Synthesis and evaluation of potent yaku'amide A analogs

Three new bulky cycloalkyl α,β-dehydroamino acids (ΔAAs) have been designed and synthesized. Each residue enhances the rigidity of model peptides and their stability to proteolysis, with larger ring sizes exhibiting greater effects. Peptides containing bulky cycloalkyl ΔAAs are inert to conjugate addition by a nucleophilic thiol. The results suggest that these residues will be effective tools for improving the proteolytic stability of bioactive peptides.

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Synthesis and Studies of Bulky Cycloalkyl α,β-Dehydroamino Acids that Enhance Proteolytic Stability

Joaquin

Mansfield

Chanthakhoun

et al. 2022

Org. Lett.

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Synthesis and evaluation of potent yaku'amide A analogs

Abstract: Two full-length analogs of the anticancer peptide yaku’amide A (1a) and four partial structures have been synthesized. These analogs were identified by computational studies in which the three E- and...

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Synthesis and Studies of Bulky Cycloalkyl α,β-Dehydroamino Acids that Enhance Proteolytic Stability

Synthesis and Studies of Bulky Cycloalkyl α,β-Dehydroamino Acids that Enhance Proteolytic Stability

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