4.8 Article

Ribosomal ambiguity(ram) mutations promote the open (off) to closed (on) transition and thereby increase miscoding

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NUCLEIC ACIDS RESEARCH
卷 47, 期 3, 页码 1557-1563

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OXFORD UNIV PRESS
DOI: 10.1093/nar/gky1178

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资金

  1. National Institutes of Health [GM093278, GM072528]
  2. NIGMS from the NIH [P41 GM103403]
  3. NIH-ORIP HEI grant [S10 RR029205]
  4. DOE Office of Science [DE-AC02-06CH11357]
  5. NIH

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Decoding is thought to be governed by a conformational transition in the ribosomeopen (off) to closed (on)that occurs upon codon-anticodon pairing in the A site. Ribosomal ambiguity (ram) mutations increase miscoding and map to disparate regions, consistent with a role for ribosome dynamics in decoding, yet precisely how these mutations act has been unclear. Here, we solved crystal structures of 70S ribosomes harboring 16S ram mutations G299A and G347U in the absence A-site tRNA (A-tRNA) and in the presence of a near-cognate anticodon stem-loop (ASL). In the absence of an A-tRNA, each of the mutant ribosomes exhibits a partially closed (on) state. In the 70S-G347U structure, the 30S shoulder is rotated inward and intersubunit bridge B8 is disrupted. In the 70S-G299A structure, the 30S shoulder is rotated inward and decoding nucleotide G530 flips into the anti conformation. Both of these mutant ribosomes adopt the fully closed (on) conformation in the presence of near-cognate A-tRNA, just as they do with cognate A-tRNA. Thus, these ram mutations act by promoting the open (off) to closed (on) transition, albeit in somewhat distinct ways. This work reveals the functional importance of 30S shoulder rotation for productive aminoacylated-tRNA incorporation.

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