4.6 Article

ALK is frequently phosphorylated in Merkel cell carcinoma and associates with longer survival

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PLOS ONE
卷 16, 期 5, 页码 -

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PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0252099

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  1. Jane and Aatos Erkko Foundation [4706147]
  2. Hospital district of Helsinki and Uusimaa [TYH2019225]

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MCC tumor samples frequently exhibit phosphorylated ALK, which correlates with MCPyV positivity, younger age, absence of metastases at diagnosis, and better MCC-specific survival. In contrast, only a small number of MCC cell lines show low ALK phosphorylation, suggesting a disparity in ALK activity between patient derived tumors and cell line samples. Additional studies using more advanced disease models such as xenografts are needed to determine if ALK is a viable treatment target in MCC.
Merkel cell carcinoma (MCC) is a rare skin cancer with only limited therapeutic options for advanced disease. We previously showed that oncogene ALK is frequently expressed at the RNA level in MCC and further that ALK positivity by immunohistochemistry is frequent and correlates strongly with Merkel cell polyomavirus (MCPyV) positivity. In this study, we investigated whether ALK receptor is active in MCC tumor samples and MCC cell lines, and whether ALK would be a prospective treatment target in MCC. We utilized tissue microarrays constructed from 136 primary MCC tumor samples as well as nine previously established MCC cell lines to determine the presence of ALK and phosphorylated ALK (p-ALK) via immunohistochemistry. Almost half of the analyzed MCC tumors displayed ALK phosphorylation (47.8%). Analysis of MCC tumor samples revealed that the presence of p-ALK correlated to MCPyV positivity, younger age, nonexistence of metastases at diagnosis and ultimately to better MCC-specific survival. In contrast to MCC tumor samples only two out of nine MCC cell lines showed only low ALK phosphorylation by immunohistochemistry. Our study reveals clear disparity in ALK activity between patient derived tumors and cell line samples and therefore, more advanced disease models such as xenografts are necessary to resolve whether ALK is a useful treatment target in MCC.

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