Your search keyword '"Marinelli, L"' showing total 42 results

1. Challenging clinically unresponsive medullary thyroid cancer: Discovery and pharmacological activity of novel RET inhibitors.

Author

La Pietra V, Sartini S, Botta L, Antonelli A, Ferrari SM, Fallahi P, Moriconi A, Coviello V, Quattrini L, Ke YY, Hsing-Pang H, Da Settimo F, Novellino E, La Motta C, and Marinelli L

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Carcinoma, Neuroendocrine metabolism, Cell Line, Tumor, Cell Proliferation drug effects, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Humans, Molecular Structure, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors chemistry, Proto-Oncogene Proteins c-ret genetics, Proto-Oncogene Proteins c-ret metabolism, Structure-Activity Relationship, Thyroid Gland metabolism, Thyroid Gland pathology, Thyroid Neoplasms metabolism, Antineoplastic Agents pharmacology, Carcinoma, Neuroendocrine drug therapy, Drug Discovery, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-ret antagonists & inhibitors, Thyroid Gland drug effects, Thyroid Neoplasms drug therapy

Abstract

It is now known that "gain of function" mutations of RET (REarranged during Transfection) kinase are specific and key oncogenic events in the onset of thyroid gland cancers such as the Medullary Thyroid Carcinoma (MTC). Although a number of RET inhibitors exist and are capable of inhibiting RET variants, in which mutations are outside the enzyme active site, the majority becomes dramatically ineffective when mutations are within the protein active site (V804L and V804M). Pursuing a receptor-based virtual screening against the kinase domain of RET, we found that compound 5 is able to inhibit efficiently both wild type and V804L mutant RET. Compound 5 was able to significantly reduce proliferation of both commercially available TT cell lines and surgical thyroid tissues obtained from patients with MTC and displayed a suitable drug-like profile, thus standing out as a promising candidate for further development towards the treatment of clinically unresponsive MTC., (Copyright © 2018 Elsevier Masson SAS. All rights reserved.)

Published

2018

2. Beyond radio-displacement techniques for identification of CB1 ligands: the first application of a fluorescence-quenching assay.

Author

Bruno A, Lembo F, Novellino E, Stornaiuolo M, and Marinelli L

Subjects

Allosteric Regulation, Animals, Cell Line, Cell Membrane metabolism, Humans, Inhibitory Concentration 50, Kinetics, Models, Molecular, Protein Binding, Protein Conformation, Rats, Receptor, Cannabinoid, CB1 genetics, Spectrometry, Fluorescence methods, Drug Discovery methods, Ligands, Receptor, Cannabinoid, CB1 chemistry, Receptor, Cannabinoid, CB1 metabolism

Abstract

Cannabinoid type 1 Receptor (CB1) belongs to the GPCR family and it has been targeted, so far, for the discovery of drugs aimed at the treatment of neuropathic pain, nausea, vomit, and food intake disorders. Here, we present the development of the first fluorescent assay enabling the measurement of kinetic binding constants for CB1 orthosteric ligands. The assay is based on the use of T1117, a fluorescent analogue of AM251. We prove that T1117 binds endogenous and recombinant CB1 receptors with nanomolar affinity. Moreover, T1117 binding to CB1 is sensitive to the allosteric ligand ORG27569 and thus it is applicable to the discovery of new allosteric drugs. The herein presented assay constitutes a sustainable valid alternative to the expensive and environmental impacting radiodisplacement techniques and paves the way for an easy, fast and cheap high-throughput drug screening toward CB1 for identification of new orthosteric and allosteric modulators.

Published

2014

3. Phenylpyrazolo[1,5-a]quinazolin-5(4H)-one: a suitable scaffold for the development of noncamptothecin topoisomerase I (Top1) inhibitors.

Author

Taliani S, Pugliesi I, Barresi E, Salerno S, Marchand C, Agama K, Simorini F, La Motta C, Marini AM, Di Leva FS, Marinelli L, Cosconati S, Novellino E, Pommier Y, Di Santo R, and Da Settimo F

Subjects

DNA Topoisomerases, Type I chemistry, Heterocyclic Compounds, 3-Ring chemistry, Heterocyclic Compounds, 3-Ring metabolism, Humans, Molecular Docking Simulation, Protein Conformation, Pyrroles metabolism, Quinazolines metabolism, Topoisomerase I Inhibitors metabolism, DNA Topoisomerases, Type I metabolism, Drug Discovery, Heterocyclic Compounds, 3-Ring pharmacology, Pyrroles chemistry, Pyrroles pharmacology, Quinazolines chemistry, Quinazolines pharmacology, Topoisomerase I Inhibitors chemistry, Topoisomerase I Inhibitors pharmacology

Abstract

In search for a novel chemotype to develop topoisomerase I (Top1) inhibitors, the pyrazolo[1,5-a]quinazoline nucleus, structurally related to the indenoisoquinoline system precursor of well-known Top1 poisons, was variously decorated (i.e., a substituted phenyl ring at 2- or 3-position, a protonable side chain at 4- or 5-position), affording a number of Top1 inhibitors with cleavage patterns common to CPT and MJ-III-65. SARs data were rationalized by means of an advanced docking protocol.

Published

2013

4. State-of-the-art methodologies for the discovery and characterization of DNA G-quadruplex binders.

Author

Pagano B, Cosconati S, Gabelica V, Petraccone L, De Tito S, Marinelli L, La Pietra V, di Leva FS, Lauri I, Trotta R, Novellino E, Giancola C, and Randazzo A

Subjects

Calorimetry, Circular Dichroism, Fluorescence Resonance Energy Transfer, Humans, Ligands, Magnetic Resonance Spectroscopy, Spectrometry, Fluorescence, Spectrometry, Mass, Electrospray Ionization, DNA chemistry, Drug Discovery, G-Quadruplexes

Abstract

Nowadays, the molecular basis of interaction between low molecular weight compounds and biological macromolecules is the subject of numerous investigations aimed at the rational design of molecules with specific therapeutic applications. In the last decades, it has been demonstrated that DNA quadruplexes play a critical role in several biological processes both at telomeric and gene promoting levels thus providing a great stride in the discovery of ligands able to interact with such a biologically relevant DNA conformation. So far, a number of experimental and computational approaches have been successfully employed in order to identify new ligands and to characterize their binding to the DNA. The main focus of this review is the description of these methodologies, placing a particular emphasis on computational methods, isothermal titration calorimetry (ITC), mass spectrometry (MS), nuclear magnetic resonance (NMR), circular dichroism (CD) and fluorescence spectroscopies.

Published

2012

5. Halting the Spread of Herpes Simplex Virus-1: The Discovery of an Effective Dual αvβ6/αvβ8 Integrin Ligand

Author

Stefano Tomassi, Francesco Saverio Di Leva, Giovanna Musco, Salvatore Di Maro, Horst Kessler, Michael Weinmüller, Tatiana Gianni, Barbara Romano, Jussara Amato, Giacomo Quilici, Ettore Novellino, Angelo A. Izzo, Andrea Vannini, Florian Reichart, Vincenzo Maria D'Amore, Luciana Marinelli, Tomassi, S., D'Amore, V. M., Di Leva, F. S., Vannini, A., Quilici, G., Weinmuller, M., Reichart, F., Amato, J., Romano, B., Izzo, A. A., Di Maro, S., Novellino, E., Musco, G., Gianni, T., Kessler, H., Marinelli, L., Tomassi S., D'Amore V.M., Di Leva F.S., Vannini A., Quilici G., Weinmuller M., Reichart F., Amato J., Romano B., Izzo A.A., Di Maro S., Novellino E., Musco G., Gianni T., Kessler H., and Marinelli L.

Subjects

Integrins, Small interfering RNA, Molecular model, Integrin, Peptide, Herpesvirus 1, Human, Integrin ligand, Ligands, medicine.disease_cause, Peptides, Cyclic, 01 natural sciences, Article, 03 medical and health sciences, HEK293 Cell, Antigens, Neoplasm, Drug Discovery, medicine, Humans, 030304 developmental biology, chemistry.chemical_classification, Infectivity, 0303 health sciences, Binding Sites, biology, Binding Site, Virus Internalization, Combined approach, ddc, 0104 chemical sciences, Cell biology, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, HEK293 Cells, Herpes simplex virus, chemistry, biology.protein, Oligopeptide, Molecular Medicine, Oligopeptides, Human, Protein Binding

Abstract

Over recent years, αvβ6 and αvβ8 Arg-Gly-Asp (RGD) integrins have risen to prominence as interchangeable co-receptors for the cellular entry of herpes simplex virus-1 (HSV-1). In fact, the employment of subtype-specific integrin-neutralizing antibodies or gene-silencing siRNAs has emerged as a valuable strategy for impairing HSV infectivity. Here, we shift the focus to a more affordable pharmaceutical approach based on small RGD-containing cyclic pentapeptides. Starting from our recently developed αvβ6-preferential peptide [RGD-Chg-E]-CONH2 (1), a small library of N-methylated derivatives (2–6) was indeed synthesized in the attempt to increase its affinity toward αvβ8. Among the novel compounds, [RGD-Chg-(NMe)E]-CONH2 (6) turned out to be a potent αvβ6/αvβ8 binder and a promising inhibitor of HSV entry through an integrin-dependent mechanism. Furthermore, the renewed selectivity profile of 6 was fully rationalized by a NMR/molecular modeling combined approach, providing novel valuable hints for the design of RGD integrin ligands with the desired specificity profile.

Published

2021

6. Protein Flexibility in Virtual Screening: The BACE-1 Case Study

Author

Vincenza Andrisano, Valeria La Pietra, David S. Goodsell, Angela De Simone, Sandro Cosconati, Luciana Marinelli, Francesca Mancini, Arthur J. Olson, Ettore Novellino, Francesco Saverio Di Leva, S., Cosconati, Marinelli, Luciana, Di Leva, Francesco Saverio, LA PIETRA, Valeria, A., De Simone, F., Mancini, V., Andrisano, Novellino, Ettore, D. S., Goodsell, A. J., Olson, Cosconati S., Marinelli L., Di Leva F.S., La Pietra V., De Simone A., Mancini F., Andrisano V., Novellino E., Goodsell D.S., Olson A.J., Cosconati, Sandro, Marinelli, L, Di Leva, F, La Pietra, V, De Simone, A, Mancini, F, Andrisano, V, Novellino, E, Goodsell, D, and Olson, A. J.

Subjects

STRUCTURE-BASED DESIGN, FLEXIBLE SIDE-CHAINS, MEMAPSIN-2 BETA-SECRETASE, APP CLEAVING ENZYME, DRUG DESIGN, MOLECULAR RECOGNITION, ALZHEIMERS-DISEASE, LIGAND DOCKING, SOFT DOCKING, ACTIVE-SITE, Protein Conformation, General Chemical Engineering, Library and Information Sciences, Machine learning, computer.software_genre, Crystallography, X-Ray, Ligands, Molecular Docking Simulation, Article, Antiparkinson Agents, User-Computer Interface, Alzheimer Disease, High-Throughput Screening Assays, Drug Discovery, Fluorescence Resonance Energy Transfer, Aspartic Acid Endopeptidases, Humans, Simulation, Virtual screening, Binding Sites, Chemistry, business.industry, Drug discovery, General Chemistry, Grid, Computer Science Applications, Weighting, Thermodynamics, Artificial intelligence, Amyloid Precursor Protein Secretases, business, computer, Algorithms, Databases, Chemical, Protein Binding

Abstract

Simulating protein flexibility is a major issue in the docking-based drug-design process for which a single methodological solution does not exist. In our search of new anti-Alzheimer ligands, we were faced with the challenge of including receptor plasticity in a virtual screening campaign aimed at finding new β-secretase inhibitors. To this aim, we incorporated protein flexibility in our simulations by using an ensemble of static X-ray enzyme structures to screen the National Cancer Institute database. A unified description of the protein motion was also generated by computing and combining a set of grid maps using an energy weighting scheme. Such a description was used in an energy-weighted virtual screening experiment on the same molecular database. Assessment of the enrichment factors from these two virtual screening approaches demonstrated comparable predictive powers, with the energy-weighted method being faster than the ensemble method. The in vitro evaluation demonstrated that out of the 32 tested ligands, 17 featured the predicted enzyme inhibiting property. Such an impressive success rate (53.1%) demonstrates the enhanced power of the two methodologies and suggests that energy-weighted virtual screening is a more than valid alternative to ensemble virtual screening given its reduced computational demands and comparable performance. © 2012 American Chemical Society.

Published

2012

7. Novel Peptide-Based PET Probe for Non-invasive Imaging of C-X-C Chemokine Receptor Type 4 (CXCR4) in Tumors

Author

Paolo Gaballo, Stefania Scala, Stefano Tomassi, Ettore Novellino, Caterina Ieranò, Sara Santagata, Secondo Lastoria, Crescenzo D'Alterio, Luigi Portella, Salvatore Di Maro, Deborah Sementa, Margret Schottelius, Daria Di Martino, Antonio Luciano, Antonio Barbieri, Luciana Marinelli, Michela Aurilio, Anna Maria Trotta, Trotta, A. M., Aurilio, M., D'Alterio, C., Ierano, C., Di Martino, D., Barbieri, A., Luciano, A., Gaballo, P., Santagata, S., Portella, L., Tomassi, S., Marinelli, L., Sementa, D., Novellino, E., Lastoria, S., Scala, S., Schottelius, M., and Di Maro, S.

Subjects

Biodistribution, Receptors, CXCR4, Mice, Nude, Context (language use), Peptide, Gallium Radioisotopes, Mice, SCID, 01 natural sciences, 03 medical and health sciences, chemistry.chemical_compound, Heterocyclic Compounds, 1-Ring, Mice, In vivo, Neoplasms, Drug Discovery, medicine, DOTA, Animals, Humans, Tissue Distribution, Receptor, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Gallium Radioisotope, CXCR4 antagonist, medicine.diagnostic_test, Animal, Chemistry, 0104 chemical sciences, 3. Good health, 010404 medicinal & biomolecular chemistry, Positron emission tomography, Positron-Emission Tomography, Cancer research, Neoplasm, Molecular Medicine, Female, Peptides, Human

Abstract

The recently reported CXCR4 antagonist 3 (Ac-Arg-Ala-[DCys-Arg-2Nal-His-Pen]-CO2H) was investigated as a molecular scaffold for a CXCR4-targeted positron emission tomography (PET) tracer. Toward this end, 3 was functionalized with 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA) and 1,4,7-triazacyclononanetriacetic acid (NOTA). On the basis of convincing affinity data, both tracers, [68Ga]NOTA analogue ([68Ga]-5) and [68Ga]DOTA analogue ([68Ga]-4), were evaluated for PET imaging in "in vivo" models of CHO-hCXCR4 and Daudi lymphoma cells. PET imaging and biodistribution studies revealed higher CXCR4-specific tumor uptake and high tumor/background ratios for the [68Ga]NOTA analogue ([68Ga]-5) than for the [68Ga]DOTA analogue ([68Ga]-4) in both in vivo models. Moreover, [68Ga]-4 and [68Ga]-5 displayed rapid clearance and very low levels of accumulation in all nontarget tissues but the kidney. Although the high tumor/background ratios observed in the mouse xenograft model could partially derive from the hCXCR4 selectivity of [68Ga]-5, our results encourage its translation into a clinical context as a novel peptide-based tracer for imaging of CXCR4-overexpressing tumors.

Published

2021

8. Interfering with the Tumor-Immune Interface: Making Way for Triazine-Based Small Molecules as Novel PD-L1 Inhibitors

Author

Linda Cerofolini, Gerolama Condorelli, Giovanna Polcaro, Daniela Arosio, Vincenzo Maria D'Amore, Stefano Pepe, Riccardo Scaglia, Marco Fragai, E. Novellino, Giulia Assoni, Luciana Marinelli, Pasquale Russomanno, Stefano Giuntini, Jussara Amato, Diego Brancaccio, Francesco Sabbatino, Marianna Falzoni, Valeria La Pietra, Greta Donati, Paolo Orlando, Pierfausto Seneci, Cristina Quintavalle, Martina Pedrini, Bruno Pagano, Russomanno, P., Assoni, G., Amato, J., D'Amore, V. M., Scaglia, R., Brancaccio, D., Pedrini, M., Polcaro, G., La Pietra, V., Orlando, P., Falzoni, M., Cerofolini, L., Giuntini, S., Fragai, M., Pagano, B., Donati, G., Novellino, E., Quintavalle, C., Condorelli, G., Sabbatino, F., Seneci, P., Arosio, D., Pepe, S., and Marinelli, L.

Subjects

Models, Molecular, medicine.drug_class, Immune Checkpoint Inhibitor, B7-H1 Antigen, Calorimetry, Differential Scanning, Cell Line, Tumor, Coculture Techniques, Humans, Immune Checkpoint Inhibitors, Neoplasms, Small Molecule Libraries, Structure-Activity Relationship, Triazines, Calorimetry, Monoclonal antibody, Differential Scanning, Peripheral blood mononuclear cell, PD-1/PD-L1, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Immune system, Small Molecule Librarie, Models, PD-L1, Drug Discovery, medicine, Cytotoxicity, Coculture Technique, immune checkpoint, 030304 developmental biology, 0303 health sciences, Tumor, biology, Chemistry, Molecular, Small molecule, 3. Good health, Triazine, Apoptosis, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, biology.protein, Molecular Medicine, Neoplasm, Human

Abstract

The inhibition of the PD-1/PD-L1 axis by monoclonal antibodies has achieved remarkable success in treating a growing number of cancers. However, a novel class of small organic molecules, with BMS-202 (1) as the lead, is emerging as direct PD-L1 inhibitors. Herein, we report a series of 2,4,6-tri- and 2,4-disubstituted 1,3,5-triazines, which were synthesized and assayed for their PD-L1 binding by NMR and homogeneous time-resolved fluorescence. Among them, compound 10 demonstrated to strongly bind with the PD-L1 protein and challenged it in a co-culture of PD-L1 expressing cancer cells (PC9 and HCC827 cells) and peripheral blood mononuclear cells enhanced antitumor immune activity of the latter. Compound 10 significantly increased interferon γ release and apoptotic induction of cancer cells, with low cytotoxicity in healthy cells when compared to 1, thus paving the way for subsequent preclinical optimization and medical applications.

Published

2021

9. Selective Targeting of Integrin αvβ8 by a Highly Active Cyclic Peptide

Author

Markus Schwaiger, Katja Steiger, Luciana Marinelli, Markus Nieberler, Johannes Notni, Horst Kessler, Salvatore Di Maro, Michael Weinmüller, Francesco Saverio Di Leva, Oleg V. Maltsev, Hans-Jürgen Wester, Ute Reuning, Alexander Wurzer, Udaya Kiran Marelli, Roswitha Beck, Andreas F. B. Räder, Florian Reichart, Tobias G. Kapp, Reichart, Florian, Maltsev, Oleg V, Kapp, Tobias G, Räder, Andreas F B, Weinmüller, Michael, Marelli, Udaya Kiran, Notni, Johanne, Wurzer, Alexander, Beck, Roswitha, Wester, Hans-Jürgen, Steiger, Katja, Di Maro, Salvatore, Di Leva, Francesco Saverio, Marinelli, Luciana, Nieberler, Marku, Reuning, Ute, Schwaiger, Marku, Kessler, Horst, Reichart, F., Maltsev, O. V., Kapp, T. G., Rader, A. F. B., Weinmuller, M., Marelli, U. K., Notni, J., Wurzer, A., Beck, R., Wester, H. -J., Steiger, K., Di Maro, S., Di Leva, F. S., Marinelli, L., Nieberler, M., Reuning, U., Schwaiger, M., and Kessler, H.

Subjects

Boron Compounds, Integrins, Integrin, Medizin, Gallium Radioisotopes, Peptide, Molecular Dynamics Simulation, Peptides, Cyclic, Proof of Concept Study, 01 natural sciences, 03 medical and health sciences, Cell Line, Tumor, Drug Discovery, Humans, Cancer, Integrins, Peptide synthesis, Medicinal Chemistry, Molecular Imaging, Receptor, Fluorescent Dyes, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, biology, Chemistry, Ligand (biochemistry), Highly selective, Orders of magnitude (mass), Cyclic peptide, 0104 chemical sciences, Cell biology, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, Microscopy, Fluorescence, Drug Design, biology.protein, Molecular Medicine, Radiopharmaceuticals

Abstract

Integrins play important roles in physiological and pathophysiological processes. Among the RGD-recognizing integrin subtypes, the αvβ8 receptor is emerging as an attractive target because of its involvement in various illnesses, such as autoimmune diseases, viral infections, and cancer. However, its functions have, so far, not been investigated in living subjects mainly because of the lack of a selective αvβ8 ligand. Here, we report the design and potential medical applications of a cyclic octapeptide as the first highly selective small-molecule ligand for αvβ8. Remarkably, this compound displays low nanomolar αvβ8 binding affinity and a strong discriminating power of at least 2 orders of magnitude versus other RGD-recognizing integrins. Peptide functionalization with fluorescent or radioactive labels enables the selective imaging of αvβ8-positive cells and tissues. This new probe will pave the way for detailed characterization of the distinct (patho)physiological role of this relatively unexplored integrin, providing a basis to fully exploit the potential of αvβ8 as a target for molecular diagnostics and personalized therapy regimens.

Published

2019

10. Enriching the Arsenal of Pharmacological Tools against MICAL2

Author

Ivana Barravecchia, Elisabetta Barresi, Camilla Russo, Francesca Scebba, Chiara De Cesari, Valerio Mignucci, Davide De Luca, Silvia Salerno, Valeria La Pietra, Mariateresa Giustiniano, Sveva Pelliccia, Diego Brancaccio, Greta Donati, Federico Da Settimo, Sabrina Taliani, Debora Angeloni, Luciana Marinelli, Barravecchia, I., Barresi, E., Russo, C., Scebba, F., De Cesari, C., Mignucci, V., De Luca, D., Salerno, S., La Pietra, V., Giustiniano, M., Pelliccia, S., Brancaccio, D., Donati, G., Da Settimo, F., Taliani, S., Angeloni, D., and Marinelli, L.

Subjects

Passerini-like 3-CR, Multicomponent reactions (MCRs), Pharmaceutical Science, CCG-1423, MICAL2, wound healing assay, HMEC-1 endothelial cells, 786-O kidney cancer cells, metastasis, neoangiogenesis, multicomponent reactions (MCRs), Passerini 3-CR reaction, Metastasi, Article, Analytical Chemistry, HMEC-1 endothelial cell, Small Molecule Libraries, Metastasis, Neoangiogenesis, Wound healing assay, QD241-441, Drug Discovery, Humans, Enzyme Inhibitor, Anilides, Enzyme Inhibitors, Physical and Theoretical Chemistry, Molecular Structure, Microfilament Proteins, Organic Chemistry, Microfilament Protein, Neoangiogenesi, 786-O kidney cancer cell, Oxidoreductase, Chemistry (miscellaneous), Benzamides, Molecular Medicine, Oxidoreductases, Human

Abstract

Molecule interacting with CasL 2 (MICAL2), a cytoskeleton dynamics regulator, are strongly expressed in several human cancer types, especially at the invasive front, in metastasizing cancer cells and in the neo-angiogenic vasculature. Although a plethora of data exist and stress a growing relevance of MICAL2 to human cancer, it is worth noting that only one small-molecule inhibitor, named CCG-1423 (1), is known to date. Herein, with the aim to develop novel MICAL2 inhibitors, starting from CCG-1423 (1), a small library of new compounds was synthetized and biologically evaluated on human dermal microvascular endothelial cells (HMEC-1) and on renal cell adenocarcinoma (786-O) cells. Among the novel compounds, 10 and 7 gave interesting results in terms of reduction in cell proliferation and/or motility, whereas no effects were observed in MICAL2-knocked down cells. Aside from the interesting biological activities, this work provides the first structure–activity relationships (SARs) of CCG-1423 (1), thus providing precious information for the discovery of new MICAL2 inhibitors.

Published

2021

11. Targeting the KRAS oncogene: Synthesis, physicochemical and biological evaluation of novel G-Quadruplex DNA binders

Author

Pasquale Russomanno, Federico Da Settimo, Francesco Saverio Di Leva, Sabrina Taliani, Luca Pompili, Anna Maria Marini, Elisabetta Barresi, Marinella De Leo, Jussara Amato, Concetta Giancola, Senji Shirasawa, Vincenzo Maria D'Amore, Annamaria Biroccio, Pasquale Zizza, Marco Caterino, Gilmar F. Salgado, Silvia Salerno, Luciana Marinelli, Ettore Novellino, Federica D’Aria, D'Aria, F., D'Amore, V. M., Di Leva, F. S., Amato, J., Caterino, M., Russomanno, P., Salerno, S., Barresi, E., De Leo, M., Marini, A. M., Taliani, S., Da Settimo, F., Salgado, G. F., Pompili, L., Zizza, P., Shirasawa, S., Novellino, E., Biroccio, A., Marinelli, L., and Giancola, C.

Subjects

Pharmaceutical Science, Molecular modeling, Medicinal chemistry, 02 engineering and technology, medicine.disease_cause, G-quadruplex, 030226 pharmacology & pharmacy, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, KRAS, neoplasms, Cancer, Nuclease, Virtual screening, biology, Oncogene, Drug discovery, DNA G-quadruplex, Physicochemical studies, 021001 nanoscience & nanotechnology, Small molecule, digestive system diseases, chemistry, Cancer research, biology.protein, 0210 nano-technology, DNA

Abstract

The oncogene KRAS is involved in the pathogenesis of many tumors such as pancreatic, lung and colorectal cancers, thereby representing a relevant target for the treatment of these diseases. The KRAS P1 promoter contains a nuclease hypersensitive, guanine-rich sequence able to fold into a G-quadruplex motif (G4). The stabilization of this G4 structure by small molecules is emerging as a feasible approach to downregulate KRAS expression. Here, a set of novel stabilizing molecules was identified through a virtual screening campaign on the NMR structure of the 22-mer KRAS G4. The most promising hits were then submitted to structure-activity relationships studies which allowed improving their binding affinity and selectivity over double helix DNA and different G4 topologies. The best derivative (19) underwent fluorescence titration experiments and further computational studies to disclose its binding mechanism to KRAS G4. Finally, biological assays showed that this compound is capable to reduce the viability of colorectal cancer cells in which mutated KRAS acts as a driver oncogene. Thus, 19 might represent the prototype of a new class of drugs for the treatment of tumors that, expressing mutated forms of KRAS, are refractory to current therapeutic regimens.

Published

2020

12. Design, synthesis and biological evaluation of novel TRβ selective agonists sustained by ADME-toxicity analysis

Author

Amedeo Columbano, Grazia Chiellini, Luciana Marinelli, Ettore Novellino, Vincenzo Maria D'Amore, Marta Anna Kowalik, Massimiliano Runfola, Valeria La Pietra, Sheraz Gul, Lorenza Bellusci, Andrea Perra, Simona Sestito, Simona Rapposelli, Runfola, M., Sestito, S., Bellusci, L., La Pietra, V., D'Amore, V. M., Kowalik, M. A., Chiellini, G., Gul, S., Perra, A., Columbano, A., Marinelli, L., Novellino, E., and Rapposelli, S.

Subjects

Male, Thyronamine, Hep G2 Cell, Fatty-liver disorder, Liver regeneration, TRβ selective agonist, Triiodothyronine, Pharmacology, 01 natural sciences, Thyroid hormone receptor beta, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Animals, Humans, Uracil, 030304 developmental biology, ADME, 0303 health sciences, Thyroid hormone receptor, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Drug discovery, Animal, Organic Chemistry, Lipid metabolism, Thyroid Hormone Receptors beta, General Medicine, Hep G2 Cells, Rats, Inbred F344, 0104 chemical sciences, Rats, Pyridazines, chemistry, Drug Design, Toxicity, Rat, Pyridazine, Human

Abstract

Although triiodothyronine (T3) induces several beneficial effects on lipid metabolism, its use is hampered by toxic side-effects, such as tachycardia, arrhythmia, heart failure, bone and muscle catabolism and mood disturbances. Since the α isoform of thyroid hormone receptors (TRs) is the main cause of T3-related harmful effects, several efforts have been made to develop selective agonists of the β isoform that could induce some beneficial effects (i.e. lowering triglyceride and cholesterol levels reducing obesity and improving metabolic syndrome), while overcoming most of the adverse T3-dependent side effects. Herein, we describe the drug discovery process sustained by ADME-Toxicity analysis that led us to identify novel agonists with selectivity for the isoform TRβ and an acceptable off-target and absorption, distribution metabolism, excretion and toxicity (ADME-Tox) profile. Within the small series of compounds synthesized, derivatives 1 and 3, emerge from this analysis as “potentially safe” to be engaged in preclinical studies. In in vitro investigation proved that both compounds were able to reduce lipid accumulation in HepG2 and promote lipolysis with comparable effects to those elicited by T3, used as reference drug. Moreover, a preliminary in vivo study confirmed the apparent lack of toxicity, thus suggesting compounds 1 and 3 as new potential TRβ-selective thyromimetics.

Published

2019

13. Functional Selectivity Revealed by N-Methylation Scanning of Human Urotensin II and Related Peptides

Author

Alfonso Carotenuto, Paolo Grieco, William D. Lubell, Rosa Bellavita, Ettore Novellino, Etienne Billard, Diego Brancaccio, Paola Santicioli, Ali Munaim Yousif, David Chatenet, Salvatore Di Maro, Terence E. Hébert, Roberta d'Emmanuele di Villa Bianca, Francesco Merlino, Luigi Abate, Luciana Marinelli, Merlino, F., Billard, E., Yousif, A. M., Di Maro, S., Brancaccio, D., Abate, L., Carotenuto, A., Bellavita, R., D'Emmanuele Di Villa Bianca, R., Santicioli, P., Marinelli, L., Novellino, E., Hebert, T. E., Lubell, W. D., Chatenet, D., Grieco, P., Merlino, Francesco, Billard, Etienne, Yousif, Ali Munaim, Di Maro, Salvatore, Brancaccio, Diego, Abate, Luigi, Carotenuto, Alfonso, Bellavita, Rosa, d'Emmanuele di Villa Bianca, Roberta, Santicioli, Paolo, Marinelli, Luciana, Novellino, Ettore, Hébert, Terence, Lubell, William D, Chatenet, David, Grieco, Paolo, University of Naples Federico II, Institut Armand Frappier (INRS-IAF), Institut National de la Recherche Scientifique [Québec] (INRS)-Réseau International des Instituts Pasteur (RIIP), Menarini Ricerche [Florence], McGill University = Université McGill [Montréal, Canada], Université de Montréal (UdeM), and The study was supported by Canadian Institutes of Health Research (CIHR) (MOP-142184) and the Natural Sciences and Engineering Research Council of Canada (NSERC) (RGPIN-2015-04848) to D.C. We thank the Canadian Institutes of Health Research (CIHR) and the Natural Sciences and Engineering Research Council of Canada (NSERC) for funding

Subjects

Untranslated region, Male, Protein Conformation, [SDV]Life Sciences [q-bio], Peptide Hormones, Urotensins, Peptide, CHO Cells, Urotensin-II receptor, Ligands, 01 natural sciences, Methylation, Receptors, G-Protein-Coupled, Rats, Sprague-Dawley, 03 medical and health sciences, chemistry.chemical_compound, Protein structure, Cricetulus, Drug Discovery, Urotensin-II, peptide synthesis, NMR spectroscopy, N-methylation, Functional selectivity, Animals, Humans, Nuclear Magnetic Resonance, Biomolecular, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Intracellular Signaling Peptides and Proteins, Biological activity, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, HEK293 Cells, chemistry, Biochemistry, Molecular Medicine, Urotensin-II

Abstract

International audience; In accordance with their common but also divergent physiological actions, human urotensin II (1) and urotensin II-related peptide (2) could stabilize specific urotensin II receptor (UTR) conformations, thereby activating different signaling pathways, a feature referred to as biased agonism or functional selectivity. Sequential N-methylation of the amides in the conserved core sequence of 1, 2, and fragment U-II4-11 (3) shed light on structural requirements involved in their functional selectivity. Thus, 18 N-methylated UTR ligands were synthesized and their biological profiles evaluated using in vitro competition binding assays, ex vivo rat aortic ring bioassays and BRET-based biosensor experiments. Biological activity diverged from that of the parent structures contingent on the location of amide methylation, indicating relevant hydrogen-bond interactions for the function of the endogenous peptides. Conformational analysis of selected N-methyl analogs indicated the importance of specific amide residues of 2 for the distinct pharmacology relative to 1 and 3.

Published

2019

14. Cationic nucleopeptides as novel non-covalent carriers for the delivery of peptide nucleic acid (PNA) and RNA oligomers

Author

Ilaria Baglivo, Sandro Cosconati, Giuseppina Rea, Maria Napolitano, Rosita Russo, Angela Chambery, Luciana Marinelli, Ersilia Nigro, Paolo V. Pedone, Stefano Tomassi, Maria Emilia Mercurio, Anna Messere, Caterina Ieranò, Aurora Daniele, Stefania Scala, Ettore Novellino, Salvatore Di Maro, Tomassi, Stefano, Ieranò, Caterina, Mercurio, Maria Emilia, Nigro, Ersilia, Daniele, Aurora, Russo, Rosita, Chambery, Angela, Baglivo, Ilaria, Pedone, Paolo Vincenzo, Rea, Giuseppina, Napolitano, Maria, Scala, Stefania, Cosconati, Sandro, Marinelli, Luciana, Novellino, Ettore, Messere, Anna, Di Maro, Salvatore, Tomassi, S, Ieranò, C, Mercurio, Me, Nigro, E, Daniele, A, Russo, R, Chambery, A, Baglivo, I, Pedone, Pv, Rea, G, Napolitano, M, Scala, S, Cosconati, S, Marinelli, L, Novellino, E, Messere, A, and Di Maro, S.

Subjects

0301 basic medicine, Peptide Nucleic Acids, Cell Membrane Permeability, Clinical Biochemistry, Pharmaceutical Science, Transfection, Biochemistry, Nucleobase, 03 medical and health sciences, chemistry.chemical_compound, Cations, Cell Line, Tumor, Drug Discovery, Cellular-uptake, Humans, Polylysine, Molecular Biology, Nucleic acid analogue, chemistry.chemical_classification, Carrier, cellular-uptake, nucleopeptides, peptide nucleic acids, RNA, Drug Carriers, Peptide nucleic acid, Chemistry, Circular Dichroism, Organic Chemistry, Cationic polymerization, Temperature, RNA, Nucleic Acid Hybridization, Combinatorial chemistry, Amino acid, Nucleopeptide, 030104 developmental biology, Membrane, Solubility, Nucleic acid, Molecular Medicine, Nucleic Acid Conformation, Carrier, Thymine

Abstract

Cationic nucleopeptides belong to a family of synthetic oligomers composed by amino acids and nucleobases. Their capability to recognize nucleic acid targets and to cross cellular membranes provided the basis for considering them as novel non-covalent delivery agents for nucleic acid pharmaceuticals. Herein, starting from a 12-mer nucleopeptide model, the number of cationic residues was modulated in order to obtain new nucleopeptides endowed with high solubility in acqueous medium, acceptable bio-stability, low cytotoxicity and good capability to bind nucleic acid. Two candidates were selected to further investigate their potential as nucleic acid carriers, showing higher efficiency to deliver PNA in comparison with RNA. Noteworthy, this study encourages the development of nucleopeptides as new carriers to extend the known strategies for those nucleic acid analogues, especially PNA, that still remain difficult to drive into the cells.

Published

2018

15. Exploring the Chemical Space of G-Quadruplex Binders: Discovery of a Novel Chemotype Targeting the Human Telomeric Sequence

Author

Carmen D'Angelo, Francesco Saverio Di Leva, Chiara Cingolani, Annamaria Biroccio, Andrea Cavalli, Erica Salvati, Bruno Pagano, Claudia Sissi, Sandro Cosconati, Jussara Amato, Odra Pinato, Luciana Marinelli, Pasquale Zizza, Antonio Randazzo, Ettore Novellino, Di Leva, F. S., Zizza, P., Cingolani, C., D'Angelo, C., Pagano, Bruno, Amato, Jussara, Salvati, E., Sissi, C., Pinato, O., Marinelli, Luciana, Cavalli, A., Cosconati, S., Novellino, Ettore, Randazzo, Antonio, Biroccio, A., Di Leva, F, Zizza, P, Cingolani, C, D'Angelo, C, Pagano, B, Amato, J, Salvati, E, Sissi, C, Pinato, O, Marinelli, L, Cavalli, A, Cosconati, Sandro, Novellino, E, Randazzo, A, Francesco Saverio Di Leva, Pasquale Zizza, Chiara Cingolani, Carmen D’Angelo, Bruno Pagano, Jussara Amato, Erica Salvati, Claudia Sissi, Odra Pinato, Luciana Marinelli, Andrea Cavalli, Sandro Cosconati, Ettore Novellino, Antonio Randazzo, and Annamaria Biroccio

Subjects

Genetics, Virtual screening, Chemistry, DNA damage, Antineoplastic Agents, Sequence (biology), Computational biology, Telomere, Ligands, G-quadruplex, Chemical space, G-Quadruplexes, Molecular Docking Simulation, chemistry.chemical_compound, Cell Line, Tumor, Drug Discovery, Fluorescence Resonance Energy Transfer, Humans, Molecular Medicine, Receptor, G-QUADRUPLEX, Binding selectivity, DNA

Abstract

Recent findings have unambiguously demonstrated that DNA G-rich sequences can adopt a G-quadruplex folding in living cells, thus further validating them as crucial targets for anticancer therapy. Herein, to identify new potent G4 binders as antitumor drug candidates, we have targeted a 24-nt G4-forming telomeric sequence employing a receptor-based virtual screening approach. Among the best candidates, in vitro binding experiments allowed identification of three novel G4 ligands. Among them, the best compound features an unprecedented binding selectivity for the human telomeric DNA G-quadruplex with no detectable binding for other G4-forming sequences present at different genomic sites. This behavior correlates with the detected ability to generate DNA damage response in tumor cells at the telomeric level and efficient antiproliferative effect on different tumor cell lines at low micromolar concentrations. © 2013 American Chemical Society.

Published

2013

16. Ligand Based Approach to L-Type Calcium Channel by Imidazo[2,1-b]thiazole-1,4-Dihydropyridines: from Heart Activity to Brain Affinity

Author

Pierfranco Ioan, Ettore Novellino, Santi Mario Spampinato, Roberta Budriesi, Alberto Leoni, Matteo Micucci, Sandro Cosconati, Andrea Bedini, Alberto Chiarini, Luciana Marinelli, Alessandra Locatelli, A., Locatelli, S., Cosconati, M., Micucci, A., Leoni, Marinelli, Luciana, A., Bedini, P., Ioan, S. M., Spampinato, Novellino, Ettore, A., Chiarini, R., Budriesi, Locatelli, A, Cosconati, Sandro, Micucci, M, Leoni, A, Marinelli, L, Bedini, A, Ioan, P, Spampinato, Sm, Novellino, E, Chiarini, A, Budriesi, R., Alessandra Locatelli, Sandro Cosconati, Matteo Micucci, Alberto Leoni, Luciana Marinelli, Andrea Bedini, Pierfranco Ioan, Santi Mario Spampinato, Ettore Novellino, Alberto Chiarini, and Roberta Budriesi

Subjects

Models, Molecular, Gene isoform, Dihydropyridines, Calcium Channels, L-Type, Molecular model, 4-imidazo[2, Protein subunit, Guinea Pigs, functional in vitro assay, In Vitro Techniques, Structure-Activity Relationship, chemistry.chemical_compound, Heart Rate, Models, Drug Discovery, Animals, Structure–activity relationship, Myocytes, Cardiac, Computer Simulation, L-type calcium channel, Calcium Channel Blockers, Calcium Channels, Cerebral Cortex, Heart, Imidazoles, Muscle, Smooth, Myocardial Contraction, Rats, Thiazoles, Myocardium, Thiazole, cardiac and smooth muscle, NEUROPROTECTION, Myocytes, Cav1.2 and Cav1.3 isoform, Chemistry, Molecular, Ligand (biochemistry), L-Type, In vitro, 1-b]thiazole-1, Biochemistry, Muscle, Molecular Medicine, Smooth, 4-dihydropyridine, Cardiac

Abstract

The synthesis, characterization, and functional in vitro assay in cardiac and smooth muscle (vascular and nonvascular) of a series of 4-imidazo[2,1-b] thiazole-1,4-dihydropyridines are reported. To define the calcium blocker nature of the imidazo[2,1-b]thiazole-1,4-DHPs and their selectivity on Ca v1.2 and Cav1.3 isoforms, we performed binding studies on guinea pig atrial and ventricular membranes on intact cells expressing the cloned Cav1.2a subunit and on rat brain cortex. To get major insights into the reasons for the affinity for Cav1.2 and/or Ca v1.3, molecular modeling studies were also undertaken. Some physicochemical and pharmacokinetic properties of selected compounds were calculated and compared. All the biological data collected and reported herein allowed us to rationalize the structure-activity relationship of the 4-imidazo[2,1-b]thiazole-1,4-DHPs and to identify which of these enhanced the activity at the central level. © 2013 American Chemical Society.

Published

2013

17. Design, synthesis, and biological evaluation of novel aminobisphosphonates possessing an in vivo antitumor activity through a gammadelta-T lymphocytes-mediated activation mechanism

Author

Daniele Simoni, Aaron Kwaasi, Riccardo Baruchello, James E. Dunford, Carla Marchioro, L. Marinelli, Francesco Dieli, Simona Buccheri, Stefano Provera, Nadia Caccamo, Nicola Gebbia, Francesco Paolo Invidiata, Ettore Novellino, Riccardo Rondanin, Paolo Marchetti, Manlio Tolomeo, Marco Eleopra, Vittorio Limongelli, SIMONI D, GEBBIA N, INVIDIATA F, ELEOPRA M, MARCHETTI P, RONDANIN R, BARUCHELLO R, PROVERA S, MARCHIORO C, TOLOMEO M, MARINELLI L, LIMONGELLI V, NOVELLINO E, KWAASI A, DUNFORD J, BUCCHERI S, CACCAMO NR, and DIELI F

Subjects

T cell, Antineoplastic Agents, Apoptosis, Mice, SCID, Lymphocyte Activation, Mice, Structure-Activity Relationship, Antigen, In vivo, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Structure–activity relationship, Amines, Cytotoxicity, Diphosphonates, Molecular Structure, Chemistry, Receptors, Antigen, T-Cell, gamma-delta, Biological activity, In vitro, medicine.anatomical_structure, Biochemistry, Mechanism of action, Drug Design, Cancer research, Molecular Medicine, medicine.symptom, aminobisphosphonates ,gammadelta-T lymphocytes

Abstract

A small series of aminobisphosphonates (N-BPs) structurally related to zoledronic acid was synthesized with the aim of improving activity toward activation of human gammadelta T cells and in turn their in vivo antitumor activity. The absence of the 1-OH moiety, together with the position and the different basicity of the nitrogen, appears crucial for antitumor activity. In comparison to zoledronic acid, compound 6a shows a greater ability to activate gammadelta T cells expression (100 times more) and a proapoptotic effect that is better than zoledronic acid. The potent activation of gammadelta T cells, in addition to evidence of the in vivo antitumor activity of 6a, suggests it may be a new potential drug candidate for cancer treatment.

Published

2016

18. From the Pharmacophore to the Homology Model of the Benzodiazepine Receptor: The Indolyglyoxylamides Affair

Author

Ettore Novellino, Barbara Cosimelli, Sandro Cosconati, Luciana Marinelli, Giovanni Greco, Cosimelli, B, Cosconati, Sandro, Marinelli, L, Novellino, E, Greco, G., Cosimelli, Barbara, Cosconati, S., Marinelli, Luciana, Novellino, Ettore, and Greco, Giovanni

Subjects

Models, Molecular, Indoles, medicine.drug_class, Stereochemistry, benzodiazepine receptor ligand, Ligands, Docking, Structure-Activity Relationship, Drug Discovery, medicine, Humans, Hypnotics and Sedatives, Structure–activity relationship, GABA-A Receptor Agonists, GABA-A Receptor Antagonists, Homology modeling, Binding site, Receptor, Indole test, Benzodiazepine, Binding Sites, Pharmacophore, Chemistry, Brain, Glyoxylates, Benzodiazepine receptor, General Medicine, Receptors, GABA-A, Amides, Protein Subunits, Anti-Anxiety Agents, Docking (molecular), Homology modelling, Molecular modelling, indolyglyoxylamides, Protein Binding, Binding mode

Abstract

Interaction between the so-called benzodiazepine receptor (BzR) and the chemically heterogeneous class of its ligands is still one of the most challenging objects of theoretical studies. In the mid-90s our group began to collaborate with Prof. Antonio Da Settimo and coworkers to a project of synthesis and biological evaluation of indolylglyoxylamides designed as BzR ligands. Herein we review our efforts in designing these compounds and in interpreting their structure-affinity relationships. Our investigations were carried out for years by adopting the pharmacophore/topological model for BzR ligands set up by Cook's group. In an attempt to rationalize some puzzling structure-affinity relationships we speculated in 1998 that our ligands interact with the BzR by assuming one of two alternative binding modes (called "A" and "B") depending on whether or not they were substituted at the 5-position of the indole nucleus. Such a model received support from a considerable amount of experimental data accumulated throughout our researches. About a decade later, docking calculations performed on a homology-built model of the α 1 BzR subtype were found in agreement with the hypothesis of mode A and mode B of binding accessible to 5-H and, respectively, 5-Cl/NO 2 indole derivatives. © 2012 Bentham Science Publishers.

Published

2012

19. Identification of novel molecular scaffolds for the design of MMP-13 inhibitors: A first round of lead optimization

Author

Valeria La Pietra, Sabrina Taliani, Hideaki Nagase, Elisa Nuti, Robert Visse, Federico Da Settimo, Francesco Saverio Di Leva, Ettore Novellino, Luciana Marinelli, Concettina La Motta, Salvatore Santamaria, Sandro Cosconati, Matteo Morelli, Armando Rossello, F Casalini, Isabella Pugliesi, La Pietra, V, Marinelli, L, Cosconati, Sandro, Di Leva, F, Nuti, E, Santamaria, S, Pugliesi, I, Morelli, M, Casalini, F, Rossello, A, La Motta, C, Taliani, S, Visse, R, Nagase, H, da Settimo, F, Novellino, E., LA PIETRA, Valeria, Marinelli, Luciana, Cosconati, S., Di Leva, Francesco Saverio, Nuti, E., Santamaria, S., Pugliesi, I., Morelli, M., Casalini, F., Rossello, A., La Motta, C., Taliani, S., Visse, R., Nagase, H., da Settimo, F., and Novellino, Ettore

Subjects

Virtual screening, High selectivity, Drug Evaluation, Preclinical, Nanotechnology, Articular cartilage, Osteoarthritis, Matrix Metalloproteinase Inhibitors, Matrix metalloproteinase, Crystallography, X-Ray, Inhibitory Concentration 50, User-Computer Interface, Catalytic Domain, Matrix Metalloproteinase 13, Drug Discovery, medicine, Humans, Protease Inhibitors, IC50, Cancer, Pharmacology, MMP, Chemistry, Cartilage, Organic Chemistry, General Medicine, medicine.disease, medicine.anatomical_structure, Docking (molecular), Drug Design, Molecular docking, Cancer research, Osteoarthriti

Abstract

Osteoarthritis (OA) is the leading cause of joint pain and disability in middle-aged and elderly patients, and is characterized by progressive loss of articular cartilage. Among the various matrix metalloproteinases (MMPs), MMP-13 is specifically expressed in the cartilage of human OA patients and is not present in normal adult cartilage. Thus, MMP-13-selective inhibitors are promising candidates in osteoarthritis therapy. Recently, we designed an N-isopropoxy-arylsulfonamide-based hydroxamate inhibitor, which showed low nanomolar activity and high selectivity for MMP-13. In parallel to further studies aiming to assess the in vivo activity of our compound, we screened the Life Chemicals database through computational docking to seek for novel scaffolds as zinc-chelating non-hydroxamate inhibitors. Experimental evaluation of 20 selected candidate compounds verified five novel leads with IC 50 in the low μM range. These newly discovered inhibitors are structurally unrelated to the ones known so far and provide useful scaffolds to develop compounds with more desirable properties. Finally, a first round of structure-based optimization on lead 1 was accomplished and led to an increase in potency of more than 5 fold. © 2011 Elsevier Masson SAS. All rights reserved.

Published

2012

20. Imidazo[2,1-b]thiazole System: A Scaffold Endowing Dihydropyridines with Selective Cardiodepressant Activity

Author

Sandro Cosconati, Alberto Leoni, Andrea Bedini, Ettore Novellino, Rosanna Di Toro, Maria Paola Ugenti, Aldo Andreani, Santi Mario Spampinato, Roberta Budriesi, Alberto Chiarini, Luciana Marinelli, Pierfranco Ioan, Alessandra Locatelli, Budriesi, R, Ioan, P, Locatelli, A, Cosconati, Sandro, Leoni, A, Ugenti, Mp, Andreani, A, Di Toro, R, Bedini, A, Spampinato, S, Marinelli, L, Novellino, E, Chiarini, A., Budriesi, R., Ioan, P., Locatelli, A., Leoni, A., Ugenti, M. P., Andreani, A., Di Toro, R., Bedini, A., Spampinato, S., Marinelli, Luciana, Novellino, Ettore, R. Budriesi, P. Ioan, A. Locatelli, S. Cosconati, A. Leoni, M. P. Ugenti, A. Andreani, R. Di Toro, A. Bedini, S. Spampinato, L. Marinelli, E. Novellino, and A. Chiarini.

Subjects

Models, Molecular, Chronotropic, Dihydropyridines, Molecular model, Stereochemistry, Guinea Pigs, Drug Evaluation, Preclinical, Ligands, Chemical synthesis, Muscle, Smooth, Vascular, Small Molecule Libraries, Structure-Activity Relationship, chemistry.chemical_compound, Heart Rate, Drug Discovery, medicine, Animals, Computer Simulation, Myocytes, Cardiac, L-type calcium channel, Binding site, Thiazole, Binding Sites, Molecular Structure, Chemistry, Calcium channel, Imidazoles, Dihydropyridine, Heart, Myocardial Contraction, Thiazoles, Drug Design, Molecular Medicine, medicine.drug

Abstract

The synthesis, characterization, and functional in vitro assays in cardiac tissues and smooth muscle (vascular and nonvascular) of a number of 4-imidazo[2,1-b]thiazole-1,4-dihydropyridines are reported. The binding properties for the novel compounds have been investigated and the interaction with the binding site common to other aryl-dihydropyridines has been demonstrated. Interestingly, the novel 4-aryl-dihydropyridines are L-type calcium channel blockers with a peculiar pharmacological behavior. Indeed, the imidazo[2,1-b]thiazole system is found to confer to the dihydropyridine scaffold an inotropic and/or chronotropic cardiovascular activity with a high selectivity toward the nonvascular tissue. Finally, molecular modeling studies were undertaken for the most representative compounds with the aim of describing the binding properties of the new ligands at molecular level and to rationalize the found structure-activity relationship data. Due to the observed pharmacological behavior of our compounds, they might be promising agents for the treatment of specific cardiovascular pathologies such as cardiac hypertrophy and ischemia. © 2008 American Chemical Society.

Published

2008

21. Homology Modeling of NR2B Modulatory Domain of NMDA Receptor and Analysis of Ifenprodil Binding

Author

Vittorio Limongelli, Thomas Steinbrecher, David A. Case, Ettore Novellino, Alessia Bertamino, Sandro Cosconati, Luciana Marinelli, Marinelli, L, Cosconati, Sandro, Steinbrecher, T, Limongelli, V, Bertamino, A, Novellino, E, Case, Da, Marinelli, Luciana, Cosconati, S, Limongelli, Vittorio, and Novellino, Ettore

Subjects

Models, Molecular, Homology modeling, Ifenprodil, Molecular modeling, NMDA receptors, NR2B modulatory domain, Amino Acid Sequence, Animals, Excitatory Amino Acid Antagonists, Humans, Molecular Sequence Data, Piperidines, Protein Binding, Rats, Receptors, N-Methyl-D-Aspartate, Sequence Homology, Amino Acid, Pharmacology, Toxicology and Pharmaceutics (all), Organic Chemistry, Molecular Medicine, Stereochemistry, Toxicology and Pharmaceutics (all), Allosteric regulation, Sequence Homology, Plasma protein binding, Biochemistry, chemistry.chemical_compound, Models, Receptors, Drug Discovery, General Pharmacology, Toxicology and Pharmaceutics, Ion channel, Pharmacology, Rational design, Molecular, NMDA receptor, Amino Acid, nervous system, chemistry, Docking (molecular), Synaptic plasticity, Neuroscience, N-Methyl-D-Aspartate

Abstract

NMDA receptors are glutamate-gated ion channels (iGluRs) that are involved in several important physiological functions such as neuronal development, synaptic plasticity, learning, and memory. Among iGluRs, NMDA receptors have been perhaps the most actively investigated for their role in chronic neurodegeneration such as Alzheimer's, Parkinson's, and Huntington's diseases. Recent studies have shown that the NTD of subunit NR2B modulates ion channel gating through the binding of allosteric modulators such as the prototypical compound ifenprodil. In the present paper, the construction of a three-dimensional model for the NR2B modulatory domain is described and docking calculations allow, for the first time, definition of the ifenprodil binding pose at an atomic level and fully explain all the available structure-activity relationships. Moreover, in an attempt to add further insight into the ifenprodil mechanism of action, as it is not completely clear if it binds and stabilizes an open or a closed conformation of the NR2B modulatory domain, a matter, which is fundamental for the rational design of NMDA antagonists, MD simulations followed by an MM-PBSA analysis were performed. These calculations reveal that the closed conformation of the R1-R2 domain, rather than the open, constitutes the high affinity binding site for ifenprodil and that a profound stabilization of the closed conformation upon ifenprodil binding occurs. Thus, for a rational design and/or for virtual screening experiments, the closed conformation of the R1-R2 domain should be taken into account and our 3D model can provide valuable hints for the design of NR2B-selective antagonists. © 2007 Wiley-VCH Verlag GmbH & Co. KGaA.

Published

2007

22. Ensemble-Docking Approach on BACE-1: Pharmacophore Perception and Guidelines for Drug Design

Author

Ettore Novellino, Boris Schmidt, Sandro Cosconati, Hannes A. Braun, Luciana Marinelli, Vittorio Limongelli, Limongelli, V, Marinelli, L, Cosconati, Sandro, Braun, Ha, Schmidt, B, Novellino, E., Limongelli, Vittorio, Marinelli, Luciana, A., BRAUN HANNES, B., Schmidt, and Novellino, Ettore

Subjects

Drug, Molecular model, Computer science, Peptidomimetic, media_common.quotation_subject, Molecular modeling, Medicinal chemistry, Computational biology, Biochemistry, Catalytic Domain, Drug Discovery, Aspartic Acid Endopeptidases, General Pharmacology, Toxicology and Pharmaceutics, media_common, Pharmacology, Organic Chemistry, Rational design, BACE-1 inhibitor, Stereoisomerism, Combinatorial chemistry, Ensemble docking, Enzyme inhibition, Docking (molecular), Drug Design, Pharmacophore model, Molecular Medicine, Amyloid Precursor Protein Secretases, Pharmacophore

Abstract

β-Secretase (BACE-1), a key enzyme in the etiopathogenesis and progression of Alzheimer Disease, is the focus of medicinal chemistry efforts both in the pharmaceutical industry and in academia. Despite the availability of diverse peptidomimetic BACE-1 inhibitors, nonpeptidic compounds suitable for oral delivery and transport across the blood brain barrier are in great demand. Herein, a number of active and structurally diverse inhibitors were selected and subjected to an ensemble-docking process into five BACE-1 X-ray structures. The calculated bioactive conformations of these inhibitors allowed us to build an exhaustive pharmacophore model, which captures both the common geometric and electronic features essential for enzyme inhibition. The model is intended to aid the rational design of new BACE-1 inhibitors. Furthermore, a comparison of BACE/cathepsin D X-ray structures was made to provide guidelines for the design of BACE-selective inhibitors. © 2007 Wiley-VCH Verlag GmbH& Co. KGaA.

Published

2007

23. Deepening the Topology of the Translocator Protein Binding Site by Novel N,N-Dialkyl-2-arylindol-3-ylglyoxylamides

Author

Barbara Cosimelli, Simona Daniele, Anna Maria Marini, Eleonora Da Pozzo, Francesca Simorini, Luciana Marinelli, Concettina La Motta, Elisabetta Barresi, Sabrina Taliani, Chiara Giacomelli, Claudia Martini, Federico Da Settimo, Sandro Cosconati, Silvia Salerno, Giovanni Greco, Agostino Bruno, Ettore Novellino, Barresi, Elisabetta, Bruno, Agostino, Taliani, Sabrina, Cosconati, Sandro, Da Pozzo, Eleonora, Salerno, Silvia, Simorini, Francesca, Daniele, Simona, Giacomelli, Chiara, Marini, Anna Maria, La Motta, Concettina, Marinelli, Luciana, Cosimelli, Barbara, Novellino, Ettore, Greco, Giovanni, Da Settimo, Federico, Martini, Claudia, Barresi, E, Bruno, A, Taliani, S, Da Pozzo, E, Salerno, S, Simorini, F, Daniele, S, Giacomelli, C, Marini, Am, La Motta, C, Marinelli, L, Cosimelli, B, Novellino, E, Greco, G, Da Settimo, F, and Martini, C.

Subjects

Binding Sites, Indoles, biology, Ligand, Stereochemistry, Chemistry, Drug Discovery3003 Pharmaceutical Science, Rats, Structure-Activity Relationship, GABA metabolism, Receptors, GABA, Docking (molecular), Molecular Medicine, Drug Discovery, Mitochondrial Membranes, Translocator protein, biology.protein, Structure–activity relationship, Animals, Binding site, Group performance

Abstract

As a continuation of our studies on 2-phenylindol-3-ylglyoxylamides as potent and selective translocator protein (TSPO) ligands, two subsets of novel derivatives, featuring hydrophilic group (OH, NH2, COOH) at the para-position of the pendent 2-phenyl ring (8-16) or different 2-aryl moieties, namely, 3-thienyl, p-biphenyl, 2-naphthyl (23-35), were synthesized and biologically evaluated, some of them showing K-i values in the subnanomolar range and the 2-naphthyl group performance being the best. The resulting SARs confirmed the key role played by interactions taking place between ligands and the lipophilic Li pocket of the TSPO binding site. Docking simulations were performed on the most potent compound of the present series (29) exploiting the recently available 3D structures of TSPO bound to its standard ligand (PK11195). Our theoretical model was fully consistent with SARs of the newly investigated as well of the previously reported 2-phenylindol-3-ylglyoxylamide derivatives.

Published

2015

24. N‑substituted quinolinonyl diketo acid derivatives as HIV integrase strand transfer inhibitors and their activity against RNase H function of reverse transcriptase

Author

Takashi Masoaka, Antonella Messore, Giuliana Cuzzucoli Crucitti, Valentina Noemi Madia, Ettore Novellino, Sandro Cosconati, Francesco Saverio Di Leva, Silvano Tortorella, Luca Pescatori, Christophe Marchand, Suhman Chung, Stuart F.J. Le Grice, Yves Pommier, Luciana Marinelli, Giovanni Pupo, Francesco Saccoliti, Mathieu Métifiot, Luigi Scipione, Roberto Di Santo, Roberta Costi, Pescatori, L, Métifiot, M, Chung, S, Masoaka, T, Cuzzucoli Crucitti, G, Messore, A, Pupo, G, Madia, Vn, Saccoliti, F, Scipione, L, Tortorella, S, Di Leva, F, Cosconati, Sandro, Marinelli, L, Novellino, E, Le Grice, Sf, Pommier, Y, Marchand, C, Costi, R, Di Santo, R., Pescatori, Luca, Métifiot, Mathieu, Chung, Suhman, Masoaka, Takashi, Cuzzucoli Crucitti, Giuliana, Messore, Antonella, Pupo, Giovanni, Madia, Valentina Noemi, Saccoliti, Francesco, Scipione, Luigi, Tortorella, Silvano, Di Leva, Francesco Saverio, Marinelli, Luciana, Novellino, Ettore, Le Grice, Stuart F. J., Pommier, Yve, Marchand, Christophe, Costi, Roberta, and Di Santo, Roberto

Subjects

Models, Molecular, Stereochemistry, Ribonuclease H, HIV Infections, HIV Integrase, Quinolones, Virus Replication, Article, chemistry.chemical_compound, Structure-Activity Relationship, Catalytic Domain, Drug Discovery, Humans, HIV Integrase Inhibitors, Bifunctional, RNase H, IC50, biology, Molecular Structure, RNA-Directed DNA Polymerase, Keto Acids, In vitro, Reverse transcriptase, Integrase, HIV, Integrase, Ribonuclease H, Antiviral Drugs, Medicinal Chemistry, chemistry, biology.protein, Benzyl group, HIV-1, Molecular Medicine, Selectivity, HeLa Cells, immunodeficiency virus type 1, ribonuclease H, dual inhibitors, biological evaluation, in vitro, DNA, design, site, hydroxytropolones, raltegravir

Abstract

Bifunctional quinolinonyl DKA derivatives were first described as nonselective inhibitors of 3′-processing (3′-P) and strand transfer (ST) functions of HIV-1 integrase (IN), while 7-aminosubstituted quinolinonyl derivatives were proven IN strand transfer inhibitors (INSTIs) that also displayed activity against ribonuclease H (RNase H). In this study, we describe the design, synthesis, and biological evaluation of new quinolinonyl diketo acid (DKA) derivatives characterized by variously substituted alkylating groups on the nitrogen atom of the quinolinone ring. Removal of the second DKA branch of bifunctional DKAs, and the amino group in position 7 of quinolinone ring combined with a fine-tuning of the substituents on the benzyl group in position 1 of the quinolinone, increased selectivity for IN ST activity. In vitro, the most potent compound was 11j (IC50 = 10 nM), while the most active compounds against HIV infected cells were ester derivatives 10j and 10l. In general, the activity against RNase H was negligible, with only a few compounds active at concentrations higher than 10 μM. The binding mode of the most potent IN inhibitor 11j within the IN catalytic core domain (CCD) is described as well as its binding mode within the RNase H catalytic site to rationalize its selectivity. (Chemical Presented).

Published

2015

25. Structure–Activity Relationship Refinement and Further Assessment of 4-phenylquinazoline-2-carboxamide Translocator Protein (TSPO) Ligands as Antiproliferative Agents in Human Glioblastoma Tumors

Author

Luciana Marinelli, Federico Da Settimo, Giovanni Greco, Claudia Martini, Monica Viviano, Sabrina Taliani, Ciro Milite, Sandro Cosconati, Eleonora Da Pozzo, Ettore Novellino, Elisabetta Barresi, Gianluca Sbardella, Barbara Costa, Sabrina Castellano, Agostino Bruno, Castellano, S, Taliani, S, Viviano, M, Milite, C, Da Pozzo, E, Costa, B, Barresi, E, Bruno, A, Cosconati, Sandro, Marinelli, L, Greco, G, Novellino, E, Sbardella, G, Da Settimo, F, Martini, C., Sabrina, Castellano, Sabrina, Taliani, Monica, Viviano, Ciro, Milite, Eleonora Da, Pozzo, Barbara, Costa, Elisabetta, Barresi, Agostino, Bruno, Sandro, Cosconati, Marinelli, Luciana, Greco, Giovanni, Novellino, Ettore, Gianluca, Sbardella, Federico Da, Settimo, and Claudia, Martini

Subjects

Models, Molecular, 18 KDA, Molecular Conformation, Carboxamide, Plasma protein binding, translocator protein (TSPO), steroidogenesis, 4-phenylquinazoline-2-carboxamide derivatives, structure-activity relationships, pharmacophore model, Kidney, COLORECTAL-CANCER, Drug Discovery, PERIPHERAL BENZODIAZEPINE-RECEPTOR, Inner mitochondrial membrane, Membrane Potential, Mitochondrial, biology, Chemistry, DERIVATIVES, Brain Neoplasms, glioblastoma tumor, BINDING-SITES, BIOLOGICAL EVALUATION, TSPO EXPRESSION, BREAST-CANCER, CELLS, APOPTOSIS, Biochemistry, Molecular Medicine, Pharmacophore, Intracellular, Protein Binding, medicine.drug_class, Cell Survival, Antineoplastic Agents, Structure-Activity Relationship, antiproliferative agents, Receptors, GABA, Cell Line, Tumor, medicine, Translocator protein, TRANSLOCATOR PROTEIN, Structure–activity relationship, Animals, Humans, Binding site, Dose-Response Relationship, Drug, Computational Biology, Rats, Kinetics, biology.protein, Glioblastoma

Abstract

Structure-activity relationships (SARs) within the 4-phenylquinazoline-2- carboxamide series of translocator protein (TSPO) ligands have been explored further by the synthesis and TSPO binding affinity evaluation of N-benzyl-N-ethyl/methyl derivatives variously decorated at the 6-, 2′-, 4′-, and 4″-positions. Most of the compounds showed high affinity with Ki values in the nanomolar/subnanomolar range. A pharmacophore model was developed and employed to better address SAR data presented by the new TSPO ligands. A subset of the new compounds (5, 8, 12, and 19) were tested for their ability to inhibit the viability of human glioblastoma cell line U343. The observed antiproliferative effect was demonstrated to be specific for compound 19, endowed with the best combination of binding affinity and efficacy. Furthermore, the ability of 19 to induce mitochondrial membrane dissipation (Δψm) substantiated the intracellular pro-apoptotic mechanism activated by the binding of this class of ligands to TSPO. © 2014 American Chemical Society.

Published

2014

26. Basic Quinolinonyl Diketo Acid Derivatives as Inhibitors of HIV Integrase and their Activity against RNase H Function of Reverse Transcriptase

Author

Giuliana Cuzzucoli Crucitti, Kasthuraiah Maddali, Mathieu Métifiot, Roberto Di Santo, Giovanni Pupo, Stuart F.J. Le Grice, Francesco Saverio Di Leva, Christophe Marchand, Luigi Scipione, Antonella Messore, Yves Pommier, Valentina Noemi Madia, Sandro Cosconati, Roberta Costi, Angela Corona, Suhman Chung, Luca Pescatori, Ettore Novellino, Luciana Marinelli, Silvano Tortorella, Roberta, Costi, Mathieu, M?tifiot, Suhman, Chung, Giuliana Cuzzucoli Crucitti, Kasthuraiah, Maddali, Luca, Pescatori, Antonella, Messore, Valentina Noemi Madia, Giovanni, Pupo, Luigi, Scipione, Silvano, Tortorella, Di Leva, Francesco Saverio, Sandro, Cosconati, Marinelli, Luciana, Novellino, Ettore, Le Grice, Stuart F. J., Angela, Corona, Yves, Pommier, Christophe, Marchand, Roberto Di Santo, Costi, R, Metifiot, M, Chung, S, Crucitti, Gv, Maddali, K, Pescatori, L, Messore, A, Madia, Vn, Pupo, G, Scipione, L, Tortorella, S, Di Leva, F, Cosconati, Sandro, Marinelli, L, Novellino, E, Le Grice, Sfj, Corona, A, Pommier, Y, Marchand, C, and Di Santo, R.

Subjects

Models, Molecular, biology, Molecular model, Chemistry, Stereochemistry, Ribonuclease H, Quinolones, Reverse transcriptase, Article, Catalysis, Integrase, Structure-Activity Relationship, Drug Discovery, biology.protein, Molecular Medicine, Structure–activity relationship, HIV Integrase Inhibitors, Selectivity, RNase H, Function (biology)

Abstract

A series of antiviral basic quinolinonyl diketo acid derivatives were developed as inhibitors of HIV-1 IN. Compounds 12d,f,i inhibited HIV-1 IN with IC50 values below 100 nM for strand transfer and showed a 2 order of magnitude selectivity over 3′-processing. These strand transfer selective inhibitors also inhibited HIV-1 RNase H with low micromolar potencies. Molecular modeling studies based on both the HIV-1 IN and RNase H catalytic core domains provided new structural insights for the future development of these compounds as dual HIV-1 IN and RNase H inhibitors. © 2014 American Chemical Society.

Published

2014

27. Human recombinant beta-secretase immobilized enzyme reactor for fast hits’ selection and characterization from a virtual screening library

Author

Ettore Novellino, Valeria La Pietra, Luciana Marinelli, Sandro Cosconati, Vincenza Andrisano, Angela De Simone, Francesca Mancini, Angela De Simone, Francesca Mancini, Sandro Cosconati, Luciana Marinelli, Valeria La Pietra, Ettore Novellino, Vincenza Andrisano, De Simone, A., Mancini, F., Cosconati, S., Marinelli, Luciana, LA PIETRA, Valeria, Novellino, Ettore, Andrisano, V., De Simone, A, Mancini, F, Cosconati, Sandro, Marinelli, L, La Pietra, V, and Novellino, E

Subjects

Immobilized enzyme, virtual screening library, Clinical Biochemistry, Pharmaceutical Science, Sensitivity and Specificity, inhibitor hits screening, Substrate Specificity, Analytical Chemistry, law.invention, Small Molecule Libraries, Bioreactors, law, LC-Fluorescent detection, Drug Discovery, High-Throughput Screening Assays, Fluorescence Resonance Energy Transfer, Aspartic Acid Endopeptidases, Humans, Inhibition mechanism, Enzyme Inhibitors, Mode of action, Chromatography, High Pressure Liquid, Spectroscopy, chemistry.chemical_classification, Virtual screening, Chromatography, Chemistry, Enzymes, Immobilized, Combinatorial chemistry, Fluorescence, Förster resonance energy transfer, Enzyme, Recombinant DNA, online enzyme activity, hrBACE1-IMER, Amyloid Precursor Protein Secretases

Abstract

In the present work, a human recombinant BACE1 immobilized enzyme reactor (hrBACE1-IMER) has been applied for the sensitive fast screening of 38 compounds selected through a virtual screening approach. HrBACE1-IMER was inserted into a liquid chromatograph coupled with a fluorescent detector. A fluorogenic peptide substrate (M-2420), containing the β-secretase site of the Swedish mutation of APP, was injected and cleaved in the on-line HPLC-hrBACE1-IMER system, giving rise to the fluorescent product. The compounds of the library were tested for their ability to inhibit BACE1 in the immobilized format and to reduce the area related to the chromatographic peak of the fluorescent enzymatic product. The results were validated in solution by using two different FRET methods. Due to the efficient virtual screening methodology, more than fifty percent of the selected compounds showed a measurable inhibitory activity. One of the most active compound (a bis-indanone derivative) was characterized in terms of IC50 and Ki determination on the hrBACE1-IMER. Thus, the hrBACE1-IMER has been confirmed as a valid tool for the throughput screening of different chemical entities with potency lower than 30μM for the fast hits' selection and for mode of action determination. © 2012 Elsevier B.V.

Published

2013

28. Phenylpyrazolo[1,5‑a]quinazolin-5(4H)‑one: a suitable scaffold for the development of noncamptothecin topoisomerase I (Top1) inhibitors

Author

Anna Maria Marini, Christophe Marchand, Keli Agama, Luciana Marinelli, Concettina La Motta, Francesco Saverio Di Leva, Sabrina Taliani, Ettore Novellino, Silvia Salerno, Yves Pommier, Roberto Di Santo, Elisabetta Barresi, Federico Da Settimo, Francesca Simorini, Sandro Cosconati, Isabella Pugliesi, Taliani, S, Pugliesi, I, Barresi, E, Salerno, S, Marchand, C, Agama, K, Simorini, F, La Motta, C, Marini, Am, Di Leva, F, Marinelli, L, Cosconati, Sandro, Novellino, E, Pommier, Y, Di Santo, R, Da Settimo, F., Department of Pharmacy, University of Pisa - Università di Pisa, Laboratory of Molecular Pharmacology, National Cancer Institute [Bethesda] (NCI-NIH), National Institutes of Health [Bethesda] (NIH)-National Institutes of Health [Bethesda] (NIH), Department of Pharmaceutical Chemistry and Toxicology, Università degli studi di Napoli Federico II, Department of Pharmacy Naples, Université de Naples, National Institutes of Health [Bethesda] (NIH)-National Cancer Institute [Bethesda] (NCI-NIH), National Institutes of Health [Bethesda] (NIH), Department of Medicinal Chemistry and Technologies, Institut Pasteur, Fondation Cenci Bolognetti - Istituto Pasteur Italia, Fondazione Cenci Bolognetti, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], S., Taliani, I., Pugliesi, E., Barresi, S., Salerno, C., Marchand, K., Agama, F., Simorini, C., La Motta, A. M., Marini, Di Leva, Francesco Saverio, Marinelli, Luciana, S., Cosconati, Novellino, Ettore, Y., Pommier, R., Di Santo, and F., Da Settimo

Subjects

Protein Conformation, Stereochemistry, Topoisomerase-I Inhibitor, 010402 general chemistry, Cleavage (embryo), 01 natural sciences, Molecular Docking Simulation, Article, antitumor agents, chemistry.chemical_compound, MESH: Protein Conformation, MESH: Drug Discovery, Drug Discovery, inhibitors, Side chain, Quinazoline, MESH: Molecular Docking Simulation, Humans, Pyrroles, MESH: Heterocyclic Compounds, 3-Ring, topoisomerase, MESH: Humans, biology, 010405 organic chemistry, Drug discovery, Chemistry, Topoisomerase, [SDV.SP]Life Sciences [q-bio]/Pharmaceutical sciences, 0104 chemical sciences, MESH: Quinazolines, MESH: Topoisomerase I Inhibitors, DNA Topoisomerases, Type I, Docking (molecular), Quinazolines, biology.protein, MESH: Pyrroles, Molecular Medicine, Topoisomerase I Inhibitors, Heterocyclic Compounds, 3-Ring, MESH: DNA Topoisomerases, Type I

Abstract

In search for a novel chemotype to develop topoisomerase I (Top1) inhibitors, the pyrazolo[1,5-a]quinazoline nucleus, structurally related to the indenoisoquinoline system precursor of well-known Top1 poisons, was variously decorated (i.e., a substituted phenyl ring at 2- or 3-position, a protonable side chain at 4- or 5-position), affording a number of Top1 inhibitors with cleavage patterns common to CPT and MJ-III-65. SARs data were rationalized by means of an advanced docking protocol. © 2013 American Chemical Society.

Published

2013

29. Shooting for selective druglike G-quadruplex binders: evidence for telomeric DNA damage and tumor cell death

Author

Angela Maria Rizzo, Luciana Marinelli, Sandro Cosconati, Stefano De Tito, Annamaria Biroccio, Bruno Pagano, Iolanda Fotticchia, Concetta Giancola, Ettore Novellino, Antonio Randazzo, Ilaria Lauri, Roberta Trotta, Sara Iachettini, Mariateresa Giustiniano, Cosconati, S., Rizzo, A., Trotta, Roberta, Pagano, Bruno, Iachettini, S., DE TITO, Stefano, Lauri, Ilaria, Fotticchia, Iolanda, Giustiniano, Mariateresa, Marinelli, Luciana, Giancola, Concetta, Novellino, Ettore, Biroccio, A., Randazzo, Antonio, AAVV, S., Cosconati, A., Rizzo, S., Iachettini, A., Biroccio, Cosconati, Sandro, Rizzo, A, Trotta, R, Pagano, B, Iachettini, S, De Tito, S, Lauri, I, Fotticchia, I, Giustiniano, M, Marinelli, L, Giancola, C, Novellino, E, Biroccio, A, and Randazzo, A.

Subjects

Senescence, Magnetic Resonance Spectroscopy, Stereochemistry, DNA damage, Fluorescent Antibody Technique, Antineoplastic Agents, Apoptosis, G-quadruplex, ligand, chemistry.chemical_compound, Structure-Activity Relationship, Drug Discovery, Structure–activity relationship, Humans, heterocyclic compounds, Cells, Cultured, Cellular Senescence, antitumor, Molecular Structure, Circular Dichroism, Cell Cycle Checkpoints, Fibroblasts, Telomere, Flow Cytometry, Small molecule, NMR, G-Quadruplexes, chemistry, Biochemistry, Duplex (building), Molecular Medicine, DNA, DNA Damage, HeLa Cells

Abstract

Targeting of DNA secondary structures, such as G-quadruplexes, is now considered an appealing opportunity for drug intervention in anticancer therapy. So far, efforts made in the discovery of chemotypes able to target G-quadruplexes mainly succeeded in the identification of a number of polyaromatic compounds featuring end-stacking binding properties. Against this general trend, we were persuaded that the G-quadruplex grooves can recognize molecular entities with better drug-like and selectivity properties. From this idea, a set of small molecules was identified and the structural features responsible for G-quadruplex recognition were delineated. These compounds were demonstrated to have enhanced affinity and selectivity for the G-quadruplex over the duplex structure. Their ability to induce selective DNA damage at telomeric level and to induction of apoptosis and senescence on tumor cells is herein experimentally proven. © 2012 American Chemical Society.

Published

2012

30. Synthesis and Biological Evaluation of CTP Synthetase Inhibitors as Potential Agents for the Treatment of African Trypanosomiasis

Author

Luciana Marinelli, Lucia Tamborini, Paola Conti, Leonardo Lo Presti, Michael P. Barrett, Andrea Pinto, Ettore Novellino, Pui E. Wong, Terry K. Smith, Sandro Cosconati, Maria C. Iannuzzi, Louise L. Major, Carlo De Micheli, Tamborini, L, Pinto, A, Smith, Tk, Major, Ll, Iannuzzi, Mc, Cosconati, Sandro, Marinelli, L, Novellino, E, Lo Presti, L, Wong, Pe, Barrett, Mp, De Micheli, C, Conti, P., Cosconati, S, Marinelli, Luciana, and Novellino, Ettore

Subjects

Trypanosoma, Trypanosoma brucei brucei, Biochemistry, Pyrazoline, Article, Isoxazoline, chemistry.chemical_compound, Drug Discovery, medicine, Humans, Carbon-Nitrogen Ligases, African trypanosomiasis, Enzyme Inhibitors, General Pharmacology, Toxicology and Pharmaceutics, CTP synthetase, Acivicin, Trypanocidal agent, Pharmacology, chemistry.chemical_classification, biology, Organic Chemistry, Isoxazoles, biology.organism_classification, medicine.disease, Trypanocidal Agents, In vitro, Amino acid, Molecular Docking Simulation, Trypanosomiasis, African, Enzyme, chemistry, biology.protein, Pyrazoles, Molecular Medicine, HeLa Cells

Abstract

Acivicin analogues with an increased affinity for CTP synthetase (CTPS) were designed as potential new trypanocidal agents. The inhibitory activity against CTPS can be improved by increasing molecular complexity, by inserting groups able to establish additional interactions with the binding pocket of the enzyme. This strategy has been pursued with the synthesis of α-amino-substituted analogues of Acivicin and N1-substituted pyrazoline derivatives. In general, there is direct correlation between the enzymatic activity and the invitro anti-trypanosomal efficacy of the derivatives studied here. However, this cannot be taken as a general rule, as other important factors may play a role, notably the ability of uptake/diffusion of the molecules into the trypanosomes. © 2012 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

Published

2012

31. Water-Soluble Pyrazolo[4,3-e][1,2,4]triazolo[1,5-c]pyrimidines as Human A(3) Adenosine Receptor Antagonists

Author

Baraldi PG, Saponaro G, Romagnoli R, Aghazadeh Tabrizi M, Baraldi S, Moorman AR, Cosconati S, Gessi S, Merighi S, Varani K, Borea PA, Preti D., DI MARO, SALVATORE, MARINELLI, LUCIANA, NOVELLINO, ETTORE, Baraldi, Pg, Saponaro, G, Romagnoli, R, Aghazadeh Tabrizi, M, Baraldi, S, Moorman, Ar, Cosconati, S, DI MARO, Salvatore, Marinelli, Luciana, Gessi, S, Merighi, S, Varani, K, Borea, Pa, Preti, D., Novellino, Ettore, Cosconati, Sandro, and Marinelli, L

Subjects

Aqueous solution, Pyrimidine, Molecular model, Chemistry, Stereochemistry, Medicinal chemistry, Adenosine receptor, chemistry.chemical_compound, Water soluble, Drug Discovery, Molecular Medicine, Moiety, Solubility, IC50

Abstract

A relevant problem of the pyrazolo[4,3-e][1,2,4]triazolo[1,5-c]pyrimidine nucleus, an attractive scaffold for the preparation of adenosine receptor antagonists, is the low water solubility. We originally functionalized the C 5 position with a salifiable 4-pyridylcarbamoyl moiety that conferred good water solubility at low pH ( 515, IC 50(hA 2B) > 5 μM) showed a solubility of 8 mg/mL at physiological pH and gave a stable aqueous system suitable for intravenous infusion. Molecular modeling studies were helpful in rationalizing the available structure-activity relationships and the selectivity profile of the new ligands. © 2012 American Chemical Society.

Published

2012

32. 3-Aryl-[1,2,4]triazino[4,3-a]benzimidazol-4(10H)-one: a novel template for the design of highly selective A2B adenosine receptor antagonists

Author

Barbara Cosimelli, Federico Da Settimo, Ettore Novellino, Salvatore Di Maro, Sabrina Taliani, Giovanni Greco, Simona Daniele, Claudia Martini, Anna Maria Marini, Silvia Salerno, Francesca Simorini, Maria Letizia Trincavelli, Elisabetta Barresi, Isabella Pugliesi, Luciana Marinelli, Concettina La Motta, Sandro Cosconati, Taliani, S., Pugliesi, I., Barresi, E., Simorini, F., Salerno, S., La Motta, C., Marini, A. M., Cosimelli, Barbara, Cosconati, S., DI MARO, Salvatore, Marinelli, Luciana, Daniele, S., Trincavelli, M. L., Greco, Giovanni, Novellino, Ettore, Martini, C., Da Settimo, F., Taliani, S, Pugliesi, I, Barresi, E, Simorini, F, Salerno, S, La Motta, C, Marini, Am, Cosimelli, B, Cosconati, Sandro, Marinelli, L, Daniele, S, Trincavelli, Ml, Greco, G, Novellino, E, and Martini, C

Subjects

Stereochemistry, Aryl, Chlorine atom, antagonist, Highly selective, Ring (chemistry), Adenosine receptor, chemistry.chemical_compound, pharmacology, Benzimidazoles, chemistry, Drug Discovery, Molecular Medicine, adenosine receptor, Selectivity, IC50

Abstract

In an effort to identify novel ligands possessing high affinity and selectivity for the A2B AR subtype, we further investigated the class of 3-aryl[1,2,4]triazino[4,3-a]benzimidazol-4(10H)-ones V, previously disclosed by us as selective A1 AR antagonists. Preliminary assays on a number of triazinobenzimidazoles derived from our "in-house" collection revealed that all the derivatives selected showed significant affinity at A 2B AR, no affinity at A3 AR, and various degrees of selectivity toward A1 and A2A ARs. Investigation of a new series featuring modified substituents at the 10-position (4′-chlorophenyl or phenylethyl groups), and a chlorine atom at the 7-position (X) of the triazinobenzimidazole nucleus, yielded highly potent and selective A 2B AR antagonists. The presence of a pendant 3-phenyl ring appears to hamper the interaction with A2A AR, conferring high A 2B/A2A AR selectivity. Derivative 13 (X = Cl, R = C 6H5) is the most potent and selective compound, with an IC50 of 3.10 nM at A2B AR and no affinity at A 1, A2A, and A3 ARs. © 2012 American Chemical Society.

Published

2012

33. Progresses in the pursuit of aldose reductase inhibitors: The structure-based lead optimization step

Author

Vita Maglio, Sara Angiuoli, Ettore Novellino, Federico Da Settimo, Mariateresa Giustiniano, Sandro Cosconati, Stefania Sartini, Salvatore Di Maro, Valeria La Pietra, Luciana Marinelli, Concettina La Motta, Anna Ramunno, Ramunno, A, Cosconati, Sandro, Sartini, S, Maglio, V, Angiuoli, S, La Pietra, V, DI MARO, Salvatore, Giustiniano, M, La Motta, C, Da Settimo, F, Marinelli, L, Novellino, E., Cosconati, S, LA PIETRA, Valeria, Giustiniano, Mariateresa, Marinelli, Luciana, and Novellino, Ettore

Subjects

Models, Molecular, medicine.medical_specialty, Diabetic neuropathy, Drug Evaluation, Preclinical, Aldose reductase, Inflammation, Pharmacology, Diabete, Fidarestat, Metastasis, Docking, Inhibitory Concentration 50, Structure-Activity Relationship, User-Computer Interface, Aldehyde Reductase, Diabetes mellitus, Internal medicine, Catalytic Domain, Drug Discovery, medicine, Enzyme Inhibitors, Receptor, Chemistry, Organic Chemistry, General Medicine, Aldose reductase inhibitors, medicine.disease, Endocrinology, Docking (molecular), Enzyme, medicine.symptom

Abstract

Aldose reductase (ALR2) is a crucial enzyme in the development of the major complications of diabetes mellitus. Very recently it has been demonstrated that the ARL2 inhibitor, fidarestat, significantly prevents inflammatory signals (TNF-α, LPS) that cause cancer (colon, breast, prostate and lung), metastasis, asthma, and other inflammatory diseases. Currently, fidarestat is in phase III clinical trial for diabetic neuropathy and was found to be safe. Thus the finding of novel, potent ARL2 inhibitors is today more than in the past in great demand as they can pave the way for a novel therapeutic approach for a number of diseases besides the diabetes. Herein, starting from the virtual screening-derived ALR2 inhibitor S12728 (1), a rational receptor-based lead optimization has been undertaken. The design and synthetic efforts here reported led to the discovery of several new compounds endowed with low micromolar/submicromolar activities. © 2012 Elsevier Masson SAS. All rights reserved.

Published

2012

34. State-of-the-art methodologies for the discovery and characterization of DNA G-quadruplex binders

Author

Luigi Petraccone, Francesco Saverio Di Leva, Antonio Randazzo, Bruno Pagano, Roberta Trotta, Valérie Gabelica, Sandro Cosconati, Luciana Marinelli, Stefano De Tito, Valeria La Pietra, Concetta Giancola, Ilaria Lauri, Ettore Novellino, Pagano, B, Cosconati, Sandro, Gabelica, V, Petraccone, L, De Tito, S, Marinelli, L, La Pietra, V, di Leva, F. S., Lauri, I, Trotta, R, Novellino, E, Giancola, C, Randazzo, A., Pagano, Bruno, Cosconati, S., Gabelica, V., Petraccone, Luigi, DE TITO, Stefano, Marinelli, Luciana, LA PIETRA, Valeria, Di Leva, Francesco Saverio, Lauri, Ilaria, Trotta, R., Novellino, Ettore, Giancola, Concetta, and Randazzo, Antonio

Subjects

Circular dichroism, Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, QUADRUPLEX, TELOMERE, Computational biology, Calorimetry, G-quadruplex, Ligands, Fluorescence, chemistry.chemical_compound, G-Quadruplex, Drug Discovery, Fluorescence Resonance Energy Transfer, Organic chemistry, Humans, DRUG, Pharmacology, Chemistry, Drug discovery, Circular Dichroism, Rational design, Isothermal titration calorimetry, Nuclear magnetic resonance spectroscopy, DNA, Isothermal titration calorimetry (ITC), Computational method, Circular dichroism (CD), Mass spectrometry (MS), G-Quadruplexes, Förster resonance energy transfer, Spectrometry, Fluorescence, Nuclear magnetic resonance (NMR)

Abstract

Nowadays, the molecular basis of interaction between low molecular weight compounds and biological macromolecules is the subject of numerous investigations aimed at the rational design of molecules with specific therapeutic applications. In the last decades, it has been demonstrated that DNA quadruplexes play a critical role in several biological processes both at telomeric and gene promoting levels thus providing a great stride in the discovery of ligands able to interact with such a biologically relevant DNA conformation. So far, a number of experimental and computational approaches have been successfully employed in order to identify new ligands and to characterize their binding to the DNA. The main focus of this review is the description of these methodologies, placing a particular emphasis on computational methods, isothermal titration calorimetry (ITC), mass spectrometry (MS), nuclear magnetic resonance (NMR), circular dichroism (CD) and fluorescence spectroscopies. © 2012 Bentham Science Publishers.

Published

2011

35. New 2-heterocyclyl-imidazo[2,1-i]purin-5-one derivatives as potent and selective human A3 adenosine receptor antagonists

Author

Giulia Saponaro, Katia Varani, Luciana Marinelli, Abdel Naser Zaid, Pier Giovanni Baraldi, Allan R. Moorman, Sandro Cosconati, Mojgan Aghazadeh Tabrizi, Ettore Novellino, Romeo Romagnoli, Salvatore Di Maro, Stefania Baraldi, Pier Andrea Borea, Delia Preti, Baraldi, Pg, Preti, D, Zaid, An, Saponaro, G, Tabrizi, Ma, Baraldi, S, Romagnoli, R, Moorman, Ar, Varani, K, Cosconati, Sandro, DI MARO, Salvatore, Marinelli, L, Novellino, E, Borea, Pa, Pier Giovanni, Baraldi, Delia, Preti, Abdel Naser, Zaid, Giulia, Saponaro, Mojgan Aghazadeh, Tabrizi, Stefania, Baraldi, Romeo, Romagnoli, Allan R., Moorman, Katia, Varani, Sandro, Cosconati, Marinelli, Luciana, Novellino, Ettore, and Pier Andrea, Borea

Subjects

Models, Molecular, Molecular model, Stereochemistry, Molecular Sequence Data, Adenosine A3 Receptor Antagonists, A3R antagonist, CHO Cells, Ligands, Receptor, Adenosine A2B, Transfection, Radioligand Assay, Structure-Activity Relationship, Cricetulus, Cricetinae, Drug Discovery, Cyclic AMP, Animals, Humans, Amino Acid Sequence, adenosine receptor, IC50, adenosine, Ligand, Chemistry, Receptor, Adenosine A3, Stereoisomerism, A3 ADENOSINE RECEPTOR, Affinities, Adenosine receptor, Purines, Molecular Medicine, Selectivity, Antagonism, Sequence Alignment

Abstract

A series of 4-allyl/benzyl-7,8-dihydro-8-methyl/ethyl-2-[(substituted) isoxazol/pyrazol-3/5-yl]-1H-imidazo[2,1-i]purin-5(4H)-ones has been synthesized and evaluated in radioligand binding assays to determine their affinities at the human A 1, A 2A, and A 3 adenosine receptors. Efficacy at the hA 2B AR and antagonism of selected ligands at the hA 3 AR were also assessed through cAMP experiments. All of the synthesized molecules exhibited high affinity at the hA 3 AR (K i values ranging from 1.46 to 44.8 nM), as well as remarkable selectivity versus A 1, A 2A, and A 2B AR subtypes. Compound (R)-4-allyl-8-ethyl-7,8-dihydro-2-(3-methoxy-1-methyl-1H- pyrazol-5-yl)-1H-imidazo[2,1-i]purin-5(4H)-one (R-33) was found to be the most potent and selective ligand of the series (K i hA 3 = 1.46 nM, K i hA 2A/K i hA 3 > 3425; IC 50 hA 2B/K i hA 3 > 3425; K i hA 1/K i hA 3 = 1729). Molecular modeling studies were helpful in rationalizing the available structure-activity relationships along with the selectivity profiles of the new series of ligands. © 2011 American Chemical Society.

Published

2011

36. Design, synthesis, and functionalization of dimeric peptides targeting chemokine receptor CXCR4

Author

Luciana Marinelli, Horst Kessler, Udo Schumacher, Oliver Demmer, Hans-Jürgen Wester, Sandro Cosconati, Eleni Gourni, Ingrid Dijkgraaf, Demmer, O., Dijkgraaf, I., Schumacher, U., Marinelli, Luciana, Cosconati, S., Gourni, E., Wester, H. J., Kessler, H., Demmer, O, Dijkgraaf, I, Schumacher, U, Marinelli, L, Cosconati, Sandro, Gourni, E, and Wester, Hj

Subjects

Models, Molecular, Receptors, CXCR4, Stereochemistry, Mice, Nude, Gadolinium, Plasma protein binding, Ligands, Peptides, Cyclic, chemistry.chemical_compound, Chemokine receptor, Heterocyclic Compounds, 1-Ring, Mice, Structure-Activity Relationship, Coordination Complexes, Translational research [ONCOL 3], Drug Discovery, Structure–activity relationship, DOTA, Animals, Tissue Distribution, Binding site, Receptor, Chelating Agents, Binding Sites, Chemistry, chemokine receptor, CXCR4, antagonists, cyclic peptides, PET tracer, Tissue engineering and pathology [NCMLS 3], Combinatorial chemistry, Docking (molecular), Drug Design, Positron-Emission Tomography, Molecular Medicine, Radiopharmaceuticals, Dimerization, Oligopeptides, Conjugate, Protein Binding

Abstract

The chemokine receptor CXCR4 is a critical regulator of inflammation and immune surveillance, and it is specifically implicated in cancer metastasis and HIV-1 infection. On the basis of the observation that several of the known antagonists remarkably share a C 2 symmetry element, we constructed symmetric dimers with excellent antagonistic activity using a derivative of a cyclic pentapeptide as monomer. To optimize the binding affinity, we investigated the influence of the distance between the monomers and the pharmacophoric sites in the synthesized constructs. The affinity studies in combination with docking computations support a two-site binding model. In a final step, 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid (DOTA) was introduced as chelator for (radio-)metals, thus allowing to exploit these compounds as a new group of CXCR4-binding peptidic probes for molecular imaging and endoradiotherapeutic purposes. Both the DOTA conjugates and some of their corresponding metal complexes retain good CXCR4 affinity, and one 68Ga labeled compound was studied as PET tracer. © 2011 American Chemical Society.

Published

2011

37. Identification of 5-arylidene-4-thiazolidinone derivatives endowed with dual activity as aldose reductase inhibitors and antioxidant agents for the treatment of diabetic complications

Author

Mario Cappiello, Umberto Mura, Ettore Novellino, Federico Da Settimo, Stefania Sartini, Sandro Cosconati, Rosanna Maccari, Rosaria Ottanà, Luciana Marinelli, Concettina La Motta, Marco Giglio, Antonella Del Corso, Ottana, R, Maccari, R, Giglio, M, Del Corso, A, Cappiello, M, Mura, U, Cosconati, Sandro, Marinelli, L, Novellino, E, Sartini, S, La Motta, C, Da Settimo, F., Rosaria, Ottan, Rosanna, Maccari, Marco, Giglio, Antonella Del, Corso, Mario, Cappiello, Umberto, Mura, Sandro, Cosconati, Marinelli, Luciana, Novellino, Ettore, Stefania, Sartini, Concettina La, Motta, and Federico Da, Settimo

Subjects

Diabetes mellitu, Antioxidant, Antioxidant agent, medicine.medical_treatment, Aldose reductase, Acetates, medicine.disease_cause, Antioxidants, Diabetes Complications, Structure-Activity Relationship, Diabetes mellitus, Aldehyde Reductase, 5-arylidene-4-thiazolidinones, Molecular docking, Drug Discovery, 5-arylidene-4- thiazolidinone, medicine, Structure–activity relationship, Animals, Humans, Enzyme Inhibitors, Pharmacology, chemistry.chemical_classification, biology, Organic Chemistry, General Medicine, medicine.disease, Molecular Docking Simulation, Oxidative Stress, Enzyme, chemistry, Biochemistry, Enzyme inhibitor, biology.protein, Cattle, Thiazolidinediones, Oxidative stress

Abstract

In continuing the search for more effective 5-arylidene-4-thiazolidinones as aldose reductase inhibitors, a new set of suitably substituted compounds (4, 5 and 8) was explored. Acetic acids 5, particularly 5a and 5h, proved to be interesting inhibitors of the enzyme as well as excellent antioxidant agents that are potentially able to counteract the oxidative stress associated with both diabetic complications as well as other pathologies. Molecular docking experiments supported SAR studies. © 2011 Elsevier Masson SAS. All rights reserved.

Published

2011

38. Novel N(2)-Substituted Pyrazolo[3,4-d]pyrimidine Adenosine A(3) Receptor Antagonists: Inhibition of A(3)-Mediated Human Glioblastoma Cell Proliferation (dagger)

Author

Luciana Marinelli, Concettina La Motta, Claudia Martini, Giovanni Greco, Sandro Cosconati, Federico Da Settimo, L. Mugnaini, Simona Daniele, Barbara Cosimelli, Anna Maria Marini, Silvia Salerno, Osele Ciampi, Francesca Simorini, Maria Letizia Trincavelli, Sabrina Taliani, Vittorio Limongelli, Ettore Novellino, Taliani, S., La Motta, C., Mugnaini, L., Simorini, F., Salerno, S., Marini, A. M., Da Settimo, F., Cosconati, S., Cosimelli, Barbara, Greco, Giovanni, Limongelli, Vittorio, Marinelli, Luciana, Novellino, Ettore, Ciampi, O., Daniele, S., Trincavelli, M. L., Martini, C., Taliani, S, La Motta, C, Mugnaini, L, Simorini, F, Salerno, S, Marini, Am, Da Settimo, F, Cosconati, Sandro, Cosimelli, B, Greco, G, Limongelli, V, Marinelli, L, Novellino, E, Ciampi, O, Daniele, S, and Trincavelli, Ml

Subjects

Agonist, MAPK/ERK pathway, Models, Molecular, Pyrimidine, medicine.drug_class, Adenosine A3 Receptor Antagonists, Antineoplastic Agents, CHO Cells, Binding, Competitive, chemistry.chemical_compound, Radioligand Assay, Structure-Activity Relationship, Cricetulus, Adenosine A3 Receptor Agonists, Cell Line, Tumor, Cricetinae, Drug Discovery, medicine, Cyclic AMP, Animals, Humans, Phosphorylation, Cell Proliferation, Mitogen-Activated Protein Kinase 1, Glioblastoma cell, Mitogen-Activated Protein Kinase 3, Kinase, Chemistry, Molecular biology, Adenosine, Enzyme Activation, Pyrimidines, Biochemistry, Chemotherapy, Adjuvant, Molecular Medicine, Pyrazoles, Glioblastoma, Intracellular, medicine.drug

Abstract

Adenosine induces glioma cell proliferation by means of an antiapoptotic effect, which is blocked by cotreatment with selective A(3) AR antagonists. In this study, a novel series of N(2)-substituted pyrazolo[3,4-d]pyrimidines 2a-u was developed as highly potent and selective A(3) AR antagonists. The most performing compounds were derivatives 2a (R(1) = CH(3) and R(2) = COC(6)H(5); K(i) 334, 728, and 0.60 nM at the human A(1), A(2A), and A(3) ARs, respectively) and 2b (R(1) = CH(3) and R(2) = COC(6)H(4)-4-OCH(3); K(i) 1037, 3179, and 0.18 nM at the human A(1), A(2A), and A(3) ARs, respectively), which counteracted the effect of the A(3) AR agonists Cl-IB-MECA and IB-MECA on human glioma U87MG cell proliferation. This effect was concentration-dependent, with IC(50) values comparable to A(3) AR binding affinity values of 2a and 2b, thereby suggesting that their effects were receptor-mediated. Furthermore, the antiproliferative activity of the new compounds was demonstrated to be mediated by the block of A(3) AR agonist activation of intracellular kinases ERK 1/2.

Published

2010

39. Pursuing aldose reductase inhibitors through in situ cross-docking and similarity-based virtual screening

Author

Federico Da Settimo, Sandro Cosconati, Stefania Sartini, Ettore Novellino, Arthur J. Olson, Luciana Marinelli, Concettina La Motta, Cosconati, Sandro, Marinelli, L, La Motta, C, Sartini, S, Da Settimo, F, Olson, Aj, and Novellino, E.

Subjects

Models, Molecular, chemistry.chemical_classification, Virtual screening, Aldose reductase, Molecular model, biology, Protein Conformation, Chemistry, Drug Evaluation, Preclinical, Aldose reductase inhibitors, Ligands, Inhibitory Concentration 50, User-Computer Interface, Enzyme, Biochemistry, Aldehyde Reductase, Enzyme inhibitor, Drug Discovery, biology.protein, Humans, Molecular Medicine, Major complication, Enzyme Inhibitors

Abstract

Aldose reductase (ALR2) is a critical enzyme in the development of the major complications of diabetes mellitus. Herein, new molecular entities active against ALR2 were discovered through an integrated receptor- and ligand-based virtual screening campaign. Twelve candidates were found to inhibit this enzyme in the micromolar range including two ligands having an IC50 below 3 μM. Six new compounds, structurally unrelated to the known ARIs, have been identified, opening up opportunity for lead optimization. © 2009 American Chemical Society.

Published

2009

40. Specific Targeting of Highly Conserved Residues in the HIV-1 Reverse Transcriptase Primer Grip Region. 2. Stereoselective Interaction to Overcome the Effects of Drug Resistant Mutations

Author

Gianluca Giorgi, Samantha Zanoli, Michela Di Mattia, Anna Ramunno, Giuseppe Campiani, Stefania Butini, Sandra Gemma, Alberto Bergamini, Salvatore Sanna Coccone, Giuseppe Borrelli, Sandro Cosconati, Luciana Marinelli, Margherita Brindisi, Alberta Samuele, Bruno Galletti, Ettore Novellino, Giovanni Maga, Silvana Lalli, Butini, S, Brindisi, M, Cosconati, Sandro, Marinelli, L, Borrelli, G, Coccone, S, Ramunno, A, Campiani, G, Novellino, E, Zanoli, S, Samuele, A, Giorgi, G, Bergamini, A, Di Mattia, M, Lalli, S, Galletti, B, Gemma, S, Maga, G., Butini, S., Brindisi, M., Cosconati, S., Marinelli, Luciana, Borrelli, G., Coccone, S. S., Ramunno, A., Campiani, G., Novellino, Ettore, Zanoli, S., Samuele, A., Giorgi, G., Bergamini, A., Di Mattia, M., Lalli, S., Galletti, B., and Gemma, S.

Subjects

Models, Molecular, Settore MED/09 - Medicina Interna, Anti-HIV Agents, Mutant, Drug Resistance, medicine.disease_cause, law.invention, Structure-Activity Relationship, law, Drug Discovery, medicine, Humans, Conserved Sequence, chemistry.chemical_classification, Mutation, Wild type, Stereoisomerism, Nucleotidyltransferase, Reverse transcriptase, HIV Reverse Transcriptase, Enzyme, chemistry, Biochemistry, Recombinant DNA, HIV-1, Molecular Medicine, Reverse Transcriptase Inhibitors, Primer (molecular biology)

Abstract

Starting from the prototypic compound 4, we describe new, potent, and broad-spectrum pyrrolobenzo(py-rido)oxazepinones antivirals. A biochemical and enzymological investigation was performed for defining their mechanism of inhibition at either recombinant HIV-1 RT wild type and non-nucleoside reverse transcriptase inhibitors (NNRTIs)-resistant mutants. For the novel compounds (S)-(+)-5 and (S)-(-)-7,a clear-cut stereoselective mechanism of enzyme inhibition was found. Molecular modeling studies were performed for revealing the underpinnings of this behavior. © 2009 American Chemical Society.

Published

2009

41. Identification of anxiolytic/nonsedative agents among indol-3- ylglyoxylamides acting as functionally selective agonists at the γ-aminobutyric acid-A (GABAA) α2 benzodiazepine receptor

Author

Marina Montali, Giovanni Greco, Sabrina Taliani, Federico Da Settimo, Silvia Trasciatti, B Cosimelli, Barbara Costa, Luciana Marinelli, Concettina La Motta, F Salvetti, Anna Maria Marini, Francesca Simorini, Silvia Salerno, Gianluca L'Abbate, Sandro Cosconati, Ettore Novellino, Claudia Martini, Taliani, S, Cosimelli, B, Da Settimo, F, Marini, Am, La Motta, C, Simorini, F, Salerno, S, Novellino, E, Greco, G, Cosconati, Sandro, Marinelli, L, Salvetti, F, L'Abbate, G, Trasciatti, S, Montali, M, Costa, B, and Martini, C.

Subjects

Agonist, Models, Molecular, Benzodiazepine, Binding Sites, Molecular Structure, Chemistry, medicine.drug_class, GABAA receptor, Stereochemistry, Alpha (ethology), Stereoisomerism, Anxiolytic, gamma-Aminobutyric acid, Structure-Activity Relationship, Anti-Anxiety Agents, Models, Chemical, Drug Discovery, medicine, Molecular Medicine, Structure–activity relationship, Computer Simulation, GABA-A Receptor Agonists, Receptor, medicine.drug

Abstract

Anxioselective agents may be identified among compounds binding selectively to the alpha(2)beta(x)gamma(2) subtype of the gamma-aminobutyric acid-A (GABA(A))/central benzodiazepine receptor (BzR) complex and behaving as agonists or among compounds binding with comparable potency to various BzR subtypes but eliciting agonism only at the alpha(2)beta(x)gamma(2) receptor. Because of subtle steric differences among BzR subtypes, the latter approach has proved much more successful. A biological screening within the class of indol-3-ylglyoxylamides 1-3 allowed us to identify compounds 1c and 2b as potential anxiolytic/nonsedative agents showing alpha(2) selective efficacy in vitro and anxioselective effects in vivo. According to molecular modeling studies, and consistently with SARs accumulated in the past decade, 5-NO(2)- and 5-H-indole derivatives would preferentially bind to BzR by placing the indole ring in the L(Di) and the L(2) receptor binding sites, respectively.

Published

2009

42. Characterizing the 1,4-dihydropyridines binding interactions in the L-type Ca2+ channel: Model construction and docking calculations

Author

Luciana Marinelli, Sandro Cosconati, Ettore Novellino, Antonio Lavecchia, Cosconati, Sandro, Marinelli, L, Lavecchia, A, Novellino, E., S., Cosconati, Marinelli, Luciana, Lavecchia, Antonio, and Novellino, Ettore

Subjects

Models, Molecular, Dihydropyridines, Calcium Channels, L-Type, Molecular model, Stereochemistry, Molecular Sequence Data, KcsA potassium channel, Ligands, Structure-Activity Relationship, calcium antagonists, DOCK, Drug Discovery, Humans, Molecule, L-type calcium channel, Amino Acid Sequence, Binding Sites, Molecular Structure, Chemistry, Stereoisomerism, Homology modeling, Depolarization, Calcium Channel Blockers, Membrane, Docking (molecular), docking, Biophysics, Molecular Medicine, Protein Binding

Abstract

L-type Ca2+ channels (LCC) are membrane heteromultimeric proteins that allow the selective entrance of Ca2+ ions into excitable cells upon membrane depolarization. Despite the large amount of compounds (1,4-dihydropyridines, phenylalkylamines, and benzothiazepines) that impede the passage of Ca2+ ions through the channel, it is still not clear how these molecules bind to LCC at an atomic level. In this study, a 3D model of the central pore of LCC was constructed using the X-ray structure of the KcsA K+ channel as template. The resulting LCC model was then used to dock nine different DHPs to shed light on their binding mode. The accordance between the developed model and several experimental data gives us the confidence to propose our model as a valuable platform for future studies aimed at the identification of new potent and LCC-selective ligands. © 2007 American Chemical Society.

Published

2007