Artikel

A Straightforward Access to Enantiopure 4‐Hydroxy‐pipecolic Acid Peptidomimetics by aza‐Prins Cyclization/LiNTf2‐Promoted Aminolysis of Lactones

28.08.2025

Von Wiley-VCH zur Verfügung gestellt

Enantiopure constrained pseudodipeptides based on pipecolic acid scaffold are obtained by a two-step synthesis involving an aza-Prins cyclization to deliver piperidine-lactones, followed by LiNTf2-promoted aminolysis with various amino acids.


Abstract

Peptidomimetics, that can take advantage of bioavailability and metabolic stability, are considered as an important class of molecules and constitute thus a large research field in medicinal chemistry. With the aim of obtaining constrained examples for drug discovery, we designed a two-step synthesis of cis-4-hydroxy pipecolic acid derivatives as pseudodipeptides mimics. This straightforward procedure concerns the coupling of amino acid-derived homoallylic amines with glyoxylic acid via an aza-Prins cyclization to deliver piperidine-lactones, followed by LiNTf2-promoted aminolysis of the lactone with various amino acids. The 4-hydroxy pipecolic acid peptidomimetics are obtained as single enantiomers and with a high diastereomeric control and they represent original and modular scaffolds for drug discovery.

Verwandte Artikel
A Straightforward Access to Enantiopure 4‐Hydroxy‐pipecolic Acid Peptidomimetics by aza‐Prins Cyclization/LiNTf2‐Promoted Aminolysis of Lactones
In Kürze
A Straightforward Access to Enantiopure 4‐Hydroxy‐pipecolic Acid Peptidomimetics by aza‐Prins Cyclization/LiNTf2‐Promoted Aminolysis of Lactones
Ehrungen, Karriere
A Straightforward Access to Enantiopure 4‐Hydroxy‐pipecolic Acid Peptidomimetics by aza‐Prins Cyclization/LiNTf2‐Promoted Aminolysis of Lactones
Aus den Fachgruppen
A Straightforward Access to Enantiopure 4‐Hydroxy‐pipecolic Acid Peptidomimetics by aza‐Prins Cyclization/LiNTf2‐Promoted Aminolysis of Lactones
EuChemS Policy Workshop „PFAS”
A Straightforward Access to Enantiopure 4‐Hydroxy‐pipecolic Acid Peptidomimetics by aza‐Prins Cyclization/LiNTf2‐Promoted Aminolysis of Lactones
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