Expansion of the Catalytic Repertoire of Alcohol Dehydrogenases in Plant Metabolism

Langley, Chloe; Tatsis, Evangelos E.; Hong, Bo; Nakamura, Yoko; Paetz, Christian; Stevenson, Clare E. M.; Basquin, J.; Lawson, David M.; Caputi, Lorenzo; O’Connor, Sarah E.

doi:10.1101/2022.07.24.501124

Cited by 2 publications

(10 citation statements)

References 43 publications

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“…We isolated isotopically labeled (–)-tabersonine ( 2 ), Ψ-tabersonine ( 5 ), and Ψ-vincadifformine ( 9 ) and showed that the deuterium labels were incorporated at carbon 19 for (–)-tabersonine ( 2 ) as expected, 13 carbons 19 and 21 for Ψ-tabersonine ( 5 ), carbons and 19, 21, 15 for Ψ-vincadifformine ( 9 ) ( Figure 4) . We performed CD spectroscopy of these isolated products and assigned the stereochemistry as (+)-Ψ-tabersonine ( 5 ) and (+)-Ψ-vincadifformine ( 9 ), which is the expected stereochemistry based on the downstream ibophyllidine products (Figure S16).…”

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confidence: 57%

“…The (-)-tabersonine (2) product produced by TiTabS had no deuterium incorporation, as expected; for-mation of Ψ-tabersonine (5) and Ψ-vincadifformine (9) from angryline (1a) showed incorporation of one and deuterium atoms respectively and was strictly dependent upon the presence of both reductase, TiDPAS1, and dase, PAS (Figure S15). We isolated isotopically labeled (-)-tabersonine (2), Ψ-tabersonine (5), and Ψ-vincadifformine (9) and show that the deuterium labels were incorporated at carbon 19 for (-)-tabersonine (2) as expected, 13 carbons 19 and for Ψ-tabersonine (5), carbons and 19, 21, 15 for Ψ-vincadifformine (9) (Figure 4). We performed CD spect copy of these isolated products and assigned the stereochemistry as (+)-Ψ-tabersonine ( 5) and (+) vincadifformine (9), which is the expected stereochemistry based on the downstream ibophyllidine products (F ure S16).…”

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confidence: 58%

“…With TiTabS, we saw formation of the (-)tabersonine (2) product with a mass consistent with incorporation of one deuterium, as expected from the action of DPAS acting on precondylocarpine acetate (7) (Figure 4). 13 However, when TiCorS was substituted for TiTabS, the resulting Ψ-tabersonine (5) product had a mass consistent with incorporation of two deuterium atoms (Figure 4 and Figure S14), clearly demonstrating that formation of Ψ-tabersonine (5) from stemmadenine acetate (6) requires two reduction steps. Furthermore, the Ψ-vincadifformine (9) product showed a mass incorporation of three deuterium atoms (Figure 4 and Figure S14).…”

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confidence: 99%

“…Stemmadenine acetate ( 6) is first oxidized by flavin dependent enzyme precondylocarpine acetate synthase (PAS) 5 to generate precondylocarpine acetate and then undergoes a 1,4-iminium reduction by the medium chain alcohol dehydrogen dihydroprecondylocarpine acetate synthase (DPAS) (Figure 1). 13 The resulting reduced unstable prod dihydroprecondylocarpine acetate (8), undergoes elimination of an acetoxy group to yield dehydrosecodine which is then captured by one of the cyclases (Figure 1).…”

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confidence: 99%

“…Therefore, we performed the reaction in the presence of isotopically labelled NADPH (pro-(R)-NADPD) to deter-mine where the deuteride is incorporated in Ψ-tabersonine (5). 13,17,18 We incubated stemmadenine acetate (6) with CrPAS, TiDPAS1, and TiCorS or TiTabS, along with pro-(R)-NADPD, which is required for DPAS reduction (Figure S14). With TiTabS, we saw formation of the (-)tabersonine (2) product with a mass consistent with incorporation of one deuterium, as expected from the action of DPAS acting on precondylocarpine acetate (7) (Figure 4).…”

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Recycling upstream redox enzymes expands the regioselectivity of cycloaddition in pseudo-aspidosperma alkaloid biosynthesis

Kamileen

DeMars

Hong

et al. 2022

Preprint

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Nature uses cycloaddition reactions to generate complex natural product scaffolds. Dehydrosecodine is a highly reactive biosynthetic intermediate that undergoes cycloaddition to generate several alkaloid scaffolds that are the precursors to pharmacologically important compounds such as vinblastine and ibogaine. Here we report how dehydrosecodine can be subjected to redox chemistry, which in turn allows cycloaddition reactions with alternative regioselectivity. By incubating dehydrosecodine with reductase and oxidase bio-synthetic enzymes that act upstream in the pathway, we can access the rare pseudo-aspidosperma alkaloids, pseudo-tabersonine and pseudo-vincadifformine, both in vitro and by reconstitution in the plant Nicotiana benthamiana from an upstream intermediate. We propose a stepwise mechanism to explain the formation of the pseudo-tabersonine scaffold by structurally characterizing enzyme intermediates, and by monitoring the incorporation of deuterium labels. This discovery highlights how plants use redox enzymes to enantioselec-tively generate new scaffolds from common precursors.

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confidence: 57%

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confidence: 58%

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confidence: 99%

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confidence: 99%

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confidence: 99%

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Recycling upstream redox enzymes expands the regioselectivity of cycloaddition in pseudo-aspidosperma alkaloid biosynthesis

Kamileen

DeMars

Hong

et al. 2022

Preprint

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Recycling Upstream Redox Enzymes Expands the Regioselectivity of Cycloaddition in Pseudo-Aspidosperma Alkaloid Biosynthesis

et al. 2022

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Nature uses cycloaddition reactions to generate complex natural product scaffolds. Dehydrosecodine is a highly reactive biosynthetic intermediate that undergoes cycloaddition to generate several alkaloid scaffolds that are the precursors to pharmacologically important compounds such as vinblastine and ibogaine. Here we report how dehydrosecodine can be subjected to redox chemistry, which in turn allows cycloaddition reactions with alternative regioselectivity. By incubating dehydrosecodine with reductase and oxidase biosynthetic enzymes that act upstream in the pathway, we can access the rare pseudoaspidosperma alkaloids pseudo-tabersonine and pseudo-vincadifformine, both in vitro and by reconstitution in the plant Nicotiana benthamiana from an upstream intermediate. We propose a stepwise mechanism to explain the formation of the pseudo-tabersonine scaffold by structurally characterizing enzyme intermediates and by monitoring the incorporation of deuterium labels. This discovery highlights how plants use redox enzymes to enantioselectively generate new scaffolds from common precursors.

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Expansion of the Catalytic Repertoire of Alcohol Dehydrogenases in Plant Metabolism

Cited by 2 publications

References 43 publications

Recycling upstream redox enzymes expands the regioselectivity of cycloaddition in pseudo-aspidosperma alkaloid biosynthesis

Recycling upstream redox enzymes expands the regioselectivity of cycloaddition in pseudo-aspidosperma alkaloid biosynthesis

Recycling Upstream Redox Enzymes Expands the Regioselectivity of Cycloaddition in Pseudo-Aspidosperma Alkaloid Biosynthesis

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