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Alternative Reading Frames are an Underappreciated Source of Protein Sequence Novelty.

Zachary Ardern
Published in: Journal of molecular evolution (2023)
Protein-coding DNA sequences can be translated into completely different amino acid sequences if the nucleotide triplets used are shifted by a non-triplet amount on the same DNA strand or by translating codons from the opposite strand. Such "alternative reading frames" of protein-coding genes are a major contributor to the evolution of novel protein products. Recent studies demonstrating this include examples across the three domains of cellular life and in viruses. These sequences increase the number of trials potentially available for the evolutionary invention of new genes and also have unusual properties which may facilitate gene origin. There is evidence that the structure of the standard genetic code contributes to the features and gene-likeness of some alternative frame sequences. These findings have important implications across diverse areas of molecular biology, including for genome annotation, structural biology, and evolutionary genomics.
Keyphrases
  • genome wide
  • amino acid
  • genome wide identification
  • protein protein
  • copy number
  • dna methylation
  • working memory
  • single molecule
  • small molecule
  • binding protein
  • single cell
  • cell free