Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Lam, Yu-hong; Houk, K. N.; Cossy, Janine; Prado, Domingo Gomez; Cochi, Anne

doi:10.1002/hlca.201200461

Cited by 13 publications

(10 citation statements)

References 80 publications

(35 reference statements)

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“…Primarily the obtained crystal structures confirm the bicyclic structure of the aziridinium ion proposed as the intermediate of the reaction of our 3‐chloropiperidines with nucleophiles, while the structure of 11 is congruent with an already described aziridinium ion obtained by a different method [14] . Furthermore, the boat‐like structures of these intermediates match the computational calculations for C4 fluorinated bicyclic aziridinium ions obtained from the corresponding prolinol derivatives [15] . Comparison of the two structures also allows assumptions about the reactivity of the benzyl substituted aziridinium ion 11 compared to the butyl analogue 10 a .…”

Section: Resultssupporting

confidence: 83%

Understanding the Alkylation Mechanism of 3‐Chloropiperidines – NMR Kinetic Studies and Isolation of Bicyclic Aziridinium Ions

et al. 2021

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The present study describes the kinetic analysis of the 3chloropiperidine alkylation mechanism. These nitrogen mustard-based compounds are expected to react via a highly electrophilic bicyclic aziridinium ion, which is readily attacked by nucleophiles. Halide abstraction using silver salts with weakly coordinating anions lead to the isolation of these proposed intermediates, whereas their structure was confirmed by single crystal XRD. Kinetic studies of the aziridinium ions also revealed notable reactivity differences of the C5 gem-methylated compounds and their unmethylated counterparts. The observed reactivity trends were also reflected by NMR studies in aqueous solution and DNA alkylation experiments of the related 3-chloropiperidines. Therefore, the underlying Thorpe-Ingold effect might be considered as another option to adjust the alkylation activity of these compounds.

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Section: Resultssupporting

confidence: 83%

Understanding the Alkylation Mechanism of 3‐Chloropiperidines – NMR Kinetic Studies and Isolation of Bicyclic Aziridinium Ions

et al. 2021

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“…Quantum chemical computation studies will be necessary to fully understand the regioselectivity of the attack of nucleophiles on the aziridinium intermediates 49. 50…”

Section: Discussionmentioning

confidence: 99%

Access to Optically Active 3‐Substituted Piperidines by Ring Expansion of Prolinols and Derivatives

Pardo

Cossy

2014

Chemistry A European J

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The ring expansion of prolinols via an aziridinium intermediate gives C3-substituted piperidines in good yields and enantiomeric excess, the substituent at the C3 position being derived from the most reactive nucleophile in the reaction mixture. Depending on the nucleophile, the reaction proceeds under thermodynamic or kinetic control. The regioselectivity of attack of nucleophiles on the aziridinium intermediate depends on the nature of the substituents on the nitrogen atom and the C4 position of the starting prolinols.

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“…Following pathway "a", nonpeptidic NK-1 receptor antagonist L-733060 ( 48) was realized starting from 3-hydroxy-2-phenyl piperidine (47) [56,70]. Most cases with diethylaminosulfur trifluoride (DAST) have yielded enlarged fluorinated piperidine ring compounds (50) from hydroxymethylpyrrolidine (49) via fluorine-driven ring opening in a stereoselective manner [71,72]. Application of various nucleophiles through pathway "a" or "b" gives an efficient synthetic strategy to prepare various aza-cyclic valuables (Figure 5).…”

Section: Bicyclic Aziridinium From Ring Contraction Of Azaheterocyclesmentioning

confidence: 99%

“…Following pathway "a", nonpeptidic NK-1 receptor antagonist L-733060 ( 48) was realized starting from 3-hydroxy-2-phenyl piperidine (47) [56,70]. Most cases with diethylaminosulfur trifluoride (DAST) have yielded enlarged fluorinated piperidine ring compounds (50) from hydroxymethylpyrrolidine (49) via fluorine-driven ring opening in a stereoselective manner [71,72]. This reaction, generation, and ring opening of a bisaziridinium ion (52) from 3-hydroxy-3-trifluoromethyl piperidine (51) with removal of the hydroxy group could also be applicable for the synthesis of biologically important α-trifluoromethyl pyrrolidines (53) (Scheme 14) [73,74].…”

Section: Bicyclic Aziridinium From Ring Contraction Of Azaheterocyclesmentioning

confidence: 99%

Synthetic Applications of Aziridinium Ions

Ranjith

2021

Molecules

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Nonactivated aziridine with an electron-donating group at the ring nitrogen should be activated to an aziridinium ion prior to being converted to cyclic and acyclic nitrogen-containing molecules. This review describes ways to generate aziridinium ions and their utilization for synthetic purposes. Specifically, the intra- and intermolecular formation of aziridinium ions with proper electrophiles are classified, and their regio- and stereoselective transformations with nucleophiles are described on the basis of recent developments.

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Fluorine as a Regiocontrol Element in the Ring Opening of Bicyclic Aziridiniums

Cited by 13 publications

References 80 publications

Understanding the Alkylation Mechanism of 3‐Chloropiperidines – NMR Kinetic Studies and Isolation of Bicyclic Aziridinium Ions

Understanding the Alkylation Mechanism of 3‐Chloropiperidines – NMR Kinetic Studies and Isolation of Bicyclic Aziridinium Ions

Access to Optically Active 3‐Substituted Piperidines by Ring Expansion of Prolinols and Derivatives

Synthetic Applications of Aziridinium Ions

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