Human tRNA-derived small RNAs in the global regulation of RNA silencing

Haussecker, Dirk; Huang, Yong; Lau, Ashley; Parameswaran, Poornima; Fire, Andrew; Kay, Mark A.

doi:10.1261/rna.2000810

Cited by 605 publications

(768 citation statements)

References 73 publications

(112 reference statements)

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“…These new small RNAs are being noticed only now because most studies focused on sequencing reads derived from miRNAs. Accumulating evidence suggests that these RNA fragments are functional in physiological and pathological conditions (Rutjes et al ., 1999; Haussecker et al ., 2010; Anderson & Ivanov, 2014). In particular, tRNA halves have been described in the cytoplasm of stressed cultured cells where they have been reported to function in key biological processes, that is, translation and apoptosis (Ivanov et al ., 2011; Anderson & Ivanov, 2014) and may be involved in human diseases including cancer, neurodegeneration, and infection [reviewed in Anderson & Ivanov (2014)].…”

Section: Discussionmentioning

confidence: 99%

Circulating microRNA signature of genotype‐by‐age interactions in the long‐lived Ames dwarf mouse

et al. 2015

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SummaryRecent evidence demonstrates that serum levels of specific miRNAs significantly change with age. The ability of circulating sncRNAs to act as signaling molecules and regulate a broad spectrum of cellular functions implicates them as key players in the aging process. To discover circulating sncRNAs that impact aging in the long‐lived Ames dwarf mice, we conducted deep sequencing of small RNAs extracted from serum of young and old mice. Our analysis showed genotype‐specific changes in the circulating levels of 21 miRNAs during aging [genotype‐by‐age interaction (GbA)]. Genotype‐by‐age miRNAs showed four distinct expression patterns and significant overtargeting of transcripts involved in age‐related processes. Functional enrichment analysis of putative and validated miRNA targets highlighted cellular processes such as tumor suppression, anti‐inflammatory response, and modulation of Wnt, insulin, mTOR, and MAPK signaling pathways, among others. The comparative analysis of circulating GbA miRNAs in Ames mice with circulating miRNAs modulated by calorie restriction (CR) in another long‐lived mouse suggests CR‐like and CR‐independent mechanisms contributing to longevity in the Ames mouse. In conclusion, we showed for the first time a signature of circulating miRNAs modulated by age in the long‐lived Ames mouse.

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Section: Discussionmentioning

confidence: 99%

Circulating microRNA signature of genotype‐by‐age interactions in the long‐lived Ames dwarf mouse

et al. 2015

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“…Interestingly, recent studies report that these elements may contribute to gene regulation, being cleaved by DICER RNAse to produce stable RNA products rather than being just randomly generated degradation products (Haussecker et al 2010;Cole et al 2009;Sobala and Hutvagner 2011).…”

Section: Discussionmentioning

confidence: 99%

miRNA profiling in leaf and cork tissues of Quercus suber reveals novel miRNAs and tissue-specific expression patterns

Chaves

Lin

Pinto-Ricardo

et al. 2014

Tree Genetics & Genomes

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The differentiation of cork (phellem) cells from the phellogen (cork cambium) is a secondary growth process observed in the cork oak tree conferring a unique ability to produce a thick layer of cork. At present, the molecular regulators of phellem differentiation are unknown. The previously documented involvement of microRNAs in the regulation of developmental processes, including secondary growth, motivated the search for these regulators in cork oak tissues.We performed deep-sequencing of the small-RNA fraction obtained from cork oak leaves and differentiating phellem. RNA sequences with lengths of 19-25 nt derived from the two libraries were analysed, leading to the identification of 41 families of conserved miRNAs, of which the most abundant were miR167, miR165/166, miR396 and miR159. Thirty novel miRNA candidates were also unveiled, 11 of which were unique to leaves and 13 to phellem. Northern blot detection of a set of conserved and novel-miRNAs confirmed their differential expression profile. Prediction and analysis of putative miRNA target genes provided clues regarding processes taking place in leaf and phellem tissues but further experimental work will be needed for functional characterization. In conclusion, we here provide a first characterization of the miRNA population in a Fagacea species and the comparative analysis of miRNA expression in leaf and phellem libraries represents an important step to uncovering specific regulatory networks controlling phellem differentiation.

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“…Defined tRNA fragments have been identified through small RNA cloning approaches (Kawaji et al 2008;Cole et al 2009;Haussecker et al 2010), suggesting a physiological role for tRNA fragments. Interestingly, tRNA fragments can be processed to smaller RNAs by the Dicer RNase, indicating a potential interaction of tRNA-derived sequences and canonical small RNA processing pathways (Cole et al 2009).…”

Section: Functional Characterization Of Dnmt2mentioning

confidence: 99%

“…Interestingly, tRNA fragments can be processed to smaller RNAs by the Dicer RNase, indicating a potential interaction of tRNA-derived sequences and canonical small RNA processing pathways (Cole et al 2009). Indeed, a recent study provided evidence that tRNA-derived small RNAs act to down-regulate target mRNAs, and affect different RNA silencing pathways by associating with effector core components (Haussecker et al 2010). This suggests that altered tRNA cleavage (e.g., under stress conditions) could have phenotypic consequences.…”

Section: Functional Characterization Of Dnmt2mentioning

confidence: 99%

RNA methylation by Dnmt2 protects transfer RNAs against stress-induced cleavage

Schaefer¹,

Pollex²,

Hanna³

et al. 2010

Genes Dev.

601

657

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Dnmt2 proteins are the most conserved members of the DNA methyltransferase enzyme family, but their substrate specificity and biological functions have been a subject of controversy. We show here that, in addition to tRNA Asp-GTC , tRNA Val-AAC and tRNA Gly-GCC are also methylated by Dnmt2. Drosophila Dnmt2 mutants showed reduced viability under stress conditions, and Dnmt2 relocalized to stress granules following heat shock. Strikingly, stress-induced cleavage of tRNAs was Dnmt2-dependent, and Dnmt2-mediated methylation protected tRNAs against ribonuclease cleavage. These results uncover a novel biological function of Dnmt2-mediated tRNA methylation, and suggest a role for Dnmt2 enzymes during the biogenesis of tRNA-derived small RNAs.Supplemental material is available at http://www.genesdev.org.

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Human tRNA-derived small RNAs in the global regulation of RNA silencing

Cited by 605 publications

References 73 publications

Circulating microRNA signature of genotype‐by‐age interactions in the long‐lived Ames dwarf mouse

Circulating microRNA signature of genotype‐by‐age interactions in the long‐lived Ames dwarf mouse

miRNA profiling in leaf and cork tissues of Quercus suber reveals novel miRNAs and tissue-specific expression patterns

RNA methylation by Dnmt2 protects transfer RNAs against stress-induced cleavage

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