Functional Anticodon Architecture of Human tRNA<sup>Lys3</sup> Includes Disruption of Intraloop Hydrogen Bonding by the Naturally Occurring Amino Acid Modification, t<sup>6</sup>A

Stuart, J.W.; Gdaniec, Zofia; Guenther, Richard; Marszalek, Michal; Sochacka, Elżbieta; Malkiewicz, and Andrzej; Agris, Paul F.

doi:10.1021/bi0013039

Cited by 114 publications

(135 citation statements)

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“…Comparing it with various hypomodified and unmodified analogs revealed opposing effects of the base modifications on ACNase reactivity. Correlating these data with the observed contributions of the base modifications to the ASL solution structure (12,14,15) leads us to suggest that ACNase prefers substrates where the anticodon nucleotides assume a stacked A-RNA conformation and where the base pairing interactions in the ASL stem are relatively destabilized. We also show that the PrrC D287H mutation renders human tRNA Lys3 relatively more reactive than the natural substrate.…”

Section: A Trnamentioning

confidence: 84%

“…The wobble base side chain mnm 5 U34 also stabilizes the anticodon base stacking and U-turn conformation but partially counteracts the base pair disrupting effect of t 6 A37. Destabilization of the stem and/or the C 32 -A 38 base pair (21) by t 6 A37 also opposes the effect of the ⌿39 modification (12,14,15). Here we have shown that the ASL base modifications also exert distinct effects on ACNase reactivity (Tables I and II).…”

Section: The Trnamentioning

confidence: 99%

“…This assumption is backed by the following arguments. First, t 6 A37 or ms 2 t 6 A37 that dramatically enhanced the ACNase reaction rate also stabilize the anticodon A-RNA and the loops U-turn conformations and destabilize the anticodon stem and bifurcated C 32 -A 38 base pair (12,14), suggesting that ACNase favors these structural features. In agreement, ⌿39, which inhibited ACNase activity in certain cases, exerts the opposite effect on ASL base pairing interactions.…”

Section: The Trnamentioning

confidence: 99%

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Structural Features of tRNALys Favored by Anticodon Nuclease as Inferred from Reactivities of Anticodon Stem and Loop Substrate Analogs

Jiang¹,

Blanga²,

Amitsur³

et al. 2002

Journal of Biological Chemistry

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The bacterial tRNA Lys -specific PrrC-anticodon nuclease efficiently cleaved an anticodon stem-loop (ASL) oligoribonucleotide containing the natural modified bases, suggesting this region harbors the specificity determinants. Assays of ASL analogs indicated that the 6-threonylcarbamoyl adenosine modification (t 6 A37) enhances the reactivity. The side chain of the modified wobble base 5-methylaminomethyl-2-thiouridine (mnm 5 s 2 U34) has a weaker positive effect depending on the context of other modifications. The s 2 U34 modification apparently has none and the pseudouridine (⌿39) was inhibitory in most modification contexts. GC-rich but not IC-rich stems abolished the activity. Correlating the reported structural effects of the base modifications with their effects on anticodon nuclease activity suggests preference for substrates where the anticodon nucleotides assume a stacked A-RNA conformation and base pairing interactions in the stem are destabilized. Moreover, the proposal that PrrC residue Asp 287 contacts mnm 5 s 2 U34 was reinforced by the observations that the mammalian tRNA Lys-3 wobble base 5-methoxycarbonyl methyl-2-thiouridine (mcm 5 s 2 U) is inhibitory and that the D287H mutant favors tRNA Lys-3 over Escherichia coli tRNA Lys . The detection of this mutation and ability of PrrC to cleave the isolated ASL suggest that anticodon nuclease may be used to cleave tRNA Lys-3 primer molecules annealed to the genomic RNA template of the human immunodeficiency virus.

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Section: A Trnamentioning

confidence: 84%

Section: The Trnamentioning

confidence: 99%

Section: The Trnamentioning

confidence: 99%

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Structural Features of tRNALys Favored by Anticodon Nuclease as Inferred from Reactivities of Anticodon Stem and Loop Substrate Analogs

Jiang¹,

Blanga²,

Amitsur³

et al. 2002

Journal of Biological Chemistry

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“…The bulky residue prevents the intraloop hydrogen bond between residues 32 and 37, thus promoting proper pre-structuring of the ASL. 116,117 In mitochondrial tRNAs, imG 37 or its derivatives are commonly replaced by i 6 A 37 or a derivative thereof, or by a methylated purine, therefore suggesting the evolution of an alternative strategy for establishing the same functional properties by using different chemical moieties in RNA modifications. 113,116 …”

Section: The Modified Wobble Hypothesis and Decoding At Position 34mentioning

confidence: 99%

“…Furthermore, in the absence of modifications, the U-rich ASL cannot effectively form stacking interactions to stabilize its structure nor negate intraloop hydrogen bonding that effectively condenses the size of the ASL. 117 The nearly ubiquitously modified, invariable purine at position 37 can alleviate the thermodynamic penalty of a pyrimidine rich anticodon. In tRNA Lys UUU the purine at position 37 is modified to N 6 -threonylcarbamoyladenosine, t 6 A or a derivative thereof such as 2-methylthio- N 6 -threonylcarbamoyladenosine, ms 2 t 6 A 37 found in mammalian tRNA Lys3 UUU .…”

Section: The Modified Wobble Hypothesis and Decoding At Position 34mentioning

confidence: 99%

Celebrating wobble decoding: Half a century and still much is new

et al. 2017

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A simple post-transcriptional modification of tRNA, deamination of adenosine to inosine at the first, or wobble, position of the anticodon, inspired Francis Crick's Wobble Hypothesis 50 years ago. Many more naturally-occurring modifications have been elucidated and continue to be discovered. The post-transcriptional modifications of tRNA's anticodon domain are the most diverse and chemically complex of any RNA modifications. Their contribution with regards to chemistry, structure and dynamics reveal individual and combined effects on tRNA function in recognition of cognate and wobble codons. As forecast by the Modified Wobble Hypothesis 25 years ago, some individual modifications at tRNA's wobble position have evolved to restrict codon recognition whereas others expand the tRNA's ability to read as many as four synonymous codons. Here, we review tRNA wobble codon recognition using specific examples of simple and complex modification chemistries that alter tRNA function. Understanding natural modifications has inspired evolutionary insights and possible innovation in protein synthesis.

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Synthesis of Oligoribonucleotides Containing N⁶‐Alkyladenosine and 2‐Methylthio‐N⁶‐Alkyladenosine

Kierzek

2004

CP Nucleic Acid Chemistry

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The N(6)-alkyladenosines and 2-methylthio-N(6)-alkyladenosines are the most common modified adenosine nucleosides, and transfer ribonucleic acids (tRNA) are particularly rich in these modified nucleosides. They are present at position 37 of the anticodon arm, and the contributions of these hypermodified nucleosides to codon-anticodon interactions as well as to translation are significant, although they are not fully understood. This unit describes a new chemical synthesis method for oligoribonucleotides containing N(6)-alkyladenosines and 2-methylthio-N(6)-alkyladenosines via postsynthetic modifications of precursor oligoribonucleotides. To obtain oligoribonucleotides containing N(6)-alkyladenosines, a precursor oligoribonucleotide carrying 6-methylthiopurine riboside residues was used, whereas for the synthesis of oligoribonucleotides containing 2-methylthio-N(6)-alkyladenosines, a precursor oligoribonucleotide carrying the 2-methylthio-6-chloropurine riboside was applied. This allowed synthesis of modified oligoribonucleotides containing naturally occurring modified nucleosides such as N(6)-isopentenyladenosine (i(6)A), N(6)-methyladenosine (m(6)A), 2-methylthio-N(6)-isopentenyladenosine (ms(2)i(6)A), and 2-methylthio-N(6)-methyladenosine (ms(2)m(6)A), as well as several unnaturally modified adenosine derivatives.

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Functional Anticodon Architecture of Human tRNA^Lys3 Includes Disruption of Intraloop Hydrogen Bonding by the Naturally Occurring Amino Acid Modification, t⁶A

Cited by 114 publications

References 50 publications

Structural Features of tRNALys Favored by Anticodon Nuclease as Inferred from Reactivities of Anticodon Stem and Loop Substrate Analogs

Structural Features of tRNALys Favored by Anticodon Nuclease as Inferred from Reactivities of Anticodon Stem and Loop Substrate Analogs

Celebrating wobble decoding: Half a century and still much is new

Synthesis of Oligoribonucleotides Containing N⁶‐Alkyladenosine and 2‐Methylthio‐N⁶‐Alkyladenosine

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Functional Anticodon Architecture of Human tRNALys3 Includes Disruption of Intraloop Hydrogen Bonding by the Naturally Occurring Amino Acid Modification, t6A

Cited by 114 publications

References 50 publications

Structural Features of tRNALys Favored by Anticodon Nuclease as Inferred from Reactivities of Anticodon Stem and Loop Substrate Analogs

Structural Features of tRNALys Favored by Anticodon Nuclease as Inferred from Reactivities of Anticodon Stem and Loop Substrate Analogs

Celebrating wobble decoding: Half a century and still much is new

Synthesis of Oligoribonucleotides Containing N6‐Alkyladenosine and 2‐Methylthio‐N6‐Alkyladenosine

Contact Info

Product

Resources

About

Functional Anticodon Architecture of Human tRNA^Lys3 Includes Disruption of Intraloop Hydrogen Bonding by the Naturally Occurring Amino Acid Modification, t⁶A

Synthesis of Oligoribonucleotides Containing N⁶‐Alkyladenosine and 2‐Methylthio‐N⁶‐Alkyladenosine