Multifunctional P450 Monooxygenase CftA Diversifies the Clifednamide Pool through Tandem C–H Bond Activations

Yang, Jinping; Qi, Yunci; Blodgett, Joshua A. V.; Wencewicz, Timothy A.

doi:10.1021/acs.jnatprod.1c00606

Cited by 8 publications

(15 citation statements)

References 50 publications

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“…To date, all known PoTeM-associated CYPs are found to modify the polyketide moiety of PoTeMs, ,,,, and the 3-hydroxylation of the ornithine residue was exclusively catalyzed by C-3 hydroxylase, which belongs to the fatty acid desaturase family. , To provide direct evidence for the function of SahD and SahE, the corresponding genes were expressed in E. coli , and the purified enzymes were tested for activity with putative substrates. Since the native redox system required for the activity of SahD and SahE was unknown, the heterologous redox partners ferredoxin-NADP + reductase ( sel FdR0978) and ferredoxin ( sel Fdx1499) from Synechococcus elongates were used for the activity assay .…”

mentioning

confidence: 99%

Discovery of Oxidized Polycyclic Tetramate Macrolactams Bearing One or Two Rings through Combinatorial Pathway Reassembly

Zou

Xia

et al. 2022

Org. Lett.

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The structural diversity of polycyclic tetramate macrolactams (PoTeMs) are mainly generated by the cyclases and cytochrome P450s (CYPs). The PoTeM cluster sah in Saccharopolyspora hirsuta harboring two CYP genes was combinatorially reassembled and heterologously expressed in Streptomyces. As a result, six new cytotoxic PoTeMs, sahamides A−F (1−6), were discovered, and 1−3 are the first examples of oxidized one-ring PoTeMs. Remarkably, SahE represents the first CYP performing oxidative modification on the ornithine moiety of PoTeMs.

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mentioning

confidence: 99%

Discovery of Oxidized Polycyclic Tetramate Macrolactams Bearing One or Two Rings through Combinatorial Pathway Reassembly

Zou

Xia

et al. 2022

Org. Lett.

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“…The 5/5‐type pactamide C ( 6 ) was recognized by both IkaD and CftA as a substrate, and was mainly converted to pactamide M ( 6 a ), a C10 hydroxylated product (Figures 4C, S12, S20; Tables S9–S10). Pactamide M ( 6 a ) only displayed different stereochemistry on the 5/5 ring compared to combamide G, a product generated in vivo by Mg1D (a homolog of IkaD and CftA) [14b] . In addition to 6 a , both IkaD and CftA also produced the C10 and C29 dihydroxylated product 6 b , the structure of which was proposed based on that combamide G was reported to be converted in vivo to combamide B (with both C10 and C29 hydroxyl groups) by Mg1D.…”

Section: Resultsmentioning

confidence: 99%

“…For example, the P450 IkaD from Streptomyces xiamenensis 318 catalyzes the epoxidation of the C7=C8 double bond in ikarugamycin ( 1 ) to afford epoxyikarugamycin ( 1 a ), and a subsequent C29 hydroxylation, leading to capsimycin G ( 1 b ); [14e] in contrast, CftA from Streptomyces sp.JV178 (sharing ≈53 % sequence identity with IkaD) also uses 1 as the native substrate, and catalyzes a four‐electron oxidation at C29 of 1 to yield C29‐ketonyl in clifednamide A ( 1 c ), followed by a weak C30 hydroxylation to produce clifednamide C ( 1 d ) (Figure 1A). [15] Unlike other multifunctional P450s that are reported to be restricted to a single substrate, [16] in vivo combinatorial biosynthetic studies suggest that both IkaD and CftA display relaxed substrate flexibility to recognize multiple PoTeM substrates with different carbocycle ring systems [14b,17] (Figure 1B). Therefore, it provides a unique opportunity to study IkaD and CftA as models for interrogating the structure‐function relationship of multifunctional P450s, since they share the same substrate for multiple oxidations but display distinct oxidation patterns.…”

Section: Introductionmentioning

confidence: 99%

A Mechanistic Understanding of the Distinct Regio‐ and Chemoselectivity of Multifunctional P450s by Structural Comparison of IkaD and CftA Complexed with Common Substrates

Jiang,

Jin,

Zhang

et al. 2023

Angew Chem Int Ed

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Regio‐ and chemoselective C−H activation at multi‐positions of a single molecule is fascinating but chemically challenging. The homologous cytochrome P450 enzymes IkaD and CftA catalyze multiple C−H oxidations on the same polycyclic tetramate macrolactam (PoTeM) ikarugamycin, with distinct regio‐ and chemoselectivity. Herein we provide mechanistic understanding of their functional differences by solving crystal structures of IkaD and CftA in complex with ikarugamycin and unnatural substrates. Distinct conformations of the F/G region in IkaD and CftA are found to differentiate the orientation of PoTeM substrates, by causing different binding patterns with polar moieties to determine site selection, oxidation order, and chemoselectivity. Fine‐tuning the polar subpocket altered the regioselectivity of IkaD, indicating that substrate re‐orientation by mutating residues distal to the oxidation site could serve as an important method in future engineering of P450 enzymes.

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“…, transforming poorly reactive linear or cyclic alkanes to alcohols and alkenes to epoxides. 267–273 Fig. 10 summarizes bioelectrochemical transformations catalyzed by Cyt P450s, including heteroatom oxygenation, C-hydroxylation, S-oxidation, N-hydroxylation, epoxide formation and heteroatom dealkylation.…”

Section: Reactions Catalyzed By Cyt P450smentioning

confidence: 99%

Electrochemical transformations catalyzed by cytochrome P450s and peroxidases

Kumar

Rusling

2023

Chem. Soc. Rev.

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Multifunctional P450 Monooxygenase CftA Diversifies the Clifednamide Pool through Tandem C–H Bond Activations

Cited by 8 publications

References 50 publications

Discovery of Oxidized Polycyclic Tetramate Macrolactams Bearing One or Two Rings through Combinatorial Pathway Reassembly

Discovery of Oxidized Polycyclic Tetramate Macrolactams Bearing One or Two Rings through Combinatorial Pathway Reassembly

A Mechanistic Understanding of the Distinct Regio‐ and Chemoselectivity of Multifunctional P450s by Structural Comparison of IkaD and CftA Complexed with Common Substrates

Electrochemical transformations catalyzed by cytochrome P450s and peroxidases

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