[HTML][HTML] Targeting the transforming growth factor-β pathway inhibits human basal-like breast cancer metastasis
V Ganapathy, R Ge, A Grazioli, W Xie… - Molecular cancer, 2010 - Springer
V Ganapathy, R Ge, A Grazioli, W Xie, W Banach-Petrosky, Y Kang, S Lonning, J McPherson…
Molecular cancer, 2010•SpringerAbstract Background Transforming Growth Factor β (TGF-β) plays an important role in tumor
invasion and metastasis. We set out to investigate the possible clinical utility of TGF-β
antagonists in a human metastatic basal-like breast cancer model. We examined the effects
of two types of the TGF-β pathway antagonists (1D11, a mouse monoclonal pan-TGF-β
neutralizing antibody and LY2109761, a chemical inhibitor of TGF-β type I and II receptor
kinases) on sublines of basal cell-like MDA-MB-231 human breast carcinoma cells that …
invasion and metastasis. We set out to investigate the possible clinical utility of TGF-β
antagonists in a human metastatic basal-like breast cancer model. We examined the effects
of two types of the TGF-β pathway antagonists (1D11, a mouse monoclonal pan-TGF-β
neutralizing antibody and LY2109761, a chemical inhibitor of TGF-β type I and II receptor
kinases) on sublines of basal cell-like MDA-MB-231 human breast carcinoma cells that …
Background
Transforming Growth Factor β (TGF-β) plays an important role in tumor invasion and metastasis. We set out to investigate the possible clinical utility of TGF-β antagonists in a human metastatic basal-like breast cancer model. We examined the effects of two types of the TGF-β pathway antagonists (1D11, a mouse monoclonal pan-TGF-β neutralizing antibody and LY2109761, a chemical inhibitor of TGF-β type I and II receptor kinases) on sublines of basal cell-like MDA-MB-231 human breast carcinoma cells that preferentially metastasize to lungs (4175TR, 4173) or bones (SCP2TR, SCP25TR, 2860TR, 3847TR).
Results
Both 1D11 and LY2109761 effectively blocked TGF-β-induced phosphorylation of receptor-associated Smads in all MDA-MB-231 subclones in vitro. Moreover, both antagonists inhibited TGF-β stimulated in vitro migration and invasiveness of MDA-MB-231 subclones, indicating that these processes are partly driven by TGF-β. In addition, both antagonists significantly reduced the metastatic burden to either lungs or bones in vivo, seemingly independently of intrinsic differences between the individual tumor cell clones. Besides inhibiting metastasis in a tumor cell autonomous manner, the TGF-β antagonists inhibited angiogenesis associated with lung metastases and osteoclast number and activity associated with lytic bone metastases. In aggregate, these studies support the notion that TGF-β plays an important role in both bone-and lung metastases of basal-like breast cancer, and that inhibiting TGF-β signaling results in a therapeutic effect independently of the tissue-tropism of the metastatic cells. Targeting the TGF-β pathway holds promise as a novel therapeutic approach for metastatic basal-like breast cancer.
Conclusions
In aggregate, these studies support the notion that TGF-β plays an important role in both bone-and lung metastases of basal-like breast cancer, and that inhibiting TGF-β signaling results in a therapeutic effect independently of the tissue-tropism of the metastatic cells. Targeting the TGF-β pathway holds promise as a novel therapeutic approach for metastatic basal-like breast cancer.
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