A dimeric cyclic cysteine analogue, i.e. (1R,1’R,2R,2’R)-2,2’- disulfanediylbis (aminocyclohexane-1-carboxylic acid), was used as a constrained unnatural amino acid and as a folding inducer in ultra-short Leu-Val-containing peptide. Our results showed that both free dimer amino acid L1 and its peptide derivative L2 are able to chelate Cu(II). The obtained complexes resulted to be catalytically active in Michael addition reaction of nitro- methane on different types of chalcones. L1-Cu(II) was shown more reactive in terms of conversion, while, in neat conditions, L2-Cu(II) allows to obtain an interesting 60 % e.e. on pyridine chalcone.

Exploitation of Dimeric Cyclic Cysteine as Helix Inducer in Ultra‐Short Peptides for Cu(II)‐Catalyzed Asymmetric Michael Addition on Chalcones / G. Facchetti, J. Gracia Vitoria, M. Moraschi, R. Bucci, A. Abel, S. Pieraccini, S. Pellegrino, I.S. Rimoldi. - In: EUROPEAN JOURNAL OF ORGANIC CHEMISTRY. - ISSN 1434-193X. - (2023). [Epub ahead of print] [10.1002/ejoc.202300240]

Exploitation of Dimeric Cyclic Cysteine as Helix Inducer in Ultra‐Short Peptides for Cu(II)‐Catalyzed Asymmetric Michael Addition on Chalcones

G. Facchetti
Primo
;
M. Moraschi;R. Bucci;A. Abel;S. Pieraccini;S. Pellegrino
Penultimo
;
I.S. Rimoldi
Ultimo
2023

Abstract

A dimeric cyclic cysteine analogue, i.e. (1R,1’R,2R,2’R)-2,2’- disulfanediylbis (aminocyclohexane-1-carboxylic acid), was used as a constrained unnatural amino acid and as a folding inducer in ultra-short Leu-Val-containing peptide. Our results showed that both free dimer amino acid L1 and its peptide derivative L2 are able to chelate Cu(II). The obtained complexes resulted to be catalytically active in Michael addition reaction of nitro- methane on different types of chalcones. L1-Cu(II) was shown more reactive in terms of conversion, while, in neat conditions, L2-Cu(II) allows to obtain an interesting 60 % e.e. on pyridine chalcone.
Settore CHIM/06 - Chimica Organica
Settore CHIM/03 - Chimica Generale e Inorganica
2023
13-apr-2023
Article (author)
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/968359
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