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Structures of annexin A2-PS DNA complexes show dominance of hydrophobic interactions in phosphorothioate binding. | LitMetric

AI Article Synopsis

  • - The introduction of phosphorothioate (PS) linkages in therapeutic nucleic acids boosts their stability and effectiveness while altering their interactions with cellular proteins, though the underlying mechanisms are not well understood.
  • - This study focuses on annexin A2, a protein without traditional DNA binding capabilities, revealing that hydrophobic interactions between sulfur in PS groups and specific amino acids (lysine and arginine) significantly strengthen the binding affinity between the modified nucleic acids and the protein.
  • - Additionally, the research found that the stereoisomer preference of PS oligonucleotides is influenced by the hydrophobic environment surrounding the PS linkages, which is shaped by both the protein and structural components in the oligonucleotide like 5-Me

Article Abstract

The introduction of phosphorothioate (PS) linkages to the backbone of therapeutic nucleic acids substantially increases their stability and potency. It also affects their interactions with cellular proteins, but the molecular mechanisms that underlie this effect are poorly understood. Here, we report structural and biochemical studies of interactions between annexin A2, a protein that does not possess any known canonical DNA binding domains, and phosphorothioate-modified antisense oligonucleotides. We show that a unique mode of hydrophobic interactions between a sulfur atom of the phosphorothioate group and lysine and arginine residues account for the enhanced affinity of modified nucleic acid for the protein. Our results demonstrate that this mechanism of interaction is observed not only for nucleic acid-binding proteins but can also account for the association of PS oligonucleotides with other proteins. Using the anomalous diffraction of sulfur, we showed that preference for phosphorothioate stereoisomers is determined by the hydrophobic environment around the PS linkage that comes not only from protein but also from additional structural features within the ASO such as 5-Me groups on cytosine nucleobases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9943651PMC
http://dx.doi.org/10.1093/nar/gkac774DOI Listing

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