Your search keyword '"Camodeca C"' showing total 36 results

1. Synthesis and antiangiogenic activity study of new hop chalcone Xanthohumol analogues

Author

Nuti, E, Bassani, B, Camodeca, C, Rosalia, L, Cantelmo, A, Gallo, C, Baci, D, Bruno, A, Orlandini, E, Nencetti, S, Noonan, D, Albini, A, Rossello, A, Nuti E, Bassani B, Camodeca C, Rosalia L, Cantelmo A, Gallo C, Baci D, Bruno A, Orlandini E, Nencetti S, Noonan DM, Albini A, Rossello A, Nuti, E, Bassani, B, Camodeca, C, Rosalia, L, Cantelmo, A, Gallo, C, Baci, D, Bruno, A, Orlandini, E, Nencetti, S, Noonan, D, Albini, A, Rossello, A, Nuti E, Bassani B, Camodeca C, Rosalia L, Cantelmo A, Gallo C, Baci D, Bruno A, Orlandini E, Nencetti S, Noonan DM, Albini A, and Rossello A

Abstract

Angiogenesis induction is a hallmark of cancer. Antiangiogenic properties of Xanthohumol (XN), a naturally occurring prenylated chalcone from hops, have been widely reported. Here we describe the synthesis and study the antiangiogenic activity in vitro of a series of XN derivatives, where different substituents on the B-ring of the chalcone scaffold were inserted. The new XN derivatives inhibited human umbilical-vein endothelial cell (HUVEC) proliferation, adhesion, migration, invasion and their ability to form capillary-like structures in vitro at 10 mu M concentration. The preliminary results indicate that the phenolic OH group in R, present in natural XN, is not necessary for having antiangiogenic activity. In fact, the most effective compound from this series, 13, was characterized by a para-methoxy group in R and a fluorine atom in R-2 on B-ring. This study paves the way for future development of synthetic analogues of XN to be used as cancer angiopreventive and chemopreventive agents

Published

2017

2. N-O-Isopropyl Sulfonamido-Based Hydroxamates as Matrix Metalloproteinase Inhibitors: Hit Selection and in Vivo Antiangiogenic Activity

Author

Nuti, E, Cantelmo, A, Gallo, C, Bruno, A, Bassani, B, Camodeca, C, Tuccinardi, T, Vera, L, Orlandini, E, Nencetti, S, Stura, E, Martinelli, A, Dive, V, Albini, A, Rossello, A, Nuti E, Cantelmo AR, Gallo C, Bruno A, Bassani B, Camodeca C, Tuccinardi T, Vera L, Orlandini E, Nencetti S, Stura EA, Martinelli A, Dive V, Albini A, Rossello A, Nuti, E, Cantelmo, A, Gallo, C, Bruno, A, Bassani, B, Camodeca, C, Tuccinardi, T, Vera, L, Orlandini, E, Nencetti, S, Stura, E, Martinelli, A, Dive, V, Albini, A, Rossello, A, Nuti E, Cantelmo AR, Gallo C, Bruno A, Bassani B, Camodeca C, Tuccinardi T, Vera L, Orlandini E, Nencetti S, Stura EA, Martinelli A, Dive V, Albini A, and Rossello A

Abstract

Matrix metalloproteinases (MMPs) have been shown to be involved in tumor-induced angiogenesis. In particular, MMP-2, MMP-9, and MMP-14 have been reported to be crucial for tumor angiogenesis and the formation of metastasis, thus becoming attractive targets in cancer therapy. Here, we report our optimization effort to identify novel N-isopropoxy-arylsulfonamide hydroxamates with improved inhibitory activity toward MMP-2, MMP-9, and MMP-14 with respect to the previously discovered compound 1. A new series of hydroxamates was designed, synthesized, and tested for their antiangiogenic activity using in vitro assays with human umbilical vein endothelial cells (HUVECs). A nanomolar MMP-2, MMP-9, and MMP-14 inhibitor was identified, compound 3, able to potently inhibit angiogenesis in vitro and also in vivo in the matrigel sponge assay in mice. Finally, X-ray crystallographic and docking studies were conducted for compound 3 in order to investigate its binding mode to MMP-9 and MMP-14.

Published

2015

3. Development of antitubercular compounds based on a 4-quinolylhydrazone scaffold. Further structure-activity relationship studies

Author

Gemma, S, Savini, L, Altarelli, M, Tripaldi, P, Chiasserini, L, Coccone, S, Kumar, V, Camodeca, C, Campiani, G, Novellino, E, Clarizio, Sandra, Delogu, Giovanni, Butini, S., Delogu, Giovanni (ORCID:0000-0003-0182-8267), Gemma, S, Savini, L, Altarelli, M, Tripaldi, P, Chiasserini, L, Coccone, S, Kumar, V, Camodeca, C, Campiani, G, Novellino, E, Clarizio, Sandra, Delogu, Giovanni, Butini, S., and Delogu, Giovanni (ORCID:0000-0003-0182-8267)

Abstract

A series of 4-quinolylhydrazones was synthesized and tested in vitro against Mycobacterium tuberculosis. At a concentration of 6.25microg/mL, most of the newly synthesized compounds displayed 100% inhibitory activity against M. tuberculosis in cellular assays. Further screening allowed the identification of very potent antitubercular agents. Compound 4c was also tested in a time-course experiment and against mtb clinical isolates, displaying interesting results.

Published

2009

4. Synthesis and antiangiogenic activity study of new hop chalcone Xanthohumol analogues

Author

Susanna Nencetti, Caterina Camodeca, Barbara Bassani, A.R. Cantelmo, Armando Rossello, Denisa Baci, Elisabetta Orlandini, Elisa Nuti, Douglas M. Noonan, Adriana Albini, Antonino Bruno, Cristina Gallo, Lea Rosalia, Nuti, E, Bassani, B, Camodeca, C, Rosalia, L, Cantelmo, A, Gallo, C, Baci, D, Bruno, A, Orlandini, E, Nencetti, S, Noonan, D, Albini, A, and Rossello, A

Subjects

0301 basic medicine, Chalcone, Xanthohumol analogues, Prenylated chalcones, Antiangiogenic activity, Chemopreventive agents, Stereochemistry, Angiogenesis, Prenylated chalcones, Neovascularization, Physiologic, Angiogenesis Inhibitors, Apoptosis, Antiangiogenic activity, Chemopreventive agents, Xanthohumol analogues, Pharmacology, Drug Discovery3003 Pharmaceutical Science, Organic Chemistry, Hop (networking), Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Movement, Drug Discovery, Cell Adhesion, Human Umbilical Vein Endothelial Cells, Humans, Structure–activity relationship, Cell adhesion, Cells, Cultured, Cell Proliferation, Flavonoids, Propiophenones, Dose-Response Relationship, Drug, Molecular Structure, Cell growth, General Medicine, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Xanthohumol

Abstract

Angiogenesis induction is a hallmark of cancer. Antiangiogenic properties of Xanthohumol (XN), a naturally occurring prenylated chalcone from hops, have been widely reported. Here we describe the synthesis and study the antiangiogenic activity in vitro of a series of XN derivatives, where different substituents on the B-ring of the chalcone scaffold were inserted. The new XN derivatives inhibited human umbilical-vein endothelial cell (HUVEC) proliferation, adhesion, migration, invasion and their ability to form capillary-like structures in vitro at 10 μM concentration. The preliminary results indicate that the phenolic OH group in R, present in natural XN, is not necessary for having antiangiogenic activity. In fact, the most effective compound from this series, 13 , was characterized by a para-methoxy group in R and a fluorine atom in R 2 on B-ring. This study paves the way for future development of synthetic analogues of XN to be used as cancer angiopreventive and chemopreventive agents.

Published

2017

5. Development of antitubercular compounds based on a 4-quinolylhydrazone scaffold. Further structure–activity relationship studies

Author

Salvatore Sanna Coccone, Luisa Chiasserini, Ettore Novellino, Maria Altarelli, Sandra Gemma, Caterina Camodeca, Stefania Butini, Giuseppe Campiani, Vinod Kumar, Giovanni Delogu, Luisa Savini, Pierangela Tripaldi, Sandra Clarizio, Gemma, S., Savini, L., Altarelli, M., Tripaldi, P., Chiasserini, L., Coccone, S. S., Kumar, V., Camodeca, C., Campiani, G., Novellino, Ettore, Clarizio, S., Delogu, G., and Butini, S.

Subjects

Tuberculosis, Clinical Biochemistry, Antitubercular Agents, Pharmaceutical Science, Microbial Sensitivity Tests, Biochemistry, Chemical synthesis, Settore MED/07 - MICROBIOLOGIA E MICROBIOLOGIA CLINICA, Cell Line, Cercopithecus aethiops, Mycobacterium tuberculosis, Structure-Activity Relationship, Chlorocebus aethiops, Drug Discovery, medicine, Animals, Structure–activity relationship, Cytotoxicity, Vero Cells, Molecular Biology, Antibacterial agent, biology, Chemistry, Organic Chemistry, Hydrazones, biology.organism_classification, medicine.disease, In vitro, Molecular Medicine, Bacteria

Abstract

A series of 4-quinolylhydrazones was synthesized and tested in vitro against Mycobacterium tuberculosis. At a concentration of 6.25microg/mL, most of the newly synthesized compounds displayed 100% inhibitory activity against M. tuberculosis in cellular assays. Further screening allowed the identification of very potent antitubercular agents. Compound 4c was also tested in a time-course experiment and against mtb clinical isolates, displaying interesting results.

Published

2009

6. N-O-Isopropyl Sulfonamido-Based Hydroxamates as Matrix Metalloproteinase Inhibitors: Hit Selection and in Vivo Antiangiogenic Activity

Author

Adriana Albini, Antonino Bruno, Cristina Gallo, Barbara Bassani, Laura Vera, Enrico A. Stura, Vincent Dive, Armando Rossello, Tiziano Tuccinardi, Caterina Camodeca, Susanna Nencetti, Adriano Martinelli, Anna Rita Cantelmo, Elisabetta Orlandini, Elisa Nuti, Nuti, E, Cantelmo, A, Gallo, C, Bruno, A, Bassani, B, Camodeca, C, Tuccinardi, T, Vera, L, Orlandini, E, Nencetti, S, Stura, E, Martinelli, A, Dive, V, Albini, A, and Rossello, A

Subjects

Matrix metalloproteinase inhibitor, Angiogenesis, Cell Survival, Angiogenesis Inhibitors, Apoptosis, Matrix metalloproteinase, Matrix Metalloproteinase Inhibitors, Crystallography, X-Ray, Hydroxamic Acids, Mice, Structure-Activity Relationship, In vivo, Cell Movement, Drug Discovery, Human Umbilical Vein Endothelial Cells, Matrix Metalloproteinase 14, Structure–activity relationship, Animals, Humans, Matrigel, Sulfonamides, Chemistry, Angiogenesis Inhibitors/chemical synthesis/*chemistry/pharmacology Animals Apoptosis/drug effects Cell Movement/drug effects Cell Survival/drug effects Crystallography, X-Ray Human Umbilical Vein Endothelial Cells/cytology/drug effects/physiology Humans Hydroxamic Acids/chemical synthesis/*chemistry/pharmacology Matrix Metalloproteinase 14/chemistry/metabolism Matrix Metalloproteinase 2/chemistry/metabolism Matrix Metalloproteinase 9/chemistry/metabolism Matrix Metalloproteinase Inhibitors/chemical synthesis/*chemistry/pharmacology Mice Molecular Docking Simulation Stereoisomerism Structure-Activity Relationship Sulfonamides/chemical synthesis/*chemistry/pharmacology, Stereoisomerism, In vitro, Molecular Docking Simulation, Biochemistry, Matrix Metalloproteinase 9, Docking (molecular), Molecular Medicine, Matrix Metalloproteinase 2

Abstract

Matrix metalloproteinases (MMPs) have been shown to be involved in tumor-induced angiogenesis. In particular, MMP-2, MMP-9, and MMP-14 have been reported to be crucial for tumor angiogenesis and the formation of metastasis, thus becoming attractive targets in cancer therapy. Here, we report our optimization effort to identify novel N-isopropoxy-arylsulfonamide hydroxamates with improved inhibitory activity toward MMP-2, MMP-9, and MMP-14 with respect to the previously discovered compound 1. A new series of hydroxamates was designed, synthesized, and tested for their antiangiogenic activity using in vitro assays with human umbilical vein endothelial cells (HUVECs). A nanomolar MMP-2, MMP-9, and MMP-14 inhibitor was identified, compound 3, able to potently inhibit angiogenesis in vitro and also in vivo in the matrigel sponge assay in mice. Finally, X-ray crystallographic and docking studies were conducted for compound 3 in order to investigate its binding mode to MMP-9 and MMP-14.

Published

2015

7. Selective arylsulfonamide inhibitors of ADAM-17: hit optimization and activity in ovarian cancer cell models

Author

F Casalini, Ettore Novellino, Salvatore Santamaria, Silvano Ferrini, Marina Fabbi, Elisabetta Orlandini, Elisa Nuti, Susanna Nencetti, Armando Rossello, Luciana Marinelli, Caterina Camodeca, Valeria La Pietra, Grazia Carbotti, Nuti, E., Casalini, F., Santamaria, S., Fabbi, M., Carbotti, G., Ferrini, S., Marinelli, Luciana, LA PIETRA, Valeria, Novellino, Ettore, Camodeca, C., Orlandini, E., Nencetti, S., and Rossello, A.

Subjects

Models, Molecular, Cell Survival, Cell, ADAM17 Protein, Crystallography, X-Ray, Hydroxamic Acids, Cell Movement, Activated-Leukocyte Cell Adhesion Molecule, Cell Line, Tumor, Drug Discovery, medicine, Humans, Enzyme Inhibitors, ALCAM, Ovarian Neoplasms, Sulfonamides, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, In vitro toxicology, Biological activity, medicine.disease, In vitro, Protein Structure, Tertiary, carbohydrates (lipids), ADAM Proteins, medicine.anatomical_structure, Models, Chemical, Cell culture, Immunology, Cancer research, Molecular Medicine, Female, Ovarian cancer, Protein Binding

Abstract

Activated leukocyte cell adhesion molecule (ALCAM) is expressed at the surface of epithelial ovarian cancer (EOC) cells and is released in a soluble form (sALCAM) by ADAM-17-mediated shedding. This process is relevant to EOC cell motility and invasiveness, which is reduced by inhibitors of ADAM-17. In addition, ADAM-17 plays a key role in EGFR signaling and thus may represent a useful target in anticancer therapy. Herein we report our hit optimization effort to identify potent and selective ADAM-17 inhibitors, starting with previously identified inhibitor 1. A new series of secondary sulfonamido-based hydroxamates was designed and synthesized. The biological activity of the newly synthesized compounds was tested in vitro on isolated enzymes and human EOC cell lines. The optimization process led to compound 21, which showed an IC50 of 1.9 nM on ADAM-17 with greatly increased selectivity. This compound maintained good inhibitory properties on sALCAM shedding in several in vitro assays.

Published

2013

8. Mimicking the intramolecular hydrogen bond: synthesis, biological evaluation, and molecular modeling of benzoxazines and quinazolines as potential antimalarial agents

Author

Annette Habluetzel, Ettore Novellino, Emanuele Gabellieri, Gagan Kukreja, Isabella Fiorini, Stefania Butini, Roberta Gualdani, Luisa Savini, Sandra Gemma, Simone Brogi, Caterina Camodeca, Stefania Lamponi, Donatella Taramelli, Sanil Kunjir, Margherita Brindisi, Massimo Valoti, Gianluca Bartolommei, Giuseppe Campiani, Rowena E. Martin, Leonardo Lucantoni, Maria Rosa Moncelli, Francesco Tadini-Buoninsegni, Robert L. Summers, Nicoletta Basilico, Gemma, S., Camodeca, C., Brindisi, M., Brogi, S., Kukreja, G., Kunjir, S., Gabellieri, E., Lucantoni, L., Habluetzel, A., Taramelli, D., Basilico, N., Gualdani, R., Tadini Buoninsegni, F., Bartolommei, G., Moncelli, M. R., Martin, R. E., Summers, R. L., Lamponi, S., Savini, L., Fiorini, I., Valoti, M., Novellino, Ettore, Campiani, G., and Butini, S.

Subjects

Models, Molecular, Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, Molecular model, Stereochemistry, Amodiaquine, Cell Line, chemistry.chemical_compound, Antimalarials, Mice, parasitic diseases, Drug Discovery, medicine, Animals, Humans, Plasmodium berghei, Antimalarial Agent, biology, Chemistry, Hydrogen bond, Molecular Mimicry, Plasmodium falciparum, Hydrogen Bonding, biology.organism_classification, Benzoxazines, Intramolecular force, Quinazolines, Molecular Medicine, Febrifugine, medicine.drug

Abstract

The intramolecular hydrogen bond formed between a protonated amine and a neighboring H-bond acceptor group in the side chain of amodiaquine and isoquine is thought to play an important role in their antimalarial activities. Here we describe isoquine-based compounds in which the intramolecular H-bond is mimicked by a methylene linker. The antimalarial activities of the resulting benzoxazines, their isosteric tetrahydroquinazoline derivatives, and febrifugine-based 1,3-quinazolin-4-ones were examined in vitro (against Plasmodium falciparum ) and in vivo (against Plasmodium berghei ). Compounds 6b,c caused modest inhibition of chloroquine transport via the parasite's "chloroquine resistance transporter" (PfCRT) in a Xenopus laevis oocyte expression system. In silico predictions and experimental evaluation of selected drug-like properties were also performed on compounds 6b,c. Compound 6c emerged from this work as the most promising analogue of the series; it possessed low toxicity and good antimalarial activity when administered orally to P. berghei -infected mice.

Published

2012

9. From Waste Vegetable Oil to a Green Compatibilizer for HDPE/PA6 Blends.

Author

Cappello M, Strangis G, Cinelli P, Camodeca C, Filippi S, Polacco G, and Seggiani M

Abstract

When properly compatibilized, the blending of polyethylene (PE) and polyamide (PA) leads to materials that combine low prices, suitable processability, impact resistance, and attractive mechanical properties. Moreover, the possibility of using these polymers without prior separation may be a suitable opportunity for their recycling. In this work, the use of an epoxidized waste vegetable oil (EWVO) was investigated as a green compatibilizer precursor (CP) for the reactive blending of a high-density PE (HDPE) with a polyamide-6 (PA6). EWVO was synthesized from waste vegetable cooking oil (WVO) using ion-exchange resin (Amberlite) as a heterogeneous catalyst. HDPE/PA6 blends were produced with different weight ratios (25/75, 75/25, 85/15) and amounts of EWVO (1, 2, 5 phr). Samples with WVO or a commercial fossil-based CP were also prepared for comparison. All the blends were characterized by scanning electron microscopy (SEM), differential scanning calorimetry (DSC), rheology, and mechanical tests. In the case of HDPE/PA6 75/25 and 85/15 blends, the addition of EWVO at 2 phr showed a satisfactory compatibilizing effect, thus yielding a material with improved mechanical properties with respect to the blend without compatibilizer. On the contrary, the HDPE/PA6 25/75 ratio yielded a material with a high degree of crosslinking that could not be further processed or characterized. In conclusion, the results showed that EWVO had a suitable compatibilizing effect in HDPE/PA6 blends with high HDPE content, while it resulted in unsuitable for blends with high content of PA6.

Published

2023

10. New Hybrid Compounds Incorporating Natural Products as Multifunctional Agents against Alzheimer's Disease.

Author

Ciccone L, Camodeca C, Tonali N, Barlettani L, Rossello A, Fruchart Gaillard C, Kaffy J, Petrarolo G, La Motta C, Nencetti S, and Orlandini E

Abstract

A series of new hybrid derivatives 1a - c , 2a - c , 3a - c , 4a - c , 5a - c , inspired by nature, were synthesized and studied as multifunctional agents for the treatment of Alzheimer's disease (AD). These compounds were designed to merge together the trifluoromethyl benzyloxyaminic bioactive moiety, previously identified, with different acids available in nature. The ability of the synthesized compounds to chelate biometals, such as Cu 2+ , Zn 2+ and Fe 2+ , was studied by UV-Vis spectrometer, and through a preliminary screening their antioxidant activity was evaluated by DPPH. Then, selected compounds were tested by in vitro ABTS free radical method and ex vivo rat brain TBARS assay. Compounds 2a - c , combining the strongest antioxidant and biometal chelators activities, were studied for their ability to contrast Aβ 1-40 fibrillization process. Finally, starting from the promising profile obtained for compound 2a , we evaluated if it could be able to induce a positive cross-interaction between transthyretin (TTR) and Aβ in presence and in absence of Cu 2+ .

Published

2023

11. Resveratrol-like Compounds as SIRT1 Activators.

Author

Ciccone L, Piragine E, Brogi S, Camodeca C, Fucci R, Calderone V, Nencetti S, Martelli A, and Orlandini E

Subjects

Humans, Resveratrol pharmacology, Sirtuin 1 metabolism, Hydrogen Peroxide pharmacology, Oxidative Stress, Human Umbilical Vein Endothelial Cells metabolism, Sirtuins metabolism, Stilbenes pharmacology

Abstract

The sirtuin 1 (SIRT1) activator resveratrol has emerged as a promising candidate for the prevention of vascular oxidative stress, which is a trigger for endothelial dysfunction. However, its clinical use is limited by low oral bioavailability. In this work, we have applied a previously developed computational protocol to identify the most promising derivatives from our in-house chemical library of resveratrol derivatives. The most promising compounds in terms of SIRT1 activation and oral bioavailability, predicted in silico, were evaluated for their ability to activate the isolated SIRT1 enzyme. Then, we assessed the antioxidant effects of the most effective derivative, compound 3d , in human umbilical vein endothelial cells (HUVECs) injured with H 2 O 2 100 µM. The SIRT1 activator 3d significantly preserved cell viability and prevented an intracellular reactive oxygen species increase in HUVECs exposed to the oxidative stimulus. Such effects were partially reduced in the presence of a sirtuin inhibitor, sirtinol, confirming the potential role of sirtuins in the activity of resveratrol and its derivatives. Although 3d appeared less effective than resveratrol in activating the isolated enzyme, the effects exhibited by both compounds in HUVECs were almost superimposable, suggesting a higher ability of 3d to cross cell membranes and activate the intracellular target SIRT1., Competing Interests: The authors declare no conflict of interest.

Published

2022

12. Inhibitors of ADAM10 reduce Hodgkin lymphoma cell growth in 3D microenvironments and enhance brentuximab-vedotin effect.

Author

Pece R, Tavella S, Costa D, Varesano S, Camodeca C, Cuffaro D, Nuti E, Rossello A, Alfano M, D'Arrigo C, Galante D, Ravetti JL, Gobbi M, Tosetti F, Poggi A, and Zocchi MR

Subjects

Humans, Ki-1 Antigen, Membrane Proteins, Tumor Microenvironment, ADAM10 Protein antagonists & inhibitors, Brentuximab Vedotin therapeutic use, Hodgkin Disease drug therapy, Hodgkin Disease pathology, Immunoconjugates therapeutic use, Lymphoma drug therapy

Abstract

Shedding of ADAM10 substrates, like TNFa or CD30, can affect both anti-tumor immune response and antibody-drug-conjugate (ADC)-based immunotherapy. We have published two new ADAM10 inhibitors, LT4 and MN8 able to prevent such shedding in Hodgkin lymphoma (HL). Since tumor tissue architecture deeply influences the outcome of anti-cancer treatments, we set up a new threedimensional (3D) culture systems to verify whether ADAM10 inhibitors can contribute to, or enhance, the anti-lymphoma effects of the ADC brentuximab-vedotin (BtxVed). In order to recapitulate some aspects of lymphoma structure and architecture, we assembled two 3D culture models: mixed spheroids made of HL lymph node (LN) mesenchymal stromal cells (MSC) and Reed Sternberg/Hodgkin lymphoma cells (HL cells) or collagen scaffolds repopulated with LN-MSC and HL cells. In these 3D systems we found that: i) the ADAM10 inhibitors LT4 and MN8 reduce ATP content or glucose consumption, related to cell proliferation, increasing lactate dehydrogenase release as a cell damage hallmark; ii) these events are paralleled by mixed spheroids size reduction and inhibition of CD30 and TNFa shedding; iii) the effects observed can be reproduced in repopulated HL LN-derived matrix or collagen scaffolds; iv) ADAM10 inhibitors enhance the anti-lymphoma effect of the anti-CD30 ADC BtxVed both in conventional cultures and in repopulated scaffolds. Thus, we provide evidence for a direct and combined antilymphoma effect of ADAM10 inhibitors with BtxVed, leading to the improvement of ADC effects; this is documented in 3D models recapitulating features of the LN microenvironment, that can be proposed as a reliable tool for anti-lymphoma drug testing.

Published

2022

13. Discovery of Dimeric Arylsulfonamides as Potent ADAM8 Inhibitors.

Author

Cuffaro D, Camodeca C, Tuccinardi T, Ciccone L, Bartsch JW, Kellermann T, Cook L, Nuti E, and Rossello A

Abstract

The metalloproteinase ADAM8 is upregulated in several cancers but has a dispensable function under physiological conditions. In tumor cells, ADAM8 is involved in invasion, migration, and angiogenesis. The use of bivalent inhibitors could impair migration and invasion through the double binding to a homodimeric form of ADAM8 located on the cell surface of tumor cells. Herein we report the rational design and synthesis of the first dimeric ADAM8 inhibitors selective over ADAM10 and matrix metalloproteinases. Bivalent derivatives have been obtained by dimerizing the structure of a previously described ADAM17 inhibitor, JG26. In particular, derivative 2 was shown to inhibit ADAM8 proteolytic activity in vitro and in cell-based assays at nanomolar concentration. Moreover, it was more effective than the parent monomeric compound in blocking invasiveness in the breast cancer MDA-MB-231 cell line, thus supporting our hypothesis about the importance of inhibiting the active homodimer of ADAM8., Competing Interests: The authors declare no competing financial interest., (© 2021 The Authors. Published by American Chemical Society.)

Published

2021

14. Multifunctional Small Molecules as Potential Anti-Alzheimer's Disease Agents.

Author

Bargagna B, Ciccone L, Nencetti S, Santos MA, Chaves S, Camodeca C, and Orlandini E

Subjects

Amyloid beta-Peptides antagonists & inhibitors, Antioxidants chemistry, Computer Simulation, Coumaric Acids chemistry, Humans, Hydroxylamines chemistry, Hydroxylamines therapeutic use, Peptide Fragments antagonists & inhibitors, Structure-Activity Relationship, Alzheimer Disease drug therapy, Antioxidants therapeutic use, Coumaric Acids therapeutic use

Abstract

Alzheimer's disease (AD) is a severe multifactorial neurodegenerative disorder characterized by a progressive loss of neurons in the brain. Despite research efforts, the pathogenesis and mechanism of AD progression are not yet completely understood. There are only a few symptomatic drugs approved for the treatment of AD. The multifactorial character of AD suggests that it is important to develop molecules able to target the numerous pathological mechanisms associated with the disease. Thus, in the context of the worldwide recognized interest of multifunctional ligand therapy, we report herein the synthesis, characterization, physicochemical and biological evaluation of a set of five ( 1a - e ) new ferulic acid-based hybrid compounds, namely feroyl-benzyloxyamidic derivatives enclosing different substituent groups, as potential anti-Alzheimer's disease agents. These hybrids can keep both the radical scavenging activity and metal chelation capacity of the naturally occurring ferulic acid scaffold, presenting also good/mild capacity for inhibition of self-Aβ aggregation and fairly good inhibition of Cu-induced Aβ aggregation. The predicted pharmacokinetic properties point towards good absorption, comparable to known oral drugs.

Published

2021

15. Focus on Human Monoamine Transporter Selectivity. New Human DAT and NET Models, Experimental Validation, and SERT Affinity Exploration.

Author

Ortore G, Orlandini E, Betti L, Giannaccini G, Mazzoni MR, Camodeca C, and Nencetti S

Subjects

Animals, Binding Sites, Dopamine Plasma Membrane Transport Proteins metabolism, Humans, Models, Theoretical, Rabbits, Norepinephrine Plasma Membrane Transport Proteins metabolism, Serotonin Plasma Membrane Transport Proteins metabolism, Selective Serotonin Reuptake Inhibitors

Abstract

The most commonly used antidepressant drugs are the serotonin transporter inhibitors. Their effects depend strongly on the selectivity for a single monoamine transporter compared to other amine transporters or receptors, and the selectivity is roughly influenced by the spatial protein structure. Here, we provide a computational study on three human monoamine transporters, i.e., DAT, NET, and SERT. Starting from the construction of hDAT and hNET models, whose three-dimensional structure is unknown, and the prediction of the binding pose for 19 known inhibitors, 3D-QSAR models of three human transporters were built. The training set variability, which was high in structure and activity profile, was validated using a set of in-house compounds. Results concern more than one aspect. First of all, hDAT and hNET three-dimensional structures were built, validated, and compared to the hSERT one; second, the computational study highlighted the differences in binding site arrangement statistically correlated to inhibitor selectivity; third, the profiling of new inhibitors pointed out a conservation of the inhibitory activity trend between rabbit and human SERT with a difference of about 1 order of magnitude; fourth, binding and functional studies confirmed 4-(benzyloxy)-4-phenylpiperidine 20a-d and 21a-d as potent SERT inhibitors. In particular, one of the compounds (compound 20b) revealed a higher affinity for SERT than paroxetine in human platelets.

Published

2020

16. Monoaryl derivatives as transthyretin fibril formation inhibitors: Design, synthesis, biological evaluation and structural analysis.

Author

Ciccone L, Nencetti S, Tonali N, Fruchart-Gaillard C, Shepard W, Nuti E, Camodeca C, Rossello A, and Orlandini E

Subjects

Binding Sites, Crystallography, X-Ray, Humans, Models, Molecular, Molecular Conformation, Neuroprotective Agents metabolism, Neuroprotective Agents pharmacology, Prealbumin genetics, Prealbumin metabolism, Propionates metabolism, Propionates pharmacology, Protein Binding, Structure-Activity Relationship, Alzheimer Disease drug therapy, Neuroprotective Agents chemical synthesis, Prealbumin chemistry, Propionates chemistry, Protein Aggregates drug effects

Abstract

Transthyretin (TTR) is a ß-sheet-rich homotetrameric protein that transports thyroxine (T4) and retinol both in plasma and in cerebrospinal fluid. TTR also interacts with amyloid-β, playing a protective role in Alzheimer's disease. Dissociation of the native transthyretin (TTR) tetramer is widely accepted as the critical step in TTR amyloids fibrillogenesis, and is responsible for extracellular deposition of amyloid fibrils. Small molecules, able to bind in T4 binding sites and stabilize the TTR tetramer, are interesting tools to treat and prevent systemic ATTR amyloidosis. We report here the synthesis, in vitro evaluation and three-dimensional crystallographic analyses of new monoaryl-derivatives in complex with TTR. Of the derivatives reported here, the best inhibitor of TTR fibrillogenesis, 1d, exhibits an activity similar to diflunisal., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

17. Bivalent Inhibitor with Selectivity for Trimeric MMP-9 Amplifies Neutrophil Chemotaxis and Enables Functional Studies on MMP-9 Proteoforms.

Author

Nuti E, Rossello A, Cuffaro D, Camodeca C, Van Bael J, van der Maat D, Martens E, Fiten P, Pereira RVS, Ugarte-Berzal E, Gouwy M, Opdenakker G, and Vandooren J

Subjects

Animals, Cell Movement physiology, Chemotaxis physiology, Disease Models, Animal, Flow Cytometry, Humans, Leukocytosis immunology, Leukocytosis metabolism, Mice, Mice, Inbred C57BL, Neutrophils immunology, Neutrophils metabolism, Sepsis immunology, Sepsis metabolism, Endotoxemia immunology, Endotoxemia metabolism, Inflammation immunology, Inflammation metabolism, Matrix Metalloproteinase 9 chemistry, Matrix Metalloproteinase 9 metabolism

Abstract

A fundamental part of the immune response to infection or injury is leukocyte migration. Matrix metalloproteinases (MMPs) are a class of secreted or cell-bound endopeptidases, implicated in every step of the process of inflammatory cell migration. Hence, specific inhibition of MMPs is an interesting approach to control inflammation. We evaluated the potential of a bivalent carboxylate inhibitor to selectively inhibit the trimeric proteoform of MMP-9 and compared this with a corresponding monovalent inhibitor. The bivalent inhibitor efficiently inhibited trimeric MMP-9 (IC 50 = 0.1 nM), with at least 500-fold selectivity for MMP-9 trimers over monomers. Surprisingly, in a mouse model for chemotaxis, the bivalent inhibitor amplified leukocyte influxes towards lipopolysaccharide-induced inflammation. We verified by microscopic and flow cytometry analysis increased amounts of neutrophils. In a mouse model for endotoxin shock, mice treated with the bivalent inhibitor had significantly increased levels of MMP-9 in plasma and lungs, indicative for increased inflammation. In conclusion, we propose a new role for MMP-9 trimers in tempering excessive neutrophil migration. In addition, we have identified a small molecule inhibitor with a high selectivity for the trimeric proteoform of MMP-9, which will allow further research on the functions of MMP-9 proteoforms.

Published

2020

18. Matrix metalloproteinase inhibitors prevent the release and proteolytic activity of monocyte/macrophage-derived microparticles.

Author

Fogli S, Neri T, Nuti E, Mattii L, Camodeca C, and Rossello A

Subjects

Calcium metabolism, Cell Membrane drug effects, Cell Membrane metabolism, Cell-Derived Microparticles metabolism, Cells, Cultured, Cytosol drug effects, Cytosol metabolism, Humans, Leukocytes, Mononuclear metabolism, Macrophages metabolism, Monocytes metabolism, Cell-Derived Microparticles drug effects, Leukocytes, Mononuclear drug effects, Macrophages drug effects, Matrix Metalloproteinase Inhibitors pharmacology, Monocytes drug effects, Proteolysis drug effects

Abstract

Background: The role of monocyte/macrophage-derived microparticles (MPs) in the pathophysiology of cancer and chronic inflammatory diseases has been reported; nevertheless, the mechanism underlying microparticles release is currently unclear. The aim of the current study was to investigate whether matrix metalloproteinase (MMP) inhibitors could prevent MP shedding from stimulated human monocyte/macrophage., Methods: Microparticles were obtained by isolated peripheral blood mononuclear cells after stimulation with the calcium ionophore, A23187. MP shedding, intracellular calcium concentration, analysis of RhoA expression, and proteolytic activities of isolated MPs were assessed in the absence or presence of MMP inhibitors., Results: We demonstrated that MMP inhibitors remarkably prevented MP shedding in a concentration-dependent manner with IC 50 values in the nano- to micromolar range. Such an effect was related to their ability to reduce the intracellular Ca 2+ levels induced by the calcium ionophore and the consequent translocation of RhoA from cytosol to membrane. Furthermore, MMP inhibitors could inhibit the proteolytic activity of cell-derived MPs., Conclusions: The current study provide evidence that MMP inhibitors can prevent MPs shedding from stimulated human monocyte/macrophage and the proteolytic activity of released MPs. Finally, the most active compound tested might represent the lead compound of a new class of molecules with therapeutic potential in cancer and chronic inflammatory diseases., (Copyright © 2019 Institute of Pharmacology, Polish Academy of Sciences. Published by Elsevier B.V. All rights reserved.)

Published

2019

19. Design and Synthesis of Ionic Liquid-Based Matrix Metalloproteinase Inhibitors (MMPIs): A Simple Approach to Increase Hydrophilicity and to Develop MMPI-Coated Gold Nanoparticles.

Author

D'Andrea F, Nuti E, Becherini S, Cuffaro D, Husanu E, Camodeca C, De Vita E, Zocchi MR, Poggi A, D'Arrigo C, Cappello V, Gemmi M, Nencetti S, Chiappe C, and Rossello A

Subjects

Hydrophobic and Hydrophilic Interactions, Gold chemistry, Ionic Liquids, Matrix Metalloproteinase Inhibitors pharmacology, Metal Nanoparticles chemistry

Abstract

Selective and potent matrix metalloproteinase 12 (MMP-12) inhibitors endowed with improved hydrophilicity are highly sought for potential use in the treatment of lung and cardiovascular diseases. In the present paper, we modified the structure of a nanomolar MMP-12 inhibitor by incorporating an ionic liquid (IL) moiety to improve aqueous solubility. Four biologically active salts were obtained by linking the sulfonamide moiety of the MMP-12 inhibitor to imidazolium-, pyrrolidinium-, piperidinium-, and DABCO-based ILs. The imidazolium-based bioactive salt was tested on human recombinant MMPs and on monocyte-derived dendritic cells, showing activity similar to that of the parent compound, but improved water solubility. The imidazolium-based bioactive salt was then used to prepare electrostatically stabilized MMP inhibitor-coated gold nanoparticles (AuNPs) able to selectively bind MMP-12. These AuNPs were used to study subcellular localization of MMP-12 in monocyte-derived dendritic cells by transmission electron microscopy analysis., (© 2019 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2019

20. ADAM Metalloproteinases as Potential Drug Targets.

Author

Camodeca C, Cuffaro D, Nuti E, and Rossello A

Subjects

ADAM Proteins chemistry, ADAM Proteins metabolism, ADAM Proteins physiology, Animals, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents therapeutic use, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Catalytic Domain, Cell Line, Tumor, Humans, Protease Inhibitors chemistry, Protease Inhibitors pharmacology, ADAM Proteins antagonists & inhibitors, Protease Inhibitors therapeutic use

Abstract

The ADAMs, together with ADAMTSs and snake venom metalloproteases (SVMPs), are members of the Adamalysin family. Differences in structural organization, functions and localization are known and their domains, catalytic or non-catalytic, show key roles in the substrate recognition and protease activity. Some ADAMs, as membrane-bound enzymes, show sheddase activity. Sheddases are key to modulation of functional proteins such as the tumor necrosis factor, growth factors, cytokines and their receptors, adhesion proteins, signaling molecules and stress molecules involved in immunity. These activities take part in the regulation of several physiological and pathological processes including inflammation, tumor growth, metastatic progression and infectious diseases. On these bases, some ADAMs are currently investigated as drug targets to develop new alternative therapies in many fields of medicine. This review will be focused on these aspects., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2019

21. Design, synthesis and biological evaluation of bifunctional inhibitors of membrane type 1 matrix metalloproteinase (MT1-MMP).

Author

Cuffaro D, Nuti E, Gifford V, Ito N, Camodeca C, Tuccinardi T, Nencetti S, Orlandini E, Itoh Y, and Rossello A

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cell Movement drug effects, Collagen metabolism, Drug Design, Enzyme Activation drug effects, Humans, Hydroxamic Acids chemical synthesis, Hydroxamic Acids chemistry, Matrix Metalloproteinase Inhibitors chemical synthesis, Matrix Metalloproteinase Inhibitors chemistry, Molecular Dynamics Simulation, Molecular Structure, Protein Multimerization drug effects, Sulfonamides chemical synthesis, Sulfonamides chemistry, Hydroxamic Acids pharmacology, Matrix Metalloproteinase 14 metabolism, Matrix Metalloproteinase Inhibitors pharmacology, Sulfonamides pharmacology

Abstract

Collagen degradation and proMMP-2 activation are major functions of MT1-MMP to promote cancer cell invasion. Since both processes require MT1-MMP homodimerization on the cell surface, herein we propose that the use of bifunctional inhibitors of this enzyme could represent an innovative approach to efficiently reduce tumor growth. A small series of symmetrical dimers derived from previously described monomeric arylsulfonamide hydroxamates was synthesized and tested in vitro on isolated MMPs. A nanomolar MT1-MMP inhibitor, compound 6, was identified and then submitted to cell-based assays on HT1080 fibrosarcoma cells. Dimer 6 reduced MT1-MMP-dependent proMMP-2 activation, collagen degradation and collagen invasion in a dose-dependent manner with better results even compared to its monomeric analogue 4. This preliminary study suggests that dimeric MT1-MMP inhibitors might be further developed and exploited as an alternative tool to reduce cancer cell invasion., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2019

22. Matrix metalloproteinase-12 inhibitors: synthesis, structure-activity relationships and intestinal absorption of novel sugar-based biphenylsulfonamide carboxylates.

Author

Cuffaro D, Camodeca C, D'Andrea F, Piragine E, Testai L, Calderone V, Orlandini E, Nuti E, and Rossello A

Subjects

Carboxylic Acids chemical synthesis, Carboxylic Acids chemistry, Dose-Response Relationship, Drug, Humans, Matrix Metalloproteinase Inhibitors chemical synthesis, Matrix Metalloproteinase Inhibitors chemistry, Molecular Structure, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides chemistry, Carboxylic Acids pharmacology, Intestinal Absorption drug effects, Matrix Metalloproteinase 12 metabolism, Matrix Metalloproteinase Inhibitors pharmacology, Sugars chemistry, Sulfonamides pharmacology

Abstract

MMP-12 is a validated target in pulmonary and cardiovascular diseases. The principal obstacles to clinical development of MMP-12 inhibitors are an inadequate selectivity for the target enzyme and a poor water solubility, with consequent poor oral bioavailability. We recently reported a new class of sugar-based arylsulfonamide carboxylates with a nanomolar activity for MMP-12, a good selectivity and an improved water solubility. In this study, we designed and synthesized new derivatives to characterize the structure-activity relationship (SAR) within this class of glycoconjugate inhibitors. All the new derivatives were tested on human recombinant MMP-12 and MMP-9 in order to evaluate their affinity and the selectivity for the target enzyme. Among them, the four most promising compounds were selected to assess their intestinal permeability using an ex vivo everted gut sac model. Given the high polarity and structural similarity to glucose, compound 3 was demonstrated to cross the intestinal membrane by using the facilitative GLUT2 transport., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

23. Synthesis and in vitro Evaluation of ADAM10 and ADAM17 Highly Selective Bioimaging Probes.

Author

Camodeca C, Nuti E, Tosetti F, Poggi A, D'Arrigo C, Zocchi MR, and Rossello A

Subjects

ADAM10 Protein antagonists & inhibitors, ADAM17 Protein antagonists & inhibitors, Amyloid Precursor Protein Secretases antagonists & inhibitors, Antigens, CD metabolism, Carbocyanines chemistry, Cell Adhesion Molecules, Neuronal metabolism, Cell Line, Tumor, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Fetal Proteins metabolism, Fluorescein-5-isothiocyanate chemistry, Fluorescence, Fluorescent Dyes chemical synthesis, Fluorescent Dyes chemistry, Fluorescent Dyes metabolism, Humans, Membrane Proteins antagonists & inhibitors, Mesenchymal Stem Cells drug effects, Microscopy, Confocal methods, Microscopy, Fluorescence methods, Organogold Compounds chemical synthesis, Organogold Compounds chemistry, Organogold Compounds metabolism, Organogold Compounds pharmacology, Tumor Necrosis Factor-alpha metabolism, ADAM10 Protein metabolism, ADAM17 Protein metabolism, Amyloid Precursor Protein Secretases metabolism, Enzyme Inhibitors pharmacology, Fluorescent Dyes pharmacology, Membrane Proteins metabolism

Abstract

A disintegrin and metalloproteinase (ADAMs) are membrane-bound metalloproteases responsible for the ectodomain shedding of various transmembrane proteins and play important roles in multiple relevant biological processes. Their altered expression is involved in several pathological conditions, and in particular ADAM10 or ADAM17 overexpression is found in various forms of cancer. To better understand how they are regulated in the cellular context, it is useful to visualize the specific ADAMs pathway by means of molecular imaging techniques. For this purpose, we synthesized bioactive fluorescent probes suitable for cell imaging and that are able to specifically target ADAM10 or ADAM17. Two previously developed ADAM17- and ADAM10-selective inhibitors were chosen for conjugation, respectively, to a Cy5.5 dye and to Cy5.5 and FITC dyes. Herein we also report the synthesis of a gold-labeled compound as an additional bioimaging probe for ADAM10. The newly synthesized ligands were found to be active in vitro on human recombinant ADAM10 and/or ADAM17, showing IC 50 values in the nanomolar range and a good selectivity over matrix metalloproteinases (MMPs). Finally, these newly developed probes were successfully used for ADAMs staining on different lymphoma cell lines and lymph node mesenchymal stromal cells., (© 2018 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2018

24. Development of Thioaryl-Based Matrix Metalloproteinase-12 Inhibitors with Alternative Zinc-Binding Groups: Synthesis, Potentiometric, NMR, and Crystallographic Studies.

Author

Nuti E, Cuffaro D, Bernardini E, Camodeca C, Panelli L, Chaves S, Ciccone L, Tepshi L, Vera L, Orlandini E, Nencetti S, Stura EA, Santos MA, Dive V, and Rossello A

Subjects

Binding Sites, Humans, Models, Molecular, Molecular Structure, Potentiometry, Protein Binding, Protein Conformation, Structure-Activity Relationship, Crystallography, X-Ray methods, Magnetic Resonance Imaging methods, Matrix Metalloproteinase 12 chemistry, Matrix Metalloproteinase 12 metabolism, Matrix Metalloproteinase Inhibitors chemistry, Matrix Metalloproteinase Inhibitors pharmacology, Zinc metabolism

Abstract

Matrix metalloproteinase-12 (MMP-12) selective inhibitors could play a role in the treatment of lung inflammatory and cardiovascular diseases. In the present study, the previously reported 4-methoxybiphenylsulfonyl hydroxamate and carboxylate based inhibitors (1b and 2b) were modified to enhance their selectivity for MMP-12. In the newly synthesized thioaryl derivatives, the nature of the zinc binding group (ZBG) and the sulfur oxidation state were changed. Biological assays carried out in vitro on human MMPs with the resulting compounds led to identification of a sulfide, 4a, bearing an N-1-hydroxypiperidine-2,6-dione (HPD) group as new ZBG. Compound 4a is a promising hit compound since it displayed a nanomolar affinity for MMP-12 with a marked selectivity over MMP-9, MMP-1, and MMP-14. Solution complexation studies with Zn 2+ were performed to characterize the chelating abilities of the new compounds and confirmed the bidentate binding mode of HPD derivatives. X-ray crystallography studies using MMP-12 and MMP-9 catalytic domains were carried out to rationalize the biological results.

Published

2018

25. Specific ADAM10 inhibitors localize in exosome-like vesicles released by Hodgkin lymphoma and stromal cells and prevent sheddase activity carried to bystander cells.

Author

Tosetti F, Venè R, Camodeca C, Nuti E, Rossello A, D'Arrigo C, Galante D, Ferrari N, Poggi A, and Zocchi MR

Abstract

Shedding of ADAM10 substrates, like TNFα, MICA or CD30, is reported to affect both anti-tumor immune response and antibody-drug-conjugate (ADC)-based immunotherapy. Soluble forms of these molecules and ADAM10 can be carried and spread in the microenvironment by exosomes released by tumor cells. We reported new ADAM10 inhibitors able to prevent MICA shedding in Hodgkin lymphoma (HL), leading to recognition of HL cells by cytotoxic lymphocytes. In this paper, we show that the mature bioactive form of ADAM10 is released in exosome-like vesicles (ExoV) by HL cells and lymph node mesenchymal stromal cells (MSC). We demonstrate that ADAM10 inhibitors are released in ExoV by MSC or HL cells, endocytosed by bystander cells and localized in the endolysosomal compartment in HL MSC. ExoV released by HL cells can enhance MICA shedding by MSC, while ExoV from MSC induce TNFα or CD30 shedding by HL cells. Of note, ADAM10 sheddase activity carried by ExoV is prevented with the ADAM10 inhibitors LT4 and CAM29, pretreating either the ExoV-producing or the ExoV-receiving cells. In particular, both inhibitors reduce CD30 shedding maintaining the anti-tumor effects of the ADC Brentuximab-Vedotin or the anti-CD30 Iratumumab on HL cells. Thus, spreading of ADAM10 activity due to ExoV can result in the release of cytokines, like TNFα, a lymphoma growth factor, or soluble molecules, like sMICA or sCD30, that potentially interfere with host immune surveillance or immunotherapy. ADAM10 blockers can interfere with this process, allowing the development of anti-lymphoma immune response and/or efficient ADC-based or human antibody-based immunotherapy.

Published

2018

26. Bifunctional Inhibitors as a New Tool To Reduce Cancer Cell Invasion by Impairing MMP-9 Homodimerization.

Author

Nuti E, Rosalia L, Cuffaro D, Camodeca C, Giacomelli C, Da Pozzo E, Tuccinardi T, Costa B, Antoni C, Vera L, Ciccone L, Orlandini E, Nencetti S, Dive V, Martini C, Stura EA, and Rossello A

Abstract

Protein homodimers play important roles in physiological and pathological processes, including cancer invasion and metastasis. Recently, MMP-9 natural homodimerization via the PEX domain has been correlated with high migration rates of aggressive cancer cells. Here we propose that bifunctional MMP-9 inhibitors designed to impair natural MMP-9 homodimerization promoted by PEX-PEX interactions might be an effective tool to fight cancer cell invasion. Elaborating a previously described dimeric hydroxamate inhibitor 1 , new ligands were synthesized with different linker lengths and branch points. Evaluation of the modified bifunctional ligands by X-ray crystallography and biological assays showed that 7 and 8 could reduce invasion in three glioma cell lines expressing MMP-9 at different levels. To rationalize these results, we present a theoretical model of full-length MMP-9 in complex with 7 . This pioneering study suggests that a new approach using MMP-9 selective bifunctional inhibitors might lead to an effective therapy to reduce cancer cell invasion.

Published

2017

27. MMP-8 Is Critical for Dexamethasone Therapy in Alkali-Burned Corneas Under Dry Eye Conditions.

Author

Bian F, Wang C, Tukler-Henriksson J, Pflugfelder SC, Camodeca C, Nuti E, Rossello A, Li DQ, and de Paiva CS

Subjects

Alkalies, Animals, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents therapeutic use, Burns, Chemical complications, Cornea enzymology, Desiccation, Dexamethasone pharmacology, Disease Models, Animal, Dry Eye Syndromes enzymology, Eye Burns complications, Female, Matrix Metalloproteinase 8 deficiency, Matrix Metalloproteinase 8 genetics, Matrix Metalloproteinase Inhibitors pharmacology, Matrix Metalloproteinase Inhibitors therapeutic use, Mice, Inbred C57BL, Mice, Knockout, Neutrophil Infiltration drug effects, Neutrophils drug effects, Neutrophils metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Stress, Physiological, Burns, Chemical drug therapy, Burns, Chemical enzymology, Cornea pathology, Dexamethasone therapeutic use, Dry Eye Syndromes complications, Eye Burns drug therapy, Eye Burns enzymology, Matrix Metalloproteinase 8 metabolism

Abstract

Our previous studies have shown that Dexamethasone (Dex) reduced the expression of matrix-metalloproteinases (MMPs -1,-3,-9,-13), IL-1β and IL-6, while it significantly increased MMP-8 mRNA transcripts in a concomitant dry eye and corneal alkali burn murine model (CM). To investigate if MMP-8 induction is responsible for some of the protective effects of Dex in CM, MMP-8 knock out mice (MMP-8KO) were subjected to the CM for 2 or 5 days and topically treated either with 2 μl of 0.1% Dexamethasone (Dex), or saline QID. A separate group of C57BL/6 mice were topically treated with Dex or BSS and received either 100 nM CAM12 (MMP-8 inhibitor) or vehicle IP, QD. Here we demonstrate that topical Dex treated MMP-8KO mice subjected to CM showed reduced corneal clarity, increased expression of inflammatory mediators (IL-6, CXCL1, and MMP-1 mRNA) and increased neutrophil infiltration at 2D and 5D compared to Dex treated WT mice. C57BL/6 mice topically treated with Dex and CAM12 IP recapitulated findings seen with MMP-8KO mice. These results suggest that some of the anti-inflammatory effects of Dex are mediated through increased MMP-8 expression. J. Cell. Physiol. 231: 2506-2516, 2016. © 2016 Wiley Periodicals, Inc., (© 2016 Wiley Periodicals, Inc.)

Published

2016

28. Sugar-Based Arylsulfonamide Carboxylates as Selective and Water-Soluble Matrix Metalloproteinase-12 Inhibitors.

Author

Nuti E, Cuffaro D, D'Andrea F, Rosalia L, Tepshi L, Fabbi M, Carbotti G, Ferrini S, Santamaria S, Camodeca C, Ciccone L, Orlandini E, Nencetti S, Stura EA, Dive V, and Rossello A

Subjects

Acetylglucosamine chemical synthesis, Acetylglucosamine chemistry, Catalytic Domain, Glucosides chemistry, Humans, Matrix Metalloproteinase 9 chemistry, Matrix Metalloproteinase Inhibitors chemistry, Solubility, Sulfonamides chemistry, Thiourea analogs & derivatives, Thiourea chemical synthesis, Thiourea chemistry, Triazoles chemical synthesis, Triazoles chemistry, Water chemistry, Acetylglucosamine analogs & derivatives, Glucosides chemical synthesis, Matrix Metalloproteinase 12 chemistry, Matrix Metalloproteinase Inhibitors chemical synthesis, Sulfonamides chemical synthesis

Abstract

Matrix metalloproteinase-12 (MMP-12) can be considered an attractive target to study selective inhibitors useful in the development of new therapies for lung and cardiovascular diseases. In this study, a new series of arylsulfonamide carboxylates, with increased hydrophilicity resulting from conjugation with a β-N-acetyl-d-glucosamine moiety, were designed and synthesized as MMP-12 selective inhibitors. Their inhibitory activity was evaluated on human MMPs by using the fluorimetric assay, and a crystallographic analysis was performed to characterize their binding mode. Among these glycoconjugates, a nanomolar MMP-12 inhibitor with improved water solubility, compound 3 [(R)-2-(N-(2-(3-(2-acetamido-2-deoxy-β-d-glucopyranosyl)thioureido)ethyl)biphenyl-4-ylsulfonamido)-3-methylbutanoic acid], was identified., (© 2016 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2016

29. Discovery of a new selective inhibitor of A Disintegrin And Metalloprotease 10 (ADAM-10) able to reduce the shedding of NKG2D ligands in Hodgkin's lymphoma cell models.

Author

Camodeca C, Nuti E, Tepshi L, Boero S, Tuccinardi T, Stura EA, Poggi A, Zocchi MR, and Rossello A

Subjects

ADAM Proteins metabolism, ADAM10 Protein, Amyloid Precursor Protein Secretases metabolism, Crystallography, X-Ray, Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Hodgkin Disease enzymology, Hodgkin Disease pathology, Humans, Ligands, Membrane Proteins metabolism, Models, Molecular, Molecular Structure, Structure-Activity Relationship, ADAM Proteins antagonists & inhibitors, Amyloid Precursor Protein Secretases antagonists & inhibitors, Drug Discovery, Enzyme Inhibitors pharmacology, Hodgkin Disease drug therapy, Hodgkin Disease metabolism, Membrane Proteins antagonists & inhibitors, NK Cell Lectin-Like Receptor Subfamily K metabolism

Abstract

Hodgkin's lymphoma (HL) is the most common malignant lymphoma in young adults in the western world. This disease is characterized by an overexpression of ADAM-10 with increased release of NKG2D ligands, involved in an impaired immune response against tumor cells. We designed and synthesized two new ADAM-10 selective inhibitors, 2 and 3 based on previously published ADAM-17 selective inhibitor 1. The most promising compound was the thiazolidine derivative 3, with nanomolar activity for ADAM-10, high selectivity over ADAM-17 and MMPs and good efficacy in reducing the shedding of NKG2D ligands (MIC-B and ULBP3) in three different HL cell lines at non-toxic doses. Molecular modeling studies were used to drive the design and X-ray crystallography studies were carried out to explain the selectivity of 3 for ADAM-10 over MMPs., (Copyright © 2016 Elsevier Masson SAS. All rights reserved.)

Published

2016

30. Synthesis, experimental evaluation and molecular modelling of hydroxamate derivatives as zinc metalloproteinase inhibitors.

Author

Sjøli S, Nuti E, Camodeca C, Bilto I, Rossello A, Winberg JO, Sylte I, and Adekoya OA

Subjects

ADAM Proteins antagonists & inhibitors, ADAM Proteins metabolism, ADAM17 Protein, Humans, Hydroxamic Acids chemical synthesis, Hydroxamic Acids chemistry, Matrix Metalloproteinase Inhibitors chemical synthesis, Matrix Metalloproteinase Inhibitors chemistry, Models, Molecular, Molecular Structure, Thermolysin antagonists & inhibitors, Thermolysin metabolism, Hydroxamic Acids pharmacology, Matrix Metalloproteinase 2 metabolism, Matrix Metalloproteinase 9 metabolism, Matrix Metalloproteinase Inhibitors pharmacology

Abstract

Enzymes of the M4 family of zinc-metalloproteinases are virulence factors secreted from gram-positive or gram-negative bacteria, and putative drug targets in the treatment of bacterial infections. In order to have a therapeutic value such inhibitors should not interfere with endogenous zinc-metalloproteinases. In the present study we have synthesised a series of hydroxamate derivatives and validated the compounds as inhibitors of the M4 enzymes thermolysin and pseudolysin, and the endogenous metalloproteinases ADAM-17, MMP-2 and MMP-9 using experimental binding studies and molecular modelling. In general, the compounds are stronger inhibitors of the MMPs than of the M4 enzymes, however, an interesting exception is LM2. The compounds bound stronger to pseudolysin than to thermolysin, and the molecular modelling studies showed that occupation of the S2(') subpocket by an aromatic group is favourable for strong interactions with pseudolysin., (Copyright © 2015 Elsevier Masson SAS. All rights reserved.)

Published

2016

31. ADAM10 new selective inhibitors reduce NKG2D ligand release sensitizing Hodgkin lymphoma cells to NKG2D-mediated killing.

Author

Zocchi MR, Camodeca C, Nuti E, Rossello A, Venè R, Tosetti F, Dapino I, Costa D, Musso A, and Poggi A

Abstract

Hodgkin lymphoma (HL) resistant to conventional therapies is increasing, making of interest the search for new schemes of treatment. Members of the "A Disintegrin And Metalloproteases" (ADAMs) family, mainly ADAM10 or ADAM17, have been proposed as therapeutic targets in solid tumors and some ADAMs inhibitors have been shown to exert antitumor effects. We have previously described an overexpression of ADAM10 in HL, together with increased release of NKG2D ligands (NKG2D-L) and reduced activation of effector T lymphocytes with anti-lymphoma capacity. Aim of the present work was to verify whether inhibition of ADAM10 in HL cells could restore the triggering of NKG2D-dependent anti-lymphoma T cell response. As no selective ADAM10 blockers have been reported so far, we synthesized the two hydroxamate compounds LT4 and MN8 with selectivity for ADAM10 over metalloproteases (MMPs), LT4 showing higher specificity for ADAM10 over ADAM17. We show that (i) HL lymph nodes (LN) and cultured HL cells express high levels of the mature active membrane form of ADAM10; (ii) ADAM10 is the major sheddase for the NKG2D-L in HL cells; (iii) the new LT4 and MN8 compounds strongly reduce the shedding of NKG2D-L by HL cell lines and enhance the binding of NKG2D receptor; (iv) of note, these new ADAM10 inhibitors increase the sensitivity of HL cell lines to NKG2D-dependent cell killing exerted by natural killer and γδ T cells. Overall, the biologic activity of LT4 and MN8 appears to be more potent than that of the commercial inhibitor GI254023X.

Published

2015

32. N-O-Isopropyl Sulfonamido-Based Hydroxamates as Matrix Metalloproteinase Inhibitors: Hit Selection and in Vivo Antiangiogenic Activity.

Author

Nuti E, Cantelmo AR, Gallo C, Bruno A, Bassani B, Camodeca C, Tuccinardi T, Vera L, Orlandini E, Nencetti S, Stura EA, Martinelli A, Dive V, Albini A, and Rossello A

Subjects

Angiogenesis Inhibitors chemical synthesis, Angiogenesis Inhibitors pharmacology, Animals, Apoptosis drug effects, Cell Movement drug effects, Cell Survival drug effects, Crystallography, X-Ray, Human Umbilical Vein Endothelial Cells cytology, Human Umbilical Vein Endothelial Cells drug effects, Human Umbilical Vein Endothelial Cells physiology, Humans, Hydroxamic Acids chemical synthesis, Hydroxamic Acids pharmacology, Matrix Metalloproteinase 14 chemistry, Matrix Metalloproteinase 14 metabolism, Matrix Metalloproteinase 2 chemistry, Matrix Metalloproteinase 2 metabolism, Matrix Metalloproteinase 9 chemistry, Matrix Metalloproteinase 9 metabolism, Matrix Metalloproteinase Inhibitors chemical synthesis, Matrix Metalloproteinase Inhibitors pharmacology, Mice, Molecular Docking Simulation, Stereoisomerism, Structure-Activity Relationship, Sulfonamides chemical synthesis, Sulfonamides pharmacology, Angiogenesis Inhibitors chemistry, Hydroxamic Acids chemistry, Matrix Metalloproteinase Inhibitors chemistry, Sulfonamides chemistry

Abstract

Matrix metalloproteinases (MMPs) have been shown to be involved in tumor-induced angiogenesis. In particular, MMP-2, MMP-9, and MMP-14 have been reported to be crucial for tumor angiogenesis and the formation of metastasis, thus becoming attractive targets in cancer therapy. Here, we report our optimization effort to identify novel N-isopropoxy-arylsulfonamide hydroxamates with improved inhibitory activity toward MMP-2, MMP-9, and MMP-14 with respect to the previously discovered compound 1. A new series of hydroxamates was designed, synthesized, and tested for their antiangiogenic activity using in vitro assays with human umbilical vein endothelial cells (HUVECs). A nanomolar MMP-2, MMP-9, and MMP-14 inhibitor was identified, compound 3, able to potently inhibit angiogenesis in vitro and also in vivo in the matrigel sponge assay in mice. Finally, X-ray crystallographic and docking studies were conducted for compound 3 in order to investigate its binding mode to MMP-9 and MMP-14.

Published

2015

33. Selective arylsulfonamide inhibitors of ADAM-17: hit optimization and activity in ovarian cancer cell models.

Author

Nuti E, Casalini F, Santamaria S, Fabbi M, Carbotti G, Ferrini S, Marinelli L, La Pietra V, Novellino E, Camodeca C, Orlandini E, Nencetti S, and Rossello A

Subjects

ADAM Proteins chemistry, ADAM Proteins metabolism, ADAM17 Protein, Activated-Leukocyte Cell Adhesion Molecule metabolism, Cell Line, Tumor, Cell Survival drug effects, Crystallography, X-Ray, Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Female, Humans, Hydroxamic Acids chemical synthesis, Hydroxamic Acids chemistry, Hydroxamic Acids pharmacology, Models, Chemical, Models, Molecular, Molecular Structure, Ovarian Neoplasms metabolism, Ovarian Neoplasms pathology, Protein Binding, Protein Structure, Tertiary, Sulfonamides chemical synthesis, Sulfonamides chemistry, ADAM Proteins antagonists & inhibitors, Cell Movement drug effects, Enzyme Inhibitors pharmacology, Sulfonamides pharmacology

Abstract

Activated leukocyte cell adhesion molecule (ALCAM) is expressed at the surface of epithelial ovarian cancer (EOC) cells and is released in a soluble form (sALCAM) by ADAM-17-mediated shedding. This process is relevant to EOC cell motility and invasiveness, which is reduced by inhibitors of ADAM-17. In addition, ADAM-17 plays a key role in EGFR signaling and thus may represent a useful target in anticancer therapy. Herein we report our hit optimization effort to identify potent and selective ADAM-17 inhibitors, starting with previously identified inhibitor 1. A new series of secondary sulfonamido-based hydroxamates was designed and synthesized. The biological activity of the newly synthesized compounds was tested in vitro on isolated enzymes and human EOC cell lines. The optimization process led to compound 21, which showed an IC50 of 1.9 nM on ADAM-17 with greatly increased selectivity. This compound maintained good inhibitory properties on sALCAM shedding in several in vitro assays.

Published

2013

34. Mimicking the intramolecular hydrogen bond: synthesis, biological evaluation, and molecular modeling of benzoxazines and quinazolines as potential antimalarial agents.

Author

Gemma S, Camodeca C, Brindisi M, Brogi S, Kukreja G, Kunjir S, Gabellieri E, Lucantoni L, Habluetzel A, Taramelli D, Basilico N, Gualdani R, Tadini-Buoninsegni F, Bartolommei G, Moncelli MR, Martin RE, Summers RL, Lamponi S, Savini L, Fiorini I, Valoti M, Novellino E, Campiani G, and Butini S

Subjects

Animals, Cell Line, Humans, Hydrogen Bonding, Magnetic Resonance Spectroscopy, Mice, Models, Molecular, Molecular Mimicry, Spectrometry, Mass, Electrospray Ionization, Antimalarials chemistry, Antimalarials pharmacology, Benzoxazines chemistry, Benzoxazines pharmacology, Quinazolines chemistry, Quinazolines pharmacology

Abstract

The intramolecular hydrogen bond formed between a protonated amine and a neighboring H-bond acceptor group in the side chain of amodiaquine and isoquine is thought to play an important role in their antimalarial activities. Here we describe isoquine-based compounds in which the intramolecular H-bond is mimicked by a methylene linker. The antimalarial activities of the resulting benzoxazines, their isosteric tetrahydroquinazoline derivatives, and febrifugine-based 1,3-quinazolin-4-ones were examined in vitro (against Plasmodium falciparum ) and in vivo (against Plasmodium berghei ). Compounds 6b,c caused modest inhibition of chloroquine transport via the parasite's "chloroquine resistance transporter" (PfCRT) in a Xenopus laevis oocyte expression system. In silico predictions and experimental evaluation of selected drug-like properties were also performed on compounds 6b,c. Compound 6c emerged from this work as the most promising analogue of the series; it possessed low toxicity and good antimalarial activity when administered orally to P. berghei -infected mice.

Published

2012

35. Optimization of 4-aminoquinoline/clotrimazole-based hybrid antimalarials: further structure-activity relationships, in vivo studies, and preliminary toxicity profiling.

Author

Gemma S, Camodeca C, Sanna Coccone S, Joshi BP, Bernetti M, Moretti V, Brogi S, Bonache de Marcos MC, Savini L, Taramelli D, Basilico N, Parapini S, Rottmann M, Brun R, Lamponi S, Caccia S, Guiso G, Summers RL, Martin RE, Saponara S, Gorelli B, Novellino E, Campiani G, and Butini S

Subjects

Aminoquinolines pharmacokinetics, Aminoquinolines pharmacology, Animals, Antimalarials pharmacokinetics, Antimalarials pharmacology, Biological Transport, Cell Line, Chloroquine pharmacokinetics, Chloroquine pharmacology, Clotrimazole pharmacokinetics, Clotrimazole pharmacology, Drug Resistance, Female, Half-Life, Hemeproteins antagonists & inhibitors, Hemeproteins biosynthesis, Humans, Malaria drug therapy, Malaria parasitology, Male, Membrane Transport Proteins genetics, Membrane Transport Proteins physiology, Mice, Models, Molecular, Mutation, Oocytes drug effects, Oocytes metabolism, Piperazines chemical synthesis, Piperazines pharmacokinetics, Piperazines pharmacology, Plasmodium berghei, Plasmodium falciparum drug effects, Protozoan Proteins genetics, Protozoan Proteins physiology, Rats, Rats, Sprague-Dawley, Stereoisomerism, Structure-Activity Relationship, Ventricular Pressure drug effects, Xenopus laevis, Aminoquinolines chemical synthesis, Antimalarials chemical synthesis, Clotrimazole analogs & derivatives, Clotrimazole chemical synthesis

Abstract

Despite recent progress in the fight against malaria, the emergence and spread of drug-resistant parasites remains a serious obstacle to the treatment of infections. We recently reported the development of a novel antimalarial drug that combines the 4-aminoquinoline pharmacophore of chloroquine with that of clotrimazole-based antimalarials. Here we describe the optimization of this class of hybrid drug through in-depth structure-activity relationship studies. Antiplasmodial properties and mode of action were characterized in vitro and in vivo, and interactions with the parasite's 'chloroquine resistance transporter' were investigated in a Xenopus laevis oocyte expression system. These tests indicated that piperazine derivatives 4b and 4d may be suitable for coadministration with chloroquine against chloroquine-resistant parasites. The potential for metabolism of the drugs by cytochrome P450 was determined in silico, and the lead compounds were tested for toxicity and mutagenicity. A preliminary pharmacokinetic analysis undertaken in mice indicated that compound 4b has an optimal half-life.

Published

2012

36. The Ca2+-ATPase (SERCA1) is inhibited by 4-aminoquinoline derivatives through interference with catalytic activation by Ca2+, whereas the ATPase E2 state remains functional.

Author

Bartolommei G, Tadini-Buoninsegni F, Moncelli MR, Gemma S, Camodeca C, Butini S, Campiani G, Lewis D, and Inesi G

Subjects

Adenosine Triphosphate chemistry, Aminoquinolines chemistry, Animals, Calcium chemistry, Calcium metabolism, Dose-Response Relationship, Drug, Electrophysiology methods, Enzyme Inhibitors pharmacology, Hydrolysis, Inhibitory Concentration 50, Kinetics, Membrane Proteins chemistry, Models, Chemical, Phosphorylation, Rabbits, Sarcoplasmic Reticulum metabolism, Clotrimazole pharmacology, Sarcoplasmic Reticulum Calcium-Transporting ATPases metabolism

Abstract

Several clotrimazole (CLT) and 4-aminoquinoline derivatives were synthesized and found to exhibit in vitro antiplasmodial activity with IC(50) ranging from nm to μm values. We report here that some of these compounds produce inhibition of rabbit sarcoplasmic reticulum Ca(2+)-ATPase (SERCA1) with IC(50) values in the μm range. The highest affinity for the Ca(2+)-ATPase was observed with NF1442 (N-((3-chlorophenyl)(4-((4-(7-chloroquinolin-4-yl)piperazin-1-yl)methyl)phenyl)methyl)-7-chloro-4-aminoquinoline) and NF1058 (N-((3-chlorophenyl)(4-(pyrrolidin-1-ylmethyl)phenyl)methyl)-7-chloro-4-aminoquinoline),yielding IC(50) values of 1.3 and 8.0 μm as demonstrated by measurements of steady state ATPase activity as well as single cycle charge transfer. Characterization of sequential reactions comprising the ATPase catalytic and transport cycle then demonstrated that NF1058, and similarly CLT, interferes with the mechanism of Ca(2+) binding and Ca(2+)-dependent enzyme activation (E(2) to E(1)·Ca(2) transition) required for formation of phosphorylated intermediate by ATP utilization. On the other hand, Ca(2+) independent phosphoenzyme formation by utilization of P(i) (i.e. reverse of the hydrolytic reaction in the absence of Ca(2+)) was not inhibited by NF1058 or CLT. Comparative experiments showed that the high affinity inhibitor thapsigargin interferes not only with Ca(2+) binding and phosphoenzyme formation with ATP but also with phosphoenzyme formation by utilization of P(i) even though this reaction does not require Ca(2+). It is concluded that NF1058 and CLT inhibit SERCA by stabilization of an E(2) state that, as opposed to that obtained with thapsigargin, retains the functional ability to form E(2)-P by reacting with P(i).

Published

2011