Knockdown of AKT3 Activates HER2 and DDR Kinases in Bone-Seeking Breast Cancer Cells, Promotes Metastasis In Vivo and Attenuates the TGFβ/CTGF Axis.
Nico HinzAnke BaranowskyMichael HornMalte KriegsFreya SibbertsenDaniel J SmitPhilippe ClézardinTobias LangeThorsten SchinkeManfred JückerPublished in: Cells (2021)
Bone metastases frequently occur in breast cancer patients and lack appropriate treatment options. Hence, understanding the molecular mechanisms involved in the multistep process of breast cancer bone metastasis and tumor-induced osteolysis is of paramount interest. The serine/threonine kinase AKT plays a crucial role in breast cancer bone metastasis but the effect of individual AKT isoforms remains unclear. Therefore, AKT isoform-specific knockdowns were generated on the bone-seeking MDA-MB-231 BO subline and the effect on proliferation, migration, invasion, and chemotaxis was analyzed by live-cell imaging. Kinome profiling and Western blot analysis of the TGFβ/CTGF axis were conducted and metastasis was evaluated by intracardiac inoculation of tumor cells into NOD scid gamma (NSG) mice. MDA-MB-231 BO cells exhibited an elevated AKT3 kinase activity in vitro and responded to combined treatment with AKT- and mTOR-inhibitors. Knockdown of AKT3 significantly increased migration, invasion, and chemotaxis in vitro and metastasis to bone but did not significantly enhance osteolysis. Furthermore, knockdown of AKT3 increased the activity and phosphorylation of pro-metastatic HER2 and DDR1/2 but lowered protein levels of CTGF after TGFβ-stimulation, an axis involved in tumor-induced osteolysis. We demonstrated that AKT3 plays a crucial role in bone-seeking breast cancer cells by promoting metastatic potential without facilitating tumor-induced osteolysis.
Keyphrases
- signaling pathway
- cell proliferation
- breast cancer cells
- bone mineral density
- induced apoptosis
- soft tissue
- protein kinase
- bone loss
- small cell lung cancer
- high glucose
- transforming growth factor
- pi k akt
- bone regeneration
- high resolution
- type diabetes
- epithelial mesenchymal transition
- postmenopausal women
- drug induced
- south africa
- small molecule
- metabolic syndrome
- endothelial cells
- young adults
- risk assessment
- single cell
- binding protein