Abstract
Bcl-w a pro-survival member of the Bcl-2 protein family, is expressed in a variety of cancer types, including gastric and colorectal adenocarcinomas, as well as glioblastoma multiforme (GBM), the most common and lethal brain tumor type. Previously, we demonstrated that Bcl-w is upregulated in gastric cancer cells, particularly those displaying infiltrative morphology. These reports propose that Bcl-w is strongly associated with aggressive characteristic, such as invasive or mesenchymal phenotype of GBM. However, there is no information from studies of the role of Bcl-w in GBM. In the current study, we showed that Bcl-w is upregulated in human glioblastoma multiforme (WHO grade IV) tissues, compared with normal and glioma (WHO grade III) tissues. Bcl-w promotes the mesenchymal traits of glioblastoma cells by inducing vimentin expression via activation of transcription factors, β-catenin, Twist1 and Snail in glioblastoma U251 cells. Moreover, Bcl-w induces invasiveness by promoting MMP-2 and FAK activation via the PI3K-p-Akt-p-GSK3β-β-catenin pathway. We further confirmed that Bcl-w has the capacity to induce invasiveness in several human cancer cell lines. In particular, Bcl-w-stimulated β-catenin is translocated into the nucleus as a transcription factor and promotes the expression of target genes, such as mesenchymal markers or MMPs, thereby increasing mesenchymal traits and invasiveness. Our findings collectively indicate that Bcl-w functions as a positive regulator of invasiveness by inducing mesenchymal changes and that trigger their aggressiveness of glioblastoma cells.
Highlights
Bcl-w (B cell lymphoma-w), is expressed in a variety of cancer types, including glioblastoma multiforme (GBM) and colorectal adenocarcinomas, as well as gastric cancers [1]
Bcl-w is upregulated in glioblastomamultiforme tissues Notably, Bcl-w expression was upregulated in GBM tissues (WHO grades IV), compared with normal and glioma grade III tissues in all patients examined (Figure 1A)
PI3K/Akt and β-catenin/TCF-4 signaling pathways have been reported to play important roles in Epithelial-mesenchymal transition (EMT) and cancer progression [17,18,19]. In view of these data, we hypothesized that Bcl-w upregulates mesenchymal-related genes and plays a crucial role in acquisition of mesenchymal traits via stimulation of the PI3KAkt-β-catenin-TCF-4 pathway
Summary
Bcl-w (B cell lymphoma-w), is expressed in a variety of cancer types, including GBM and colorectal adenocarcinomas, as well as gastric cancers [1]. GBM is difficult to treat using the conventional therapeutic options of standard surgical resection, radiation and chemotherapy, owing to its high frequency of recurrence [2], as well as is related to the upregulation of Bcl-w [3], MMP-2 (matrix metalloproteinase-2) [4,5,6,7] and β-catenin [8]. This cancer type is highly proliferative and exhibits mesenchymal characteristics, leading to tumor progression through acquisition of invasive or metastatic potential. Based on the current findings, we conclude that Bcl-w is critical for malignancy by functioning as a positive regulator of mesenchymal traits and invasion, and contribute significantly to a more comprehensive understanding of the tissue-specific role of Bcl-w in GBM
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