Depsipeptide

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A depsipeptide is a peptide in which one or more of its amide, -C(O)NHR-, groups are replaced by the corresponding ester, -C(O)OR-.[1] Many depsipeptides have both peptide and ester linkages.[2] Elimination of the N–H group in a peptide structure results in a decrease of H-bonding capability, which is responsible for secondary structure and folding patterns of peptides, thus inducing structural deformation of the helix and β-sheet structures.[2][3] Because of decreased resonance delocalization in esters relative to amides, depsipeptides have lower rotational barriers for cis-trans isomerization and therefore they have more flexible structures than their native analogs.[2][3] They are mainly found in marine and microbial natural products.[4]

File:Depsipeptide Principle V.1.png
Example of a depsipeptide with 3 amide groups (highlighted blue) and one ester group (highlighted green). R1 and R3 are organic groups (e. g. methyl) or a hydrogen atom found in α-hydroxycarboxylic acids. R2, R4 and R5 are organic groups or a hydrogen atom found in common amino acids.

Depsipeptide natural products

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File:Enterobactin.svg
Enterochelin is a depsipeptide that is an iron-transporter.[5]

Several depsipeptides have been found to exhibit anti-cancer properties.[6]

A depsipeptide enzyme inhibitor includes romidepsin, a member of the bicyclic peptide class, a known histone deacetylase inhibitors (HDACi). It was first isolated as a fermentation product from Chromobacterium violaceum by the Fujisawa Pharmaceutical Company.[7]

Streptogramins, specifically streptogramin B antibiotics, are depsipeptides that bind to the 50S subunit of bacterial ribosomes.[8] Etamycin was shown in preliminary data in 2010 to have potent activity against MRSA in a mouse model.[9]

Several depsipeptides from Streptomyces exhibit antimicrobial activity.[10][11] These form a new, potential class of antibiotics known as acyldepsipeptides (ADEPs). ADEPs target and activate the casein lytic protease (ClpP) to initiate uncontrolled peptide and unfolded protein degradation, killing many Gram-positive bacteria.[12][13][14]

Depsipeptides can be formed through a Passerini reaction.[15]

References

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  1. ^ IUPAC, Compendium of Chemical Terminology, 5th ed. (the "Gold Book") (2025). Online version: (2006–) "depsipeptides". Lua error in Module:Citation/CS1/Configuration at line 2172: attempt to index field '?' (a nil value).
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  10. ^ K. H. Michel, R. E. Kastner (Eli Lilly and Company), US 4492650, 1985 [Chem. Abstr. 1985, 102, 130459]
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Further reading

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  • papuamide Lua error in Module:Citation/CS1/Configuration at line 2172: attempt to index field '?' (a nil value).
  • neamphamide A Lua error in Module:Citation/CS1/Configuration at line 2172: attempt to index field '?' (a nil value).
  • callipeltin A Lua error in Module:Citation/CS1/Configuration at line 2172: attempt to index field '?' (a nil value).
  • mirabamides A-D Lua error in Module:Citation/CS1/Configuration at line 2172: attempt to index field '?' (a nil value).; Lua error in Module:Citation/CS1/Configuration at line 2172: attempt to index field '?' (a nil value).