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Abstract By using human melanoma and glioblastoma cell lines and their derivative BCL-X L overexpressing clones, we investigated the role of BCL-X L in aggressive features of these two tumor histotypes. We found that in both models, BCL-X L overexpression increased in vitro cell migration and invasion and facilitated tumor cells to form de novo vasculogenic structures. Furthermore, BCL-X L overexpressing cells exhibited higher tumors sphere formation capacity and expressed higher levels of some stem cell markers, supporting the concept that BCL-X L plays essential roles in the maintenance of cancer stem cell phenotype. BCL-X L expression reduction by siRNA, the exposure to a BCL-X L -specific inhibitor and the use of a panel of human melanoma cell lines corroborated the evidence that BCL-X L regulates tumor progression-associated properties. Finally, the vascular markers and the vasculogenic mimicry were up-regulated in the BCL-X L overexpressing xenografts derived from both tumor histotypes. In conclusion, our work brings further support to the understanding of the malignant actions of BCL-X L and, in particular, to the concept that BCL-X L promotes stemness and contributes to the aggressiveness of both melanoma and glioblastoma.
Trisciuoglio et al. (Wed,) studied this question.
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