Biosynthesis-Inspired Intramolecular Oxa-Conjugate Cyclization of α,β-Unsaturated Thioesters: Stereoselective Synthesis of 2,6-<i>cis</i>-Substituted Tetrahydropyrans

Fuwa, Haruhiko; Noto, Kenkichi; Sasaki, Makoto

doi:10.1021/ol200333p

Cited by 35 publications

(16 citation statements)

References 46 publications

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“…aldehyde 4d ), the second step of this tandem sequence, that is, the oxa‐Michael addition, did not take place, and uncyclized alcohol 2db was obtained in 80 % yield (Table 2, entry 3). This was perhaps the result of the low reactivity of the α,β‐unsaturated ester as the conjugate acceptor under the reaction conditions employed 8,11,12. In contrast, aldehyde 4e , bearing a more reactive alkylidine malonate as Michael acceptor, was found to work efficiently, and corresponding cis ‐THP derivative 1eb was formed in good yield with good diastereoselectivity (Table 2, entry 4).…”

Section: Resultsmentioning

confidence: 99%

Tandem Nucleophilic Addition/Oxa‐Michael Reaction for the Synthesis of cis‐2,6‐Disubstituted Tetrahydropyrans

2014

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Section: Resultsmentioning

confidence: 99%

Tandem Nucleophilic Addition/Oxa‐Michael Reaction for the Synthesis of cis‐2,6‐Disubstituted Tetrahydropyrans

2014

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“…Chemical IMOMA, often integrated into efficient tandem processes, gained growing attention for the stereoselective synthesis of tetrahydropyrans (THPs) during recent years. − It has been shown that the cis - or trans -THP selectivity of IMOMA can be influenced by kinetic or thermodynamic reaction control, by the type of activation (acid, base, or metal catalysis), by the configuration of the double bond, and by the nature of the acceptor moiety. − Although the reaction outcome is predictable for some systems (tandem-cross metathesis-IMOMA with vinylketone intermediates for example reliably leads to cis -THPs with diastereomeric excess > 5:1), low to moderate d.e. s are rather common and have only occasionally been improved by extensive reaction optimization or product re-equilibration (see, e.g., refs − ).…”

Section: Introductionmentioning

confidence: 99%

“…s are rather common and have only occasionally been improved by extensive reaction optimization or product re-equilibration (see, e.g., refs − ). Pioneering studies on the thioester IMOMA have provided valuable insight into the reasons for the high substrate dependence of the cis - trans selectivity, along with the establishment of guidelines for diastereoselective THP cyclization in specific systems. − …”

Section: Introductionmentioning

confidence: 99%

Biocatalysts from Biosynthetic Pathways: Enabling Stereoselective, Enzymatic Cycloether Formation on a Gram Scale

et al. 2020

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Biosynthetic pathways of natural products contain many enzymes that contribute to the rapid assembly of molecular complexity. Enzymes that form complex structural elements with multiple stereocenters, like chiral saturated oxygen heterocycles (CSOH), are of particular interest for a synthetic application, as their use promises to significantly simplify access to these elements. Here, the biocatalytic characterization of AmbDH3, an enzyme that catalyzes intramolecular oxa-Michael addition (IMOMA) is reported. This reaction essentially gives access to various types of CSOH with adjacent stereocenters, but it is not yet part of the repertoire of preparative biocatalysis. An in-depth study on the synthetic utility of AmbDH3 was performed, which made extensive use of complex synthetic precursor surrogates. The enzyme exhibited stability and broad substrate tolerance in in vitro experiments, which was in agreement with the results of molecular modeling. Its selectivity profile enabled kinetic resolution of chiral tetrahydropyrans (THPs) under control of up to four stereocenters. A systematic optimization of the reaction conditions enabled gram-scale conversions yielding preparative amounts of chiral THP. The synthetic utility of AmbDH3 was finally demonstrated by its successful application in the key step of a chemoenzymatic total synthesis to the THP-containing phenylheptanoid (−)-centrolobine. These results highlight the synthetic potential of AmbDH3 and related IMOMA cyclases as a biocatalytic alternative that further develops the available chemical-synthetic IMOMA methodology.

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“…17 The C20-C32 tetrahydropyran core of the phorboxazoles and the C22 epimer were synthesised in the Clarke group using silyl ether deprotection/oxy-Michael cyclisation as the key step. Fuwa 18 speculated that the replacement of α,β-unsaturated ester Michael acceptor with α,β-unsaturated thioester Michael acceptor may enhance the 2,6-cis-selectivities of THP formation. The Clarke group found that using a Michael cyclisation reaction and a thioester electrophile they could generate either the 2,6-cis-or 2,6-trans-THP unit with excellent selectivities depending on the reaction conditions used.…”

Section: Michael Reactionsmentioning

confidence: 99%

Strategies for the construction of tetrahydropyran rings in the synthesis of natural products

2014

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This review focuses on the methodology used for the construction of tetrahydropyran (THP) rings in the synthesis of natural products over the last seven years. While methods like cyclisation onto oxocarbenium ions, reduction of cyclic hemi-ketals, Michael reactions, hetero-Diels-Alder cycloadditions and cyclisations onto epoxides continue to find application, several other strategies including metal-mediated cyclisations, ring-closing metathesis, radical cyclisations and carbocation cyclisations have also found use. This review is intended to provide an overview of the area for those who are unfamiliar, and to refresh and remind those who do work in the area of the exciting developments in the field.

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Biosynthesis-Inspired Intramolecular Oxa-Conjugate Cyclization of α,β-Unsaturated Thioesters: Stereoselective Synthesis of 2,6-cis-Substituted Tetrahydropyrans

Cited by 35 publications

References 46 publications

Tandem Nucleophilic Addition/Oxa‐Michael Reaction for the Synthesis of cis‐2,6‐Disubstituted Tetrahydropyrans

Tandem Nucleophilic Addition/Oxa‐Michael Reaction for the Synthesis of cis‐2,6‐Disubstituted Tetrahydropyrans

Biocatalysts from Biosynthetic Pathways: Enabling Stereoselective, Enzymatic Cycloether Formation on a Gram Scale

Strategies for the construction of tetrahydropyran rings in the synthesis of natural products

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