Alejandro Guarnieri‐Ibáñez scite author profile

Polycyclic indoline‐benzodiazepines can be accessed through the intermolecular reaction of Tröger bases with N‐sulfonyl‐1,2,3‐triazoles. Under RhII catalysis, α‐imino carbenes are generated and a subsequent cascade of [1,2]‐Stevens, Friedel–Crafts, Grob, and aminal formation reactions yield the polycyclic heterocycles as single isomers (d.r.>49:1, four stereocenters including two bridgehead N atoms). Further ring expansion by insertion of a second α‐imino carbene leads to elaborated polycyclic 9‐membered‐ring triazonanes.

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Regiodivergent synthesis of pyrazino-indolines vs. triazocines via α-imino carbenes addition to imidazolidines

Guarnieri‐Ibáñez

Aguirre

Besnard

et al. 2021

Chem. Sci.

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Diversity-oriented synthesis of heterocycles and macrocycles by controlled reactions of oxetanes with α-iminocarbenes

et al. 2017

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Configurational Lability of Imino‐Substituted Ethano Tröger Bases. Insight on the Racemization Mechanism

Bosmani

Guarnieri‐Ibáñez

Lacour

2019

Helvetica Chimica Acta

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Polycyclic indoline‐benzodiazepines are afforded in one step by the reaction of Tröger bases with N‐sulfonyl‐1,2,3‐triazoles under Rh(II) catalysis. After α‐imino carbene formation, the process involves a cascade of [1,2]‐Stevens rearrangement, Friedel‐Crafts, Grob fragmentation, and aminal formation reactions. It is highly diastereoselective (d.r. >49:1, four stereocenters incl. two bridgehead N‐atoms). However and in contrast with other reported carbene additions to these moieties, full racemization occurs when enantiopure Tröger bases are used as substrates. To pinpoint the origin of this unexpected behavior, a key elemental step of the mechanism was evaluated and tested. Interestingly, it is not only the initial ring‐opening but also the latter reversible Mannich reaction of the imino‐substituted ethano Tröger base intermediate that is responsible for the loss of enantiospecificity.

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