Your search keyword '"Alessia Lucidi"' showing total 15 results

1. Synthesis and characterisation of a new benzamide-containing nitrobenzoxadiazole as a GSTP1-1 inhibitor endowed with high stability to metabolic hydrolysis

Author

Veronica Di Paolo, Chiara Fulci, Dante Rotili, Francesca Sciarretta, Alessia Lucidi, Blasco Morozzo della Rocca, Anastasia De Luca, Antonio Rosato, Luigi Quintieri, and Anna Maria Caccuri

Subjects

nitrobenzoxadiazoles, gstp1-1, traf2, glutathione, a375 human melanoma, Therapeutics. Pharmacology, RM1-950

Abstract

The antitumor agent 6-((7-nitrobenzo[c][1,2,5]oxadiazol-4-yl)thio)hexan-1-ol (1) is a potent inhibitor of GSTP1-1, a glutathione S-transferase capable of inhibiting apoptosis by binding to JNK1 and TRAF2. We recently demonstrated that, unlike its parent compound, the benzoyl ester of 1 (compound 3) exhibits negligible reactivity towards GSH, and has a different mode of interaction with GSTP1-1. Unfortunately, 3 is susceptible to rapid metabolic hydrolysis. In an effort to improve the metabolic stability of 3, its ester group has been replaced by an amide, leading to N-(6-((7-nitrobenzo[c][1,2,5]oxadiazol-4-yl)thio)hexyl)benzamide (4). Unlike 3, compound 4 was stable to human liver microsomal carboxylesterases, but retained the ability to disrupt the interaction between GSTP1-1 and TRAF2 regardless of GSH levels. Moreover, 4 exhibited both a higher stability in the presence of GSH and a greater cytotoxicity towards cultured A375 melanoma cells, in comparison with 1 and its analog 2. These findings suggest that 4 deserves further preclinical testing.

Published

2019

2. Novel non-covalent LSD1 inhibitors endowed with anticancer effects in leukemia and solid tumor cellular models

Author

Martina Menna, Francesco Fiorentino, Biagina Marrocco, Alessia Lucidi, Stefano Tomassi, Domenica Cilli, Mauro Romanenghi, Matteo Cassandri, Silvia Pomella, Michele Pezzella, Donatella Del Bufalo, Mohammad Salik Zeya Ansari, Nevena Tomašević, Milan Mladenović, Monica Viviano, Gianluca Sbardella, Rossella Rota, Daniela Trisciuoglio, Saverio Minucci, Andrea Mattevi, Dante Rotili, Antonello Mai, Menna, Martina, Fiorentino, Francesco, Marrocco, Biagina, Lucidi, Alessia, Tomassi, Stefano, Cilli, Domenica, Romanenghi, Mauro, Cassandri, Matteo, Pomella, Silvia, Pezzella, Michele, Del Bufalo, Donatella, Zeya Ansari, Mohammad Salik, Tomašević, Nevena, Mladenović, Milan, Viviano, Monica, Sbardella, Gianluca, Rota, Rossella, Trisciuoglio, Daniela, Minucci, Saverio, Mattevi, Andrea, Rotili, Dante, and Mai, Antonello

Subjects

Histone Demethylases, Pharmacology, Leukemia, Drug discovery, Polypharmacology, Organic Chemistry, General Medicine, Cancer, Histone lysine methyltransferases, Lysine-specific demethylase 1, Settore MED/05, Histone lysine methyltransferase, Cell Line, Tumor, Humans, Enzyme Inhibitor, Histone Demethylase, Enzyme Inhibitors, Cell Proliferation, Human

Abstract

LSD1 is a histone lysine demethylase proposed as therapeutic target in cancer. Chemical modifications applied at C2, C4 and/or C7 positions of the quinazoline core of the previously reported dual LSD1/G9a inhibitor 1 led to a series of non-covalent, highly active, and selective LSD1 inhibitors (2-4 and 6-30) and to the dual LSD1/G9a inhibitor 5 that was more potent than 1 against LSD1. In THP-1 and MV4-11 leukemic cells, the most potent compounds (7, 8, and 29) showed antiproliferative effects at sub-micromolar level without significant toxicity at 1μM in non-cancer AHH-1cells. In MV4-11cells, the new derivatives increased the levels of the LSD1 histone mark H3K4me2 and induced the re-expression of the CD86 gene silenced by LSD1, thereby confirming the inhibition of LSD1 at cellular level. In breast MDA-MB-231 as well as in rhabdomyosarcoma RD and RH30cells, taken as examples of solid tumors, the same compounds displayed cell growth arrest in the same IC50 range, highlighting a crucial anticancer role for LSD1 inhibition and suggesting no added value for the simultaneous G9a inhibition in these tumor cell lines.

Published

2022

3. α,γ-Diketocarboxylic Acids and Their Esters Act as Carbonic Anhydrase IX and XII Selective Inhibitors

Author

Nicola Baldini, Claudiu T. Supuran, Francesca Perut, Alessia Lucidi, Paola Gratteri, Antonello Mai, Alessio Nocentini, Daniela Tomaselli, Dante Rotili, Annamaria Massa, Nocentini A., Lucidi A., Perut F., Massa A., Tomaselli D., Gratteri P., Baldini N., Rotili D., Mai A., and Supuran C.T.

Subjects

Gene isoform, Stereochemistry, Metalloenzyme, Carboxylic acid, carbonic anhydrase, 01 natural sciences, Biochemistry, selective inhibition, Carbonic anhydrase, Drug Discovery, antitumor, chemistry.chemical_classification, biology, 010405 organic chemistry, Organic Chemistry, Carbonic Anhydrase IX, Ethyl ester, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Cytosol, Enzyme, chemistry, carbonic anhydrase inhibitors, α,γ-diketocarboxylic acids, α,γ-diketocarboxylic esters, Cell culture, biology.protein, carboxylic acid

Abstract

Among human carbonic anhydrase (CA) inhibitors, the alpha,gamma-diketocarboxylic acids and esters are still poorly investigated. Here, we report the first compounds of this class (1-6) acting as potent inhibitors at low nanomolar level against the cancer-related human CA IX and XII, and 2-3 magnitude orders selective toward the cytosolic isoforms hCA I and II. At enzymatic level, the alpha,gamma-diketoacids 1-3 were more effective inhibitors compared to the corresponding ethyl esters 4-6. The phenyl- and alpha-naphthyl-containing compounds (1, 3, 4, and 6) behaved as dual hCA IX/XII inhibitors, while the beta-naphthyl analogues (2 and 5) exhibited hCA IX-selective inhibition. In MG63 and HOS osteosarcoma (OS) cell lines, the ethyl esters 5 and 6 displayed dose-dependent reduction of viability and proliferation after 72 h treatment, with 6 being more potent than 5 likely for its dual hCA IX/XII inhibition.

Published

2019

4. Mechanism-based inhibitors of SIRT2: structure–activity relationship, X-ray structures, target engagement, regulation of α-tubulin acetylation and inhibition of breast cancer cell migration

Author

Alexander L. Nielsen, Andreas Stahl Madsen, Nima Rajabi, Kathrine Lundø, Minoru Yoshida, Norio Kudo, Michael Bæk, Christian A. Olsen, Carlos Moreno-Yruela, Alessia Lucidi, and Martin Fontenas

Subjects

Lysine, Cell, SIRT2, Biochemistry, Genetics and Molecular Biology (miscellaneous), Biochemistry, 01 natural sciences, 03 medical and health sciences, medicine, Structure–activity relationship, Molecular Biology, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, biology, 010405 organic chemistry, Chemistry, Cancer, medicine.disease, 0104 chemical sciences, 3. Good health, medicine.anatomical_structure, Enzyme, Chemistry (miscellaneous), Cell culture, Acetylation, Sirtuin, biology.protein, Alpha-tubulin acetylation

Abstract

Sirtuin 2 (SIRT2) is a protein deacylase enzyme that removes acetyl groups and longer chain acyl groups from post-translationally modified lysine residues. It affects diverse biological functions in the cell and has been considered a drug target in relation to both neurodegenerative diseases and cancer. Therefore, access to well-characterized and robust tool compounds is essential for the continued investigation of the complex functions of this enzyme. Here, we report a collection of chemical probes that are potent, selective, stable in serum, water-soluble, and inhibit SIRT2-mediated deacetylation and demyristoylation in cells. Compared to the current landscape of SIRT2 inhibitors, this is a unique ensemble of features built into a single compound. We expect the developed chemotypes to find broad application in the interrogation of SIRT2 functions in both healthy and diseased cells, and to provide a foundation for the development of future therapeutics., Sirtuin 2 (SIRT2) is a protein deacylase enzyme that removes acetyl groups and longer chain acyl groups from post-translationally modified lysine residues. Here, we developed small peptide-based inhibitors of its activity in living cells in culture.

Published

2020

5. Structure-Reactivity Relationships on Substrates and Inhibitors of the Lysine Deacylase Sirtuin 2 from

Author

Daria, Monaldi, Dante, Rotili, Julien, Lancelot, Martin, Marek, Nathalie, Wössner, Alessia, Lucidi, Daniela, Tomaselli, Elizabeth, Ramos-Morales, Christophe, Romier, Raymond J, Pierce, Antonello, Mai, and Manfred, Jung

Subjects

Niacinamide, Oxadiazoles, Lysine, Helminth Proteins, Schistosoma mansoni, Substrate Specificity, Kinetics, Structure-Activity Relationship, Pyrimidines, Sirtuin 2, Larva, Animals, Humans, Schistosomiasis, Peptides

Abstract

The only drug currently available for treatment of the neglected disease Schistosomiasis is Praziquantel, and the possible emergence of resistance makes research on novel therapeutic agents necessary and urgent. To this end, the targeting of

Published

2019

6. Structure-Reactivity Relationships on Substrates and Inhibitors of the Lysine Deacylase Sirtuin 2 from Schistosoma Mansoni (SmSirt2)

Author

Raymond J. Pierce, Nathalie Wössner, Christophe Romier, Elizabeth Ramos-Morales, Daria Monaldi, Antonello Mai, Dante Rotili, Manfred Jung, Alessia Lucidi, Julien Lancelot, Daniela Tomaselli, Martin Marek, University of Freiburg [Freiburg], Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], Centre d’Infection et d’Immunité de Lille - INSERM U 1019 - UMR 9017 - UMR 8204 (CIIL), Centre National de la Recherche Scientifique (CNRS)-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Université de Lille-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP), Institut de Génétique et de Biologie Moléculaire et Cellulaire (IGBMC), Université de Strasbourg (UNISTRA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), This work was supported by Deutsche Forschungsgemeinschaft (DFG, GRK1976, to D.M., N.W., and M.J., testing on human Sirtuins Ju295/14-1), Italian PRIN 2015 (prot. 20152TE5PK to A.M.), AIRC 2016 (n. 19162 to A.M.), Progetto Ateneo Sapienza 2017 (to D.R.), and the A-ParaDDisE program funded under the European Union’s Seventh Framework Programme (grant agreement no. 602080 to M.J., C.R., R.J.P., A.M.) It was also supported by the grant ANR-10-LABX-0030-INRT, a French State fund managed by the Agence Nationale de la Recherche under the frame program Investissements d’Avenir ANR-10-IDEX-0002-02 to C.R., M.M., and E.R.-M. J.L. and R.J.P. are supported by institutional funds from the Centre National de la Recherche Scientifique (CNRS), the Institut National de la Sante et de la Recherche, Medicale (INSERM), the Institut Pasteur de Lille, and the Universite de Lille., The authors acknowledge GSK for kindly donating the Kineto Boxes compounds (aka TCKAS) for biological testing and the COST action CM1406 (Epigenetic Chemical Biology) for support., Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome] (UNIROMA), Institut Pasteur de Lille, and Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lille-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Drug, media_common.quotation_subject, Lysine, Schistosomiasis, Pharmacology, 01 natural sciences, 03 medical and health sciences, sirtuins, schistosomiasis, Drug Discovery, parasitic diseases, medicine, Epigenetics, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], 030304 developmental biology, media_common, Schistosoma, chemistry.chemical_classification, 0303 health sciences, epigenetics, biology, 010405 organic chemistry, Chemistry, Neglected Disease, Structure reactivity, medicine.disease, biology.organism_classification, In vitro, 3. Good health, 0104 chemical sciences, Praziquantel, Enzyme, Biochemistry, Acetylation, schistosoma mansoni, Sirtuin, biology.protein, Molecular Medicine, Schistosoma mansoni, medicine.drug

Abstract

The standard drug for treatment of the neglected disease Schistosomiasis is Praziquantel, and the possible emergence of resistance to this treatment makes the research on novel therapeutic agents necessary and urgent. To this end, the targeting of Schistosoma mansoni epigenetic enzymes, which regulate the parasitic life cycle, emerged as promising approach. Due to strong effects of human Sirtuin inhibitors on parasite survival and reproduction, Schistosoma sirtuins were postulated as potential therapeutic targets. In vitro testing of synthetic substrates of SmSirt2 and kinetic experiments on a myristoylated peptide newly demonstrated lysine long chain deacylation as an intrinsic SmSirt2 activity in addition to the known deacetylation. Focused in vitro screening of the GSK Kinetobox library and structure-activity relationships (SAR) of identified hits, led to the first SmSirt2 inhibitors with activity in the low micromolar range. Several SmSirt2 inhibitors showed potency against both larval schistosomes (viability) and adult worms (pairing, egg laying) in culture without general toxicity to human cancer cells.

Published

2019

7. Effect of α-methoxy substitution on the anti-HIV activity of dihydropyrimidin-4(3 H)-ones

Author

Emmanuele Crespan, Giovanni Maga, Roberto Cirilli, Antonello Mai, Cristina Panella, Mariantonietta Forgione, Alessia Lucidi, Ivan A Kirillov, Rino Ragno, Eva Riveira-Muñoz, Alexandros Patsilinakos, Roger Badia, José A. Esté, M. B. Nawrozkij, Dante Rotili, Gebremedhin Solomon Hailu, Jorge I. Armijos Rivera, Daniela Tomaselli, and Alexandre S. Yablokov

Subjects

molecular medicine, drug discovery3003, pharmaceutical science, Stereochemistry, Anti-HIV Agents, Mutant, Stereoisomerism, Pyrimidinones, 01 natural sciences, High-performance liquid chromatography, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Protein structure, Drug Discovery, Drug Resistance, Viral, Structure–activity relationship, Potency, Humans, Binding site, 030304 developmental biology, 0303 health sciences, Binding Sites, virus diseases, HIV Reverse Transcriptase, 0104 chemical sciences, Protein Structure, Tertiary, Molecular Docking Simulation, 010404 medicinal & biomolecular chemistry, chemistry, Mutation, HIV-1, Methyl group

Abstract

Conformational restriction applied to dihydrobenzylpyrimidin-4-(3 H)-ones (DABOs) by the intoduction of a methyl group at the α-benzylic position is known to massively improve the anti-HIV-1 activity of these compounds. Here, we report the effects of methoxy substitution at the α-benzylic position in S-, NH-, and N, N-DABOs carrying 2,6-difluoro, 2-chloro-6-fluoro, or 2,6-dichloro substituted benzyl moieties. The various α-methoxy DABO series (12-14) present different SAR at the dihalo benzyl substitution, with the most potent compounds (12d,e and 13c) showing similar (picomolar/nanomolar) anti-HIV-1 potency as the corresponding α-methyl analogues against wt HIV-1, and 10-100-fold increased potency (up to low nanomolar) against clinically relevant K103N, Y181C, Y188L, IRLL98, and K103N+Y181C HIV-1 mutant strains, highlighting the importance of the α-methoxy substitution to provide highly efficient DABOs as "second generation" NNRTIs. HPLC enantioseparation of three of the most potent derivatives (12d, 13c, and 14c) provided single enantiomers with significant enantioselectivity in HIV-1 inhibition. Computational studies allowed to correlate the best antiviral activity with the ( R) absolute configuration at the α-methoxy stereogenic center.

Published

2019

8. Identification of novel quinazoline derivatives as potent antiplasmodial agents

Author

Johan Schultz, Dany Pechalrieu, Sergio Valente, Anne Bouchut, Tina S. Skinner-Adams, Giancarlo Fabrizi, Paola B. Arimondo, Urban Hoglund, Katherine T. Andrews, Roberta Mazzone, Sophia Lafitte, Antonello Mai, Alessia Lucidi, Christine Pierrot, Ming Jang Chua, Jamal Khalife, Dante Rotili, Institut Pasteur de Lille, Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome] [UNIROMA], Pharmacochimie de la Régulation Epigénétique du Cancer [ETaC], Réseau International des Instituts Pasteur (RIIP), Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], Kancera AB [Sweden], Adlego Biomedical AB [Sweden], Pharmacochimie de la Régulation Epigénétique du Cancer (ETaC), PIERRE FABRE-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS), Centre National de la Recherche Scientifique (CNRS), GRIFFITH UNIVERSITY AUS, Partenaires IRSTEA, Institut national de recherche en sciences et technologies pour l'environnement et l'agriculture (IRSTEA)-Institut national de recherche en sciences et technologies pour l'environnement et l'agriculture (IRSTEA), This work was supported by the Australian National Health and Medical Research Council (APP1074016 to K.T.A.), Italian PRIN 2016 (prot. 20152TE5PK to A.M.), AIRC 2016 (n. 19162 to A.M.), NIH (n. R01GM114306 to A.M.), Progetto Ateneo Sapienza 2017 (to D.R.), the A-ParaDDisE program funded under the European Union's Seventh Framework Programme (grant agreement no. 602080 to A.B., C.P., S.L., A.M., D.R., S.V., J.S., U.H., K.T.A. and J.K.) and Griffith University (GUIPRS and GUPRS scholarships to M.J.C.). We thank Mary Clarke (Griffith University) for technical assistance. We also thank the BioImaging Center Lille Facility for access to the BD FACSCanto II cytometer., European Project: 602080,EC:FP7:HEALTH,FP7-HEALTH-2013-INNOVATION-1,A-PARADDISE(2014), Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome] (UNIROMA), Griffith University [Brisbane], Centre d’Infection et d’Immunité de Lille (CIIL) - INSERM U1019 - UMR 9017 (CIIL), Université de Lille-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre Hospitalier Régional Universitaire [Lille] (CHRU Lille)-Centre National de la Recherche Scientifique (CNRS)-Institut Pasteur de Lille, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP), Università degli Studi di Roma 'La Sapienza' [Rome], and PIERRE FABRE-Centre National de la Recherche Scientifique (CNRS)

Subjects

Plasmodium berghei, Molecular Conformation, Pharmacology, MESH: Parasitic Sensitivity Tests, 01 natural sciences, Antimalarial agents, MESH: Dose-Response Relationship, Drug, Mice, MESH: Structure-Activity Relationship, Parasitic Sensitivity Tests, PK studies, Histone deacetylase inhibitors, Drug Discovery, P. berghei mouse model, MESH: Animals, Antimalarial Agent, DNA methyltransferase inhibitors, Artemisinin, MESH: Plasmodium falciparum, media_common, 0303 health sciences, Mice, Inbred BALB C, biology, Chemistry, General Medicine, 3. Good health, MESH: Quinazolines, [SDV.MP]Life Sciences [q-bio]/Microbiology and Parasitology, medicine.drug, Drug, antimalarial agents, histone deacetylase inhibitors, media_common.quotation_subject, Plasmodium falciparum, MESH: Mice, Inbred BALB C, Context (language use), 03 medical and health sciences, Antimalarials, Structure-Activity Relationship, In vivo, parasitic diseases, medicine, MESH: Plasmodium berghei, [CHIM]Chemical Sciences, Animals, Humans, MESH: Mice, 030304 developmental biology, MESH: Molecular Conformation, MESH: Humans, Dose-Response Relationship, Drug, 010405 organic chemistry, Organic Chemistry, Fibroblasts, biology.organism_classification, medicine.disease, MESH: Antimalarials, 0104 chemical sciences, MESH: Fibroblasts, Quinazolines, [SDV.SPEE]Life Sciences [q-bio]/Santé publique et épidémiologie, Malaria

Abstract

International audience; Despite the recent reductions in the global burden of malaria, this disease remains a devastating cause of death in tropical and subtropical regions. As there is no broadly effective vaccine for malaria, prevention and treatment still rely on chemotherapy. Unfortunately, emerging resistance to the gold standard artemisinin combination therapies means that new drugs with novel modes of action are urgently needed. In this context, Plasmodium histone modifying enzymes have emerged as potential drug targets, prompting us to develop and optimize compounds directed against such epigenetic targets. A panel of 51 compounds designed to target different epigenetic enzymes were screened for activity against Plasmodium falciparum parasites. Based on in vitro activity against drug susceptible and drug-resistant P. falciparum lines, selectivity index criterion and favorable pharmacokinetic properties, four compounds, one HDAC inhibitor (1) and three DNMT inhibitors (37, 43 and 45), were selected for preclinical studies in a mouse model of malaria. In vivo data showed that 37, 43 and 45 exhibited oral efficacy in the mouse model of Plasmodium berghei infection. These compounds represent promising starting points for the development of novel antimalarial drugs.

Published

2019

9. Synthesis and characterisation of a new benzamide-containing nitrobenzoxadiazole as a GSTP1-1 inhibitor endowed with high stability to metabolic hydrolysis

Author

Antonio Rosato, Luigi Quintieri, Francesca Sciarretta, Chiara Fulci, Veronica Di Paolo, Dante Rotili, Anastasia De Luca, Blasco Morozzo della Rocca, Anna Maria Caccuri, and Alessia Lucidi

Subjects

Models, Molecular, A375 human melanoma, glutathione, GSTP1-1, nitrobenzoxadiazoles, TRAF2, 4-chloro-7-nitrobenzofurazan, antineoplastic agents, benzamides, cell line, tumor, cell proliferation, cell survival, dose-response relationship, drug, drug screening assays, antitumor, enzyme inhibitors, glutathione S-transferase pi, humans, hydrolysis, models, molecular, molecular structure, structure-activity relationship, Drug Screening Assays, 01 natural sciences, Nitrobenzoxadiazoles, 4-Chloro-7-nitrobenzofurazan, Antineoplastic Agents, Benzamides, Cell Line, Tumor, Cell Proliferation, Cell Survival, Dose-Response Relationship, Drug, Drug Screening Assays, Antitumor, Enzyme Inhibitors, Glutathione S-Transferase pi, Humans, Hydrolysis, Molecular Structure, Structure-Activity Relationship, metabolic stability, chemistry.chemical_compound, Models, Amide, Drug Discovery, Benzamide, Cytotoxicity, Tumor, General Medicine, Drug, Stereochemistry, Thio, Article, metabolic stability, Cell Line, Dose-Response Relationship, Structure-Activity Relationship, Structure–activity relationship, Settore BIO/10, Pharmacology, 010405 organic chemistry, lcsh:RM1-950, Molecular, Glutathione, Antitumor, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, lcsh:Therapeutics. Pharmacology, chemistry, Microsome

Abstract

The antitumor agent 6-((7-nitrobenzo[c][1,2,5]oxadiazol-4-yl)thio)hexan-1-ol (1) is a potent inhibitor of GSTP1-1, a glutathione S-transferase capable of inhibiting apoptosis by binding to JNK1 and TRAF2. We recently demonstrated that, unlike its parent compound, the benzoyl ester of 1 (compound 3) exhibits negligible reactivity towards GSH, and has a different mode of interaction with GSTP1-1. Unfortunately, 3 is susceptible to rapid metabolic hydrolysis. In an effort to improve the metabolic stability of 3, its ester group has been replaced by an amide, leading to N-(6-((7-nitrobenzo[c][1,2,5]oxadiazol-4-yl)thio)hexyl)benzamide (4). Unlike 3, compound 4 was stable to human liver microsomal carboxylesterases, but retained the ability to disrupt the interaction between GSTP1-1 and TRAF2 regardless of GSH levels. Moreover, 4 exhibited both a higher stability in the presence of GSH and a greater cytotoxicity towards cultured A375 melanoma cells, in comparison with 1 and its analog 2. These findings suggest that 4 deserves further preclinical testing.

Published

2019

10. DNA Methylation: Biological Implications and Modulation of Its Aberrant Dysregulation

Author

Alessia Lucidi, Dante Rotili, Daniela Tomaselli, and Antonello Mai

Subjects

Tumor suppressor genes, Epigenetics, DNA methyltransferase, DNMT inhibitors, Anticancer therapy, Cancer, DNA Methyltransferase Inhibitor, Computational biology, Biology, medicine.disease, Mechanism of action, DNA methylation, medicine, medicine.symptom

Abstract

The alteration of the DNA methylation pattern is often related to the onset of diseases based on epigenetic dysregulation, primarily cancer. In this scenery the development of DNA methyltransferase inhibitors is one of the most attractive challenges for anticancer therapy. The present chapter proposes a comprehensive classification of the DNA methyltransferase inhibitors known in literature, on the basis of their natural or synthetic nature and their mechanism of action.

Published

2019

11. Epigenetic polypharmacology: A new frontier for epi-drug discovery

Author

Antonello Mai, Dante Rotili, Alessia Lucidi, and Daniela Tomaselli

Subjects

Combination therapy, hybrid molecules design, Polypharmacology, Computational biology, cancer, epigenetics, polypharmacology, Ligands, Article, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Drug Discovery, Medicine, Animals, Humans, Target therapy, Epigenetics, 030304 developmental biology, Pharmacology, 0303 health sciences, Clinical Trials as Topic, business.industry, Drug discovery, Advanced stage, Molecular network, 030220 oncology & carcinogenesis, Molecular Medicine, Histone deacetylase, business

Abstract

Recently, despite the great success achieved by the so-called "magic bullets" in the treatment of different diseases through a marked and specific interaction with the target of interest, the pharmacological research is moving toward the development of "molecular network active compounds," embracing the related polypharmacology approach. This strategy was born to overcome the main limitations of the single target therapy leading to a superior therapeutic effect, a decrease of adverse reactions, and a reduction of potential mechanism(s) of drug resistance caused by robustness and redundancy of biological pathways. It has become clear that multifactorial diseases such as cancer, neurological, and inflammatory disorders, may require more complex therapeutic approaches hitting a certain biological system as a whole. Concerning epigenetics, the goal of the multi-epi-target approach consists in the development of small molecules able to simultaneously and (often) reversibly bind different specific epi-targets. To date, two dual histone deacetylase/kinase inhibitors (CUDC-101 and CUDC-907) are in an advanced stage of clinical trials. In the last years, the growing interest in polypharmacology encouraged the publication of high-quality reviews on combination therapy and hybrid molecules. Hence, to update the state-of-the-art of these therapeutic approaches avoiding redundancy, herein we focused only on multiple medication therapies and multitargeting compounds exploiting epigenetic plus nonepigenetic drugs reported in the literature in 2018. In addition, all the multi-epi-target inhibitors known in literature so far, hitting two or more epigenetic targets, have been included.

Published

2018

12. Pharmacological activation of SIRT6 triggers lethal autophagy in human cancer cells

Author

Dante Rotili, Clemens Steegborn, Luca Di Leo, Alessia Lucidi, Antonello Mai, Annamaria Biroccio, Carlo Leonetti, Pasquale Zizza, Daniela Trisciuoglio, Donatella Del Bufalo, Sara Iachettini, Erica Salvati, Angela Maria Rizzo, and Maria Rosa Ciriolo

Subjects

0301 basic medicine, SIRT6, immunology, cellular and molecular neuroscience, cell biology, cancer research, Cancer Research, Programmed cell death, Immunology, Apoptosis, AMP-Activated Protein Kinases, Histones, 03 medical and health sciences, Cellular and Molecular Neuroscience, Enzyme activator, 0302 clinical medicine, Neoplasms, Quinoxalines, Autophagy, Autophagy-Related Protein-1 Homolog, Humans, Sirtuins, Pyrroles, lcsh:QH573-671, Settore BIO/10, Caspase, Cell Proliferation, biology, Activator (genetics), Chemistry, lcsh:Cytology, Cell Cycle, Autophagosomes, Intracellular Signaling Peptides and Proteins, Acetylation, Cell Biology, Cell cycle, HCT116 Cells, Cell biology, Enzyme Activation, cell death, 030104 developmental biology, 030220 oncology & carcinogenesis, Sirtuin, biology.protein, Reactive Oxygen Species, HeLa Cells, Signal Transduction

Abstract

Sirtuin 6 (SIRT6) is a member of the NAD+-dependent class III deacetylase sirtuin family, which plays a key role in cancer by controlling transcription, genome stability, telomere integrity, DNA repair, and autophagy. Here we analyzed the molecular and biological effects of UBCS039, the first synthetic SIRT6 activator. Our data demonstrated that UBCS039 induced a time-dependent activation of autophagy in several human tumor cell lines, as evaluated by increased content of the lipidated form of LC3B by western blot and of autophagosomal puncta by microscopy analysis of GFP-LC3. UBCS039-mediated activation of autophagy was strictly dependent on SIRT6 deacetylating activity since the catalytic mutant H133Y failed to activate autophagy. At the molecular level, SIRT6-mediated autophagy was triggered by an increase of ROS levels, which, in turn, resulted in the activation of the AMPK-ULK1-mTOR signaling pathway. Interestingly, antioxidants were able to completely counteract UBCS039-induced autophagy, suggesting that ROS burst had a key role in upstream events leading to autophagy commitment. Finally, sustained activation of SIRT6 resulted in autophagy-related cell death, a process that was markedly attenuated using either a pan caspases inhibitor (zVAD-fmk) or an autophagy inhibitor (CQ). Overall, our results identified UBCS039 as an efficient SIRT6 activator, thereby providing a proof of principle that modulation of the enzyme can influence therapeutic strategy by enhancing autophagy-dependent cell death.

Published

2018

13. Pyrrole- and indole-containing tranylcypromine derivatives as novel lysine-specific demethylase 1 inhibitors active on cancer cells

Author

Stefano Rovida, Giulia Stazi, Paola Dessanti, Veronica Rodriguez, Mario Varasi, Oronza A. Botrugno, Dante Rotili, Antonello Mai, Ciro Mercurio, Andrea Mattevi, Saverio Minucci, Giuseppe Ciossani, Sergio Valente, Alessia Lucidi, and Paola Vianello

Subjects

animal structures, Stereochemistry, tranylcypromine, Pharmaceutical Science, Biochemistry, Residue (chemistry), chemistry.chemical_compound, lysine-specific demethylase 1, Drug Discovery, medicine, stereoisomers, Moiety, Pyrrole, Pharmacology, Indole test, epigenetics, Cell growth, Chemistry, Organic Chemistry, Tranylcypromine, leukemia, Cell culture, Cancer cell, Molecular Medicine, medicine.drug

Abstract

On the basis of previous research showing the capability of N-carbobenzyloxy-(Z-)amino acid-tranylcypromine (-TCPA) derivatives to inhibit LSD1, we inserted at the 4-amino-TCPA moiety first a Z-Pro (9) and a Z-Gly (10) residue and then, after the encouraging data obtained for 9, a pyrrole and an indole ring in which the relative N1 position carried a acetophenone, a N-phenyl/benzylacetamide, or a Z chain (11a–f and 12a–f, respectively). In both series, the Z-pyrrole and indole derivatives 11e, f and 12e, f displayed high LSD1 inhibitory activity. The compounds are able to inhibit LSD1 in NB4 cells, increasing the expression of two related genes, GFI-1b and ITGAM, and to induce cell growth arrest in the AML MB4-11 and APL NB4 cell lines.

Published

2015

14. Development of 1,2,4-Oxadiazoles as Potent and Selective Inhibitors of the Human Deacetylase Sirtuin 2: Structure-Activity Relationship, X-ray Crystal Structure, and Anticancer Activity

Author

Francesca Baratta, Clemens Steegborn, Mariantonietta Forgione, Vincenzo Carafa, Angela Nebbioso, Daniela Passeri, Gebremedhin Solomon Hailu, Dante Rotili, Nicola Giacchè, Roberto Pellicciari, Sébastien Moniot, Lucia Altucci, Antonello Mai, Alessia Lucidi, Moniot, Sébastien, Forgione, Mariantonietta, Lucidi, Alessia, Hailu, Gebremedhin S, Nebbioso, Angela, Carafa, Vincenzo, Baratta, Francesca, Altucci, Lucia, Giacché, Nicola, Passeri, Daniela, Pellicciari, Roberto, Mai, Antonello, Steegborn, Clemen, and Rotili, Dante

Subjects

Models, Molecular, 0301 basic medicine, Stereochemistry, Antineoplastic Agents, Apoptosis, Peptide, Crystallography, X-Ray, mammalian sirtuins, tumor-suppressor, Parkinsons-disease, emerging role, cell-cycle, discovery, targets, design, cancer, tumorigenesis, SIRT2, 01 natural sciences, Structure-Activity Relationship, 03 medical and health sciences, Sirtuin 2, Western blot, Cell Line, Tumor, Neoplasms, Drug Discovery, medicine, Humans, Structure–activity relationship, chemistry.chemical_classification, Oxadiazoles, biology, U937 cell, medicine.diagnostic_test, 010405 organic chemistry, Chemistry, 3. Good health, 0104 chemical sciences, 030104 developmental biology, Biochemistry, Sirtuin, biology.protein, Molecular Medicine, NAD+ kinase

Abstract

Sirt2 is a target for the treatment of neurological, metabolic, and age-related diseases including cancer. Here we report a series of Sirt2 inhibitors based on the 1,2,4-oxadiazole scaffold. These compounds are potent Sirt2 inhibitors active at single-digit μM level by using the Sirt2 substrate α-tubulin-acetylLys40 peptide and inactive up to 100 μM against Sirt1, -3, and -5 (deacetylase and desuccinylase activities). Their mechanism of inhibition is uncompetitive toward both the peptide substrate and NAD(+), and the crystal structure of a 1,2,4-oxadiazole analog in complex with Sirt2 and ADP-ribose reveals its orientation in a still unexplored subcavity useful for further inhibitor development. Tested in leukemia cell lines, 35 and 39 induced apoptosis and/or showed antiproliferative effects at 10 or 25 μM after 48 h. Western blot analyses confirmed the involvement of Sirt2 inhibition for their effects in NB4 and in U937 cells. Our results provide novel Sirt2 inhibitors with a compact scaffold and structural insights for further inhibitor improvement.

Published

2017

15. Polymyxins and quinazolines are LSD1/KDM1A inhibitors with unusual structural features

Author

Dante Rotili, Simona Pilotto, Biagina Marrocco, Andrea Mattevi, Alessia Lucidi, Giuseppe Ciossani, Parinaz Mehdipour, Antonello Mai, Federico Forneris, Valentina Speranzini, Mariantonietta Forgione, and Sameer Velankar

Subjects

0301 basic medicine, Epigenomics, reversible inhibition, LSD1, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Histone demethylation, Neoplasms, Quinazoline, Moiety, Animals, Humans, Polymyxins, Enzyme Inhibitors, histone demethylation, polymyxin, quinazoline, Research Articles, chemistry.chemical_classification, Histone Demethylases, Multidisciplinary, biology, SciAdv r-articles, KDM1A, 3. Good health, Amino acid, 030104 developmental biology, Histone, Enzyme, chemistry, 030220 oncology & carcinogenesis, biology.protein, Quinazolines, Demethylase, Protein Binding, Research Article

Abstract

The binding mode of newly discovered histone demethylase inhibitors could have applications in the design and repurposing of drugs., Because of its involvement in the progression of several malignant tumors, the histone lysine-specific demethylase 1 (LSD1) has become a prominent drug target in modern medicinal chemistry research. We report on the discovery of two classes of noncovalent inhibitors displaying unique structural features. The antibiotics polymyxins bind at the entrance of the substrate cleft, where their highly charged cyclic moiety interacts with a cluster of positively charged amino acids. The same site is occupied by quinazoline-based compounds, which were found to inhibit the enzyme through a most peculiar mode because they form a pile of five to seven molecules that obstruct access to the active center. These data significantly indicate unpredictable strategies for the development of epigenetic inhibitors.

Published

2016