An overview of late-stage functionalization in today’s drug discovery

Moir, Michael; Danon, Jonathan J.; Reekie, Tristan A.; Kassiou, Michael

doi:10.1080/17460441.2019.1653850

Cited by 158 publications

(101 citation statements)

References 70 publications

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“…Fluoride ions are demonstrated to cause racemisation of the sulfonimidoyl fluorides, which is avoided by fluoride trapping. The mild coupling reagents allow the use of neutral primary and secondary amines, and the methodology is exemplified in the functionalisation of amine containing drug compounds, showing the potential for its use to rapidly prepare novel chemical entities and diverse chemical libraries . A readily removed N‐Boc (Boc= tert ‐butyloxycarbonyl) protecting group on the imide nitrogen is employed, which also increased the electrophilicity of the sulfonimidoyl fluoride.…”

Section: Figurementioning

confidence: 99%

Synthesis of Highly Enantioenriched Sulfonimidoyl Fluorides and Sulfonimidamides by Stereospecific Sulfur–Fluorine Exchange (SuFEx) Reaction

Greed

Briggs

Idiris

et al. 2020

Chemistry A European J

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Sulfonimidamides present exciting opportunities as chiral isosteres of sulfonamides, with potential for additional directional interactions. Here, we present the first modular enantioselective synthesis of sulfonimidamides, including the first stereoselective synthesis of enantioenriched sulfonimidoyl fluorides, and studies on their reactivity. A new route to sulfonimidoyl fluorides is presented from solid bench‐stable, N‐Boc‐sulfinamide (Boc= tert ‐butyloxycarbonyl) salt building blocks. Enantioenriched arylsulfonimidoyl fluorides are shown to be readily racemised by fluoride ions. Conditions are developed, which trap fluoride and enable the stereospecific reaction of sulfonimidoyl fluorides with primary and secondary amines (100 % es , es =enantiospecificity) generating sulfonimidamides with up to 99 % ee . Aryl and alkyl sulfonimidoyl fluoride reagents are suitable for mild late stage functionalisation reactions, exemplified by coupling with a selection of complex amines in marketed drugs.

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Section: Figurementioning

confidence: 99%

Synthesis of Highly Enantioenriched Sulfonimidoyl Fluorides and Sulfonimidamides by Stereospecific Sulfur–Fluorine Exchange (SuFEx) Reaction

Greed

Briggs

Idiris

et al. 2020

Chemistry A European J

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“…Such a strategy cannot disrupt the potential binding of a pharmacophore to a target, so this fragment growing strategy was benchmarked to modify 1,5-oxaza spiroquinone 1. For this purpose, we should also consider late-stage functionalization for efficient introduction of diverse substituents in the very last steps of the synthesis 44,45 . As shown in Fig.…”

Section: Resultsmentioning

confidence: 99%

Positioning of an unprecedented spiro[5.5]undeca ring system into kinase inhibitor space

Venkanna

Subedi

Teli

et al. 2020

Sci Rep

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In-house 1,5-oxaza spiroquinone 1, with spiro[5.5]undeca ring system, was announced as an unprecedented anti-inflammatory scaffold through chemistry-oriented synthesis (ChOS), a chemocentric approach. Herein, we studied how to best position the spiro[5.5]undeca ring system in kinase inhibitor space. Notably, late-stage modification of the scaffold 1 into compounds 2a-r enhanced kinase-likeness of the scaffold 1. The improvement could be depicted with (1) selectivity with target shift (from JNK-1 into GSK-3) and (2) potency (> 20-fold). In addition, ATP independent IC50 of compound 2j suggested a unique binding mode of this scaffold between ATP site and substrate site, which was explained by docking based optimal site selection and molecular dynamic simulations of the optimal binding site. Despite the shift of kinase profiling, the anti-inflammatory activity of compounds 2a-r could be retained in hyperactivated microglial cells.

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“…As a critical component of many medicinal chemistry campaigns or total syntheses, LSF allows for the incorporation of important functional groups in the final steps of a synthesis, creating the need for efficient methodologies. 37 When the in situ reaction conditions were applied to the LSF of Telmisartan, a carboxylic acid-containing drug used for the treatment of hypertension, the desired ketone (4a) product was isolated in 91% yield. This direct, one-step alkylation was applied to various other pharmaceutical compounds to afford the ketone products (4b-c) in moderate-togood yields (Scheme 2).…”

Section: Scheme 1 Oxidations Of the Breslow Intermediate And Expansimentioning

confidence: 99%

Combined Photoredox and Carbene Catalysis for the Synthesis of Ketones from Carboxylic Acids

Bay¹,

fitzpatrick²,

Betori³

et al. 2020

Preprint

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Disclosed herein is the development of a novel single-electron reduction of acyl azoliums for the formation of ketones from carboxylic acids. Facile construction of the acyl azolium <i>in situ</i> followed by a radical-radical coupling was made possible using merged NHC-photoredox catalysis. The utility of this protocol in synthesis was demonstrated in the late-stage functionalization of a variety of pharmaceutical compounds.

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An overview of late-stage functionalization in today’s drug discovery

Cited by 158 publications

References 70 publications

Synthesis of Highly Enantioenriched Sulfonimidoyl Fluorides and Sulfonimidamides by Stereospecific Sulfur–Fluorine Exchange (SuFEx) Reaction

Synthesis of Highly Enantioenriched Sulfonimidoyl Fluorides and Sulfonimidamides by Stereospecific Sulfur–Fluorine Exchange (SuFEx) Reaction

Positioning of an unprecedented spiro[5.5]undeca ring system into kinase inhibitor space

Combined Photoredox and Carbene Catalysis for the Synthesis of Ketones from Carboxylic Acids

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