Evolution of a Human-Specific De Novo Open Reading Frame and Its Linked Transcriptional Silencer.

Int J Mol Sci

Department of Microbiology and Immunology, Renaissance School of Medicine, Stony Brook University, Stony Brook, NY 11794, USA.

Published: March 2024

AI Article Synopsis

  • - The study explores two open reading frames (ORFs) in the human genome, highlighting their distinct evolutionary paths and translational characteristics, one being ultra-conserved and originating over 462 million years ago, while the other, 107 amino acids long, emerged more recently in primate evolution from an ancestral non-coding region.
  • - The 107 aa ORF is suggested to play a crucial role in human brain development and has complex evolutionary origins within the Afrothere clade of placental mammals, indicating that it may have evolved through specific mutations, some of which led to dead ends.
  • - The findings on the regulatory silencer associated with the 107 aa ORF hint at its potential transcriptional control in embryonic development,

Article Abstract

In the human genome, two short open reading frames (ORFs) separated by a transcriptional silencer and a small intervening sequence stem from the gene . The two ORFs show different translational characteristics, and they also show divergent patterns of evolutionary development. The studies presented here describe the evolution of the components of . One ORF consists of an ultra-conserved 68 amino acid (aa) sequence, whose origins can be traced beyond the evolutionary age of divergence of the elephant shark, ~462 MYA. The silencer also has ancient origins, but it has a complex and divergent pattern of evolutionary formation, as it overlaps both at the 68 aa ORF and the intervening sequence. The other ORF consists of 107 aa. It develops during primate evolution but is found to originate de novo from an ancestral non-coding genomic region with root origins within the Afrothere clade of placental mammals, whose evolutionary age of divergence is ~99 MYA. The formation of the complete 107 aa ORF during primate evolution is outlined, whereby sequence development is found to occur through biased mutations, with disruptive random mutations that also occur but lead to a dead-end. The 107 aa ORF is of particular significance, as there is evidence to suggest it is a protein that may function in human brain development. Its evolutionary formation presents a view of a human-specific ORF and its linked silencer that were predetermined in non-primate ancestral species. The genomic position of the silencer offers interesting possibilities for the regulation of transcription of the 107 aa ORF. A hypothesis is presented with respect to possible spatiotemporal expression of the 107 aa ORF in embryonic tissues.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11011693PMC
http://dx.doi.org/10.3390/ijms25073924DOI Listing

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Evolution of a Human-Specific De Novo Open Reading Frame and Its Linked Transcriptional Silencer.

Int J Mol Sci

March 2024

Department of Microbiology and Immunology, Renaissance School of Medicine, Stony Brook University, Stony Brook, NY 11794, USA.

Article Synopsis
  • - The study explores two open reading frames (ORFs) in the human genome, highlighting their distinct evolutionary paths and translational characteristics, one being ultra-conserved and originating over 462 million years ago, while the other, 107 amino acids long, emerged more recently in primate evolution from an ancestral non-coding region.
  • - The 107 aa ORF is suggested to play a crucial role in human brain development and has complex evolutionary origins within the Afrothere clade of placental mammals, indicating that it may have evolved through specific mutations, some of which led to dead ends.
  • - The findings on the regulatory silencer associated with the 107 aa ORF hint at its potential transcriptional control in embryonic development,
View Article and Find Full Text PDF

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