Toxins (Jan 2023)

Brown Spider Venom Phospholipase-D Activity upon Different Lipid Substrates

  • Daniele Chaves-Moreira,
  • Luiza Helena Gremski,
  • Fábio Rogério de Moraes,
  • Larissa Vuitika,
  • Ana Carolina Martins Wille,
  • Jorge Enrique Hernández González,
  • Olga Meiri Chaim,
  • Andrea Senff-Ribeiro,
  • Raghuvir Krishnaswamy Arni,
  • Silvio Sanches Veiga

DOI
https://doi.org/10.3390/toxins15020109
Journal volume & issue
Vol. 15, no. 2
p. 109

Abstract

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Brown spider envenomation results in dermonecrosis, characterized by an intense inflammatory reaction. The principal toxins of brown spider venoms are phospholipase-D isoforms, which interact with different cellular membrane components, degrade phospholipids, and generate bioactive mediators leading to harmful effects. The Loxosceles intermedia phospholipase D, LiRecDT1, possesses a loop that modulates the accessibility to the active site and plays a crucial role in substrate. In vitro and in silico analyses were performed to determine aspects of this enzyme’s substrate preference. Sphingomyelin d18:1/6:0 was the preferred substrate of LiRecDT1 compared to other Sphingomyelins. Lysophosphatidylcholine 16:0/0:0 was preferred among other lysophosphatidylcholines, but much less than Sphingomyelin d18:1/6:0. In contrast, phosphatidylcholine d18:1/16:0 was not cleaved. Thus, the number of carbon atoms in the substrate plays a vital role in determining the optimal activity of this phospholipase-D. The presence of an amide group at C2 plays a key role in recognition and activity. In silico analyses indicated that a subsite containing the aromatic residues Y228 and W230 appears essential for choline recognition by cation-π interactions. These findings may help to explain why different cells, with different phospholipid fatty acid compositions exhibit distinct susceptibilities to brown spider venoms.

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