Improvement of reading frame maintenance is a common function for several tRNA modifications

Urbonavičius, Jaunius; Qian, Qiang; Durand, Jérôme M. B.; Hagervall, Tord G.; Björk, Glenn R.

doi:10.1093/emboj/20.17.4863

Cited by 439 publications

(442 citation statements)

References 35 publications

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“…Q is a hypermodified nucleoside found at the wobble position of GUN anticodons in tRNAs for Tyr, Asn, Asp, and His in most bacteria (Harada and Nishimura 1972). The Q modification is known to be important for translational fidelity (Bienz and Kubli 1981;Meier et al 1985;Urbonavičius et al 2001). Q biosynthesis starts with GTP and proceeds through the intermediate preQ 0 (7-cyano-7-deazaguanine) and preQ 1 (7-aminomethyl-7-deazaguanine) in a series of enzymatic steps (Kuchino et al 1976;Okada et al 1978;Iwata-Reuyl 2003;Gaur and Varshney 2005;Van Lanen et al 2005).…”

Section: Introductionmentioning

confidence: 99%

Confirmation of a second natural preQ₁ aptamer class in Streptococcaceae bacteria

Meyer¹,

Roth²,

Chervin³

et al. 2008

RNA

108

155

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Bioinformatics searches of eubacterial genomes have yielded many riboswitch candidates where the identity of the ligand is not immediately obvious on examination of associated genes. One of these motifs is found exclusively in the family Streptococcaceae within the 59 untranslated regions (UTRs) of genes encoding the hypothetical membrane protein classified as COG4708 or DUF988. While the function of this protein class is unproven, a riboswitch binding the queuosine biosynthetic intermediate pre-queuosine 1 (preQ 1 ) has been identified in the 59 UTR of homologous genes in many Firmicute species of bacteria outside of Streptococcaceae. Here we show that a representative of the COG4708 RNA motif from Streptococcus pneumoniae R6 also binds preQ 1 . Furthermore, representatives of this RNA have structural and molecular recognition characteristics that are distinct from those of the previously described preQ 1 riboswitch class. PreQ 1 is the second metabolite for which two or more distinct classes of natural aptamers exist, indicating that natural aptamers utilizing different structures to bind the same metabolite may be more common than is currently known. Additionally, the association of preQ 1 binding RNAs with most genes encoding proteins classified as COG4708 strongly suggests that these proteins function as transporters for preQ 1 or another queuosine biosynthetic intermediate.

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Section: Introductionmentioning

confidence: 99%

Confirmation of a second natural preQ₁ aptamer class in Streptococcaceae bacteria

Meyer¹,

Roth²,

Chervin³

et al. 2008

RNA

108

155

View full text Add to dashboard Cite

show abstract

“…At present, 81 different modified residues have been identified that most frequently involve the wobble position (residue 34) and the position 3 0 adjacent to the anticodon (residue 37) (Rozenski et al, 1999). All of these modifications have been shown to be essential in maintaining the correct reading frame of the translational machinery, thus improving fidelity and efficiency of protein synthesis and avoiding errors that could be detrimental for cells (Persson, 1993;Bjork et al, 1999;Urbonavicius et al, 2001). N 6 -isopentenyladenosine (i 6 A) is the only known cytokinin existing in animal tRNAs and is specifically found at position 37 of tRNA molecules that bind codons starting with uridine (Persson et al, 1994).…”

Section: Introductionmentioning

confidence: 99%

Identification and functional characterization of the candidate tumor suppressor gene TRIT1 in human lung cancer

et al. 2005

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“…As a tRNA modification, i 6 A contributes to reading frame maintenance, 3 and the lack of i 6 A in selenocysteine tRNA can affect synthesis of selenoproteins. 4 We previously showed that i 6 A exerts potent in vitro antitumour activity on human epithelial cancer cell lines derived from different types of tumours.…”

mentioning

confidence: 99%

Pharmacogenomics and analogues of the antitumour agent N⁶‐isopentenyladenosine

Colombo

Falvella

Cecco

et al. 2009

Intl Journal of Cancer

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N6‐isopentenyladenosine (i6A), a member of the cytokinin family of plant hormones, has potent in vitro antitumour activity in different types of human epithelial cancer cell lines. Gene expression profile analysis of i6A‐treated cells revealed induction of genes (e.g., PPP1R15A, DNAJB9, DDIT3, and HBP1) involved in the negative regulation of cell cycle progression and reportedly up‐regulated during cell cycle arrest in stress conditions. Of 6 i6A analogues synthesized, only the 1 with a saturated double bond of the isopentenyl side chain had in vitro antitumour activity, although weaker than that of i6A, suggesting that i6A biological activity is highly linked to its structure. In vivo analysis of i6A and the active analogue revealed no significant inhibition of cancer cell growth in mice by either reagent. Thus, although i6A may inhibit cell proliferation by regulating the cell cycle, further studies are needed to identify active analogues potentially useful in vivo. © 2008 Wiley‐Liss, Inc.

show abstract

Improvement of reading frame maintenance is a common function for several tRNA modifications

Cited by 439 publications

References 35 publications

Confirmation of a second natural preQ₁ aptamer class in Streptococcaceae bacteria

Confirmation of a second natural preQ₁ aptamer class in Streptococcaceae bacteria

Identification and functional characterization of the candidate tumor suppressor gene TRIT1 in human lung cancer

Pharmacogenomics and analogues of the antitumour agent N⁶‐isopentenyladenosine

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Improvement of reading frame maintenance is a common function for several tRNA modifications

Cited by 439 publications

References 35 publications

Confirmation of a second natural preQ1 aptamer class in Streptococcaceae bacteria

Confirmation of a second natural preQ1 aptamer class in Streptococcaceae bacteria

Identification and functional characterization of the candidate tumor suppressor gene TRIT1 in human lung cancer

Pharmacogenomics and analogues of the antitumour agent N6‐isopentenyladenosine

Contact Info

Product

Resources

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Confirmation of a second natural preQ₁ aptamer class in Streptococcaceae bacteria

Confirmation of a second natural preQ₁ aptamer class in Streptococcaceae bacteria

Pharmacogenomics and analogues of the antitumour agent N⁶‐isopentenyladenosine