A spirocyclic backbone accesses new conformational space in an extended, dipole-stabilized foldamer

Roe, William E.; Warnock, Toyah M. C.; Knipe, Peter C.

doi:10.1038/s42004-023-00868-8

“…In our previous studies dipolar repulsion between adjacent monomers was used as the primary determinant of conformation, specifically between azenes and imidazolidine‐2‐one [6] and spirocyclic bis‐lactam [7] linkers. Related systems undergo acid‐mediated switching between an extended and helical conformation [5k,o] .…”

Section: Figurementioning

confidence: 99%

“…Protonation of the pyridines would subvert this interaction and lead to the manner of switching outlined in Figure 1A. We have utilized the principal axes of aviation to convey the conformational effects of monomers within foldamers [7] . Here, we anticipate that the substitution pattern on the azene linker and dipolar repulsion effects will achieve control about both the yaw and roll axes.…”

Section: Figurementioning

confidence: 99%

Non‐Covalent Interactions Enforce Conformation in Switchable and Water‐Soluble Diketopiperazine‐Pyridine Foldamers

McCann,

Roe,

Agnew

et al. 2023

Angewandte Chemie

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To reach their potential as mimics of the dynamic molecules present in biological systems, foldamers must be designed to display stimulus‐responsive behavior. Here we report such a foldamer architecture based on alternating pyridine‐diketopiperazine linkers. Epimerization is conveniently prevented through a copper‐catalyzed coupling protocol. The compounds’ native unswitched conformation is first discovered in the solid and solution state. The foldamers can be solubilized in DMSO and pH 9.5 buffer, retaining conformational control to a large degree. Lastly, dynamic switching is demonstrated through treatment with acid, leading to behaviour we describe as stimulus‐responsive sidechain reconfiguration.

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“…We have utilized the principal axes of aviation to convey the conformational effects of monomers within foldamers. [7] Here, we anticipate that the substitution pattern on the azene linker and dipolar repulsion effects will achieve control about both the yaw and roll axes.…”

mentioning

confidence: 99%

“…[4] As a result, switching within foldamers has been reported in response to diverse stimuli including light, solvent polarity and ionbinding. [1a,5] In our previous studies dipolar repulsion between adjacent monomers was used as the primary determinant of conformation, specifically between azenes and imidazolidine-2-one [6] and spirocyclic bis-lactam [7] linkers. Related systems undergo acid-mediated switching between an extended and helical conformation.…”

mentioning

confidence: 99%

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Non‐Covalent Interactions Enforce Conformation in Switchable and Water‐Soluble Diketopiperazine‐Pyridine Foldamers

McCann,

Roe,

Agnew

et al. 2023

Angew Chem Int Ed

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0

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To reach their potential as mimics of the dynamic molecules present in biological systems, foldamers must be designed to display stimulus‐responsive behavior. Here we report such a foldamer architecture based on alternating pyridine‐diketopiperazine linkers. Epimerization is conveniently prevented through a copper‐catalyzed coupling protocol. The compounds’ native unswitched conformation is first discovered in the solid and solution state. The foldamers can be solubilized in DMSO and pH 9.5 buffer, retaining conformational control to a large degree. Lastly, dynamic switching is demonstrated through treatment with acid, leading to behaviour we describe as stimulus‐responsive sidechain reconfiguration.

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Atropisomeric Foldamers

Ansari,

Knipe

2024

ChemPlusChem

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This concept article explores the emerging role of atropisomerism in foldamer chemistry, a field focussed on oligomers that adopt well‐defined conformations through non‐covalent interactions. Atropisomerism introduces a novel dimension to foldamer design by restricting rotational freedom around single bonds to dictate molecular shape with precision. Despite the prevalence of atropisomeric bonds in organic synthesis, their application within foldamers remains underexplored. Here, we discuss key developments in both backbone and sidechain atropisomerism, and suggest future directions for atropisomeric foldamers in the context of a recent surge in atropselective synthetic methods. We propose that judicious use of atropisomerism may serve as a transformative tool in the construction of shape‐defined macromolecules.

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A spirocyclic backbone accesses new conformational space in an extended, dipole-stabilized foldamer

Cited by 3 publications

References 78 publications

Non‐Covalent Interactions Enforce Conformation in Switchable and Water‐Soluble Diketopiperazine‐Pyridine Foldamers

Non‐Covalent Interactions Enforce Conformation in Switchable and Water‐Soluble Diketopiperazine‐Pyridine Foldamers

Non‐Covalent Interactions Enforce Conformation in Switchable and Water‐Soluble Diketopiperazine‐Pyridine Foldamers

Atropisomeric Foldamers

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