Total Synthesis and Biological Assessment of Novel Albicidins Discovered by Mass Spectrometric Networking

Eckardstein, Leonard von; Petras, Daniel; Dang, Tam; Cociancich, Stéphane; Sabri, Souhir; Gratz, S.; Kerwat, Dennis; Seidel, Maria; Pesic, Alexander; Dorrestein, Pieter C.; Royer, Monique; Weston, John B.; Süssmuth, Roderich D.

doi:10.1002/chem.201704074

Cited by 32 publications

(32 citation statements)

References 26 publications

(57 reference statements)

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“…[13] Based on our previous investigations [11] we first sought a viable replacement for the hydrolyticallyu nstable b-cyanoalanine as building block C. The noncanonical amino acid 2amino-3-(1H-1,2,3-triazol-4-yl)propanoic acid (azahistidine) appealed to us as as uitable substitute as it mimics the cyanoalanine and methoxy-asparagine moieties presenti nt he naturally occurring variants of albicidin (1). [14] Indeed, the synthetic variant 2 exhibited superior antibacterial activity against the tested E. coli, S. typhimurium, B. subtilis and M. luteus strains,a s well as an eight-fold highera ctivity against ciprofloxacin (CIP) sensitive K. pneumoniae (Supporting Information, Ta ble S1). Consequently,w eu sed azahistidine-albicidin 2 as at emplate structuref or the subsequent SAR study:T he first set of analogues (3-17)a rises from sequential deletiono ft he methoxy and hydroxy groups present in the C-terminal dipeptidic pABA moiety ( Table 1, green).…”

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“…Previous findings have shown at olerance for iso-propoxy groups as methoxy-substitutes. [14,15] Therefore, we hoped that more hydrophobic alkoxy groups in building blocks Ea nd F might help boost activity.T ot est this hypothesis, the methoxy moietieso ft he parentc ompound 2 were successively replaced by ethoxy groups to produce synthetic analogues 18-20 (Table 1, blue). Althoughe ach of the three compoundsi nhibited DNA gyrase and showed high to very high activities throughout the series of tested pathogens-except for Klebsiella strains-the doubly substituted analogue 20 stands out ( Figure 2).…”

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confidence: 99%

“…Possibly,t he deleterious effect caused by the Table 1. Assignment of the residuesf or albicidin analogues with sequential deletion of the substituents of the C-terminal dipeptidic moiety (3)(4)(5)(6)(7)(8)(9)(10)(11)(12)(13)(14)(15)(16)(17), sequential replacement of the methoxy groups with ethoxyg roups (18)(19)(20), sequentialr eplacement of the phenolic core structure with pyridines (21-23), andw ith replacement of the carboxylic acid groupw ith a sulfonic acid group( 24). All derivatives contain azahistidine as building block C. O ne could conclude that the hydroxy group in building block Fi s imperative, but ad irect comparison of 22,f or example, with the trisubstituted ands till active analogue 6,n egates that assumption and makes adversee lectronic effects and H-bonding interactions between the nitrogen atom of the pyridine and the adjacent carboxylg roup more likely.…”

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Extensive Structure–Activity Relationship Study of Albicidin's C‐Terminal Dipeptidic p‐Aminobenzoic Acid Moiety

Behroz

Durkin

Gratz

et al. 2019

Chemistry A European J

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Albicidin is ar ecently described natural product that strongly inhibits bacterial DNA gyrase. The pronounced activity,particularly against Gram-negative bacteria, turns it into ap romising lead structure for an antibacterial drug. Hence, structure-activity relationship studies are key for the in-depth understanding of structuralf eatures/moieties affectingg yrase inhibition, antibacteriala ctivity ando vercomingr esistance. The 27 newly synthesized albicidinsg ive profound insights into possibilities for variations of the C-terminus.F urthermore, in the present study,anovel derivative has been identified as overcoming resistance posed by the Klebsiella-protease AlbD. Structural modifications include, for example,a zahistidine replacing the previous instable cyanoalanine as the central amino acid, as well as at riazole amide bond isostere between building blocks Da nd E.

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Extensive Structure–Activity Relationship Study of Albicidin's C‐Terminal Dipeptidic p‐Aminobenzoic Acid Moiety

Behroz

Durkin

Gratz

et al. 2019

Chemistry A European J

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“…Accordingly, the individual middle, C‐ and N‐terminal rings were prepared followed by the coupling of the constituents. We established brief and efficient synthetic pathways for novel as well as reported amino acids, which are also precursors of other NPs (Scheme S1). Compared to previous methods, the middle ring of 2 ( 20 ) was prepared in only four steps using catechol as a starting material.…”

Section: Resultsmentioning

confidence: 99%

Cystobactamid 507: Concise Synthesis, Mode of Action, and Optimization toward More Potent Antibiotics

Elgaher

Hamed

Baumann

et al. 2020

Chemistry A European J

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Lack of new antibiotics and increasing antimicrobial resistance are among the main concerns of healthcare communities nowadays, and these concerns necessitate the search for novel antibacterial agents. Recently, we discovered the cystobactamids—a novel natural class of antibiotics with broad‐spectrum antibacterial activity. In this work, we describe 1) a concise total synthesis of cystobactamid 507, 2) the identification of the bioactive conformation using noncovalently bonded rigid analogues, and 3) the first structure–activity relationship (SAR) study for cystobactamid 507 leading to new analogues with high metabolic stability, superior topoisomerase IIA inhibition, antibacterial activity and, importantly, stability toward the resistant factor AlbD. Deeper insight into the mode of action revealed that the cystobactamids employ DNA minor‐groove binding as part of the drug–target interaction without showing significant intercalation. By designing a new analogue of cystobactamid 919‐2, we finally demonstrated that these findings could be further exploited to obtain more potent hexapeptides against Gram‐negative bacteria.

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“…Die Naturstoffe und ihre entsprechenden BGCs wurden unabhängig voneinander in zwei nichtverwandten Spezies, Cystobacter sp. [165] isolierte Analoga namens Coralmycin A/B gehçren, sowie zahlreiche natürliche und synthetische Albicidin-Analoga [166][167][168][169] beschrieben. Beide Stoffklassen zeigen ausgezeichnete Wirksamkeit im niedrigen mgmL À1 -Bereich nicht nur gegen Gram-positive,s ondern auch gegen Gram-negative Bakterien und sind auch in klinisch relevanten ESKAPE-Stämmen aktiv.E sw urden zahlreiche Vertreter beider Klassen synthetisiert, wodurch auch die Konfiguration der zentralen Aminosäure eindeutig bestimmt werden konnte.D ie verschiedenen Derivate unterscheiden sich im Aminosäure-Motiv,d en pABA-Substituenten und der N-terminalen Modifikation.…”

Section: Cystobactamide Und Albicidineunclassified

Über bisherige Denkweisen hinaus – neue Wirkstoffe zur Überwindung der Antibiotika‐Krise

et al. 2018

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Die öffentliche Wahrnehmung von Antibiotika als verlässliche Arzneimittel veränderte sich drastisch, als Meldungen über “multiresistente Super‐Erreger” die Nachrichten aufrüttelten. Während die Ursachen für die bakterielle Resistenzentwicklung schnell erkannt wurden, befindet sich die Forschung zur Wiedergewinnung von Antibiotika als effektive Arzneistoffe immer noch am Anfang. Dieser Aufsatz umfasst zahlreiche Aspekte des Entwicklungsprozesses neuer Antibiotika, von der Grundlagenforschung bis zum fertigen Medikament. Er bietet einen interdisziplinären Überblick über Methoden zur Identifizierung neuer Antibiotika und erörtert Strategien, um ihren molekularen Wirkmechanismus aufzuklären. Die Darstellung ausgewählter Antibiotika, die kürzlich mithilfe dieser Plattformen entdeckt wurden, verdeutlicht die Effizienz der Ansätze und hebt vielversprechende klinische Kandidaten mit therapeutischem Potential hervor. Zusätzlich wird das Konzept von Molekülen erörtert, die Krankheitserreger “entwaffnen”, indem sie Schlüsselpunkte der Virulenz adressieren. Der Aufsatz schließt mit einer kritischen Beurteilung jener antibakteriellen Wirkstoffe, die sich derzeit in klinischer Entwicklung befinden. Insgesamt soll dieser Aufsatz ausgewählte, innovative antibakterielle Ansätze verknüpfen, um interdisziplinäre Partnerschaften zwischen Chemikern aus der akademischen und industriellen Forschung anzuregen.

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Total Synthesis and Biological Assessment of Novel Albicidins Discovered by Mass Spectrometric Networking

Cited by 32 publications

References 26 publications

Extensive Structure–Activity Relationship Study of Albicidin's C‐Terminal Dipeptidic p‐Aminobenzoic Acid Moiety

Extensive Structure–Activity Relationship Study of Albicidin's C‐Terminal Dipeptidic p‐Aminobenzoic Acid Moiety

Cystobactamid 507: Concise Synthesis, Mode of Action, and Optimization toward More Potent Antibiotics

Über bisherige Denkweisen hinaus – neue Wirkstoffe zur Überwindung der Antibiotika‐Krise

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