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Cross-talk between alternatively spliced ugt1a isoforms and colon cancer cell metabolism

Molecular Pharmacology. 2017; 
Yannick Audet-Delage, Michèle Rouleau, Mélanie Rouleau, Joannie Roberge, Stéphanie Miard, Frédéric Picard, Bernard Têtu and Chantal Guillemette
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PCR Cloning and Subcloning Primary antibodies were anti-PKM2 (1:500, #3198S; Cell Signaling, Danvers, MA) and the custom mouse monoclonal anti-i2s (1:100, #4C5E7; GenScript, Piscataway, NJ) described by Rouleau et al. (2016). Get A Quote

摘要

Alternative splicing at the human glucuronosyltransferase 1 gene locus (UGT1) produces alternate isoforms UGT1A_i2s that control glucuronidation activity through protein-protein interactions. Here, we hypothesized that UGT1A_i2s function as a complex protein network connecting other metabolic pathways with an influence on cancer cell metabolism. This is based on a pathway enrichment analysis of proteomic data that identified several high-confidence candidate interaction proteins of UGT1A_i2 proteins in human tissues—namely, the rate-limiting enzyme of glycolysis pyruvate kinase (PKM), which plays a critical role in cancer cell metabolism and tumor growth. The partnership of UGT1A_i2 and PKM2 was confirmed by ... More

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