Why Do Some Fischer Indolizations Fail?

Çelebi‐Ölçüm, Nihan; Boal, Ben W.; Huters, Alexander D.; Garg, Neil K.; Houk, K. N.

doi:10.1021/ja201035b

Cited by 55 publications

(29 citation statements)

References 33 publications

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“…23,31 Finally, the viability of the Fischer indolization reaction was a notable concern considering the substrate's complexity, its differences compared to ketolactone 19 used in the synthesis of aspidophylline A, 23 and our prior experiences with challenging Fischer indolizations of related substrates. 32 ■ RESULTS AND DISCUSSION Initial Forays and First-Generation Retrosynthetic Analysis. Based on the synthetic plan mentioned above, we tested the Fischer indolization of ketone 24, a known intermediate from our prior synthesis of aspidophylline A ( Figure 5).…”

Section: ■ Introductionmentioning

confidence: 99%

Fischer Indolizations as a Strategic Platform for the Total Synthesis of Picrinine

et al. 2015

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Picrinine, which is a member of the akuammiline family of alkaloids, was first isolated in 1965 from the leaves of Alstonia scholaris. The natural product possesses a daunting polycyclic skeleton that contains a furanoindoline, a bridged [3.3.1]azabicycle, two N,O-acetal linkages, and six stereogenic centers. These structural features render picrinine a challenging and attractive target for total synthesis. This paper provides a full account of our synthetic forays toward picrinine, which culminates in the first total synthesis of this long-standing target. Central to the success of our approach is the use of the Fischer indolization reaction to introduce the C7 quaternary stereocenter and the indoline nucleus of the natural product's scaffold. We probe some of the subtleties of this classic transformation by examining some of the most complex Fischer indolization substrates to date. Additionally, we describe various roadblocks encountered in our experimental efforts, which were successfully overcome to complete the total synthesis of picrinine.

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Section: ■ Introductionmentioning

confidence: 99%

Fischer Indolizations as a Strategic Platform for the Total Synthesis of Picrinine

et al. 2015

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“…We pursued the natural product psychotrimine, which led to mechanistic insight pertaining to the Fischer indolization and an exciting collaboration with my colleague Professor Ken Houk. 22 We used the interrupted Fischer indolization to construct the core of the communesins. 23 Moreover, we completed a concise synthesis of phenserine, 24 a compound undergoing clinical trials for the treatment of Alzheimer’s disease.…”

Section: Interrupted Fischer Indolization Methodologymentioning

confidence: 99%

Pardon the Interruption: A Modification of Fischer’s Venerable Reaction for the Synthesis of Heterocycles and Natural Products

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Morrill

Picazo

et al. 2016

Synlett

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This account provides an overview of our laboratory’s studies of an unusual variant of the Fischer indolization reaction. We describe the discovery of the so-called ‘interrupted Fischer indolization’ and the development of the reaction from a methodological standpoint. In addition, our efforts to evaluate and apply this methodology in the context of akuammiline alkaloid total synthesis are discussed.

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“…12), which provided the best results in an equivalent key [3,3]-sigmatropic rearrangement step of the acid-promoted Fischer indole reaction, where B3LYP optimizations were shown to yield highly asynchronous and dissociative transition states. 40 In the first step of the pericyclic cascade mechanism, the 3 + 2 cycloaddition between nitrone and ketene across the CvO bond forms the substituted 1,2,4-dioxazolidine. The 3 + 2 cycloaddition transition structure, TS-(3 + 2), is predicted to be 16.7 kcal mol −1 uphill from the starting nitrone and ketene (Fig.…”

Section: Mechanistic Validationmentioning

confidence: 99%

An asymmetric pericyclic cascade approach to 3-alkyl-3-aryloxindoles: generality, applications and mechanistic investigations

et al. 2015

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The reaction of L-serine derived N-arylnitrones with alkylarylketenes generates asymmetric 3-alkyl-3-aryloxindoles in good to excellent yields (up to 93%) and excellent enantioselectivity (up to 98% ee) via a pericyclic cascade process. The optimization, scope and applications of this transformation are reported, alongside further synthetic and computational investigations. The preparation of the enantiomer of a Roche anti-cancer agent (RO4999200) 1 (96% ee) in three steps demonstrates the potential utility of this methodology.

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Why Do Some Fischer Indolizations Fail?

Cited by 55 publications

References 33 publications

Fischer Indolizations as a Strategic Platform for the Total Synthesis of Picrinine

Fischer Indolizations as a Strategic Platform for the Total Synthesis of Picrinine

Pardon the Interruption: A Modification of Fischer’s Venerable Reaction for the Synthesis of Heterocycles and Natural Products

An asymmetric pericyclic cascade approach to 3-alkyl-3-aryloxindoles: generality, applications and mechanistic investigations

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Why Do Some Fischer Indolizations Fail?

Cited by 55 publications

References 33 publications

Fischer Indolizations as a Strategic Platform for the Total Synthesis of Picrinine

Fischer Indolizations as a Strategic Platform for the Total Synthesis of Picrinine

Pardon the Interruption: A Modification of Fischer’s Venerable ­Reaction for the Synthesis of Heterocycles and Natural Products

An asymmetric pericyclic cascade approach to 3-alkyl-3-aryloxindoles: generality, applications and mechanistic investigations

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Pardon the Interruption: A Modification of Fischer’s Venerable Reaction for the Synthesis of Heterocycles and Natural Products