Your search keyword '"Dafne Ruggiero"' showing total 13 results

1. Identification of a New Promising BAG3 Modulator Featuring the Imidazopyridine Scaffold

Author

Dafne Ruggiero, Emis Ingenito, Eleonora Boccia, Vincenzo Vestuto, Maria Rosaria Miranda, Stefania Terracciano, Gianluigi Lauro, Giuseppe Bifulco, and Ines Bruno

Subjects

BAG3 protein, BAG domain modulator, Groebke–Blackburn–Bienaymé reaction, imidazopyridine scaffold, Surface Plasmon Resonance assay, Organic chemistry, QD241-441

Abstract

The antiapoptotic BAG3 protein plays a crucial role in cellular proteostasis and it is involved in several signalling pathways governing cell proliferation and survival. Owing to its multimodular structure, it possesses an extensive interactome including the molecular chaperone HSP70 and other specific cellular partners, which make it an eminent factor in several pathologies, particularly in cancer. Despite its potential as a therapeutic target, very few BAG3 modulators have been disclosed so far. Here we describe the identification of a promising BAG3 modulator able to bind the BAG domain of the protein featuring an imidazopyridine scaffold and obtained through the application of the Groebke–Blackburn–Bienaymé chemical synthesis procedure. The disclosed compound 10 showed a relevant cytotoxic activity, and in line with the biological profile of BAG3 disruption, it induced the activation of caspase 3 and 9.

Published

2024

2. Chemoproteomics Reveals USP5 (Ubiquitin Carboxyl-Terminal Hydrolase 5) as Promising Target of the Marine Polyketide Gracilioether A

Author

Alessandra Capuano, Gilda D’Urso, Michela Aliberti, Dafne Ruggiero, Stefania Terracciano, Carmen Festa, Alessandra Tosco, Maria Giovanna Chini, Gianluigi Lauro, Giuseppe Bifulco, and Agostino Casapullo

Subjects

proteomics, drug affinity target stability, targeted-limited proteolysis, multiple reaction monitoring, marine bioactive compound, molecular docking, Biology (General), QH301-705.5

Abstract

Mass spectrometry-based chemical proteomic approaches using limited proteolysis have become a powerful tool for the identification and analysis of the interactions between a small molecule (SM) and its protein target(s). Gracilioether A (GeA) is a polyketide isolated from a marine sponge, for which we aimed to trace the interactome using this strategy. DARTS (Drug Affinity Responsive Target Stability) and t-LiP-MS (targeted-Limited Proteolysis-Mass Spectrometry) represented the main techniques used in this study. DARTS was applied on HeLa cell lysate for the identification of the GeA target proteins, and t-LiP-MS was employed to investigate the protein’s regions involved in the binding with GeA. The results were complemented through the use of binding studies using Surface Plasmon Resonance (SPR) and in silico molecular docking experiments. Ubiquitin carboxyl-terminal hydrolase 5 (USP5) was identified as a promising target of GeA, and the interaction profile of the USP5-GeA complex was explained. USP5 is an enzyme involved in the pathway of protein metabolism through the disassembly of the polyubiquitin chains on degraded proteins into ubiquitin monomers. This activity is connected to different cellular functions concerning the maintenance of chromatin structure and receptors and the degradation of abnormal proteins and cancerogenic progression. On this basis, this structural information opens the way to following studies focused on the definition of the biological potential of Gracilioether A and the rational development of novel USP5 inhibitors based on a new structural skeleton.

Published

2024

3. Identification of 2-(thiophen-2-yl)acetic Acid-Based Lead Compound for mPGES-1 Inhibition

Author

Simone Di Micco, Stefania Terracciano, Dafne Ruggiero, Marianna Potenza, Maria C. Vaccaro, Katrin Fischer, Oliver Werz, Ines Bruno, and Giuseppe Bifulco

Subjects

fragment-based approach, Suzuki-Miyaura cross-coupling, mPGES-1 inhibitors, anti-inflammatory drugs, anticancer agents, Chemistry, QD1-999

Abstract

We report the implementation of our in silico/synthesis pipeline by targeting the glutathione-dependent enzyme mPGES-1, a valuable macromolecular target in both cancer therapy and inflammation therapy. Specifically, by using a virtual fragment screening approach of aromatic bromides, straightforwardly modifiable by the Suzuki-Miyaura reaction, we identified 3-phenylpropanoic acid and 2-(thiophen-2-yl)acetic acid to be suitable chemical platforms to develop tighter mPGES-1 inhibitors. Among these, compounds 1c and 2c showed selective inhibitory activity against mPGES-1 in the low micromolar range in accordance with molecular modeling calculations. Moreover, 1c and 2c exhibited interesting IC50 values on A549 cell lines compared to CAY10526, selected as reference compound. The most promising compound 2c induced the cycle arrest in the G0/G1 phase at 24 h of exposure, whereas at 48 and 72 h, it caused an increase of subG0/G1 fraction, suggesting an apoptosis/necrosis effect.

Published

2021

4. Repositioning of Quinazolinedione-Based Compounds on Soluble Epoxide Hydrolase (sEH) through 3D Structure-Based Pharmacophore Model-Driven Investigation

Author

Erica Gazzillo, Stefania Terracciano, Dafne Ruggiero, Marianna Potenza, Maria Giovanna Chini, Gianluigi Lauro, Katrin Fischer, Robert Klaus Hofstetter, Assunta Giordano, Oliver Werz, Ines Bruno, and Giuseppe Bifulco

Subjects

drug repositioning, soluble epoxide hydrolase, drug discovery, computational techniques, chemical synthesis, anti-inflammatory agents, Organic chemistry, QD241-441

Abstract

The development of new bioactive compounds represents one of the main purposes of the drug discovery process. Various tools can be employed to identify new drug candidates against pharmacologically relevant biological targets, and the search for new approaches and methodologies often represents a critical issue. In this context, in silico drug repositioning procedures are required even more in order to re-evaluate compounds that already showed poor biological results against a specific biological target. 3D structure-based pharmacophoric models, usually built for specific targets to accelerate the identification of new promising compounds, can be employed for drug repositioning campaigns as well. In this work, an in-house library of 190 synthesized compounds was re-evaluated using a 3D structure-based pharmacophoric model developed on soluble epoxide hydrolase (sEH). Among the analyzed compounds, a small set of quinazolinedione-based molecules, originally selected from a virtual combinatorial library and showing poor results when preliminarily investigated against heat shock protein 90 (Hsp90), was successfully repositioned against sEH, accounting the related built 3D structure-based pharmacophoric model. The promising results here obtained highlight the reliability of this computational workflow for accelerating the drug discovery/repositioning processes.

Published

2022

5. Structural Refinement of 2,4-Thiazolidinedione Derivatives as New Anticancer Agents Able to Modulate the BAG3 Protein

Author

Dafne Ruggiero, Stefania Terracciano, Gianluigi Lauro, Michela Pecoraro, Silvia Franceschelli, Giuseppe Bifulco, and Ines Bruno

Subjects

BAG3 protein, chaperones, cancer, virtual screening, 2,4-thiazolidinedione scaffold, BAG domain modulators, Organic chemistry, QD241-441

Abstract

The multidomain BAG3 protein is a member of the BAG (Bcl-2-associated athanogene) family of co-chaperones, involved in a wide range of protein–protein interactions crucial for many key cellular pathways, including autophagy, cytoskeletal dynamics, and apoptosis. Basal expression of BAG3 is elevated in several tumor cell lines, where it promotes cell survival signaling and apoptosis resistance through the interaction with many protein partners. In addition, its role as a key player of several hallmarks of cancer, such as metastasis, angiogenesis, autophagy activation, and apoptosis inhibition, has been established. Due to its involvement in malignant transformation, BAG3 has emerged as a potential and effective biological target to control multiple cancer-related signaling pathways. Recently, by using a multidisciplinary approach we reported the first synthetic BAG3 modulator interfering with its BAG domain (BD), based on a 2,4-thiazolidinedione scaffold and endowed with significant anti-proliferative activity. Here, a further in silico-driven selection of a 2,4-thiazolidinedione-based compound was performed. Thanks to a straightforward synthesis, relevant binding affinity for the BAG3BD domain, and attractive biological activities, this novel generation of compounds is of great interest for the development of further BAG3 binders, as well as for the elucidation of the biological roles of this protein in tumors. Specifically, we found compound 6 as a new BAG3 modulator with a relevant antiproliferative effect on two different cancer cell lines (IC50: A375 = 19.36 μM; HeLa = 18.67 μM).

Published

2022

6. Protein Preparation Automatic Protocol for High-Throughput Inverse Virtual Screening: Accelerating the Target Identification by Computational Methods.

Author

Simona De Vita, Gianluigi Lauro, Dafne Ruggiero, Stefania Terracciano, Raffaele Riccio, and Giuseppe Bifulco

Published

2019

7. Identification of 2,4,5-trisubstituted-2,4-dihydro-3H-1,2,4-triazol-3-one-based small molecules as selective BRD9 binders

Author

Ester Colarusso, Sara Ceccacci, Maria Chiara Monti, Erica Gazzillo, Assunta Giordano, Maria Giovanna Chini, Maria Grazia Ferraro, Marialuisa Piccolo, Dafne Ruggiero, Carlo Irace, Stefania Terracciano, Ines Bruno, Giuseppe Bifulco, Gianluigi Lauro, Colarusso, Ester, Ceccacci, Sara, Monti, Maria Chiara, Gazzillo, Erica, Giordano, Assunta, Chini, Maria Giovanna, Ferraro, Maria Grazia, Piccolo, Marialuisa, Ruggiero, Dafne, Irace, Carlo, Terracciano, Stefania, Bruno, Ine, Bifulco, Giuseppe, and Lauro, Gianluigi

Subjects

Pharmacology, Virtual screening, Organic Chemistry, Drug Discovery, Bromodomain, Epigenetic, Epigenetics, General Medicine, Bromodomains, Cancer

Abstract

Targeting bromodomain-containing protein 9 (BRD9) represents a promising strategy for the development of new agents endowed with anticancer properties. With this aim, a set of 2,4,5-trisubstituted-2,4-dihydro-3H-1,2,4-triazol-3-one-based compounds was investigated following a combined approach that relied on in silico studies, chemical synthesis, biophysical and biological evaluation of the most promising items. The protocol was initially based on molecular docking experiments, accounting a library of 1896 potentially synthesizable items tested in silico against the bromodomain of BRD9. A first set of 21 compounds (1-21) was selected and the binding on BDR9 was assessed through AlphaScreen assays. The obtained results disclosed compounds 17 and 20 able to bind BRD9 in the submicromolar range (IC50 = 0.35 ± 0.18 μM and IC50 = 0.14 ± 0.03 μM, respectively) showing a promising selectivity profile when tested against further nine bromodomains. Taking advantage of 3D structure-based pharmacophore models, additional 10 derivatives were selected in silico for the synthetic step and binding assessment, highlighting seven compounds (22, 23, 25, 26, 28, 29, 31) able to selectively bind BRD9 among different bromodomains. The ability of the identified BRD9 binders to cross artificial membranes in vitro was also assessed, revealing a very good passive permeability profile. Preliminary studies were carried out on a panel of healthy and cancer human cell lines to explore the biological behavior of the selected compounds, disclosing a moderate activity and significant selectivity profile towards leukaemia cells. These results highlighted the applicability of the reported multidisciplinary approach for accelerating the selection of promising items and for driving the chemical synthesis of novel selective BRD9 binders. Moreover, the low molecular weight of the reported 2,4,5-trisubstituted-2,4-dihydro-3H-1,2,4-triazol-3-one-based BRD9 binders suggests the possibility for further exploring the chemical space in order to obtain new analogues with improved potency.

Published

2023

8. A Combinatorial Virtual Screening Approach Driving the Synthesis of 2,4‐Thiazolidinedione‐Based Molecules as New Dual mPGES‐1/5‐LO Inhibitors

Author

Simona Pace, Vincenza Cantone, Dafne Ruggiero, Katrin Fischer, Stefania Terracciano, Oliver Werz, Giuseppe Bifulco, Ines Bruno, and Gianluigi Lauro

Subjects

Models, Molecular, Molecular model, medicine.drug_class, Anti-Inflammatory Agents, Drug Evaluation, Preclinical, Computational biology, 01 natural sciences, Biochemistry, Chemical synthesis, antitumor agents, computational chemistry, inflammation, molecular modeling, Drug Discovery, medicine, Humans, Molecule, Enzyme Inhibitors, General Pharmacology, Toxicology and Pharmaceutics, Thiazolidinedione, Prostaglandin-E Synthases, Pharmacology, chemistry.chemical_classification, Virtual screening, Arachidonate 5-Lipoxygenase, Molecular Structure, 010405 organic chemistry, Chemistry, Organic Chemistry, DUAL (cognitive architecture), 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Enzyme, A549 Cells, Molecular Medicine, Thiazolidinediones, Eicosanoid biosynthesis

Abstract

Dual inhibition of microsomal prostaglandin E2 synthase-1 (mPGES-1) and 5-lipoxygenase (5-LO), two key enzymes involved in pro-inflammatory eicosanoid biosynthesis, represents a new strategy for treating inflammatory disorders. Herein we report the discovery of 2,4-thiazolidinedione-based mPGES-1/5-LO dual inhibitors following a multidisciplinary protocol, involving virtual combinatorial screening, chemical synthesis, and validation of the biological activities for the selected compounds. Following the multicomponent-based chemical route for the decoration of the 2,4-thiazolidinedione core, a large library of virtual compounds was built (∼2.0×104 items) and submitted to virtual screening. Nine selected molecules were synthesized and biologically evaluated, disclosing among them four compounds able to reduce the activity of both enzymes in the mid- and low- micromolar range of activities. These results are of interest for further expanding the chemical diversity around the 2,4-thiazolidinedione central core, facilitating the identification of novel anti-inflammatory agents endowed with a promising and safer pharmacological profile.

Published

2020

9. Structural Refinement of 2,4-Thiazolidinedione Derivatives as New Anticancer Agents Able to Modulate the BAG3 Protein

Author

Dafne Ruggiero, Stefania Terracciano, Gianluigi Lauro, Michela Pecoraro, Silvia Franceschelli, Giuseppe Bifulco, and Ines Bruno

Subjects

Virtual screening, 2,4-thiazolidinedione scaffold, BAG domain modulators, BAG3 protein, chaperones, cancer, virtual screening, surface plasmon resonance (SPR) assay, Pharmaceutical Science, Organic chemistry, Antineoplastic Agents, Apoptosis, 4-thiazolidinedione scaffold, Analytical Chemistry, QD241-441, Neoplasms, Drug Discovery, Chaperones, Cancer, Surface plasmon resonance (SPR) assay, Adaptor Proteins, Signal Transducing, Apoptosis Regulatory Proteins, Autophagy, Cell Proliferation, Gene Expression Regulation, Neoplastic, Humans, Thiazolidinediones, Tumor Cells, Cultured, Physical and Theoretical Chemistry, Neoplastic, Cultured, Signal Transducing, Adaptor Proteins, Tumor Cells, Gene Expression Regulation, Chemistry (miscellaneous), Molecular Medicine

Abstract

The multidomain BAG3 protein is a member of the BAG (Bcl-2-associated athanogene) family of co-chaperones, involved in a wide range of protein–protein interactions crucial for many key cellular pathways, including autophagy, cytoskeletal dynamics, and apoptosis. Basal expression of BAG3 is elevated in several tumor cell lines, where it promotes cell survival signaling and apoptosis resistance through the interaction with many protein partners. In addition, its role as a key player of several hallmarks of cancer, such as metastasis, angiogenesis, autophagy activation, and apoptosis inhibition, has been established. Due to its involvement in malignant transformation, BAG3 has emerged as a potential and effective biological target to control multiple cancer-related signaling pathways. Recently, by using a multidisciplinary approach we reported the first synthetic BAG3 modulator interfering with its BAG domain (BD), based on a 2,4-thiazolidinedione scaffold and endowed with significant anti-proliferative activity. Here, a further in silico-driven selection of a 2,4-thiazolidinedione-based compound was performed. Thanks to a straightforward synthesis, relevant binding affinity for the BAG3BD domain, and attractive biological activities, this novel generation of compounds is of great interest for the development of further BAG3 binders, as well as for the elucidation of the biological roles of this protein in tumors. Specifically, we found compound 6 as a new BAG3 modulator with a relevant antiproliferative effect on two different cancer cell lines (IC50: A375 = 19.36 μM; HeLa = 18.67 μM).

Published

2021

10. Identification of 2-(thiophen-2-yl)acetic Acid-Based Lead Compound for mPGES-1 Inhibition

Author

Oliver Werz, Maria C. Vaccaro, Ines Bruno, Katrin Fischer, Giuseppe Bifulco, Dafne Ruggiero, Marianna Potenza, Stefania Terracciano, and Simone Di Micco

Subjects

Molecular model, In silico, anti-inflammatory drugs, anticancer agents, fragment-based approach, mPGES-1 inhibitors, Suzuki-Miyaura cross-coupling, 01 natural sciences, 03 medical and health sciences, Acetic acid, chemistry.chemical_compound, QD1-999, 030304 developmental biology, Original Research, A549 cell, chemistry.chemical_classification, 0303 health sciences, 010405 organic chemistry, General Chemistry, Combinatorial chemistry, 0104 chemical sciences, Chemistry, Enzyme, chemistry, Apoptosis, Lead compound, Macromolecule

Abstract

We report the implementation of our in silico/synthesis pipeline by targeting the glutathione-dependent enzyme mPGES-1, a valuable macromolecular target in both cancer therapy and inflammation therapy. Specifically, by using a virtual fragment screening approach of aromatic bromides, straightforwardly modifiable by the Suzuki-Miyaura reaction, we identified 3-phenylpropanoic acid and 2-(thiophen-2-yl)acetic acid to be suitable chemical platforms to develop tighter mPGES-1 inhibitors. Among these, compounds 1c and 2c showed selective inhibitory activity against mPGES-1 in the low micromolar range in accordance with molecular modeling calculations. Moreover, 1c and 2c exhibited interesting IC50 values on A549 cell lines compared to CAY10526, selected as reference compound. The most promising compound 2c induced the cycle arrest in the G0/G1 phase at 24 h of exposure, whereas at 48 and 72 h, it caused an increase of subG0/G1 fraction, suggesting an apoptosis/necrosis effect.

Published

2021

11. Protein Preparation Automatic Protocol for High-Throughput Inverse Virtual Screening: Accelerating the Target Identification by Computational Methods

Author

Gianluigi Lauro, Raffaele Riccio, Stefania Terracciano, Dafne Ruggiero, Simona De Vita, and Giuseppe Bifulco

Subjects

Computer science, General Chemical Engineering, Computational biology, Library and Information Sciences, 01 natural sciences, Workflow, Small Molecule Libraries, Viral Proteins, Drug Discovery, 0103 physical sciences, Animals, Humans, Databases, Protein, Throughput (business), Protocol (object-oriented programming), Virtual screening, 010304 chemical physics, Drug discovery, Proteins, General Chemistry, Small molecule, 0104 chemical sciences, Computer Science Applications, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, Identification (information), Drug Design, Protein Binding

Abstract

Structure-based virtual screening is highly used in the early stages of drug discovery to identify new putative lead compounds for a given target. However, when a small molecule elicits a biological effect, but its target is unknown, or the side effects it causes arise from its undesired interaction with unknown counterparts, the identification of its interacting targets represents an indispensable task. The computational procedure named inverse virtual screening, which relies on docking a molecule (or a small set of compounds) against panels of target proteins to select the most promising complexes, could be useful to overcome these issues. Panels can contain thousands of proteins, and they must be correctly prepared to assure the best docking performance. Therefore, the preparation of panels of proteins collected in the Protein Data Bank ( www.rcsb.org ), if manually performed, may be costly in terms of time and efforts, and this can limit the applicability of this approach in high-throughput virtual screening workflows. We here show an automated workflow to speed up panel preparation and development, and to test its performance, this protocol was initially applied to a panel of 628 viral proteins and, afterward, to a panel of transferase proteins (2789 entries) to perform a large inverse virtual screening study, testing a small set of compounds synthesized in our laboratory. Tankyrase 2 (PARP 5b) was selected as their preferred target of interaction, and the predicted binding was validated by means of surface plasmon resonance experiments. This protocol is useful for the rapid identification of the interacting target for a bioactive compound; accordingly, it facilitates the re-evaluation of the pharmacological activity of known active compounds, addressing the repurposing and the polypharmacology concepts.

Published

2019

12. Discovery of noscapine derivatives as potential β-tubulin inhibitors

Author

Stefania Terracciano, Faezeh Nemati, Maryam Mohebbi, Gianluigi Lauro, Peyman Salehi, Morteza Bararjanian, Dafne Ruggiero, Nasim Hadian, Giuseppe Bifulco, and Ines Bruno

Subjects

Noscapine, Cell Survival, Clinical Biochemistry, Triazole, Pharmaceutical Science, Huisgen reaction, 01 natural sciences, Biochemistry, Tubulin binding, Structure-Activity Relationship, chemistry.chemical_compound, Tubulin, Surface plasmon resonance, Drug Discovery, medicine, Humans, MTT assay, Viability assay, Molecular Biology, Dose-Response Relationship, Drug, Molecular Structure, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Biological activity, Combinatorial chemistry, Tubulin Modulators, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Docking (molecular), MCF-7 Cells, biology.protein, Thermodynamics, Molecular Medicine, Female, medicine.drug

Abstract

Twenty novel 1,2,3-triazole noscapine derivatives were synthesized starting from noscapine by consecutive N-demethylation, reduction of lactone ring, N-propargylation and Huisgen 1,3-dipolar cycloaddition reaction. In order to select the most promising molecules to subject to further biophysical and biological evaluation, a molecular docking analysis round was performed using noscapine as the reference compound. The molecules featuring docking predicted binding affinity better than that of noscapine were then subjected to MTT assay against MCF7 cell line. The obtained results depicted that all the selected triazole derivatives exhibited a remarkably lower cell viability compared to noscapine in the range of 20 μM in 48h. In an attempt to correlate the biological activity with the ability to bind tubulin, the surface plasmon resonance (SPR) assay was employed. Compounds 8a, 8h, 9c, 9f and 9j were able to bind tubulin with an affinity constant values in the nanomolar range and higher if compared to noscapine. Integrating computational predictions and experimental evaluation, two promising compounds (8h and 9c) were identified, whose relevant cytotoxicity was supposed to be correlated with that of tubulin binding affinity. These findings shed more lights onto structural modifications of noscapine toward the identification of more potent cytotoxic agents targeting tubulin.

Published

2020

13. Identification by Inverse Virtual Screening of magnolol-based scaffold as new tankyrase-2 inhibitors

Author

Dafne Ruggiero, Corrado Tringali, Stefania Terracciano, Maria C. Vaccaro, Nunzio Cardullo, Vera Muccilli, Luana Pulvirenti, Alessandra Russo, Simone Di Micco, Raffaele Riccio, Giuseppe Bifulco, and Ines Bruno

Subjects

0301 basic medicine, In silico, Clinical Biochemistry, Drug Evaluation, Preclinical, Pharmaceutical Science, Tankyrase-2 inhibitors, Antineoplastic Agents, Anti-cancer drugs, 01 natural sciences, Biochemistry, Lignans, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, Tumor Cells, Cultured, Humans, Surface plasmon resonance, Inverse Virtual Screening, Molecular Biology, Cell Proliferation, A549 cell, Tankyrases, Virtual screening, Natural product, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Drug Discovery3003 Pharmaceutical Science, Biphenyl Compounds, Organic Chemistry, Surface Plasmon Resonance, Tankyrase-2, Recombinant Proteins, Magnolol, 0104 chemical sciences, Bromodomain, 030104 developmental biology, chemistry, Thermodynamics, Biomimetic compounds, Molecular Medicine, 3003, Drug Screening Assays, Antitumor, Casein kinase 2, Algorithms

Abstract

The natural product magnolol (1) and a selection of its bioinspired derivatives 2-5, were investigated by Inverse Virtual Screening in order to identify putative biological targets from a panel of 308 proteins involved in cancer processes. By this in silico analysis we selected tankyrase-2 (TNKS2), casein kinase 2 (CK2) and bromodomain 9 (Brd9) as potential targets for experimental evaluations. The Surface Plasmon Resonance assay revealed that 3-5 present a good affinity for tankyrase-2, and, in particular, 3 showed an antiproliferative activity on A549 cells higher than the well-known tankyrase-2 inhibitor XAV939 used as reference compound.

Published

2018