Structure-Based Engineering of Steroidogenic CYP260A1 for Stereo- and Regioselective Hydroxylation of Progesterone

Khatri, Yogan; Jozwik, I.K.; Ringle, Michael; Ionescu, Irina; Litzenburger, Martin; Hutter, Michael C.; Thunnissen, A.M.W.H.; Bernhardt, Rita

doi:10.1021/acschembio.8b00026

Cited by 29 publications

(30 citation statements)

References 46 publications

(96 reference statements)

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“…Structure-guided rational design was conducted to mutate S326 to an asparagine, resulting in mutant S326R that displayed much better activity and selectivity for the formation of Best CYP106A2 mutants on progesterone. Relative values [%] of progesterone substrate and monohydroxylated products (15β-, 11α-, 9α-and 6β) produced by CYP106A2 WT mutants A395I and G395W/G397K, and best combinatorially derived mutants in 6 h whole-cell biotransformations with 200 μM of progesterone (Nguyen et al 2012) 1α-hydroxy-11-deoxycorticosterone compared to the WT parent (Khatri et al 2018).…”

Section: Cyp260a1: Cytochrome P450 From Myxobacterium Sorangium Cellumentioning

confidence: 99%

“…In order to improve its regio-and stereoselectivity for progesterone transformation, Khatri et al cloned and expressed truncated protein of CYP260A1 (∆CYP260A1) (Khatri et al 2018), and the first 50 N-terminal residues were removed based on the alternative predicted gene transcript from the NCBI database (Khatri et al 2016a, b). Laborious efforts combining rational design and directed evolution were employed to create mutants of ∆CYP260A1 with improved regioselectivity towards progesterone hydroxylation (Khatri et al 2018). After recovery of complete activity of ∆CYP260A1, the substrate was docked into ∆CYP260A1 active site to explore potential hotspot residues.…”

Section: Cyp260a1: Cytochrome P450 From Myxobacterium Sorangium Cellumentioning

confidence: 99%

“…Relative values in % of progesterone and its monohydroxylated products 15β-, 11α-, 9α-and 6β-hydroxyprogesterone after 24 h in vivo conversion of 200 μM progesterone catalyzed by WT CYP106A2 and mutant proteins thereof. Values show percentages with the sum of the substrate progesterone and all monohydroxylated products set as 100% (n.d.*: not detectable) (Nikolaus et al 2017 (Khatri et al 2018). With the addition of position 17α to the above targeted positions, it is clear that directed evolution can generate highly regio-and stereoselective enzymes for challenging biotransformation.…”

Section: Table 2 Selection Of Cyp106a2 Mutants With Different Profilementioning

confidence: 99%

“…Engineering CYP260A1 for progesterone functionalization at positions 1α and 17α. Strategy for constructing mutants of CYP260A1 and experimental workflow(Khatri et al 2018) References Acevedo-Rocha CG, Gamble C, Lonsdale R, Li A, Nett N, Hoebenreich S, Deege A (2018) P450-catalyzed regio-and diastereoselective steroid hydroxylation: efficient directed evolution enabled by mutability landscaping. ACS Catal 8(4):3395-3410 Agematu H, Matsumoto N, Fujii Y, Kabumoto H, Doi S, Machia K, Arisawa A (2006) Hydroxylation of testosterone by bacterial cytochromes P450 using the Escherichia coli expression system.…”

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confidence: 99%

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Bacterial cytochrome P450-catalyzed regio- and stereoselective steroid hydroxylation enabled by directed evolution and rational design

Zhang

Peng

Zhao

et al. 2020

Bioresour. Bioprocess.

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Steroids are the most widely marketed products by the pharmaceutical industry after antibiotics. Steroid hydroxylation is one of the most important functionalizations because their derivatives enable a higher biological activity compared to their less polar non-hydroxylated analogs. Bacterial cytochrome P450s constitute promising biocatalysts for steroid hydroxylation due to their high expression level in common workhorses like Escherichia coli. However, they often suffer from wrong or insufficient regio-and/or stereoselectivity, low activity, narrow substrate range as well as insufficient thermostability, which hampers their industrial application. Fortunately, these problems can be generally solved by protein engineering based on directed evolution and rational design. In this work, an overview of recent developments on the engineering of bacterial cytochrome P450s for steroid hydroxylation is presented.

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Section: Cyp260a1: Cytochrome P450 From Myxobacterium Sorangium Cellumentioning

confidence: 99%

Section: Cyp260a1: Cytochrome P450 From Myxobacterium Sorangium Cellumentioning

confidence: 99%

Section: Table 2 Selection Of Cyp106a2 Mutants With Different Profilementioning

confidence: 99%

mentioning

confidence: 99%

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Bacterial cytochrome P450-catalyzed regio- and stereoselective steroid hydroxylation enabled by directed evolution and rational design

Zhang

Peng

Zhao

et al. 2020

Bioresour. Bioprocess.

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show abstract

“…Such a map of the sequence‐function relationship was generated for the F87A template enzyme by analysing previous data from Commandeur et al ., Payne et al ., and their own lab, and by screening mutants available from a previous study . For example the group of Commandeur had identified residue 72 to be important for substrate orientation, and showed that it was completely inverting the stereoselectivity of C16 hydroxylation .…”

Section: Examplesmentioning

confidence: 99%

P450 Monooxygenases Enable Rapid Late‐Stage Diversification of Natural Products via C−H Bond Activation

Fessner

2019

ChemCatChem

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The biological potency of natural products has been exploited for decades. Their inherent structural complexity and natural diversity might hold the key to efficiently address the urgent need for the development of novel pharmaceuticals. At the same time, it is that very complexity, which impedes necessary chemical modifications such as structural diversification, to improve the effectiveness of the drug. For this purpose, Cytochrome P450 enzymes, which possess unique abilities to activate inert sp3‐hybridised C−H bonds in a late‐stage fashion, offer an attractive synthetic tool. In this review the potential of cytochrome P450 enzymes in chemoenzymatic lead diversification is illustrated discussing studies reporting late‐stage functionalisations of natural products and other high‐value compounds. These enzymes were proven to extend the synthetic toolbox significantly by adding to the flexibility and efficacy of synthetic strategies of natural product chemists, and scientists of other related disciplines.

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Cytochrome P450 Monooxygenases Catalyse Steroid Nucleus Hydroxylation with Regio‐ and Stereo‐Selectivity

et al. 2022

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Steroids are the second largest class of drugs with a wide range of pharmacological properties. Hydroxylation of steroids seriously affects their biological activities and other properties. However, steroids are mostly sp 3 hybridized carbons with numerous CÀ H bonds far from the functional group that can activate them, and achieving regio-and stereo-selective hydroxylation on steroids is a highly challenging task that is almost impossible to achieve using modern organic synthesis techniques. Interestingly, cytochrome P450 monooxygenases possess the ability to catalyse regio-and stereo-selective oxidations of nonactivated CÀ H bonds in complex organic molecules under mild conditions. This review summarizes the P450s identified and engineered in recent years that can catalyse steroid nucleus hydroxylation stereo-and regio-selectively.1.

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Structure-Based Engineering of Steroidogenic CYP260A1 for Stereo- and Regioselective Hydroxylation of Progesterone

Cited by 29 publications

References 46 publications

Bacterial cytochrome P450-catalyzed regio- and stereoselective steroid hydroxylation enabled by directed evolution and rational design

Bacterial cytochrome P450-catalyzed regio- and stereoselective steroid hydroxylation enabled by directed evolution and rational design

P450 Monooxygenases Enable Rapid Late‐Stage Diversification of Natural Products via C−H Bond Activation

Cytochrome P450 Monooxygenases Catalyse Steroid Nucleus Hydroxylation with Regio‐ and Stereo‐Selectivity

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