P450-Mediated Coupling of Indole Fragments To Forge Communesin and Unnatural Isomers

Lin, Hsiao‐Ching; McMahon, Travis C.; Patel, Ashay; Corsello, Michael A.; Simon, Adam J.; Xu, Wei; Zhao, Min; Houk, K. N.; Garg, Neil K.; Tang, Yi

doi:10.1021/jacs.6b01413

Cited by 60 publications

(54 citation statements)

References 36 publications

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“…23 Significantly, only the desired heptacycle 52 was formed in preference to other constitutional isomers. 15b Methanol was found to be an excellent solvent 38 for this transformation, likely due to its ability to stabilize reactive intermediates as the corresponding O -alkyl-hemiaminals. Although intermediate 52 could be observed by in situ 1 H NMR spectroscopy, 23 this compound did not show sufficient stability for isolation.…”

Section: Resultsmentioning

confidence: 99%

“…A highly convergent enantioselective total synthesis of (−)-communesin F ( 1 ) with late-stage chemistry that parallels the latest insights 15 and hypotheses concerning the biogenesis of these alkaloids is described. Our expedient synthesis involves the union of fragments (+)- 24 and (+)- 27 to provide complex sulfamide (+)- 50 on gram-scale.…”

Section: Resultsmentioning

confidence: 99%

“…12,14, While our biosynthetic considerations were purely hypothetical at the outset of this synthesis campaign, Houk, Garg, and Tang have recently disclosed 15 incisive biosynthetic and computational studies that echo the key transformations developed in our synthesis. Herein, we present the shortest enantioselective total chemical synthesis of (−)-communesin F ( 1 ) with late-stage chemistry that fortuitously parallels the latest insights 15b and hypotheses concerning the biogenesis of these alkaloids.…”

Section: Introductionmentioning

confidence: 97%

“…Consistent with this hypothesis, an enzyme capable of the oxidative coupling of tryptamines and Penicillium fungal alkaloid (−)-aurantioclavine ( 12 ) 17,18 has been identified that leads to the formation of the communesin core or an isomeric heptacycle depending on the tryptamine. 15b We began our studies with the recognition that successful implementation of a biomimetic strategy for the efficient synthesis of these alkaloids requires the directed and stereocontrolled union of two dissimilar fragments followed by selective reorganization of a C3a–C3a′ linked heterodimer to a single constitutional isomer consistent with the communesin skeleton 18 .…”

Section: Introductionmentioning

confidence: 99%

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Convergent and Biomimetic Enantioselective Total Synthesis of (−)-Communesin F

et al. 2016

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The first biomimetic enantioselective total synthesis of (−)-communesin F based on a late-stage heterodimerization and aminal exchange is described. Our synthesis features the expedient diazene–directed assembly of two advanced fragments to secure the congested C3a–C3a′ linkage in three steps, followed by a highly efficient biogenetically inspired aminal reorganization to access the heptacyclic communesin core in only two additional steps. Enantioselective syntheses of the two fragments were developed, with highlights including the catalytic asymmetric halocyclization and diastereoselective oxyamination reactions of tryptamine derivatives, a stereoselective sulfinimine allylation, and an efficient cyclotryptamine–C3a-sulfamate synthesis by either a new silver–promoted nucleophilic amination or a rhodium–catalyzed C–H amination protocol. The versatile synthesis of the fragments, their stereocontrolled assembly, and the efficient aminal–exchange as supported by in situ monitoring experiments, in addition to the final stage N1′-acylation of the communesin core provide a highly convergent synthesis of (−)-communesin F.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 97%

Section: Introductionmentioning

confidence: 99%

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Convergent and Biomimetic Enantioselective Total Synthesis of (−)-Communesin F

et al. 2016

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“…While numerous total syntheses of communesin have been reported, 77–87 the biosynthetic pathway was only recently uncovered from P. expansum and was shown to be highly efficient (Scheme 15). 88,89 The two indole-containing building blocks are tryptamine ( 50 ) derived from decarboxylation of L-tryptophan, and (−)-aurantioclavine ( 53 ) derived from the decarboxylative cyclization of 4-dimethylallyltryptophan. A P450 enzyme (CnsC) was found to be solely responsible in combining the two fragments to generate the core structure 63 , which is one N- methylation step away from the stable communesin K ( 65 ).…”

Section: Radical Cyclization Mechanismsmentioning

confidence: 99%

Oxidative Cyclization in Natural Product Biosynthesis

et al. 2016

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Oxidative cyclizations are important transformations that occur widely during natural product biosynthesis. The transformations from acyclic precursors to cyclized products can afford morphed scaffolds, structural rigidity and biological activities. Some of the most dramatic structural alterations in natural product biosynthesis occur through oxidative cyclization. In this review, we examine the different strategies used by Nature to create new intra-(inter-)-molecular bonds via redox chemistry. The review will cover both oxidation- and reduction-enabled cyclization mechanisms, with an emphasis on the former. Radical cyclizations catalyzed by P450, nonheme iron, α-KG dependent oxygenases and radical SAM enzymes are discussed to illustrate the use of molecular oxygen and S-adenosylmethionine to forge new bonds at unactivated sites via one-electron manifolds. Nonradical cyclizations catalyzed by flavin-dependent monooxygenases and NAD(P)H-dependent reductases are covered to show the use of two-electron manifolds in initiating cyclization reactions. The oxidative installation of epoxides and halogens into acyclic scaffolds to drive subsequent cyclizations are separately discussed as examples of “disappearing” reactive handles. Lastly, oxidative rearrangement of rings systems, including contractions and expansions will be covered.

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Exploring the Diverse Landscape of Fungal Cytochrome P450‐Catalyzed Regio‐ and Stereoselective Dimerization of Diketopiperazines

Ma,

Wang,

Zhang

et al. 2024

Advanced Science

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Dimeric indole‐containing diketopiperazines (di‐DKPs) are a diverse group of natural products produced through cytochrome P450‐catalyzed C–C or C–N coupling reactions. The regio‐ and stereoselectivity of these reactions plays a significant role in the structural diversity of di‐DKPs. Despite their pivotal role, the mechanisms governing the selectivity in fungi are not fully understood. Employing bioinformatics analysis and heterologous expression experiments, five undescribed P450 enzymes (AmiP450, AcrP450, AtP450, AcP450, and AtuP450) responsible for the regio‐ and stereoselective dimerization of diketopiperazines (DKPs) in fungi are identified. The function of these P450s is consistent with phylogenetic analysis, highlighting their dominant role in controlling the dimerization modes. Combinatorial biosynthesis‐based pathway reconstitution of non‐native gene clusters expands the chemical space of fungal di‐DKPs and reveals that the regioselectivity is influenced by the substrate. Furthermore, multiple sequence alignment and molecular docking of these enzymes demonstrate a C‐terminal variable region near the substrate tunnel entrance in AtuP450 that is crucial for its regioselectivity. These findings not only reveal the secret of fungal di‐DKPs diversity but also deepen understanding of the mechanisms and catalytic specificity involved in P450‐catalyzed dimerization reactions.

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P450-Mediated Coupling of Indole Fragments To Forge Communesin and Unnatural Isomers

Cited by 60 publications

References 36 publications

Convergent and Biomimetic Enantioselective Total Synthesis of (−)-Communesin F

Convergent and Biomimetic Enantioselective Total Synthesis of (−)-Communesin F

Oxidative Cyclization in Natural Product Biosynthesis

Exploring the Diverse Landscape of Fungal Cytochrome P450‐Catalyzed Regio‐ and Stereoselective Dimerization of Diketopiperazines

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