AI Article Synopsis
- αB-crystallin is identified as a new oncoprotein in breast cancer, correlating with poor outcomes, and its phosphorylation state has not been thoroughly explored in this context.
- The study reveals that serine 59 is the main phosphorylation site of αB-crystallin in MCF7 breast cancer cells treated with vinblastine, where it is linked to increased apoptosis.
- Overexpression of a mutant form of αB-crystallin that mimics phosphorylation enhances apoptosis in treated cells, while wild-type or non-phosphorylatable variants lead to drug resistance, indicating the potential of targeting phosphorylation to improve cancer therapies.
Article Abstract
The small heat shock protein (sHSP) αB-crystallin is a new oncoprotein in breast carcinoma that predicts poor clinical outcome in breast cancer. However, although several reports have demonstrated that phosphorylation of sHSPs modify their structural and functional properties, the significance of αB-crystallin phosphorylation in cancer cells has not yet been investigated. In this study, we have characterized the phosphorylation status of αB-crystallin in breast epithelial carcinoma cells line MCF7 submitted to anti-cancer agents like vinblastine. We have showed that the main phosphorylation site of αB-crystallin in response to vinblastine is serine 59 and determined a correlation between this post-translational modification and higher apoptosis level. The overexpression of the serine 59 "pseudophosphorylated" mutant (S59E) induces a significant increase in the apoptosis level of vinblastine-treated MCF7 cells. In contrast, overexpression of wild-type αB-crystallin or "nonphosphorylatable" mutant (S59A) result in a resistance to this microtubule-depolymerizing agent, while inhibition of endogenous levels of αB-crystallin by expression of shRNA lowers it. Analyzing further the molecular mechanism of this phenomenon, we report for the first time that phosphorylated αB-crystallin preferentially interacts with Bcl-2, an anti-apoptotic protein, and this interaction prevents the translocation of Bcl-2 to mitochondria. Hence, this study identifies serine 59 phosphorylation as an important key in the down-regulation of αB-crystallin anti-apoptotic function in breast cancer and suggests new strategies to improve anti-cancer treatments.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2988338 | PMC |
| http://dx.doi.org/10.1074/jbc.M110.124388 | DOI Listing |
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