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RKIP and HMGA2 regulate breast tumor survival and metastasis through lysyl oxidase and syndecan-2.

Oncogene. 2014; 
Sun M, Gomes S, Chen P, Frankenberger CA, Sankarasharma D, Chung CH, Chada KK, Rosner MR.
Products/Services Used Details Operation
PCR Cloning and Subcloning Cloning of luciferase reporter plasmid, pMSCVPIG-miR-200b plasmid and luciferase reporter assay Wild-type (LOX-wt-UTR) and mutated (LOX-mut-UTR) 3’UTR fragment (Figure 3c) from the human LOX gene were designed using TargetScanS program21 and synthesized by GenScript.... The miR-200b precursor was synthesized by GenScript and was then ligated into the pMSCVPIG vector at XhoI/EcoRI sites. Get A Quote

摘要

Elucidating targets of physiological tumor metastasis suppressors can highlight key signaling pathways leading to invasion and metastasis. To identify downstream targets of the metastasis suppressor Raf-1 kinase inhibitory protein (RKIP/PEBP1), we utilized an integrated approach based upon statistical analysis of tumor gene expression data combined with experimental validation. Previous studies from our laboratory identified the architectural transcription factor and oncogene, high mobility group AT-hook 2 (HMGA2), as a target of inhibition by RKIP. Here we identify two signaling pathways that promote HMGA2-driven metastasis. Using both human breast tumor cells and an MMTV-Wnt mouse breast tumor model, we show ... More

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