AI Article Synopsis
- Triple negative breast cancer (TNBC) is highly aggressive and varies significantly in its characteristics and treatment responses, with the Akt signaling pathway being a key target for therapy.
- Research indicates that Vav1 can down-regulate the Akt2 isoform in TNBC cells by increasing levels of miR-29b, which may help reduce tumor spread to the lungs.
- This Vav1/miR-29b mechanism varies across different TNBC tumors and may improve tumor classification and lead to more effective, tailored treatments for patients resistant to existing therapies.
Article Abstract
Triple negative breast cancer (TNBC) represents the most aggressive breast tumor, showing a high intrinsic variability in terms of both histopathological features and response to therapies. Blocking the Akt signaling pathway is a well-studied approach in the treatment of aggressive breast tumors. The high homology among the Akt isoforms and their distinct, and possibly opposite, oncogenic functions made it difficult to develop effective drugs. Here we investigated the role of Vav1 as a potential down-regulator of individual Akt isozymes. We revealed that the over-expression of Vav1 in triple negative MDA-MB-231 cells reduced only the Akt2 isoform, acting at the post-transcriptional level through the up-modulation of miR-29b. The Vav1/miR-29b dependent decrease in Akt2 was correlated with a reduced lung colonization of circulating MDA-MB-231 cells. In cell lines established from PDX, the Vav1 induced down-modulation of Akt2 is strongly dependent on miR-29b and occurs only in some TNBC tumors. These findings may contribute to better classify breast tumors having the triple negative phenotype, and suggest that the activation of the Vav1/miR-29b axis, precisely regulating the amount of an Akt isozyme crucial for tumor dissemination, could have great potential for driving more accurate therapies to TNBCs, often not eligible or resistant to treatments.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9224635 | PMC |
| http://dx.doi.org/10.3390/jpm12060993 | DOI Listing |
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