4.5 Article

A biophysical basis for the emergence of the genetic code in protocells

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ELSEVIER
DOI: 10.1016/j.bbabio.2022.148597

关键词

Origin of life; Genetic code; Protocells; Autotrophy

资金

  1. Biotechnology and Biological Sciences Research Council [BB/V003542/1]
  2. Natural Environment Research Council [2236041]

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This study presents a new framework based on autotrophic growth of protocells, predicting most codon assignments and showing a correlation between the first letter of the codon and distance from CO2 fixation as well as the second position of the anticodon and the hydrophobicity of the encoded amino acid.
The origin of the genetic code is an abiding mystery in biology. Hints of a 'code within the codons' suggest biophysical interactions, but these patterns have resisted interpretation. Here, we present a new framework, grounded in the autotrophic growth of protocells from CO2 and H-2. Recent work suggests that the universal core of metabolism recapitulates a thermodynamically favoured protometabolism right up to nucleotide synthesis. Considering the genetic code in relation to an extended protometabolism allows us to predict most codon as-signments. We show that the first letter of the codon corresponds to the distance from CO2 fixation, with amino acids encoded by the purines (G followed by A) being closest to CO2 fixation. These associations suggest a purine-rich early metabolism with a restricted pool of amino acids. The second position of the anticodon corresponds to the hydrophobicity of the amino acid encoded. We combine multiple measures of hydrophobicity to show that this correlation holds strongly for early amino acids but is weaker for later species. Finally, we demonstrate that redundancy at the third position is not randomly distributed around the code: non-redundant amino acids can be assigned based on size, specifically length. We attribute this to additional stereochemical interactions at the anticodon. These rules imply an iterative expansion of the genetic code over time with codon assignments depending on both distance from CO2 and biophysical interactions between nucleotide sequences and amino acids. In this way the earliest RNA polymers could produce non-random peptide sequences with selectable functions in autotrophic protocells.

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