The -C-C-A End of tRNA and Its Role in Protein Biosynthesis

Sprinzl, Mathias; Cramer, Friedrich

doi:10.1016/s0079-6603(08)60798-9

Cited by 165 publications

(120 citation statements)

References 150 publications

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“…1). Chemical and nuclease protection studies indicate that the 3'-CCA sequence also functions in later steps of protein synthesis: in formation of a ternary complex between aminoacyl-tRNA, elongation factor Tu, and GTP (1) and in the binding of tRNA to 23S rRNA at the A, P, and E sites of the 50S ribosomal subunit during the elongation and translocation steps of the translation cycle (2)(3)(4)(5)(6).…”

mentioning

confidence: 99%

Functional transfer RNAs with modifications in the 3'-CCA end: differential effects on aminoacylation and polypeptide synthesis.

Liu¹,

Horowitz²

1994

Proc. Natl. Acad. Sci. U.S.A.

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mentioning

confidence: 99%

Functional transfer RNAs with modifications in the 3'-CCA end: differential effects on aminoacylation and polypeptide synthesis.

Liu¹,

Horowitz²

1994

Proc. Natl. Acad. Sci. U.S.A.

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“…1,2 This reaction is performed by the CCA-adding family of nucleotidyltransferases, which on the one hand catalyze the high-fidelity incorporation of the three nucleotides in the absence of a nucleic acid template, 3 and on the other hand act by proofreading unstable tRNAs. 4 Archeal genomes encode class I CCA-adding enzymes, 5 while class II is found in eubacteria and eukaryotes.…”

Section: Introductionmentioning

confidence: 99%

NMR reveals structural rearrangements associated to substrate insertion in nucleotide‐adding enzymes

et al. 2016

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The protein NP_344798.1 from Streptococcus pneumoniae TIGR4 exhibits a head and base-interacting neck domain architecture, as observed in class II nucleotide-adding enzymes. Although it has less than 20% overall sequence identity with any member of this enzyme family, the residues involved in substrate-recognition and catalysis are highly conserved in NP_344798.1. NMR studies showed binding affinity of NP_344798.1 for nucleotides and revealed ls to ms time scale rate processes involving residues constituting the active site. The results thus obtained indicate that large-amplitude rearrangements of regular secondary structures facilitate the penetration of the substrate into the occluded nucleotide-binding site of NP_344798.1 and, by inference based on sequence and structural homology, probably a wide range of other nucleotideadding enzymes.

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“…The modified tRNAs of this type allowed us to reveal some details of the molecular mechanism of the aminoacyl-tRNA enzymatic synthesis [ 1,2] and ribosomal synthesis of proteins [2,3]. ATP(3 'NH2) also effectively inhibited the DNAdependent RNA polymerase from the Ehrlich ascites tumour cells [4] and E. coli [5,6].…”

Section: Introductionmentioning

confidence: 99%

3′‐Deoxy‐3′‐aminonucleoside 5′‐triphosphates — Terminators of RNA synthesis, catalyzed by DNA‐dependent RNA polymerase from Escherichia coli

Beabealashvili¹,

Azhayev²,

Krayevsky³

1983

FEBS Letters

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The -C-C-A End of tRNA and Its Role in Protein Biosynthesis

Cited by 165 publications

References 150 publications

Functional transfer RNAs with modifications in the 3'-CCA end: differential effects on aminoacylation and polypeptide synthesis.

Functional transfer RNAs with modifications in the 3'-CCA end: differential effects on aminoacylation and polypeptide synthesis.

NMR reveals structural rearrangements associated to substrate insertion in nucleotide‐adding enzymes

3′‐Deoxy‐3′‐aminonucleoside 5′‐triphosphates — Terminators of RNA synthesis, catalyzed by DNA‐dependent RNA polymerase from Escherichia coli

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