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Synfacts 2019; 15(05): 0569
DOI: 10.1055/s-0037-1612447
Peptide Chemistry
© Georg Thieme Verlag Stuttgart · New York

Efficient Macrocyclization of Small Peptides

Rezensent(en):
Hisashi Yamamoto
,
Amit Banerjee
Roesner S, Saunders GJ, Wilkening I, Jayawant E, Geden JV, Kerby P, Dixon AM, Notman R, Shipman M. * University of Warwick, Coventry, UK
Macrocyclisation of Small Peptides Enabled by Oxetane Incorporation.

Chem. Sci. 2019;
10: 2465-2472
CrossrefPubMedSuche in Google Scholar
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Publikationsverlauf

Publikationsdatum:
15. April 2019 (online)

 
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Key words

cyclic peptides - macrocyclization - oxetane - disulfide bond - amino acids

Significance

Cyclic peptides have recently emerged as a new source of drug molecules, but very few in clinical use are derived from natural sources. The main problem is associated with their synthesis, which often suffers from C-terminal epimerization, cyclooligomerization, and byproduct formation during macrocyclization. Shipman and co-workers have developed a simple, mild, and efficient macrocyclization strategy, which involves the incorporation of an oxetane ring, for synthesizing cyclic peptides in good yields by using an appropriate coupling reagent.


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Comment

Cyclic peptide drugs are more useful than the linear peptides, but their synthesis is quite challenging. The present approach shows that macrocyclization of head-to-tail peptide can be improved by substituting one of the backbone amide C=O bonds with a simple oxetane ring. In addition, a variety of cyclic peptides with challenging ring sizes (tetra-, penta-, or hexapeptides) were synthesized. Further study showed that the bioactivity does not change upon replacing the amide C=O bond with an oxetane ring.


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