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2. Synthesis and Biological Evaluation of New 3-Phenyl-1-[(4-arylpiperazin-1-yl)alkyl]- piperidine-2,6-diones

Author

Loddo R, La Colla P, Anna Bielenica, Jerzy Kossakowski, Ibba C, Izabela Dybała, and Struga M

Subjects
chemistry.chemical_classification, Antifungal, 3-Phenylpiperidine-2,6-dione, Stereochemistry, medicine.drug_class, Cytotoxicity, Pharmaceutical Science, Combinatorial chemistry, In vitro, chemistry.chemical_compound, chemistry, medicine, Piperidine, Antiviral activity, Alkyl, Research Article, X-ray crystallography, Biological evaluation
Abstract

A set of 13 alkyl derivatives of 3-phenylpiperidine-2,6-dione were synthesized. Newly obtained compounds were investigated in vitro against HIV-1 and other selected viruses. The benzyl 3f and fluorophenyl 3g derivatives showed moderate protection against CVB-2 and the compound 3g also against HSV-1. Derivatives were tested also for their antibacterial and antifungal activity. The molecular structures of 3a and 3d were determined by an X-ray analysis.

Published
2011

3. Look Back in Anger. Toxicity vs. Activity for Acridine Derivatives as HCV RNADependent RNA-polymerase Inhibitors

Author

Pricl, Sabrina, Laurini, Erik, Col, V. Dal, Fermeglia, Maurizio, Loddo, R, Tonelli, M., Pricl, Sabrina, Laurini, Erik, Col, V. Dal, Fermeglia, Maurizio, Loddo, R, and Tonelli, M.

Subjects
Antiviras, drug design, Antiviras, HCV RdRp, drug design, toxicity, DNA, toxicity, DNA, HCV RdRp
Abstract

Acridines are known deoxyribonucleic acid (DNA) intercalators. Accordingly, the interaction of the present acridine derivatives within the DNA double helix was extensively investigated via a sophisticated ensemble of molecular simulation techniques. The results showed that an intricate balance of molecular features contributed to the thermodynamic/kinetics aspects of acridines/DNA binding and, hence, to the ultimate STR for these series of HCV RdRp inhibitors. Among these factors, the length of the large side chain R was found to play a primary role in determining DNA binding strength and, hence, cellular toxicity.

Published
2013

4. 2,3-Dihydro-1,2-Diphenyl-substituted 4H-Pyridinone Derivatives as New Anti Flaviviridae Inhibitors

Author

Peduto, A, Massa, A, Di Mola, A, de Caprariis, P, La Colla, P, Loddo, R, Altamura, S, Maga, G, FILOSA, Rosanna, Peduto, A, Massa, A, Di Mola, A, de Caprariis, P, La Colla, P, Loddo, R, Altamura, S, Maga, G, and Filosa, Rosanna

Subjects
3-dihydro-1, flavivirus, viruses, 2-diphenyl-substituted 4H-pyridinone
Abstract

With the aim of identifying novel lead compounds active against emergent human infectious diseases, a series of 2,3-dihydro-4H-pyridinone derivatives has been prepared and evaluated for antiviral activity. Compounds were evaluated in vitro in cell-based assays for cytotoxicity and against a wide spectrum of viruses. In the antiviral screening, several compounds showed to be fairly active against viruses belonging to the Flaviviridae family. The Pestiviruses (bovine viral diarrhoea virus) were inhibited by 4acis (CC(50) > 100 mu m; EC(50) = 14 mu m), compounds 4ccis and 6a showed a significant activity against Flaviviruses (Yellow Fever Virus) (CC(50) > 100 mu m; EC(50) = 18 mu m, CC(50) > 100 mu m; EC(50) = 10 mu m). Among these, compound 6a displayed great inhibitory activity against Hepaciviruses (hepatitis C virus) in replicon assay [CC(50) > 100 mu m; EC(50)(1b) = 4 mu m]. In vitro inhibitory activity against the HCV RNA-dependent RNA polymerase (NS5B) of title compounds is discussed. The antiviral screening of viral strains indicated that compound 6a can be selected as promising tool in novel anti-flaviviruses development.

Published
2011

5. Antiviral and cytotoxic activities of aminoarylazo compoundsand aryltriazene derivatives

Author

Tonelli, M, Vazzana, I, Tasso, B, Boido, V, Sparatore, F, Fermeglia, Maurizio, Paneni, Maria Silvia, Posocco, Paola, Pricl, Sabrina, LA COLLA, P, Ibba, C, Secci, B, Collu, G, Loddo, R., Tonelli, M, Vazzana, I, Tasso, B, Boido, V, Sparatore, F, Fermeglia, Maurizio, Paneni, Maria Silvia, Posocco, Paola, Pricl, Sabrina, LA COLLA, P, Ibba, C, Secci, B, Collu, G, and Loddo, R.

Subjects
antiviral research
Published
2009

6. Design, synthesis and anti flaviviridae activity of N6-, -O- and 5 O-substituted adenine nucleoside analogs

Author

ANGUSTI A, MANFREDINI S, DURINI E, CILIBERTI N, VERTUANI S, SOLAROLI N, LODDO R, SECCI B, VISIOLI A, SANNA T, COLLU G, PEZZULLO M, LA COLLA P., PRICL, SABRINA, FERRONE, MARCO, FERMEGLIA, MAURIZIO, Angusti, A, Manfredini, S, Durini, E, Ciliberti, N, Vertuani, S, Solaroli, N, Pricl, Sabrina, Ferrone, Marco, Fermeglia, Maurizio, Loddo, R, Secci, B, Visioli, A, Sanna, T, Collu, G, Pezzullo, M, and LA COLLA, P.

Published
2008

8. Design, synthesis and preliminary in vitro and in silico antiviral activity of [4,7]phenantrolines and 1-oxo-1,4-dihydro-[4,7]phenantrolines against a single-stranded positive sense RNA genome viruses

Author

CARTA A, LORIGA M, PAGLIETTI G, SANNA T, IBBA C, LA COLLA P, LODDO R., FERRONE, MARCO, FERMEGLIA, MAURIZIO, PRICL, SABRINA, Carta, A, Loriga, M, Paglietti, G, Ferrone, Marco, Fermeglia, Maurizio, Pricl, Sabrina, Sanna, T, Ibba, C, LA COLLA, P, and Loddo, R.

Subjects
Antiviral Agents
Published
2007

9. Chasing the evaders. Design, synthesis, activity and molecular modelling of a new small molecule with activity against drug-resistant HIV-1-mutants

Author

Pricl, Sabrina, Ferrone, Marco, Posocco, Paola, Fermeglia, Maurizio, Sanna, G., Collu, G., La Colla, P., Loddo, R., Sias, A., Piras, S., Carta, A., Pricl, Sabrina, Ferrone, Marco, Posocco, Paola, Fermeglia, Maurizio, Sanna, G., Collu, G., La Colla, P., Loddo, R., Sias, A., Piras, S., and Carta, A.

Subjects
reverse transcriptase, hiv, Computer simulation
Published
2006

10. A new twist for an old song. The DABO story revisited

Author

Pricl, Sabrina, Ferrone, Marco, Posocco, Paola, Pavan, G. M., Fermeglia, Maurizio, La Colla, P., Loddo, R., Pricl, Sabrina, Ferrone, Marco, Posocco, Paola, Pavan, G. M., Fermeglia, Maurizio, La Colla, P., and Loddo, R.

Subjects
hiv, reverse transcriptase, computer simulation
Published
2006

11. A combined in silico / in vitro approach unveils common molecular requirements for efficient BVDV RdRp binding of linear aromatic N-polycyclic systems

Author

Carta, A., primary, Briguglio, I., additional, Piras, S., additional, Corona, P., additional, Ibba, R., additional, Laurini, E., additional, Fermeglia, M., additional, Pricl, S., additional, Desideri, N., additional, Atzori, E.M., additional, La Colla, P., additional, Collu, G., additional, Delogu, I., additional, and Loddo, R., additional

Published
2016
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12. Hindered nucleoside analogs as hinibitors of HCV RNA-dependent RNA-polymerase: evolving vistas

Author

MANFREDINI S., ANGUSTI A., CILIBERTI N., DURINI E., VERTUANI S., BUZZONI L., COSLANICH A., FERMEGLIA, MAURIZIO, FERRONE M., PANENI M. S., LA COLLA P., SANNA G., CADEDDU A., MURA M., LODDO R., PRICL, SABRINA, SCHINAZI, R., E. SCHIFF, Manfredini, S., Angusti, A., Ciliberti, N., Durini, E., Vertuani, S., Buzzoni, L., Coslanich, A., Fermeglia, Maurizio, Ferrone, M., Paneni, M. S., Pricl, Sabrina, LA COLLA, P., Sanna, G., Cadeddu, A., Mura, M., and Loddo, R.

Published
2005

13. Three-dimensional Pharmacophore Modeling of Hindered Nucleoside Analogs (HNAs) as Inhibitors of the Hepatitis C virus NS5B Polymerase

Author

Ferrone, Marco, Pricl, Sabrina, Fermeglia, Maurizio, Paneni, Maria Silvia, Angusti, A., Ciliberti, N., Buzzoni, L., Durini, E., Vertuani, S., Manfredini, S., Loddo, R., La Colla, P., Ferrone, Marco, Pricl, Sabrina, Fermeglia, Maurizio, Paneni, Maria Silvia, Angusti, A., Ciliberti, N., Buzzoni, L., Durini, E., Vertuani, S., Manfredini, S., Loddo, R., and La Colla, P.

Subjects
HCV, computer-assisted drug design
Published
2005

14. Non-nucleoside anti-Flaviviridae agents from different molecular classes: a jointed experimental/modeling effort

Author

Angusti A., Auzzas L., Boido V., Canu C., Carta A., Ciliberti N., Loddo R., La Colla P., Loriga M., Manfredini S., Mazzei M., Nieddu E., Paglietti G., Paneni M. S., Rassu G., Sparatore F., Tasso B., Vitale G., FERRONE, MARCO, PRICL, SABRINA, Angusti, A., Auzzas, L., Boido, V., Canu, C., Carta, A., Ciliberti, N., Ferrone, Marco, Loddo, R., La Colla, P., Loriga, M., Manfredini, S., Mazzei, M., Nieddu, E., Paglietti, G., Paneni, M. S., Pricl, Sabrina, Rassu, G., Sparatore, F., Tasso, B., and Vitale, G.

Subjects
HCV, RdRp inhibitors, computer-assisted drug design, RdRp inhibitor
Published
2005

15. Hindered Nucleoside Analogs (HNA) as Antiflaviviridae Agents

Author

Manfredini, S., Angusti, A., Veronese, A. C., Durini, E., Vertuani, S., Nalin, F., Solaroli, N., Ferrone, Marco, Pricl, Sabrina, Mura, M., Piano, M. A., Poddesu, B., Cadeddu, A., LA COLLA, P., Loddo, R., Manfredini, S., Angusti, A., VERONESE A., C, Durini, E., Vertuani, S., Nalin, F., Solaroli, N., Ferrone, Marco, Pricl, Sabrina, Mura, M., PIANO M., A, Poddesu, B., Cadeddu, A., LA COLLA, P., and Loddo, R.

Published
2004

16. Prediction fo HIV-1 resistance to NNRITs: a computer-aided molecular-based rationale

Author

Pricl, Sabrina, Coslanich, Alessandro, Fermeglia, Maurizio, Ferrone, Marco, Paneni, Maria Silvia, Loddo, R., Cabizza, A., Sanna, G., Murreddu, M., La Colla, P., Pricl, Sabrina, Coslanich, Alessandro, Fermeglia, Maurizio, Ferrone, Marco, Paneni, Maria Silvia, Loddo, R., Cabizza, A., Sanna, G., Murreddu, M., and La Colla, P.

Subjects
antiviral drug design, HIV, computer-assisted drug design
Published
2004

17. Synthesis of a New Series of Nucleoside Analogs with Antiflaviviridae Activity and Their Interaction with RNA-Dependent RNA-Polymerase

Author

Pricl, S., Coslanich, A., Fermeglia, M., Ferrone, M., Merzek, M., Angusti, Angela, Ciliberti, Nunzia, Durini, Elisa, Stefano Manfredini, Musiu, C., Marco Mura, Loddo, R., La Colla, P., Pricl, Sabrina, Coslanich, A., Fermeglia, Maurizio, Ferrone, Marco, Merzek, M., Angusti, A., Ciliberti, N., Durini, E., Manfredini, S., Musiu, C., Mura, M., Loddo, R., and La Colla, P.

Subjects
antiviral drug, HCV, computer assistged drug design
Published
2003

18. Antitumor agents. 1. Synthesis, Biological evaluation and molecular modeling of 5H-pyrido[3,2-a]phenoxazin-5-one, a new actynomicin D analog with potent antiproliferative activity

Author

BOLOGNESE A., CORREALE G., MANFRA M., LAVECCHIA A., MAZZONI O., NOVELLINO E., LA COLLA P., LODDO R., MURGIONI C., PANI A., SERRA I., SETZU G., BARONE, VINCENZO, Bolognese, A., Correale, G., Manfra, M., Lavecchia, A., Mazzoni, O., Novellino, E., Barone, Vincenzo, LA COLLA, P., Loddo, R., Murgioni, C., Pani, A., Serra, I., and Setzu, G.

Published
2002

19. Structure-Based Design, Synthesis and Biological Evaluation of Conformationally Restricted Novel 2-Alkylthio-6-[1-(2,6-difluorophenyl)alkyl]-3,4-dihydro-5-alkylpyrimidin-4(3H)-ones (S-DABOs) as Non-Nucleoside Inhibitors of HIV-1 Reverse Transcriptase

Author

MAI A., SBARDELLA G., ARTICO M., RAGNO R., MASSA S., MUSIU C., LA COLLA M., MURGIONI C., LA COLLA P., LODDO R., NOVELLINO, ETTORE, GRECO, GIOVANNI, LAVECCHIA, ANTONIO, Mai, A., Sbardella, G., Artico, M., Ragno, R., Massa, S., Novellino, Ettore, Greco, Giovanni, Lavecchia, Antonio, Musiu, C., LA COLLA, M., Murgioni, C., LA COLLA, P., and Loddo, R.

Published
2001

22. Structure-based Design, Parallel Synthesis, SAR and Molecular Modelling Studies of Thiocarbamates, New Potent Non-Nucleoside HIV-1 Reverse Transcriptase Inhibitor Isosteres of Phenethylthiazolylthiourea (PETT) Derivatives

Author

Ranise, Angelo, Spallarossa, Andrea, Cesarini, Sara, Bondavalli, Francesco, Schenone, Silvia, Bruno, Olga, Menozzi, Giulia, Fossa, Paola, Mosti, Luisa, LA COLLA, M., Sanna, G., Murreddu, M., Collu, G., Busonera, B., Marongiu, M. E., Pani, A., LA COLLA, P., and Loddo, R.

Subjects
molecular modeling, HIV-1, reverse transcriptase inhibitor
Published
2005

27. 2,6-Bis(3,4,5-trihydroxybenzylydene) derivatives of cyclohexanone: novel potent HIV-1 integrase inhibitors that prevent HIV-1 multiplication in cell-based assays

Author

Costi, Roberta, DI SANTO, Roberto, Artico, Marino, Massa, S., Ragno, Rino, Loddo, R., La Colla, M., Tramomtano, E., La Colla, P., and Pani, A.

Subjects
anti-hiv-1-in agents, Anti-HIV Agents, Cyclohexanones, Cell Line, Tumor, cyclohexanone derivatives, polyhydroxylated aromatics, qsar studies, HIV-1, Humans, HIV Integrase, HIV Integrase Inhibitors, Virus Replication
Abstract

A number of 2,6-bisbenzylidenecyclohexane-1-one derivatives have been synthesized and tested as HIV-1 integrase (IN) inhibitors with the aim of obtaining compounds capable to elicit antiviral activity at non-cytotoxic concentrations in cell-based assays. 3,5-Bis(3,4,5-trihydroxybenzylidene)-4-oxocyclohexaneacetic acid (20d) resulted one of the most potent and selective derivatives in acutely infected MT-4 cells (EC(50) and CC(50) values of 2 and 40 microM, respectively). In enzyme assays with recombinant HIV-1 integrase (rIN), this compound proved able to inhibit both 3'-processing and disintegration with IC(50) values of 0.2 and 0.5 microM, respectively. In order to develop a model capable to predict the anti HIV-IN activity and useful to design novel derivatives, we performed a comparative molecular field analysis (CoMFA) like 3-D-QSAR. In our model the ligands were described quantitatively in the GRID program, and the model was optimized by selecting only the most informative variables in the GOLPE program. We found the predictive ability of the model to increase significantly when the number of variables was reduced from 20,925 to 1327. A Q(2) of 0.73 was obtained with the final model, confirming the predictive ability of the model. By studying the PLS coefficients in informative 3-D contour plots, ideas for the synthesis of new compounds could be generated.

Published
2003

28. Pirrolo[1, 2-f]phenantridines and Related Non-Rigid Analogues as Antiviral Agents

Author

Almerico A.M., Mingoia F., Diana P., Barraja P., Montalbano A., Lauria A., Loddo R., Sanna L., Delpiano D., Setzu M.G., and Musiu C.

Abstract

As extension of previous studies on polycyclic planar systems which synthetic approach and antiproliferative activity against leukemic cells (FLC, DRTL) were reported, now we became interested to test their antireplicative activity against human immunodeficiency virus since the incorporation of the pyrrole moiety has already led to several classes of non nucleoside reverse transcriptase inhibitors. For this purpose new and non new derivatives of the planar system pyrrolo[1,2-f]phenanthridine and their “non-rigid analogues” were chosen as model framework reaching in total to more than forty compounds variously functionalized. The need for the search of new anti-HIV agent is still pursued because of the increasing spread of the disease in spite of several prevention campaigns, and because of the rapid appearance of drug resistant viral strains which limits drug effectiveness. Among the current anti-HIV agents the reverse transcriptase inhibitors the Nevirapine and TIBO have an important clinical role. It is suggested that they interact with an allosteric site of the enzyme assuming a “butterfly conformation.” This type of conformation is proposed in our “non-rigid” analogue derivatives tested. Molecular modelling studies by using some physico-chemical descriptors (molecular volume, accessible surface area) evidenced good similarities when compared with planar derivatives and highly described substituted pyrroles and were found in good agreement with the docking studies performed by Ding et al, which proposed a receptor having a “butterfly shape region”. At the same time, the superimposition in the conformation of the minimum of energy between Nevirapine, some selected planar compounds and the corresponding non-rigid analogues showed a good geometric fit between the structures (RMS in the range 0.0270-0.0455). These data suggest that a lot of our derivatives could fit favourably in the same binding pocket. Biological screenings evidenced that only few derivatives showed a moderate selectivity against HIV-1, suggesting that even planar molecules having suitable size can inhibit virus replication probably interacting with the same receptor. Moreover, an interesting biological new data has emerged: a planar derivative showed unique properties being able not only to reduce the virus-induced cyto-pathogenecity, but also to stimulate the growth (20-35%) of the same lymphocytes. Considering that the stimulation of the lymphocytes cells can be a crucial factor in anti-AIDS therapy, this class of compounds can be considered for further developments of new candidates which join anti-AIDS and immuno-stimulant activity.

Published
2002

40. Structure-Based Design, Parallel Synthesis, Structure−Activity Relationship, and Molecular Modeling Studies of Thiocarbamates, New Potent Non-Nucleoside HIV-1 Reverse Transcriptase Inhibitor Isosteres of Phenethylthiazolylthiourea Derivatives

Author

Ranise, A., Spallarossa, A., Cesarini, S., Bondavalli, F., Schenone, S., Bruno, O., Menozzi, G., Fossa, P., Mosti, L., Colla, M. La, Sanna, G., Murreddu, M., Collu, G., Busonera, B., Marongiu, M. E., Pani, A., Colla, P. La, and Loddo, R.

Abstract

In this paper we describe our structure-based ligand design, synthetic strategy, and structure−activity relationship (SAR) studies that led to the identification of thiocarbamates (TCs), a novel class of non-nucleoside reverse transcriptase inhibitors (NNRTIs), isosteres of phenethylthiazolylthiourea (PETT) derivatives. Assuming as a lead compound O-[2-(phthalimido)ethyl]phenylthiocarbamate 12, one of the precursors of the previously described acylthiocarbamates (Ranise, A.; et al. J. Med. Chem. 2003, 46, 768−781), two targeted solution-phase TC libraries were prepared by parallel synthesis. The lead optimization strategy led to para-substituted TCs 31, 33, 34, 39, 40, 41, 44, 45, and 50, which were active against wild-type HIV-1 in MT-4-based assays at nanomolar concentrations (EC50 range:  0.04−0.01 μM). The most potent congener 50 (EC50 = 0.01 μM) bears a methyl group at position 4 of the phthalimide moiety and a nitro group at the para position of the N-phenyl ring. Most of the TCs showed good selectivity indices, since no cytotoxic effect was detected at concentrations as high as 100 μM. TCs 31, 37, 39, 40, and 44 significantly reduced the multiplication of the Y181C mutant, but they were inactive against K103R and K103N + Y181C mutants. Nevertheless, the fold increase in resistance of 41 was not greater than that of efavirenz against the K103R mutant in enzyme assays. The docking model predictions were consistent with in vitro biological assays of the anti-HIV-1 activity of the TCs and related compounds synthesized.

Published
2005

41. Simple, Short Peptide Derivatives of a Sulfonylindolecarboxamide (L-737,126) Active in Vitro against HIV-1 Wild Type and Variants Carrying Non-Nucleoside Reverse Transcriptase Inhibitor Resistance Mutations

Author

Silvestri, R., Artico, M., Martino, G. De, Regina, G. La, Loddo, R., Colla, M. La, and Colla, P. La

Abstract

Non-nucleoside reverse transcriptase inhibitors (NNRTIs) active against NNRTI-resistant mutants were obtained by introducing two methyl groups at positions 3 and 5 of the benzenesulfonyl moiety of L-737,126 (1) and coupling one to three glycinamide/alaninamide units to its carboxyamide function. In cell-based assays, the new derivatives showed activities against HIV-1 wild type and NNRTI-resistant mutants [Y181C, K103N−Y181C, and triple mutant (K103R, V179D, P225H) highly resistant to efavirenz] superior to that of the parent indole derivative 1.

Published
2004

42. Antitumor Agents. 3. Design, Synthesis, and Biological Evaluation of New Pyridoisoquinolindione and Dihydrothienoquinolindione Derivatives with Potent Cytotoxic Activity

Author

Bolognese, A., Correale, G., Manfra, M., Lavecchia, A., Mazzoni, O., Novellino, E., Colla, P. La, Sanna, G., and Loddo, R.

Abstract

New antiproliferative compounds, the 1-aryl-3-ethoxycarbonyl-pyrido[2,3-g]isoquinolin-5,10-diones (PIQDs, 17), were designed on the basis of a molecular model obtained by aligning the common quinolinquinone substructure of 5H-pyrido[3,2-a]phenoxazin-5-one (PPH) and some known anticancer agents. A Diels−Alder reaction between quinolin-5,8-dione (QD) and a 2-azadiene, formed by demolition of 2-aryl-1,3-thiazolidine ethyl esters (T compounds), was used to produce 17 and the isomeric 1-aryl-3-ethoxycarbonylpyrido[3,2-g]isoquinolin-5,10-diones (814). Two other compounds, the 3-amino-3-ethoxycarbonyldihydrothieno[2,3-g]quinolin-4,9-dione (15) and the 3-amino-3-ethoxycarbonyldihydrothieno[3,2-g]quinolin-4,9-dione (16), arising from a 1,4 Michael reaction of QD with a thiolate species formed by opening of T compounds, were recovered from the reaction mixture. The antiproliferative activity of 116 was evaluated against representative human liquid and solid neoplastic cell lines. The IC50 of these compounds had median values in the range 2.00−0.01 μM, with 24 and 15 exhibiting significantly higher in vitro cytotoxic activity. Compound 2, also evaluated against KB subclones (KBMDR, KB7D, and KBV20C), was shown to be scarcely subject to the MDR1/P-glycoprotein drug efflux pump responsible for drug resistance. The noncovalent DNA-binding properties of PIQDs were examined using UV−vis and 1H NMR spectroscopy experiments. Accordingly, these compounds were confirmed to have an ability to intercalate into double-stranded DNA by topoisomerase I superhelix unwinding assay. Interesting structure−activity relationships were found. Three important features seem to contribute to the cytotoxic activity of these anticancer ligands:  (i) the DNA intercalating capability of the three-cyclic quinonic system, typical of this class of compounds, (ii) the position of the pendant phenyl ring that, according to the superimposition model, must occupy the same area of the corresponding benzo-fused ring A of PPH, and (iii) the effect of electron-withdrawing substituents on the phenyl ring, which can contribute improving the π−π stacking interactions between ligand and DNA base pairs. Besides, a mechanism of action suspected to involve topoisomerases could be hypothesized to interpret the antiproliferative activity of the thienoquinolindione 15, which can be regarded as a cyclic cysteine derivative.

Published
2004

43. Antitumor Agents. 2. Synthesis, Structure−Activity Relationships, and Biological Evaluation of Substituted 5H-Pyridophenoxazin-5-ones with Potent Antiproliferative Activity

Author

Bolognese, A., Correale, G., Manfra, M., Lavecchia, A., Mazzoni, O., Novellino, E., Barone, V., Colla, P. La, and Loddo, R.

Abstract

New antiproliferative compounds, 5H-pyrido[3,2-a]phenoxazin-5-ones (110), 5H-benzophenoxazin-5-one (11), 5H-pyrido[2,3-a]phenoxazin-5-one (12), 5H-pyrido[3,4-a]phenoxazin-5-one (13), and 5H-pyrido[4,3-a]phenoxazin-5-one (14), were synthesized and evaluated against representative human neoplastic cell lines. The excellent cytotoxic activity of these polycyclic phenoxazinones, structurally related to the actinomycin chromophore, is discussed in terms of structural changes made to rings A and D (Chart 1). Electron-withdrawing or electron-donating substituents were introduced at different positions of ring A to probe the electronic and positional effects of the substitution. A nitro group in R2 or in R1 increases the cytotoxic activity, whereas electron-donating methyl groups in any position lead to 10- to 100-fold decreasing of the activity. The low antiproliferative activity of benzophenoxazinone 11 and pyridophenoxazinones 13 and 14 confirms the crucial role of pyridine nitrogen in the W position of ring D in DNA binding. The unexpected high activity exhibited by 12, which has the nitrogen in the X position, could be ascribed to a different mechanism of action, which needs further investigation.

Published
2002
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44. Antitumor Agents. 1. Synthesis, Biological Evaluation, and Molecular Modeling of 5H-Pyrido[3,2-a]phenoxazin-5-one, a Compound with Potent Antiproliferative Activity

Author

Bolognese, A., Correale, G., Manfra, M., Lavecchia, A., Mazzoni, O., Novellino, E., Barone, V., Pani, A., Tramontano, E., Colla, P. La, Murgioni, C., Serra, I., Setzu, G., and Loddo, R.

Abstract

The iminoquinone is an important moiety of a large number of antineoplastic drugs and plays a significant role in the nucleus of actinomycins, powerful, highly toxic, natural antibiotics that target DNA as intercalating agents. A series of polycyclic iminoquinonic compounds, 2-amino-3H-phenoxazin-3-one (1), 2-amino-1,9-diacetyl-3H-phenoxazin-3-one (2), 2-acetylamino-3H-phenoxazin-3-one (3), 3H-phenoxazin-3-one (4), 5H-pyrido[3,2-a]phenoxazin-5-one (5), and 5H-pyrido[3,2-a]phenothiazin-5-one (6), strictly related to the actinomycin chromophore, were synthesized for developing new anticancer intercalating drugs. The antiproliferative activity of these compounds, evaluated against representative human liquid and solid neoplastic cell lines, showed that 5 and its isoster 6 were the most active compounds inhibiting cell proliferation in a submicromolar range. Compound 5 was also evaluated against KB subclones (KBMDR, KB7D, and KBV20C), which overexpress the MDR1/P-glycoprotein drug efflux pump responsible for drug resistance. All the above KB subclones did not show altered sensitivity to the antiproliferative activity of 5. UV−vis and 1H NMR spectroscopy experiments support the phenoxazinone 5/DNA binding. Molecular mechanics methods were used to build a three-dimensional model of the 5/[d(GAAGCTTC)]2 complex. Electrostatic interactions between the hydrogen of the positively charged pyridine nitrogen of 5 and the negatively charged oxygen atoms (O4‘ and O5‘) of the cytosine C5 residue together with stacking forces contribute to the high antiproliferative activity. The metal(II)-assisted synthesis procedure of 5 is described, and the formation mechanism is proposed.

Published
2002
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45. Synthesis, Biological Evaluation, and Binding Mode of Novel 1-[2-(Diarylmethoxy)ethyl]-2-methyl-5-nitroimidazoles Targeted at the HIV-1 Reverse Transcriptase

Author

Silvestri, R., Artico, M., Martino, G. De, Ragno, R., Massa, S., Loddo, R., Murgioni, C., Loi, A. G., Colla, P. La, and Pani, A.

Abstract

A novel series of 1-[2-(diarylmethoxy)ethyl]-2-methyl-5-nitroimidazole (DAMNI) analogues were synthesized and tested in cell-based assays and in enzyme assays against HIV-1 recombinant reverse transcriptase (RT). Preparation of the new derivatives was performed by reacting the appropriate benzhydrols or the correspondig bromides with 1-(2-hydroxyethyl)-2-methyl-5-nitroimidazole or the 3-hydroxypropyl homologue. Several compounds showed anti-HIV-1 activity in the submicromolar range. Structure−activity relationship studies suggested that meta substitution at one phenyl ring of the diarylmethane moiety strongly influences the antiviral activity. The 3,5-disubstitution at the same phenyl ring led to less potent derivatives. Molecular modeling and docking studies within the RT non-nucleoside binding site confirmed that DAMNIs, similar to other NNRTIs such as TNK-651 and delavirdine (BHAP U90152), assume a butterfly-like conformation that appears to be halfway between that of classical NNRTIs, such as nevirapine, HEPT, TBZ, TIBO, and DABOs, and the conformation of BHAPs. In particular, the diphenylmethane moiety mimics the wings whereas the 1-(2-methyl-5-nitroimidazolyl)ethane portion resembles the BHAP 5-methanesulfonamidoindole-2-carbonylpiperazine portion.

Published
2002
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46. Structure-Based Design, Synthesis, and Biological Evaluation of Conformationally Restricted Novel 2-Alkylthio-6-[1-(2,6-difluorophenyl)alkyl]- 3,4-dihydro-5-alkylpyrimidin-4(3H)-ones as Non-nucleoside Inhibitors of HIV-1 Reverse Transcriptase

Author

Mai, A., Sbardella, G., Artico, M., Ragno, R., Massa, S., Novellino, E., Greco, G., Lavecchia, A., Musiu, C., Colla, M. La, Murgioni, C., Colla, P. La, and Loddo, R.

Abstract

5-Alkyl-2-(alkylthio)-6-(2,6-difluorobenzyl)-3,4-dihydropyrimidin-4(3H)-ones (S-DABOs, 2) have been recently described as a new class of human immunodeficiency virus type 1 (HIV-1) non-nucleoside reverse transcriptase (RT) inhibitors (NNRTIs) active at nanomolar concentrations (Mai, A. et al. J. Med. Chem. 1999, 42, 619−627). In pursuing our lead optimization efforts, we designed novel conformationally restricted S-DABOs, 3, featuring a methyl at the benzylic carbon (Y = Me) and at the pyrimidine 5-position (R = Me). Conformational analyses and docking simulations suggested that the presence of both methyls would significantly reduce conformational flexibility without compromising, in the R enantiomers, the capability of fitting into the RT non-nucleoside binding pocket. To develop structure−activity relationships, we prepared several congeners of type 3 belonging to the thymine (R = Me) and uracil (R = H) series, featuring various 2-alkylthio side chains (X = Me, i-Pr, n-Bu, i-Bu, s-Bu, c-pentyl, and c-hexyl) and aryl moieties different from the 2,6-difluorophenyl (Ar = phenyl, 2,6-dichlorophenyl, 1-naphthyl). Moreover, α-ethyl derivatives (Y = Et) were included in the synthetic project in addition to α-methyl derivatives (Y = Me). All of the new compounds were evaluated for their cytotoxicity and anti-HIV-1 activity in MT-4 cells, and some of them were assayed against highly purified recombinant wild-type HIV-1 RT using homopolymeric template primers. The results were expressed as CC50 (cytotoxicity), EC50 (anti-HIV-1 activity), SI (selectivity, given by the CC50/EC50 ratio), and IC50 (RT inhibitory activity) values. In the 2,6-difluorobenzylthymine (R = Me) series, methylation of the benzylic carbon improved anti-HIV-1 and RT inhibitory activities together with selectivity. Compound 3w (Ar = 2,6-F2-Ph, R = Y = Me, X = c-pentyl) turned out the most potent and selective among the S-DABOs reported to date (CC50 > 200 μM, EC50 = 6 nM, IC50 = 5 nM, and SI > 33 333). Assays performed on the pure enantiomer (+)-3w, much more active than (−)-3w, yielded the following results:  CC50 > 200 μM, EC50 = 2 nM, IC50 = 8 nM, and SI > 100 000, under conditions wherein MKC-442 was less active and selective (CC50 > 200 μM, EC50 = 30 nM, IC50 = 40 nM, SI > 6666). The 2,6-difluorophenylethylthymines (R = Me) were generally endowed with higher potency compared with the uracil counterparts (R = H). In the 2,6-difluorophenyl series the best and the least performant 2-alkylthio side chains were the 2-c-pentylthio and the 2-methylthio, respectively. When the methyl at the benzylic carbon was replaced by an ethyl, activity was retained or decreased slightly, thus suggesting that the dimensions of the cavity within the RT hosting this substituent would not be compatible with groups larger than ethyl. Aryl moieties different from the 2,6-difluorophenyl (phenyl, 1-naphthyl, 2,6-dichlorophenyl) were generally detrimental to activity, consistent with a favorable electronic effect exerted by the 2,6-fluorines on a putative charge-transfer interaction between the aromatic moieties of the inhibitor and Tyr188.

Published
2001

50. 3-Aryl-2-[1H-benzotriazol-1-yl]acrylonitriles: a novel class of potent tubulin inhibitors

Author

Antonio Carta, Manlio Tolomeo, Sabrina Pricl, Paolo La Colla, Maurizio Fermeglia, Erik Laurini, Stefania Grimaudo, Roberta Loddo, Giampiero Boatto, Antonietta Di Cristina, Sandra Piras, Maria Silvia Paneni, Rosaria Maria Pipitone, Irene Briguglio, Paola Posocco, Carta, A., Briguglio, I., Piras, S., Boatto, G., la Colla, P., Loddo, R., Tolomeo, M., Grimaudo, S., Di Cristina, A., Pipitone, M. R., Laurini, Erik, Paneni, Maria Silvia, Posocco, Paola, Fermeglia, Maurizio, Pricl, Sabrina, Carta, A, Briguglio, I, Piras, S, Boatto, G, La Colla, P, Loddo, R, Tolomeo, M, Grimaudo, S, Di Cristina, A, Pipitone, R, Laurini, E, Paneni, M, Posocco, P, Fermeglia, M, and Pricl, S

Subjects
Models, Molecular, Magnetic Resonance Spectroscopy, Molecular model, Stereochemistry, Anti-cancer drugs, Binding, Competitive, Gas Chromatography-Mass Spectrometry, Anti-cancer drug, chemistry.chemical_compound, Structure-Activity Relationship, Tubulin, drug design and development, computer assisted drug design, Drug Discovery, K562 Cell, medicine, Structure–activity relationship, Humans, Pharmacology, biology, Acrylonitrile, Chemistry, Aryl, Organic Chemistry, Cell Cycle, General Medicine, Cell cycle, Triazoles, Podophyllotoxin, Cell culture, Tubulin Binding Agent, biology.protein, Triazole, Colchicine, K562 Cells, Human, medicine.drug
Abstract

During a screening for compounds that could act against Mycobacterium tuberculosis, a series of new cellular antiproliferative agents was identified. The most cytotoxic molecules were evaluated against a panel of human cell lines derived from hematological and solid human tumors. In particular, (E)-2-(1H-benzo[d] [1,2,3]triazol-1-yl)-3-(4-methoxyphenyl)acrylonitrile (1) was found to be of a potency comparable to etoposide and greater than 6-mercaptopurine in all cell lines tested. Accordingly, a synthesis of a new series of (E)-2-(5,6-dichloro-1H-benzo[d] [1,2,3]triazol-1-yl)-3-(4-R-phenyl)acrylonitriles was conducted in order to extend the studies of structure-activity relationship (SAR) for this class of molecules. With the aim to evaluate if 3-aryl-2-[1H-benzotriazol-1-yl]acrylonitriles were able to act like tubulin binding agents, the effects on cell cycle distribution of the most active compounds (1, 2a, 3 and 4) were analyzed in K562 cells. A detailed molecular modeling study of the putative binding mode of this series of compounds on tubulin is also reported.

Published
2011

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