Mutagenesis-Independent Stabilization of Class B Flavin Monooxygenases in Operation

Leticia C.P. Goncalves; Daniel Kracher; Sofia Milker; Michael J. Fink; Florian Rudroff; Roland Ludwig; Andreas S. Bommarius; Marko D. Mihovilovic

doi:10.1002/adsc.201700585

Mutagenesis-Independent Stabilization of Class B Flavin Monooxygenases in Operation

Leticia C.P. Goncalves, Daniel Kracher, Sofia Milker, Michael J. Fink^*, Florian Rudroff, Roland Ludwig, Andreas S. Bommarius, Marko D. Mihovilovic

^*Korrespondierende/r Autor/-in für diese Arbeit

Publikation: Beitrag in einer Fachzeitschrift › Artikel › Begutachtung

Abstract

This paper describes the stabilization of flavin-dependent monooxygenases under reaction conditions, using an engineered formulation of additives (the natural cofactors NADPH and FAD, and superoxide dismutase and catalase as catalytic antioxidants). This way, a 10³- to 10⁴-fold increase of the half-life was reached without resource-intensive directed evolution or structure-dependent protein engineering methods. The stabilized enzymes are highly valued for their synthetic potential in biotechnology and medicinal chemistry (enantioselective sulfur, nitrogen and Baeyer–Villiger oxidations; oxidative human metabolism), but widespread application was so far hindered by their notorious fragility. Our technology immediately enables their use, does not require structural knowledge of the biocatalyst, and creates a strong basis for the targeted development of improved variants by mutagenesis. (Figure presented.).

Originalsprache	englisch
Seiten (von - bis)	2121-2131
Seitenumfang	11
Fachzeitschrift	Advanced Synthesis and Catalysis
Jahrgang	359
Ausgabenummer	12
DOIs	https://doi.org/10.1002/adsc.201700585
Publikationsstatus	Veröffentlicht - 19 Juni 2017
Extern publiziert	Ja

ASJC Scopus subject areas

Katalyse
Organische Chemie

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title = "Mutagenesis-Independent Stabilization of Class B Flavin Monooxygenases in Operation",

abstract = "This paper describes the stabilization of flavin-dependent monooxygenases under reaction conditions, using an engineered formulation of additives (the natural cofactors NADPH and FAD, and superoxide dismutase and catalase as catalytic antioxidants). This way, a 103- to 104-fold increase of the half-life was reached without resource-intensive directed evolution or structure-dependent protein engineering methods. The stabilized enzymes are highly valued for their synthetic potential in biotechnology and medicinal chemistry (enantioselective sulfur, nitrogen and Baeyer–Villiger oxidations; oxidative human metabolism), but widespread application was so far hindered by their notorious fragility. Our technology immediately enables their use, does not require structural knowledge of the biocatalyst, and creates a strong basis for the targeted development of improved variants by mutagenesis. (Figure presented.).",

keywords = "biocatalysis, cofactors, enzyme stabilization, oxygenation, reactive oxygen species",

author = "Goncalves, {Leticia C.P.} and Daniel Kracher and Sofia Milker and Fink, {Michael J.} and Florian Rudroff and Roland Ludwig and Bommarius, {Andreas S.} and Mihovilovic, {Marko D.}",

note = "Funding Information: We thank David Siebert (TU Wien) for the purification of FAD, Dr. Anna M{\"u}nch (NanoTemper Technologies GmbH) for generously providing access to the DSF fluorimeter, and Prof. Marco W. Fraaije (University of Groningen) for kindly providing a sample of the CHMO-PTDH fusion enzyme. This work was supported by the Austrian Science Fund FWF (grants no. I723-N17 and P24483-B20), by the COST action Systems Biocatalysis WG2, by TU Wien (ABC-Top Anschubfinanzierung), by the European Commission Project INDOX (grant no. FP7-KBBE-2013-7-613549), and by the Coordination for the Improvement of Higher Education Personnel (grant no. CAPES/CsF, 2505-13-4). Publisher Copyright: {\textcopyright} 2017 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim",

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month = jun,

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doi = "10.1002/adsc.201700585",

language = "English",

volume = "359",

pages = "2121--2131",

journal = "Advanced Synthesis and Catalysis",

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T1 - Mutagenesis-Independent Stabilization of Class B Flavin Monooxygenases in Operation

AU - Goncalves, Leticia C.P.

AU - Kracher, Daniel

AU - Milker, Sofia

AU - Fink, Michael J.

AU - Rudroff, Florian

AU - Ludwig, Roland

AU - Bommarius, Andreas S.

AU - Mihovilovic, Marko D.

N1 - Funding Information: We thank David Siebert (TU Wien) for the purification of FAD, Dr. Anna Münch (NanoTemper Technologies GmbH) for generously providing access to the DSF fluorimeter, and Prof. Marco W. Fraaije (University of Groningen) for kindly providing a sample of the CHMO-PTDH fusion enzyme. This work was supported by the Austrian Science Fund FWF (grants no. I723-N17 and P24483-B20), by the COST action Systems Biocatalysis WG2, by TU Wien (ABC-Top Anschubfinanzierung), by the European Commission Project INDOX (grant no. FP7-KBBE-2013-7-613549), and by the Coordination for the Improvement of Higher Education Personnel (grant no. CAPES/CsF, 2505-13-4). Publisher Copyright: © 2017 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim

PY - 2017/6/19

Y1 - 2017/6/19

N2 - This paper describes the stabilization of flavin-dependent monooxygenases under reaction conditions, using an engineered formulation of additives (the natural cofactors NADPH and FAD, and superoxide dismutase and catalase as catalytic antioxidants). This way, a 103- to 104-fold increase of the half-life was reached without resource-intensive directed evolution or structure-dependent protein engineering methods. The stabilized enzymes are highly valued for their synthetic potential in biotechnology and medicinal chemistry (enantioselective sulfur, nitrogen and Baeyer–Villiger oxidations; oxidative human metabolism), but widespread application was so far hindered by their notorious fragility. Our technology immediately enables their use, does not require structural knowledge of the biocatalyst, and creates a strong basis for the targeted development of improved variants by mutagenesis. (Figure presented.).

AB - This paper describes the stabilization of flavin-dependent monooxygenases under reaction conditions, using an engineered formulation of additives (the natural cofactors NADPH and FAD, and superoxide dismutase and catalase as catalytic antioxidants). This way, a 103- to 104-fold increase of the half-life was reached without resource-intensive directed evolution or structure-dependent protein engineering methods. The stabilized enzymes are highly valued for their synthetic potential in biotechnology and medicinal chemistry (enantioselective sulfur, nitrogen and Baeyer–Villiger oxidations; oxidative human metabolism), but widespread application was so far hindered by their notorious fragility. Our technology immediately enables their use, does not require structural knowledge of the biocatalyst, and creates a strong basis for the targeted development of improved variants by mutagenesis. (Figure presented.).

KW - biocatalysis

KW - cofactors

KW - enzyme stabilization

KW - oxygenation

KW - reactive oxygen species

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JO - Advanced Synthesis and Catalysis

JF - Advanced Synthesis and Catalysis

IS - 12

ER -

Mutagenesis-Independent Stabilization of Class B Flavin Monooxygenases in Operation

Abstract

ASJC Scopus subject areas

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