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G3BP1-linked mRNA partitioning supports selective protein synthesis in response to oxidative stress

Nucleic Acids Res. 2020-05; 
Syam Prakash Somasekharan, Fan Zhang, Neetu Saxena, Jia Ni Huang, I-Chih Kuo, Caitlin Low, Robert Bell, Hans Adomat, Nikolay Stoynov, Leonard Foster, Martin Gleave, Poul H Sorensen
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Recombinant Proteins … and cycloheximide were from Sigma; DMEM without L-lysine and L-arginine was from Caisson Labs (USA); 13C6-arginine and D4- lysine were from Silantes; FluorSave was from Merck; and G3BP1-APEX and CTRL-APEX constructs were custom made from GenScript Get A Quote

摘要

Cells limit energy-consuming mRNA translation during stress to maintain metabolic homeostasis. Sequestration of mRNAs by RNA binding proteins (RBPs) into RNA granules reduces their translation, but it remains unclear whether RBPs also function in partitioning of specific transcripts to polysomes (PSs) to guide selective translation and stress adaptation in cancer. To study transcript partitioning under cell stress, we catalogued mRNAs enriched in prostate carcinoma PC-3 cell PSs, as defined by polysome fractionation and RNA sequencing (RNAseq), and compared them to mRNAs complexed with the known SG-nucleator protein, G3BP1, as defined by spatially-restricted enzymatic tagging and RNAseq. By comparing these comp... More

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