Synthesis of Guaianolide Analogues with a Tunable α-Methylene−γ-lactam Electrophile and Correlating Bioactivity with Thiol Reactivity

Jackson, Paul; Schares, Henry A.M.; Jones, Katherine F.; Widen, John C.; Dempe, Daniel P; Grillet, François; Cuellar, Matthew E.; Walters, Michael A.; Harki, Daniel A.; Brummond, Kay M.

doi:10.1021/acs.jmedchem.0c01464

Cited by 17 publications

(20 citation statements)

References 66 publications

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“…In this case, the chemical nature of the group on the lactam nitrogen greatly impacted the reactivity of the α-methylene-γ-lactams toward a model thiol compound (cysteamine). α-Methylene-γ-lactam guaianolides maintaining an inhibitory activity toward NFκB were identified, but there is positive correlation between the thiol reactivity of the compounds and their NFκB inhibitory activity [145]. Another option consists of removing the exomethylene unit, replacing it with a less-or non-reactive group.…”

Section: Thiol Reactivitymentioning

confidence: 99%

Anticancer Targets and Signaling Pathways Activated by Britannin and Related Pseudoguaianolide Sesquiterpene Lactones

Bailly

2021

Biomedicines

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Sesquiterpene lactones (SLs) are abundant in plants and display a large spectrum of bioactivities. The compound britannin (BRT), found in different Inula species, is a pseudoguaianolide-type SL equipped with a typical and highly reactive α-methylene-γ-lactone moiety. The bioproperties of BRT and related pseudoguaianolide SLs, including helenalin, gaillardin, bigelovin and others, have been reviewed. Marked anticancer activities of BRT have been evidenced in vitro and in vivo with different tumor models. Three main mechanisms are implicated: (i) interference with the NFκB/ROS pathway, a mechanism common to many other SL monomers and dimers; (ii) blockade of the Keap1-Nrf2 pathway, with a covalent binding to a cysteine residue of Keap1 via the reactive α-methylene unit of BRT; (iii) a modulation of the c-Myc/HIF-1α signaling axis leading to a downregulation of the PD-1/PD-L1 immune checkpoint and activation of cytotoxic T lymphocytes. The non-specific reactivity of the α-methylene-γ-lactone moiety with the sulfhydryl groups of proteins is discussed. Options to reduce or abolish this reactivity have been proposed. Emphasis is placed on the capacity of BRT to modulate the tumor microenvironment and the immune-modulatory action of the natural product. The present review recapitulates the anticancer effects of BRT, some central concerns with SLs and discusses the implication of the PD1/PD-L1 checkpoint in its antitumor action.

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Section: Thiol Reactivitymentioning

confidence: 99%

Anticancer Targets and Signaling Pathways Activated by Britannin and Related Pseudoguaianolide Sesquiterpene Lactones

Bailly

2021

Biomedicines

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“…[20] Other sesquiterpene lactones (pseudoguaianolide, guaianolides,a nd beyond) and semisynthetic analogues have also shown promising biological activities. [30][31][32][33][34][35][36] As such, the (pseudo)guaianolide family and their analogues have been implicated as leads in drug development. While the majority of medicinal chemistry and drug discoverye fforts re- lated to (pseudo)guaianolides involves isolation and/or semisynthesis, [37] there are numerous total syntheses(pseudoguaianolides [12][13][14][15] and guaianolides [38][39][40][41][42][43][44][45] )m ethods/approaches, [36,[46][47][48][49][50][51] and de novo analogue syntheses.…”

Section: Introductionmentioning

confidence: 99%

“…[30][31][32][33][34][35][36] As such, the (pseudo)guaianolide family and their analogues have been implicated as leads in drug development. While the majority of medicinal chemistry and drug discoverye fforts re- lated to (pseudo)guaianolides involves isolation and/or semisynthesis, [37] there are numerous total syntheses(pseudoguaianolides [12][13][14][15] and guaianolides [38][39][40][41][42][43][44][45] )m ethods/approaches, [36,[46][47][48][49][50][51] and de novo analogue syntheses. [52,53] For drug discovery purposes, it would be ideal to have am odularr oute to pseudoguaianolide-analogues that retains the structural complexityo f the natural product family,c an tempert he reactivity of the Michael acceptors, [36] and allows for significant diversification aroundt he scaffold.…”

Section: Introductionmentioning

confidence: 99%

“…While the majority of medicinal chemistry and drug discoverye fforts re- lated to (pseudo)guaianolides involves isolation and/or semisynthesis, [37] there are numerous total syntheses(pseudoguaianolides [12][13][14][15] and guaianolides [38][39][40][41][42][43][44][45] )m ethods/approaches, [36,[46][47][48][49][50][51] and de novo analogue syntheses. [52,53] For drug discovery purposes, it would be ideal to have am odularr oute to pseudoguaianolide-analogues that retains the structural complexityo f the natural product family,c an tempert he reactivity of the Michael acceptors, [36] and allows for significant diversification aroundt he scaffold. [54] With these goals in mind, we sought to develop af unction-oriented synthetic route [54] to structurally complexp seudoguaianolidec hemical space whereby the lactone-ringi sc leaved and a" functional group" ("FG") is installed at the C-1 position (Figure 2B).…”

Section: Introductionmentioning

confidence: 99%

“…Of direct relevance to this report, helenalin has been shown to activate Nrf2 [20] . Other sesquiterpene lactones (pseudoguaianolide, guaianolides, and beyond) and semisynthetic analogues have also shown promising biological activities [30–36] . As such, the (pseudo)guaianolide family and their analogues have been implicated as leads in drug development.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Function‐Oriented and Modular (+/−)‐cis‐Pseudoguaianolide Synthesis: Discovery of New Nrf2 Activators and NF‐κB Inhibitors

Emmetiere

Ratnayake

Schares

et al. 2021

Chemistry A European J

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Described herein is af unction-oriented synthesis route and biological evaluation of pseudoguaianolide analogues. The 10-step synthetic route developed retains the topological complexity of the natural product, installs functional handles for late-stage diversification, and forges the key bioactive Michael acceptors early in the synthesis. The analogues were found to be low-micromolar Nrf2 activators and micromolar NF-kBi nhibitors and dependent on the local environment of the Michael acceptor moieties.

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[3+2] Cycloaddition of Vinyl Cyclopropane and Hydroxylamines via Isocynate Intermediate to γ‐Lactams

Huang

Luan

2023

Chin. J. Chem.

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Comprehensive Summary A general and efficient strategy for the synthesis of γ‐lactams has been reported. The hydroxylamines form Lossen rearrangement products of electron‐deficient group migration with base and then undergo [3+2] cycloaddition reaction with vinyl cyclopropane, which could be performed with broad substrate scope, excellent functional group tolerance and high efficiency to produce the desired products. It also allowed further modification to other derivatives of these γ‐lactams.

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Synthesis of Guaianolide Analogues with a Tunable α-Methylene−γ-lactam Electrophile and Correlating Bioactivity with Thiol Reactivity

Cited by 17 publications

References 66 publications

Anticancer Targets and Signaling Pathways Activated by Britannin and Related Pseudoguaianolide Sesquiterpene Lactones

Anticancer Targets and Signaling Pathways Activated by Britannin and Related Pseudoguaianolide Sesquiterpene Lactones

Function‐Oriented and Modular (+/−)‐cis‐Pseudoguaianolide Synthesis: Discovery of New Nrf2 Activators and NF‐κB Inhibitors

[3+2] Cycloaddition of Vinyl Cyclopropane and Hydroxylamines via Isocynate Intermediate to γ‐Lactams

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