Your search keyword '"Cannalire, Rolando"' showing total 17 results

1. An overview on small molecules acting as broad-spectrum agents for yellow fever infection

Author

Desantis, J., Felicetti, T., Cannalire, R., Desantis, Jenny, Felicetti, Tommaso, and Cannalire, Rolando

Subjects

Antiviral Agent, NS3, antiviral drug, NS5, broad-spectrum agent, Flaviviru, Animal, Antiviral Agents, medicinal chemistry, Drug Discovery, Yellow Fever, Animals, Humans, Yellow fever virus, Yellow fever viru, Human

Abstract

Yellow fever virus (YFV) is a mosquito-borne flavivirus, endemic in 47 countries in Africa and South America, which causes febrile symptoms that can evolve in 15% of the patients to serious hemorrhagic conditions, liver injury, and multiorgan failure. Although a highly effective vaccine (YF-17D vaccine) is available, to date, no antiviral drugs have been approved for the prevention and treatment of YFV infections.This review article focuses on the description of viral targets that have been considered within YFV and flavivirus drug discovery studies and on the most relevant candidates reported so far that elicit broad-spectrum inhibition against relevant strains and mutants of YFV.Considering the growing interest on (re)emerging vector-borne viral infections, it is expected that flavivirus drug discovery will quickly deliver potential candidates for clinical evaluation. Due to similarity among flaviviral targets, several candidates identified against different flaviviruses have shown broad-spectrum activity, thus exhibiting anti-YFV activity, as well. In this regard, it would be desirable to routinely include the assessment of antiviral activity against different YFV strains. On the other hand, the development of host targeting agents are still at an initial stage and deserve further focused efforts.

Published

2022

2. Ethidium bromide exposure unmasks an antibiotic efflux system in Rhodococcus equi

Author

Donatella Pietrella, Marco Pepe, Stefano Sabatini, Rolando Cannalire, Tommaso Felicetti, Fabrizio Passamonti, Elisa Rampacci, Stefano Giovagnoli, Maria Luisa Marenzoni, Rampacci, Elisa, Marenzoni, Maria Luisa, Cannalire, Rolando, Pietrella, Donatella, Sabatini, Stefano, Giovagnoli, Stefano, Felicetti, Tommaso, Pepe, Marco, and Passamonti, Fabrizio

Subjects

0301 basic medicine, Microbiology (medical), 030106 microbiology, Microbial Sensitivity Tests, 03 medical and health sciences, chemistry.chemical_compound, 23S ribosomal RNA, Rhodococcus equi, Ethidium, Gene expression, Genotype, Anti-Bacterial Agent, Humans, Rhodococcus, Pharmacology (medical), TetR, Pharmacology, biology, Microbial Sensitivity Test, biology.organism_classification, Molecular biology, Major facilitator superfamily, Anti-Bacterial Agents, 030104 developmental biology, Infectious Diseases, chemistry, Efflux, Ethidium bromide, Human, Rhodococcu

Abstract

Background This study introduces a newly created strain (Rhodococcus equiEtBr25) by exposing R. equi ATCC 33701 to ethidium bromide (EtBr), a substrate for MDR transporters. Such an approach allowed us to investigate the resulting phenotype and genetic mechanisms underlying the efflux-mediated resistance in R. equi. Methods R. equi ATCC 33701 was stimulated with increasing concentrations of EtBr. The antimicrobial susceptibility of the parental strain and R. equiEtBr25 was investigated in the presence/absence of efflux pump inhibitors (EPIs). EtBr efflux was evaluated by EtBr-agar method and flow cytometry. The presence of efflux pump genes was determined by conventional PCR before to quantify the expression of 30 genes coding for membrane transporters by qPCR. The presence of erm(46) and mutations in 23S rRNA, and gyrA/gyrB was assessed by PCR and DNA sequencing to exclude the occurrence of resistance mechanisms other than efflux. Results R. equi EtBr25 showed an increased EtBr efflux. Against this strain, the activity of EtBr, azithromycin and ciprofloxacin was more affected than that of rifampicin and azithromycin/rifampicin combinations. Resistances were reversed by combining the antimicrobials with EPIs. Gene expression analysis detected a marked up-regulation of REQ_RS13460 encoding for a Major Facilitator Superfamily (MFS) transporter. G→A transition occurred in the transcriptional repressor tetR/acrR adjacent to REQ_RS13460. Conclusions Exposure of R. equi to EtBr unmasked an efflux-mediated defence against azithromycin and ciprofloxacin, which seemingly correlates with the overexpression of a specific MFS transporter. This genotype may mirror an insidious low-level resistance of clinically important isolates that could be countered by EPI-based therapies.

Published

2021

3. From Quinoline to Quinazoline-Based S. aureus NorA Efflux Pump Inhibitors by Coupling a Focused Scaffold Hopping Approach and a Pharmacophore Search

Author

Andrea Astolfi, Violetta Cecchetti, Tommaso Felicetti, Giuseppe Manfroni, Salvatore Vaiasicca, Oriana Tabarrini, Rolando Cannalire, Gianmarco Mangiaterra, Giada Cernicchi, Stefano Sabatini, Serena Massari, Francesca Biavasco, Nicholas Cedraro, Maria Letizia Barreca, Cedraro, Nichola, Cannalire, Rolando, Astolfi, Andrea, Mangiaterra, Gianmarco, Felicetti, Tommaso, Vaiasicca, Salvatore, Cernicchi, Giada, Massari, Serena, Manfroni, Giuseppe, Tabarrini, Oriana, Cecchetti, Violetta, Barreca, Maria Letizia, Biavasco, Francesca, and Sabatini, Stefano

Subjects

NorA efflux pump inhibitors, Staphylococcus aureus, antibiotics, medicinal chemistry, quinazoline derivatives, Quinoline, medicine.disease_cause, 01 natural sciences, Biochemistry, Chemical synthesis, chemistry.chemical_compound, antibiotic, Drug Discovery, Quinazoline, General Pharmacology, Toxicology and Pharmaceutics, Full Paper, Molecular Structure, Methicillin-Resistant Staphylococcus aureu, Microbial Sensitivity Test, Full Papers, Anti-Bacterial Agents, Quinolines, Staphylococcus aureu, Molecular Medicine, Efflux, Pharmacophore, Multidrug Resistance-Associated Proteins, Human, Methicillin-Resistant Staphylococcus aureus, Cell Survival, NorA efflux pump inhibitor, Bacterial Protein, Microbial Sensitivity Tests, quinazoline derivative, Cell Line, Structure-Activity Relationship, Antibiotic resistance, Bacterial Proteins, Anti-Bacterial Agent, medicine, Humans, Multidrug Resistance-Associated Protein, Pharmacology, Virtual screening, Dose-Response Relationship, Drug, 010405 organic chemistry, Organic Chemistry, Combinatorial chemistry, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry, Quinazolines

Abstract

Antibiotic resistance breakers, such as efflux pump inhibitors (EPIs), represent a powerful alternative to the development of new antimicrobials. Recently, by using previously described EPIs, we developed pharmacophore models able to identify inhibitors of NorA, the most studied efflux pump of Staphylococcus aureus. Herein we report the pharmacophore‐based virtual screening of a library of new potential NorA EPIs generated by an in‐silico scaffold hopping approach of the quinoline core. After chemical synthesis and biological evaluation of the best virtual hits, we found the quinazoline core as the best performing scaffold. Accordingly, we designed and synthesized a series of functionalized 2‐arylquinazolines, which were further evaluated as NorA EPIs. Four of them exhibited a strong synergism with ciprofloxacin and a good inhibition of ethidium bromide efflux on resistant S. aureus strains coupled with low cytotoxicity against human cell lines, thus highlighting a promising safety profile., Resistance breakers: By using scaffolds of approved drugs, we performed a scaffold hopping of the quinoline core coupled with a pharmacophore‐based virtual screen. The best hits were synthesized and evaluated as NorA efflux pump inhibitors (EPIs), and two 2‐arylquinazoline analogues were identified as potent NorA EPIs nontoxic toward human cells.

Published

2021

4. Targeting SARS-CoV-2 Proteases and Polymerase for COVID-19 Treatment: State of the Art and Future Opportunities

Author

Francesco Saverio Di Leva, Rolando Cannalire, Carmen Cerchia, Vincenzo Summa, Andrea R. Beccari, Cannalire, Rolando, Cerchia, Carmen, Beccari, Andrea R, Di Leva, Francesco Saverio, and Summa, Vincenzo

Subjects

Proteases, viruses, medicine.medical_treatment, Computational biology, medicine.disease_cause, Antiviral Agents, 01 natural sciences, Virus, 03 medical and health sciences, Drug Discovery, medicine, Humans, Protease Inhibitors, Pathogen, Coronavirus 3C Proteases, Polymerase, 030304 developmental biology, Coronavirus, chemistry.chemical_classification, 0303 health sciences, Protease, Molecular Structure, biology, SARS-CoV-2, Chemistry, COVID-19, virus diseases, RNA-Dependent RNA Polymerase, COVID-19 Drug Treatment, 3. Good health, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Enzyme, Perspective, biology.protein, Molecular Medicine, Identification (biology)

Abstract

The newly emerged coronavirus, called SARS-CoV-2, is the causing pathogen of pandemic COVID-19. The identification of drugs to treat COVID-19 and other coronavirus diseases is an urgent global need, thus different strategies targeting either virus or host cell are still under investigation. Direct-acting agents, targeting protease and polymerase functionalities, represent a milestone in antiviral therapy. The 3C-like (or Main) protease (3CLpro) and the nsp12 RNA-dependent RNA-polymerase (RdRp) are the best characterized SARS-CoV-2 targets and show the highest degree of conservation across coronaviruses fostering the identification of broad-spectrum inhibitors. Coronaviruses also possess a papain-like protease, another essential enzyme, still poorly characterized and not equally conserved, limiting the identification of broad-spectrum agents. Herein, we provide an exhaustive comparative analysis of SARS-CoV-2 proteases and RdRp with respect to other coronavirus homologues. Moreover, we highlight the most promising inhibitors of these proteins reported so far, including the possible strategies for their further development.

Published

2020

5. Structural Modifications of the Quinolin-4-yloxy Core to Obtain New Staphylococcus aureus NorA Inhibitors

Author

Francesca Biavasco, Andrea Astolfi, Rolando Cannalire, Giuseppe Manfroni, Maria Letizia Barreca, Gianmarco Mangiaterra, Tommaso Felicetti, Violetta Cecchetti, Oriana Tabarrini, Serena Massari, Salvatore Vaiasicca, Stefano Sabatini, Nicholas Cedraro, Cannalire, Rolando, Mangiaterra, Gianmarco, Felicetti, Tommaso, Astolfi, Andrea, Cedraro, Nichola, Massari, Serena, Manfroni, Giuseppe, Tabarrini, Oriana, Vaiasicca, Salvatore, Letizia Barreca, Maria, Cecchetti, Violetta, Biavasco, Francesca, and Sabatini, Stefano

Subjects

0301 basic medicine, THP-1 Cells, Antibiotics, Drug Resistance, Staphylococcus aureus, scaffold hopping, Pharmacology, antimicrobial resistance breakers (ARBs), medicine.disease_cause, NorA, lcsh:Chemistry, chemistry.chemical_compound, quinoline, lcsh:QH301-705.5, Spectroscopy, efflux pump inhibitors, antimicrobial resistance, pharmacophore model, virtual screening, A549 Cells, Anti-Bacterial Agents, Bacterial Proteins, Humans, Multidrug Resistance-Associated Proteins, Quinolines, Structure-Activity Relationship, Drug Resistance, Multiple, Bacterial, Chemistry, Bacterial, General Medicine, Antimicrobial, Computer Science Applications, Ciprofloxacin, Efflux, Pharmacophore, Ethidium bromide, Multiple, medicine.drug, medicine.drug_class, 030106 microbiology, Catalysis, Inorganic Chemistry, 03 medical and health sciences, Antibiotic resistance, medicine, Physical and Theoretical Chemistry, Molecular Biology, Organic Chemistry, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999

Abstract

Tackling antimicrobial resistance (AMR) represents a social responsibility aimed at renewing the antimicrobial armamentarium and identifying novel therapeutical approaches. Among the possible strategies, efflux pumps inhibition offers the advantage to contrast the resistance against all drugs which can be extruded. Efflux pump inhibitors (EPIs) are molecules devoid of any antimicrobial activity, but synergizing with pumps-substrate antibiotics. Herein, we performed an in silico scaffold hopping approach starting from quinolin-4-yloxy-based Staphylococcus aureus NorA EPIs by using previously built pharmacophore models for NorA inhibition activity. Four scaffolds were identified, synthesized, and modified with appropriate substituents to obtain new compounds, that were evaluated for their ability to inhibit NorA and synergize with the fluoroquinolone ciprofloxacin against resistant S. aureus strains. The two quinoline-4-carboxamide derivatives 3a and 3b showed the best results being synergic (4-fold MIC reduction) with ciprofloxacin at concentrations as low as 3.13 and 1.56 &micro, g/mL, respectively, which were nontoxic for human THP-1 and A549 cells. The NorA inhibition was confirmed by SA-1199B ethidium bromide efflux and checkerboard assays against the isogenic pair SA-K2378 (norA++)/SA-K1902 (norA-). These in vitro results indicate the two compounds as valuable structures for designing novel S. aureus NorA inhibitors to be used in association with fluoroquinolones.

Published

2020

6. Broad-Spectrum Flavivirus Inhibitors: a Medicinal Chemistry Point of View

Author

Giuseppe Manfroni, Violetta Cecchetti, Rolando Cannalire, Tommaso Felicetti, Felicetti, Tommaso, Manfroni, Giuseppe, Cecchetti, Violetta, and Cannalire, Rolando

Subjects

Chemistry, Pharmaceutical, viruses, Host factors, Medicinal chemistry, 01 natural sciences, Biochemistry, Flavivirus Infections, Dengue fever, Dengue, Broad spectrum, Zika, Cell Line, Tumor, flavivirus inhibitors, Drug Discovery, antiviral agents, medicine, Global health, Animals, Humans, Enzyme Inhibitors, General Pharmacology, Toxicology and Pharmaceutics, Pharmacology, biology, 010405 organic chemistry, Flavivirus, Organic Chemistry, Yellow fever, virus diseases, biology.organism_classification, medicine.disease, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Drug repositioning, Molecular Medicine, Identification (biology)

Abstract

Infections by flaviviruses, such as Dengue, West Nile, Yellow Fever and Zika viruses, represent a growing risk for global health. There are vaccines only for few flaviviruses while no effective treatments are available. Flaviviruses share epidemiological, structural, and ecologic features and often different viruses can co-infect the same host. Therefore, the identification of broad-spectrum inhibitors is highly desirable either for known flaviviruses or for viruses that likely will emerge in the future. Strategies targeting both virus and host factors have been pursued to identify broad-spectrum antiflaviviral agents. In this review, we describe the most promising and best characterized targets and their relative broad-spectrum inhibitors, identified by drug repurposing/libraries screenings and by focused medicinal chemistry campaigns. Finally, we discuss about future strategies to identify new broad-spectrum antiflavivirus agents.

Published

2020

7. Functionalized 2,1-benzothiazine 2,2-dioxides as new inhibitors of Dengue NS5 RNA-dependent RNA polymerase

Author

Giuseppe Manfroni, Andrea Astolfi, Serena Massari, Stefano Sabatini, Delia Tarantino, Violetta Cecchetti, Gilles Querat, Maria Letizia Barreca, Eloise Mastrangelo, Mario Milani, Rolando Cannalire, Oriana Tabarrini, Cannalire, Rolando, Delia, Tarantino, Andrea, Astolfi, Maria Letizia Barreca, Stefano, Sabatini, Serena, Massari, Oriana, Tabarrini, Mario, Milani, Gilles, Querat, Eloise, Mastrangelo, Giuseppe, Manfroni, and Cecchetti, Violetta

Subjects

Models, Molecular, 0301 basic medicine, viruses, 01 natural sciences, 2-dioxides, Dengue fever, chemistry.chemical_compound, RNA polymerase, Chlorocebus aethiops, Drug Discovery, Enzyme Inhibitors, Molecular Structure, General Medicine, Antivirals, Biochemistry, Molecular docking, DENV NS5 RdRp inhibitor, Cell Survival, RNA-dependent RNA polymerase, Context (language use), Microbial Sensitivity Tests, Flavivirus polymerase, Antiviral Agents, Structure-Activity Relationship, 03 medical and health sciences, Encephalitis Viruses, medicine, Animals, Humans, Antiviral, DENV NS5 RdRp inhibitors, 2,1-benzothiazine 2,2-dioxides, Vero Cells, NS5B, Pharmacology, Dose-Response Relationship, Drug, 010405 organic chemistry, Organic Chemistry, RNA, Dengue Virus, RNA-Dependent RNA Polymerase, medicine.disease, Virology, 2-dioxide, 0104 chemical sciences, 030104 developmental biology, chemistry, Viral replication, 1-benzothiazine 2, Caco-2 Cells

Abstract

Over recent years, many RNA viruses have been “re-discovered”, including life-threatening flaviviruses, such as Dengue, Zika, and several encephalitis viruses. Since no specific inhibitors are currently available to treat these infections, there is a pressing need for new therapeutics. Among the flaviviral proteins, NS5 RNA-dependent RNA polymerase (RdRp) represents a validated target being essential for viral replication and it has no human analog. To date, few NS5 RdRp inhibitor chemotypes have been reported and no inhibitors are currently in clinical development. In this context, after an in vitro screening against Dengue 3 NS5 RdRp of our in-house HCV NS5B inhibitors focused library, we found that 2,1-benzothiazine 2,2-dioxides are promising non-nucleoside inhibitors of flaviviral RdRp with compounds 8 and 10 showing IC50 of 0.6 and 0.9 μM, respectively. Preliminary structure-activity relationships indicated a key role for the C-4 benzoyl group and the importance of a properly functionalized C-6 phenoxy moiety to modulate potency. Compound 8 acts as non-competitive inhibitor and its proposed pose in the so-called N pocket of the RdRp thumb domain allowed to explain the key contribution of the benzoyl and the phenoxy moieties for the ligand binding.

Published

2018

8. Searching for Novel Inhibitors of theS. aureusNorA Efflux Pump: Synthesis and Biological Evaluation of the 3-Phenyl-1,4-benzothiazine Analogues

Author

Rolando Cannalire, Maria Letizia Barreca, Tommaso Felicetti, Maria Sole Burali, Bryan D. Schindler, Serena Massari, Glenn W. Kaatz, Giuseppe Manfroni, Violetta Cecchetti, Oriana Tabarrini, Stefano Sabatini, Felicetti, Tommaso, Cannalire, Rolando, Burali, MARIA SOLE, Massari, Serena, Manfroni, Giuseppe, Barreca, MARIA LETIZIA, Tabarrini, Oriana, Schindler, Bryan D, Sabatini, Stefano, Kaatz, Glenn W, and Cecchetti, Violetta

Subjects

0301 basic medicine, Staphylococcus aureus, Cell Survival, Thiazines, NorA efflux pump, Microbial Sensitivity Tests, Pharmacology, Benzothiazine, medicine.disease_cause, 01 natural sciences, Biochemistry, Microbiology, 03 medical and health sciences, chemistry.chemical_compound, Antibiotic resistance, Bacterial Proteins, antimicrobial resistance (AMR), Ciprofloxacin, medicinal chemistry, inhibitors, Drug Discovery, medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Active site, Antimicrobial, Anti-Bacterial Agents, 0104 chemical sciences, inhibitor, 030104 developmental biology, Drug Design, antimicrobial resistance (AMR), inhibitors, medicinal chemistry, NorA efflux pump, Staphylococcus aureus, Quinolines, biology.protein, Molecular Medicine, Efflux, Multidrug Resistance-Associated Proteins, Antibacterial activity, HeLa Cells, medicine.drug

Abstract

Bacterial resistance to antimicrobial agents has become an increasingly serious health problem in recent years. Among the strategies by which resistance can be achieved, overexpression of efflux pumps such as NorA of Staphylococcus aureus leads to a sub-lethal concentration of the antibacterial agent at the active site that in turn may predispose the organism to the development of high-level target-based resistance. With an aim to improve both the chemical stability and potency of our previously reported 3-phenyl-1,4-benzothiazine NorA inhibitors, we replaced the benzothiazine core with different nuclei. None of the new synthesized compounds showed any appreciable intrinsic antibacterial activity, and, in particular, 2-(3,4-dimethoxyphenyl)quinoline (6 c) was able to decrease, in a concentration-dependent manner, the ciprofloxacin MIC against the norA-overexpressing strains S. aureus SA-K2378 (norA++) and SA-1199B (norA+/A116E GrlA).

Published

2017

9. Discovery of potent p38α MAPK inhibitors through a funnel like workflow combining in silico screening and in vitro validation

Author

Stefano Sabatini, Maria Letizia Barreca, Mark Kudolo, Deborah Palazzotti, Stefan Laufer, Serena Massari, Andrea Astolfi, José Brea, María Isabel Loza, Giorgia Manni, Federica Cecchetti, Violetta Cecchetti, Tommaso Felicetti, Francesca Fallarino, Giuseppe Manfroni, Oriana Tabarrini, Rolando Cannalire, Astolfi, Andrea, Kudolo, Mark, Brea, Jose, Manni, Giorgia, Manfroni, Giuseppe, Palazzotti, Deborah, Sabatini, Stefano, Cecchetti, Federica, Felicetti, Tommaso, Cannalire, Rolando, Massari, Serena, Tabarrini, Oriana, Loza, Maria Isabel, Fallarino, Francesca, Cecchetti, Violetta, Laufer, Stefan A, and Barreca, Maria Letizia

Subjects

Virtual screening, Models, Molecular, Kinase, P38α mapk, In silico, 1,4-Benzodioxane, KNIME, p38α MAPK inhibitors, Pharmacophore modeling, Dose-Response Relationship, Drug, Drug Evaluation, Preclinical, Healthy Volunteers, Humans, Mitogen-Activated Protein Kinase 14, Molecular Structure, Protein Kinase Inhibitors, Structure-Activity Relationship, Drug Discovery, Protein Kinase Inhibitor, Computational biology, Dose-Response Relationship, Models, Structure–activity relationship, IC50, Pharmacology, 4-Benzodioxane, Chemistry, Drug discovery, Organic Chemistry, Molecular, General Medicine, Healthy Volunteer, In vitro, Preclinical, Drug Evaluation, p38α MAPK inhibitor, Drug, Human

Abstract

This work describes the rational discovery of novel chemotypes of p38α MAPK inhibitors using a funnel approach consisting of several computer-aided drug discovery methods and biological experiments. Among the identified hits, four compounds belonging to different chemical families showed IC50 values lower than 10 μM. In particular, the 1,4-benzodioxane derivative 5 turned out to be a potent and efficient p38α MAPK inhibitor having IC50 = 0.07 μM, and LEexp and LipE values of 0.38 and 4.8, respectively; noteworthy, the compound had also a promising kinase selectivity profile and the capability to suppress p38α MAPK effects in human immune cells. Overall, the collected findings highlight that the applied strategy has been successful in generating chemical novelty in the inhibitor kinase field, providing suitable chemical candidates for further inhibitor optimization.

Published

2019

10. Broad spectrum anti-flavivirus pyridobenzothiazolones leading to less infective virions

Author

Rolando Cannalire, Mario Milani, Giuseppe Manfroni, Géraldine Piorkowski, Serena Massari, Violetta Cecchetti, Maria Letizia Barreca, Tommaso Felicetti, Gilles Querat, Delia Tarantino, Tea Carletti, Alessandro Marcello, Stefano Sabatini, Oriana Tabarrini, Eloise Mastrangelo, Cannalire, Rolando, Tarantino, D., Piorkowski, G., Carletti, T., Massari, S., Felicetti, T., Barreca, M. L., Sabatini, S., Tabarrini, O., Marcello, A., Milani, M., Cecchetti, V., Mastrangelo, E., Manfroni, G., Querat, G., Università degli Studi di Perugia = University of Perugia (UNIPG), Sezione di Fisiologia e Biochimica delle Piante, Dipartimento di Biologia, Università degli Studi di Milano = University of Milan (UNIMI), Unité des Virus Emergents (UVE), Institut de Recherche pour le Développement (IRD)-Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratory of Molecular Virology, International Centre for Genetic Engineering and Biotechnology (ICGEB), Dipartimento di Biotecnologie e Bioscienze (Università di Milano-Bicocca), Université de Milan, Istituto di Biofisica del CNR, Emergence des Pathologies Virales (EPV), Institut de Recherche pour le Développement (IRD)-Aix Marseille Université (AMU)-Assistance Publique - Hôpitaux de Marseille (APHM)-Institut National de la Santé et de la Recherche Médicale (INSERM), Università degli Studi di Perugia (UNIPG), Università degli Studi di Milano [Milano] (UNIMI), Aix Marseille Université (AMU)-Institut de Recherche pour le Développement (IRD)-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut de Recherche pour le Développement (IRD)-Aix Marseille Université (AMU)-Assistance Publique - Hôpitaux de Marseille (APHM), and HAL AMU, Administrateur

Subjects

0301 basic medicine, Pyridines, viruses, [SDV]Life Sciences [q-bio], Flavivirus replication, Virus Replication, Dengue fever, Zika virus, Antiviral small molecules, Flavivirus inhibitor, Flavivirus inhibitors, ComputingMilieux_MISCELLANEOUS, [SDV.MP.VIR] Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Infectivity, biology, Yellow fever, Antivirals, 3. Good health, [SDV] Life Sciences [q-bio], Flavivirus, Antiviral small molecule, [SDV.MP]Life Sciences [q-bio]/Microbiology and Parasitology, Flavivirus inhibitors Antiviral small molecules Flavivirus replication Antivirals Dengue inhibitors Zika virus, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, RNA, Viral, Yellow fever virus, Dengue inhibitor, West Nile virus, Dengue inhibitors, 030106 microbiology, Antiviral Agents, Encephalitis Viruses, Tick-Borne, 03 medical and health sciences, Virology, medicine, Encephalitis Viruses, Animals, Humans, Antiviral, [SDV.MP] Life Sciences [q-bio]/Microbiology and Parasitology, Virus classification, Oxazocines, Pharmacology, Flaviviridae, Virion, Dengue Virus, Japanese encephalitis, medicine.disease, biology.organism_classification, 030104 developmental biology

Abstract

We report the design, synthesis, and biological evaluation of a class of 1H-pyrido[2,1-b][1,3]benzothiazol-1-ones originated from compound 1, previously identified as anti-flavivirus agent. Some of the new compounds showed activity in low ?M range with reasonable selectivity against Dengue 2, Yellow fever (Bolivia strain), and West Nile viruses. One of the most interesting molecules, compound 16, showed broad antiviral activity against additional flaviviruses such as Dengue 1, 3 and 4, Zika, Japanese encephalitis, several strains of Yellow fever, and tick-borne encephalitis viruses. Compound 16 did not exert any effect on alphaviruses and phleboviruses and its activity was maintained in YFV infected cells from different species. The activity of 16 appears specific for flavivirus with respect to other virus families, suggesting, but not proving, that it might be targeting a viral factor. We demonstrated that the antiviral effect of 16 is not related to reduced viral RNA synthesis or virion release. On the contrary, viral particles grown in the presence of 16 showed reduced infectivity, being unable to perform a second round of infection. The chemical class herein presented thus emerges as suitable to provide pan-flavivirus inhibitors.

Published

2019

11. 2-Phenylquinoline S. aureus NorA Efflux Pump Inhibitors : evaluation of the Importance of Methoxy Group Introduction

Author

Oriana Tabarrini, Maria Letizia Barreca, Bryan D. Schindler, Serena Massari, Glenn W. Kaatz, Gniewomir Latacz, Giuseppe Manfroni, Tommaso Felicetti, Violetta Cecchetti, Katarzyna Kieć-Kononowicz, Donatella Pietrella, Stefano Sabatini, Rolando Cannalire, Annamaria Lubelska, Felicetti, Tommaso, Cannalire, Rolando, Pietrella, Donatella, Latacz, Gniewomir, Lubelska, Annamaria, Manfroni, Giuseppe, Letizia Barreca, Maria, Massari, Serena, Tabarrini, Oriana, Kieć-Kononowicz, Katarzyna, Schindler, Bryan D., Kaatz, Glenn W., Cecchetti, Violetta, and Sabatini, Stefano

Subjects

0301 basic medicine, Drug, Models, Molecular, Staphylococcus aureus, medicine.drug_class, media_common.quotation_subject, 030106 microbiology, Antibiotics, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, medicine.disease_cause, 03 medical and health sciences, Structure-Activity Relationship, Antibiotic resistance, Bacterial Proteins, Drug Discovery, Drug Resistance, Bacterial, medicine, Humans, Tissue Distribution, Pharmaceutical sciences, media_common, Molecular Structure, Chemistry, Drug discovery, Hep G2 Cells, Staphylococcal Infections, Anti-Bacterial Agents, Ciprofloxacin, 030104 developmental biology, Quinolines, Molecular Medicine, Efflux, Multidrug Resistance-Associated Proteins, medicine.drug

Abstract

Antimicrobial resistance (AMR) represents a hot topic in drug discovery. Besides the identification of new antibiotics, the use of nonantibiotic molecules to block resistance mechanisms is a powerful alternative. Bacterial efflux pumps exert an early step in AMR development by allowing bacteria to grow at subinhibitorial drug concentrations. Thus, efflux pump inhibitors (EPIs) offer a great opportunity to fight AMR. Given our experience in developing Staphylococcus aureus NorA EPIs, in this work, starting from the 2-phenylquinoline hit 1, we planned the introduction of methoxy groups on the basis of their presence in known NorA EPIs. Among the 35 different synthesized derivatives, compounds 3b and 7d exhibited the best NorA inhibition activity by restoring at very low concentrations ciprofloxacin MICs against resistant S. aureus strains. Interestingly, both compounds displayed EPI activities at nontoxic concentrations for human cells as well as highlighted promising results by preliminary pharmacokinetic studies.

Published

2018

12. The Versatile Nature of the 6-Aminoquinolone Scaffold: Identification of Submicromolar Hepatitis C Virus NS5B Inhibitors

Author

Nunzio Iraci, Violetta Cecchetti, Amartya Basu, Giuseppe Manfroni, Stefano Sabatini, Pieter Leyssen, Rolando Cannalire, Neerja Kaushik-Basu, Oriana Tabarrini, Rupa Guhamazumder, Jan Paeshuyse, Maria Letizia Barreca, Johan Neyts, Johan Winquist, U. Helena Danielson, Dinesh Manvar, Manfroni, Giuseppe, Cannalire, Rolando, Barreca Maria, Letizia, Kaushik-Basu, Neerja, Leyssen, Pieter, Winquist, Johan, Iraci, Nunzio, Manvar, Dinesh, Paeshuyse, Jan, Guhamazumder, Rupa, Basu, Amartya, Sabatini, Stefano, Tabarrini, Oriana, Danielson U., Helena, Neyts, Johan, and Cecchetti, Violetta

Subjects

Magnetic Resonance Spectroscopy, medicine.drug_class, Hepatitis C virus, induced-fit docking, RNA-dependent RNA polymerase, Context (language use), Hepacivirus, Viral Nonstructural Proteins, medicine.disease_cause, Antiviral Agents, Article, NS5B inhibitor, Cell Line, chemistry.chemical_compound, quinolone, Drug Discovery, medicine, Humans, Enzyme Inhibitors, NS5B, IC50, chemistry.chemical_classification, Hepatitis C virus (HCV), quinolones, Drug discovery, virus diseases, Surface Plasmon Resonance, Quinolone, digestive system diseases, Molecular Docking Simulation, Enzyme, Biochemistry, chemistry, Aminoquinolines, Molecular Medicine

Abstract

We have previously reported that the 6-aminoquinolone chemotype is a privileged scaffold to obtain antibacterial and antiviral agents. Herein we describe the design, synthesis, enzymatic and cellular characterization of new 6-aminoquinolone derivatives as potent inhibitors of NS5B polymerase, an attractive and viable therapeutic target to develop safe anti-HCV agents. The 6-amino-7-[4-(2-pyridinyl)-1-piperazinyl] quinolone derivative 8 proved to be the best compound of this series, exhibiting IC50 value of 0.069 µM against NS5B polymerase and selective antiviral effect (EC50 = 3.03 µM, EC90 =13.5 µM) coupled with the absence of any cytostatic effect (CC50 >163 µM, SI >54) in Huh-9-13 cells carrying a HCV genotype 1b, as measured by MTS assay. These results indicate that the 6-aminoquinolone scaffold is worthy of further investigation in the context of NS5B-targeted HCV drug discovery programs.

Published

2013

13. A Journey around the Medicinal Chemistry of Hepatitis C Virus Inhibitors Targeting NS4B: From Target to Preclinical Drug Candidates

Author

Maria Letizia Barreca, Violetta Cecchetti, Rolando Cannalire, Giuseppe Manfroni, Cannalire, Rolando, Barreca Maria, Letizia, Manfroni, Giuseppe, and Cecchetti, Violetta

Subjects

0301 basic medicine, Drug, medicinal chemistry, antiviral drug, hepatitis C virus, viruses, Hepatitis C virus, media_common.quotation_subject, Drug Evaluation, Preclinical, Context (language use), Hepacivirus, Biology, Viral Nonstructural Proteins, medicine.disease_cause, Virus Replication, Medicinal chemistry, Antiviral Agents, 03 medical and health sciences, Structure-Activity Relationship, Drug Discovery, medicine, Global health, Humans, Enzyme Inhibitors, ADME, media_common, Hepatitis C, medicine.disease, High-Throughput Screening Assays, 030104 developmental biology, Hepatocellular carcinoma, Molecular Medicine, Identification (biology)

Abstract

Hepatitis C virus (HCV) infection is a global health burden with an estimated 130-170 million chronically infected individuals and is the cause of serious liver diseases such as cirrhosis and hepatocellular carcinoma. HCV NS4B protein represents a validated target for the identification of new drugs to be added to the combination regimen recently approved. During the last years, NS4B has thus been the object of impressive medicinal chemistry efforts, which led to the identification of promising preclinical candidates. In this context, the present review aims to discuss research published on NS4B functional inhibitors focusing the attention on hit identification, hit-to-lead optimization, ADME profile evaluation, and the structure-activity relationship data raised for each compound family taken into account. The information delivered in this review will be a useful and valuable tool for those medicinal chemists dealing with research programs focused on NS4B and aimed at the identification of innovative anti-HCV compounds.

Published

2016

14. Tumour cell population growth inhibition and cell death induction of functionalized 6-aminoquinolone derivatives

Author

Oriana Tabarrini, Gianluigi Franci, Giuseppe Manfroni, Maria Letizia Barreca, Violetta Cecchetti, Tommaso Felicetti, Lucia Altucci, A Salvato, Rolando Cannalire, Franci, G, Manfroni, Giuseppe, Cannalire, Rolando, Felicetti, Tommaso, Tabarrini, Oriana, Salvato, A, Barreca, MARIA LETIZIA, Altucci, L, Cecchetti, Violetta, Manfroni, G, Cannalire, R, Felicetti, T, Tabarrini, O, Barreca, M. L, Altucci, Lucia, and Cecchetti, V.

Subjects

Programmed cell death, Cell division, Cell, Antineoplastic Agents, Apoptosis, Breast Neoplasms, DNA Fragmentation, Biology, Cell Line, Tumor, medicine, Humans, Benzothiazoles, Naphthyridines, Cell Proliferation, 6-aminoquinolone derivatives, Cell growth, Cell Cycle, Cell Biology, General Medicine, Original Articles, Cell cycle, Blot, medicine.anatomical_structure, Biochemistry, Cell culture, Aminoquinolines, MCF-7 Cells, Female, Cell Division

Abstract

Objectives A number of previous studies has provided evidence that the well-known anti-bacterial quinolones may have potential as anti-cancer drugs. The aim of this study was to evaluate potential anti-tumour activity and selectivity of a set of 6-aminoquinolones showing some chemical similarity to naphthyridone derivative CX-5461, recently described as innovative anti-cancer agent. Materials and methods In-house quinolones 1-8 and ad hoc synthesized derivatives 9-13 were tested on Michigan Cancer Foundation-7 (MCF-7) breast cancer cells and mesenchymal progenitor (MePR2B) cell lines, analysing their effects on the cell cycle and cell death using FACS methodology. Activation of p53 was evaluated by western blotting. Results Benzyl esters 4, 5 and their amide counterparts 12, 13 drastically modulated MCF-7 cell cycles inducing DNA fragmentation and cell death, thus proving to be potential anti-tumour compounds. When assayed in non-tumour MePR2B cells, compounds 4 and 5 were cytotoxic while 12 and 13 had a certain degree of selectivity, with compound 12 emerging as the most promising. Western blot analysis revealed that severe p53-K382ac activation was promoted by benzylester 5. In contrast, amide 12 exerted only a moderate effect which was, however, comparable to that of suberoylanilide hydoxamic acid (SAHA). Conclusions Taken together, these results further reinforce evidence that quinolones have potential as anti-cancer agents. Future work will be focused on understanding compound 12 mechanisms of action, and to obtain more potent and selective compounds.

Published

2015

15. The Pyrazolobenzothiazine Core as a New Chemotype of p38 Alpha Mitogen-Activated Protein Kinase Inhibitors

Author

Silke M. Bauer, Violetta Cecchetti, Rolando Cannalire, Francesca Fallarino, Andrea Astolfi, Giuseppe Manfroni, Stefano Sabatini, José Brea, Matteo Pirro, Stefan Laufer, Marco Gargaro, Oriana Tabarrini, María Isabel Loza, Serena Massari, Maria Letizia Barreca, Carmine Vacca, Sabatini, Stefano, Manfroni, Giuseppe, Barreca Maria, Letizia, Bauer Silke, M, Gargaro, Marco, Cannalire, Rolando, Astolfi, Andrea, Brea, Jose, Vacca, Carmine, Pirro, Matteo, Massari, Serena, Tabarrini, Oriana, Loza Maria, Isabel, Fallarino, Francesca, Laufer Stefan, A, and Cecchetti, Violetta

Subjects

pyrazolobenzothiazines, MAP Kinase Signaling System, Stereochemistry, p38 mitogen-activated protein kinases, Anti-Inflammatory Agents, Alpha (ethology), anti-TNF agent, Benzothiadiazines, p38 Mitogen-Activated Protein Kinases, Biochemistry, Drug Discovery, Humans, Protein Kinase Inhibitors, IC50, Cells, Cultured, Pharmacology, Ligand efficiency, biology, Chemotype, ligand efficiency, Tumor Necrosis Factor-alpha, Kinase, Organic Chemistry, p38α MAPK inhibitors, Biological activity, anti-TNF agents, molecular docking, Mitogen-activated protein kinase, biology.protein, Molecular Medicine, p38α MAPK inhibitor

Abstract

The identification, synthesis, biological activity, and binding mode prediction of a series of pyrazolobenzothiazines as novel p38α MAPK inhibitors are reported. Some of these compounds showed interesting activity in both p38α MAPK and TNF-α release assays. Derivative 6 emerged as the most interesting compound with IC50 (p38α) = 0.457 μm, IC50 (TNF-α) = 0.5 μm and a promising kinase selectivity profile. The obtained results strongly indicate the pyrazolobenzothiazine core as a new p38α inhibitor chemotype worthy of future chemical optimization efforts directed toward identifying a new generation of anti-inflammatory agents.

Published

2015

16. New Pyrazolobenzothiazine Derivatives as Hepatitis C Virus NS5B Polymerase Palm Site I Inhibitors

Author

Jan Paeshuyse, Rolando Cannalire, Johan Neyts, Maria Letizia Barreca, Oriana Tabarrini, Giuseppe Manfroni, Stefano Sabatini, Violetta Cecchetti, Claudio Zamperini, Nunzio Iraci, Pieter Leyssen, Dinesh Manvar, Elena Dreassi, Neerja Kaushik-Basu, Amartya Basu, Maxim Chudaev, Manfroni, Giuseppe, Manvar, Dinesh, Barreca Maria, Letizia, Kaushik-Basu, Neerja, Leyssen, Pieter, Paeshuyse, Jan, Cannalire, Rolando, Iraci, Nunzio, Basu, Amartya, Chudaev, Maxim, Zamperini, Claudio, Dreassi, Elena, Sabatini, Stefano, Tabarrini, Oriana, Neyts, Johan, and Cecchetti, Violetta

Subjects

Hepatitis C Virus, In silico, Hepacivirus, Hepatitis C virus, Mutant, Viral Nonstructural Proteins, medicine.disease_cause, NS5B palm site I, Pyrazolobenzothiazine derivatives, 01 natural sciences, Antiviral Agents, Hepatitis C Viru, Article, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, medicine, Structure–activity relationship, Humans, Binding site, NS5B, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Binding Sites, biology, 010405 organic chemistry, Chemistry, NS5B polymerase, virus diseases, biology.organism_classification, Molecular biology, digestive system diseases, 3. Good health, 0104 chemical sciences, Enzyme, Biochemistry, Drug Design, Molecular Medicine, Pyrazoles

Abstract

We have previously identified the pyrazolobenzothiazine scaffold as a promising chemotype against hepatitis C virus (HCV) NS5B polymerase, a validated and promising anti-HCV target. Herein we describe the design, synthesis, enzymatic and cellular characterization of new pyrazolobenzothiazines as anti-HCV inhibitors. The binding site for a representative derivative was mapped to NS5B palm site I employing a mutant counter screen assay, thus validating our previous in silico predictions. Derivative 2b proved to be the best selective anti-HCV derivative within the new series, exhibiting IC50 value of 7.9 µM against NS5B polymerase and antiviral effect (EC50 = 8.1 µM, EC90 = 23.3 µM) coupled with the absence of any antimetabolic effect (CC50 >224 µM, SI >28) in a cell based HCV replicon system assay. Significantly, microscopic analysis showed that, unlike the parent compounds, derivative 2b did not show any significant cell morphological alterations. Furthermore, since most of the pyrazolobenzothiazines tested altered cell morphology, this undesired aspect was further investigated by exploring possible perturbation of lipid metabolism during compound treatment.

Published

2014

17. SARS-CoV-2 Entry Inhibitors: Small Molecules and Peptides Targeting Virus or Host Cells

Author

Sveva Pelliccia, Irina Stefanelli, Andrea R. Beccari, Carmen Cerchia, Vincenzo Summa, Rolando Cannalire, Cannalire, Rolando, Stefanelli, Irina, Cerchia, Carmen, R Beccari, Andrea, Pelliccia, Sveva, and Summa, Vincenzo

Subjects

0301 basic medicine, Serine Proteinase Inhibitors, viruses, Angiotensin-Converting Enzyme Inhibitors, Context (language use), Spike, Review, Biology, medicine.disease_cause, Antiviral Agents, TMPRSS2, Catalysis, Virus, Inorganic Chemistry, lcsh:Chemistry, Betacoronavirus, 03 medical and health sciences, 0302 clinical medicine, Viral entry, medicine, Animals, Humans, Physical and Theoretical Chemistry, Molecular Biology, lcsh:QH301-705.5, Spectroscopy, peptides inhibitors, Coronavirus, SARS-CoV-2, Host (biology), Organic Chemistry, small molecules inhibitors, Lipid bilayer fusion, COVID-19, General Medicine, Virus Internalization, Small molecule, Virology, Cathepsins, 3. Good health, Computer Science Applications, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, 030220 oncology & carcinogenesis, SARS-CoV-2 entry inhibitors, Spike Glycoprotein, Coronavirus

Abstract

The pandemic evolution of SARS-CoV-2 infection is forcing the scientific community to unprecedented efforts to explore all possible approaches against COVID-19. In this context, targeting virus entry is a promising antiviral strategy for controlling viral infections. The main strategies pursued to inhibit the viral entry are considering both the virus and the host factors involved in the process. Primarily, direct-acting antivirals rely on inhibition of the interaction between ACE2 and the receptor binding domain (RBD) of the Spike (S) protein or targeting the more conserved heptad repeats (HRs), involved in the membrane fusion process. The inhibition of host TMPRSS2 and cathepsins B/L may represent a complementary strategy to be investigated. In this review, we discuss the development entry inhibitors targeting the S protein, as well as the most promising host targeting strategies involving TMPRSS2 and CatB/L, which have been exploited so far against CoVs and other related viruses.