A slow-cycling subpopulation of melanoma cells with highly invasive properties.

Oncogene. 2018 Jan 18;37(3):302-312. Epub 2017 Sep 18

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摘要

Melanoma is a heterogeneous tumor with different subpopulations showing different proliferation rates. Slow-cycling cells were previously identified in melanoma, but not fully biologically characterized. Using the label-retention method, we identified a subpopulation of slow-cycling cells, defined as label-retaining cells (LRC), with strong invasive properties. We demonstrate through live imaging that LRC are leaving the primary tumor mass at a very early stage and disseminate to peripheral organs. Through global proteome analyses, we identified the secreted protein SerpinE2/protease nexin-1 as causative for the highly invasive potential of LRC in melanomas.

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A slow-cycling subpopulation of melanoma cells with highly invasive properties.

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