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Modulated Expression of Specific tRNAs Drives Gene Expression and Cancer Progression

机译:特定tRNA的调节表达驱动基因表达和癌症进展。

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摘要

Transfer RNAs (tRNAs) are primarily viewed as static contributors to gene expression. By developing a high-throughput tRNA profiling method, we find that specific tRNAs are upregulated in human breast cancer cells as they gain metastatic activity. Through loss-of-function, gain-of-function, and clinical-association studies, we implicate tRNAGluUUC and tRNAArgCCG as promoters of breast cancer metastasis. Upregulation of these tRNAs enhances stability and ribosome occupancy of transcripts enriched for their cognate codons. Specifically, tRNAGluUUC promotes metastatic progression by directly enhancing EXOSC2 expression and enhancing GRIPAP1-constituting an "inducible" pathway driven by a tRNA. The cellular proteomic shift toward a prometastatic state mirrors global tRNA shifts, allowing for cell-state and cell-type transgene expression optimization through codon content quantification. TRNA modulation represents a mechanism by which cells achieve altered expression of specific transcripts and proteins. TRNAs are thus dynamic regulators of gene expression and the tRNA codon landscape can causally and specifically impact disease progression.
机译:转移RNA(tRNA)主要被视为基因表达的静态贡献者。通过开发高通量的tRNA分析方法,我们发现特定的tRNA在人乳腺癌细胞中具有转移活性,因此被上调。通过功能丧失,功能获得和临床关联研究,我们认为tRNAGluUUC和tRNAArgCCG是乳腺癌转移的促进剂。这些tRNA的上调可增强其同源密码子富集的转录物的稳定性和核糖体占有率。具体而言,tRNAGluUUC通过直接增强EXOSC2表达和增强GRIPAP1(构成由tRNA驱动的“可诱导”途径)来促进转移进程。细胞向前转移状态的蛋白质组学转变反映了整体tRNA的变化,从而允许通过密码子含量定量优化细胞状态和细胞类型的转基因表达。 TRNA调节代表了一种机制,细胞可通过这种机制改变特定转录本和蛋白质的表达。因此,TRNA是基因表达的动态调节剂,并且tRNA密码子分布可以因果关系且特异性地影响疾病进程。

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