Abstract
This review describes a selection of macrocyclic natural products and structurally modified analogs containing peptidic and non-peptidic elements as structural features that potentially modulate cellular permeability. Examples range from exclusively peptidic structures like cyclosporin A or phepropeptins to compounds with mostly non-peptidic character, such as telomestatin or largazole. Furthermore, semisynthetic approaches and synthesis platforms to generate general and focused libraries of compounds at the interface of cyclic peptides and non-peptidic macrocycles are discussed.
Keywords:
Cellular permeability; Library; Macrocycle; Modular synthesis; Semi-synthesis.
MeSH terms
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Biological Products
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Cyclization
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Depsipeptides / chemistry
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Depsipeptides / metabolism
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Humans
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Lactones / chemistry
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Lactones / metabolism
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Macrocyclic Compounds / chemical synthesis
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Macrocyclic Compounds / chemistry*
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Oxazoles / chemistry
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Oxazoles / metabolism
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Peptide Library
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Peptides, Cyclic / chemical synthesis
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Peptides, Cyclic / chemistry*
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Peptides, Cyclic / metabolism
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Permeability
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Protein Conformation
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Spiro Compounds / chemistry
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Spiro Compounds / metabolism
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Streptogramins / chemistry
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Streptogramins / metabolism
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Thiazoles / chemistry
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Thiazoles / metabolism
Substances
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Biological Products
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Depsipeptides
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Lactones
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Macrocyclic Compounds
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Oxazoles
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Peptide Library
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Peptides, Cyclic
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Spiro Compounds
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Streptogramins
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Thiazoles
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apratoxin A
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largazole
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sanglifehrin A
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telomestatin
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jasplakinolide