Cyclic Thiosulfonates for Thiol-Mediated Uptake: Cascade Exchangers, Transporters, Inhibitors

Kato, Takehiro; Lim, Bumhee; Cheng, Yangyang; Pham, Anh-Tuan; Maynard, John R. J.; Moreau, Dimitri; Poblador‐Bahamonde, Amalia I.; Sakai, Naomi; Matile, Stefan

doi:10.1021/jacsau.1c00573

Cited by 18 publications

(54 citation statements)

References 89 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The low energy barriers are consistent with the observations of Matile et al . that the ring‐opening of cyclic thiosulfonates proceeds at a high rate (instantaneous on the NMR timescale) in a solution of D 2 O/DMSO‐ d 6 [14a] . Overall, the data obtained by DFT simulations suggest that all cyclic thiosulfonates studied are potentially reactive toward sulfhydryl moieties.…”

Section: Resultsmentioning

confidence: 77%

Anticancer Agents Derived from Cyclic Thiosulfonates: Structure‐Reactivity and Structure‐Activity Relationships

et al. 2022

View full text Add to dashboard Cite

Reported are structure‐property‐function relationships associated with a class of cyclic thiosulfonate molecules—disulfide‐bond disrupting agents (DDAs)—with the ability to downregulate the Epidermal Growth Factor Receptor (HER) family in parallel and selectively induce apoptosis of EGFR+ or HER2+ breast cancer cells. Recent findings have revealed that the DDA mechanism of action involves covalent binding to the thiol(ate) from the active site cysteine residue of members of the protein disulfide isomerase (PDI) family. Reported is how structural modifications to the pharmacophore can alter the anticancer activity of cyclic thiosulfonates by tuning the dynamics of thiol‐thiosulfonate exchange reactions, and the studies reveal a correlation between the biological potency and thiol‐reactivity. Specificity of the cyclic thiosulfonate ring‐opening reaction by a nucleophilic attack can be modulated by substituent addition to a parent scaffold. Lead compound optimization efforts are also reported, and have resulted in a considerable decrease of the IC50/IC90 values toward HER‐family overexpressing breast cancer cells.

show abstract

Section: Resultsmentioning

confidence: 77%

Anticancer Agents Derived from Cyclic Thiosulfonates: Structure‐Reactivity and Structure‐Activity Relationships

et al. 2022

View full text Add to dashboard Cite

show abstract

“…Without bismuth, the DTT or DTE precursors fail to inhibit thiol-mediated uptake . Their activation as cascade exchangers by oxidation to thiosulfonate 18 gave an IC 50 ≈ 50 μM and inactivity at 10 μM (Figure A). , The inhibition of SARS-CoV-2 lentivector uptake by CAX 18 was thus five times weaker compared to p-CAX 3 with IC 50 ≈ 10 μM. This comparison supported that the activation of cyclic disulfides by ring expansion with pnictogen relays is more powerful than activation by oxidation.…”

Section: Results and Discussionmentioning

confidence: 99%

“…They are also much better than the popular ebselen, 61 − 63 which inhibits also both thiol-mediated cytosolic delivery with transporter 21 and the entry of SARS-CoV-2 lentivectors, but the latter only at high IC 50 with high toxicity. 60 The availability of privileged scaffolds with and without permanent phenyl substituent on the pnictogen relay is important because they provide access to different cascade exchange chemistries ( Figures 1 C,D, 3 , and 4 ). The availability of privileged scaffolds with As(III) and Bi(III) relays is attractive because their coordination chemistry covers two extremes that provide complementary characteristics in the dynamic covalent exchange cascades related to thiol-mediated uptake ( Figure 4 C,D).…”

Section: Discussionmentioning

confidence: 99%

Pnictogen-Centered Cascade Exchangers for Thiol-Mediated Uptake: As(III)-, Sb(III)-, and Bi(III)-Expanded Cyclic Disulfides as Inhibitors of Cytosolic Delivery and Viral Entry

Lim

Kato

Besnard

et al. 2022

JACS Au

Self Cite

View full text Add to dashboard Cite

Dynamic covalent exchange cascades with cellular thiols are of interest to deliver substrates to the cytosol and to inhibit the entry of viruses. The best transporters and inhibitors known today are cyclic cascade exchangers (CAXs), producing a new exchanger with every exchange, mostly cyclic oligochalcogenides, particularly disulfides. The objective of this study was to expand the dynamic covalent chalcogen exchange cascades in thiol-mediated uptake by inserting pnictogen relays. A family of pnictogen-expanded cyclic disulfides covering As(III), Sb(III), and Bi(III) is introduced. Their ability to inhibit thiol-mediated cytosolic delivery is explored with fluorescently labeled CAXs as transporters. The promise of inhibiting viral entry is assessed with SARS-CoV-2 lentiviral vectors. Oxygen-bridged seven-membered 1,3,2-dithiabismepane rings are identified as privileged scaffolds. The same holds for six-membered 1,3,2-dithiarsinane rings made from asparagusic acid and para -aminophenylarsine oxide, which are inactive or toxic when used alone. These chemically complementary Bi(III) and As(III) cascade exchangers inhibit both thiol-mediated cytosolic delivery and SARS-CoV-2 lentivector uptake at concentrations of 10 μM or lower. Crystal structures, computational models, and exchange kinetics support that lentivector entry inhibition of the contracted dithiarsinane and the expanded dithiabismepane rings coincides with exchange cascades that occur without the release of the pnictogen relay and benefit from noncovalent pnictogen bonds. The identified leads open perspectives regarding drug delivery as well as unorthodox approaches toward dynamic covalent inhibition of cellular entry.

show abstract

“…41 The ~9-fold increase in uptake efficiency observed between AspA and CTO complexes exceeds the ~3fold difference seen with small molecule fluorophore cargoes, the greater differential perhaps resulting from the additional hydrophobic directing group provided by the CF3-functionalised aromatic unit, which is known to be more important for CTO transporters. 41 In the case of AspA and CTO, a diffuse pattern of fluorescence was observed in spinning disk confocal microscopy (SDCM) images (Figure 1d and e). In line with previous reports, this implied delivery to the cytosol rather than entrapment within endosomes following endocytosis, whereas N3 complex 18 showed a punctate fluorescence indicative of endocytosis (Figure 1c).…”

Section: Application To the Thiol-mediated Cellular Uptake Of Strepta...mentioning

confidence: 97%

“…41 Structure-activity relationships for cyclic thiosulfonate transporters and thiol-mediated uptake inhibitors revealed a strong dependence in either case on the presence of hydrophobic directing groups to target aprotic environments such as the cellular membrane and proteins, in which the proticity-dependent cascade exchange of cyclic thiosulfonates is enhanced. 41 The ~9-fold increase in uptake efficiency observed between AspA and CTO complexes exceeds the ~3fold difference seen with small molecule fluorophore cargoes, the greater differential perhaps resulting from the additional hydrophobic directing group provided by the CF3-functionalised aromatic unit, which is known to be more important for CTO transporters. 41 In the case of AspA and CTO, a diffuse pattern of fluorescence was observed in spinning disk confocal microscopy (SDCM) images (Figure 1d and e).…”

Section: Application To the Thiol-mediated Cellular Uptake Of Strepta...mentioning

confidence: 99%

Tyrosine Bioconjugation with Hypervalent Iodine

Declas

Maynard

Menin

et al. 2022

Preprint

Self Cite

View full text Add to dashboard Cite

Hypervalent iodine reagents have recently emerged as powerful tools for late-stage peptide and protein functionalization. Herein we report a tyrosine bioconjugation methodology for the introduction of hypervalent iodine onto biomolecules under physiological conditions. Tyrosine residues were engaged in a selective addition onto the alkynyl bond of ethynylbenziodoxolones (EBX), resulting in stable vinylbenziodoxolones (VBX) bioconjugates. The methodology was successfully applied to peptides and proteins and tolerated all other nucleophilic residues, with the exception of cysteine. The generated VBX were further functionalized by palladium-catalyzed cross-coupling and azide-alkyne cycloaddition reactions. The method could be successfully used to modify bioactive natural products and native streptavidin to enable thiol-mediated cellular uptake.

show abstract

Cyclic Thiosulfonates for Thiol-Mediated Uptake: Cascade Exchangers, Transporters, Inhibitors

Cited by 18 publications

References 89 publications

Anticancer Agents Derived from Cyclic Thiosulfonates: Structure‐Reactivity and Structure‐Activity Relationships

Anticancer Agents Derived from Cyclic Thiosulfonates: Structure‐Reactivity and Structure‐Activity Relationships

Pnictogen-Centered Cascade Exchangers for Thiol-Mediated Uptake: As(III)-, Sb(III)-, and Bi(III)-Expanded Cyclic Disulfides as Inhibitors of Cytosolic Delivery and Viral Entry

Tyrosine Bioconjugation with Hypervalent Iodine

Contact Info

Product

Resources

About