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ShcA signalling is essential for tumour progression in mouse models of human breast cancer.
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The ShcA PTB domain functions as a biological sensor of phosphotyrosine signaling during breast cancer progression.
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Receptor tyrosine kinase signaling favors a protumorigenic state in breast cancer cells by inhibiting the adaptive immune response.
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The ShcA adaptor protein is a critical regulator of breast cancer progression.
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Integration of Distinct ShcA Signaling Complexes Promotes Breast Tumor Growth and Tyrosine Kinase Inhibitor Resistance.
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Interplay between ShcA Signaling and PGC-1α Triggers Targetable Metabolic Vulnerabilities in Breast Cancer.
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Multiple anti-tumor programs are activated by blocking BAD phosphorylation.
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Targeting fatty acid oxidation enhances response to HER2-targeted therapy.
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Elevated expression of wildtype RhoC promotes ErbB2- and Pik3ca-induced mammary tumor formation.
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USP22 overexpression fails to augment tumor formation in MMTV-ERBB2 mice but loss of function impacts MMTV promoter activity.
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Ezh2 promotes mammary tumor initiation through epigenetic regulation of the Wnt and mTORC1 signaling pathways.
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Dissecting metastasis using preclinical models and methods.
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HER2-driven breast cancer suppression by the JNK signaling pathway.
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RAC1B function is essential for breast cancer stem cell maintenance and chemoresistance of breast tumor cells.
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Elevated expression of DecR1 impairs ErbB2/Neu-induced mammary tumor development.
Mol Cell Biol. 2007 Sep;27(18):6361-71. doi: 10.1128/MCB.00686-07. Epub 2007 Jul 16.
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Combinatorial ShcA docking interactions support diversity in tissue morphogenesis.
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Differential regulation of MAP kinase signalling by dual-specificity protein phosphatases.
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Insights from transgenic mouse models of ERBB2-induced breast cancer.
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Screening for PTB domain binding partners and ligand specificity using proteome-derived NPXY peptide arrays.
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Beta 4 integrin amplifies ErbB2 signaling to promote mammary tumorigenesis.
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Do myoepithelial cells hold the key for breast tumor progression?
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A quantitative protein interaction network for the ErbB receptors using protein microarrays.
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