On the Asymmetric Induction in Proline‐Catalyzed Aldol Reactions: Reagent‐Controlled Addition Reactions of 2,2‐Dimethyl‐1,3‐dioxane‐5‐one to Acyclic Chiral α‐Branched Aldehydes

Trajkovic, Jasna Marjanovic; Milanović, Vesna; Ferjancic, Zorana; Saičić, Radomir N.

doi:10.1002/ejoc.201701073

Cited by 9 publications

(5 citation statements)

References 54 publications

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“…Notably, when this reaction was repeated in CH 2 Cl 2 or DMSO, the yield was significantly lower. The l -proline-catalyzed aldol reaction between ( S )-2-Cbz-aminopentanal and dioxanone yielded the corresponding anti-aminohydrin as the sole product, and both l - and d -proline-catalyzed aldol reactions of ( S )- N -Cbz prolinal (Supplementary Schemes 1 and 2 ) each gave single products without epimerization of the α-stereocenter, further confirming that α-aminoaldehydes do not racemize under these reaction conditions ( k rac << k aldol ) 47 . We also examined the l -proline-catalyzed aldol reaction of (±)-2-phenylpropanal and dioxanone 13 (Supplementary Scheme 3 ), which afforded an equal mixture of syn- and anti- diastereomers again suggesting k rac << k aldol .…”

Section: Resultsmentioning

confidence: 66%

Diversity-oriented synthesis of glycomimetics

et al. 2021

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Glycomimetics are structural mimics of naturally occurring carbohydrates and represent important therapeutic leads in several disease treatments. However, the structural and stereochemical complexity inherent to glycomimetics often challenges medicinal chemistry efforts and is incompatible with diversity-oriented synthesis approaches. Here, we describe a one-pot proline-catalyzed aldehyde α-functionalization/aldol reaction that produces an array of stereochemically well-defined glycomimetic building blocks containing fluoro, chloro, bromo, trifluoromethylthio and azodicarboxylate functional groups. Using density functional theory calculations, we demonstrate both steric and electrostatic interactions play key diastereodiscriminating roles in the dynamic kinetic resolution. The utility of this simple process for generating large and diverse libraries of glycomimetics is demonstrated in the rapid production of iminosugars, nucleoside analogues, carbasugars and carbohydrates from common intermediates.

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Section: Resultsmentioning

confidence: 66%

Diversity-oriented synthesis of glycomimetics

et al. 2021

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“…However, there were contradictory reports regarding double asymmetric synthesis in proline‐ catalyzed dioxanone addition to chiral aldehydes: whereas it was generally accepted that ( R )‐Pro/( S )‐aldehyde (or ( S )‐Pro/( R )‐aldehyde) constitute a matched pair (in line with calculations presented above), one report claimed reverse stereochemical matching of reactants ( i. e ., ( S )‐Pro/( S )‐aldehyde) and low reactivity in mismatched case [25c] . Subsequent study found that a range of α‐substituted (as well as α,β‐disubstituted) aldehydes 8 a – e (containing a suitably protected nitrogen substituent at α‐ or β‐position, for consecutive reductive amination) can be used as acceptors, where the combination of ( R )‐Pro and ( S )‐aldehyde was a matched case [28] . In most of mismatched cases, reagent control provided synthetically useful levels of stereoselectivity, provided the α‐substituent is not part of a cyclic structure (see aldehyde 8 e , entry 5, where poor yield and low stereoselectivity are observed with).…”

Section: Organocatalyzed Aldolization/reductive Amination As the Key Step In Synthesis Of Iminosugarsmentioning

confidence: 99%

“…At subinhibitory concentrations, DGJ acts as a pharmacological chaperon for mutated α‐galactosidase A, thus allowing it to escape from the quality control in endoplasmic reticulum and become active in glycoprotein processing [30] . This compound, clinically approved under commercial name Galafold ® (generic: migalastat), is synthesized according to Scheme 3 [28] . ( R )‐Proline‐catalyzed aldol addition of dioxanone 1 to isoserinal 8 b provided aldol 10 b with 13 : 1 selectivity; however, the purification of the required isomer is greatly facilitated by the fact that it spontaneously cyclizes into hemiaminal 12 , whereas the minor diastereoisomer does not (this appears to be is a general feature of Cbz‐ and Boc‐protected 3‐ and 4‐amino‐substituted aldols).…”

Section: Organocatalyzed Aldolization/reductive Amination As the Key Step In Synthesis Of Iminosugarsmentioning

confidence: 99%

Combining Organocatalyzed Aldolization and Reductive Amination: An Efficient Reaction Sequence for the Synthesis of Iminosugars

Ferjancic

Saičić

2021

Eur J Org Chem

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Over the past two decades, organocatalytic aldol reaction emerged as a powerful method for the enantioselective carbon-carbon bond formation, often offering more efficient, economical and environmentally friendly synthesis of chiral molecules. On the other hand, reductive amination is one of the most important reactions in synthesis of biologically active compounds and drug candidates. Coupling these two reactions results in a powerful combination that allows for a rapid, stereoselective access to substituted, highly functionalized fiveand six-membered N-heterocycles. This minireview illustrates the applicability of this approach as the key feature in syntheses of various iminosugars -a class of polyhydroxylated alkaloids with a range of interesting biological activities and high pharmacological potential.

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“…A peculiar case was represented by ionic liquids (ILs) [67][68][69][70][71][72], which allowed in a few cases to decrease the catalyst loading (up to 1 mol%) and, during the work-up, to confine proline in a separate phase, enabling a simple product isolation and the reuse of the catalytic system. In recent literature, attempts are reported where proline is used in acetone/CHCl 3 mixtures [73], in DMF at 4 • C (a condition that often requires several days) [74], in tert-butyl methyl ether (MTBE) [75], in deep eutectic solvents [76,77], or under solvent-free conditions, with [78][79][80] or without [81] the ball milling approach. However, many issues associated with the use of proline remain unsolved and polar aprotic solvents are characterized by several undesirable features (toxicity, high production cost, high environmental impact, difficult product recovery) [82][83][84].…”

Section: Introductionmentioning

confidence: 99%

A Simple and Efficient Protocol for Proline-Catalysed Asymmetric Aldol Reaction

et al. 2020

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The proline-catalysed asymmetric aldol reaction is usually carried out in highly dipolar aprotic solvents (dimethylsulfoxide, dimethylformamide, acetonitrile) where proline presents an acceptable solubility. Protic solvents are generally characterized by poor stereocontrol (e.g., methanol) or poor reactivity (e.g., water). Here, we report that water/methanol mixtures are exceptionally simple and effective reaction media for the intermolecular organocatalytic aldol reaction using the simple proline as the catalyst.

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On the Asymmetric Induction in Proline‐Catalyzed Aldol Reactions: Reagent‐Controlled Addition Reactions of 2,2‐Dimethyl‐1,3‐dioxane‐5‐one to Acyclic Chiral α‐Branched Aldehydes

Cited by 9 publications

References 54 publications

Diversity-oriented synthesis of glycomimetics

Diversity-oriented synthesis of glycomimetics

Combining Organocatalyzed Aldolization and Reductive Amination: An Efficient Reaction Sequence for the Synthesis of Iminosugars

A Simple and Efficient Protocol for Proline-Catalysed Asymmetric Aldol Reaction

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