Ring-Strain-Enabled Reaction Discovery: New Heterocycles from Bicyclo[1.1.0]butanes

Walczak, M; Krainz, Tanja; Wipf, Peter

doi:10.1021/ar500437h

Cited by 161 publications

(94 citation statements)

References 99 publications

(127 reference statements)

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“…We began our studies by directly generating 1-lithio bicyclo[1.1.0]butane 3 from 1,1-dibromo-2-(chloromethyl)cyclopropane 2 using Wipf's procedure 21 (Figure 1d). Whilst reaction of 3 with cyclohexyl pinacol boronic ester did indeed result in formation of the intermediate bicyclo[1.1.0]butyl boronate complex (as observed by 11 B NMR spectroscopic analysis of the reaction mixture), all attempts at subsequent cross-coupling were unsuccessful.…”

Section: Resultsmentioning

confidence: 99%

“…Bicyclo[1.1.0]butane (1) has received considerable interest, where its ring strain has previously been harnessed to stimulate a variety of transition-metal-mediated rearrangements. 21,22 We therefore reasoned that if we could prepare a bicyclo[1.1.0]butyl boronate complex, with its weakened C−C -bond, the tendency of the boronic ester substituent to undergo 1,2-migration would provide sufficient 'push' to promote reaction with an electrophilic palladium-aryl complex at the -carbon. This would result in 1,2migration of the boron substituent to the -carbon with simultaneous cleavage of the C−C -bond and formation of a C-Pd bond at the -carbon.…”

Section: Introductionmentioning

confidence: 99%

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Carbopalladation of C–C σ-bonds enabled by strained boronate complexes

2018

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Transition metal-catalysed cross-coupling reactions, particularly those mediated by palladium, are some of the most broadly used chemical transformations. The fundamental reaction steps of such crosscouplings typically include oxidative addition, transmetalation, carbopalladation of a -bond, and/or reductive elimination. Herein, we describe an unprecedented fundamental reaction step: a C−C σ-bond carbopalladation. Specifically, an aryl palladium(II) complex interacts with a −bond of a strained bicyclo[1.1.0]butyl boronate complex to enable addition of the aryl palladium(II) species and an organoboronic ester substituent across a C−C -bond. The overall process couples readily available aryl triflates and organoboronic esters across a cyclobutane unit with total diastereocontrol. The pharmaceutically-relevant 1,1,3-trisubstituted cyclobutane products are decorated with an array of modular building blocks, including a boronic ester which can be readily derivatized.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Carbopalladation of C–C σ-bonds enabled by strained boronate complexes

2018

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“…39 We envisioned that general conditions could be developed for the homoconjugate addition of Grignard reagents, with subsequent enolate trapping to form highly functionalized cyclobutanes. In 1981, Ganem first prepared bicyclobutane carboxylates via treatment of ethyl α-allyl-α-diazoacetate with Rh 2 (OAc) 4 to give ethyl bicyclobutane-1-carboxylate (51%) along with competing β-hydride migration (39%).…”

Section: Asymmetric Cyclobutane Synthesis Via Intramolecular Bicyclobmentioning

confidence: 99%

Rh-Catalyzed Intermolecular Reactions of α-Alkyl-α-Diazo Carbonyl Compounds with Selectivity over β-Hydride Migration

2015

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CONSPECTUS Rh-carbenes derived from α-diazocarbonyl compounds have found broad utility across a remarkable range of reactivity, including cyclopropanation, cyclopropenation, C–H insertions, heteroatom–H insertions, and ylide forming reactions. However, in contrast to α-aryl or α-vinyl-α-diazocarbonyl compounds, the utility of α-alkyl-α-diazocarbonyl compounds had been moderated by the propensity of such compounds to undergo intramolecular β-hydride migration to give alkene products. Especially challenging had been intermolecular reactions involving α-alkyl-α-diazocarbonyl compounds.

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“…The goal was to generate a stable reagent that would enable both rapid and mild "cyclobutylation" of amines but also permit further functionalization of intermediate adducts. Bicyclobutane and its substituted derivatives, since their first preparation in 1959 (24), have been the subject of many synthetic studies, the majority of which either engaged the strained system as a nucleophile or cleaved the center bond via a transition metal-mediated process (25, 26). Rather than pursuing the parent bicyclobutane (a gas at room temperature) (27), we appended an arylsulfonyl group as a means to both activate the strained C–C bond and render the reagent bench stable.…”

Section: Introduction Of Cyclobutane Via Strain-releasementioning

confidence: 99%

Strain-release amination

Gianatassio

Lopchuk

Wang

et al. 2016

Science

406

254

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To optimize drug candidates, modern medicinal chemists are increasingly turning to an unconventional structural motif: small, strained ring systems. However, the difficulty of introducing substituents such as bicyclo[1.1.1]pentanes, azetidines, or cyclobutanes often outweighs the challenge of synthesizing the parent scaffold itself. Thus, there is an urgent need for general methods to rapidly and directly append such groups onto core scaffolds. Here we report a general strategy to harness the embedded potential energy of effectively spring-loaded C–C and C–N bonds with the most oft-encountered nucleophiles in pharmaceutical chemistry, amines. Strain release amination can diversify a range of substrates with a multitude of desirable bioisosteres at both the early and late-stages of a synthesis. The technique has also been applied to peptide labeling and bioconjugation.

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Ring-Strain-Enabled Reaction Discovery: New Heterocycles from Bicyclo[1.1.0]butanes

Cited by 161 publications

References 99 publications

Carbopalladation of C–C σ-bonds enabled by strained boronate complexes

Carbopalladation of C–C σ-bonds enabled by strained boronate complexes

Rh-Catalyzed Intermolecular Reactions of α-Alkyl-α-Diazo Carbonyl Compounds with Selectivity over β-Hydride Migration

Strain-release amination

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