High-Throughput Access to Libraries of N-Acylsulfamide Derivatives, a Bioisostere of Carboxylic Acids

Antonia F. Stepan; Nicholas A. Meanwell

doi:10.1055/s-0043-1775033

Synfacts, Table of Contents

Synfacts 2024; 20(09): 0981
DOI: 10.1055/s-0043-1775033

Innovative Drug Discovery and Development

High-Throughput Access to Libraries of N-Acylsulfamide Derivatives, a Bioisostere of Carboxylic Acids

Contributor(s):

Antonia F. Stepan (Roche)

,

Nicholas A. Meanwell (Baruch S. Blumberg Institute, U. Michigan, Rutgers U.)

Abstract

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Weng J, *, Wang S.-C, Zhou X, Li Y.-X, Zhang C.-Y, Zhang Z.-Y, Xiong Y.-S, Lu G, Dong J. Sun Yat-Sen University, Guangzhou, P. R. of China
Enabling Modular Click Chemistry Library through Sequential Ligations of Carboxylic Acids and Amines.

Angew. Chem. Int. Ed. 2024; e202410699
DOI: 10.1002/anie.202410699

Key words

bioisostere design - carboxylic acid bioisosteres - N-acylsulfamides - library generation

Significance

N-Acylsulfamides have been established as bioisosteres of carboxylic acids, notably in the HCV NS5B polymerase inhibitor beclabuvir which was approved in Japan, the Nav1.7 inhibitor GDC-0276 and the herbicide safluenacil. The process developed in this article is mild and high yielding, amenable to the generation of large libraries of N-acylsulfamide derivatives with products typically isolated by a simple filtration after acidification of the reaction mixture The process was demonstrated with a range of carboxylic acid derivatives that explored only relatively benign substituents (for example, there was an absence of alcohols or amides in the acids), although the amines contained a broader range of functionality that included acids, tertiary amines, and alkynes. Bis-carboxylic acids could be fully or partially converted by controlling the ratio of reagents. The process has potential for late-stage functionalization of carboxylic acids, the scope of which will depend on the functionality inherent to a molecule.

Comment

Exposure of a carboxylic acid to the highly electrophilic but readily available fluorosulfuryl isocyanate in CH₃CN, determined to be the crucial solvent, at room temperature afforded an N-fluorosulfonyl amide in yields typically >90%. The scope of the process extended to aromatic, heteroaromatic and aliphatic carboxylic acids with limited polar functionality, although NH-sulfonamide and imide functionality were compatible, and the reaction was tolerant of steric encumbrance. Electron-deficient acids required heating to 50–60 °C in order to complete the reaction. Reaction of the N-fluorosulfonyl amides with aromatic and aliphatic amines occurred in H₂O with Na₂CO₃ as the base heated at 80 °C for 12 hours to afford N-acylsulfamides in good to excellent yields, with the products typically isolated by acidification and simple filtration to afford the product. Execution of a 13x24 library in 96 well plates generated 312 products, with 281 proceeding with >90% conversion and 97% proceeding with >80% conversion.

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