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Spleen Tyrosine Kinase-Mediated Autophagy Is Required for Epithelial-Mesenchymal Plasticity and Metastasis in Breast Cancer.

Cancer Res.. 2019; 
ShindeAparna,HardyShana D,KimDongwook,AkhandSaeed Salehin,JollyMohit Kumar,WangWen-Hung,AndersonJoshua C,KhodadadiRyan B,BrownWells S,GeorgeJason T,LiuSheng,WanJun,LevineHerbert,WilleyChristopher D,KrusemarkCasey J,GeahlenRobert L,WendtMicha
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Peptide Synthesis Briefly, a selective SYK peptide substrate derived from phage display selections (SYKtide, EDPDYEWPSA) was purchased from GenScript on Rink amide polystyrene resin, and the N-terminus was acylated with 6-hexynoic acid. Get A Quote

摘要

The ability of breast cancer cells to transiently transition between epithelial and mesenchymal states contributes to their metastatic potential. Therefore, driving tumor cells into a stable mesenchymal state, as opposed to complete tumor cell eradication, presents an opportunity to pharmacologically limit disease progression by promoting an asymptomatic state of dormancy. Here, we compare a reversible model of epithelial-mesenchymal transition (EMT) induced by TGFβ to a stable mesenchymal phenotype induced by chronic exposure to the ErbB kinase inhibitor lapatinib. Only cells capable of returning to an epithelial phenotype resulted in skeletal metastasis. Gene expression analyses of the two mesenchyma... More

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