Segment Solid‐Phase Total Synthesis of the Anthelmintic Cyclooctadepsipeptides PF1022A and Emodepside

Scherkenbeck, Jürgen; Lüttenberg, Sebastian; Ludwig, Monika; Brücher, Karin; Kotthaus, Andreas

doi:10.1002/ejoc.201101421

Cited by 16 publications

(9 citation statements)

References 40 publications

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“…A segment total synthesis based on couplings of the didepsipeptides prepared in solution developed by the same group worked well on both Wang- and Kaiser-resin (Scheme 17) [112]. The advantage of this procedure is, that in the coupling steps solely amide bonds are formed which succeeds in higher yields as ester formation.…”

Section: Cyclooctadepsipeptidesmentioning

confidence: 99%

Cyclodepsipeptides: A Rich Source of Biologically Active Compounds for Drug Research

Sivanathan

Scherkenbeck

2014

Molecules

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Abstract:Faced with the need to find new drugs for all kinds of diseases, science sees that Nature offers numerous classes of compounds showing an impressively high biological potential. Among those are the cyclodepsipeptides, hybrid structures composed of amino and hydroxy acids. In the past decades numerous cyclodepsipeptides have been isolated and their potential as drugs has been studied extensively. For several cyclodepsipeptides total syntheses both in solution and on solid-phase have been established, allowing the production of combinatorial libraries. In addition, the biosynthesis of specific cyclodepsipeptides has been elucidated and used for the chemoenzymatic preparation of nonnatural analogues. This review summarizes the recent literature on cyclic tetra-to decadepsipeptides, composed exclusively of α-amino-and α-hydroxy acids.

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Section: Cyclooctadepsipeptidesmentioning

confidence: 99%

Cyclodepsipeptides: A Rich Source of Biologically Active Compounds for Drug Research

Sivanathan

Scherkenbeck

2014

Molecules

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“…[1] In particular, α-hydroxy acids are essential constituents of depsipeptides where they function as mimetics for the corresponding natural amino acids; thus causing a wide range of biological activities. [9,10] Despite there being different routes to α-hydroxy acids, no general methods are available that allow the synthesis of a broad variety of structurally diverse aryllactic acids. [9,10] Despite there being different routes to α-hydroxy acids, no general methods are available that allow the synthesis of a broad variety of structurally diverse aryllactic acids.…”

Section: Introductionmentioning

confidence: 99%

“…[2][3][4][5][6][7][8] During our studies on the solid-phase synthesis of the anthelmintic PF1022A and related biologically active cyclodepsipeptides, we required a set of enantiomerically pure d-aryllactic and dhetaryllactic acids. [9,10] Despite there being different routes to α-hydroxy acids, no general methods are available that allow the synthesis of a broad variety of structurally diverse aryllactic acids. The basic methods to enantiomerically pure, or at least enantiomerically enriched, phenyllactic acids can be attributed to four basic strategies ( Figure 1).…”

Section: Introductionmentioning

confidence: 99%

Enantioselective Reduction of 3‐Aryl‐2‐oxo‐propanoic Acids: A Comparison of Enzymatic and Transition‐Metal‐Catalyzed Methods

Lüttenberg

Heyden

et al. 2013

Eur J Org Chem

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Phenyllactic acids are important constituents of depsipeptides, which are a large class of natural products expressing a wide range of biological activities. Despite there being several methods for the enantioselective synthesis of α‐hydroxy acids, almost no studies are available addressing the substrate selectivity of transition‐metal and enzyme‐catalyzed methods for the preparation of substituted phenyllactic or more general aryllactic acids. We report herein comparative results for Rh‐DiPAMP (DiPAMP = 1,2‐ethandiylbis[(o‐methoxyphenyl)phenylphosphane]) and lactate dehydrogenase catalyzed enantioselective reductions of several 3‐aryl‐2‐oxopropanoic acids.

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“…[27] Apart from the suitable protecting-group strategy,t echnical difficul- ties to be mastered by chemical synthesis comprise racemization and hindered couplingo fN -methyl amino acids. [43,44] Our approachp rovides ar obust in vivo system for the generation of structurally diverseC PDs, and we have significantly expandedt he possibilities for the design and engineering of CDP synthetasesw ith novel biosynthetic capabilities. The newly generated chimeric compounds point to af uture of rational engineering of CDP structures that might have beneficial pharmacological effects.…”

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confidence: 99%

Reprogramming the Biosynthesis of Cyclodepsipeptide Synthetases to Obtain New Enniatins and Beauvericins

et al. 2016

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Non-ribosomal peptide synthetases are complex multimodular biosynthetic machines that assemble various important and medically relevant peptide antibiotics. An interesting subgroup comprises the cyclodepsipeptide synthetases from fungi synthesizing cyclohexa- and cyclo-octadepsipeptides with antibacterial, anthelmintic, insecticidal, and anticancer properties; some are marketed drugs. We exploit the modularity of these highly homologous synthetases by fusing the hydroxy-acid-activating module of PF1022 synthetase with the amino-acid-activating modules of enniatin and beauvericin synthetase, thus yielding novel hybrid synthetases. The artificial synthetases expressed in Escherichia coli and the fungus Aspergillus niger yielded new cyclodepsipeptides, thus paving the way for the exploration of these derivatives for their bioactivity.

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Segment Solid‐Phase Total Synthesis of the Anthelmintic Cyclooctadepsipeptides PF1022A and Emodepside

Cited by 16 publications

References 40 publications

Cyclodepsipeptides: A Rich Source of Biologically Active Compounds for Drug Research

Cyclodepsipeptides: A Rich Source of Biologically Active Compounds for Drug Research

Enantioselective Reduction of 3‐Aryl‐2‐oxo‐propanoic Acids: A Comparison of Enzymatic and Transition‐Metal‐Catalyzed Methods

Reprogramming the Biosynthesis of Cyclodepsipeptide Synthetases to Obtain New Enniatins and Beauvericins

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