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Fbxo4-mediated degradation of Fxr1 suppresses tumorigenesis in head and neck squamous cell carcinoma.

Nat Commun. 2017; 
Qie S, Majumder M,, Mackiewicz K, Howley BV, Peterson YK, Howe PH, Palanisamy V,, Diehl JA.
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Catalog Antibody The same amounts of cell lysate were applied in immunoprecipitation using Flag af?nity gel, anti-c-Myc agarose af?nity gel (A7470, Sigma-Aldrich) or anti-His af?nity resin (L00439, GenScript). Get A Quote

摘要

The Fbxo4 tumour suppressor is a component of an Skp1-Cul1-F-box E3 ligase for which two substrates are known. Here we show purification of SCFFbxo4 complexes results in the identification of fragile X protein family (FMRP, Fxr1 and Fxr2) as binding partners. Biochemical and functional analyses reveal that Fxr1 is a direct substrate of SCFFbxo4. Consistent with a substrate relationship, Fxr1 is overexpressed in Fbxo4 knockout cells, tissues and in human cancer cells, harbouring inactivating Fbxo4 mutations. Critically, in head and neck squamous cell carcinoma, Fxr1 overexpression correlates with reduced Fbxo4 levels in the absence of mutations or loss of mRNA, suggesting the potential?for feedback regulation. ... More

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