Your search keyword '"Stefano Tomassi"' showing total 17 results

1. Click‐Chemistry (CuAAC) Trimerization of an α v β 6 Integrin Targeting Ga‐68‐Peptide: Enhanced Contrast for in‐Vivo PET Imaging of Human Lung Adenocarcinoma Xenografts

Author

Johannes Notni, Stefano Tomassi, Luciana Marinelli, Francesco Saverio Di Leva, Neil Gerard Quigley, Salvatore Di Maro, Frauke Richter, Katja Steiger, Susanne Kossatz, Quigley, Neil Gerard, Tomassi, Stefano, Di Leva, Francesco Saverio, Di Maro, Salvatore, Richter, Frauke, Steiger, Katja, Kossatz, Susanne, Marinelli, Luciana, Notni, Johannes, Quigley, N. G., Tomassi, S., Di Leva, F. S., Di Maro, S., Richter, F., Steiger, K., Kossatz, S., Marinelli, L., and Notni, J.

Subjects

Positron emission tomography, Biodistribution, Integrin, Peptide, 010402 general chemistry, 01 natural sciences, Biochemistry, Fibrosis, In vivo, medicine, Molecular Biology, chemistry.chemical_classification, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Transforming growth factor beta, medicine.disease, Molecular biology, Transmembrane protein, ddc, 0104 chemical sciences, Radionuclide, biology.protein, Molecular Medicine, CuAAC, Transforming growth factor

Abstract

αv β6 Integrin is an epithelial transmembrane protein that recognizes latency-associated peptide (LAP) and primarily activates transforming growth factor beta (TGF-β). It is overexpressed in carcinomas (most notably, pancreatic) and other conditions associated with αv β6 integrin-dependent TGF-β dysregulation, such as fibrosis. We have designed a trimeric Ga-68-labeled TRAP conjugate of the αv β6 -specific cyclic pentapeptide SDM17 (cyclo[RGD-Chg-E]-CONH2 ) to enhance αv β6 integrin affinity as well as target-specific in-vivo uptake. Ga-68-TRAP(SDM17)3 showed a 28-fold higher αv β6 affinity than the corresponding monomer Ga-68-NOTA-SDM17 (IC50 of 0.26 vs. 7.4 nM, respectively), a 13-fold higher IC50 -based selectivity over the related integrin αv β8 (factors of 662 vs. 49), and a threefold higher tumor uptake (2.1 vs. 0.66 %ID/g) in biodistribution experiments with H2009 tumor-bearing SCID mice. The remarkably high tumor/organ ratios (tumor-to-blood 11.2; -to-liver 8.7; -to-pancreas 29.7) enabled high-contrast tumor delineation in PET images. We conclude that Ga-68-TRAP(SDM17)3 holds promise for improved clinical PET diagnostics of carcinomas and fibrosis.

Published

2020

2. A novel smaller β‐defensin‐derived peptide is active against multidrug‐resistant bacterial strains

Author

Elena Scaglione, Francesco Salvatore, Chiara Pagliuca, Aurora Daniele, Antonello Pessi, Fortunata Carbone, Sandro Cosconati, Roberta Colicchio, Stefano Tomassi, Salvatore Di Maro, Irene Colavita, Maria Vincenza Carriero, Paola Salvatore, Giuseppe Matarese, Ersilia Nigro, Colicchio, R., Nigro, E., Colavita, I., Pagliuca, C., Di Maro, S., Tomassi, S., Scaglione, E., Carbone, F., Carriero, M. V., Matarese, G., Daniele, A., Cosconati, S., Pessi, A., Salvatore, F., Salvatore, P., Colicchio, Roberta, Nigro, Ersilia, Colavita, Irene, Pagliuca, Chiara, Di Maro, Salvatore, Tomassi, Stefano, Scaglione, Elena, Carbone, Fortunata, Carriero, Maria Vincenza, Matarese, Giuseppe, Daniele, Aurora, Cosconati, Sandro, Pessi, Antonello, Salvatore, Francesco, and Salvatore, Paola

Subjects

beta-Defensins, medicine.drug_class, Antibiotics, Antimicrobial peptides, multidrug-resistant bacteria, Peptide, Microbial Sensitivity Tests, Biochemistry, Microbiology, chemistry.chemical_compound, Antibiotic resistance, Drug Resistance, Multiple, Bacterial, Anti-Bacterial Agent, Genetics, Peptide synthesis, medicine, Humans, γ-core, Molecular Biology, Defensin, chemistry.chemical_classification, antimicrobial activity, Bacteria, Microbial Sensitivity Test, Antimicrobial Peptide, Biofilm, peptide synthesi, Anti-Bacterial Agents, Multiple drug resistance, chemistry, Biofilms, human β-defensin 3, Antimicrobial Peptides, Human, Biotechnology

Abstract

Antibiotic resistance is becoming a severe obstacle in the fight against acute and chronic infectious diseases that accompany most degenerative illnesses from neoplasia to osteo-arthritis and obesity. Currently, the race is on to identify pharmaceutical molecules or combinations of molecules able to prevent or reduce the insurgence and/or progression of infectivity. Attempts to substitute antibiotics with antimicrobial peptides have, thus far, met with little success against multidrug-resistant (MDR) bacterial strains. During the last decade, we designed and studied the activity and features of human β-defensin analogs, which are salt-resistant, and hence active also under high salt concentrations as, for instance, in cystic fibrosis. Herein, we describe the design, synthesis, and major features of a new 21 aa long molecule, peptide γ2. The latter derives from the γ-core of the β-defensin natural molecules, a small fragment of these molecules still bearing high antibacterial activity. We found that peptide γ2, which contains only one disulphide bond, recapitulates most of the biological properties of natural human β-defensins and can also counteract both Gram-positive and Gram-negative MDR bacterial strains and biofilm formation. Moreover, it has great stability in human serum thereby enhancing its antibacterial presence and activity without cytotoxicity in human cells. In conclusion, peptide γ2 is a promising new weapon also in the battle against intractable infectious diseases.

Published

2021

3. Characterization of water-soluble esters of nitrobenzoxadiazole-based GSTP1-1 inhibitors for cancer treatment

Author

Cristina Geroni, Veronica Di Paolo, Anastasia De Luca, Chiara Fulci, Manuel Scimeca, Dante Rotili, Anna Maria Caccuri, Luigi Quintieri, Stefano Tomassi, Massimo Serra, Di Paolo, V., Fulci, C., Rotili, D., De Luca, A., Tomassi, S., Serra, M., Scimeca, M., Geroni, C., Quintieri, L., and Caccuri, A. M.

Subjects

0301 basic medicine, Male, Melanoma xenografts, NBDHEX, Oxadiazole, Mice, Nude, Settore CHIM/08, Antineoplastic Agents, Pharmacology, Biochemistry, 03 medical and health sciences, GSTP1, chemistry.chemical_compound, Mice, 0302 clinical medicine, Potassium phosphate, Cell Line, Tumor, Neoplasms, GSTP1-1, Animals, Humans, Solubility, Settore BIO/10, Cytotoxicity, Glutathione Transferase, Melanoma xenograft, MC3181, Metabolic stability, Phosphate esters, Water, Esters, Glutathione, Phosphate, Xenograft Model Antitumor Assays, In vitro, 030104 developmental biology, 4-Chloro-7-nitrobenzofurazan, chemistry, Glutathione S-Transferase pi, 030220 oncology & carcinogenesis, Female

Abstract

The 7-nitrobenzo[c][1,2,5]oxadiazole (NBD) derivative NBDHEX (compound 1) and its analogue MC3181 (compound 2) have been found to be potent inhibitors of tumor cell growth in vitro and therapeutically active and safe in mice bearing human melanoma xenografts. To enhance the aqueous solubility of these compounds, we synthesized the hemisuccinate of 1 (compound 3) and the phosphate monoesters of 1 and 2 (compound 4 and 5, respectively). These novel NBD derivatives displayed a solubility in the conventional phosphate-buffered saline up to 150-fold higher than that of 1, and up to 4-fold higher than that of 2. Notably, solubility of phosphates 4 and 5 in a potassium phosphate buffer at pH 7.4, was up to 500-fold higher than that of 1, and ~10-fold higher than that of 2. Compounds 3-5 retained high cytotoxicity towards cultured human melanoma and osteosarcoma cells and were cleaved in vitro by both human and murine hydrolases, thus releasing the corresponding parent compound (i.e., 1 or 2). Interestingly, esters 3-5 displayed high inhibitory activity towards the glutathione transferase (GST) isoform GSTP1-1 and showed a reactivity towards reduced glutathione comparable to that of the respective parent compound. Finally, both 4 and 5 were safe and effective when administered intravenously or orally as an aqueous solution to mice xenografted with A375 human melanoma tumors. Collectively, these results and the previously observed synergistic interaction between 1 and 2 and various approved anticancer drugs, suggest the possible utility of phosphates 4 and 5 as single agents and in combination regimens in cancers with unmet medical need, including melanoma.

Published

2020

4. HOPPI-NMR: Hot-Peptide-Based Screening Assay for Inhibitors of Protein–Protein Interactions by NMR

Author

Stefano Tomassi, Salvatore Di Maro, Claudio Luchinat, Stefano Giuntini, Ettore Novellino, Alfonso Carotenuto, Pasquale Russomanno, Marco Fragai, Linda Cerofolini, Antonio Limatola, Diego Brancaccio, Francesco Merlino, Brancaccio, Diego, Di Maro, Salvatore, Cerofolini, Linda, Giuntini, Stefano, Fragai, Marco, Luchinat, Claudio, Tomassi, Stefano, Limatola, Antonio, Russomanno, Pasquale, Merlino, Francesco, Novellino, Ettore, Carotenuto, Alfonso, Brancaccio, D, Di Maro, S, Cerofolini, L, Giuntini, S, Fragai, M, Luchinat, C, Tomassi, S, Limatola, A, Russomanno, P, Merlino, F, Novellino, E, and Carotenuto, A.

Subjects

chemistry.chemical_classification, 010405 organic chemistry, Chemistry, Organic Chemistry, Cancer, Screening assay, Peptide, macromolecular substances, Computational biology, medicine.disease, 01 natural sciences, Biochemistry, NMR, 0104 chemical sciences, Protein–protein interaction, 010404 medicinal & biomolecular chemistry, Drug Discovery, medicine

Abstract

[Image: see text] Protein–protein interactions (PPIs) contribute to the onset and/or progression of several diseases, especially cancer, and this discovery has paved the way for considering disruption of the PPIs as an attractive anti-tumor strategy. In this regard, simple and efficient biophysical methods for detecting the interaction of the inhibitors with the protein counterpart are still in high demand. Herein, we describe a convenient NMR method for the screening of putative PPI inhibitors based on the use of “hot peptides” (HOPPI-NMR). As a case study, HOPPI-NMR was successful applied to the well-known p53/MDM2 system. Our outcomes highlight the main advantages of the method, including the use of a small amount of unlabeled proteins, the minimization of the risk of protein aggregation, and the ability to identify weak binders. The last leaves open the possibility for application of HOPPI-NMR in tandem with fragment-based drug discovery as a valid strategy for the identification of novel chemotypes acting as PPI inhibitors.

Published

2020

5. New insights in the structure-activity relationships of 2-phenylamino-substituted benzothiopyrano[4,3-d]pyrimidines as kinase inhibitors

Author

Francesca Simorini, Lisa Dalla Via, Stefano Tomassi, Giorgio Amendola, Sabrina Taliani, Concettina La Motta, Anna Maria Marini, Elisabetta Barresi, Federico Da Settimo, Silvia Salerno, Ettore Novellino, Sandro Cosconati, Aída Nelly García-Argáez, Salerno, Silvia, García-Argáez, Aída Nelly, Barresi, Elisabetta, Taliani, Sabrina, Simorini, Francesca, La Motta, Concettina, Amendola, Giorgio, Tomassi, Stefano, Cosconati, Sandro, Novellino, Ettore, Da Settimo, Federico, Marini, Anna Maria, Via, Lisa Dalla, Salerno, S, García-Argáez, An, Barresi, E, Taliani, S, Simorini, F, La Motta, C, Amendola, G, Tomassi, S, Cosconati, S, Novellino, E, Da Settimo, F, Marini, Am, and Via, Ld.

Subjects

Models, Molecular, 0301 basic medicine, Pyrimidine, medicine.drug_class, Angiogenesis, Antineoplastic Agents, Antiproliferative activity, Monoclonal antibody, Structure-Activity Relationship, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cell Line, Tumor, Drug Discovery, Human Umbilical Vein Endothelial Cells, medicine, Humans, Protein Kinase Inhibitors, Cell Proliferation, Pyrans, Pharmacology, Kinase inhibitor, Aniline Compounds, Dose-Response Relationship, Drug, Molecular Structure, Kinase, Drug Discovery3003 Pharmaceutical Science, Organic Chemistry, Kinase insert domain receptor, General Medicine, Vascular Endothelial Growth Factor Receptor-2, Small molecule, Benzothiopyranopyrimidine, Pyrimidines, 030104 developmental biology, chemistry, Biochemistry, Kinase inhibitors, Cell culture, KDR kinase, 030220 oncology & carcinogenesis, Drug Screening Assays, Antitumor, Benzothiopyranopyrimidines, Signal transduction

Abstract

Inhibition of angiogenesis via blocking vascular endothelial growth factor receptor (VEGFR) signaling pathway emerged as an established approach in anticancer therapy. So far, many monoclonal antibodies and ATP-competitive small molecule inhibitors have been clinically validated and approved. In this study, structure-activity relationships (SAR) within the 2-phenylamino-substituted benzothiopyrano[4,3-d]pyrimidine class of kinase inhibitors were further refined by the synthesis and biological evaluation of new compounds 1–21 featuring different substitution patterns on the pendant phenyl moiety, combined with H, OCH3, or Cl at 8-position. Most compounds showed a promising human kinase insert domain receptor (KDR) inhibition profile, with IC50 values in the submicromolar/low micromolar range, and promising antiproliferative activity on human umbilical vein endothelial cells (HUVECs) as well as on a panel of three human tumor cell lines. The angio-kinase selectivity profile was assessed for the most promising compound 16 against a set of six human kinases. Finally, computational studies allowed clarifying at molecular level the interaction pattern established by the compounds with KDR, highlighting key stable cation-π interactions, and thus providing the basis for further designing novel inhibitors.

Published

2018

6. Discovery of Pyrido[3′,2′:5,6]thiopyrano[4,3-d]pyrimidine-Based Antiproliferative Multikinase Inhibitors

Author

Giorgio Amendola, Sabrina Taliani, Sandro Cosconati, Ettore Novellino, Aída Nelly García-Argáez, Elisabetta Barresi, Federico Da Settimo, Stefano Tomassi, Francesca Simorini, Silvia Salerno, Anna Maria Marini, Lisa Dalla Via, Silviasalerno, Elisabettabarresi, AídaNellyGarcía-Argaéz, Sabrinataliani, Francescasimorini, Giorgio, Amendola, Tomassi, S, Sandro, Cosconati, Novellino, Ettore, Federico Da Settimo, Anna Maria Marini, Lisa Dalla Via, Salerno, S., Barresi, E., Garcia-Argaez, A. N., Taliani, S., Simorini, F., Amendola, G., Tomassi, S., Cosconati, S., Novellino, E., Da Settimo, F., Marini, A. M., and Dalla Via, L.

Subjects

antiproliferative activity, Pyridothiopyranopyrimidines, Pyrimidine, Angiogenesis, Kinase, Organic Chemistry, Pyridothiopyranopyrimidine, Biochemistry, Multikinase inhibitor, Human tumor, chemistry.chemical_compound, chemistry, Cell culture, KDR kinase, Drug Discovery, Cancer cell, multitargeted kinase inhibitors, Cancer research, Tumor growth, multitargeted kinase inhibitor

Abstract

[Image: see text] Protein kinases dysregulation is extremely common in cancer cells, and the development of new agents able to simultaneously target multiple kinase pathways involved in angiogenesis and tumor growth may offer several advantages in the treatment of cancer. Herein we report the discovery of new pyridothiopyranopyrimidine derivatives (2–4) showing high potencies in VEGFR-2 KDR inhibition as well as antiproliferative effect on a panel of human tumor cell lines. Investigation on the selectivity profile of the representative 2-anilino-substituted compounds 3b, 3i, and 3j revealed a multiplicity of kinase targets that should account for the potent antiproliferative effect produced by these pyridothiopyranopyrimidine derivatives.

Published

2019

7. Exploring the N-Terminal Region of C-X-C Motif Chemokine 12 (CXCL12): Identification of Plasma-Stable Cyclic Peptides As Novel, Potent C-X-C Chemokine Receptor Type 4 (CXCR4) Antagonists

Author

Deborah Sementa, Anna Maria Trotta, Luciana Marinelli, Maria Napolitano, Stefano Tomassi, Valeria La Pietra, Luigi Portella, Stefania Scala, Caterina Ieranò, Ettore Novellino, Crescenzo D'Alterio, Diego Brancaccio, Salvatore Di Maro, Rosa Anna Siciliano, Alfonso Carotenuto, Francesco Saverio Di Leva, DI MARO, Salvatore, Trotta, Anna Maria, Brancaccio, Diego, Di Leva, Francesco Saverio, La Pietra, Valeria, Ieranò, Caterina, Napolitano, Maria, Portella, Luigi, D'Alterio, Crescenzo, Siciliano, Rosa Anna, Sementa, Deborah, Tomassi, Stefano, Carotenuto, Alfonso, Novellino, Ettore, Scala, Stefania, Marinelli, Luciana, and LA PIETRA, Valeria

Subjects

Models, Molecular, 0301 basic medicine, Receptors, CXCR4, Drug Discovery, Pharmaceutical Science, media_common.quotation_subject, Antineoplastic Agents, Peptide, Peptides, Cyclic, 03 medical and health sciences, Chemokine receptor, 0302 clinical medicine, Cell Movement, In vivo, Cell Line, Tumor, Drug Discovery, Humans, Amino Acid Sequence, Phosphorylation, Receptor, Internalization, media_common, chemistry.chemical_classification, Leukemia, CXCR4 antagonist, Drug Discovery3003 Pharmaceutical Science, Chemokine CXCL12, Cyclic peptide, In vitro, 030104 developmental biology, chemistry, Biochemistry, 030220 oncology & carcinogenesis, Colonic Neoplasms, Molecular Medicine

Abstract

We previously reported the discovery of a CXCL12-mimetic cyclic peptide (2) as a selective CXCR4 antagonist showing promising in vitro and in vivo anticancer activity. However, further development of this peptide was hampered by its degradation in biological fluids as well as by its low micromolar affinity for the receptor. Herein, extensive chemical modifications led to the development of a new analogue (10) with enhanced potency, specificity, and plasma stability. A combined approach of Ala-amino acid scan, NMR, and molecular modeling unraveled the reasons behind the improved binding properties of 10 vs 2. Biological investigations on leukemia (CEM) and colon (HT29 and HCT116) cancer cell lines showed that 10 is able to impair CXCL12-mediated cell migration, ERK-phosphorylation, and CXCR4 internalization. These outcomes might pave the way for the future preclinical development of 10 in CXCR4 overexpressing leukemia and colon cancer.

Published

2016

8. 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

9. Structure-Activity Relationships and Biological Characterization of a Novel, Potent, and Serum Stable C-X-C Chemokine Receptor Type 4 (CXCR4) Antagonist

Author

Luigi Portella, Francesco Saverio Di Leva, Diego Brancaccio, Luciana Marinelli, Alfonso Carotenuto, Ettore Novellino, Anna Messere, Stefano Tomassi, Stefania Scala, Secondo Lastoria, Deborah Sementa, Michela Aurilio, Anna Maria Trotta, Salvatore Di Maro, Di Maro, Salvatore, Di Leva, Francesco Saverio, Trotta, Anna Maria, Brancaccio, Diego, Portella, Luigi, Aurilio, Michela, Tomassi, Stefano, Messere, Anna, Sementa, Deborah, Lastoria, Secondo, Carotenuto, Alfonso, Novellino, Ettore, Scala, Stefania, and Marinelli, Luciana

Subjects

0301 basic medicine, Receptors, CXCR4, Molecular model, Stereochemistry, Peptide, CHO Cells, CXCR3, 03 medical and health sciences, Chemokine receptor, Structure-Activity Relationship, 0302 clinical medicine, Cricetulus, Cell Movement, Cell Line, Tumor, Drug Discovery, Potency, Animals, Humans, IC50, chemistry.chemical_classification, CXCR4 antagonist, Animal, Drug Discovery3003 Pharmaceutical Science, HCT116 Cells, Amino acid, Molecular Docking Simulation, 030104 developmental biology, CHO Cell, chemistry, Biochemistry, HCT116 Cell, 030220 oncology & carcinogenesis, Molecular Medicine, Cricetulu, Peptides, Human

Abstract

In our ongoing pursuit of CXCR4 antagonists as potential anticancer agents, we recently developed a potent, selective and plasma stable peptide, Ac-Arg-Ala-[D-Cys-Arg-Phe-Phe-Cys]-COOH (3). Nevertheless, this compound was still not enough potent (IC50 ≈ 53 nM) to enter preclinical studies. Thus, a lead-optimization campaign was here undertaken to further improve the binding affinity of 3 while preserving its selectivity and proteolytic stability. Specifically, extensive structure-activity relationships (SARs) investigations were carried out on both its aromatic and disulfide forming amino acids. One among the synthesized analogue, Ac-Arg-Ala-[D-Cys-Arg-Phe-His-Pen]-COOH (19), displayed subnanomolar affinity towards CXCR4, with a marked selectivity over CXCR3 and CXCR7. NMR and molecular modeling studies disclosed the molecular bases for the binding of 19 to CXCR4 and for its improved potency compared to the lead 3. Finally, biological assays on specific cancer cell lines showed that 19 can impair CXCL12-mediated cell migration and CXCR4 internalization more efficiently than the clinically approved CXCR4 antagonist, plerixafor. In our ongoing pursuit of CXCR4 antagonists as potential anticancer agents, we recently developed a potent, selective, and plasma stable peptide, Ac-Arg-Ala-[D-Cys-Arg-Phe-Phe-Cys]-COOH (3). Nevertheless, this compound, was still not potent enough (IC50 approximate to 53 nM) to enter preclinical studies. Thus, a lead-optimization campaign was here undertaken to further improve the binding affinity of 3 while preserving its selectivity and proteolytic stability. Specifically, extensive structure activity relationships (SARs) investigations were carried out on both its aromatic and disulfide forming amino acids. One among the synthesized analogue, Ac-Arg-Ala-[D-Cys-Arg-Phe-His-Pen]-COOH (19), displayed subnanomolar affinity toward CXCR4, with a marked selectivity over CXCR3 and CXCR7. NMR and molecular modeling studies disclosed the molecular bases for the binding of 19 to CXCR4 and for its improved potency compared to the lead 3. Finally, biological assays on specific cancer cell lines showed that 19 can impair CXCL12-mediated cell migration and CXCR4 internalization more efficiently than the clinically approved CXCR4 antagonist plerixafor.

Published

2017

10. Phenotypic Identification of a Novel Autophagy Inhibitor Chemotype Targeting Lipid Kinase VPS34

Author

Daniel Rauh, Yao-Wen Wu, Michael Winzker, Makoto Muroi, Luca Laraia, Marjorie A. Carnero Corrales, Nobumoto Watanabe, Lucas Robke, André Richters, Stefano Tomassi, Julian Engel, Hiroyuki Osada, Herbert Waldmann, Tobias Engbring, Georgios Konstantinidis, Robke, L, Laraia, L, Carnero Corrales, Ma, Konstantinidis, G, Muroi, M, Richters, A, Winzker, M, Engbring, T, Tomassi, S, Watanabe, N, Osada, H, Rauh, D, Waldmann, H, Wu, Yw, and Engel, J.

Subjects

0301 basic medicine, phenotypic identification, Regulator, Cellular homeostasis, BAG3, 01 natural sciences, Catalysis, 03 medical and health sciences, Structure-Activity Relationship, 0302 clinical medicine, Drug Discovery, Autophagy, Humans, Protein Kinase Inhibitors, Sirolimus, Organisk kemi, 010405 organic chemistry, Kinase, Chemistry, Organic Chemistry, Autophagosomes, General Medicine, General Chemistry, Metabolism, Phenotype, Class III Phosphatidylinositol 3-Kinases, 3. Good health, 0104 chemical sciences, lipid kinase VPS34, Cytosol, 030104 developmental biology, HEK293 Cells, Pyrimidines, Biochemistry, MCF-7 Cells, Pyrazoles, 030217 neurology & neurosurgery, HeLa Cells

Abstract

Autophagy is a critical regulator of cellular homeostasis and metabolism. Interference with this process is considered a new approach for the treatment of disease, in particular cancer and neurological disorders. Therefore, novel small‐molecule autophagy modulators are in high demand. We describe the discovery of autophinib, a potent autophagy inhibitor with a novel chemotype. Autophinib was identified by means of a phenotypic assay monitoring the formation of autophagy‐induced puncta, indicating accumulation of the lipidated cytosolic protein LC3 on the autophagosomal membrane. Target identification and validation revealed that autophinib inhibits autophagy induced by starvation or rapamycin by targeting the lipid kinase VPS34.

Published

2017

11. Pan-histone demethylase inhibitors simultaneously targeting Jumonji C and lysine-specific demethylases display high anticancer activities

Author

Donatella Labella, Lucia Altucci, Anthony Tumber, Biagina Marrocco, Clarence Yapp, Giuseppe Ciossani, Dante Rotili, Oliver N. King, Marcello Tortorici, Sergio Valente, Richard J. Hopkinson, Stefano Tomassi, Mariarosaria Conte, Andrea Mattevi, Akane Kawamura, Ettore Novellino, Rosaria Benedetti, Antonello Mai, Christopher J. Schofield, Rotili, D, Tomassi, S, Conte, M, Benedetti, R, Tortorici, M, Ciossani, G, Valente, S, Marrocco, B, Labella, D, Novellino, E, Mattevi, A, Altucci, Lucia, Tumber, A, Yapp, C, King, On, Hopkinson, Rj, Kawamura, A, Schofield, Cj, Mai, A., Dante, Rotili, Tomassi, Stefano, Mariarosaria, Conte, Rosaria, Benedetti, Marcello, Tortorici, Giuseppe, Ciossani, Sergio, Valente, Biagina, Marrocco, Donatella, Labella, Novellino, Ettore, Andrea, Mattevi, Lucia, Altucci, Anthony, Tumber, Clarence, Yapp, King, Oliver N. F., Hopkinson, Richard J., Akane, Kawamura, Schofield, Christopher J., and Antonello, Mai

Subjects

Jumonji Domain-Containing Histone Demethylases, Lysine, Antineoplastic Agents, Apoptosis, Pan-Histone Demethylase, Jumonji C, Inhibitors, prostate cancer, KDM, Structure-Activity Relationship, Prostate cancer, Cell Line, Tumor, Drug Discovery, LNCaP, medicine, Humans, Enzyme Inhibitors, Cancer, Histone Demethylases, biology, epigenetics, Chemistry, Tranylcypromine, medicine.disease, 3. Good health, Molecular Docking Simulation, Androgen receptor, Histone, Biochemistry, biology.protein, Cancer research, Molecular Medicine, Demethylase, medicine.drug

Abstract

In prostate cancer, two different types of histone lysine demethylases (KDM), LSD1/KDM1 and JMJD2/KDM4, are co-expressed and co-localize with the androgen receptor. We designed and synthesized hybrid LSD1/JmjC - "pan-KDM" - inhibitors 1-6, by coupling the skeleton of tranylcypromine 7, a known LSD1 inhibitor, with 4-carboxy-4'-carbomethoxy-2,2'-bipyridine 8 or 5-carboxy-8-hydroxyquinoline 9, two 2-oxoglutarate competitive templates developed for JmjC inhibition. Hybrid compounds 1-6 are able to simultaneously target both KDM families, and have been validated as potential antitumor agents in cells. Among them, compounds 2 and 3 increase H3K4 and H3K9 methylation levels in cells and cause growth arrest and substantial apoptosis in LNCaP prostate and HCT116 colon cancer cells. When tested in non-cancer mesenchymal progenitor (MePR) cells, 2 and 3 induced little and no apoptosis, respectively, thus showing a cancer-selective inhibiting action.

Published

2016

12. Switchable Protecting Strategy for Solid Phase Synthesis of DNA and RNA Interacting Nucleopeptides

Author

Sandro Cosconati, Paola Stiuso, Maria Gaglione, Maria Emilia Mercurio, Anna Messere, Angela Chambery, Stefano Tomassi, Rosita Russo, Ettore Novellino, Salvatore Di Maro, Stefania Lama, Mercurio, Me, Tomassi, S, Gaglione, M, Russo, R, Chambery, A, Lama, S, Stiuso, P, Cosconati, S, Novellino, E, Di Maro, S, Messere, A., Mercurio, Maria Emilia, Tomassi, Stefano, Gaglione, Maria, Russo, Rosita, Chambery, Angela, Lama, Stefania, Stiuso, Paola, Cosconati, Sandro, Novellino, Ettore, DI MARO, Salvatore, and Messere, Anna

Subjects

Sequence (biology), 010402 general chemistry, 01 natural sciences, solid phase peptide synthesis, Nucleobase, chemistry.chemical_compound, Solid-phase synthesis, Cell Line, Tumor, Protective group, Humans, Amino Acid Sequence, Peptide sequence, Solid-Phase Synthesis Techniques, 010405 organic chemistry, Circular Dichroism, Organic Chemistry, Nuclear Proteins, RNA, DNA, Combinatorial chemistry, 0104 chemical sciences, Nucleopeptide, Biochemistry, chemistry, Nucleic acid, Chemical stability, Peptides

Abstract

Nucleopeptides are promising nucleic acid mimetics in which the peptide backbone bears nucleobases. They can recognize DNA and RNA targets modulating their biological functions. To date, the lack of an effective strategy for the synthesis of nucleopeptides prevents their evaluation for biological and biomedical applications. Herein, we describe an unprecedented approach that enables the synthesis of cationic both homo and heterosequence nucleopeptides wholly on solid support with high yield and purity. Spectroscopic studies indicate advantageous properties of the nucleopeptides in terms of binding, thermodynamic stability and sequence specific recognition. Biostability assay and laser scanning confocal microscopy analyses reveal that the nucleopeptides feature acceptable serum stability and ability to cross the cell membrane.

Published

2016

13. Targeting Drug Resistance in EGFR with Covalent Inhibitors: A Structure-Based Design Approach

Author

Martin Termathe, René P. Zahedi, Johannes M. Heuckmann, Matthäus Getlik, Daniel Rauh, Stefano Tomassi, Franziska Hoffgaard, Niklas Schaumann, Julian Engel, Verena Tinnefeld, Carsten Schultz-Fademrecht, Jasmin Krüll, Christian Grütter, Martin L. Sos, Simone Eppmann, Stefan M. Kast, Patrick Kibies, Marina Keul, Sascha Menninger, Svenja C. Mayer-Wrangowski, Sandra Ortiz-Cuaran, Roman K. Thomas, Jonas Lategahn, André Richters, Niklas Uhlenbrock, Christian Becker, Jochen Heil, Engel, J, Richters, A, Getlik, M, Tomassi, S, Keul, M, Termathe, M, Lategahn, J, Becker, C, Mayer-Wrangowski, S, Grütter, C, Uhlenbrock, N, Krüll, J, Schaumann, N, Eppmann, S, Kibies, P, Hoffgaard, F, Heil, J, Menninger, S, Ortiz-Cuaran, S, Heuckmann, Jm, Tinnefeld, V, Zahedi, Rp, Sos, Ml, Schultz-Fademrecht, C, Thomas, Rk, Kast, Sm, and Rauh

Subjects

Models, Molecular, Cell Membrane Permeability, Lung Neoplasms, EGFR, Molecular Conformation, Antineoplastic Agents, Crystallography, X-Ray, Receptor tyrosine kinase, Small Molecule Libraries, T790M, Structure-Activity Relationship, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Drug Discovery, Structure–activity relationship, Humans, Epidermal growth factor receptor, EGFR inhibitors, biology, Chemistry, Rational design, Proteolytic enzymes, Ligand (biochemistry), structure-based design, respiratory tract diseases, ErbB Receptors, Kinetics, Pyrimidines, src-Family Kinases, Biochemistry, Solubility, Drug Resistance, Neoplasm, Drug Design, Mutation, biology.protein, Quinazolines, Molecular Medicine, covalent inhibitor, Pyrazoles, Databases, Chemical

Abstract

Receptor tyrosine kinases represent one of the prime targets in cancer therapy, as the dysregulation of these elementary transducers of extracellular signals, like the epidermal growth factor receptor (EGFR), contributes to the onset of cancer, such as non-small cell lung cancer (NSCLC). Strong efforts were directed to the development of irreversible inhibitors and led to compound CO-1686, which takes advantage of increased residence time at EGFR by alkylating Cys797 and thereby preventing toxic effects. Here, we present a structure-based approach, rationalized by subsequent computational analysis of conformational ligand ensembles in solution, to design novel and irreversible EGFR inhibitors based on a screening hit that was identified in a phenotype screen of 80 NSCLC cell lines against approximately 1500 compounds. Using protein X-ray crystallography, we deciphered the binding mode in engineered cSrc (T338M/S345C), a validated model system for EGFR-T790M, which constituted the basis for further rational design approaches. Chemical synthesis led to further compound collections that revealed increased biochemical potency and, in part, selectivity toward mutated (L858R and L858R/T790M) vs nonmutated EGFR. Further cell-based and kinetic studies were performed to substantiate our initial findings. Utilizing proteolytic digestion and nano-LC-MS/MS analysis, we confirmed the alkylation of Cys797.

Published

2015

14. Quinoline-Based p300 Histone Acetyltransferase Inhibitors with Pro-apoptotic Activity in Human Leukemia U937 Cells

Author

Rosaria Benedetti, Simone Carradori, Gianluca Sbardella, Alessia Lenoci, Stefano Tomassi, Lucia Altucci, Ettore Novellino, Veronica Rodriguez, Antonello Mai, Patrizia Filetici, Daniela Secci, Sabrina Castellano, Mariarosaria Conte, Dante Rotili, Lenoci, A, Tomassi, S, Conte, M, Benedetti, R, Rodriguez, V, Carradori, S, Secci, D, Castellano, S, Sbardella, G, Filetici, P, Novellino, E, Altucci, Lucia, Rotili, D, Mai, A., Alessia, Lenoci, Tomassi, Stefano, Mariarosaria, Conte, Rosaria, Benedetti, Veronica, Rodriguez, Simone, Carradori, Daniela, Secci, Sabrina, Castellano, Gianluca, Sbardella, Patrizia, Filetici, Novellino, Ettore, Lucia, Altucci, Dante, Rotili, and Antonello, Mai

Subjects

Biochemistry, chemistry.chemical_compound, 0302 clinical medicine, lysine acetyltransferases (KATs), quinoline, Drug Discovery, Tumor Cells, Cultured, Enzyme Inhibitors, General Pharmacology, Toxicology and Pharmaceutics, 0303 health sciences, Molecular Structure, biology, U937 cell, Quinoline, apoptosis, leukemia, Cell Differentiation, U937 Cells, 3. Good health, Leukemia, 030220 oncology & carcinogenesis, Quinolines, Molecular Medicine, epigenetic, U937, Antineoplastic Agents, p300, Structure-Activity Relationship, 03 medical and health sciences, Histone H3, HATs, histone acetyltransferase inhibitors, medicine, Humans, cancer, Epigenetics, epigenetics, HAT, structure–activity relationships, 030304 developmental biology, Pharmacology, Dose-Response Relationship, Drug, structure-activity relationships, Organic Chemistry, Histone acetyltransferase, medicine.disease, Molecular biology, chemistry, Apoptosis, Acetylation, biology.protein, Drug Screening Assays, Antitumor

Abstract

Chemical manipulations performed on 2-methyl-3-carbethoxyquinoline (1), a histone acetyltransferase inhibitor previously identified by our research group and active at the sub-millimolar/millimolar level, led to compounds bearing higher alkyl groups at the C2-quinoline or additional side chains at the C6-quinoline positions. Such compounds displayed at least threefold improved inhibitory potency toward p300 protein lysine acetyltransferase activity; some of them decreased histone H3 and H4 acetylation levels in U937 cells and induced high degrees of apoptosis (three compounds >10-fold higher than compound 1) after treatment of U937 cells.

Published

2014

15. tert-Butylcarbamate-Containing Histone Deacetylase Inhibitors: Apoptosis Induction, Cytodifferentiation, and Antiproliferative Activities in Cancer Cells

Author

Antonello Mai, Daniela Secci, Donatella Labella, Stefano Tomassi, Lucia Altucci, Ettore Novellino, Sandro Cosconati, Rosaria Benedetti, Maria Tardugno, Salvatore Di Maro, Donatella Del Bufalo, Sergio Valente, Daniela Trisciuoglio, Ciro Mercurio, Roberto Boggio, S., Valente, D., Trisciuoglio, M., Tardugno, R., Benedetti, D., Labella, D., Secci, C., Mercurio, R., Boggio, Tomassi, Stefano, DI MARO, Salvatore, Novellino, Ettore, L., Altucci, D., Del Bufalo, A., Mai, S., Cosconati, Valente, S, Trisciuoglio, D, Tardugno, M, Benedetti, R, Labella, D, Secci, D, Mercurio, C, Boggio, R, Tomassi, S, Novellino, E, Altucci, Lucia, Del Bufalo, D, Mai, A, and Cosconati, Sandro

Subjects

Models, Molecular, Apoptosis, Histone Deacetylase 1, Pyrrole, Histone Deacetylase 6, Biochemistry, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, Drug Discovery, General Pharmacology, Toxicology and Pharmaceutics, 0303 health sciences, Molecular Structure, Myeloid leukemia, Cell Differentiation, U937 Cells, Recombinant Proteins, 3. Good health, 030220 oncology & carcinogenesis, Hydroxamate, MCF-7 Cells, Molecular Medicine, Growth inhibition, HT29 Cells, Antineoplastic Agents, Biology, Histone Deacetylases, 03 medical and health sciences, Structure-Activity Relationship, tert-butylcarbamate, Cell Line, Tumor, Humans, Histone H3 acetylation, 030304 developmental biology, Cell Proliferation, Pharmacology, Dose-Response Relationship, Drug, Organic Chemistry, Anilide, Apoptosi, HCT116 Cells, Histone Deacetylase Inhibitors, Repressor Proteins, chemistry, Cell culture, Cancer cell, Cancer research, Histone deacetylase, Carbamates, Drug Screening Assays, Antitumor, K562 Cells, K562 cells

Abstract

"Herein we report novel pyrrole- and benzene-based hydroxamates (8, 10) and 2'-aminoanilides (9, 11) bearing the tert-butylcarbamate group at the CAP moiety as histone deacetylase (HDAC) inhibitors. Compounds 8 b and 10 c selectively inhibited HDAC6 at the nanomolar level, whereas the other hydroxamates effected an increase in acetyl-α-tubulin levels in human acute myeloid leukemia U937 cells. In the same cell line, compounds 8 b and 10 c elicited 18.4 and 21.4 % apoptosis, respectively (SAHA: 16.9 %), and the pyrrole anilide 9 c displayed the highest cytodifferentiating effect (90.9 %). In tests against a wide range of various cancer cell lines to determine its antiproliferative effects, compound 10 c exhibited growth inhibition from sub-micromolar (neuroblastoma LAN-5 and SH-SY5Y cells, chronic myeloid leukemia K562 cells) to low-micromolar (lung H1299 and A549, colon HCT116 and HT29 cancer cells) concentrations. In HT29 cells, 10 c increased histone H3 acetylation, and decreased the colony-forming potential of the cancer cells by up to 60 %." Herein we report novel pyrrole- and benzene-based hydroxamates (8, 10) and 2′-aminoanilides (9, 11) bearing the tert-butylcarbamate group at the CAP moiety as histone deacetylase (HDAC) inhibitors. Compounds 8b and 10c selectively inhibited HDAC6 at the nanomolar level, whereas the other hydroxamates effected an increase in acetyl-α-tubulin levels in human acute myeloid leukemia U937 cells. In the same cell line, compounds 8b and 10c elicited 18.4 and 21.4% apoptosis, respectively (SAHA: 16.9%), and the pyrrole anilide 9c displayed the highest cytodifferentiating effect (90.9%). In tests against a wide range of various cancer cell lines to determine its antiproliferative effects, compound 10c exhibited growth inhibition from sub-micromolar (neuroblastoma LAN-5 and SH-SY5Y cells, chronic myeloid leukemia K562 cells) to low-micromolar (lung H1299 and A549, colon HCT116 and HT29 cancer cells) concentrations. In HT29 cells, 10c increased histone H3 acetylation, and decreased the colony-forming potential of the cancer cells by up to 60%. © 2013 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

Published

2013

16. Identification of PR-SET7 and EZH2 selective inhibitors inducing cell death in human leukemia U937 cells

Author

Antonello Mai, Lucia Altucci, Maria Tardugno, Gianluca Sbardella, Ilaria Lepore, Salvatore Di Maro, Sergio Valente, Ettore Novellino, Stefano Tomassi, Roberta Costi, Sabrina Castellano, Roberto Di Santo, Carmela Dell'Aversana, 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], Dipartimento di Patologia Generale, Seconda Università degli studi di Napoli, Dipartimento di Scienze Farmaceutiche e Biomediche, Università degli Studi di Salerno (UNISA), Department of Pharmacy Naples, Université de Naples, Valente, S, Lepore, I, Dell'Aversana, C, Tardugno, M, Castellano, S, Sbardella, G, Tomassi, S, DI MARO, Salvatore, Novellino, E, Di Santo, R, Costi, R, Altucci, Lucia, Mai, A., S., Valente, I., Lepore, C., Dell'Aversana, M., Tardugno, S., Castellano, G., Sbardella, Tomassi, Stefano, Novellino, Ettore, R., Di Santo, R., Costi, L., Altucci, and A., Mai

Subjects

MESH: Cell Death, Cellular differentiation, MESH: Cell Cycle, Biochemistry, Histone methylation, Substrate Specificity, Histones, 0302 clinical medicine, Histocompatibility Antigens, Enzyme Inhibitors, chemistry.chemical_classification, MESH: Histones, 0303 health sciences, Leukemia, Cell Death, U937 cell, medicine.diagnostic_test, Cell Cycle, MESH: Drug Screening Assays, Antitumor, Polycomb Repressive Complex 2, Epigenetic, Cell Differentiation, General Medicine, Cell cycle, [SDV.SP]Life Sciences [q-bio]/Pharmaceutical sciences, 3. Good health, MESH: Enzyme Inhibitors, 030220 oncology & carcinogenesis, MESH: Granulocytes, Histone Methyltransferases, MESH: Polycomb Repressive Complex 2, MESH: Cell Differentiation, Programmed cell death, MESH: Cell Line, Tumor, macromolecular substances, Biology, Methylation, MESH: Methylation, 03 medical and health sciences, Western blot, Cell Line, Tumor, MESH: Leukemia, medicine, Humans, Enhancer of Zeste Homolog 2 Protein, 030304 developmental biology, MESH: Humans, MESH: Histocompatibility Antigens, MESH: Histone-Lysine N-Methyltransferase, Histone-Lysine N-Methyltransferase, Epi-drug, medicine.disease, Molecular biology, Enzyme, chemistry, Cell culture, Bis(bromo- and dibromo-phenol) compound, MESH: Substrate Specificity, Drug Screening Assays, Antitumor, Granulocytes

Abstract

Chemical manipulations undertaken on some bis(bromo- and dibromo-phenol) compounds previously reported by us as wide-spectrum epigenetic inhibitors let us to identify bis (bromo- and dibromo-methoxyphenyl) derivatives highly selective for PR-SET7 and EZH2 (compounds 4, 5, 9, and 10). Western blot analyses were carried out in U937 cells to determine the effects of such compounds on the methyl marks related to the tested enzymes (H3K4me1, H3K9me2, H4H20me1, and H3K27me3). The 1,5-bis(3-bromo-4-methoxyphenyl)penta-1,4-dien-3- one 4 (EC50 vs EZH2 = 74.9 μM), tested in U937 cells at 50 μM, induced massive cell death and 28% of granulocytic differentiation, highlighting the potential use of EZH2 inhibitors in cancer. © 2012 Elsevier Masson SAS. All rights reserved.

Published

2012

17. Cover Picture:tert-Butylcarbamate-Containing Histone Deacetylase Inhibitors: Apoptosis Induction, Cytodifferentiation, and Antiproliferative Activities in Cancer Cells (ChemMedChem 5/2013)

Author

Maria Tardugno, Sandro Cosconati, Donatella Labella, Roberto Boggio, Stefano Tomassi, Donatella Del Bufalo, Daniela Trisciuoglio, Ciro Mercurio, Lucia Altucci, Salvatore Di Maro, Daniela Secci, Antonello Mai, Ettore Novellino, Rosaria Benedetti, and Sergio Valente

Subjects

Pharmacology, Biochemistry, Chemistry, Apoptosis, Organic Chemistry, Drug Discovery, Cancer cell, Molecular Medicine, Cover (algebra), Histone deacetylase, General Pharmacology, Toxicology and Pharmaceutics, Apoptosis induction

Published

2013