Enzyme discovery beyond homology: a unique hydroxynitrile lyase in the Bet v1 superfamily

Elisa Lanfranchi; Tea Pavkov-Keller; Eva-Maria Koehler; Matthias Diepold; Kerstin Steiner; Barbara Darnhofer; Jürgen Hartler; Tom Van Den Bergh; Henk-Jan Joosten; Mandana Gruber-Khadjawi; Gerhard G Thallinger; Ruth Birner-Gruenberger; Karl Gruber; Margit Winkler; Anton Glieder

doi:10.1038/srep46738

Enzyme discovery beyond homology: a unique hydroxynitrile lyase in the Bet v1 superfamily

Elisa Lanfranchi, Tea Pavkov-Keller, Eva-Maria Koehler, Matthias Diepold, Kerstin Steiner, Barbara Darnhofer, Jürgen Hartler, Tom Van Den Bergh, Henk-Jan Joosten, Mandana Gruber-Khadjawi, Gerhard G Thallinger, Ruth Birner-Gruenberger, Karl Gruber, Margit Winkler, Anton Glieder

Institute of Molecular Biotechnology (6550)

Research output: Contribution to journal › Article › peer-review

Abstract

Homology and similarity based approaches are most widely used for the identification of new enzymes for biocatalysis. However, they are not suitable to find truly novel scaffolds with a desired function and this averts options and diversity. Hydroxynitrile lyases (HNLs) are an example of non-homologous isofunctional enzymes for the synthesis of chiral cyanohydrins. Due to their convergent evolution, finding new representatives is challenging. Here we show the discovery of unique HNL enzymes from the fern Davallia tyermannii by coalescence of transcriptomics, proteomics and enzymatic screening. It is the first protein with a Bet v1-like protein fold exhibiting HNL activity, and has a new catalytic center, as shown by protein crystallography. Biochemical properties of D. tyermannii HNLs open perspectives for the development of a complementary class of biocatalysts for the stereoselective synthesis of cyanohydrins. This work shows that systematic integration of -omics data facilitates discovery of enzymes with unpredictable sequences and helps to extend our knowledge about enzyme diversity.

Original language	English
Article number	46738
Journal	Scientific Reports
Volume	7
Early online date	3 May 2017
DOIs	https://doi.org/10.1038/srep46738
Publication status	Published - 10 May 2017

Fields of Expertise

Human- & Biotechnology

Access to Document

10.1038/srep46738

Discovery, characterization and application of carboxylic acid reductases
Margit Winkler (Speaker)
12 Nov 2018
Activity: Talk or presentation › Invited talk › Science to science

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Lanfranchi, E., Pavkov-Keller, T., Koehler, E-M., Diepold, M., Steiner, K., Darnhofer, B., Hartler, J., Van Den Bergh, T., Joosten, H-J., Gruber-Khadjawi, M., Thallinger, G. G., Birner-Gruenberger, R., Gruber, K., Winkler, M., & Glieder, A. (2017). Enzyme discovery beyond homology: a unique hydroxynitrile lyase in the Bet v1 superfamily. Scientific Reports, 7, Article 46738. https://doi.org/10.1038/srep46738

Lanfranchi, E, Pavkov-Keller, T, Koehler, E-M, Diepold, M, Steiner, K, Darnhofer, B, Hartler, J, Van Den Bergh, T, Joosten, H-J, Gruber-Khadjawi, M, Thallinger, GG, Birner-Gruenberger, R, Gruber, K , Winkler, M & Glieder, A 2017, 'Enzyme discovery beyond homology: a unique hydroxynitrile lyase in the Bet v1 superfamily', Scientific Reports, vol. 7, 46738. https://doi.org/10.1038/srep46738

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title = "Enzyme discovery beyond homology: a unique hydroxynitrile lyase in the Bet v1 superfamily",

abstract = "Homology and similarity based approaches are most widely used for the identification of new enzymes for biocatalysis. However, they are not suitable to find truly novel scaffolds with a desired function and this averts options and diversity. Hydroxynitrile lyases (HNLs) are an example of non-homologous isofunctional enzymes for the synthesis of chiral cyanohydrins. Due to their convergent evolution, finding new representatives is challenging. Here we show the discovery of unique HNL enzymes from the fern Davallia tyermannii by coalescence of transcriptomics, proteomics and enzymatic screening. It is the first protein with a Bet v1-like protein fold exhibiting HNL activity, and has a new catalytic center, as shown by protein crystallography. Biochemical properties of D. tyermannii HNLs open perspectives for the development of a complementary class of biocatalysts for the stereoselective synthesis of cyanohydrins. This work shows that systematic integration of -omics data facilitates discovery of enzymes with unpredictable sequences and helps to extend our knowledge about enzyme diversity.",

author = "Elisa Lanfranchi and Tea Pavkov-Keller and Eva-Maria Koehler and Matthias Diepold and Kerstin Steiner and Barbara Darnhofer and J{\"u}rgen Hartler and {Van Den Bergh}, Tom and Henk-Jan Joosten and Mandana Gruber-Khadjawi and Thallinger, {Gerhard G} and Ruth Birner-Gruenberger and Karl Gruber and Margit Winkler and Anton Glieder",

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AU - Lanfranchi, Elisa

AU - Pavkov-Keller, Tea

AU - Koehler, Eva-Maria

AU - Diepold, Matthias

AU - Steiner, Kerstin

AU - Darnhofer, Barbara

AU - Hartler, Jürgen

AU - Van Den Bergh, Tom

AU - Joosten, Henk-Jan

AU - Gruber-Khadjawi, Mandana

AU - Thallinger, Gerhard G

AU - Birner-Gruenberger, Ruth

AU - Gruber, Karl

AU - Winkler, Margit

AU - Glieder, Anton

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Y1 - 2017/5/10

N2 - Homology and similarity based approaches are most widely used for the identification of new enzymes for biocatalysis. However, they are not suitable to find truly novel scaffolds with a desired function and this averts options and diversity. Hydroxynitrile lyases (HNLs) are an example of non-homologous isofunctional enzymes for the synthesis of chiral cyanohydrins. Due to their convergent evolution, finding new representatives is challenging. Here we show the discovery of unique HNL enzymes from the fern Davallia tyermannii by coalescence of transcriptomics, proteomics and enzymatic screening. It is the first protein with a Bet v1-like protein fold exhibiting HNL activity, and has a new catalytic center, as shown by protein crystallography. Biochemical properties of D. tyermannii HNLs open perspectives for the development of a complementary class of biocatalysts for the stereoselective synthesis of cyanohydrins. This work shows that systematic integration of -omics data facilitates discovery of enzymes with unpredictable sequences and helps to extend our knowledge about enzyme diversity.

AB - Homology and similarity based approaches are most widely used for the identification of new enzymes for biocatalysis. However, they are not suitable to find truly novel scaffolds with a desired function and this averts options and diversity. Hydroxynitrile lyases (HNLs) are an example of non-homologous isofunctional enzymes for the synthesis of chiral cyanohydrins. Due to their convergent evolution, finding new representatives is challenging. Here we show the discovery of unique HNL enzymes from the fern Davallia tyermannii by coalescence of transcriptomics, proteomics and enzymatic screening. It is the first protein with a Bet v1-like protein fold exhibiting HNL activity, and has a new catalytic center, as shown by protein crystallography. Biochemical properties of D. tyermannii HNLs open perspectives for the development of a complementary class of biocatalysts for the stereoselective synthesis of cyanohydrins. This work shows that systematic integration of -omics data facilitates discovery of enzymes with unpredictable sequences and helps to extend our knowledge about enzyme diversity.

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VL - 7

JO - Scientific Reports

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ER -

Enzyme discovery beyond homology: a unique hydroxynitrile lyase in the Bet v1 superfamily

Abstract

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Discovery, characterization and application of carboxylic acid reductases

Cite this