Heterologous Expression, Biosynthetic Studies, and Ecological Function of the Selective Gq‐Signaling Inhibitor FR900359

Crüsemann, Max; Reher, Raphael; Schamari, Isabella; Brachmann, Alexander O.; Ohbayashi, Tsubasa; Kuschak, Markus; Malfacini, Davide; Seidinger, Alexander; Pinto‐Carbó, Marta; Richarz, René; Reuter, Tatjana; Kehraus, Stefan; Hallab, Asis; Attwood, Misty M.; Schiöth, Helgi B.; Mergaert, Peter; Kikuchi, Yoshitomo; Schäberle, Till F.; Kostenis, Evi; Wenzel, Daniela; Müller, Christa E.; Piel, Jörn; Carlier, Aurélien; Eberl, Leo; König, Gabriele M.

doi:10.1002/anie.201707996

Cited by 62 publications

(101 citation statements)

References 31 publications

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“…MD simulation studies of Gα q protein in complex with FR and YM, respectively, indicated that the kinetic differences are largely contributed by the isopropyl (R 2 in Figure b) interaction with Phe75 in the binding pocket. The new tracers will allow to study binding kinetics of other compounds that bind to the same site, for example, novel analogues and derivatives of YM and FR, that are accessible by chemical synthesis (Rensing, Uppal, Blumer, & Moeller, ; Xiong et al, ; Zhang et al, ), and by biotechnological approaches (Crüsemann et al, ; Taniguchi et al, ). The new tracers will help to design and develop G q inhibitors with specific, desired kinetic profiles.…”

Section: Resultsmentioning

confidence: 99%

“…YM is produced by Chromobacterium sp. (Taniguchi et al, ), while FR was isolated from the plant Ardisia crenata Sims and is produced by the bacterial endophyte Candidatus Burkholderia crenata that is present as a symbiont in the leaves of the plant (Crüsemann et al, ; Fujioka, Koda, & Morimoto, ). A few analogues of FR have also been isolated, however, in tiny amounts (Crüsemann et al, ; Reher et al, ).…”

Section: Introductionmentioning

confidence: 99%

“…(Taniguchi et al, ), while FR was isolated from the plant Ardisia crenata Sims and is produced by the bacterial endophyte Candidatus Burkholderia crenata that is present as a symbiont in the leaves of the plant (Crüsemann et al, ; Fujioka, Koda, & Morimoto, ). A few analogues of FR have also been isolated, however, in tiny amounts (Crüsemann et al, ; Reher et al, ). Recently, the total syntheses of 1 and 2 and some analogues were described, but they represent labour‐intensive procedures providing only small amounts of the products; all of the synthesized analogues showed moderate potency or were inactive (Xiong et al, ; Zhang et al, ).…”

Section: Introductionmentioning

confidence: 99%

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Cell‐permeable high‐affinity tracers for G_q proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Kuschak

Namasivayam

Rafehi

et al. 2020

British J Pharmacology

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Background and Purpose G proteins are intracellular switches that transduce and amplify extracellular signals from GPCRs. The Gq protein subtypes, which are coupled to PLC activation, can act as oncogenes, and their expression was reported to be up‐regulated in cancer and inflammatory diseases. Gq inhibition may be an efficient therapeutic strategy constituting a new level of intervention. However, diagnostic tools and therapeutic drugs for Gq proteins are lacking. Experimental Approach We have now developed Gq‐specific, cell‐permeable 3H‐labelled high‐affinity probes based on the macrocyclic depsipeptides FR900359 (FR) and YM‐254890 (YM). The tracers served to specifically label and quantify Gq proteins in their native conformation in cells and tissues with high accuracy. Key Results FR and YM displayed low nanomolar affinity for Gαq, Gα11 and Gα14 expressed in CRISPR/Cas9 Gαq‐knockout cells, but not for Gα15. The two structurally very similar tracers showed strikingly different dissociation kinetics, which is predicted to result in divergent biological effects. Computational studies suggested a “dowel” effect of the pseudoirreversibly binding FR. A high‐throughput binding assay led to the discovery of novel Gq inhibitors, which inhibited Gq signalling in recombinant cells and primary murine brown adipocytes, resulting in enhanced differentiation. Conclusions and Implications The Gq protein inhibitors YM and FR are pharmacologically different despite similar structures. The new versatile tools and powerful assays will contribute to the advancement of the rising field of G protein research.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Cell‐permeable high‐affinity tracers for G_q proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Kuschak

Namasivayam

Rafehi

et al. 2020

British J Pharmacology

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“…Synthetic FR900359 has been pharmacologically characterized on G q ‐, G s ‐, and G i ‐mediated signaling and compared to natural (isolated) FR900359, showing identical biological activity (Figure ). Recently, Crüsemann et al reported the first heterologous biosynthesis of FR900359 in a cultivable, bacterial ( Escherichia coli ) host by expression of the FR nonribosomal peptide synthetase (frs) genes, which were revealed by sequencing the uncultured endosymbiont of A. crenata …”

Section: Selective Gq Inhibitorsmentioning

confidence: 99%

Recent achievements in developing selective G_q inhibitors

Zhang

Nielsen

Strømgaard

2019

Medicinal Research Reviews

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G proteins are key mediators of G protein‐coupled receptor (GPCR) signaling, facilitating a plethora of important physiological processes. The role of G proteins is much less understood than other aspects of GPCR function, which is largely due to the shortage of potent and selective G protein inhibitors. The natural cyclic depsipeptides YM‐254890 and FR900359 are two of the very few known selective inhibitors of the Gq subfamily, and are used as unique pharmacological tools in the study of G q‐mediated signaling. Moreover, a peptide‐based G protein antagonist‐2A (GP‐2A), a 27‐residue peptide (27mer(I860A)) derived from phospholipase C‐β3 (PLC‐β3), and the small molecule BIM‐46187 have also been characterized as selective G q inhibitors within the past 5 years. In this review, we highlight the recent development in chemical syntheses, characterization, and mechanism of action of these selective G q inhibitors. The development and application of G q‐selective inhibitors will expand our knowledge of the structure and function of G protein‐mediated signaling, shed light on the development of inhibitors for other G protein classes, and feed in to drug discovery for diseases where G proteins are implicated, including various forms of cancer.

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“…Burkholderia leaf nodule symbionts show extensive signs of reductive genome evolution, with coding capacities ranging from 41.7 % to 67.3 % and an accumulation of pseudogenes and insertion sequences [10–12]. Despite extensive genome erosion, some symbionts have been shown to produce secondary metabolites, likely involved in the protection of the host from herbivory, such as the insecticidal kirkamide and the depsipeptide FR900359, as well as the herbicidal streptol-glucoside possibly involved in allelopathic interactions [12–14]. Because of genomic instability and evolved co-dependence, it is unclear whether secondary metabolism was present in the ancestor of leaf nodule Burkholderia or acquired as a secondary trait.…”

Section: Introductionmentioning

confidence: 99%

Early steps in the evolution of vertical transmission revealed by a plant-bacterium symbiosis

Danneels

Acar

et al. 2019

Preprint

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Various plant species establish intimate symbioses with bacteria within their aerial organs. The bacteria are contained within nodules or glands often present in distinctive patterns on the leaves in what is commonly referred to as leaf nodule symbiosis. We describe here a highly specific symbiosis between a wild yam species from Madagascar, Dioscorea sansibarensis and bacteria of the species Orrella dioscoreae. Using whole genome sequencing of plastid and bacteria from wild-collected samples, we show phylogenetic patterns consistent with a vertical transmission of the symbionts. Unique among leaf nodule symbioses, the bacteria can be cultured and are amenable to comparative transcriptomics and phenotypic characterization, revealing a potential role in complementing the host's arsenal of secondary metabolites. We propose a very recent acquisition of the vertical mode of transmission in this symbiosis which, together with a large effective populations size explain the cultivability and remarkable lack of genome reductive evolution in O. dioscoreae. We leverage these unique features to reveal pathways and functions under positive selection in these specialized endophytes, highlighting the mechanisms enabling a permanent association in the phyllosphere.

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Heterologous Expression, Biosynthetic Studies, and Ecological Function of the Selective Gq‐Signaling Inhibitor FR900359

Cited by 62 publications

References 31 publications

Cell‐permeable high‐affinity tracers for G_q proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Cell‐permeable high‐affinity tracers for G_q proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Recent achievements in developing selective G_q inhibitors

Early steps in the evolution of vertical transmission revealed by a plant-bacterium symbiosis

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Heterologous Expression, Biosynthetic Studies, and Ecological Function of the Selective Gq‐Signaling Inhibitor FR900359

Cited by 62 publications

References 31 publications

Cell‐permeable high‐affinity tracers for Gq proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Cell‐permeable high‐affinity tracers for Gq proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Recent achievements in developing selective Gq inhibitors

Early steps in the evolution of vertical transmission revealed by a plant-bacterium symbiosis

Contact Info

Product

Resources

About

Cell‐permeable high‐affinity tracers for G_q proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Cell‐permeable high‐affinity tracers for G_q proteins provide structural insights, reveal distinct binding kinetics and identify small molecule inhibitors

Recent achievements in developing selective G_q inhibitors