Selective Modification of Ribosomally Synthesized and Post‐Translationally Modified Peptides (RiPPs) through Diels–Alder Cycloadditions on Dehydroalanine Residues

Vries, Reinder H. de; Viel, Jakob; Oudshoorn, Ruben; Kuipers, Oscar P.; Roelfes, Gérard

doi:10.1002/chem.201902907

Cited by 27 publications

(37 citation statements)

References 45 publications

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“…Site‐specific modification in the tail region of thiostrepton should also likely be beneficial for maintaining antibacterial activity. X‐ray structural determination of thiostrepton bound to the 50S ribosomal subunit have established that the tail region is solvent exposed, with modifications to this region generally well tolerated –. Analogs 2 a – l and 4 a – g were consequently evaluated for activity against a broad spectrum of Gram‐positive bacteria (Table ).…”

Section: Resultsmentioning

confidence: 99%

“…Moreover, by introducing an aldehyde group with C−H amidation, oxime ligation could be employed to install an even greater range of functionality. Many of the analogs maintained potent antibacterial activity with only a moderate reduction relative to thiostrepton perhaps because Dha1 is located in a solvent exposed region of thiostrepton with modifications to this region generally well‐tolerated –. Most importantly, many analogs showed significantly greater solubility in pH 7.2 aqueous solution with up to 28‐fold improvement to 83 μg mL −1 , surpassing the aqueous solubility of all previously reported thiostrepton derivatives prepared by semisynthetic or biosynthetic methods …”

Section: Introductionmentioning

confidence: 96%

“…Importantly, many of the synthesized thiostrepton derivatives maintained potent antibacterial activity with only moderate reductions relative to 1 . However, hydrophobic functionality has generally been introduced, including in recent work involving cycloaddition to the Dha residues, and aqueous solubility has not been reported for any of these derivatives of 1 . Moreover, physicochemical properties of derivatives of 1 have not been characterized, except for studies by Honek and co‐workers on several thiol Michael adducts showing qualitative increases in overall polarity by RP‐HPLC and improvements in theoretical logP …”

Section: Introductionmentioning

confidence: 99%

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Cobalt(III)‐Catalyzed C−H Amidation of Dehydroalanine for the Site‐Selective Structural Diversification of Thiostrepton

et al. 2019

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Thiostrepton is a potent antibiotic against a broad range of Gram‐positive bacteria, but its medical applications have been limited by its poor aqueous solubility. In this work, the first C(sp2)−H amidation of dehydroalanine (Dha) residues was applied to the site selective modification of thiostrepton to prepare a variety of derivatives. Unlike all prior methods for the modification of thiostrepton, the alkene framework of the Dha residue is preserved and with complete selectivity for the Z‐stereoisomer. Additionally, an aldehyde group was introduced by C−H amidation, enabling oxime ligation for the installation of an even greater range of functionality. The thiostrepton derivatives generally maintain antimicrobial activity, and importantly, eight of the derivatives displayed improved aqueous solubility (up to 28‐fold), thereby addressing a key shortcoming of this antibiotic. The exceptional functional group compatibility and site selectivity of CoIII‐catalyzed C(sp2)−H Dha amidation suggests that this approach could be generalized to other natural products and biopolymers containing Dha residues.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 96%

Section: Introductionmentioning

confidence: 99%

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Cobalt(III)‐Catalyzed C−H Amidation of Dehydroalanine for the Site‐Selective Structural Diversification of Thiostrepton

et al. 2019

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“…Dehydroalanine (ΔAla) are naturally occurring non‐coded amino acid, found primarily in peptides. In this context, ΔAla appendage is a useful synthetic tool for simple modification of peptides or proteins by different reactions such as Michael addition, Diels‐Alder cycloaddition and radical coupling under mild conditions . Dehydroalanine derivatives are also widely applied as electrophilic partners in the range of ionic reactions for the asymmetric synthesis of unusual AAs .…”

Section: Dehydroalanine Derivatives As Substratesmentioning

confidence: 99%

Advances in Asymmetric Amino Acid Synthesis Enabled by Radical Chemistry

2020

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Chiral amino acids (AAs), being the main "building" blocks of the living organisms, are also an important class of organic compounds which broadly applied in synthetic chemistry, biochemistry, catalysis and the designing of new drugs. According to the industrial-commodity market, chiral non-proteinogenic AAs containing various functional groups come to the fore. To date, radical cross-coupling reactions are becoming an option as an attractive powerful tool for AA syntheses. Owing to mild reaction conditions and high functional-group tolerance, radical chemistry represents an ideal strategy for the synthesis of challenging complex non-proteinogenic AAs. Moreover, the radical cross-coupling allows introducing AA residue into drug scaffolds and natural compounds. In the present review, we wish to summarize and discuss all the reported to date methods of the asymmetric synthesis of AAs using radical chemistry by presenting a comprehensive account of the literature in this field going back to 1990. We especially emphasize on a radical chemistry approach and, exclusively, on stereoselective synthesis of various α-, β-, γ-AAs and derivatives employing a different type of radical initiators starting from AIBN and organostannes and ending with powerful photoredox catalysis. Furthermore, the mechanism of the reported reactions will be discussed. Radicals Generated from AA Derivatives in Conjugate Additions 6.1. Radicals Generated from α-Substituted Glycine Derivatives in AA Synthesis 6.2. Modification of Chiral AA Side Chain by Radical Chemistry 7.

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“…[5] Previously, several studies have been carried out on additions to the Dha residues in 1 (Figure 1, middle). [6,7] Va riable Dha site selectivity was observed depending on the transformation and reaction conditions,with notable site and diastereoselectivity achieved for Rh-catalyzed arylboronic acid additions. [6b] Importantly,many of the synthesized thiostrepton derivatives maintained potent antibacterial activity with only moderate reductions relative to 1.H owever,h ydrophobic functionality has generally been introduced, including in recent work involving cycloaddition to the Dha residues, [7a] and aqueous solubility has not been reported for any of these derivatives of 1.M oreover,p hysicochemical properties of derivatives of 1 have not been characterized, except for studies by Honek and co-workers on several thiol Michael adducts showing qualitative increases in overall polarity by RP-HPLC and improvements in theoretical logP.…”

Section: Introductionmentioning

confidence: 99%

Cobalt(III)‐Catalyzed C−H Amidation of Dehydroalanine for the Site‐Selective Structural Diversification of Thiostrepton

et al. 2019

View full text Add to dashboard Cite

show abstract

Selective Modification of Ribosomally Synthesized and Post‐Translationally Modified Peptides (RiPPs) through Diels–Alder Cycloadditions on Dehydroalanine Residues

Cited by 27 publications

References 45 publications

Cobalt(III)‐Catalyzed C−H Amidation of Dehydroalanine for the Site‐Selective Structural Diversification of Thiostrepton

Cobalt(III)‐Catalyzed C−H Amidation of Dehydroalanine for the Site‐Selective Structural Diversification of Thiostrepton

Advances in Asymmetric Amino Acid Synthesis Enabled by Radical Chemistry

Cobalt(III)‐Catalyzed C−H Amidation of Dehydroalanine for the Site‐Selective Structural Diversification of Thiostrepton

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