International Journal of Molecular Sciences (Jun 2023)

Enhancing the Catalytic Activity of Thermo-Asparaginase from <i>Thermococcus sibiricus</i> by a Double Mesophilic-like Mutation in the Substrate-Binding Region

  • Maria Dumina,
  • Dmitry Zhdanov,
  • Alexander Zhgun,
  • Marina Pokrovskaya,
  • Svetlana Aleksandrova,
  • Alexander Veselovsky,
  • Michael El’darov

DOI
https://doi.org/10.3390/ijms24119632
Journal volume & issue
Vol. 24, no. 11
p. 9632

Abstract

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L-asparaginases (L-ASNases) of microbial origin are the mainstay of blood cancer treatment. Numerous attempts have been performed for genetic improvement of the main properties of these enzymes. The substrate-binding Ser residue is highly conserved in L-ASNases regardless of their origin or type. However, the residues adjacent to the substrate-binding Ser differ between mesophilic and thermophilic L-ASNases. Based on our suggestion that the triad, including substrate-binding Ser, either GSQ for meso-ASNase or DST for thermo-ASNase, is tuned for efficient substrate binding, we constructed a double mutant of thermophilic L-ASNase from Thermococcus sibiricus (TsA) with a mesophilic-like GSQ combination. In this study, the conjoint substitution of two residues adjacent to the substrate-binding Ser55 resulted in a significant increase in the activity of the double mutant, reaching 240% of the wild-type enzyme activity at the optimum temperature of 90 °C. The mesophilic-like GSQ combination in the rigid structure of the thermophilic L-ASNase appears to be more efficient in balancing substrate binding and conformational flexibility of the enzyme. Along with increased activity, the TsA D54G/T56Q double mutant exhibited enhanced cytotoxic activity against cancer cell lines with IC90 values from 2.8- to 7.4-fold lower than that of the wild-type enzyme.

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