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Elucidating the Ionic Liquid-Induced Mixed Inhibition of GH1 β-Glucosidase H0HC94.

Bharat MannaPinaki ChandaSupratim DattaAmit Ghosh
Published in: The journal of physical chemistry. B (2023)
Deciphering the ionic liquid (IL) tolerance of glycoside hydrolases (GHs) to improve their hydrolysis efficiency for fermentable sugar synthesis in the "one-pot" process has long been a hurdle for researchers. In this work, we employed experimental and theoretical approaches to investigate the 1-ethyl-3-methylimidazolium acetate ([C 2 C 1 im][MeCO 2 ])-induced inhibition of GH1 β-glucosidase (H0HC94) from Agrobacterium tumefaciens 5A. At 10-15% [C 2 C 1 im][MeCO 2 ] concentration, H0HC94 experiences competitive inhibition ( R 2 = 0.97, alpha = 2.8). As the IL content increased to 20-25%, the inhibition pattern shifted to mixed-type inhibition ( R 2 = 0.98, alpha = 3.4). These findings were further confirmed through characteristic inhibition plots using Lineweaver-Burk plots. Atomistic molecular dynamics simulations conducted with 0% [C 2 C 1 im][MeCO 2 ], 10% [C 2 C 1 im][MeCO 2 ], and 25% [C 2 C 1 im][MeCO 2 ] revealed the accumulation of [C 2 C 1 im] + at the negatively charged active site of H0HC94 in 10% [C 2 C 1 im][MeCO 2 ], supporting the occurrence of competitive inhibition at lower IL concentrations. At higher IL concentrations, the cations and anions bound to the secondary binding sites (SBSs) of H0HC94, leading to a tertiary conformational change, as captured by the principal component analysis based on the free-energy landscape and protein structure networks. The altered conformation of H0HC94 affected the interaction with [C 2 C 1 im][MeCO 2 ], which could possibly shift the inhibition from competitive to more mixed-type (competitive + noncompetitive) inhibition, as observed in the experiments. For the first time, we report a combined experimental and theoretical insight behind the mixed inhibition of a GH1 β-glucosidase. Our findings indicated the role of SBS in IL-induced inhibition, which could aid in developing more IL-tolerant β-glucosidases for biorefinery applications.
Keyphrases
  • ionic liquid
  • molecular dynamics simulations
  • molecular docking
  • high glucose
  • risk assessment
  • mental health
  • endothelial cells
  • binding protein