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Article Abstract

The Δ133p53β isoform is increased in many primary tumors and has many tumor-promoting properties that contribute to increased proliferation, migration and inflammation. Here we investigated whether Δ133p53β contributed to some of the most aggressive tumors that had metastasized to the brain. mRNA expression was measured in lung, breast, melanoma, colorectal metastases and, where available, the matched primary tumor. The presence of expression was associated with the time for the primary tumor to metastasize and overall survival once the tumor was detected in the brain. was present in over 50% of lung, breast, melanoma and colorectal metastases to the brain. It was also increased in the brain metastases compared with the matched primary tumor. Brain metastases with expressed were associated with a reduced time for the primary tumor to metastasize to the brain compared with tumors with no expression. In-vitro-based analyses in Δ133p53β-expressing cells showed increased cancer-promoting proteins on the cell surface and increased downstream p-AKT and p-MAPK signaling. Δ133p53β-expressing cells also invaded more readily across a mock blood-brain barrier. Together these data suggested that Δ133p53β contributes to brain metastases by making cells more likely to invade the brain.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9866425PMC
http://dx.doi.org/10.3390/ijms24021267DOI Listing

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