On the expanding roles of tRNA fragments in modulating cell behavior

Magee, Rogan; Rigoutsos, Isidore

doi:10.1093/nar/gkaa657

Cited by 130 publications

(151 citation statements)

References 150 publications

(231 reference statements)

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“…Among tRNA roles outside ribosomal protein synthesis, the following have been previously highlighted: nutrient sensing, transcription regulation, retroelement insertion, translation kinetics and protein folding, stress response, immune response, apoptosis inhibition, peptidic antibiotic biosynthesis, bacterial wall biosynthesis, post-translational protein modification, membrane lipid modification, retroviral replication, mitochondrial ribosome assembly, and mitochondrial DNA replication ( Seligmann, 2010 ; Raina and Ibba, 2014 ; Katz et al, 2016 ; Balasubramaniam et al, 2017 ; Bogenhagen et al, 2018 ; Su et al, 2020 ; and this issue). Also, several roles have been described for tRNA fragments, among which the following stand out: gene silencing, translation regulation, transposable element regulation, noncoding RNA regulation, cell differentiation, cell proliferation and cancer, host defense, stress response, apoptosis, and epigenetic inheritance ( Magee and Rigoutsos, 2020 ; Polacek and Ivanov, 2020 ; Su et al, 2020 ; and this issue). In most cases, the information about the precise isotype, state of post-transcriptional modification, recognition by the cognate aminoacyl-tRNA synthetase, and aminoacylation state is still scarce, leaving the door open for new research avenues.…”

Section: Possible Clues For the Absence Of Trna Genesmentioning

confidence: 99%

On the Track of the Missing tRNA Genes: A Source of Non-Canonical Functions?

Ehrlich

Davyt

López

et al. 2021

Front. Mol. Biosci.

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Cellular tRNAs appear today as a diverse population of informative macromolecules with conserved general elements ensuring essential common functions and different and distinctive features securing specific interactions and activities. Their differential expression and the variety of post-transcriptional modifications they are subject to, lead to the existence of complex repertoires of tRNA populations adjusted to defined cellular states. Despite the tRNA-coding genes redundancy in prokaryote and eukaryote genomes, it is surprising to note the absence of genes coding specific translational-active isoacceptors throughout the phylogeny. Through the analysis of different releases of tRNA databases, this review aims to provide a general summary about those “missing tRNA genes.” This absence refers to both tRNAs that are not encoded in the genome, as well as others that show critical sequence variations that would prevent their activity as canonical translation adaptor molecules. Notably, while a group of genes are universally missing, others are absent in particular kingdoms. Functional information available allows to hypothesize that the exclusion of isodecoding molecules would be linked to: 1) reduce ambiguities of signals that define the specificity of the interactions in which the tRNAs are involved; 2) ensure the adaptation of the translational apparatus to the cellular state; 3) divert particular tRNA variants from ribosomal protein synthesis to other cellular functions. This leads to consider the “missing tRNA genes” as a source of putative non-canonical tRNA functions and to broaden the concept of adapter molecules in ribosomal-dependent protein synthesis.

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Section: Possible Clues For the Absence Of Trna Genesmentioning

confidence: 99%

On the Track of the Missing tRNA Genes: A Source of Non-Canonical Functions?

Ehrlich

Davyt

López

et al. 2021

Front. Mol. Biosci.

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“…Although the function of tRNAs as adapter molecules is well known, recent studies have shown that they are a major source of small noncoding RNAs that, together with other small RNAs such as PIWI-interacting RNAs (piRNAs), ribosomal-derived small RNAs, small nucleolar RNAs (snRNAs), and microRNAs (miRNAs), play an active role in diverse biological processes such as RNA processing, post-transcriptional and post-translational regulation, cell proliferation and apoptosis, vesicle-mediated intercellular communication, and intergenerational inheritance [27][28][29][30][31][32][33][34][35][36][37][38][39][40][41][42]. Small RNAs derived from tRNAs are generated by enzymatic cleavage of the parental (precursor and mature) tRNAs [19,35,36,39,43] ( Figure 1). A large variety of tRNA fragments exists which have been classified into seven groups based on their position within the parental tRNA sequence: 5 or 3 small tRNA fragments (tRFs) of ≤30 nucleotides that are generated from the 5 or 3 ends of the parental mature tRNA, internal tRNA fragments (i-tRFs) of varying lengths (16 to 33 nucleotides), 5 or 3 33 nucleotide-long tRNA halves (tRHs) and 5 U-tRFs and tRF-1s derived from precursor tRNAs and containing part of the 5 leader or 3 trailer sequence, respectively [35] ( Figure 1).…”

Section: Trna Fragments a New Class Of Small Noncoding Rnasmentioning

confidence: 99%

“…Small RNAs derived from tRNAs are generated by enzymatic cleavage of the parental (precursor and mature) tRNAs [19,35,36,39,43] ( Figure 1). A large variety of tRNA fragments exists which have been classified into seven groups based on their position within the parental tRNA sequence: 5 or 3 small tRNA fragments (tRFs) of ≤30 nucleotides that are generated from the 5 or 3 ends of the parental mature tRNA, internal tRNA fragments (i-tRFs) of varying lengths (16 to 33 nucleotides), 5 or 3 33 nucleotide-long tRNA halves (tRHs) and 5 U-tRFs and tRF-1s derived from precursor tRNAs and containing part of the 5 leader or 3 trailer sequence, respectively [35] ( Figure 1). The endonucleases Angiogenin, RNAse T2, Dicer, and RNaseZ/ELAC2 generate some but not all tRNA fragments [27,[44][45][46], suggesting that other tRNA cleaving enzymes remain to be identified [47].…”

Section: Trna Fragments a New Class Of Small Noncoding Rnasmentioning

confidence: 99%

“…Reduced tRNA modifications, as a consequence of mutations or impaired function of tRNA-modifying enzymes or increased demethylase activity, may also lead to tRNA fragmentation [52][53][54][55][56]. Dysregulated tRNA fragmentation has been detected in different diseases [35,36] including cancer [45,54,57,58], neurological disorders [52,[59][60][61][62], metabolic disorders [30,31,53,55], and osteoarthritis [63].…”

Section: Trna Fragments a New Class Of Small Noncoding Rnasmentioning

confidence: 99%

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tRNA Biology in the Pathogenesis of Diabetes: Role of Genetic and Environmental Factors

Arroyo

Green²,

Cnop³

et al. 2021

IJMS

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The global rise in type 2 diabetes results from a combination of genetic predisposition with environmental assaults that negatively affect insulin action in peripheral tissues and impair pancreatic β-cell function and survival. Nongenetic heritability of metabolic traits may be an important contributor to the diabetes epidemic. Transfer RNAs (tRNAs) are noncoding RNA molecules that play a crucial role in protein synthesis. tRNAs also have noncanonical functions through which they control a variety of biological processes. Genetic and environmental effects on tRNAs have emerged as novel contributors to the pathogenesis of diabetes. Indeed, altered tRNA aminoacylation, modification, and fragmentation are associated with β-cell failure, obesity, and insulin resistance. Moreover, diet-induced tRNA fragments have been linked with intergenerational inheritance of metabolic traits. Here, we provide a comprehensive review of how perturbations in tRNA biology play a role in the pathogenesis of monogenic and type 2 diabetes.

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“…The exploration of miRNA expression profiles has added valuable insights into mechanisms of cell processes in health and disease (2,9). tRNA fragments and halves (tRFs) have more recently become of interest through their role in pathophysiology (10). They are thought to increase based on cell stressors and have variable expression patterns based on cell type and method of cell stress (11).…”

Section: Introductionmentioning

confidence: 99%

miRge3.0: a comprehensive microRNA and tRF sequencing analysis pipeline

Patil

Halushka

2021

Preprint

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MicroRNAs and tRFs are classes of small non-coding RNAs, known for their roles in translational regulation of genes. Advances in next-generation sequencing (NGS) have enabled high-throughput small RNA-seq studies, which require robust alignment pipelines. Our laboratory previously developed miRge and miRge2.0, as flexible tools to process sequencing data for annotation of miRNAs and other small-RNA species and further predict novel miRNAs using a support vector machine approach. Although, miRge2.0 is a leading analysis tool in terms of speed with unique quantifying and annotation features, it has a few limitations. We present miRge3.0 which provides additional features along with compatibility to newer versions of Cutadapt and Python. The revisions of the tool include the ability to process Unique Molecular Identifiers (UMIs) to account for PCR duplicates while quantifying miRNAs in the datasets and an accurate GFF3 formatted isomiR tool. miRge3.0 also has speed improvements benchmarked to miRge2.0, Chimira and sRNAbench. Finally, miRge3.0 output integrates into other packages for a streamlined analysis process and provides a cross-platform Graphical User Interface (GUI). In conclusion miRge3.0 is our 3rd generation small RNA-seq aligner with improvements in speed, versatility, and functionality over earlier iterations.

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On the expanding roles of tRNA fragments in modulating cell behavior

Cited by 130 publications

References 150 publications

On the Track of the Missing tRNA Genes: A Source of Non-Canonical Functions?

On the Track of the Missing tRNA Genes: A Source of Non-Canonical Functions?

tRNA Biology in the Pathogenesis of Diabetes: Role of Genetic and Environmental Factors

miRge3.0: a comprehensive microRNA and tRF sequencing analysis pipeline

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