4.4 Article

Bladder cancer cell lines adapt their aggressiveness profile to oxygen tension

Journal

ONCOLOGY LETTERS
Volume 24, Issue 1, Pages -

Publisher

SPANDIDOS PUBL LTD
DOI: 10.3892/ol.2022.13341

Keywords

hypoxia; proliferation; migration; extracellular matrix; angiogenesis; cell death

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The hypoxic condition during tumor growth has a significant impact on the survival and migration properties of bladder cancer cells. Low-grade bladder cancer cells tend to become more aggressive under hypoxic culture conditions, while high-grade cells tend to exhibit less aggressive characteristics. Hypoxia greatly alters the properties of bladder cancer cells, including matrix metalloproteinases expression and metabolic changes. Studying bladder cancer cells in hypoxic environments is vital for translating in vitro findings to an in vivo context.
During the process of tumor growth, cancer cells will be subjected to intermittent hypoxia. This results from the delay in the development of the vascular network in relation to the proliferation of cancer cells. The hypoxic nature of a tumor has been demonstrated as a negative factor for patient survival. To evaluate the impact of hypoxia on the survival and migration properties of low and high-grade bladder cancer cell lines, two low-grade (MGHU-3 and SW-780) and two high-grade (SW-1710 and T24) bladder cancer cell lines were cultured in normoxic (20% O-2) or hypoxic atmospheric conditions (2% O-2). The response of bladder cancer cell lines to hypoxic atmospheric cell culture conditions was examined under several parameters, including epithelial-mesenchymal transition, doubling time and metabolic activities, thrombospondin-1 expression, whole Matrix Metallo-Proteinase activity, migration and resistance to oxidative stress. The low-grade cell line response to hypoxia was heterogeneous even if it tended to adopt a more aggressive profile. Hypoxia enhanced migration and pro-survival properties of MGHU-3 cells, whereas these features were reduced for the SW-780 cell line cultured under low oxygen tension. The responses of tested high-grade cell lines were more homogeneous and tended to adopt a less aggressive profile. Hypoxia drastically changed some of the bladder cancer cell line properties, for example matrix metalloproteinases expression for all cancer cells but also switch in glycolytic metabolism of low grade cancer cells. Overall, studying bladder cancer cells in hypoxic environments are relevant for the translation from in vitro findings to in vivo context.

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