Broad and adaptable RNA structure recognition by the human interferon-induced tetratricopeptide repeat protein IFIT5

Katibah, George E.; Qin, Yidan; Sidote, David J.; Yao, Jun; Lambowitz, Alan M.; Collins, Kathleen

doi:10.1073/pnas.1412842111

Cited by 77 publications

(125 citation statements)

References 32 publications

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“…1B) to include RNAs with post-transcriptionally added nucleotides, such as the 3 ′ CCA of tRNAs or poly(U) tails (Malecki et al 2013;Katibah et al 2014). Like other RTs and DNA polymerases, TGIRTs can add a small number of extra nontemplated nucleotides to the 3 ′ ends of cDNAs (referred to as terminal transferase activity) (Clark 1988;Golinelli and Hughes 2002).…”

Section: Preparation Of Human Plasma Rnasmentioning

confidence: 99%

“…7B). In contrast to retroviral RTs, which terminate at base modifications that affect Watson-Crick base-pairing interactions (Burnett and McHenry 1997;Ansmant et al 2001;Jackman et al 2003), TGIRTs frequently read through a number of such modifications (e.g., m 1 A58 and m 1 G9) by misincorporation, with the spectrum of misincorporated nucleotides characteristic of the modification (Katibah et al 2014;Shen et al 2015). tRNA-protein complexes have been identified previously in human sera as autoantigens in patients with autoimmune diseases, a wellstudied example being HisGUG, which is bound to histidyl-tRNA synthetase in the polymyositis-specific autoantigen Jo-1 (Hardin et al 1982;Mathews and Bernstein 1983;Rosa et al 1983).…”

Section: Wwwrnajournalorg 119mentioning

confidence: 99%

“…We showed that TGIRT-seq enables miRNA profiling with less bias than two commercial RNAseq kits that rely on RNA ligation for RNA-seq adapter addition (Mohr et al 2013). Recently, we used TGIRT-seq to profile RNAs associated with the human interferon-induced protein IFIT5 (Katibah et al 2014); to identify tRNAs associated with a yeast ribosome quality control complex (Shen et al 2015); and in combination with a demethylase, for quantitative profiling of cellular tRNAs (Zheng et al 2015). These studies demonstrated that TGIRT-seq yields full-length reads of highly structured RNAs, including precursor and mature tRNAs, enables the quantification of charged and uncharged tRNAs, and facilitates the analysis of post-transcriptional modifications, including base modifications on the Watson-Crick face, many of which can be read through and result in distinctive patterns of misincorporated nucleotides.…”

Section: Introductionmentioning

confidence: 99%

“…In the initial TGIRT-seq method, the cDNAs with an RNA-seq adapter linked by TGIRT during reverse transcription were size-selected on a denaturing polyacrylamide gel and circularized with CircLigaseII ssDNA Ligase (Epicentre) prior to PCR amplification (Mohr et al 2013;Katibah et al 2014;Shen et al 2015;Zheng et al 2015). Although this procedure remains useful for RNA-seq of specific RNA size classes or homogenously sized RNA fragments in procedures like HITS-CLIP or ribosome profiling, disadvantages include (1) size limitations introduced by CircLigase, whose efficiency decreases for longer cDNAs (Epicentre product literature); (2) a gel-purification step, which is time consuming and results in loss of material; and (3) the use of hazardous chemicals, such as phenol and chloroform.…”

Section: Introductionmentioning

confidence: 99%

“…In the previous TGIRT-seq method, referred to as the small RNA/CircLigase method, cDNAs were linked by TGIRT template-switching to an RNA-seq adapter containing the complements to both the Illumina Read 2 (R2R) and Read 1 (R1R) primer-binding sites, gel purified and then circularized with CircLigase prior to PCR amplification (Katibah et al 2014;Shen et al 2015;Zheng et al 2015). In contrast, in the new TGIRT-seq method developed here, the cDNAs with an attached R2R adapter sequence are processed into RNA-seq libraries without size selection by ligating a 5 ′ -adenylated (5 ′ App) DNA oligonucleotide containing the R1R adapter to the cDNA 3 ′ end with Thermostable 5 ′ AppDNA/RNA Ligase (New England Biolabs).…”

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confidence: 99%

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High-throughput sequencing of human plasma RNA by using thermostable group II intron reverse transcriptases

Qin

Yao

et al. 2015

RNA

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115

187

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Next-generation RNA-sequencing (RNA-seq) has revolutionized transcriptome profiling, gene expression analysis, and RNA-based diagnostics. Here, we developed a new RNA-seq method that exploits thermostable group II intron reverse transcriptases (TGIRTs) and used it to profile human plasma RNAs. TGIRTs have higher thermostability, processivity, and fidelity than conventional reverse transcriptases, plus a novel template-switching activity that can efficiently attach RNA-seq adapters to target RNA sequences without RNA ligation. The new TGIRT-seq method enabled construction of RNA-seq libraries from <1 ng of plasma RNA in <5 h. TGIRT-seq of RNA in 1-mL plasma samples from a healthy individual revealed RNA fragments mapping to a diverse population of protein-coding gene and long ncRNAs, which are enriched in intron and antisense sequences, as well as nearly all known classes of small ncRNAs, some of which have never before been seen in plasma. Surprisingly, many of the small ncRNA species were present as full-length transcripts, suggesting that they are protected from plasma RNases in ribonucleoprotein (RNP) complexes and/or exosomes. This TGIRT-seq method is readily adaptable for profiling of whole-cell, exosomal, and miRNAs, and for related procedures, such as HITS-CLIP and ribosome profiling.

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Section: Preparation Of Human Plasma Rnasmentioning

confidence: 99%

Section: Wwwrnajournalorg 119mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

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High-throughput sequencing of human plasma RNA by using thermostable group II intron reverse transcriptases

Qin

Yao

et al. 2015

RNA

Self Cite

115

187

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Unconventional RNA‐binding proteins step into the virus–host battlefront

2018

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The crucial participation of cellular RNA-binding proteins (RBPs) in virtually all steps of virus infection has been known for decades. However, most of the studies characterizing this phenomenon have focused on well-established RBPs harboring classical RNA-binding domains (RBDs). Recent proteome-wide approaches have greatly expanded the census of RBPs, discovering hundreds of proteins that interact with RNA through unconventional RBDs. These domains include protein-protein interaction platforms, enzymatic cores, and intrinsically disordered regions. Here, we compared the experimentally determined census of RBPs to gene ontology terms and literature, finding that 472 proteins have previous links with viruses. We discuss what these proteins are and what their roles in infection might be. We also review some of the pioneering examples of unorthodox RBPs whose RNA-binding activity has been shown to be critical for virus infection. Finally, we highlight the potential of these proteins for host-based therapies against viruses. This article is categorized under: RNA Interactions with Proteins and Other Molecules > Protein-RNA Interactions: Functional Implications RNA in Disease and Development > RNA in Disease RNA Interactions with Proteins and Other Molecules > RNA-Protein Complexes.

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The Pol III transcriptome: Basic features, recurrent patterns, and emerging roles in cancer

Zhou

Bortle

2023

WIREs RNA

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The RNA polymerase III (Pol III) transcriptome is universally comprised of short, highly structured noncoding RNA (ncRNA). Through RNA–protein interactions, the Pol III transcriptome actuates functional activities ranging from nuclear gene regulation (7SK), splicing (U6, U6atac), and RNA maturation and stability (RMRP, RPPH1, Y RNA), to cytoplasmic protein targeting (7SL) and translation (tRNA, 5S rRNA). In higher eukaryotes, the Pol III transcriptome has expanded to include additional, recently evolved ncRNA species that effectively broaden the footprint of Pol III transcription to additional cellular activities. Newly evolved ncRNAs function as riboregulators of autophagy (vault), immune signaling cascades (nc886), and translation (Alu, BC200, snaR). Notably, upregulation of Pol III transcription is frequently observed in cancer, and multiple ncRNA species are linked to both cancer progression and poor survival outcomes among cancer patients. In this review, we outline the basic features and functions of the Pol III transcriptome, and the evidence for dysregulation and dysfunction for each ncRNA in cancer. When taken together, recurrent patterns emerge, ranging from shared functional motifs that include molecular scaffolding and protein sequestration, overlapping protein interactions, and immunostimulatory activities, to the biogenesis of analogous small RNA fragments and noncanonical miRNAs, augmenting the function of the Pol III transcriptome and further broadening its role in cancer.This article is categorized under: RNA in Disease and Development > RNA in Disease RNA Processing > Processing of Small RNAs RNA Interactions with Proteins and Other Molecules > Protein‐RNA Interactions: Functional Implications

show abstract

Broad and adaptable RNA structure recognition by the human interferon-induced tetratricopeptide repeat protein IFIT5

Cited by 77 publications

References 32 publications

High-throughput sequencing of human plasma RNA by using thermostable group II intron reverse transcriptases

High-throughput sequencing of human plasma RNA by using thermostable group II intron reverse transcriptases

Unconventional RNA‐binding proteins step into the virus–host battlefront

The Pol III transcriptome: Basic features, recurrent patterns, and emerging roles in cancer

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