GIST cell cycle dysregulation is required for progression to high-risk disease but not for resistance to kinase inhibitors. Homo sapiens
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https://www.ncbi.nlm.nih.gov/bioproject/PRJNA256344
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Background: To understand the transcriptional consequences of a TP53 modulation in the GIST cell context, we treated GIST430 with increasing doses of the MDM2-inhibitor nutlin-3 (racemate). Overall design: In this study, 3’ end RNA Sequencing (3SEQ) was used to expression profile GIST430 cell lines treated with DMSO and Nutlin-3, 2.5µM or 10µM for 18h. Then the gene expression profiles between these concentrations were compared.
创建时间:
2014-07-28



