Publication | Open Access
Kindlin 2 promotes breast cancer invasion via epigenetic silencing of the microRNA200 gene family
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Citations
29
References
2013
Year
Breast OncologyGeneticsFocal Adhesion ProteinMicrorna200 Gene FamilyCancer BiologyEpigeneticsKindlin 2Tumor BiologyEpigenetic SilencingSignaling PathwayCell SignalingGene ExpressionMicrorna DetectionCell BiologyTumor MicroenvironmentCell-matrix InteractionBreast Cancer InvasionBreast CancerTumor SuppressorSystems BiologyMedicine
Kindlin 2, as a focal adhesion protein, controls integrin activation and regulates Wnt signaling in an integrin-binding independent manner. However, the association of Kindlin 2 with cancer-related microRNAs is unknown. Here, we report that Kindlin 2 markedly downregulates the expression of miR-200 family by inducing CpG island hypermethylation. Mechanistically, Kindlin 2 forms a complex with DNMT3A in the cell nucleus and the two proteins co-occupy the promoter of miRNA-200b. Functionally, repression of miR-200b is required for Kindlin 2-induced breast cancer cell invasion and tumor formation. Our data indicate that Kindlin 2 plays a novel role in epigenetic repression of miR-200 family, a mechanism that promotes breast cancer invasion.
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