AI Article Synopsis

  • The tetrapod proteins ARC and dARC1 are related but have distinct roles in neuron development, stemming from an ancient retrotransposon.
  • The crystal structure of dARC1 CA shows that it has similarities to retroviral CA proteins but with significant differences in certain terminal domains.
  • These differences indicate that dARC1 and mammalian ARC are adaptations of the same ancestral protein, but they evolved separately in tetrapods and insects.

Article Abstract

The tetrapod neuronal protein ARC and its homolog, dARC1, have important but differing roles in neuronal development. Both are thought to originate through exaptation of ancient Ty3/Gypsy retrotransposon Gag, with their novel function relying on an original capacity for self-assembly and encapsidation of nucleic acids. Here, we present the crystal structure of dARC1 CA and examine the relationship between dARC1, mammalian ARC, and the CA protein of circulating retroviruses. We show that while the overall architecture is highly related to that of orthoretroviral and spumaretroviral CA, there are substantial deviations in both amino- and carboxyl-terminal domains, potentially affecting recruitment of partner proteins and particle assembly. The degree of sequence and structural divergence suggests that Ty3/Gypsy Gag has been exapted on two separate occasions and that, although mammalian ARC and dARC1 share functional similarity, the structures have undergone different adaptations after appropriation into the tetrapod and insect genomes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6938703PMC
http://dx.doi.org/10.1126/sciadv.aay6354DOI Listing

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