Deployment of Sulfinimines in Charge-Accelerated Sulfonium Rearrangement Enables a Surrogate Asymmetric Mannich Reaction

Feng, Minghao; Mosiagin, Ivan; Kaiser, Daniel; Maryasin, Boris; Maulide, Nuno

doi:10.1021/jacs.2c05368

Cited by 25 publications

(16 citation statements)

References 53 publications

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“…Ladungsbeschleunigte Sulfoniumumlagerungen haben sich als nützliche Strategie für die Knüpfung von C−C und C−N Bindungen erwiesen [8] . Kürzlich beschrieb unsere Gruppe erfolgreich eine direkte Kupplung von Amiden und Sulfiniminen, die die Synthese von β‐Aminoamiden via einer [3,3]‐sigmatropen Sulfoniumumlagerung ermöglicht [8i] . Basierend auf diesen Ergebnisse stellten wir die Hypothese auf, dass die Umsetzung von tert ‐Butylsulfinamid [9] ( 1 ) mit einem geeigneten Vinylkation (I) [10, 11] in der Bildung einer neuen C−N Bindung resultieren und so einen direkten Zugang zur Einführung einer primären Aminogruppe in einem Schritt ermöglichen sollte.…”

Section: Methodsunclassified

Transfer freier Aminogruppen via α‐Aminierung von Carbonylen

et al. 2023

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Eine Strategie zur direkten α‐Aminierung unfunktionalisierter Carbonylverbindungen wird berichtet. Unter Verwendung einer kommerziell verfügbaren Stickstoffquelle zur Übertragung der freien Aminogruppe (NH2) werden primäre α‐Aminocarbonylverbindungen unter besonders milden Bedingungen hergestellt. Die direkte Einführung einer ungeschützten, primären Aminogruppe ermöglicht in der Folge zahlreiche in situ Funktionalisierungen der erhaltenen Reaktionsprodukte, einschließlich Peptidkupplungen und Pictet–Spengler Cyclisierungen.

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Section: Methodsunclassified

Transfer freier Aminogruppen via α‐Aminierung von Carbonylen

et al. 2023

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“…During the past decade, considerable advancements on the direct transformations of amides have been achieved (14)(15)(16)(17)(18) either via the electrophilic activation of amides (19)(20)(21)(22)(23)(24)(25)(26)(27)(28)(29)(30)(31) or via catalytic partial reduction of amides (32)(33)(34)(35)(36)(37)(38)(39)(40). However, very few examples of the asymmetric transformations of amides have been reported (41)(42)(43)(44), and those involving the catalytic asymmetric reductive transformation of the amide group itself is even more scarce (42,43). Recently, we disclosed the catalytic asymmetric reductive cyanation and phosphonylation of secondary amides using iridium/chiral thiourea relay catalysis (42).…”

Section: Introductionmentioning

confidence: 99%

Multicatalysis protocol enables direct and versatile enantioselective reductive transformations of secondary amides

Chen

Shao

et al. 2022

Sci. Adv.

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The catalytic asymmetric geminal bis-nucleophilic addition to nonreactive functional groups is a type of highly desirable yet challenging transformation in organic chemistry. Here, we report the first catalytic asymmetric reductive/deoxygenative alkynylation of secondary amides. The method is based on a multicatalysis strategy that merges iridium/copper relay catalysis with organocatalysis. A further combination with the palladium-catalyzed alkyne hydrogenation allows the one-pot enantioselective reductive alkylation of secondary amides. This versatile protocol allows the efficient synthesis of four types of α-branched chiral amines, which are prevalent structural motifs of active pharmaceutical ingredients. The protocol also features excellent enantioselectivity, chemoselectivity, and functional group tolerance to be compatible with more reactive functional groups such as ketone and aldehyde. The synthetic utility of the method was further demonstrated by the late-stage functionalization of two drug derivatives and the concise, first catalytic asymmetric approach to the κ-opioid antagonist aticaprant.

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“…Accordingly, considerable efforts have been devoted to the development of asymmetric methods for the construction of these motifs . Particularly, using metal-based chiral Lewis acids as catalysts, various asymmetric vinylogous Mannich reactions have been developed, yielding chiral amino butenolides with 1,2-stereocenters (Scheme C). − However, efficient constructions of amino butenolides with remote 1,4-stereocenters remains an unmet challenge.…”

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confidence: 99%

One-Step Asymmetric Construction of 1,4-Stereocenters via Tandem Mannich-Isomerization Reactions Mediated by a Dual-Functional Betaine Catalyst

Shi

et al. 2022

JACS Au

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The construction of chiral motifs containing nonadjacent stereocenters stands out as a major challenge as they are usually constructed in separate steps utilizing different chiral catalysts. Therefore, the development of new strategies to streamline the construction of such complex motifs has become a major focus of asymmetric synthesis. We report here an unprecedented asymmetric tandem Mannich-isomerization reaction that allows the direct construction of 1,4-stereocenters in a highly stereoselective manner. This asymmetric transformation demonstrated the potential of a tandem nucleophilic addition-isomerization reaction as a broadly useful strategy for the efficient construction of 1,4-stereocenters. Notably, this tandem reaction was mediated by a single chiral betaine as a dual-functional catalyst, promoting first an enantioselective intermolecular C–C bond forming reaction and next a stereoselective intramolecular 1,3-proton transfer reaction.

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Deployment of Sulfinimines in Charge-Accelerated Sulfonium Rearrangement Enables a Surrogate Asymmetric Mannich Reaction

Cited by 25 publications

References 53 publications

Transfer freier Aminogruppen via α‐Aminierung von Carbonylen

Transfer freier Aminogruppen via α‐Aminierung von Carbonylen

Multicatalysis protocol enables direct and versatile enantioselective reductive transformations of secondary amides

One-Step Asymmetric Construction of 1,4-Stereocenters via Tandem Mannich-Isomerization Reactions Mediated by a Dual-Functional Betaine Catalyst

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