Solid-Phase Synthesis and Antibacterial Activity of Cyclohexapeptide Wollamide B Analogs

Tsutsumi, Lissa S.; Elmore, John M; Dang, Uyen; Wallace, Miranda J.; Marreddy, Ravi K. R.; Lee, Robin B.; Tan, Ghee Teng; Hurdle, Julian G.; Lee, Richard; Sun, Dianqing

doi:10.1021/acscombsci.7b00189

Cited by 18 publications

(28 citation statements)

References 31 publications

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“…2) Together with the SAR data presented here, this observation supports the proposition that wollamides act via a specific and well-defined molecular target, where activity or binding can be negated by even minor changes to the wollamide structure (i.e., changes to a single amino acid residue or a single stereocenter). Preferential activity of wollamides against mycobacteria compared to that of Gram-positive and Gram-negative bacteria (8,10,12) further supports the hypothesis that a specific wollamide molecular target exists. Within the infected host, M. tuberculosis bacteria vary greatly with respect to replication, metabolic status, and susceptibility to antibiotics (14)(15)(16).…”

Section: Discussionmentioning

confidence: 58%

“…Wollamide-producing Streptomyces species are exceptionally rare and to the best of our knowledge cannot be sourced from existing repositories (i.e., the ATCC). Our initial identification of the synthetically accessible antimycobacterial cyclic hexapeptide wollamides (8) have led to reports on the chemical synthesis of wollamides (9,11,12) and SAR investigations against M. tuberculosis H37Rv (11,12). The present study assessed 36 new synthetic wollamides and compared their structure-activity relationships to those of 46 known cyclic peptide wollamide derivatives.…”

Section: Discussionmentioning

confidence: 99%

“…Preliminary structure-activity relationship (SAR) studies, comparing the naturally produced wollamides and desotamides, highlighted the importance of amino acid residue VI (i.e., D-Orn over Gly) and suggested that compound 2 held promise. The solid-phase synthesis of compound 2 was subsequently described (9,10), as were SAR studies for some synthetic wollamides, assessing in vitro growth-inhibitory activity against M. tuberculosis H37Rv (11,12). Here, we report the synthesis and antimycobacterial activity of 36 new wollamide analogues and compare their antimycobacterial activity with that of 46 known wollamides.…”

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confidence: 97%

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Structure-Activity Relationships of Wollamide Cyclic Hexapeptides with Activity against Drug-Resistant and Intracellular Mycobacterium tuberculosis

Khalil

Hill

León-Rodríguez

et al. 2019

Antimicrob Agents Chemother

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Wollamides are cyclic hexapeptides, recently isolated from an Australian soil Streptomyces isolate, that exhibit promising in vitro antimycobacterial activity against Mycobacterium bovis Bacille Calmette Guérin without displaying cytotoxicity against a panel of mammalian cells. Here, we report the synthesis and antimycobacterial activity of 36 new synthetic wollamides, collated with all known synthetic and natural wollamides, to reveal structure characteristics responsible for in vitro growth-inhibitory activity against Mycobacterium tuberculosis (H37Rv, H37Ra, CDC1551, HN878, and HN353). The most potent antimycobacterial wollamides were those where residue VI d-Orn (wollamide B) was replaced by d-Arg (wollamide B1) or d-Lys (wollamide B2), with all activity being lost when residue VI was replaced by Gly, l-Arg, or l-Lys (wollamide B3). Substitution of other amino acid residues mainly reduced or ablated antimycobacterial activity. Significantly, whereas wollamide B2 was the most potent in restricting M. tuberculosis in vitro, wollamide B1 restricted M. tuberculosis intracellular burden in infected macrophages. Wollamide B1 synergized with pretomanid (PA-824) in inhibiting M. tuberculosis in vitro growth but did not antagonize prominent first- and second-line tuberculosis antibiotics. Furthermore, wollamide B1 exerted bactericidal activity against nonreplicating M. tuberculosis and impaired growth of multidrug- and extensively drug-resistant clinical isolates. In vivo pharmacokinetic profiles for wollamide B1 in rats and mice encourage further optimization of the wollamide pharmacophore for in vivo bioavailability. Collectively, these observations highlight the potential of the wollamide antimycobacterial pharmacophore.

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Section: Discussionmentioning

confidence: 58%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 97%

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Structure-Activity Relationships of Wollamide Cyclic Hexapeptides with Activity against Drug-Resistant and Intracellular Mycobacterium tuberculosis

Khalil

Hill

León-Rodríguez

et al. 2019

Antimicrob Agents Chemother

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“…Whereas molecules whose interactions are with proteinaceous receptors can be made inefficient by one or a few changes in amino acid sequence, polypeptides that act by disrupting the lipid bilayer physicochemical properties are less likely to become inactivated by resistance (Rollins-Smith et al 2002). Indeed the amphipathic nature of AMPs has been found essential and can be achieved by helical (Sansom 1991;Bechinger 1997), cyclic (Cao et al 2018Laurencin et al 2018;Tsutsumi et al 2018;Zhao et al 2018), and/or β-sheet arrangements (Hong and Su 2011; Rautenbach et al 2016a, b;Sychev et al 2017;Usachev et al 2017). Thus the insights gained from the studies of cationic amphipathic antimicrobial peptides have stimulated the design of a number of small amphipathic molecules (Arnusch et al 2012;Ghosh et al 2014), pseudopeptides (Porter et al 2002;Patch and Barron 2003;Kuroda and DeGrado 2005;Violette et al 2006;Makovitzki et al 2008;Scott et al 2008;Rotem and Mor 2009;Palermo and Kuroda 2010;Laurencin et al 2018), and polymers (Rank et al 2017) with potent antimicrobial properties.…”

Section: Introductionmentioning

confidence: 99%

The Mechanisms of Action of Cationic Antimicrobial Peptides Refined by Novel Concepts from Biophysical Investigations

Aisenbrey¹,

Marquette²,

Bechinger³

2019

Advances in Experimental Medicine and Biology

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Even 30 years after the discovery of magainins, biophysical and structural investigations on how these peptides interact with membranes can still bear surprises and add new interesting detail to how these peptides exert their antimicrobial action. Early on, using oriented solid-state NMR spectroscopy, it was found that the amphipathic helices formed by magainins are active when being oriented parallel to the membrane surface. More recent investigations indicate that this in-planar alignment is also found when PGLa and magainin in combination exert synergistic pore-forming activities, where studies on the mechanism of synergistic interaction are ongoing. In a related manner, the investigation of dimeric antimicrobial peptide sequences has become an interesting topic of research which bears promise to refine our views how antimicrobial action occurs. The molecular shape concept has been introduced to explain the effects of lipids and peptides on membrane morphology, locally and globally, and in particular of cationic amphipathic helices that partition into the membrane interface. This concept has been extended in this review to include more recent ideas on soft membranes that can adapt to external stimuli including membrane-disruptive molecules. In this manner, the lipids can change their shape in the presence of low peptide concentrations, thereby maintaining the bilayer properties. At higher peptide concentrations, phase transitions occur which lead to the formation of pores and membrane lytic processes. In the context of the molecular shape concept, the properties of lipopeptides, including surfactins, are shortly presented, and comparisons with the hydrophobic alamethicin sequence are made. Keywords (separated by "-") Magainin-PGLa-Cecropin-LL37-Surfacting alamethicin-Membrane topology-Membrane pore-Membrane macroscopic phase-SMART model-Carpet model-Toroidal pore-Peptide-lipid interactions-Molecular shape concept

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“…In contrast, molecules that specifically target proteinaceous receptors can be made inefficient by mutagenesis of one or a few sites, and it is much less likely that bacteria develop resistance to compounds whose primary target is the destruction of the physico-chemical properties of the lipid membrane [ 15 ]. Membrane-active peptides exhibit a wide range of structural features some being helical in their bilayer-associated state [ 16 , 17 ], others forming cyclic [ 18 , 19 , 20 , 21 ] and/or β-sheet arrangements [ 22 , 23 , 24 , 25 , 26 ]. Indeed, following the insights gained from the studies of cationic amphipathic antimicrobial peptides a number of small amphipathic molecules [ 27 , 28 ], pseudopeptides [ 21 , 29 , 30 , 31 , 32 , 33 , 34 , 35 , 36 ], and polymers [ 37 ] have been designed and investigated, and found to also exhibit potent antimicrobial activities.…”

Section: Introductionmentioning

confidence: 99%

Biophysical Investigations Elucidating the Mechanisms of Action of Antimicrobial Peptides and Their Synergism

Marquette

Bechinger

2018

Biomolecules

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Biophysical and structural investigations are presented with a focus on the membrane lipid interactions of cationic linear antibiotic peptides such as magainin, PGLa, LL37, and melittin. Observations made with these peptides are distinct as seen from data obtained with the hydrophobic peptide alamethicin. The cationic amphipathic peptides predominantly adopt membrane alignments parallel to the bilayer surface; thus the distribution of polar and non-polar side chains of the amphipathic helices mirror the environmental changes at the membrane interface. Such a membrane partitioning of an amphipathic helix has been shown to cause considerable disruptions in the lipid packing arrangements, transient openings at low peptide concentration, and membrane disintegration at higher peptide-to-lipid ratios. The manifold supramolecular arrangements adopted by lipids and peptides are represented by the ‘soft membranes adapt and respond, also transiently’ (SMART) model. Whereas molecular dynamics simulations provide atomistic views on lipid membranes in the presence of antimicrobial peptides, the biophysical investigations reveal interesting details on a molecular and supramolecular level, and recent microscopic imaging experiments delineate interesting sequences of events when bacterial cells are exposed to such peptides. Finally, biophysical studies that aim to reveal the mechanisms of synergistic interactions of magainin 2 and PGLa are presented, including unpublished isothermal titration calorimetry (ITC), circular dichroism (CD) and dynamic light scattering (DLS) measurements that suggest that the peptides are involved in liposome agglutination by mediating intermembrane interactions. A number of structural events are presented in schematic models that relate to the antimicrobial and synergistic mechanism of amphipathic peptides when they are aligned parallel to the membrane surface.

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Solid-Phase Synthesis and Antibacterial Activity of Cyclohexapeptide Wollamide B Analogs

Cited by 18 publications

References 31 publications

Structure-Activity Relationships of Wollamide Cyclic Hexapeptides with Activity against Drug-Resistant and Intracellular Mycobacterium tuberculosis

Structure-Activity Relationships of Wollamide Cyclic Hexapeptides with Activity against Drug-Resistant and Intracellular Mycobacterium tuberculosis

The Mechanisms of Action of Cationic Antimicrobial Peptides Refined by Novel Concepts from Biophysical Investigations

Biophysical Investigations Elucidating the Mechanisms of Action of Antimicrobial Peptides and Their Synergism

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