Enantioselective Synthesis of 6,6‐Disubstituted Pentafulvenes Containing a Chiral Pendant Hydroxy Group

Nouch, Ryan; Cini, Melchior; Magre, Marc; Abid, Mohammed; Diéguez, Montserrat; Pàmies, Òscar; Woodward, Simon; Lewis, William

doi:10.1002/chem.201704247

Cited by 12 publications

(9 citation statements)

References 24 publications

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“…All other chemicals were purchased from ABCR, Acros, Alfa Aesar, Fluorochem, Merck, Sigma-Aldrich, and TCI Europe at highest commercially available purity and used without further purification. Compound 2b and 3b were prepared according to the procedures reported by Capitosti et al Compounds 8 , 13 , and 17 were prepared according to the procedures previously reported. − Thin-layer chromatography (TLC) was performed on Merck silica gel 60 F 254 TLC aluminium sheets and visualized by ultraviolet light (254 nm) and/or with ceric ammonium molybdate, potassium permanganate, or ninhydrine staining solution. Flash column chromatography was performed on Acros silica gel 35–70, 60 Å, using a forced flow of eluent (method of Still).…”

Section: Experimental Sectionmentioning

confidence: 99%

De-Novo Design of Cereblon (CRBN) Effectors Guided by Natural Hydrolysis Products of Thalidomide Derivatives

et al. 2019

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Targeted protein degradation via cereblon (CRBN), a substrate receptor of an E3 ubiquitin ligase complex, is an increasingly important strategy in various clinical settings, in which the substrate specificity of CRBN is altered via the binding of small-molecule effectors. To date, such effectors are derived from thalidomide and confer a broad substrate spectrum that is far from being fully characterized. Here, we employed a rational and modular approach to design novel and minimalistic CRBN effectors. In this approach, we took advantage of the binding modes of hydrolyzed metabolites of several thalidomide-derived effectors, which we elucidated via crystallography. These yielded key insights for the optimization of the minimal core binding moiety and its linkage to a chemical moiety that imparts substrate specificity. Based on this scaffold, we present a first active de-novo CRBN effector that is able to degrade the neo-substrate IKZF3 in the cell culture.

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Section: Experimental Sectionmentioning

confidence: 99%

De-Novo Design of Cereblon (CRBN) Effectors Guided by Natural Hydrolysis Products of Thalidomide Derivatives

et al. 2019

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“…Such conditions are indeed known to be beneficial for standard Knoevenagel reactions, , to which fulvene synthesis is closely related. Buffered media were also very recently successfully employed for the organocatalytic synthesis of chiral fulvenes. − In this work, we demonstrate that it is indeed possible to significantly increase the formation rate of certain fulvenes by employing a pyrrolidine-buffered acetonitrile solution. A kinetic investigation of the catalyzed reactions of two different groups of substrates by NMR and UV–vis spectroscopy yielded a mechanistic model that rationalizes previous observations.…”

Section: Introductionmentioning

confidence: 71%

Kinetics and Mechanism of Pyrrolidine Buffer-Catalyzed Fulvene Formation

et al. 2018

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Rapid synthesis of fulvenes is achieved using pyrrolidinium/pyrrolidine buffers in anhydrous acetonitrile. Time-dependent UV−vis absorption and NMR spectroscopy reveal that the rate and yield of fulvene formation depend strongly on both the presence of acid in the medium and the choice of solvent, and they are negatively affected by water. Kinetic data have been collected for various substrates, and the synthetic benefits of the adjusted reaction conditions are showcased. Enhancements of reaction rates are found in comparison to literature procedures. α-Unsaturated fulvenes that were previously difficult to access can now be obtained in good yields.

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“…[5g] However, the use of this solvent might be limited by its higher cost than other typical organic solvents, and it also shows toxicity such as serious eye damage. We thus examined this reaction using catalyst 19 with a di ‐phenylmethanol moiety and related catalyst 20 with a mono ‐phenylmethanol moiety, in our identified superior i Pr 2 O solvent (entries 1 and 2, Table ). However, neither catalyst 19 nor catalyst 20 showed better catalytic activities than our 2‐azanorbornane catalyst 7 .…”

Section: Resultsmentioning

confidence: 99%

2‐Azanorbornane‐Based Amino Alcohol Organocatalysts for Asymmetric Michael Reaction of β‐Keto Esters with Nitroolefins

et al. 2019

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Enantioselective Synthesis of 6,6‐Disubstituted Pentafulvenes Containing a Chiral Pendant Hydroxy Group

Cited by 12 publications

References 24 publications

De-Novo Design of Cereblon (CRBN) Effectors Guided by Natural Hydrolysis Products of Thalidomide Derivatives

De-Novo Design of Cereblon (CRBN) Effectors Guided by Natural Hydrolysis Products of Thalidomide Derivatives

Kinetics and Mechanism of Pyrrolidine Buffer-Catalyzed Fulvene Formation

2‐Azanorbornane‐Based Amino Alcohol Organocatalysts for Asymmetric Michael Reaction of β‐Keto Esters with Nitroolefins

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