Sulfonyl Ynamides as Useful Tools for N-Heterocyclic Chemistry

Sulfonyl Ynamides as Useful Tools for N-Heterocyclic Chemistry
Author :
Publisher : Logos Verlag Berlin GmbH
Total Pages : 253
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ISBN-10 : 9783832543976
ISBN-13 : 383254397X
Rating : 4/5 (97X Downloads)

Book Synopsis Sulfonyl Ynamides as Useful Tools for N-Heterocyclic Chemistry by : Tim Wezeman

Download or read book Sulfonyl Ynamides as Useful Tools for N-Heterocyclic Chemistry written by Tim Wezeman and published by Logos Verlag Berlin GmbH. This book was released on 2016-12-31 with total page 253 pages. Available in PDF, EPUB and Kindle. Book excerpt: Sulfonyl ynamides are highly versatile and synthetically useful reagents. This thesis details the modular synthesis and use of sulfonyl ynamides in order to access N-heterocyclic scaffolds, such as quinolines and pyrazoles. The synthesis of a wide array of sulfonyl ynamides can be realized via copper-catalyzed amidative cross-couplings or by elimination of dichloroenamide precursors. Additionally the use of Sonogashira chemistry to further diversify terminal ynamides and the synthesis of solid-supported ynamides was investigated. Electrophilically-activated amides can be reacted with sulfonyl ynamides in order to access highly functionalized 4-aminoquinolines. The straightforward amide activation procedure with triflic anhydride and 2-chloropyridine was found to tolerate a wide range of substrates, which allowed for the development of a library of 4-aminoquinolines with ease. Moreover, 4-aminopyrazoles can be prepared by reacting terminal sulfonyl ynamides with sydnones under copper catalysis. However, as the copper catalysts were also found to promote the degradation of the ynamides, a copper-free strain-promoted alternative was developed. An in situ prepared 3-azacyclohexyne was found to tolerate a wide array of C-4 substituted sydnones, producing a mixture of both the 3,4- and 4,3-fused pyrazoles in good yields. Additional investigations into heterocyclic methodology led to the development of highly sophisticated, non-symmetrical and axially-chiral dibenzo-1,3-diazepines, -oxazepines and -thiazepines from simple, commercially available anilines. The anilines were coupled to their corresponding reaction partners via a chloromethyl intermediate and the 7-membered ring was subsequently formed using direct arylation.


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