percentage was increased in co-cultures with HBMECs, pointing to differences in the response of primary cells to immortalized cell lines. The expression of vWF indicates the early stages of trans-differentiation of LN229 cells to an endothelial cell phenotype. We then investigated the effect of chemotherapeutic drugs temozolomide (TMZ) and Avastin® in the PVN model. TMZ was observed to primarily affect LN229 cells, by reducing their alignment as well as causing cell death. Avastin® treatment resulted in changes to ECs. Networks and cell growth were significantly reduced after Avastin® treatment. When either TMZ or Avastin® was administered, the secretion of TGF-β, was reduced.

Glioblastoma

perivascular niche

trans-differentiation

intercellular interactions

chemotherapy

Investigation of Altered Cell-Cell Interactions and Signaling Mechanisms in <i>Drosophila</i> Tumor Models

Waghmare, Indrayani

08 September 2016

No description available.

Biology

Studium mezibuněčných interakcí v nádorech. / Studies of intercellular interactions in tumours

Jechová, Alžběta

January 2019

Beside tumor cells themselves, tumors consist of many non-malignantly transformed cellular elements and an extracellular matrix. This so-called tumor microenvironment, or stroma, significantly influences the biological properties of the tumor through intercellular interactions. In this thesis I have focused on the study of tumor-associated fibroblasts in squamous cell carcinomas of the head and neck, malignant melanoma and glioblastoma. The data show the presence of cells with mesenchymal characteristics, present even in the glioblastoma stroma, which could potentially have a positive effect on proliferative activity and invasiveness of glioblastoma cells. In malignant melanoma, the presence of keratinocytes should also be considered, as they are the major cells of the epidermis influencing tumor melanocytes. The conditioned medium from UVB irradiated keratinocytes and non-irradiated fibroblasts stimulates the invasion of malignant melanoma cells. Targeting the tumor stroma may be a new direction in oncological therapy, so we have focused on the influence of synthetic polyamine on the formation of myofibroblasts, which are an active part of the population of tumor-associated fibroblasts. The tested polyamine prevents the formation of myofibroblasts but has no effect on those already formed nor on...