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Screening the human miRNA interactome reveals coordinated up-regulation in melanoma, adding bidirectional regulation to miRNA networks

SCIENCE ADVANCES. 2025-01; 
Faezeh Jame-Chenarboo , Joseph N Reyes , Nicholas M Twells , Hoi Hei Ng , Dawn Macdonald , Eva Hernando , Lara K Mahal Department of Chemistry, University of Alberta
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Gene Synthesis CD98hc, ST3GAL1, and ST3GAL2 3′UTRs were amplified via polymerase chain reaction (PCR) from genomic DNA (10 μg; from the MCF-7 cell line: CD98hc) or gene synthesis (GenScript Gene Synthesis Company: ST3GAL1 and ST3GAL2) using the primers shown in table S1. Get A Quote

摘要

Cellular protein expression is coordinated posttranscriptionally by an intricate regulatory network. The current presumption is that microRNAs (miRNAs) work by repression of functionally related targets within a system. In recent work, up-regulation of protein expression via direct interactions of messenger RNA with miRNA has been found in dividing cells, providing an additional mechanism of regulation. Herein, we demonstrate coordinated up-regulation of functionally coupled proteins by miRNA. We focused on CD98hc, the heavy chain of the amino acid transporter LAT-1, and α-2,3-sialyltransferases ST3GAL1 and ST3GAL2, which are critical for CD98hc stability in melanoma. Profiling miRNA regulation using our high-... More

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