Your search keyword '"Madia VN"' showing total 46 results

1. Discovery of N-aryl-naphthylamines as in vitro inhibitors of the interaction between HIV integrase and the cofactor LEDGF/p75

Author

Francesco Saccoliti, Luigi Scipione, Giuliana Cuzzucoli Crucitti, Ettore Novellino, Francesco Saverio Di Leva, Luca Pescatori, Silvano Tortorella, Zeger Debyser, Sandro Cosconati, Giovanni Pupo, Antonella Messore, Valentina Noemi Madia, Roberta Costi, Roberto Di Santo, Frauke Christ, Cuzzucoli Crucitti, G, Pescatori, L, Messore, A, Madia, Vn, Pupo, G, Saccoliti, F, Scipione, L, Tortorella, S, Di Leva, F, Cosconati, Sandro, Novellino, E, Debyser, Z, Christ, F, Costi, R, Di Santo, R., Cuzzucoli Crucitti, Giuliana, Pescatori, Luca, Messore, Antonella, Madia, Valentina Noemi, Pupo, Giovanni, Saccoliti, Francesco, Scipione, Luigi, Tortorella, Silvano, Di Leva, Francesco Saverio, Novellino, Ettore, Debyser, Zeger, Christ, Frauke, Costi, Roberta, and Di Santo, Roberto

Subjects

LEDGINs, Models, Molecular, Molecular model, Stereochemistry, Plasma protein binding, HIV Integrase, Integrase, N-aryl-naphthylamine, Cofactor, Structure-Activity Relationship, para-Aminobenzoate, LEDGF/p75, Drug Discovery, Intercellular Signaling Peptides and Protein, Tumor Cells, Cultured, para-Aminobenzoates, Structure–activity relationship, Humans, LEDGIN, HIV Integrase Inhibitors, Pharmacology, biology, Dose-Response Relationship, Drug, Molecular Structure, Chemistry, Drug discovery, Drug Discovery3003 Pharmaceutical Science, Organic Chemistry, General Medicine, Small molecule, In vitro, HIV Integrase Inhibitor, integrase, drug discovery3003 pharmaceutical science, organic chemistry, pharmacology, 1-Naphthylamine, biology.protein, Intercellular Signaling Peptides and Proteins, Human, Protein Binding

Abstract

A series of N-aryl-naphthylamines, exemplified by the structures 11-16, were chosen for an in-house library screening to assay their ability to disrupt the interaction between the LEDGF cofactor and the HIV integrase. Structure modification led also to design and synthesize new compounds 17a-f. Compounds 11e,h,k,n, 13b, and 14 showed good activity in AlphaScreen assay. The most active compound 11e (IC50 Combining double low line 2.5 μM) was selected for molecular modeling studies and showed a binding mode similar to the one of the known LEDGIN 8.

Published

2015

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

Author

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

Subjects

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

Abstract

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

Published

2015

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

Author

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

Subjects

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

Abstract

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

Published

2014

4. Quinolinonyl Derivatives as Dual Inhibitors of the HIV-1 Integrase Catalytic Site and Integrase-RNA interactions.

Author

Patacchini E, Madia VN, Albano A, Ruggieri G, Messore A, Ialongo D, Saccoliti F, Scipione L, Cosconati S, Koneru PC, Haney R, Kvaratskhelia M, Di Santo R, and Costi R

Abstract

The HIV-1 integrase (IN) plays a critical role in the viral lifecycle by integrating the viral DNA into the host chromosome. The catalytic function of IN has been exploited as a target, with five drugs acting as active site binders (IN strand transfer inhibitors, INSTIs). However, IN mutations conferring low-level resistance to INSTIs have been reported. Therefore, new IN inhibitors with different mechanisms of action are needed. The allosteric inhibition of IN, exerted by allosteric IN inhibitors (ALLINIs), is gaining interest. ALLINIs inhibit IN by inducing aberrant IN multimerization with different mechanisms. Furthermore, recent discoveries unveiled that IN has an under-studied yet equally vital second function. This involves IN binding to the RNA genome in virions, necessary for proper virion maturation. In this work, we describe a series of quinolinonyl derivatives as inhibitors of both the IN catalytic functions and IN-RNA interactions, which impair both early and late steps of viral replication., Competing Interests: The authors declare no competing financial interest., (© 2024 American Chemical Society.)

Published

2024

5. New Thiazolidine-4-One Derivatives as SARS-CoV-2 Main Protease Inhibitors.

Author

Messore A, Malune P, Patacchini E, Madia VN, Ialongo D, Arpacioglu M, Albano A, Ruggieri G, Saccoliti F, Scipione L, Tramontano E, Canton S, Corona A, Scognamiglio S, Paulis A, Suleiman M, Al-Maqtari HM, Abid FMA, Kawsar SMA, Sankaranarayanan M, Di Santo R, Esposito F, and Costi R

Abstract

It has been more than four years since the first report of SARS-CoV-2, and humankind has experienced a pandemic with an unprecedented impact. Moreover, the new variants have made the situation even worse. Among viral enzymes, the SARS-CoV-2 main protease (M pro ) has been deemed a promising drug target vs. COVID-19. Indeed, M pro is a pivotal enzyme for viral replication, and it is highly conserved within coronaviruses. It showed a high extent of conservation of the protease residues essential to the enzymatic activity, emphasizing its potential as a drug target to develop wide-spectrum antiviral agents effective not only vs. SARS-CoV-2 variants but also against other coronaviruses. Even though the FDA-approved drug nirmatrelvir, a M pro inhibitor, has boosted the antiviral therapy for the treatment of COVID-19, the drug shows several drawbacks that hinder its clinical application. Herein, we report the synthesis of new thiazolidine-4-one derivatives endowed with inhibitory potencies in the micromolar range against SARS-CoV-2 M pro . In silico studies shed light on the key structural requirements responsible for binding to highly conserved enzymatic residues, showing that the thiazolidinone core acts as a mimetic of the Gln amino acid of the natural substrate and the central role of the nitro-substituted aromatic portion in establishing π-π stacking interactions with the catalytic His-41 residue.

Published

2024

6. Miconazole-like Scaffold is a Promising Lead for Naegleria fowleri -Specific CYP51 Inhibitors.

Author

Sharma V, Madia VN, Tudino V, Nguyen JV, Debnath A, Messore A, Ialongo D, Patacchini E, Palenca I, Basili Franzin S, Seguella L, Esposito G, Petrucci R, Di Matteo P, Bortolami M, Saccoliti F, Di Santo R, Scipione L, Costi R, and Podust LM

Subjects

14-alpha Demethylase Inhibitors pharmacology, Drug Discovery, Miconazole, Naegleria fowleri

Abstract

Developing drugs for brain infection by Naegleria fowleri is an unmet medical need. We used a combination of cheminformatics, target-, and phenotypic-based drug discovery methods to identify inhibitors that target an essential N. fowleri enzyme, sterol 14-demethylase (NfCYP51). A total of 124 compounds preselected in silico were tested against N. fowleri . Nine primary hits with EC 50 ≤ 10 μM were phenotypically identified. Cocrystallization with NfCYP51 focused attention on one primary hit, miconazole-like compound 2a . The S -enantiomer of 2a produced a 1.74 Å cocrystal structure. A set of analogues was then synthesized and evaluated to confirm the superiority of the S -configuration over the R -configuration and the advantage of an ether linkage over an ester linkage. The two compounds, S - 8b and S - 9b , had an improved EC 50 and K D compared to 2a . Importantly, both were readily taken up into the brain. The brain-to-plasma distribution coefficient of S - 9b was 1.02 ± 0.12, suggesting further evaluation as a lead for primary amoebic meningoencephalitis.

Published

2023

7. Diketo acid inhibitors of nsp13 of SARS-CoV-2 block viral replication.

Author

Corona A, Madia VN, De Santis R, Manelfi C, Emmolo R, Ialongo D, Patacchini E, Messore A, Amatore D, Faggioni G, Artico M, Iaconis D, Talarico C, Di Santo R, Lista F, Costi R, and Tramontano E

Subjects

Humans, Viral Nonstructural Proteins genetics, RNA Helicases metabolism, Virus Replication, Antiviral Agents pharmacology, SARS-CoV-2 metabolism, COVID-19

Abstract

For RNA viruses, RNA helicases have long been recognized to play critical roles during virus replication cycles, facilitating proper folding and replication of viral RNAs, therefore representing an ideal target for drug discovery. SARS-CoV-2 helicase, the non-structural protein 13 (nsp13) is a highly conserved protein among all known coronaviruses, and, at the moment, is one of the most explored viral targets to identify new possible antiviral agents. In the present study, we present six diketo acids (DKAs) as nsp13 inhibitors able to block both SARS-CoV-2 nsp13 enzymatic functions. Among them four compounds were able to inhibit viral replication in the low micromolar range, being active also on other human coronaviruses such as HCoV229E and MERS CoV. The experimental investigation of the binding mode revealed ATP-non-competitive kinetics of inhibition, not affected by substrate-displacement effect, suggesting an allosteric binding mode that was further supported by molecular modelling calculations predicting the binding into an allosteric conserved site located in the RecA2 domain., 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 © 2023 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2023

8. Role of a Novel Heparanase Inhibitor on the Balance between Apoptosis and Autophagy in U87 Human Glioblastoma Cells.

Author

Manganelli V, Misasi R, Riitano G, Capozzi A, Mattei V, Caglar TR, Ialongo D, Madia VN, Messore A, Costi R, Di Santo R, Sorice M, and Garofalo T

Subjects

Humans, Apoptosis, Apoptosis Regulatory Proteins metabolism, Autophagy, Cell Line, Tumor, Glucuronidase antagonists & inhibitors, Glucuronidase metabolism, Glioblastoma metabolism

Abstract

Background: Heparanase (HPSE) is an endo-β-glucuronidase that cleaves heparan sulfate side chains, leading to the disassembly of the extracellular matrix, facilitating cell invasion and metastasis dissemination. In this research, we investigated the role of a new HPSE inhibitor, RDS 3337, in the regulation of the autophagic process and the balance between apoptosis and autophagy in U87 glioblastoma cells., Methods: After treatment with RDS 3337, cell lysates were analyzed for autophagy and apoptosis-related proteins by Western blot., Results: We observed, firstly, that LC3II expression increased in U87 cells incubated with RDS 3337, together with a significant increase of p62/SQSTM1 levels, indicating that RDS 3337 could act through the inhibition of autophagic-lysosomal flux of LC3-II, thereby leading to accumulation of lipidated LC3-II form. Conversely, the suppression of autophagic flux could activate apoptosis mechanisms, as revealed by the activation of caspase 3, the increased level of cleaved Parp1, and DNA fragmentation., Conclusions: These findings support the notion that HPSE promotes autophagy, providing evidence that RDS 3337 blocks autophagic flux. It indicates a role for HPSE inhibitors in the balance between apoptosis and autophagy in U87 human glioblastoma cells, suggesting a potential role for this new class of compounds in the control of tumor growth progression.

Published

2023

9. Effects of Modified Glucosamine on the Chondrogenic Potential of Circulating Stem Cells under Experimental Inflammation.

Author

Gasparella M, Cenzi C, Piccione M, Madia VN, Di Santo R, Tudino V, Artico M, Taurone S, De Ponte C, Costi R, and Di Liddo R

Subjects

Humans, NF-KappaB Inhibitor alpha metabolism, Tumor Necrosis Factor-alpha metabolism, Stem Cells, Cell Differentiation, Inflammation drug therapy, Inflammation metabolism, Chondrogenesis, Cells, Cultured, Glucosamine pharmacology, Glucosamine metabolism, Chondrocytes metabolism

Abstract

Glucosamine (GlcN) is a glycosaminoglycan (GAGs) constituent in connective tissues. It is naturally produced by our body or consumed from diets. In the last decade, in vitro and in vivo trials have demonstrated that the administration of GlcN or its derivates has a protective effect on cartilage when the balance between catabolic and anabolic processes is disrupted and cells are no longer able to fully compensate for the loss of collagen and proteoglycans. To date, these benefits are still controversial because the mechanism of action of GlcN is not yet well clarified. In this study, we have characterized the biological activities of an amino acid (AA) derivate of GlcN, called DCF001, in the growth and chondrogenic induction of circulating multipotent stem cells (CMCs) after priming with tumor necrosis factor-alpha (TNFα), a pleiotropic cytokine commonly expressed in chronic inflammatory joint diseases. In the present work, stem cells were isolated from the human peripheral blood of healthy donors. After priming with TNFα (10 ng/mL) for 3 h, cultures were treated for 24 h with DCF001 (1 μg/mL) dissolved in a proliferative (PM) or chondrogenic (CM) medium. Cell proliferation was analyzed using a Corning ® Cell Counter and trypan blue exclusion technique. To evaluate the potentialities of DCF001 in counteracting the inflammatory response to TNFα, we measured the amount of extracellular ATP (eATP) and the expression of adenosine-generating enzymes CD39/CD73, TNFα receptors, and NF-κB inhibitor IκBα using flow cytometry. Finally, total RNA was extracted to perform a gene expression study of some chondrogenic differentiation markers (COL2A1, RUNX2, and MMP13). Our analysis has shed light on the ability of DCF001 to (a) regulate the expression of CD39, CD73, and TNF receptors; (b) modulate eATP under differentiative induction; (c) enhance the inhibitory activity of IκBα, reducing its phosphorylation after TNFα stimulation; and (d) preserve the chondrogenic potentialities of stem cells. Although preliminary, these results suggest that DCF001 could be a valuable supplement for ameliorating the outcome of cartilage repair interventions, enhancing the efficacy of endogenous stem cells under inflammatory stimuli.

Published

2023

10. Synergistic Effects of Caffeine in Combination with Conventional Drugs: Perspectives of a Drug That Never Ages.

Author

Ialongo D, Tudino V, Arpacioglu M, Messore A, Patacchini E, Costi R, Di Santo R, and Madia VN

Abstract

Plants have been known since ancient times for their healing properties, being used as preparations against human diseases of different etiologies. More recently, natural products have been studied and characterized, isolating the phytochemicals responsible for their bioactivity. Most certainly, there are currently numerous active compounds extracted from plants and used as drugs, dietary supplements, or sources of bioactive molecules that are useful in modern drug discovery. Furthermore, phytotherapeutics can modulate the clinical effects of co-administered conventional drugs. In the last few decades, the interest has increased even more in studying the positive synergistic effects between plant-derived bioactives and conventional drugs. Indeed, synergism is a process where multiple compounds act together to exert a merged effect that is greater than that of each of them summed together. The synergistic effects between phytotherapeutics and conventional drugs have been described in different therapeutic areas, and many drugs are based on synergistic interactions with plant derivatives. Among them, caffeine has shown positive synergistic effects with different conventional drugs. Indeed, in addition to their multiple pharmacological activities, a growing body of evidence highlights the synergistic effects of caffeine with different conventional drugs in various therapeutic fields. This review aims to provide an overview of the synergistic therapeutic effects of caffeine and conventional drugs, summarizing the progress reported to date.

Published

2023

11. Plants and Small Molecules: An Up-and-Coming Synergy.

Author

Lepri A, Longo C, Messore A, Kazmi H, Madia VN, Di Santo R, Costi R, and Vittorioso P

Abstract

The emergence of Arabidopsis thaliana as a model system has led to a rapid and wide improvement in molecular genetics techniques for studying gene function and regulation. However, there are still several drawbacks that cannot be easily solved with molecular genetic approaches, such as the study of unfriendly species, which are of increasing agronomic interest but are not easily transformed, thus are not prone to many molecular techniques. Chemical genetics represents a methodology able to fill this gap. Chemical genetics lies between chemistry and biology and relies on small molecules to phenocopy genetic mutations addressing specific targets. Advances in recent decades have greatly improved both target specificity and activity, expanding the application of this approach to any biological process. As for classical genetics, chemical genetics also proceeds with a forward or reverse approach depending on the nature of the study. In this review, we addressed this topic in the study of plant photomorphogenesis, stress responses and epigenetic processes. We have dealt with some cases of repurposing compounds whose activity has been previously proven in human cells and, conversely, studies where plants have been a tool for the characterization of small molecules. In addition, we delved into the chemical synthesis and improvement of some of the compounds described.

Published

2023

12. Pyrrolyl and Indolyl α-γ-Diketo Acid Derivatives Acting as Selective Inhibitors of Human Carbonic Anhydrases IX and XII.

Author

Ialongo D, Messore A, Madia VN, Tudino V, Nocentini A, Gratteri P, Giovannuzzi S, Supuran CT, Nicolai A, Scarpa S, Taurone S, Camarda M, Artico M, Papa V, Saccoliti F, Scipione L, Di Santo R, and Costi R

Abstract

Solid tumors are active tissues containing hypoxic regions and producing metabolic acids. By decreasing pH, cancer cells create a hostile environment for surrounding host cells and foster tumor growth and progression. By governing acid/base regulation, carbonic anhydrases (CAs) are involved in several physiological/pathological processes, including tumors. Indeed, CAs are clinically relevant in cancer therapy as among the fifteen human isoforms, two of them, namely CA IX (overexpressed in solid tumors and associated with increased metastasis and poor prognosis) and CA XII (overexpressed in some tumors) are involved in tumorigenesis. Targeting these two isoforms is considered as a pertinent approach to develop new cancer therapeutics. Several CA inhibitors (CAIs) have been described, even though they are unselective inhibitors of different isoforms. Thus, efforts are needed to find new selective CAIs. In this work, we described new diketo acid derivatives as CAIs, with the best acting compounds 1c and 5 as nanomolar inhibitors of CA IX and XII, being also two orders of magnitude selective over CAs I and II. Molecular modeling studies showed the different binding poses of the best acting CAIs within CA II and IX, highlighting the key structural features that could confer the ability to establish specific interactions within the enzymes. In different tumor cell lines overexpressing CA IX and XII, the tested compounds showed antiproliferative activity already at 24 h treatment, with no effects on somatic not transformed cells.

Published

2023

13. Inhibition of Leishmania infantum Trypanothione Reductase by New Aminopropanone Derivatives Interacting with the NADPH Binding Site.

Author

Madia VN, Ialongo D, Patacchini E, Exertier C, Antonelli L, Colotti G, Messore A, Tudino V, Saccoliti F, Scipione L, Ilari A, Costi R, and Di Santo R

Subjects

Humans, NADP metabolism, Models, Molecular, NADH, NADPH Oxidoreductases, Binding Sites, Leishmania infantum, Antiprotozoal Agents pharmacology

Abstract

Background: As a result of the paucity of treatment, Leishmaniasis continues to provoke about 60,000 deaths every year worldwide. New molecules are needed, and drug discovery research is oriented toward targeting proteins crucial for parasite survival. Among them, trypanothione reductase (TR) is of remarkable interest owing to its vital role in Leishmania species protozoan parasite life. Our previously identified compound 1 is a novel chemotype endowed with a unique mode of TR inhibition thanks to its binding to a formerly unknown but druggable site at the entrance of the NADPH binding cavity, absent in human glutathione reductase (hGR)., Methods: We designed and synthesized new 3-amino-1-arylpropan-1-one derivatives structurally related to compound 1 and evaluated their potential inhibition activity on TR from Leishmania infantum (LiTR). Cluster docking was performed to assess the binding poses of the compounds., Results: The newly synthesized compounds were screened at a concentration of 100 μM in in vitro assays and all of them proved to be active with residual activity percentages lower than 75%., Conclusions: Compounds 2a and 2b were the most potent inhibitors found, suggesting that an additional aromatic ring might be promising for enzymatic inhibition. Further structure-activity relationships are needed to optimize our compounds activity.

Published

2023

14. New Inhibitors of the Human p300/CBP Acetyltransferase Are Selectively Active against the Arabidopsis HAC Proteins.

Author

Longo C, Lepri A, Paciolla A, Messore A, De Vita D, Bonaccorsi di Patti MC, Amadei M, Madia VN, Ialongo D, Di Santo R, Costi R, and Vittorioso P

Subjects

Acetylation, Arsenate Reductases metabolism, CREB-Binding Protein metabolism, Ethylenes metabolism, Histone Acetyltransferases metabolism, Histones metabolism, Humans, Mediator Complex metabolism, p300-CBP Transcription Factors metabolism, Arabidopsis metabolism, Arabidopsis Proteins genetics, Arabidopsis Proteins metabolism

Abstract

Histone acetyltransferases (HATs) are involved in the epigenetic positive control of gene expression in eukaryotes. CREB-binding proteins (CBP)/p300, a subfamily of highly conserved HATs, have been shown to function as acetylases on both histones and non-histone proteins. In the model plant Arabidopsis thaliana among the five CBP/p300 HATs, HAC1, HAC5 and HAC12 have been shown to be involved in the ethylene signaling pathway. In addition, HAC1 and HAC5 interact and cooperate with the Mediator complex, as in humans. Therefore, it is potentially difficult to discriminate the effect on plant development of the enzymatic activity with respect to their Mediator-related function. Taking advantage of the homology of the human HAC catalytic domain with that of the Arabidopsis, we set-up a phenotypic assay based on the hypocotyl length of Arabidopsis dark-grown seedlings to evaluate the effects of a compound previously described as human p300/CBP inhibitor, and to screen previously described cinnamoyl derivatives as well as newly synthesized analogues. We selected the most effective compounds, and we demonstrated their efficacy at phenotypic and molecular level. The in vitro inhibition of the enzymatic activity proved the specificity of the inhibitor on the catalytic domain of HAC1, thus substantiating this strategy as a useful tool in plant epigenetic studies.

Published

2022

15. Ultrastructural Damages to H1N1 Influenza Virus Caused by Vapor Essential Oils.

Author

Madia VN, Toscanelli W, De Vita D, De Angelis M, Messore A, Ialongo D, Scipione L, Tudino V, D'Auria FD, Di Santo R, Garzoli S, Stringaro A, Colone M, Marchetti M, Superti F, Nencioni L, and Costi R

Subjects

Antiviral Agents pharmacology, Anti-Infective Agents pharmacology, Eucalyptus chemistry, Influenza A Virus, H1N1 Subtype, Melaleuca chemistry, Oils, Volatile chemistry, Oils, Volatile pharmacology

Abstract

Influenza viruses are transmitted from human to human via airborne droplets and can be transferred through contaminated environmental surfaces. Some works have demonstrated the efficacy of essential oils (EOs) as antimicrobial and antiviral agents, but most of them examined the liquid phases, which are generally toxic for oral applications. In our study, we describe the antiviral activity of Citrus bergamia , Melaleuca alternifolia , Illicium verum and Eucalyptus globulus vapor EOs against influenza virus type A. In the vapor phase, C. bergamia and M. alternifolia strongly reduced viral cytopathic effect without exerting any cytotoxicity. The E. globulus vapor EO reduced viral infection by 78% with no cytotoxicity, while I. verum was not effective. Furthermore, we characterized the EOs and their vapor phase by the head-space gas chromatography-mass spectrometry technique, observing that the major component found in each liquid EO is the same one of the corresponding vapor phases, with the exception of M. alternifolia . To deepen the mechanism of action, the morphological integrity of virus particles was checked by negative staining transmission electron microscopy, showing that they interfere with the lipid bilayer of the viral envelope, leading to the decomposition of membranes. We speculated that the most abundant components of the vapor EOs might directly interfere with influenza virus envelope structures or mask viral structures important for early steps of viral infection.

Published

2022

16. Design, Synthesis, and In Vitro, In Silico and In Cellulo Evaluation of New Pyrimidine and Pyridine Amide and Carbamate Derivatives as Multi-Functional Cholinesterase Inhibitors.

Author

Bortolami M, Pandolfi F, Tudino V, Messore A, Madia VN, De Vita D, Di Santo R, Costi R, Romeo I, Alcaro S, Colone M, Stringaro A, Espargaró A, Sabatè R, and Scipione L

Abstract

Alzheimer disease is an age-linked neurodegenerative disorder representing one of the greatest medical care challenges of our century. Several drugs are useful in ameliorating the symptoms, even if none could stop or reverse disease progression. The standard approach is represented by the cholinesterase inhibitors (ChEIs) that restore the levels of acetylcholine (ACh) by inhibiting the acetylcholinesterase (AChE). Still, their limited efficacy has prompted researchers to develop new ChEIs that could also reduce the oxidative stress by exhibiting antioxidant properties and by chelating the main metals involved in the disease. Recently, we developed some derivatives constituted by a 2-amino-pyrimidine or a 2-amino-pyridine moiety connected to various aromatic groups by a flexible amino-alkyl linker as new dual inhibitors of AChE and butyrylcholinesterase (BChE). Following our previous studies, in this work we explored the role of the flexible linker by replacing the amino group with an amide or a carbamic group. The most potent compounds showed higher selectivity against BChE in respect to AChE, proving also to possess a weak anti-aggregating activity toward Aβ 42 and tau and to be able to chelate Cu 2+ and Fe 3+ ions. Molecular docking and molecular dynamic studies proposed possible binding modes with the enzymes. It is noteworthy that these compounds were predicted as BBB-permeable and showed low cytotoxicity on the human brain cell line.

Published

2022

17. Oxidative stress and visual system: a review.

Author

Taurone S, Ralli M, Artico M, Madia VN, Scarpa S, Nottola SA, Maconi A, Betti M, Familiari P, Nebbioso M, Costi R, and Micera A

Abstract

Different types of tissues respond differently to the action of oxidative stress. The visual system is very sensitive to oxidative action due to continuous exposure to light. In consideration of the growing interest of scientific studies towards various compounds endowed with antioxidant and anti-inflammatory properties, we performed a review of the literature focusing on the use of some antioxidant molecules for the treatment of conditions affecting the visual system. In this study, we focused on the ability of two antioxidant agents, the small molecule α-lipoic acid (ALA) and the enzyme superoxide dismutase (SOD), to influence the neurodegenerative physiological processes related to aging and oxidative stress affecting the ocular segment. The literature data report that ALA and SOD can protect against neurodegenerative effects both the optic nerve and retina and, if administered together, they are able to lower the levels of oxidative stress, thus preventing neurodegeneration and reducing the apoptotic process., (Copyright © 2022 Taurone et al.)

Published

2022

18. New Pyrimidine and Pyridine Derivatives as Multitarget Cholinesterase Inhibitors: Design, Synthesis, and In Vitro and In Cellulo Evaluation.

Author

Bortolami M, Pandolfi F, Tudino V, Messore A, Madia VN, De Vita D, Di Santo R, Costi R, Romeo I, Alcaro S, Colone M, Stringaro A, Espargaró A, Sabatè R, and Scipione L

Subjects

Acetylcholinesterase metabolism, Animals, Butyrylcholinesterase metabolism, Horses, Humans, Molecular Docking Simulation, Molecular Structure, Pyridines, Pyrimidines pharmacology, Structure-Activity Relationship, Alzheimer Disease, Cholinesterase Inhibitors pharmacology

Abstract

A new series of pyrimidine and pyridine diamines was designed as dual binding site inhibitors of cholinesterases (ChEs), characterized by two small aromatic moieties separated by a diaminoalkyl flexible linker. Many compounds are mixed or uncompetitive acetylcholinesterase (AChE) and/or butyrylcholinesterase (BChE) nanomolar inhibitors, with compound 9 being the most active on Electrophorus electricus AChE ( Ee AChE) ( K i = 0.312 μM) and compound 22 on equine BChE ( eq BChE) ( K i = 0.099 μM). Molecular docking and molecular dynamic studies confirmed the interaction mode of our compounds with the enzymatic active site. UV-vis spectroscopic studies showed that these compounds can form complexes with Cu 2+ and Fe 3+ and that compounds 18 , 20 , and 30 have antioxidant properties. Interestingly, some compounds were also able to reduce Aβ 42 and tau aggregation, with compound 28 being the most potent (22.3 and 17.0% inhibition at 100 μM on Aβ 42 and tau, respectively). Moreover, the most active compounds showed low cytotoxicity on a human brain cell line and they were predicted as BBB-permeable.

Published

2021

19. Towards a new application of amaranth seed oil as an agent against Candida albicans .

Author

De Vita D, Messore A, Toniolo C, Frezza C, Scipione L, Bertea CM, Micera M, Di Sarno V, Madia VN, Pindinello I, Roscilli P, Botto A, Simonetti G, Orekhova A, Manfredini S, Costi R, and Di Santo R

Subjects

Antifungal Agents pharmacology, Microbial Sensitivity Tests, Plant Oils pharmacology, Seeds, Candida, Candida albicans

Abstract

Amaranthu s spp. (Amaranthaceae family), known as amaranth, are plants native of Central America, today produced in many parts of the world. due to their popularity popular as a health food. Because of its composition, amaranth can be considered to be attractive not only as a food but also for pharmaceutical and cosmetics uses. To date, antifungal activity of amaranth extracts has not been totally investigated, therefore the scope of this study was to evaluate the antifungal effect of the apolar fraction from Amaranthus cruentus L. seeds extract, alone and in association with antifungal drugs terbinafine, a common antifungal agent, which itself has only fungistatic effect on Candida albicans strains without exerting fungicidal activity. Our results demonstrate that this amaranth oil in combination with terbinafine has synergic fungistatic and fungicidal activity, with FICI of 0.466 and 0.496, respectively. No fungistatic and fungicidal activity of terbinafine alone at concentrations up to 64 μg/mL and amaranth oil alone at concentrations up to 2000 μg/mL, against all tested C. albicans strains, were observed. does not show activity towards Candida albicans strains but it can effectively potentiate the antifungal activity of terbinafine, a common antifungal agent which itself This result suggests the possible application of amaranth oil in the preparation of formulations with terbinafine for topical use.

Published

2021

20. Toxicological aspects of cannabinoid, pesticide and metal levels detected in light Cannabis inflorescences grown in Italy.

Author

Amendola G, Bocca B, Picardo V, Pelosi P, Battistini B, Ruggieri F, Attard Barbini D, De Vita D, Madia VN, Messore A, Di Santo R, and Costi R

Subjects

Cannabinoids analysis, Italy, Metals analysis, Pesticides analysis, Cannabinoids toxicity, Cannabis chemistry, Inflorescence chemistry, Metals toxicity, Pesticides toxicity

Abstract

Recently, the cultivation of light Cannabis, with a total THC content less than 0.6%, has been encouraged due to its industrial and therapeutic potential. This has increased the consumption of hemp for both smoking purposes and food preparation. Even so, Cannabis inflorescences are not subject to EU regulations and standards provided for food and tobacco products. A study was carried out on thirty-one inflorescences samples, collected in different Italian regions, in order to determine cannabinoids, pesticides and metals and to evaluate the exposure of consumers to contaminants and ensure a safe consumption. Contents of THC were always below 0.5%, while CBD ranged between 0.3 and 8.64%. The determination of 154 pesticides showed that 87% of the samples contained fungicides and insecticides in the range 0.01-185 μg/g. The most found are spinosad and cyprodinil. The concentration of metals ranged from 1 to more than 100 μg/g and As, Cd, Co, Cr, Hg, Cu, Mo, Ni and V exceeded the regulatory US limits for inhaled Cannabis products, while Pb exceeded them for both oral and inhaled products. These contaminants are intrinsically toxic and may affect public health. Actions are needed to establish regulatory measures and reduce the adverse effects caused by contaminants in Cannabis., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

21. Recent Advances in Recovery of Lycopene from Tomato Waste: A Potent Antioxidant with Endless Benefits.

Author

Madia VN, De Vita D, Ialongo D, Tudino V, De Leo A, Scipione L, Di Santo R, Costi R, and Messore A

Subjects

Antioxidants isolation & purification, Food Handling methods, Lycopene isolation & purification, Solanum lycopersicum chemistry, Solanum lycopersicum metabolism

Abstract

Growing attention to environmental protection leads food industries to adopt a model of "circular economy" applying safe and sustainable technologies to recover, recycle and valorize by-products. Therefore, by-products become raw material for other industries. Tomato processing industry produces significant amounts of by-products, consisting of skins and seeds. Tomato skin is very rich in lycopene, and from its seeds, high nutritional oil can be extracted. Alternative use of the two fractions not only could cut disposal costs but also allow one to extract bioactive compounds and an oil with a high nutritional value. This review focused on the recent advance in extraction of lycopene, whose beneficial effects on health are widely recognized.

Published

2021

22. Quinolinonyl Non-Diketo Acid Derivatives as Inhibitors of HIV-1 Ribonuclease H and Polymerase Functions of Reverse Transcriptase.

Author

Messore A, Corona A, Madia VN, Saccoliti F, Tudino V, De Leo A, Ialongo D, Scipione L, De Vita D, Amendola G, Novellino E, Cosconati S, Métifiot M, Andreola ML, Esposito F, Grandi N, Tramontano E, Costi R, and Di Santo R

Subjects

Anti-HIV Agents chemical synthesis, Anti-HIV Agents metabolism, HeLa Cells, Humans, Magnesium metabolism, Microbial Sensitivity Tests, Molecular Docking Simulation, Mutagenesis, Site-Directed, Mutation, Protein Binding, Quinolones chemical synthesis, Quinolones metabolism, Reverse Transcriptase Inhibitors chemical synthesis, Reverse Transcriptase Inhibitors metabolism, Ribonuclease H, Human Immunodeficiency Virus genetics, Ribonuclease H, Human Immunodeficiency Virus metabolism, Virus Replication drug effects, Anti-HIV Agents pharmacology, HIV-1 enzymology, Quinolones pharmacology, Reverse Transcriptase Inhibitors pharmacology, Ribonuclease H, Human Immunodeficiency Virus antagonists & inhibitors

Abstract

Novel anti-HIV agents are still needed to overcome resistance issues, in particular inhibitors acting against novel viral targets. The ribonuclease H (RNase H) function of the reverse transcriptase (RT) represents a validated and promising target, and no inhibitor has reached the clinical pipeline yet. Here, we present rationally designed non-diketo acid selective RNase H inhibitors (RHIs) based on the quinolinone scaffold starting from former dual integrase (IN)/RNase H quinolinonyl diketo acids. Several derivatives were synthesized and tested against RNase H and viral replication and found active at micromolar concentrations. Docking studies within the RNase H catalytic site, coupled with site-directed mutagenesis, and Mg 2+ titration experiments demonstrated that our compounds coordinate the Mg 2+ cofactor and interact with amino acids of the RNase H domain that are highly conserved among naïve and treatment-experienced patients. In general, the new inhibitors influenced also the polymerase activity of RT but were selective against RNase H vs the IN enzyme.

Published

2021

23. Anti-Tumoral Effects of a (1 H -Pyrrol-1-yl)Methyl-1 H -Benzoimidazole Carbamate Ester Derivative on Head and Neck Squamous Carcinoma Cell Lines.

Author

Nicolai A, Madia VN, Messore A, De Vita D, De Leo A, Ialongo D, Tudino V, Tortorella E, Scipione L, Taurone S, Pergolizzi T, Artico M, Di Santo R, Costi R, and Scarpa S

Abstract

Nocodazole is an antineoplastic agent that exerts its effects by depolymerizing microtubules. Herein we report a structural analog of nocodazole, a (1 H -pyrrol-1-yl)methyl-1 H -benzoimidazole carbamate ester derivative, named RDS 60. We evaluated the antineoplastic properties of RDS 60 in two human head and neck squamous cell carcinoma (HNSCC) cell lines and we found that this compound significantly inhibited replication of both HNSCC cell lines without inducing any important cytotoxic effect on human dermal fibroblasts and human keratinocytes. The treatment of HNSCC cell lines with 1 μM RDS 60 for 24 h stopped development of normal bipolar mitotic spindles and, at the same time, blocked the cell cycle in G2/M phase together with cytoplasmic accumulation of cyclin B1. Consequently, treatment with 2 μM RDS 60 for 24 h induced the activation of apoptosis in both HNSCC cell lines. Additionally, RDS 60 was able to reverse the epithelial-mesenchymal transition and to inhibit cell migration and extracellular matrix infiltration of both HNSCC cell lines. The reported results demonstrate that this compound has a potent effect in blocking cell cycle, inducing apoptosis and inhibiting cell motility and stromal invasion of HNSCC cell lines. Therefore, the ability of RDS 60 to attenuate the malignancy of tumor cells suggests its potential role as an interesting and powerful tool for new approaches in treating HNSCC.

Published

2021

24. Acetylcholinesterase inhibitors for the treatment of Alzheimer's disease - a patent review (2016-present).

Author

Bortolami M, Rocco D, Messore A, Di Santo R, Costi R, Madia VN, Scipione L, and Pandolfi F

Subjects

Alzheimer Disease physiopathology, Animals, Cholinesterase Inhibitors administration & dosage, Disease Progression, Humans, Molecular Targeted Therapy, Patents as Topic, Alzheimer Disease drug therapy, Cholinesterase Inhibitors pharmacology, Drug Development

Abstract

Introduction - AD, the most common form of dementia, has a multifactorial etiology, and the current therapy (AChEIs and memantine) is unable to interrupt its progress and fatal outcome. This is reflected in the research programs that are oriented toward the development of new therapeutics able to operate on multiple targets involved in the disease progression. Areas covered - The patents from 2016 to present regarding the use of AChEIs in AD, concerns the development of new AChEIs, multitarget or multifunctional ligands, or the associations of currently used AChEIs with other compounds acting on different targets involved in the AD. Expert opinion - The development of new multitarget AChEIs promises to identify compounds with great therapeutic potential but requires more time and effort in order to obtain drugs with the optimal pharmacodynamic profile. Otherwise, the research on new combinations of existing drugs, with known pharmacodynamic and ADME profile, could shorten the time and reduce the costs to develop a new therapeutic treatment for AD. From the analyzed data, it seems more likely that a response to the urgent need to develop effective treatments for AD therapy could come more quickly from studies on drug combinations than from the development of new AChEIs.

Published

2021

25. Analytical Characterization of an Inulin-Type Fructooligosaccharide from Root-Tubers of Asphodelus ramosus L.

Author

Madia VN, De Vita D, Messore A, Toniolo C, Tudino V, De Leo A, Pindinello I, Ialongo D, Saccoliti F, D'Ursi AM, Grimaldi M, Ceccobelli P, Scipione L, Di Santo R, and Costi R

Abstract

Plant-based systems continue to play a pivotal role in healthcare, and their use has been extensively documented. Asphodelus L. is a genus comprising various herbaceous species, known by the trivial name Asphodelus. These plants have been known since antiquity for both food and therapeutic uses, especially for treating several diseases associated with inflammatory and infectious skin disorders. Phytochemical studies revealed the presence of different constituents, mainly anthraquinones, triterpenoids, phenolic acids, and flavonoids. Although extensive literature has been published on these constituents, a paucity of information has been reported regarding the carbohydrate composition, such as fructans and fructan-like derivatives. The extraction of water-soluble neutral polysaccharides is commonly performed using water extraction, at times assisted by microwaves and ultrasounds. Herein, we reported the investigation of the alkaline extraction of root-tubers of Asphodelus ramosus L., analyzing the water-soluble polysaccharides obtained by precipitation from the alkaline extract and its subsequent purification by chromatography. A polysaccharide was isolated by alkaline extraction; the HPTLC study to determine its composition showed fructose as the main monosaccharide. FT-IR analysis showed the presence of an inulin-type structure, and NMR analyses allowed us to conclude that A. ramosus roots contain polysaccharide with an inulin-type fructooligosaccharide with a degree of polymerization of 7-8.

Published

2021

26. Investigation of Commiphora myrrha (Nees) Engl. Oil and Its Main Components for Antiviral Activity.

Author

Madia VN, De Angelis M, De Vita D, Messore A, De Leo A, Ialongo D, Tudino V, Saccoliti F, De Chiara G, Garzoli S, Scipione L, Palamara AT, Di Santo R, Nencioni L, and Costi R

Abstract

The resinous exudate produced by Commiphora myrrha (Nees) Engl. is commonly known as true myrrh and has been used since antiquity for several medicinal applications. Hundreds of metabolites have been identified in the volatile component of myrrh so far, mainly sesquiterpenes. Although several efforts have been devoted to identifying these sesquiterpenes, the phytochemical analyses have been performed by gas-chromatography/mass spectrometry (GC-MS) where the high temperature employed can promote degradation of the components. In this work, we report the extraction of C. myrrha by supercritical CO 2 , an extraction method known for the mild extraction conditions that allow avoiding undesired chemical reactions during the process. In addition, the analyses of myrrh oil and of its metabolites were performed by HPLC and GC-MS. Moreover, we evaluated the antiviral activity against influenza A virus of the myrrh extracts, that was possible to appreciate after the addition of vitamin E acetate (α-tocopheryl acetate) to the extract. Further, the single main bioactive components of the oil of C. myrrha commercially available were tested. Interestingly, we found that both furanodienone and curzerene affect viral replication by acting on different steps of the virus life cycle.

Published

2021

27. Design, Synthesis and Biological Evaluation of New Pyrimidine Derivatives as Anticancer Agents.

Author

Madia VN, Nicolai A, Messore A, De Leo A, Ialongo D, Tudino V, Saccoliti F, De Vita D, Scipione L, Artico M, Taurone S, Taglieri L, Di Santo R, Scarpa S, and Costi R

Subjects

Antineoplastic Agents chemistry, Cell Line, Tumor, Cell Proliferation drug effects, Chemistry Techniques, Synthetic, Humans, Pyrimidines chemistry, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Drug Design, Pyrimidines chemical synthesis, Pyrimidines pharmacology

Abstract

Background: Anticancer drug resistance is a challenging phenomenon of growing concern which arises from alteration in drug targets. Despite the fast speed of new chemotherapeutic agent design, the increasing prevalence of this phenomenon requires further research and treatment development. Recently, we reported a new aminopyrimidine compound-namely RDS 344-as a potential innovative anticancer agent., Methods: Herein, we report the design, synthesis, and anti-proliferative activity of new aminopyrimidine derivatives structurally related to RDS 3442 obtained by carrying out substitutions at position 6 of the pyrimidine core and/or on the 2-aniline ring of our hit. The ability to inhibit cell proliferation was evaluated on different types of tumors, glioblastoma, triple-negative breast cancer, oral squamous cell carcinomas and colon cancer plus on human dermal fibroblasts chosen as control of normal cells., Results: The most interesting compound was the N -benzyl counterpart of RDS 3442, namely 2a , that induced a significant decrease in cell viability in all the tested tumor cell lines, with EC 50 s ranging from 4 and 8 μM, 4-13 times more active of hit., Conclusions: These data suggest a potential role for this class of molecules as promising tool for new approaches in treating cancers of different histotype.

Published

2021

28. Small-molecule Inhibitors of HIV-1 Reverse Transcriptase-Associated Ribonuclease H Function: Challenges and Recent Developments.

Author

Madia VN, Messore A, De Leo A, Tudino V, Pindinello I, Saccoliti F, De Vita D, Scipione L, Costi R, and Di Santo R

Subjects

Antiviral Agents, Drug Design, Humans, HIV Reverse Transcriptase, Ribonuclease H

Abstract

Multiple combinations of antiretroviral drugs have remarkably improved the treatment of HIV-1 infection. However, life-long treatments and drug resistance are still an open issue that requires continuous efforts for the identification of novel antiviral drugs., Background: The reverse transcriptase-associated ribonuclease H (RNase H) hydrolyzes the HIV genome to allow synthesizing viral DNA. Currently, no RNase H inhibitors (RHIs) have reached the clinical phase. Therefore, RNase H can be defined as an attractive target for drug design., Objective: Despite the wealth of information available for RNase H domain, the development of RHIs with high specificity and low cellular toxicity has been disappointing. However, it is now becoming increasingly evident that reverse transcriptase is a highly versatile enzyme, undergoing major structural alterations to complete its catalysis, and that exists a close spatial and temporal interplay between reverse transcriptase polymerase and RNase H domains. This review sums up the present challenges in targeting RNase H encompassing the challenges in selectively inhibiting RNase H vs polymerase and/or HIV-1 integrase and the weak antiviral activity of active site inhibitors, probably for a substrate barrier that impedes small molecules to reach the targeted site. Moreover, the focus is given on the most recent progress in the field of medicinal chemistry that has led to the identification of several small molecules as RHIs in the last few years., Conclusion: RHIs could be a new class of drugs with a novel mechanism of action highly precious for the treatment of resistant HIV strains., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2021

29. Comparison of different methods for the extraction of cannabinoids from cannabis.

Author

De Vita D, Madia VN, Tudino V, Saccoliti F, De Leo A, Messore A, Roscilli P, Botto A, Pindinello I, Santilli G, Scipione L, Costi R, and Di Santo R

Subjects

Cannabinoids chemistry, Microwaves, Molecular Structure, Plant Extracts chemistry, Polysorbates chemistry, Surface-Active Agents chemistry, Ultrasonics, Cannabinoids isolation & purification, Cannabis chemistry, Chemical Fractionation methods

Abstract

Cannabis oils, namely concentrated cannabis extracts, are getting plenty of attention because of their therapeutic potential for treatment of patients with cancer, HIV, multiple sclerosis and several other pathologies. Here we propose the use of ultrasound-assisted extraction (UAE) and microwave-assisted extraction (MAE) as alternative methods to the current protocols followed by pharmacists, the only authorized to manipulate standardized Cannabis. A third method, consisting of the use of Tween 20 as surfactant, was considered. Our best extraction methodology for commercial hemp extraction was applied to medicinal cannabis. Here we report the results obtained for 'Eletta campana', 'Carmagnola selezionata', Bediol ® , FM2 ® and Bedrocan ® .

Published

2020

30. Pyrrolyl Pyrazoles as Non-Diketo Acid Inhibitors of the HIV-1 Ribonuclease H Function of Reverse Transcriptase.

Author

Messore A, Corona A, Madia VN, Saccoliti F, Tudino V, De Leo A, Scipione L, De Vita D, Amendola G, Di Maro S, Novellino E, Cosconati S, Métifiot M, Andreola ML, Valenti P, Esposito F, Grandi N, Tramontano E, Costi R, and Di Santo R

Abstract

Due to the biological liability of diketo acid (DKA) chain, we transferred this element of our previously reported anti-HIV-1 pyrrolyl derivatives to a non-DKA scaffold, obtaining a series of pyrrolyl-pyrazole carboxylic acids as new RNase H inhibitors. Among the newly synthesized derivatives, oxyphenylpyrrolyl-pyrazoles demonstrated inhibitory activities within the low micromolar/submicromolar range with compound 11b being the most potent. Interestingly, all tested compounds showed up to 2 orders of magnitude of selectivity for RNase H vs integrase. Docking studies within the RNase H catalytic site, coupled with site-directed mutagenesis, showed the key structural features that could confer the ability to establish specific interactions within RNase H. Furthermore, they proved the ability of our compounds to interact with amino acids highly conserved among HIV-1 subspecies isolated among patients carrying drug-resistant variants. In the end, the newly discovered pyrazole carboxylic acid derivatives feature promising serum stability with respect to their corresponding DKAs., Competing Interests: The authors declare no competing financial interest., (Copyright © 2020 American Chemical Society.)

Published

2020

31. Discovery of a pyrimidine compound endowed with antitumor activity.

Author

Taglieri L, Saccoliti F, Nicolai A, Peruzzi G, Madia VN, Tudino V, Messore A, Di Santo R, Artico M, Taurone S, Salvati M, Costi R, and Scarpa S

Subjects

Antineoplastic Agents chemistry, Apoptosis, Breast Neoplasms pathology, Cell Cycle, Cell Line, Tumor, Cell Proliferation, Colonic Neoplasms pathology, Drug Screening Assays, Antitumor, Female, Glioblastoma pathology, Humans, Structure-Activity Relationship, Antineoplastic Agents pharmacology, Breast Neoplasms drug therapy, Colonic Neoplasms drug therapy, Drug Discovery, Glioblastoma drug therapy, Pyrimidines chemistry

Abstract

Recently, some synthetic nitrogen-based heterocyclic molecules, such as PJ34, have shown pronounced antitumor activity. Therefore, we designed and synthesized new derivatives characterized by a nitrogen-containing scaffold and evaluated their antiproliferative properties in tumor cells. We herein report the effects of three newly synthesized compounds on cell lines from three different human cancers: triple-negative breast cancer, colon carcinoma and glioblastoma. We found that two of these compounds did not affect proliferation, while the third significantly inhibited replication of the three cell lines. Moreover, this third molecule at 20 μM led to the upregulation of p21 and p27 and blockage of the cell cycle at G0/G1; in addition, it induced apoptosis in all three cell lines when used at higher concentrations (30-50 μM). The results demonstrate that this compound is a potent inhibitor of replication, an inducer of apoptosis and a negative regulator of cell cycle progression for cancer cells of different histotypes. Our data suggest a potential role for this new molecule as an interesting and powerful tool for new approaches in treating various cancers.

Published

2020

32. Structure-guided approach to identify a novel class of anti-leishmaniasis diaryl sulfide compounds targeting the trypanothione metabolism.

Author

Colotti G, Saccoliti F, Gramiccia M, Di Muccio T, Prakash J, Yadav S, Dubey VK, Vistoli G, Battista T, Mocci S, Fiorillo A, Bibi A, Madia VN, Messore A, Costi R, Di Santo R, and Ilari A

Subjects

Amino Acid Motifs, Catalytic Domain, Glutathione analogs & derivatives, Glutathione metabolism, Humans, Leishmania infantum enzymology, Leishmania infantum metabolism, Leishmaniasis drug therapy, Leishmaniasis parasitology, Models, Molecular, NADH, NADPH Oxidoreductases antagonists & inhibitors, NADH, NADPH Oxidoreductases chemistry, NADH, NADPH Oxidoreductases genetics, NADH, NADPH Oxidoreductases metabolism, Protozoan Proteins antagonists & inhibitors, Protozoan Proteins chemistry, Protozoan Proteins genetics, Protozoan Proteins metabolism, Spermidine analogs & derivatives, Spermidine metabolism, Antiprotozoal Agents chemistry, Antiprotozoal Agents pharmacology, Leishmania infantum drug effects, Sulfides chemistry, Sulfides pharmacology

Abstract

Leishmania protozoans are the causative agent of leishmaniasis, a neglected tropical disease consisting of three major clinical forms: visceral leishmaniasis (VL), cutaneous leishmaniasis, and mucocutaneous leishmaniasis. VL is caused by Leishmania donovani in East Africa and the Indian subcontinent and by Leishmania infantum in Europe, North Africa, and Latin America, and causes an estimated 60,000 deaths per year. Trypanothione reductase (TR) is considered to be one of the best targets to find new drugs against leishmaniasis. This enzyme is fundamental for parasite survival in the human host since it reduces trypanothione, a molecule used by the tryparedoxin/tryparedoxin peroxidase system of Leishmania to neutralize the hydrogen peroxide produced by host macrophages during infection. Recently, we solved the X-ray structure of TR in complex with the diaryl sulfide compound RDS 777 (6-(sec-butoxy)-2-((3-chlorophenyl)thio)pyrimidin-4-amine), which impairs the parasite defense against the reactive oxygen species by inhibiting TR with high efficiency. The compound binds to the catalytic site and engages in hydrogen bonds the residues more involved in the catalysis, namely Glu466', Cys57 and Cys52, thereby inhibiting the trypanothione binding. On the basis of the RDS 777-TR complex, we synthesized structurally related diaryl sulfide analogs as TR inhibitors able to compete for trypanothione binding to the enzyme and to kill the promastigote in the micromolar range. One of the most active among these compounds (RDS 562) was able to reduce the trypanothione concentration in cell of about 33% via TR inhibition. RDS 562 inhibits selectively Leishmania TR, while it does not inhibit the human homolog glutathione reductase.

Published

2020

33. Tegaserod for the Treatment of Irritable Bowel Syndrome.

Author

Madia VN, Messore A, Saccoliti F, Tudino V, De Leo A, De Vita D, Bortolami M, Scipione L, Pindinello I, Costi R, and Di Santo R

Subjects

Animals, Humans, Indoles adverse effects, Indoles pharmacokinetics, Indoles pharmacology, Irritable Bowel Syndrome metabolism, Serotonin metabolism, Serotonin Receptor Agonists adverse effects, Serotonin Receptor Agonists pharmacokinetics, Serotonin Receptor Agonists pharmacology, Indoles therapeutic use, Irritable Bowel Syndrome drug therapy, Serotonin Receptor Agonists therapeutic use

Abstract

Background: Tegaserod (Zelnorm®) is a 5-hydroxytryptamine (serotonin) type 4 receptor agonist for the treatment of hypomotility disorders of the lower gastrointestinal tract associated with the irritable bowel syndrome with constipation (IBS-C)., Objective: The authors provide the reader with a better understanding on tegaserod mechanism of action, on its pharmacodynamics and pharmacokinetic properties, on safety and tolerability, with a summary of the key published clinical trials conducted in patients with irritable bowel syndrome (IBS). Its effects on colon inflammation have also been described., Results: Tegaserod was withdrawn in 2007 due to increased risks of cardiovascular adverse effects. The manufacturer denied this, because pre-existing cardiovascular disease or risk factors were attributed to all affected patients. Thus, no causal relationship between tegaserod use and cardiovascular events was clearly shown. A matched case-control study of tegaserod-treated with untreated patients found no association between tegaserod and adverse cardiovascular outcomes. Despite its adverse effects, tegaserod resulted to be effective in treating chronic constipation in adult women aged < 65 years with IBS-C, while the safety and effectiveness of tegaserod in men with IBS-C have not been established. Tegaserod was resubmitted to the Food and Drug Administration in 2018 for use in a low-risk population. Moreover, tegaserod has also been shown to improve symptoms, enhance gastric accommodation and significantly attenuate visceral pain arising from the colon in functional dyspepsia patients. Treatment with tegaserod seems also to exert a protective effect in inflamed colons, reducing the severity of colitis in animal models., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2020

34. Inhibition of Polycomb Repressive Complex 2 activity reduces trimethylation of H3K27 and affects development in Arabidopsis seedlings.

Author

Ruta V, Longo C, Boccaccini A, Madia VN, Saccoliti F, Tudino V, Di Santo R, Lorrai R, Dello Ioio R, Sabatini S, Costi R, Costantino P, and Vittorioso P

Subjects

Arabidopsis drug effects, Arabidopsis growth & development, Arabidopsis metabolism, Arabidopsis Proteins genetics, Enhancer of Zeste Homolog 2 Protein, Enzyme Inhibitors pharmacology, Gene Expression Regulation, Developmental, Lysine metabolism, Methylation, Polycomb Repressive Complex 2, Repressor Proteins genetics, Rutin analogs & derivatives, Rutin pharmacology, Seedlings drug effects, Seedlings genetics, Seedlings growth & development, Seedlings metabolism, Seeds drug effects, Seeds genetics, Seeds growth & development, Seeds metabolism, Arabidopsis genetics, Arabidopsis Proteins antagonists & inhibitors, Gene Expression Regulation, Plant, Histones metabolism, Repressor Proteins antagonists & inhibitors

Abstract

Background: Polycomb repressive complex 2 (PRC2) is an epigenetic transcriptional repression system, whose catalytic subunit (ENHANCER OF ZESTE HOMOLOG 2, EZH2 in animals) is responsible for trimethylating histone H3 at lysine 27 (H3K27me3). In mammals, gain-of-function mutations as well as overexpression of EZH2 have been associated with several tumors, therefore making this subunit a suitable target for the development of selective inhibitors. Indeed, highly specific small-molecule inhibitors of EZH2 have been reported. In plants, mutations in some PRC2 components lead to embryonic lethality, but no trial with any inhibitor has ever been reported., Results: We show here that the 1,5-bis (3-bromo-4-methoxyphenyl)penta-1,4-dien-3-one compound (RDS 3434), previously reported as an EZH2 inhibitor in human leukemia cells, is active on the Arabidopsis catalytic subunit of PRC2, since treatment with the drug reduces the total amount of H3K27me3 in a dose-dependent fashion. Consistently, we show that the expression level of two PRC2 targets is significantly increased following treatment with the RDS 3434 compound. Finally, we show that impairment of H3K27 trimethylation in Arabidopsis seeds and seedlings affects both seed germination and root growth., Conclusions: Our results provide a useful tool for the plant community in investigating how PRC2 affects transcriptional control in plant development.

Published

2019

35. Design, Synthesis, and Biological Evaluation of New 1-(Aryl-1 H-pyrrolyl)(phenyl)methyl-1 H-imidazole Derivatives as Antiprotozoal Agents.

Author

Saccoliti F, Madia VN, Tudino V, De Leo A, Pescatori L, Messore A, De Vita D, Scipione L, Brun R, Kaiser M, Mäser P, Calvet CM, Jennings GK, Podust LM, Pepe G, Cirilli R, Faggi C, Di Marco A, Battista MR, Summa V, Costi R, and Di Santo R

Subjects

Animals, Antiprotozoal Agents chemical synthesis, Cytochrome P-450 Enzyme Inhibitors pharmacology, Humans, Imidazoles chemical synthesis, Parasitic Sensitivity Tests, Antiprotozoal Agents chemistry, Antiprotozoal Agents pharmacology, Drug Design, Drug Evaluation, Preclinical, Imidazoles chemistry, Imidazoles pharmacology, Trypanosoma drug effects

Abstract

We have designed and synthesized a series of new imidazole-based compounds structurally related to an antiprotozoal agent with nanomolar activity which we identified recently. The new analogues possess micromolar activities against Trypanosoma brucei rhodesiense and Leishmania donovani and nanomolar potency against Plasmodium falciparum. Most of the analogues displayed IC 50 within the low nanomolar range against Trypanosoma cruzi, with very high selectivity toward the parasite. Discussion of structure-activity relationships and in vitro biological data for the new compounds are provided against a number of different protozoa. The mechanism of action for the most potent derivatives (5i, 6a-c, and 8b) was assessed by a target-based assay using recombinant T. cruzi CYP51. Bioavailability and efficacy of selected hits were assessed in a T. cruzi mouse model, where 6a and 6b reduced parasitemia in animals >99% following intraperitoneal administration of 25 mg/kg/day dose for 4 consecutive days.

Published

2019

36. In Vitro Antiviral Activity of New Oxazoline Derivatives as Potent Poliovirus Inhibitors.

Author

Madia VN, Messore A, Pescatori L, Saccoliti F, Tudino V, De Leo A, Scipione L, Fiore L, Rhoden E, Manetti F, Oberste MS, Di Santo R, and Costi R

Subjects

Antiviral Agents chemical synthesis, Antiviral Agents pharmacology, Binding Sites, HeLa Cells, Humans, Molecular Dynamics Simulation, Oxazoles chemical synthesis, Oxazoles pharmacology, Poliovirus chemistry, Structure-Activity Relationship, Virus Replication drug effects, Antiviral Agents chemistry, Oxazoles chemistry, Poliovirus physiology

Abstract

The final stages of polio eradication are proving more difficult than the early phases, and the development of effective drugs and treatments is considered a priority; thus, the research is ongoing. A screening of our in-house chemical library against poliovirus Sabin strains led to the identification of compounds 5 and 6 as hits active at submicromolar concentrations. Derivatives of these compounds were synthesized as a preliminary structure-activity-relationship study. Among them, 7 and 11 were highly active against poliovirus Sabin 1-3. Compound 11 was also very potent against a large panel of wild and vaccine-derived polioviruses. Time-of-addition experiments suggest that 5 and 7 could be active at an early stage of viral replication, whereas 11 was active at same concentration at all stages of viral replication. A ligand-based approach was applied to find the common structural features shared by the new compounds and already-known poliovirus inhibitors.

Published

2019

37. Novel Symmetrical Benzazolyl Derivatives Endowed with Potent Anti-Heparanase Activity.

Author

Messore A, Madia VN, Pescatori L, Saccoliti F, Tudino V, De Leo A, Bortolami M, De Vita D, Scipione L, Pepi F, Costi R, Rivara S, Scalvini L, Mor M, Ferrara FF, Pavoni E, Roscilli G, Cassinelli G, Milazzo FM, Battistuzzi G, Di Santo R, and Giannini G

Subjects

Cell Line, Tumor, Cell Proliferation drug effects, Glucuronidase chemistry, Humans, Models, Molecular, Protein Conformation, Azoles chemistry, Azoles pharmacology, Drug Design, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Glucuronidase antagonists & inhibitors

Abstract

Heparanase is the only mammalian endo-β-d-glucuronidase involved in a variety of major diseases. The up-regulation of heparanase expression increases tumor size, angiogenesis, and metastasis, representing a validated target in the anti-cancer field. To date, only a few small-molecule inhibitors have been described, but none have gotten through pre-clinical development. Previously, we explored 2-(4-(4-(bromo-methoxybenzamido)benzylamino)phenyl) benzazole derivatives as anti-heparanase agents, proposing this scaffold for development of broadly effective heparanase inhibitors. Herein, we report an extended investigation of new symmetrical 2-aminophenyl-benzazolyl-5-acetate derivatives, proving that symmetrical compounds are more effective than asymmetrical analogues, with the most-potent compound, 7g, being active at nanomolar concentration against heparanase. Molecular docking studies were performed on the best-acting compounds 5c and 7g to rationalize their interaction with the enzyme. Moreover, invasion assay confirmed the anti-metastatic potential of compounds 5c, 7a, and 7g, proving the inhibition of the expression of proangiogenic factors in tumor cells.

Published

2018

38. Novel Benzazole Derivatives Endowed with Potent Antiheparanase Activity.

Author

Madia VN, Messore A, Pescatori L, Saccoliti F, Tudino V, De Leo A, Bortolami M, Scipione L, Costi R, Rivara S, Scalvini L, Mor M, Ferrara FF, Pavoni E, Roscilli G, Cassinelli G, Milazzo FM, Battistuzzi G, Di Santo R, and Giannini G

Subjects

Cell Line, Tumor, Drug Design, Glucuronidase chemistry, Humans, Inhibitory Concentration 50, Models, Molecular, Protein Conformation, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Glucuronidase antagonists & inhibitors, Indoles chemistry, Indoles pharmacology

Abstract

Heparanase is the sole mammalian enzyme capable of cleaving glycosaminoglycan heparan sulfate side chains of heparan sulfate proteoglycans. Its altered activity is intimately associated with tumor growth, angiogenesis, and metastasis. Thus, its implication in cancer progression makes it an attractive target in anticancer therapy. Herein, we describe the design, synthesis, and biological evaluation of new benzazoles as heparanase inhibitors. Most of the designed derivatives were active at micromolar or submicromolar concentration, and the most promising compounds are fluorinated and/or amino acids derivatives 13a, 14d, and 15 that showed IC 50 0.16-0.82 μM. Molecular docking studies were performed to rationalize their interaction with the enzyme catalytic site. Importantly, invasion assay confirmed the antimetastatic potential of compounds 14d and 15. Consistently with its ability to inhibit heparanase, compound 15 proved to decrease expression of genes encoding for proangiogenic factors such as MMP-9, VEGF, and FGFs in tumor cells.

Published

2018

39. Biological evaluation and structure-activity relationships of imidazole-based compounds as antiprotozoal agents.

Author

Saccoliti F, Madia VN, Tudino V, De Leo A, Pescatori L, Messore A, De Vita D, Scipione L, Brun R, Kaiser M, Mäser P, Calvet CM, Jennings GK, Podust LM, Costi R, and Di Santo R

Subjects

Animals, Antiprotozoal Agents chemical synthesis, Antiprotozoal Agents therapeutic use, Cell Line, Female, Humans, Imidazoles chemical synthesis, Imidazoles therapeutic use, Inhibitory Concentration 50, Leishmania donovani drug effects, Leishmaniasis, Visceral drug therapy, Malaria, Falciparum drug therapy, Mice, Mice, Inbred BALB C, Parasitic Sensitivity Tests, Plasmodium falciparum drug effects, Rats, Structure-Activity Relationship, Trypanosoma brucei rhodesiense drug effects, Trypanosomiasis, African drug therapy, Antiprotozoal Agents chemistry, Antiprotozoal Agents pharmacology, Chagas Disease drug therapy, Imidazoles chemistry, Imidazoles pharmacology, Trypanosoma cruzi drug effects

Abstract

We discovered a series of azole antifungal compounds as effective antiprotozoal agents. They displayed promising inhibitory activities within the micromolar-submicromolar range against P. falciparum, L. donovani, and T. b. rhodesiense. Moreover, most of such compounds showed excellent nanomolar IC 50 against T. cruzi, showing also very low cytotoxicity. Discussion of structure-activity relationships and biological data for these compounds are provided against the different parasites. To assess the mechanism of action against T. cruzi we proved that the most potent compounds (3b, 3j-l) inhibited the T. cruzi CYP51. Moreover, the most active derivative 3j dramatically reduced parasitemia in T. cruzi mouse model without acute toxicity., (Copyright © 2018 Elsevier Masson SAS. All rights reserved.)

Published

2018

40. Inhibition of Leishmania infantum trypanothione reductase by diaryl sulfide derivatives.

Author

Saccoliti F, Angiulli G, Pupo G, Pescatori L, Madia VN, Messore A, Colotti G, Fiorillo A, Scipione L, Gramiccia M, Di Muccio T, Di Santo R, Costi R, and Ilari A

Subjects

Crystallography, X-Ray, Models, Molecular, NADH, NADPH Oxidoreductases chemistry, Leishmania infantum enzymology, NADH, NADPH Oxidoreductases antagonists & inhibitors, Sulfides pharmacology

Abstract

The study presented here aimed at identifying a new class of compounds acting against Leishmania parasites, the causative agent of Leishmaniasis. For this purpose, the thioether derivatives of our in-house library have been evaluated in whole-cell screening assays in order to determine their in vitro activity against Leishmania protozoan. Among them, promising results have been achieved with compound RDS 777 (6-(sec-butoxy)-2-((3-chlorophenyl)thio)pyrimidin-4-amine) (IC 50  =   29.43 µM), which is able to impair the mechanism of the parasite defence against the reactive oxygen species by inhibiting the trypanothione reductase (TR) with high efficiency (K i 0.25 ± 0.18 µM). The X-ray structure of L. infantum TR in complex with RDS 777 disclosed the mechanism of action of this compound that binds to the catalytic site and engages in hydrogen bonds the residues more involved in the catalysis, namely Glu466', Cys57 and Cys52, thereby inhibiting the trypanothione binding and avoiding its reduction.

Published

2017

41. Structure-Activity Relationships on Cinnamoyl Derivatives as Inhibitors of p300 Histone Acetyltransferase.

Author

Madia VN, Benedetti R, Barreca ML, Ngo L, Pescatori L, Messore A, Pupo G, Saccoliti F, Valente S, Mai A, Scipione L, Zheng YG, Tintori C, Botta M, Cecchetti V, Altucci L, Di Santo R, and Costi R

Subjects

Apoptosis drug effects, Benzylidene Compounds chemistry, Benzylidene Compounds metabolism, Benzylidene Compounds pharmacology, Binding Sites, Cell Line, Cinnamates metabolism, Cinnamates pharmacology, Cyclohexanones chemistry, Cyclohexanones metabolism, Cyclohexanones pharmacology, E1A-Associated p300 Protein antagonists & inhibitors, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, G2 Phase Cell Cycle Checkpoints drug effects, Humans, Inhibitory Concentration 50, Molecular Docking Simulation, Protein Binding, Protein Structure, Tertiary, Structure-Activity Relationship, Cinnamates chemistry, E1A-Associated p300 Protein metabolism, Enzyme Inhibitors chemistry

Abstract

Human p300 is a polyhedric transcriptional coactivator that plays a crucial role in acetylating histones on specific lysine residues. A great deal of evidence shows that p300 is involved in several diseases, including leukemia, tumors, and viral infection. Its involvement in pleiotropic biological roles and connections to diseases provide the rationale to determine how its modulation could represent an amenable drug target. Several p300 inhibitors (i.e., histone acetyltransferase inhibitors, HATis) have been described so far, but they all suffer from low potency, lack of specificity, or low cell permeability, which thus highlights the need to find more effective inhibitors. Our cinnamoyl derivative, 2,6-bis(3-bromo-4-hydroxybenzylidene)cyclohexanone (RC56), was identified as an active and selective p300 inhibitor and was proven to be a good hit candidate to investigate the structure-activity relationship toward p300. Herein, we describe the design, synthesis, and biological evaluation of new HATis structurally related to our hit; moreover, we investigate the interactions between p300 and the best-emerged hits by means of induced-fit docking and molecular-dynamics simulations, which provided insight into the peculiar chemical features that influence their activity toward the targeted enzyme., (© 2017 Wiley-VCH Verlag GmbH & Co. KGaA, Weinheim.)

Published

2017

42. New insights into the interaction between pyrrolyl diketoacids and HIV-1 integrase active site and comparison with RNase H.

Author

Corona A, di Leva FS, Rigogliuso G, Pescatori L, Madia VN, Subra F, Delelis O, Esposito F, Cadeddu M, Costi R, Cosconati S, Novellino E, di Santo R, and Tramontano E

Subjects

Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Binding Sites, Catalytic Domain, Drug Resistance, Viral, HIV Infections virology, HIV Integrase drug effects, HIV Integrase genetics, HIV Integrase Inhibitors chemistry, HIV Integrase Inhibitors pharmacology, HIV-1 drug effects, HIV-1 enzymology, Humans, Models, Molecular, Molecular Structure, Mutagenesis, Site-Directed, Pyrroles chemistry, Pyrroles pharmacology, Ribonuclease H pharmacology, Structure-Activity Relationship, Virus Replication drug effects, HIV Integrase metabolism, HIV Integrase Inhibitors metabolism, HIV-1 metabolism, Pyrroles metabolism, Ribonuclease H metabolism

Abstract

HIV-1 integrase (IN) inhibitors are one of the most recent innovations in the treatment of HIV infection. The selection of drug resistance viral strains is however a still open issue requiring constant efforts to identify new anti-HIV-1 drugs. Pyrrolyl diketo acid (DKA) derivatives inhibit HIV-1 replication by interacting with the Mg 2+ cofactors within the HIV-1 IN active site or within the HIV-1 reverse-transcriptase associated ribonuclease H (RNase H) active site. While the interaction mode of pyrrolyl DKAs with the RNase H active site has been recently reported and substantiated by mutagenesis experiments, their interaction within the IN active site still lacks a detailed understanding. In this study, we investigated the binding mode of four pyrrolyl DKAs to the HIV-1 IN active site by molecular modeling coupled with site-directed mutagenesis studies showing that the DKA pyrrolyl scaffold primarily interacts with the IN amino residues P145, Q146 and Q148. Importantly, the tested DKAs demonstrated good effectiveness against HIV-1 Raltegravir resistant Y143A and N155H INs, thus showing an interaction pattern with relevant differences if compared with the first generation IN inhibitors. These data provide precious insights for the design of new HIV inhibitors active on clinically selected Raltegravir resistant variants. Furthermore, this study provides new structural information to modulate IN and RNase H inhibitory activities for development of dual-acting anti-HIV agents., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

43. Discovery of N-aryl-naphthylamines as in vitro inhibitors of the interaction between HIV integrase and the cofactor LEDGF/p75.

Author

Cuzzucoli Crucitti G, Pescatori L, Messore A, Madia VN, Pupo G, Saccoliti F, Scipione L, Tortorella S, Di Leva FS, Cosconati S, Novellino E, Debyser Z, Christ F, Costi R, and Di Santo R

Subjects

1-Naphthylamine chemical synthesis, 1-Naphthylamine chemistry, 1-Naphthylamine pharmacology, Dose-Response Relationship, Drug, HIV Integrase Inhibitors chemical synthesis, HIV Integrase Inhibitors chemistry, Humans, Models, Molecular, Molecular Structure, Protein Binding drug effects, Structure-Activity Relationship, Tumor Cells, Cultured, para-Aminobenzoates chemical synthesis, para-Aminobenzoates chemistry, 1-Naphthylamine analogs & derivatives, Drug Discovery, HIV Integrase metabolism, HIV Integrase Inhibitors pharmacology, Intercellular Signaling Peptides and Proteins metabolism, para-Aminobenzoates pharmacology

Abstract

A series of N-aryl-naphthylamines, exemplified by the structures 11-16, were chosen for an in-house library screening to assay their ability to disrupt the interaction between the LEDGF cofactor and the HIV integrase. Structure modification led also to design and synthesize new compounds 17a-f. Compounds 11e,h,k,n, 13b, and 14 showed good activity in AlphaScreen assay. The most active compound 11e (IC50 = 2.5 μM) was selected for molecular modeling studies and showed a binding mode similar to the one of the known LEDGIN 8., (Copyright © 2015 Elsevier Masson SAS. All rights reserved.)

Published

2015

44. N-Substituted Quinolinonyl Diketo Acid Derivatives as HIV Integrase Strand Transfer Inhibitors and Their Activity against RNase H Function of Reverse Transcriptase.

Author

Pescatori L, Métifiot M, Chung S, Masoaka T, Cuzzucoli Crucitti G, Messore A, Pupo G, Madia VN, Saccoliti F, Scipione L, Tortorella S, Di Leva FS, Cosconati S, Marinelli L, Novellino E, Le Grice SF, Pommier Y, Marchand C, Costi R, and Di Santo R

Subjects

Catalytic Domain, HIV Infections drug therapy, HIV Infections virology, HIV Integrase Inhibitors chemistry, HIV-1 drug effects, HeLa Cells, Humans, Keto Acids chemistry, Models, Molecular, Molecular Structure, Quinolones chemistry, Structure-Activity Relationship, Virus Replication drug effects, HIV Integrase chemistry, HIV Integrase Inhibitors pharmacology, Keto Acids pharmacology, Quinolones pharmacology, RNA-Directed DNA Polymerase chemistry, Ribonuclease H antagonists & inhibitors

Abstract

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

Published

2015

45. Structure-activity relationship of pyrrolyl diketo acid derivatives as dual inhibitors of HIV-1 integrase and reverse transcriptase ribonuclease H domain.

Author

Cuzzucoli Crucitti G, Métifiot M, Pescatori L, Messore A, Madia VN, Pupo G, Saccoliti F, Scipione L, Tortorella S, Esposito F, Corona A, Cadeddu M, Marchand C, Pommier Y, Tramontano E, Costi R, and Di Santo R

Subjects

Dose-Response Relationship, Drug, HIV enzymology, HIV Integrase Inhibitors chemical synthesis, HIV Integrase Inhibitors chemistry, HIV Reverse Transcriptase chemistry, HIV Reverse Transcriptase metabolism, Microbial Sensitivity Tests, Molecular Structure, Protein Structure, Tertiary drug effects, Pyrroles chemical synthesis, Pyrroles chemistry, Reverse Transcriptase Inhibitors chemical synthesis, Reverse Transcriptase Inhibitors chemistry, Ribonuclease H metabolism, Structure-Activity Relationship, Virus Replication drug effects, HIV drug effects, HIV Integrase metabolism, HIV Integrase Inhibitors pharmacology, HIV Reverse Transcriptase antagonists & inhibitors, Pyrroles pharmacology, Reverse Transcriptase Inhibitors pharmacology, Ribonuclease H antagonists & inhibitors

Abstract

The development of HIV-1 dual inhibitors is a highly innovative approach aimed at reducing drug toxic side effects as well as therapeutic costs. HIV-1 integrase (IN) and reverse transcriptase-associated ribonuclease H (RNase H) are both selective targets for HIV-1 chemotherapy, and the identification of dual IN/RNase H inhibitors is an attractive strategy for new drug development. We newly synthesized pyrrolyl derivatives that exhibited good potency against IN and a moderate inhibition of the RNase H function of RT, confirming the possibility of developing dual HIV-1 IN/RNase H inhibitors and obtaining new information for the further development of more effective dual HIV-1 inhibitors.

Published

2015

46. Basic quinolinonyl diketo acid derivatives as inhibitors of HIV integrase and their activity against RNase H function of reverse transcriptase.

Author

Costi R, Métifiot M, Chung S, Cuzzucoli Crucitti G, Maddali K, Pescatori L, Messore A, Madia VN, Pupo G, Scipione L, Tortorella S, Di Leva FS, Cosconati S, Marinelli L, Novellino E, Le Grice SF, Corona A, Pommier Y, Marchand C, and Di Santo R

Subjects

HIV Integrase Inhibitors pharmacology, Models, Molecular, Quinolones pharmacology, Structure-Activity Relationship, HIV Integrase Inhibitors chemical synthesis, Quinolones chemical synthesis, Ribonuclease H antagonists & inhibitors

Abstract

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

Published

2014