The tumor suppressor microRNA let-7 inhibits human LINE-1 retrotransposition

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作者
Pablo Tristán-Ramos
Alejandro Rubio-Roldan
Guillermo Peris
Laura Sánchez
Suyapa Amador-Cubero
Sebastien Viollet
Gael Cristofari
Sara R. Heras
机构
[1] GENYO,Dept. Biochemistry and Molecular Biology II
[2] Centre for Genomics and Oncological Research: Pfizer/University of Granada/Andalusian Regional Government. PTS Granada,Dept. of Computer Languages and Systems
[3] Faculty of Pharmacy,undefined
[4] University of Granada,undefined
[5] Campus Universitario de Cartuja,undefined
[6] Universitat Jaume I,undefined
[7] Université Côte d’Azur,undefined
[8] CNRS,undefined
[9] INSERM,undefined
[10] IRCAN,undefined
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摘要
Nearly half of the human genome is made of transposable elements (TEs) whose activity continues to impact its structure and function. Among them, Long INterspersed Element class 1 (LINE-1 or L1) elements are the only autonomously active TEs in humans. L1s are expressed and mobilized in different cancers, generating mutagenic insertions that could affect tumor malignancy. Tumor suppressor microRNAs are ∼22nt RNAs that post-transcriptionally regulate oncogene expression and are frequently downregulated in cancer. Here we explore whether they also influence L1 mobilization. We show that downregulation of let-7 correlates with accumulation of L1 insertions in human lung cancer. Furthermore, we demonstrate that let-7 binds to the L1 mRNA and impairs the translation of the second L1-encoded protein, ORF2p, reducing its mobilization. Overall, our data reveals that let-7, one of the most relevant microRNAs, maintains somatic genome integrity by restricting L1 retrotransposition.
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