Synthesis and antiviral effect of novel fluoxetine analogues as enterovirus 2C inhibitors

Manganaro, Roberto; Zonsics, Birgit; Bauer, Lisa; Lopez, Moira Lorenzo; Donselaar, Tim; Zwaagstra, Marleen; Saporito, Fabiana; Ferla, Salvatore; Strating, Jeroen R.P.M.; Coutard, Bruno; Hurdiss, Daniel L.; Kuppeveld, Frank J. M. van; Brancale, Andrea

doi:10.1016/j.antiviral.2020.104781

Cited by 24 publications

(24 citation statements)

References 24 publications

(18 reference statements)

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“…The data suggested a worsening of patient condition, possibly due to its SSRI activity [26]. Additionally, our previous work showed that the antiviral activity of fluoxetine is unlikely to be decoupled from its SSRI activity [24,27]. This clearly demonstrates that more potent and safer molecules are needed for treatment of EV infections.…”

Section: Plos Biologymentioning

confidence: 93%

“…Subsequently, protein was expressed for 16 h at 18˚C, with shaking at 200 rpm. Further protein purification steps were performed essentially as described previously [27], with the exception that TEV protease was replaced with 3C protease (Sigma-Aldrich). The final size-exclusion chromatography step was performed at 4˚C with buffer containing 25 mM Tris (pH 8), 300 mM NaCl, and 1 mM MgCl2, using a superose 6 increase 10/ 300 column GL (GE Healthcare Life Science, Eindhoven, The Netherlands).…”

Section: Plos Biologymentioning

confidence: 99%

“…The final size-exclusion chromatography step was performed at 4˚C with buffer containing 25 mM Tris (pH 8), 300 mM NaCl, and 1 mM MgCl2, using a superose 6 increase 10/ 300 column GL (GE Healthcare Life Science, Eindhoven, The Netherlands). The binding of (S)-and (R)-fluoxetine and both 2b-enantiomers to WT CV-B3 2C, and the F190L variant, was monitored by the fluorescence-based thermal shift assay using a Roche LightCycler480, as described previously [27]. Each well of the thermal shift assay plates contained WT or F190L 2C protein (final concentration of 10 μM in 50 mM Tris, 300 mM NaCl, and 1 mM MgCl2 [pH 8]) and a SYPRO orange solution in concentrations recommended by the manufacturer, in a final volume of 25 μL.…”

Section: Plos Biologymentioning

confidence: 99%

“…We previously established that fluoxetine inhibits viral replication stereospecifically by directly binding 2C [24]. Unfortunately, the chemical moiety important for the SSRI activity is essential for the antiviral activity, and thus far these two activities could not be uncoupled [27]. This raises concerns about the therapeutic application of fluoxetine and shows that other, potent, biosafe, and broad-spectrum antiviral inhibitors are needed.…”

Section: Introductionmentioning

confidence: 99%

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Rational design of highly potent broad-spectrum enterovirus inhibitors targeting the nonstructural protein 2C

et al. 2020

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There is a great need for antiviral drugs to treat enterovirus (EV) and rhinovirus (RV) infections, which can be severe and occasionally life-threatening. The conserved nonstructural protein 2C, which is an AAA+ ATPase, is a promising target for drug development. Here, we present a structure-activity relationship study of a previously identified compound that targets the 2C protein of EV-A71 and several EV-B species members, but not poliovirus (PV) (EV-C species). This compound is structurally related to the Food and Drug Administration (FDA)-approved drug fluoxetine—which also targets 2C—but has favorable chemical properties. We identified several compounds with increased antiviral potency and broadened activity. Four compounds showed broad-spectrum EV and RV activity and inhibited contemporary strains of emerging EVs of public health concern, including EV-A71, coxsackievirus (CV)-A24v, and EV-D68. Importantly, unlike (S)-fluoxetine, these compounds are no longer neuroactive. By raising resistant EV-A71, CV-B3, and EV-D68 variants against one of these inhibitors, we identified novel 2C resistance mutations. Reverse engineering of these mutations revealed a conserved mechanism of resistance development. Resistant viruses first acquired a mutation in, or adjacent to, the α2 helix of 2C. This mutation disrupted compound binding and provided drug resistance, but this was at the cost of viral fitness. Additional mutations at distantly localized 2C residues were then acquired to increase resistance and/or to compensate for the loss of fitness. Using computational methods to identify solvent accessible tunnels near the α2 helix in the EV-A71 and PV 2C crystal structures, a conserved binding pocket of the inhibitors is proposed.

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Section: Plos Biologymentioning

confidence: 93%

Section: Plos Biologymentioning

confidence: 99%

Section: Plos Biologymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Rational design of highly potent broad-spectrum enterovirus inhibitors targeting the nonstructural protein 2C

et al. 2020

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“…Whereas the number of clinical trials cannot be extensively multiplied, libraries of “old” drugs can be screened in vitro in medium- to high-throughput assays to significantly reduce the number of candidate molecules. In addition, screening of approved drugs can also pave the way for medicinal chemistry programs 6 . Screenings of drugs to be repositioned against SARS-CoV, MERS-CoV or other viruses already showed their relevance for the selection of antivirals active at least in vitro 7 – 9 .…”

Section: Introductionmentioning

confidence: 99%

In vitro screening of a FDA approved chemical library reveals potential inhibitors of SARS-CoV-2 replication

Touret

Gilles

Barral

et al. 2020

Sci Rep

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326

274

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A novel coronavirus, named SARS-CoV-2, emerged in 2019 in China and rapidly spread worldwide. As no approved therapeutics exists to treat COVID-19, the disease associated to SARS-Cov-2, there is an urgent need to propose molecules that could quickly enter into clinics. Repurposing of approved drugs is a strategy that can bypass the time-consuming stages of drug development. In this study, we screened the PRESTWICK CHEMICAL LIBRARY composed of 1,520 approved drugs in an infected cell-based assay. The robustness of the screen was assessed by the identification of drugs that already demonstrated in vitro antiviral effect against SARS-CoV-2. Thereby, 90 compounds were identified as positive hits from the screen and were grouped according to their chemical composition and their known therapeutic effect. Then EC50 and CC50 were determined for a subset of 15 compounds from a panel of 23 selected drugs covering the different groups. Eleven compounds such as macrolides antibiotics, proton pump inhibitors, antiarrhythmic agents or CNS drugs emerged showing antiviral potency with 2 < EC50 ≤ 20 µM. By providing new information on molecules inhibiting SARS-CoV-2 replication in vitro, this study provides information for the selection of drugs to be further validated in vivo. Disclaimer: This study corresponds to the early stages of antiviral development and the results do not support by themselves the use of the selected drugs to treat SARS-CoV-2 infection.

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Combating coxsackievirus B infections

Nekoua

Mercier

Vergez

et al. 2022

Reviews in Medical Virology

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Coxsackieviruses B (CVB) are small, non‐enveloped, single‐stranded RNA viruses belonging to the Enterovirus genus of the Picornaviridae family. They are common worldwide and cause a wide variety of human diseases ranging from those having relatively mild symptoms to severe acute and chronic pathologies such as cardiomyopathy and type 1 diabetes. The development of safe and effective strategies to combat these viruses remains a challenge. The present review outlines current approaches to control CVB infections and associated diseases. Various drugs targeting viral or host proteins involved in viral replication as well as vaccines have been developed and shown potential to prevent or combat CVB infections in vitro and in vivo in animal models. Repurposed drugs and alternative strategies targeting miRNAs or based on plant extracts and probiotics and their derivatives have also shown antiviral effects against CVB. In addition, clinical trials with vaccines and drugs are underway and offer hope for the prevention or treatment of CVB‐induced diseases.

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Synthesis and antiviral effect of novel fluoxetine analogues as enterovirus 2C inhibitors

Cited by 24 publications

References 24 publications

Rational design of highly potent broad-spectrum enterovirus inhibitors targeting the nonstructural protein 2C

Rational design of highly potent broad-spectrum enterovirus inhibitors targeting the nonstructural protein 2C

In vitro screening of a FDA approved chemical library reveals potential inhibitors of SARS-CoV-2 replication

Combating coxsackievirus B infections

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