Your search keyword '"Fiorillo, Bianca"' showing total 36 results

1. Microbial-derived bile acid reverses inflammation in IBD via GPBAR1 agonism and RORγt inverse agonism

Author

Biagioli, Michele, Di Giorgio, Cristina, Massa, Carmen, Marchianò, Silvia, Bellini, Rachele, Bordoni, Martina, Urbani, Ginevra, Roselli, Rosalinda, Lachi, Ginevra, Morretta, Elva, Piaz, Fabrizio Dal, Charlier, Bruno, Fiorillo, Bianca, Catalanotti, Bruno, Cari, Luigi, Nocentini, Giuseppe, Ricci, Patrizia, Distrutti, Eleonora, Festa, Carmen, Sepe, Valentina, Zampella, Angela, Monti, Maria Chiara, and Fiorucci, Stefano

Published

2024

2. Development of bile acid activated receptors hybrid molecules for the treatment of inflammatory and metabolic disorders

Author

Fiorucci, Stefano, Sepe, Valentina, Biagioli, Michele, Fiorillo, Bianca, Rapacciuolo, Pasquale, Distrutti, Eleonora, and Zampella, Angela

Published

2023

3. Design, Synthesis, and Pharmacological Evaluation of Dual FXR-LIFR Modulators for the Treatment of Liver Fibrosis.

Author

Rapacciuolo, Pasquale, Finamore, Claudia, Giorgio, Cristina Di, Fiorillo, Bianca, Massa, Carmen, Urbani, Ginevra, Marchianò, Silvia, Bordoni, Martina, Cassiano, Chiara, Morretta, Elva, Spinelli, Lucio, Lupia, Antonio, Moraca, Federica, Biagioli, Michele, Sepe, Valentina, Monti, Maria Chiara, Catalanotti, Bruno, Fiorucci, Stefano, and Zampella, Angela

Published

2024

4. Structural insights into the unexpected agonism of tetracyclic antidepressants at serotonin receptors 5-HT 1e R and 5-HT 1F R

Author

Zilberg, Gregory, primary, Parpounas, Alexandra K., additional, Warren, Audrey L., additional, Fiorillo, Bianca, additional, Provasi, Davide, additional, Filizola, Marta, additional, and Wacker, Daniel, additional

Published

2024

5. A microbial derived bile acid acts as GPBAR1 agonist and RORγt inverse agonist and reverses inflammation in inflammatory bowel disease

Author

Biagioli, Michele, primary, Di Giorgio, Cristina, additional, Massa, Carmen, additional, Marchianò, Silvia, additional, Bellini, Rachele, additional, Bordoni, Martina, additional, Urbani, Ginevra, additional, Roselli, Rosalinda, additional, Lachi, Ginevra, additional, Morretta, Elva, additional, Dal Piaz, Fabrizio, additional, Charlier, Bruno, additional, Fiorillo, Bianca, additional, Catalanotti, Bruno, additional, Cari, Luigi, additional, Nocentini, Giuseppe, additional, Ricci, Patrizia, additional, Distrutti, Eleonora, additional, Sepe, Valentina, additional, Zampella, Angela, additional, Monti, Maria Chiara, additional, and Fiorucci, Stefano, additional

Published

2024

6. Discovery of a AHR pelargonidin agonist that counter-regulates Ace2 expression and attenuates ACE2-SARS-CoV-2 interaction

Author

Biagioli, Michele, Marchianò, Silvia, Roselli, Rosalinda, Di Giorgio, Cristina, Bellini, Rachele, Bordoni, Martina, Gidari, Anna, Sabbatini, Samuele, Francisci, Daniela, Fiorillo, Bianca, Catalanotti, Bruno, Distrutti, Eleonora, Carino, Adriana, Zampella, Angela, Costantino, Gabriele, and Fiorucci, Stefano

Published

2021

7. Correction to “Discovery of a Novel Class of Dual GPBAR1 Agonists–RORγt Inverse Agonists for the Treatment of IL-17-Mediated Disorders”

Author

Fiorillo, Bianca, primary, Roselli, Rosalinda, additional, Finamore, Claudia, additional, Biagioli, Michele, additional, di Giorgio, Cristina, additional, Bordoni, Martina, additional, Conflitti, Paolo, additional, Marchianò, Silvia, additional, Bellini, Rachele, additional, Rapacciuolo, Pasquale, additional, Cassiano, Chiara, additional, Limongelli, Vittorio, additional, Sepe, Valentina, additional, Catalanotti, Bruno, additional, Fiorucci, Stefano, additional, and Zampella, Angela, additional

Published

2023

8. Structural Insights into the Unexpected Agonism of Tetracyclic Antidepressants at Serotonin Receptors 5-HT1eR and 5-HT1FR

Author

Zilberg, Gregory, primary, Parpounas, Alexandra K., additional, Warren, Audrey L., additional, Fiorillo, Bianca, additional, Provasi, Davide, additional, Filizola, Marta, additional, and Wacker, Daniel, additional

Published

2023

9. The TBC1D31/praja2 complex controls primary ciliogenesis through PKA‐directed OFD1 ubiquitylation

Author

Senatore, Emanuela, Chiuso, Francesco, Rinaldi, Laura, Intartaglia, Daniela, Delle Donne, Rossella, Pedone, Emilia, Catalanotti, Bruno, Pirone, Luciano, Fiorillo, Bianca, Moraca, Federica, Giamundo, Giuliana, Scala, Giovanni, Raffeiner, Andrea, Torres‐Quesada, Omar, Stefan, Eduard, Kwiatkowski, Marcel, van Pijkeren, Alienke, Morleo, Manuela, Franco, Brunella, Garbi, Corrado, Conte, Ivan, and Feliciello, Antonio

Published

2021

10. AI-assisted de novo design of selective κ-opioid receptor antagonists for the treatment of opioid addiction

Author

Salas Estrada, Letty Leslie Ann, primary, Provasi, Davide, additional, Lamim Ribeiro, Joao Marcelo, additional, Fiorillo, Bianca, additional, and Filizola, Marta, additional

Published

2023

11. Computational characterization of the binding mode and mechanism of action of tricyclic small molecules at 5-HT1E and 5-HT1F receptors

Author

Fiorillo, Bianca, primary, Zilberg, Gregory, additional, Wacker, Daniel, additional, and Filizola, Marta, additional

Published

2023

12. Discovery of a Novel Class of Dual GPBAR1 Agonists–RORγt Inverse Agonists for the Treatment of IL-17-Mediated Disorders

Author

Fiorillo, Bianca, primary, Roselli, Rosalinda, additional, Finamore, Claudia, additional, Biagioli, Michele, additional, di Giorgio, Cristina, additional, Bordoni, Martina, additional, Conflitti, Paolo, additional, Marchianò, Silvia, additional, Bellini, Rachele, additional, Rapacciuolo, Pasquale, additional, Cassiano, Chiara, additional, Limongelli, Vittorio, additional, Sepe, Valentina, additional, Catalanotti, Bruno, additional, Fiorucci, Stefano, additional, and Zampella, Angela, additional

Published

2023

13. Metadynamics simulations leveraged by statistical analyses and artificial intelligence-based tools to inform the discovery of G protein-coupled receptor ligands

Author

Salas-Estrada, Leslie, primary, Fiorillo, Bianca, additional, and Filizola, Marta, additional

Published

2022

14. Molecular Basis for Non-Covalent, Non-Competitive FAAH Inhibition

Author

Morgillo, Carmine Marco, primary, Lupia, Antonio, additional, Deplano, Alessandro, additional, Pirone, Luciano, additional, Fiorillo, Bianca, additional, Pedone, Emilia, additional, Luque, F. Javier, additional, Onnis, Valentina, additional, Moraca, Federica, additional, and Catalanotti, Bruno, additional

Published

2022

15. Combinatorial targeting of G‐protein‐coupled bile acid receptor 1 and cysteinyl leukotriene receptor 1 reveals a mechanistic role for bile acids and leukotrienes in drug‐induced liver injury

Author

Biagioli, Michele, primary, Marchianò, Silvia, additional, di Giorgio, Cristina, additional, Roselli, Rosalinda, additional, Bordoni, Martina, additional, Bellini, Rachele, additional, Fiorillo, Bianca, additional, Sepe, Valentina, additional, Catalanotti, Bruno, additional, Cassiano, Chiara, additional, Monti, Maria Chiara, additional, Distrutti, Eleonora, additional, Zampella, Angela, additional, and Fiorucci, Stefano, additional

Published

2022

16. Combinatorial targeting of G‐protein‐coupled bile acid receptor 1 and cysteinyl leukotriene receptor 1 reveals a mechanistic role for bile acids and leukotrienes in drug‐induced liver injury.

Author

Biagioli, Michele, Marchianò, Silvia, di Giorgio, Cristina, Roselli, Rosalinda, Bordoni, Martina, Bellini, Rachele, Fiorillo, Bianca, Sepe, Valentina, Catalanotti, Bruno, Cassiano, Chiara, Monti, Maria Chiara, Distrutti, Eleonora, Zampella, Angela, and Fiorucci, Stefano

Published

2023

17. Discovery of a Potent and Orally Active Dual GPBAR1/CysLT1R Modulator for the Treatment of Metabolic Fatty Liver Disease

Author

Fiorucci, Stefano, primary, Rapacciuolo, Pasquale, additional, Fiorillo, Bianca, additional, Roselli, Rosalinda, additional, Marchianò, Silvia, additional, Di Giorgio, Cristina, additional, Bordoni, Martina, additional, Bellini, Rachele, additional, Cassiano, Chiara, additional, Conflitti, Paolo, additional, Catalanotti, Bruno, additional, Limongelli, Vittorio, additional, Sepe, Valentina, additional, Biagioli, Michele, additional, and Zampella, Angela, additional

Published

2022

18. Combinatorial targeting of GPBAR1 and CYSLTR1 reveals a mechanistic role for bile acids and leukotrienes in drug induced liver injury

Author

Biagioli, Michele, Marchianò, Silvia, di Giorgio, Cristina, Roselli, Rosalinda, Bordoni, Martina, Bellini, Rachele, Fiorillo, Bianca, Sepe, Valentina, Catalanotti, Bruno, Cassiano, Chiara, Monti, Maria Chiara, Distrutti, Eleonora, Zampella, Angela, and Fiorucci, Stefano

Published

2022

19. 913 THE BILE ACIDS METABOLITES PRODUCED BY THE INTESTINAL MICROBIOTA ACT AS GPBAR1 AGONIST AND RORΓT INVERSE AGONIST DETERMINING THE COURSE OF INFLAMMATORY BOWEL DISEASE

Author

Biagioli, Michele, Giorgio, Cristina Di, Massa, Carmen, Marchianò, Silvia, Bellini, Rachele, Bordoni, Martina, Urbani, Ginevra, Lachi, Ginevra, Khan, Rana Sami Ullah, Monti, Maria Chiara, Morretta, Elva, Fiorillo, Bianca, Catalanotti, Bruno, Cari, Luigi, Nocentini, Giuseppe, Ricci, Patrizia, Distrutti, Eleonora, Zampella, Angela, and Fiorucci, Stefano

Published

2024

20. Expanding the Library of 1,2,4-Oxadiazole Derivatives: Discovery of New Farnesoid X Receptor (FXR) Antagonists/Pregnane X Receptor (PXR) Agonists.

Author

Finamore, Claudia, Festa, Carmen, Fiorillo, Bianca, Leva, Francesco Saverio Di, Roselli, Rosalinda, Marchianò, Silvia, Biagioli, Michele, Spinelli, Lucio, Fiorucci, Stefano, Limongelli, Vittorio, Zampella, Angela, and De Marino, Simona

Subjects

PREGNANE X receptor, FARNESOID X receptor, MOLECULAR docking, NITROGEN compounds

Abstract

Compounds featuring a 1,2,4-oxadiazole core have been recently identified as a new chemotype of farnesoid X receptor (FXR) antagonists. With the aim to expand this class of compounds and to understand the building blocks necessary to maintain the antagonistic activity, we describe herein the synthesis, the pharmacological evaluation, and the in vitro pharmacokinetic properties of a novel series of 1,2,4-oxadiazole derivatives decorated on the nitrogen of the piperidine ring with different N-alkyl and N-aryl side chains. In vitro pharmacological evaluation showed compounds 5 and 11 as the first examples of nonsteroidal dual FXR/Pregnane X receptor (PXR) modulators. In HepG2 cells, these compounds modulated PXR- and FXR-regulated genes, resulting in interesting leads in the treatment of inflammatory disorders. Moreover, molecular docking studies supported the experimental results, disclosing the ligand binding mode and allowing rationalization of the activities of compounds 5 and 11. [ABSTRACT FROM AUTHOR]

Published

2023

21. Allosteric communication across the μ-opioid receptor-Gi1 protein complex induced by ligands of varying efficacy

Author

Fiorillo, Bianca, Ghosh, Rikhia, Konovalov, Kirill, Provasi, Davide, and Filizola, Marta

Published

2024

22. Discovery of Bile Acid Derivatives as Potent ACE2 Activators by Virtual Screening and Essential Dynamics

Author

Fiorillo, Bianca, primary, Marchianò, Silvia, additional, Moraca, Federica, additional, Sepe, Valentina, additional, Carino, Adriana, additional, Rapacciuolo, Pasquale, additional, Biagioli, Michele, additional, Limongelli, Vittorio, additional, Zampella, Angela, additional, Catalanotti, Bruno, additional, and Fiorucci, Stefano, additional

Published

2021

23. Structural Basis for Developing Multitarget Compounds Acting on Cysteinyl Leukotriene Receptor 1 and G-Protein-Coupled Bile Acid Receptor 1

Author

Fiorillo, Bianca, primary, Sepe, Valentina, additional, Conflitti, Paolo, additional, Roselli, Rosalinda, additional, Biagioli, Michele, additional, Marchianò, Silvia, additional, De Luca, Pasquale, additional, Baronissi, Giuliana, additional, Rapacciuolo, Pasquale, additional, Cassiano, Chiara, additional, Catalanotti, Bruno, additional, Zampella, Angela, additional, Limongelli, Vittorio, additional, and Fiorucci, Stefano, additional

Published

2021

24. Discovery of a AhR flavonoid agonist that counter-regulates ACE2 expression in rodent models of inflammation and attenuates ACE2-SARS-CoV2 interaction in vitro

Author

Biagioli, Michele, primary, Marchianò, Silvia, additional, Roselli, Rosalinda, additional, Giorgio, Cristina Di, additional, Bellini, Rachele, additional, Bordoni, Martina, additional, Gidari, Anna, additional, Sabbatini, Samuele, additional, Francisci, Daniela, additional, Fiorillo, Bianca, additional, Catalanotti, Bruno, additional, Distrutti, Eleonora, additional, Carino, Adriana, additional, Zampella, Angela, additional, Costantino, Gabriele, additional, and Fiorucci, Stefano, additional

Published

2021

25. Su1416 NATURAL AND SYNTHETIC BILE ACIDS FUNCTION AS LEUKEMYA INHIBITORY FACTOR RECEPTOR (LIFR) ANTAGONISTS AND REVERT PROLIFERATION AND MIGRATION IN PANCREATIC CANCER CELL LINES

Author

Giorgio, Cristina Di, Bellini, Rachele, Lupia, Antonio, Roselli, Rosalinda, Massa, Carmen, Bordoni, Martina, Urbani, Ginevra, Marchianò, Silvia, Biagioli, Michele, Fiorillo, Bianca, Catalanotti, Bruno, Zampella, Angela, and Fiorucci, Stefano

Published

2023

26. Discovery of a Potent and Orally Active Dual GPBAR1/CysLT1R Modulator for the Treatment of Metabolic Fatty Liver Disease.

Author

Fiorucci, Stefano, Rapacciuolo, Pasquale, Fiorillo, Bianca, Roselli, Rosalinda, Marchianò, Silvia, Di Giorgio, Cristina, Bordoni, Martina, Bellini, Rachele, Cassiano, Chiara, Conflitti, Paolo, Catalanotti, Bruno, Limongelli, Vittorio, Sepe, Valentina, Biagioli, Michele, and Zampella, Angela

Subjects

FATTY liver, FARNESOID X receptor, NON-alcoholic fatty liver disease, ADIPOSE tissues, G proteins

Abstract

Nonalcoholic fatty liver disease (NAFLD) and nonalcoholic steatohepatitis (NASH) are two highly prevalent human diseases caused by excessive fat deposition in the liver. Although multiple approaches have been suggested, NAFLD/NASH remains an unmet clinical need. Here, we report the discovery of a novel class of hybrid molecules designed to function as cysteinyl leukotriene receptor 1 (CysLT1R) antagonists and G protein bile acid receptor 1 (GPBAR1/TGR5) agonists for the treatment of NAFLD/NASH. The most potent of these compounds generated by harnessing the scaffold of the previously described CystLT1R antagonists showed efficacy in reversing liver histopathology features in a preclinical model of NASH, reshaping the liver transcriptome and the lipid and energy metabolism in the liver and adipose tissues. In summary, the present study described a novel orally active dual CysLT1R antagonist/GPBAR1 agonist that effectively protects against the development of NAFLD/NASH, showing promise for further development. [ABSTRACT FROM AUTHOR]

Published

2022

27. Hijacking SARS-CoV-2/ACE2 Receptor Interaction by Natural and Semi-synthetic Steroidal Agents Acting on Functional Pockets on the Receptor Binding Domain

Author

Carino, Adriana, primary, Moraca, Federica, additional, Fiorillo, Bianca, additional, Marchianò, Silvia, additional, Sepe, Valentina, additional, Biagioli, Michele, additional, Finamore, Claudia, additional, Bozza, Silvia, additional, Francisci, Daniela, additional, Distrutti, Eleonora, additional, Catalanotti, Bruno, additional, Zampella, Angela, additional, and Fiorucci, Stefano, additional

Published

2020

28. Hijacking SARS-Cov-2/ACE2 receptor interaction by natural and semi-synthetic steroidal agents acting on functional pockets on receptor binding region

Author

Carino, Adriana, primary, Moraca, Federica, additional, Fiorillo, Bianca, additional, Marchianò, Silvia, additional, Sepe, Valentina, additional, Biagioli, Michele, additional, Finamore, Claudia, additional, Bozza, Silvia, additional, Francisci, Daniela, additional, Distrutti, Eleonora, additional, Catalanotti, Bruno, additional, Zampella, Angela, additional, and Fiorucci, Stefano, additional

Published

2020

29. Discovery of Bile Acid Derivatives as Potent ACE2 Activators by Virtual Screening and Essential Dynamics.

Author

Fiorillo, Bianca, Marchianò, Silvia, Moraca, Federica, Sepe, Valentina, Carino, Adriana, Rapacciuolo, Pasquale, Biagioli, Michele, Limongelli, Vittorio, Zampella, Angela, Catalanotti, Bruno, and Fiorucci, Stefano

Published

2022

30. Allosteric communication across the μ-opioid receptor-Gi1protein complex induced by ligands of varying efficacy

Author

Fiorillo, Bianca, Ghosh, Rikhia, Konovalov, Kirill, Provasi, Davide, and Filizola, Marta

Published

2024

31. Structural insights into the unexpected agonism of tetracyclic antidepressants at serotonin receptors 5-HT1eRand 5-HT1FR.

Author

Gregory Zilberg, Parpounas, Alexandra K., Warren, Audrey L., Fiorillo, Bianca, Provasi, Davide, Filizola, Marta, and Wacker, Daniel

Subjects

*SEROTONIN receptors, *SEROTONIN, *ANTIDEPRESSANTS, *DRUG target, *MIRTAZAPINE, *PHARMACOLOGY, *MUTAGENESIS

Abstract

Serotonin [5-hydroxytryptamine (5-HT)] acts via 13 different receptors in humans. Of these receptor subtypes, all but 5-HT1eR have confirmed roles in native tissue and are validated drug targets. Despite 5-HT1eR's therapeutic potential and plausible druggability, the mechanisms of its activation remain elusive. To illuminate 5-HT1eR's pharmacology in relation to the highly homologous 5-HT1FR, we screened a library of aminergic receptor ligands at both receptors and observe 5-HT1eR/5-HT1FR agonism by multicyclic drugs described as pan-antagonists at 5-HT receptors. Potent agonism by tetracyclic antidepressants mianserin, setiptiline, and mirtazapine suggests a mechanism for their clinically observed antimigraine properties. Using cryo-EM and mutagenesis studies, we uncover and characterize unique agonist-like binding poses of mianserin and setiptiline at 5-HT1eR distinct from similar drug scaffolds in inactive-state 5-HTR structures. Together with computational studies, our data suggest that these binding poses alongside receptor-specific allosteric coupling in 5-HT1eR and 5-HT1FR contribute to the agonist activity of these antidepressants. [ABSTRACT FROM AUTHOR]

Published

2024

32. Expanding the Library of 1,2,4-Oxadiazole Derivatives: Discovery of New Farnesoid X Receptor (FXR) Antagonists/Pregnane X Receptor (PXR) Agonists

Author

Claudia Finamore, Carmen Festa, Bianca Fiorillo, Francesco Saverio Di Leva, Rosalinda Roselli, Silvia Marchianò, Michele Biagioli, Lucio Spinelli, Stefano Fiorucci, Vittorio Limongelli, Angela Zampella, Simona De Marino, Finamore, Claudia, Festa, Carmen, Fiorillo, Bianca, Di Leva, Francesco Saverio, Roselli, Rosalinda, Marchianò, Silvia, Biagioli, Michele, Spinelli, Lucio, Fiorucci, Stefano, Limongelli, Vittorio, Zampella, Angela, and DE MARINO, Simona

Subjects

pregnane X receptor agonist, Chemistry (miscellaneous), Organic Chemistry, Drug Discovery, inflammatory disorder, 1,2,4-oxadiazole, Molecular Medicine, Pharmaceutical Science, Physical and Theoretical Chemistry, farnesoid X receptor antagonist, inflammatory disorders, Analytical Chemistry

Abstract

Compounds featuring a 1,2,4-oxadiazole core have been recently identified as a new chemotype of farnesoid X receptor (FXR) antagonists. With the aim to expand this class of compounds and to understand the building blocks necessary to maintain the antagonistic activity, we describe herein the synthesis, the pharmacological evaluation, and the in vitro pharmacokinetic properties of a novel series of 1,2,4-oxadiazole derivatives decorated on the nitrogen of the piperidine ring with different N-alkyl and N-aryl side chains. In vitro pharmacological evaluation showed compounds 5 and 11 as the first examples of nonsteroidal dual FXR/Pregnane X receptor (PXR) modulators. In HepG2 cells, these compounds modulated PXR- and FXR-regulated genes, resulting in interesting leads in the treatment of inflammatory disorders. Moreover, molecular docking studies supported the experimental results, disclosing the ligand binding mode and allowing rationalization of the activities of compounds 5 and 11.

Published

2023

33. Molecular Basis for Non-Covalent, Non-Competitive FAAH Inhibition

Author

Carmine Marco Morgillo, Antonio Lupia, Alessandro Deplano, Luciano Pirone, Bianca Fiorillo, Emilia Pedone, F. Javier Luque, Valentina Onnis, Federica Moraca, Bruno Catalanotti, Morgillo, CARMINE MARCO, Lupia, Antonio, Deplano, Alessandro, Pirone, Luciano, Fiorillo, Bianca, Pedone, Emilia, Javier Luque, F., Onnis, Valentina, Moraca, Federica, and Catalanotti, Bruno

Subjects

FAAH inhibitor, Inflammation, propanamide derivative, Polyunsaturated Alkamides, Organic Chemistry, molecular dynamics simulations, General Medicine, Molecular Dynamics Simulation, Catalysis, Computer Science Applications, Amidohydrolases, Inorganic Chemistry, Humans, Neuralgia, FAAH inhibitors, propanamide derivatives, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Endocannabinoids

Abstract

Fatty acid amide hydrolase (FAAH) plays a key role in the control of cannabinoid signaling and it represents a promising therapeutic strategy for the treatment of a wide range of diseases, including neuropathic pain and chronic inflammation. Starting from kinetics experiments carried out in our previous work for the most potent inhibitor 2-amino-3-chloropyridine amide (TPA14), we have investigated its non-competitive mechanism of action using molecular dynamics, thermodynamic integration and QM-MM/GBSA calculations. The computational studies highlighted the impact of mutations on the receptor binding pockets and elucidated the molecular basis of the non-competitive inhibition mechanism of TPA14, which prevents the endocannabinoid anandamide (AEA) from reaching its pro-active conformation. Our study provides a rationale for the design of non-competitive potent FAAH inhibitors for the treatment of neuropathic pain and chronic inflammation.

Published

2022

34. Discovery of Bile Acid Derivatives as Potent ACE2 Activators by Virtual Screening and Essential Dynamics

Author

Bianca Fiorillo, Silvia Marchianò, Federica Moraca, Valentina Sepe, Adriana Carino, Pasquale Rapacciuolo, Michele Biagioli, Vittorio Limongelli, Angela Zampella, Bruno Catalanotti, Stefano Fiorucci, Fiorillo, Bianca, Marchianò, Silvia, Moraca, Federica, Sepe, Valentina, Carino, Adriana, Rapacciuolo, Pasquale, Biagioli, Michele, Limongelli, Vittorio, Zampella, Angela, Catalanotti, Bruno, and Fiorucci, Stefano

Subjects

General Chemical Engineering, Library and Information Sciences, Antiviral Agents, 01 natural sciences, Article, Bile Acids and Salts, 03 medical and health sciences, 0103 physical sciences, Humans, Bile Acids and Salts, COVID-19, Pandemics, Protein Binding, SARS-CoV-2, Spike Glycoprotein, Coronavirus, Essential dynamics, Pandemics, 030304 developmental biology, 0303 health sciences, 010304 chemical physics, SARS-CoV-2, COVID-19, Angiotensin-Converting Enzyme 2, Antiviral Agent, General Chemistry, Spike Glycoprotein, 3. Good health, Computer Science Applications, Coronavirus, Spike Glycoprotein, Coronavirus, Angiotensin-Converting Enzyme 2, hormones, hormone substitutes, and hormone antagonists, Protein Binding

Abstract

The angiotensin-converting enzyme II (ACE2) is a key molecular player in the regulation of vessel contraction, inflammation, and reduction of oxidative stress. In addition, ACE2 has assumed a prominent role in the fight against the COVID-19 pandemic-causing virus SARS-CoV-2, as it is the very first receptor in the host of the viral spike protein. The binding of the spike protein to ACE2 triggers a cascade of events that eventually leads the virus to enter the host cell and initiate its life cycle. At the same time, SARS-CoV-2 infection downregulates ACE2 expression especially in the lung, altering the biochemical signals regulated by the enzyme and contributing to the poor clinical prognosis characterizing the late stage of the COVID-19 disease. Despite its important biological role, a very limited number of ACE2 activators are known. Here, using a combined in silico and experimental approach, we show that ursodeoxycholic acid (UDCA) derivatives work as ACE2 activators. In detail, we have identified two potent ACE2 ligands, BAR107 and BAR708, through a docking virtual screening campaign and elucidated their mechanism of action from essential dynamics of the enzyme observed during microsecond molecular dynamics calculations. The in silico results were confirmed by in vitro pharmacological assays with the newly identified compounds showing ACE2 activity comparable to that of DIZE, the most potent ACE2 activator known so far. Our work provides structural insight into ACE2/ligand-binding interaction useful for the design of compounds with therapeutic potential against SARS-CoV-2 infection, inflammation, and other ACE2-related diseases.

35. Structural Insights into the Unexpected Agonism of Tetracyclic Antidepressants at Serotonin Receptors 5-HT1eR and 5-HT1FR.

Author

Zilberg G, Parpounas AK, Warren AL, Fiorillo B, Provasi D, Filizola M, and Wacker D

Abstract

Serotonin (5-hydroxytryptamine, 5-HT) acts via 13 different receptors in humans. Of these receptor subtypes, all but 5-HT 1e R have confirmed roles in native tissue and are validated drug targets. Despite 5-HT 1e R's therapeutic potential and plausible druggability, the mechanisms of its activation remain elusive. To illuminate 5-HT 1e R's pharmacology in relation to the highly homologous 5-HT 1F R, we screened a library of aminergic receptor ligands at both receptors and observe 5-HT1e/1FR agonism by multicyclic drugs described as pan-antagonists at 5-HT receptors. Potent agonism by tetracyclic antidepressants mianserin, setiptiline, and mirtazapine suggests a mechanism for their clinically observed anti-migraine properties. Using cryoEM and mutagenesis studies, we uncover and characterize unique agonist-like binding poses of mianserin and setiptiline at 5-HT 1e R distinct from similar drug scaffolds in inactive-state 5-HTR structures. Together with computational studies, our data suggest that these binding poses alongside receptor-specific allosteric coupling in 5-HT 1e R and 5-HT 1F R contribute to the agonist activity of these antidepressants., Competing Interests: Competing interests: The authors declare that they have no competing interests.

Published

2023

36. Discovery of a Potent and Orally Active Dual GPBAR1/CysLT 1 R Modulator for the Treatment of Metabolic Fatty Liver Disease.

Author

Fiorucci S, Rapacciuolo P, Fiorillo B, Roselli R, Marchianò S, Di Giorgio C, Bordoni M, Bellini R, Cassiano C, Conflitti P, Catalanotti B, Limongelli V, Sepe V, Biagioli M, and Zampella A

Abstract

Nonalcoholic fatty liver disease (NAFLD) and nonalcoholic steatohepatitis (NASH) are two highly prevalent human diseases caused by excessive fat deposition in the liver. Although multiple approaches have been suggested, NAFLD/NASH remains an unmet clinical need. Here, we report the discovery of a novel class of hybrid molecules designed to function as cysteinyl leukotriene receptor 1 (CysLT 1 R) antagonists and G protein bile acid receptor 1 (GPBAR1/TGR5) agonists for the treatment of NAFLD/NASH. The most potent of these compounds generated by harnessing the scaffold of the previously described CystLT 1 R antagonists showed efficacy in reversing liver histopathology features in a preclinical model of NASH, reshaping the liver transcriptome and the lipid and energy metabolism in the liver and adipose tissues. In summary, the present study described a novel orally active dual CysLT 1 R antagonist/GPBAR1 agonist that effectively protects against the development of NAFLD/NASH, showing promise for further development., Competing Interests: The authors declare the following competing financial interest(s): SF and AZ have filed the Italian patent application no. 102020000019210 and the corresponding PCT application (PCT/IB 2021/057,131) in the name of PRECISION BIO-THERAPEUTICS S.R.L, a spinoff of the University of Perugia, on same the compounds described in this paper. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Fiorucci, Rapacciuolo, Fiorillo, Roselli, Marchianò, Di Giorgio, Bordoni, Bellini, Cassiano, Conflitti, Catalanotti, Limongelli, Sepe, Biagioli and Zampella.)

Published

2022