Title : Critical assessment of structure-based approaches to improve protein resistance in aqueous ionic liquids by enzyme-wide saturation mutagenesis - El Harrar_2022_Comput.Struct.Biotechnol.J_20_399 |
Author(s) : El Harrar T , Davari MD , Jaeger KE , Schwaneberg U , Gohlke H |
Ref : Comput Struct Biotechnol J , 20 :399 , 2022 |
Abstract :
Ionic liquids (IL) and aqueous ionic liquids (aIL) are attractive (co-)solvents for green industrial processes involving biocatalysts, but often reduce enzyme activity. Experimental and computational methods are applied to predict favorable substitution sites and, most often, subsequent site-directed surface charge modifications are introduced to enhance enzyme resistance towards aIL. However, almost no studies evaluate the prediction precision with random mutagenesis or the application of simple data-driven filtering processes. Here, we systematically and rigorously evaluated the performance of 22 previously described structure-based approaches to increase enzyme resistance to aIL based on an experimental complete site-saturation mutagenesis library of Bacillus subtilis Lipase A (BsLipA) screened against four aIL. We show that, surprisingly, most of the approaches yield low gain-in-precision (GiP) values, particularly for predicting relevant positions: 14 approaches perform worse than random mutagenesis. Encouragingly, exploiting experimental information on the thermostability of BsLipA or structural weak spots of BsLipA predicted by rigidity theory yields GiP = 3.03 and 2.39 for relevant variants and GiP = 1.61 and 1.41 for relevant positions. Combining five simple-to-compute physicochemical and evolutionary properties substantially increases the precision of predicting relevant variants and positions, yielding GiP = 3.35 and 1.29. Finally, combining these properties with predictions of structural weak spots identified by rigidity theory additionally improves GiP for relevant variants up to 4-fold to -10 and sustains or increases GiP for relevant positions, resulting in a prediction precision of -90% compared to -9% in random mutagenesis. This combination should be applicable to other enzyme systems for guiding protein engineering approaches towards improved aIL resistance. |
PubMedSearch : El Harrar_2022_Comput.Struct.Biotechnol.J_20_399 |
PubMedID: 35070165 |
El Harrar T, Davari MD, Jaeger KE, Schwaneberg U, Gohlke H (2022)
Critical assessment of structure-based approaches to improve protein resistance in aqueous ionic liquids by enzyme-wide saturation mutagenesis
Comput Struct Biotechnol J
20 :399
El Harrar T, Davari MD, Jaeger KE, Schwaneberg U, Gohlke H (2022)
Comput Struct Biotechnol J
20 :399