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pmid: 32413989
pmc: PMC7281538
handle: 10261/212546 , 20.500.12530/82651 , 10486/703008 , 10902/19263 , 20.500.12105/11010
pmid: 32413989
pmc: PMC7281538
handle: 10261/212546 , 20.500.12530/82651 , 10486/703008 , 10902/19263 , 20.500.12105/11010
Adaptation to hypoxia is a common feature in solid tumors orchestrated by oxygen-dependent and independent upregulation of the hypoxia-inducible factor-1α (HIF-1α). We unveiled that G protein-coupled receptor kinase (GRK2), known to be overexpressed in certain tumors, fosters this hypoxic pathway via phosphorylation of the mRNA-binding protein HuR, a central HIF-1α modulator. GRK2-mediated HuR phosphorylation increases the total levels and cytoplasmic shuttling of HuR in response to hypoxia, and GRK2-phosphodefective HuR mutants show defective cytosolic accumulation and lower binding to HIF-1α mRNA in hypoxic Hela cells. Interestingly, enhanced GRK2 and HuR expression correlate in luminal breast cancer patients. GRK2 also promotes the HuR/HIF-1α axis and VEGF-C accumulation in normoxic MCF7 breast luminal cancer cells and is required for the induction of HuR/HIF1-α in response to adrenergic stress. Our results point to a relevant role of the GRK2/HuR/HIF-1α module in the adaptation of malignant cells to tumor microenvironment-related stresses.
GRK2 Gene, HeLa Cell Line, GRK2, mRNA regulation, Gene, Article, Protein Phosphorylation, breast cancer, Breast cancer, β-adrenergic signaling, Breast Cancer, HIF1α, HIF1 alpha, Hypoxia, Epithelium Cell, [beta]-Adrenergic Signaling, hypoxia, BREAST-CANCER CELLS, HuR Gene, HIF1[alfa], Biología y Biomedicina / Biología, VEGF, Nucleocytoplasmic Shuttling, MCF-7 Cell Line, HuR, Nucleocytoplasmic shuttling, beta-adrenergic signaling, mRNA Regulation, Protein Binding, nucleocytoplasmic shuttling
GRK2 Gene, HeLa Cell Line, GRK2, mRNA regulation, Gene, Article, Protein Phosphorylation, breast cancer, Breast cancer, β-adrenergic signaling, Breast Cancer, HIF1α, HIF1 alpha, Hypoxia, Epithelium Cell, [beta]-Adrenergic Signaling, hypoxia, BREAST-CANCER CELLS, HuR Gene, HIF1[alfa], Biología y Biomedicina / Biología, VEGF, Nucleocytoplasmic Shuttling, MCF-7 Cell Line, HuR, Nucleocytoplasmic shuttling, beta-adrenergic signaling, mRNA Regulation, Protein Binding, nucleocytoplasmic shuttling
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| impulse This indicator reflects the initial momentum of an article directly after its publication, based on the underlying citation network. | Top 10% |
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