Your search keyword '"MARONGIU, M. E."' showing total 44 results

1. Targeting HIV: old and new players.

Author

Pani A, Loi AG, Mura M, Marceddu T, La Colla P, and Marongiu ME

Subjects

Antiretroviral Therapy, Highly Active, Capsid Proteins drug effects, Cell Nucleus drug effects, Cell Nucleus virology, Gene Expression Regulation, Viral drug effects, HIV Infections prevention & control, HIV Infections virology, HIV Reverse Transcriptase antagonists & inhibitors, Humans, Receptors, Virus drug effects, Reverse Transcriptase Inhibitors pharmacology, Reverse Transcriptase Inhibitors therapeutic use, Anti-HIV Agents pharmacology, Anti-HIV Agents therapeutic use, HIV drug effects, HIV Infections drug therapy

Abstract

Despite the unprecedented successes in the therapy of HIV infection, AIDS remains a major world health problem being the first cause of death in Africa and the fourth leading cause of death worldwide. Rapid emergence of drug-resistant HIV variants and severe side effects limit the efficacy of existing therapies. The intrinsic high variability of HIV calls for combining different drugs with distinct mode of action to achieve synergistic antiviral activity. Efforts are being made to develop agents addressing new steps in HIV replication and to optimize both antiviral activity and pharmacokinetic of the current drugs targeting reverse transcriptase and protease. The class of viral entry inhibitors is undergoing evaluation for both systemic and topical administration, and compounds targeting the fusion step may be the first to reach the market. Identification of compounds unambiguously affecting HIV replication by targeting integrase supports the potential of this crucial viral enzyme as a drug target. Targeting HIV gene regulation, which could also lead to cellular toxicity, may also become an important discovery strategy, provided that inhibitors with sufficient specificity are identified. In this review we will summarize the current understanding of the key steps in HIV life cycle in the context of representative inhibitors based on their modes of action. We then present a summary of compounds under clinical development, with the aim of providing a picture of the current potential for targeting HIV.

Published

2002

2. 1,5-Benzodiazepines. Part XII. Synthesis and biological evaluation of tricyclic and tetracyclic 1,5-benzodiazepine derivatives as nevirapine analogues.

Author

Di Braccio M, Grossi G, Roma G, Vargiu L, Mura M, and Marongiu ME

Subjects

Benzodiazepines chemistry, Benzodiazepines pharmacology, Cell Line, HIV Reverse Transcriptase antagonists & inhibitors, Humans, Microbial Sensitivity Tests, Nevirapine analogs & derivatives, Nevirapine chemistry, Nevirapine pharmacology, Recombinant Proteins antagonists & inhibitors, Reverse Transcriptase Inhibitors chemistry, Reverse Transcriptase Inhibitors pharmacology, Benzodiazepines chemical synthesis, HIV-1 drug effects, Nevirapine chemical synthesis, Reverse Transcriptase Inhibitors chemical synthesis, T-Lymphocytes drug effects

Abstract

A number of properly substituted 5H-pyrimido[4,5-b][1,5]benzodiazepines (2) and pyrazolo[3,4-b][1,5]benzodiazepines (3 and 4), as well as compounds 5-7, which are derivatives of new tetracyclic systems, were prepared as nevirapine analogues through multistep synthetic routes. The cytotoxic and anti-HIV-1 properties of compounds 2-7 were evaluated in cell-based assays, together with their inhibitory activity against the HIV-1 recombinant reverse transcriptase (rRT) in enzyme assays. The modifications introduced into nevirapine heterocyclic skeleton proved to have a negative effect for the anti-HIV-1 activity. It is worth noting that some of the new derivatives proved to be cytotoxic in the low micromolar range.

Published

2001

3. DABOs as candidates to prevent mucosal HIV transmission.

Author

Pani A, Musiu C, Loi AG, Mai A, Loddo R, La Colla P, and Marongiu ME

Subjects

Cell Line, DNA, Viral analysis, HIV Infections transmission, HIV-1 drug effects, HIV-1 genetics, HIV-1 physiology, Humans, In Vitro Techniques, Virus Replication drug effects, Anti-HIV Agents pharmacology, HIV Infections prevention & control, Mucous Membrane virology, Pyrimidines pharmacology, Reverse Transcriptase Inhibitors pharmacology

Abstract

Worldwide, the heterosexual route is the prevalent mode of transmission of AIDS; therefore, demands have been raised for measures that block sexual spreading of the HIV infection. Development of microbicides for topical use may represent an efficacious alternative to condoms. Several approaches are being investigated. Besides surfactants, which directly act on the virus particle, and measures that enhance natural defence mechanisms, promising new candidates appear to be drugs that block the early steps of HIV multiplication. We describe herein a long-term assay which enables the establishment of whether the above drugs reversibly (virustatic action) or irreversibly (virucidal action) inhibit HIV-1 multiplication, thus allowing screening for effective and potent microbicides. We validated our assay with nucleoside (NRTIs) and non-nucleoside reverse transcriptase inhibitors (NNRTIs). Following a chronic treatment, the NRTIs tested (didanosine, zalcitabine, stavudine and lamivudine) simply delayed the viral breakthrough with respect to infected, untreated controls. Under the same experimental conditions, non-nucleoside reveres transcriptase inhibitors (NNRTIs), such as MKC-442, alphaAPA, nevirapine, efavirenz and 3,4-dihydro-2-alkoxy-6-benzyl-4-oxopyrimidines (DABOs) MC 1047 and MC 1220 suppressed HIV-1 replication for the entire experimental period (40 days). When cell culture samples were evaluated for the presence of infectious virus, p24 antigen and viral DNA sequences, none of them was detected up to day 40 post-infection (p.i.). Identical results were obtained after a treatment with the above NNRTIs limited to the first 4 days p.i. Under more selective experimental conditions, that is drug treatments limited to the first 4 h p.i., nevirapine and efavirenz proved to be virustatic; in fact, viral breakthrough ensued shortly after their removal from the culture medium. Conversely, DABO MC 1220 was endowed with potent virucidal activity; in fact, at 3.5 microM it was able to suppress HIV-1 multiplication in cultures acutely infected with a very high multiplicity of infection (5 CCID50/cell), thus allowing exponential cell multiplication as in uninfected cultures for the next 40 days.

Published

2001

4. Structure-activity relationship studies on new DABOS: effect of substitutions at pyrimidine C-5 and C-6 positions on anti-HIV-1 activity.

Author

Sbardella G, Mai A, Artico M, Chimenti P, Massa S, Loddo R, Marongiu ME, La Collat P, and Pani A

Subjects

Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, Anti-HIV Agents toxicity, Cell Line, Chemical Phenomena, Chemistry, Physical, Drug Design, HIV-1 physiology, HIV-2 physiology, Humans, Molecular Structure, Pyrimidinones chemical synthesis, Pyrimidinones pharmacology, Pyrimidinones toxicity, Reverse Transcriptase Inhibitors chemical synthesis, Reverse Transcriptase Inhibitors pharmacology, Reverse Transcriptase Inhibitors toxicity, Structure-Activity Relationship, Virus Replication drug effects, Anti-HIV Agents chemistry, HIV-1 drug effects, HIV-2 drug effects, Pyrimidinones chemistry, Reverse Transcriptase Inhibitors chemistry

Abstract

Several 5-alkyl, 5-alkenyl, 5-iso-alkyl, 5-halo, 5-aminomethyl and 5-carboxy derivatives of S-DABOs (dihydro-alkyl (or cyclo-alkyl)thio-benzyloxopyrimidines), DATNOs (dihydro-alkylthionaphthylmethyl-oxopyrimidines) and F2-S-DABOs (dihydro-alkyl (or cyclo-alkyl)thio-2,6-difluorobenzyl-oxopyrimidines) have been prepared and tested as anti-HIV-1 agents. S-DABO derivatives bearing at C-6 position monosubstituted phenylmethyl or heteroarylmethyl units have also been synthesized. 2-Alkylthio-3,4-dihydropyrimidin-4(3H)-one derivatives of F2-S-DABO series bearing small alkyl groups at C-5 proved to be potent inhibitors of HIV-1 replication in vitro with selectivity indexes ranging from 250 to >2,500.

Published

2001

5. Synthesis and antimicrobial activity of new 3-(1-R-3(5)-methyl-4-nitroso-1H-5(3)-pyrazolyl)-5-methylisoxazoles.

Author

Aiello E, Aiello S, Mingoia F, Bacchi A, Pelizzi G, Musiu C, Setzu MG, Pani A, La Colla P, and Marongiu ME

Subjects

Anti-Bacterial Agents, Anti-Infective Agents chemical synthesis, Anti-Infective Agents chemistry, Anti-Infective Agents pharmacology, Antifungal Agents chemistry, Cryptococcus neoformans drug effects, Fungi drug effects, Gram-Negative Bacteria drug effects, Gram-Positive Bacteria drug effects, HIV-1 drug effects, Humans, Isoxazoles chemistry, Microbial Sensitivity Tests, Structure-Activity Relationship, Antifungal Agents chemical synthesis, Antifungal Agents pharmacology, Isoxazoles chemical synthesis, Isoxazoles pharmacology

Abstract

A number of new 3-(1-R-3(5)-methyl-4-nitroso-1H-5(3)-pyrazolyl)-5-methylisoxazoles 6a-g (7b-f) were synthesized and tested for antibacterial and antifungal activity. Some of these compounds displayed antifungal activity at non-cytotoxic concentrations. Derivative 6c was 9 times more potent in vitro than miconazole and 20 times more selective against C. neoformans. 6c was also 8- and 125-fold more potent than amphotericin B and fluconazole, respectively. None of the compounds was active against bacteria. Preliminary structure-activity relationship (SAR) studies showed that the NO group at position 4 of the pyrazole ring is essential for the activity. Lipophilicity of the pyrazole moiety, N-alkyl chain length and planarity of the two heterocyclic rings appear to play a decisive role in modulating cytotoxicity and antifungal activity.

Published

2000

6. Structure-activity relationship studies on potential non-nucleoside DABO-like inhibitors of HIV-1 reverse transcriptase.

Author

Costi R, Di Santo R, Artico M, Massa S, Lavecchia A, Marceddu T, Sanna L, La Colla P, and Marongiu ME

Subjects

Drug Evaluation, Preclinical methods, Humans, Microbial Sensitivity Tests methods, Nucleosides chemistry, Pyrimidinones chemistry, Pyrimidinones pharmacology, Structure-Activity Relationship, Sulfides chemistry, Sulfides pharmacology, Reverse Transcriptase Inhibitors chemistry, Reverse Transcriptase Inhibitors pharmacology

Abstract

Using 2,6-dichloro-4-aminopyrimidine, a number of uracil and cytosine derivatives with both arylthio and alkoxy moieties were prepared. These novel pyrimidines share chemical similarities with DABOs and HEPTs, two classes of non-nucleoside human immunodeficiency virus type 1 (HIV-1) reverse transcriptase inhibitors (NNRTIs), which have been widely studied of late. All new derivatives were tested in MT-4 cells to explore their potential in vivo anti-HIV activity. Like other NNRTIs, they selectively inhibit HIV-1 but not HIV-2. The majority of test derivatives were found to have low potency and were sometimes more cytotoxic than zidovudine and emivirine (formerly MKC-442), used here as reference drugs. Uracil and cytosine derivatives bearing a sec-butoxy chain and a methyl-substituted benzenesulphonyl moiety were the most potent. Enzyme assays proved that these derivatives target RT. Structure-activity relationship studies established a correlation between the anti-HIV-1 activity and the meta substitution on the phenyl ring; furthermore, oxidation of sulphide to sulphone significantly increased the potency of certain derivatives.

Published

2000

7. Peptide T-araC conjugates: solid-phase synthesis and biological activity of N4-(acylpeptidyl)-araC.

Author

Manfredini S, Marastoni-M, Tomatis R, Durini E, Spisani S, Pani A, Marceddu T, Musiu C, Marongiu ME, and La Colla P

Subjects

Antimetabolites, Antineoplastic chemistry, Antimetabolites, Antineoplastic pharmacology, CD4 Antigens, Cell Division drug effects, Chemotaxis drug effects, Cytarabine chemical synthesis, Dose-Response Relationship, Drug, Drug Carriers chemical synthesis, Drug Carriers chemistry, Drug Stability, Humans, Inhibitory Concentration 50, Monocytes drug effects, Oligopeptides chemical synthesis, Oligopeptides metabolism, Peptide Hydrolases metabolism, Peptide T chemical synthesis, Prodrugs chemical synthesis, Prodrugs pharmacology, Time Factors, Tumor Cells, Cultured drug effects, Cytarabine chemistry, Cytarabine pharmacology, Peptide T chemistry, Peptide T pharmacology

Abstract

Due to the capability of peptidyl derivatives of araC to behave as prodrugs of this antimetabolite, and because of the well known biological properties of peptide T and its analogues (in particular that of targeting CD4+ cells), new peptide T-araC conjugates were prepared and tested in vitro for antiproliferative activity. The aim was that of specifically delivering the antitumor drug to CD4+ cells. N4-(Acylpeptidyl)-derivatives of araC were synthesized by a new general approach involving solid-phase synthesis, which allows mild conditions, avoids the usually required protection of the glycoside portion of nucleosides and affords high yields of the final products. After the demonstration that peptide T-araC conjugates were able to activate chemotaxis by binding CD4 receptor on monocyte membranes, the antiproliferative activity was evaluated against a panel of leukemia lymphoma and carcinoma cell lines derived from human tumors, three CD4+ cell lines included. Title compounds resulted effective as antiproliferative agents at concentrations 4- to 10-fold higher than those of araC alone, did not preferentially inhibit CD4+ cells and proved stable not only in cell culture medium containing 20% FCS, but also in human plasma. All this suggests their potential utility in vivo.

Published

2000

8. Anti-HIV-1 integrase drugs: how far from the shelf?

Author

Pani A and Marongiu ME

Subjects

Animals, HIV Infections drug therapy, HIV Infections virology, HIV Integrase Inhibitors chemical synthesis, HIV Integrase Inhibitors therapeutic use, HIV-1 drug effects, HIV-1 enzymology, HIV-1 ultrastructure, Humans, Drug Design, HIV Integrase metabolism, HIV Integrase Inhibitors pharmacology

Abstract

Chemotherapy of HIV-1 infection/AIDS currently employs inhibitors of two products of the viral pol gene, the reverse transcriptase and protease enzymes. However, a third product of the pol gene is essential for retroviral multiplication, the integrase. As no cellular homologue of HIV integrase has been described, potential inhibitors could be relatively nontoxic. Development of HIV-1 integrase inhibitors could have favorable implication for combination therapy, including potential synergy with currently available inhibitors, as well as prevention of the chronic carrier state and the emergence of resistant mutants. Although several classes of putative integrase inhibitors that been described, still no clinically useful anti-integration drugs are available. It is the structural and functional complexity of the integration process together with the limitations of the available in vitro assays that has made it problematic to develop inhibitors of the HIV integrase. In this review we summarize current knowledge concerning the biology of this enzyme and of the integration process, and discuss major classes representatives of integrase inhibitors considering the obstacles to the development of true anti-integrase drugs.

Published

2000

9. Derivatives of the new ring system indolo[1,2-c]benzo[1,2,3]triazine with potent antitumor and antimicrobial activity.

Author

Cirrincione G, Almerico AM, Barraja P, Diana P, Lauria A, Passannanti A, Musiu C, Pani A, Murtas P, Minnei C, Marongiu ME, and La Colla P

Subjects

Anti-Bacterial Agents, Anti-HIV Agents chemical synthesis, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Anti-Infective Agents chemistry, Anti-Infective Agents pharmacology, Antifungal Agents chemical synthesis, Antifungal Agents chemistry, Antifungal Agents pharmacology, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Bacteria drug effects, Bacteria isolation & purification, Drug Evaluation, Preclinical, Drug Resistance, Multiple, Drug Resistance, Neoplasm, HIV-1, Humans, Microbial Sensitivity Tests, Structure-Activity Relationship, Triazines chemistry, Triazines pharmacology, Tumor Cells, Cultured, Anti-Infective Agents chemical synthesis, Antineoplastic Agents chemical synthesis, Triazines chemical synthesis

Abstract

Derivatives of the new ring system indolo[1,2-c]benzo[1,2,3]triazine 5 were synthesized by diazotization of substituted 2-(2-aminophenyl)indoles followed by an intramolecular coupling reaction of the diazonium group with the indole nitrogen. To obtain the indolobenzotriazine system it was necessary to protect the 3 position of the indole nucleus to avoid cyclization into the indolo[3,2-c]cinnoline system 4. Indolobenzotriazines 5a-g were evaluated in vitro for antitumor activity against a panel of leukemia-, lymphoma-, carcinoma-, and neuroblastoma-derived cell lines. Some compounds inhibited the proliferation of T and B cell lines at submicromolar concentrations, whereas their activity against solid tumor cell lines was in the micromolar range. When evaluated for their antifungal potential 5a,d inhibited some of the fungi tested, although at concentrations very close to those inhibiting the proliferation of human cells. On the contrary, all indolobenzotriazines proved fairly potent and selective inhibitors of Streptococcus and Staphylococcus. In particular 5b,c,g were up to 80 times more potent than the reference drug streptomycin and inhibited the growth of the above Gram-positive bacteria at concentrations far lower than those cytotoxic for animal cells.

Published

1999

10. 5-Alkyl-2-(alkylthio)-6-(2,6-dihalophenylmethyl)-3, 4-dihydropyrimidin-4(3H)-ones: novel potent and selective dihydro-alkoxy-benzyl-oxopyrimidine derivatives.

Author

Mai A, Artico M, Sbardella G, Massa S, Novellino E, Greco G, Loi AG, Tramontano E, Marongiu ME, and La Colla P

Subjects

Animals, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Cell Line, Cell Survival drug effects, Drug Design, HIV-1 drug effects, Mice, Models, Molecular, Pyrimidines chemistry, Pyrimidines pharmacology, Recombinant Proteins antagonists & inhibitors, Reverse Transcriptase Inhibitors chemistry, Reverse Transcriptase Inhibitors pharmacology, Structure-Activity Relationship, Anti-HIV Agents chemical synthesis, HIV Reverse Transcriptase antagonists & inhibitors, Pyrimidines chemical synthesis, Reverse Transcriptase Inhibitors chemical synthesis

Abstract

Molecular modeling analysis of compounds belonging to the recently published series of dihydro-alkoxy-benzyl-oxopyrimidines (DABOs), such as S-DABOs and DATNOs, gave support to the design of new 2, 6-disubstituted benzyl-DABO derivatives as highly potent and specific inhibitors of the HIV-1 reverse transcriptase (RT). To follow up on the novel DABO derivatives, we decided to investigate the effect of electron-withdrawing substituents in the benzyl unit of the S-DABO skeleton versus their anti-HIV-1 activity. Such chemical modifications impacted the inhibitory activity, especially when two halogen units were introduced at positions 2 and 6 in the phenyl portion of the benzyl group bound to C-6 of the pyrimidine ring. Various 5-alkyl-2-(alkyl(or cycloalkyl)thio)-6-(2, 6-dichloro(or 2,6-difluoro)phenylmethyl)-3, 4-dihydropyrimidin-4(3H)-ones were then synthesized and tested as anti-HIV-1 agents in both cell-based and enzyme (recombinant reverse transcriptase, rRT) assays. Among the various mono- and disubstituted phenyl derivatives, the most potent were those containing a 6-(2,6-difluorophenylmethyl) substituent (F-DABOs), which showed EC50's ranging between 40 and 90 nM and selectivity indexes up to >/=5000. An excellent correlation was found between EC50 and IC50 values which confirmed that these compounds act as inhibitors of the HIV-1 RT. The structure-activity relationships of the newly synthesized pyrimidinones are presented herein.

Published

1999

11. Geometrically and conformationally restrained cinnamoyl compounds as inhibitors of HIV-1 integrase: synthesis, biological evaluation, and molecular modeling.

Author

Artico M, Di Santo R, Costi R, Novellino E, Greco G, Massa S, Tramontano E, Marongiu ME, De Montis A, and La Colla P

Subjects

Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Cell Division drug effects, Crystallography, X-Ray, HIV-1 drug effects, HIV-1 growth & development, Humans, Structure-Activity Relationship, Tumor Cells, Cultured, Virus Replication drug effects, Anti-HIV Agents chemical synthesis, Anti-HIV Agents chemistry, Anti-HIV Agents pharmacology, Cinnamates chemical synthesis, Cinnamates chemistry, Cinnamates pharmacology, HIV Integrase Inhibitors chemical synthesis, HIV Integrase Inhibitors chemistry, HIV Integrase Inhibitors pharmacology, HIV-1 enzymology, Models, Molecular

Abstract

Various cinnammoyl-based structures were synthesized and tested in enzyme assays as inhibitors of the HIV-1 integrase (IN). The majority of compounds were designed as geometrically or conformationally constrained analogues of caffeic acid phenethyl ester (CAPE) and were characterized by a syn disposition of the carbonyl group with respect to the vinylic double bond. Since the cinnamoyl moiety present in flavones such as quercetin (inactive on HIV-1-infected cells) is frozen in an anti arrangement, it was hoped that fixing our compounds in a syn disposition could favor anti-HIV-1 activity in cell-based assays. Geometrical and conformational properties of the designed compounds were taken into account through analysis of X-ray structures available from the Cambridge Structural Database. The polyhydroxylated analogues were prepared by reacting 3,4-bis(tetrahydropyran-2-yloxy)benzaldehyde with various compounds having active methylene groups such as 2-propanone, cyclopentanone, cyclohexanone, 1,3-diacetylbenzene, 2, 4-dihydroxyacetophenone, 2,3-dihydro-1-indanone, 2,3-dihydro-1, 3-indandione, and others. While active against both 3'-processing and strand-transfer reactions, the new compounds, curcumin included, failed to inhibit the HIV-1 multiplication in acutely infected MT-4 cells. Nevertheless, they specifically inhibited the enzymatic reactions associated with IN, being totally inactive against other viral (HIV-1 reverse transcriptase) and cellular (RNA polymerase II) nucleic acid-processing enzymes. On the other hand, title compounds were endowed with remarkable antiproliferative activity, whose potency correlated neither with the presence of catechols (possible source of reactive quinones) nor with inhibition of topoisomerases. The SARs developed for our compounds led to novel findings concerning the molecular determinants of IN inhibitory activity within the class of cinnamoyl-based structures. We hypothesize that these compounds bind to IN featuring the cinnamoyl residue C=C-C=O in a syn disposition, differently from flavone derivatives characterized by an anti arrangement about the same fragment. Certain inhibitors, lacking one of the two pharmacophoric catechol hydroxyls, retain moderate potency thanks to nonpharmacophoric fragments (i.e., a m-methoxy group in curcumin) which favorably interact with an "accessory" region of IN. This region is supposed to be located adjacent to the binding site accommodating the pharmacophoric dihydroxycinnamoyl moiety. Disruption of coplanarity in the inhibitor structure abolishes activity owing to poor shape complementarity with the target or an exceedingly high strain energy of the coplanar conformation.

Published

1998

12. Synthesis and biological evaluation of a series of substituted pyrazolo[3,4-d]-1,2,3-triazoles and pyrazolo[3,4-d]oxazoles.

Author

Vicentini CB, Manfredini S, Manfrini M, Bazzanini R, Musiu C, Putzolu M, Perra G, and Marongiu ME

Subjects

Anti-Bacterial Agents pharmacology, Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, Antifungal Agents chemical synthesis, Antifungal Agents pharmacology, Bacteria drug effects, Humans, Microbial Sensitivity Tests, Oxazoles pharmacology, Triazoles pharmacology, Anti-Bacterial Agents chemical synthesis, Oxazoles chemical synthesis, Triazoles chemical synthesis

Abstract

In view of the biological relevance of triazole-based heterocyclic structures as antifungal, antiviral, and antitumor agents, we have synthesized a series of substituted pyrazolo[3,4-d]-1,2,3-triazoles (2e-h, 2j, 4b) which we evaluated for their cytostatic and antiviral (HIV-1 included) activity and for their capability to inhibit the multiplication of various human pathogenic fungi and bacteria. Moreover, the biological activities of a few compounds, namely pyrazolo[3,4-d]oxazoles (3a-e) and pyrazolo[3,4-d]-1,2,3-triazoles (2a-d, 4a, 5), previously obtained by us but not investigated for their biological activity, were also studied. Only compounds 3a-e were endowed with a significative antiproliferative activity on the human lymphoblastoid cell line MT-4 cells. All pyrazole derivatives proved ineffective in protecting cell cultures against the HIV-1-induced cytopathogenicity, and none of the compounds was active against the bacteria and fungi tested.

Published

1998

13. In vitro and in vivo antiproliferative activity of IPCAR, a new pyrazole nucleoside analog.

Author

Pani A, Marongiu ME, Pinna E, Scintu F, Perra G, Montis AD, Manfredini S, and La Colla P

Subjects

Animals, Antimetabolites, Antineoplastic therapeutic use, CHO Cells, Cells, Cultured, Cricetinae, Drug Resistance, Multiple, Drug Resistance, Neoplasm, Female, HeLa Cells, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells drug effects, Humans, IMP Dehydrogenase antagonists & inhibitors, KB Cells, Lymphocytes cytology, Lymphocytes drug effects, Mice, Mice, Inbred BALB C, Mice, Inbred DBA, Molecular Structure, Nucleosides chemical synthesis, Nucleosides therapeutic use, Purines pharmacology, Pyrazoles chemical synthesis, Pyrazoles therapeutic use, Pyrimidines pharmacology, Ribavirin analogs & derivatives, Ribavirin toxicity, Ribonucleosides pharmacology, Survival Rate, Tumor Cells, Cultured, Antimetabolites, Antineoplastic toxicity, Cell Survival drug effects, Leukemia L1210 drug therapy, Nucleosides toxicity, Pyrazoles toxicity

Abstract

IPCAR is a pyrazole nucleoside analog which belongs to a class of compounds structurally related to the inosine monophosphate (IMP) dehydrogenase (IMPDH) inhibitors ribavirin, selenazofurin and tiazofurin. Unlike other anticancer drugs, IPCAR showed a potent and broad-spectrum antiproliferative activity in vitro coupled with low cytotoxicity for resting PBL and CFU-GM. IPCAR proved fully inhibitory against human nasopharyngeal carcinoma KB cells expressing the MDR phenotype, whereas IPCAR-resistant renal adenocarcinoma ACHN/R1 cells were fully susceptible to inhibition by a number of anticancer drugs, with the exception of 6TG, 6MP and 5FU towards which they showed a partial cross-resistance. In combinations studies, IPCAR proved synergistic with 6MP, 6TG, 5FU and ribavirin, and additive with ara-A, MTX, doxorubicin, taxol and tiazofurin. Antagonistic effects were never observed. Although the precise molecular target of IPCAR remains to be identified, the data presented herein suggest that, unlike ribavirin and tiazofurin, this drug inhibits a step of the de novo purine biosynthesis different from the conversion of IMP into GMP. In vivo, IPCAR showed low acute toxicity (DL10 > 1000 mg/kg) and was active against the L1210 murine lymphocytic leukemia model. Drug doses of 125 and 250 mg/kg on a day-1, -3 and -5 dosing schedule increased the life span (ILS) relative to untreated control mice of 36.4 and 68.2%, respectively, whereas administration of 500 mg/kg on days 1 and 3 resulted in a ILS of 86.4% and also increased the 30-day survival rate (25% of the mice).

Published

1998

14. Potent and selective inhibitors of human immunodeficiency virus protease structurally related to L-694,746.

Author

Franchetti P, Perlini P, Abu Sheikha G, Cappellacci L, Grifantini M, Loi AG, De Montis A, Pani A, Marongiu ME, and La Colla P

Subjects

Amides chemical synthesis, Anti-HIV Agents pharmacology, Antiviral Agents chemical synthesis, Antiviral Agents pharmacology, Cell Line, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors pharmacology, Humans, Molecular Structure, Morpholines pharmacology, Anti-HIV Agents chemical synthesis, HIV Protease Inhibitors chemical synthesis, Peptides pharmacology

Abstract

A series of human immunodeficiency virus (HIV) protease inhibitors, which are analogues of N-[2(R)-hydroxy-1(S)- indanyl]-5(S)-[(tert-butyloxycarbonyl)amino]-4(S)-hydroxy-6-phenyl-2-(R) - [[4-(carboxymethoxy)phenyl]methyl]hexanamide (L-694,746), a metabolite of the anti-HIV agent L-689,502, were synthesized. In these compounds, the acetic group linked to the para position of the P1' phenyl in the reference inhibitor was replaced either by the bioisosteric phosphonomethoxy group and its diisopropyl/dibenzyl derivatives, or the 1H-tetrazol-5-yl-methoxy group and its 1-benzyl derivative. In enzyme assays, phosphonomethoxy and tetrazolmethoxy analogues proved to be potent inhibitors of the HIV-1 protease, with IC50 values as low as 0.04 nM. When tested for anti-HIV-1 activity in cell-based assays, most of the new derivatives proved active, with benzyl derivatives being more active than their highly polar, unsubstituted counterparts. The dibenzylphosphonomethoxy analogue was the most active compound, with an EC50 value of 10 nM and a selectivity index of 20,000. When compounds were examined for their capability to reduce p24 levels in both acutely and chronically infected MT-4 and H9/IIIB cells, all of them were found to be active at concentrations close to those capable of preventing HIV-1-induced cytopathic effect.

Published

1998

15. Glycosidopyrroles. Part 3. Effect of the benzocondensation on acyclic derivatives: 1-(2-hydroxyethoxy) methylindoles as potential antiviral agents.

Author

Almerico AM, Barraja P, Diana P, Cirrincione G, Mingoia F, Musiu C, Perra G, Putzolu M, and Marongiu ME

Subjects

Animals, Anti-HIV Agents pharmacology, Cell Line, Chlorocebus aethiops, Cytopathogenic Effect, Viral drug effects, Gram-Negative Bacteria drug effects, Gram-Positive Bacteria drug effects, HIV-1 drug effects, HIV-1 pathogenicity, Humans, Microbial Sensitivity Tests, Pyrroles pharmacology, Vero Cells, Virus Replication drug effects, Anti-HIV Agents chemistry, Indoles chemistry, Pyrroles chemistry

Abstract

The new of 1-(2-hydroxyethoxy)methylindole derivatives 3a-i were prepared in good yields. None of them showed any significant anti-HIV activity and therefore the benzocondensation between the 2 and 3 positions of the pyrrole ring definitely reduced the weak activity found in the analogues 1a-c.

Published

1998

16. Synthesis and biological evaluation of 5H-indolo [3,2-b][1,5]benzothiazepine derivatives, designed as conformationally constrained analogues of the human immunodeficiency virus type 1 reverse transcriptase inhibitor L-737,126.

Author

Silvestri R, Artico M, Bruno B, Massa S, Novellino E, Greco G, Marongiu ME, Pani A, De Montis A, and La Colla P

Subjects

Anti-HIV Agents chemistry, Cell Line, HIV Reverse Transcriptase drug effects, Humans, Indoles chemistry, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Structure, Reverse Transcriptase Inhibitors chemistry, Structure-Activity Relationship, Sulfones chemistry, Anti-HIV Agents chemical synthesis, Anti-HIV Agents pharmacology, HIV-1 drug effects, HIV-2 drug effects, Indoles chemical synthesis, Indoles pharmacology, Reverse Transcriptase Inhibitors chemical synthesis, Reverse Transcriptase Inhibitors pharmacology, Sulfones chemical synthesis, Sulfones pharmacology

Abstract

In the presence of sodium hydride, reaction of aryl-disulphides with ethyl esters of indole-2-carboxylic acids furnished ethyl 3-arylthioindole-2-carboxylates, which were cyclized intramolecularly to afford 5H-indolo[3,2-b][1,5]benzothiazepin-6(7H)-ones or hydrolysed in alkaline medium to give 3-arylthioindole-2-carboxylic acids. These acids, also obtained by the action of aryldisulphides on indole-2-carboxylic acids, afforded tetracyclic 5H-indolo [3,2-b][1,5]benzothiazepin-6(7H)-ones upon treatment with EDCI-DMAP. Transformation of cyclic sulphides into the required sulphones was achieved by treatment with hydrogen peroxide or with m-chloroperbenzoic acid. The title derivatives are conformationally constrained analogues of the potent human immunodeficiency virus type 1 (HIV-1) reverse transcriptase inhibitor 3-benzene-sulphonyl-5-chloroindole-2-carboxamide (L-737, 126). Although the indolobenzothiazepine derivatives, as well as the indolyl aryl sulphones used for their synthesis, were endowed with anti-HIV-1 activities in the submicromolar and micromolar range, none of them proved more potent than L-737,126.

Published

1998

17. 1,2,5-Benzothiadiazepine and pyrrolo[2,1-d]-[1,2,5]benzothiadiazepine derivatives with specific anti-human immunodeficiency virus type 1 activity.

Author

Di Santo R, Costi R, Artico M, Massa S, Marongiu ME, Loi AG, De Montis A, and La Colla P

Subjects

Anti-HIV Agents chemistry, Azepines chemistry, Benzothiadiazines chemistry, Cell Line, Cytopathogenic Effect, Viral drug effects, HIV-1 pathogenicity, HIV-1 physiology, HIV-2 pathogenicity, HIV-2 physiology, Humans, Structure-Activity Relationship, Virus Replication drug effects, Anti-HIV Agents pharmacology, Azepines pharmacology, Benzothiadiazines pharmacology, HIV-1 drug effects, HIV-2 drug effects

Abstract

We synthesized and tested as novel inhibitors of human immunodeficiency virus type 1 (HIV-1) bi- and tricyclic thiadiazine ring homologues of 7-chloro-2-ethyl-2H-1,2,4-benzothiadiazin-3-(4H)-one 1,1-dioxide, which is a compound endowed with anti-HIV-1 activity at low micromolar concentrations. Benzothiadiazepine derivatives were obtained by alkylation of 8-chloro-2,3-dihydro-3-methyl-1,2,5-benzothiadiazepin-4(5H)-one 1,1-dioxide, which was obtained by intramolecular cyclization of 2-(2-amino-5-chloro-benzenesulphonamido) propanoic acid. Pyrrolobenzothiadiazepines were synthesized from N-substituted 5-chloro-2-(1H-pyrrol-1-yl)benzene-sulphonamides by treating with triphosgene. N6-substituted pyrrolo[2,1-d][1,2,5]benzothiazepin-7(6H)-one 5,5-dioxides were active, though not very potent. Both a chlorine atom and an unsaturated alkyl chain were found to be determinants of anti-HIV-1 activity. The highest potency was shown by a derivative with a TIBO-related 3,3-dimethylallyl chain. 2,3-Dihydro-1,2,5-benzothiadiazepin-4(5H)-one 1,1-dioxides were scarcely active in HIV-1-infected MT-4 cell assays; however, the introduction of the dimethylallyl chain into 7-chloro-1,2,5-benzothiadiazepine moiety led to a bicyclic derivative which was more potent and less cytotoxic than the tricyclic pyrrole-containing counterpart.

Published

1998

18. Glycosidopyrroles. Part 2. Acyclic derivatives: 1-(1,3-dihydroxy-2-propoxy)methylpyrroles as potential antiviral agents.

Author

Almerico AM, Diana P, Barraja P, Dattolo G, Mingoia F, Putzolu M, Perra G, Milia C, Musiu C, and Marongiu ME

Subjects

Animals, Anti-HIV Agents chemical synthesis, Anti-HIV Agents chemistry, Chlorocebus aethiops, HIV-1 drug effects, HIV-1 physiology, Humans, Pyrroles chemical synthesis, Pyrroles chemistry, Vero Cells, Virus Replication drug effects, Anti-HIV Agents pharmacology, Pyrroles pharmacology

Abstract

The series of 1-(1,3-dihydroxy-2-propoxy)methylpyrroles 2a-o were prepared in good overall yields according to Scheme I. When evaluated for antiviral activity against HIV-1, only compounds of the triphenyl series (R3 = NH2, N3, Br) were found to inhibit the HIV-1 replication at concentrations that were very not cytotoxic for MT-4 cells, with selectivity index 1.5-9.3. None of these compounds showed antibacterial or antifungal activity.

Published

1997

19. Native oligodeoxynucleotides specifically active against human immunodeficiency virus type 1 in vitro: a G-quartet-driven effect?

Author

Tondelli L, Colonna FP, Garbesi A, Zanella S, Marongiu ME, Corrias S, Loi AG, and La Colla P

Subjects

Anti-HIV Agents analysis, Cell Fusion, Cells, Cultured, Circular Dichroism, Genes, Viral, HIV Infections virology, HIV Reverse Transcriptase antagonists & inhibitors, HIV-2 drug effects, Humans, Oligonucleotides analysis, Structure-Activity Relationship, Virus Replication drug effects, Anti-HIV Agents pharmacology, HIV-1 drug effects, Oligonucleotides pharmacology

Abstract

Among a series of unmodified phosphodiester (PO)-oligodeoxynucleotides (PO-ODNs) complementary to some of the human immunodeficiency virus type 1 (HIV-1) regulatory genes, several PO-ODN sequences complementary to the vpr gene (PO-ODNs-a-vpr, where a-vpr is the antisense vpr sequence) emerged as potent inhibitors (at concentrations of 0.8 to 3.3 microM) of HIV-1 multiplication in de novo infected MT-4 cells, while they showed no cytotoxicity for uninfected cells at concentrations up to 100 microM. Unlike phosphorothioate counterparts, PO-ODN-a-vpr sequences were not inhibitory to HIV-2 multiplication in de novo infected C8166 cells and neither prevented the fusion between chronically infected and bystander CD4+ cells nor inhibited the activity of the HIV-1 reverse transcriptase in enzyme assays. Moreover, they were not inhibitory to HIV-1 multiplication in chronically infected cells. Delayed addition experiments showed that PO-ODNs-a-vpr inhibit an event in the HIV-1 replication cycle following adsorption to the host cell, but preceding reverse transcription. Structure-activity relationship studies indicated that the antiviral activity of the test PO-ODN-a-vpr sequences is not related to an antisense mechanism but to the presence, within the active sequences, of contiguous guanine residues. Physical characterization of the test PO-ODNs suggested that the active structure is a tetramer stabilized by G quartets (i.e., four G residues connected by eight hydrogen bonds).

Published

1996

20. Enhancement of the anti-HIV-1 activity of ddAdo by coformycin, EHNA and deaza-EHNA derivatives.

Author

Marongiu ME, Pani A, Tinti E, Grifantini M, Franchetti P, Cristalli G, and La Colla P

Subjects

Adenine administration & dosage, Cell Line, Drug Evaluation, Preclinical, Drug Synergism, HIV-1 physiology, Humans, Virus Replication drug effects, Adenine analogs & derivatives, Adenosine Deaminase Inhibitors, Antiviral Agents administration & dosage, Coformycin administration & dosage, Dideoxyadenosine administration & dosage, Enzyme Inhibitors administration & dosage, HIV-1 drug effects

Abstract

2',3'-dideoxyadenosine (ddAdo) and 2',3'-dideoxyinosine (ddIno) are potent and selective inhibitors of the replication of the human immunodeficiency virus type 1 (HIV1) in several cell culture systems. Equipotent in terms of antiviral activity, both compounds selectively inhibit the reverse transcription of HIV-1 by virtue of their conversion into ddATP. In human lymphoid cells ddAdo is converted to the active metabolite, ddATP, but it also undergoes rapid deamination, via adenosine deaminase, to form ddIno. ddIno, like ddAdo, gives rise to dideoxynucleotides of the dideoxy-adenylate series (ddAMP, ddADP and ddATP), as well as to IMP and to adenylate ribonucleotides. With the main object of blocking the deamination of ddAdo, we studied its anti-HIV-1 activity in the presence of different adenosine deaminase inhibitors, namely Coformycin (CF), 9-(erythro-2-hydroxy-3-nonyl) adenine (EHNA) and some deaza-EHNA derivatives. In contrast with reports on 2'-deoxycoformycin (Cooney et al., 1987), the adenosine deaminase inhibitors tested by us showed a significant increase in the antiviral activity of ddAdo, but not of ddIno. Enhancement was obtained with EHNA and CF concentrations up to 250 and > 12,500 times lower than their respective maximum non toxic doses. In combination with EHNA or CF, ddAdo could be used at concentrations up to ten times lower than those required to obtain the same degree of inhibition when ddAdo (or ddIno) was used alone. The use of EHNA or CF in combination with ddAdo at concentrations that inhibit the multiplication of HIV-1, allowed uninfected cells to maintain their normal multiplication rates. In fact, in combination experiments, cytotoxic effects were evident only with doses of EHNA, or CF and ddAdo 10 to 100 or more times higher than those required to inhibit HIV-1 significantly. The in vivo implications of these results for anti-HIV chemotherapy are discussed.

Published

1995

21. [[[(Thienylcarbonyl)alkyl]oxy]phenyl]- and [[[(pyrrylcarbonyl)alkyl]oxy]phenyl]oxazoline derivatives with potent and selective antihuman rhinovirus activity.

Author

Massa S, Corelli F, Artico M, Mai A, Ragno R, De Montis A, Loi AG, Corrias S, Marongiu ME, and La Colla P

Subjects

Cytopathogenic Effect, Viral drug effects, HeLa Cells, Humans, Structure-Activity Relationship, Tetrazolium Salts, Thiazoles, Antiviral Agents chemical synthesis, Antiviral Agents pharmacology, Oxazoles chemical synthesis, Oxazoles pharmacology, Rhinovirus drug effects

Abstract

As an approach to more extensive structural modifications of [(oxazolylphenoxy)alkyl]isoxazoles, we synthesized new compounds characterized by the replacement of the isoxazole nucleus with furan, pyrrole, and thiophene rings and by the presence of a ketocarbonyl group in the aliphatic chain connecting these pentatomic heterocycles to the 4-(4,5-dihydro-2-oxazolyl)phenoxy, 4-(ethoxycarbonyl)phenoxy, and 4-carboxyphenoxy moieties. Some pentamethylene derivatives were also prepared, and their antirhinovirus activity was compared to that of the corresponding ketomethylene derivatives. Syntheses were carried out by Friedel-Crafts acylation of the above pentatomic heterocycles and subsequent reaction of chloroalkyl ketones with the proper 4-substituted phenol. Reduction of the ketone function afforded the related polymethylene derivatives. The new compounds were tested for antirhinovirus activity and cytotoxicity in comparison with WIN 51711, used as reference drug. Inspection of the structure-activity relationships revealed that the thiophene ring and the carbonyl group are the structural components which to a large extent contribute to the positive biological profile in terms of both wideness of spectrum and low cytotoxicity. Among the various derivatives, compounds 8e,d showed in vitro the same potency of WIN 51711 but a cytotoxicity at least 10 times lower.

Published

1995

22. Characterization of the anti-HIV-1 activity of 3,4-dihydro-2-alkoxy-6-benzyl-4-oxopyrimidines (DABOs), new non-nucleoside reverse transcriptase inhibitors.

Author

Tramontano E, Marongiu ME, de Montis A, Loi AG, Artico M, Massa S, Mai A, and la Colla P

Subjects

Antiviral Agents chemistry, Antiviral Agents toxicity, Cells, Cultured, Dideoxynucleotides, Drug Interactions, HIV Reverse Transcriptase, HIV-1 enzymology, HIV-1 growth & development, Pyrimidines toxicity, Pyrimidinones pharmacology, Thymine Nucleotides pharmacology, Virus Replication drug effects, Zidovudine analogs & derivatives, Zidovudine pharmacology, Antiviral Agents pharmacology, HIV-1 drug effects, Pyrimidines pharmacology, Reverse Transcriptase Inhibitors

Abstract

Novel 3,4-dihydro-6-benzyl-4-oxopyrimidines (DABOs), variously substituted at both the C-2 and C-5 positions of the pyrimidine ring, proved to be specific inhibitors of the human immunodeficiency virus type 1 (HIV-1) in vitro. Some compounds showed potency at micromolar doses, no cytotoxicity at the maximum testable doses and selectivity indexes comparable to that of 2'-3'-dideoxyinosine (ddI). Mode of action studies suggested that DABOs interfered with a step of the virus multiplication cycle following adsorption and preceding integration. Enzyme assays indicated that DABOs targeted HIV-1 reverse transcriptase: they inhibited the RNA-dependent DNA polymerase activity in a template-dependent manner and, to a lesser extent, the DNA-dependent DNA polymerase activity. No inhibition of the RNase-H associated activity was observed. When DABOs were assayed in combination with 3'-azido-3'-dideoxythymidine (AZT) or ddI against HIV-1 in cell cultures, a slightly synergistic inhibitory effect was observed. The combination of DABO 546 and AZTTP in enzyme assays showed that the two compounds were kinetically mutually exclusive.

Published

1994

23. Modulatory effect of N-acetyl-L-cysteine on the HIV-1 multiplication in chronically and acutely infected cell lines.

Author

Pani A, Marongiu ME, and La Colla P

Subjects

Acquired Immunodeficiency Syndrome drug therapy, Cell Division drug effects, Cell Fusion physiology, Cell Line, Dextran Sulfate pharmacology, HIV-1 growth & development, Humans, Lymphoid Tissue cytology, Lymphoid Tissue microbiology, T-Lymphocytes drug effects, Zidovudine pharmacology, Acetylcysteine pharmacology, Antiviral Agents pharmacology, HIV-1 drug effects, HIV-1 physiology, T-Lymphocytes microbiology, Virus Replication drug effects

Abstract

N-acetyl-L-cysteine (NAC) is known to antagonize the PMA- or cytokine-stimulated HIV-1 replication in latently and acutely infected monocytic and lymphocytic cell lines, and to reduce the virus multiplication in acutely infected, PHA-stimulated PBMC. We here report on the modulatory effects of NAC on the HIV-1 multiplication in both chronically and acutely infected lymphocytes that produce high virus levels independently from cytokine activation. In both cases, NAC doses of 0.12 and 0.25 mM decreased, whereas doses of 0.5-2 mM increased the infectious HIV-1 yield. At these concentrations, the modulatory effect of NAC on the HIV-1 multiplication paralleled that on cell proliferation, suggesting a close correlation between the two phenomena; in fact, under conditions where NAC could not modulate the cell growth, the drug also failed to modulate the HIV-1 multiplication. High NAC concentrations (4-16 mM), which were able to increase the proliferative rate of both chronically infected H9/IIIB and normal T lymphocytes, increased up to 6-fold the virus multiplication in H9/IIIB cells but were inhibitory to HIV-1 in acutely infected cells. This inhibition was due to the fact that, like dextran sulfate, NAC interfered with an early event in the virus growth cycle. The finding that high NAC doses were also capable of preventing syncytium formation in H9/IIIB and C8166 (or MT-4) cocultures further indicated an interference of the drug with receptor-binding-related events.

Published

1993

24. Pyrazole-related nucleosides. Synthesis and antiviral/antitumor activity of some substituted pyrazole and pyrazolo[4,3-d]-1,2,3-triazin-4-one nucleosides.

Author

Manfredini S, Bazzanini R, Baraldi PG, Guarneri M, Simoni D, Marongiu ME, Pani A, Tramontano E, and La Colla P

Subjects

Animals, Antineoplastic Agents pharmacology, Antiviral Agents pharmacology, B-Lymphocytes drug effects, Cell Division drug effects, Cyclization, Enterovirus drug effects, Glycosylation, HIV-1 drug effects, Humans, Leukemia L1210 pathology, Mice, Molecular Structure, Nucleosides pharmacology, Pyrazoles pharmacology, Silicon, Structure-Activity Relationship, T-Lymphocytes drug effects, Tumor Cells, Cultured, Vero Cells, Antineoplastic Agents chemical synthesis, Antiviral Agents chemical synthesis, Nucleosides chemical synthesis, Organosilicon Compounds, Pyrazoles chemical synthesis

Abstract

Several pyrazole and pyrazolo[4,3-d]-1,2,3-triazin-4-one ribonucleosides were prepared and tested for antiviral/antitumor activities. Appropriate heterocyclic bases were prepared by standard methodologies. Glycosylation of pyrazoles 6a-e,g,i and of pyrazolo[4,3-d]-1,2,3-triazin-4-ones 12f-1 mediated by silylation with hexamethyldisilazane, with 1-beta-O-acetyl-2,3,5-tri-O-benzoyl-D-ribofuranose, gave in good yields the corresponding glycosides 7a-e,g, 8g,i, 13f,h,k, and 14f, but could not be applied to compounds 12g,i,j,l. To overcome this occurrence, a different strategy involving the preparation, diazotization, and in situ cyclization of opportune pyrazole glycosides 9 and 10 was required. Moreover derivatives having the general formula 5 were considered not only as synthetic intermediates in the synthesis of 3 but also as carbon bioisosteres of ribavirin 4. All compounds were evaluated in vitro for cytostatic and antiviral activity. The pyrazolo[4,3-d]-1,2,3-triazin-4-one nucleosides that resulted were substantially devoid of any activity; only 15h,k showed a moderate cytostatic activity against T-cells. However, pyrazole nucleosides 9b,c,e were potent and selective cytotoxic agents against T-lymphocytes, whereas 9e showed a selective, although not very potent, activity against coxsackie B1.

Published

1992

25. Antimicrobial and antiviral activity of xylosyl-methylthio-adenosine, a naturally occurring analogue of methylthio-adenosine from Doris verrucosa.

Author

Pani A, Marongiu ME, Obino P, Gavagnin M, and La Colla P

Subjects

Adenosine pharmacology, Animals, Cell Survival drug effects, Cells, Cultured, Adenosine analogs & derivatives, Anti-Bacterial Agents, Antifungal Agents, Antiviral Agents pharmacology, Deoxyadenosines pharmacology, Mollusca chemistry, Thionucleosides pharmacology

Abstract

Xylosyl-methylthio-adenosine, a naturally occurring analogue of 5'-deoxy-5'-methylthio-adenosine, has been postulated to play a protective role during egg development in the mollusc Doris verrucosa. However, in vitro tests showed that this analogue is devoid of activity against fungi, bacteria and viruses.

Published

1991

26. Antiviral agents: synthesis of furylpyrimidinones and evaluation of their cytostatic and antiviral activity.

Author

Botta M, De Angelis F, Corelli F, Menichincheri M, Nicoletti R, Marongiu ME, Pani A, and La Colla P

Subjects

Animals, Furans pharmacology, HIV-1 drug effects, Humans, Mice, Pyrimidinones pharmacology, Simplexvirus drug effects, Tumor Cells, Cultured drug effects, Vero Cells, Antineoplastic Agents chemical synthesis, Antiviral Agents chemical synthesis, Furans chemical synthesis, Pyrimidinones chemical synthesis

Abstract

Condensation between furyllithium reagents and pyrimidinones 1, 2, 3, and 4 has been studied. The product composition is strongly dependent upon the reaction conditions and purification methodologies. Cytostatic and antiviral activities of some substrates and reaction products is reported.

Published

1991

27. Effect of ultraviolet light on DNA structure in 5-iodo-2'-deoxyuridine-substituted HSV-1 DNA.

Author

Wood TG, Marongiu ME, and Prusoff WH

Subjects

DNA Damage, DNA, Viral genetics, DNA, Viral ultrastructure, Simplexvirus ultrastructure, DNA, Viral radiation effects, Idoxuridine, Simplexvirus genetics, Ultraviolet Rays

Abstract

Herpes simplex virus type-1 (HSV-1) was grown in the presence of 5-iodo-2'-deoxyuridine (IdUrd), and the virion-DNA was isolated by isopycnic centrifugation in CsCl. Irradiation of IdUrd-containing HSV DNA with either 302 nm or 254 nm ultraviolet (UV) light introduced strand breakage into the DNA in a dose-dependent manner when analyzed by alkaline sucrose density gradient sedimentation. Irradiation of unsubstituted HSV DNA under similar conditions produced little strand breakage. These observations are in agreement with the proposed mechanism for photochemical generation of strand breakage in 5-halo-2'-deoxyuridine-containing DNA. Irradiation of IdUrd-substituted virions followed by analysis of the isolated DNA indicated less strand breakage than irradiation of isolated IdUrd-substituted DNA under equivalent conditions. The dosage of irradiation required to introduce DNA strand breakage in IdUrd-substituted virions was equivalent to that employed to affect greater than 99% loss of infectious virus activity in both control and IdUrd-containing virions. It is suggested that the relative UV insensitivity of IdUrd-substituted HSV may be due to the microstructure environment of the substituted HSV DNA which may favor recombination of the photochemically formed halogen-uracil radical pairs.

Published

1991

28. Synthesis and antimicrobial and cytotoxic activities of pyrrole-containing analogues of trichostatin A.

Author

Massa S, Artico M, Corelli F, Mai A, Di Santo R, Cortes S, Marongiu ME, Pani A, and La Colla P

Subjects

Animals, Anti-Bacterial Agents chemistry, Antifungal Agents chemistry, Antiviral Agents chemistry, Cell Division drug effects, Cell Survival drug effects, Chemical Phenomena, Chemistry, Physical, Dose-Response Relationship, Drug, Hydroxamic Acids antagonists & inhibitors, Hydroxamic Acids chemical synthesis, Hydroxamic Acids chemistry, Pyrroles, Regression Analysis, Structure-Activity Relationship, Vero Cells, Anti-Bacterial Agents chemical synthesis, Antifungal Agents chemical synthesis, Antiviral Agents chemical synthesis

Abstract

A number of aroylpyrroleacrylic acid derivatives were synthesized by standard procedures and evaluated for cytotoxicity in Vero cells and for capacity to inhibit the multiplication of viruses, bacteria, and fungi. While none of the test compounds showed any activity against bacteria and fungi, most of them inhibited the replication of some DNA viruses at concentrations allowing the exponential growth of uninfected cells. In particular three compounds (8, 9c, and 10h) showed an antiviral activity at doses that were from 4- to greater than 8-fold lower than the maximum nontoxic doses.

Published

1990

29. Effect of 3'-deoxythymidin-2'-ene (d4T) on nucleoside metabolism in H9 cells.

Author

Marongiu ME, August EM, and Prusoff WH

Subjects

Amino Acids metabolism, Cell Division drug effects, Cell Survival drug effects, Cells, Cultured drug effects, Cytidine metabolism, Deoxycytidine metabolism, Humans, Stavudine, Thymidine metabolism, Thymidine Kinase metabolism, Uridine metabolism, Dideoxynucleosides pharmacology, Nucleosides metabolism

Abstract

The effect of 3'-deoxythymidin-2'-ene (d4T) on the metabolism of exogenously supplied radiolabeled nucleosides was investigated. Following a 24-hr exposure to 250 microM d4T, we observed no significant effect on the incorporation of [3H]thymidine or [3H]deoxycytidine into DNA. In contrast, the amounts of [3H]uridine, [3H]deoxyuridine, and [3H]cytidine were significantly lower than those incorporated by control cultures. d4T had no significant effect on the incorporation of [3H]uridine or [3H]cytidine into RNA, or the incorporation of 3H-labeled amino acids into protein. In d4T-treated cells the relative proportions of [3H]dTMP, [3H]dTDP, and [3H]dTTP formed did not change but their absolute concentrations were increased. d4T significantly reduced the level of [3H]dUMP, and a parallel decrease in [3H]dTMP derived from [3H]dUMP was also evident. d4T increased the amounts of labeled deoxycytidine metabolites formed, with increased dCMP levels the most prominent. In a cell-free extract, [3H]d4T was phosphorylated at a rate of 1.6 pmol/30 min. Increasing concentrations of both thymidine and deoxyuridine inhibited the phosphorylation of [3H]d4T with IC50 values of 5.7 and 35 microM respectively. d4T was found to be a weak substrate for purified H9 cytosolic thymidine kinase (Km = 138 microM) and a weak competitive inhibitor of thymidine and deoxyuridine phosphorylation by this enzyme (Ki = 1.37 and 0.33 mM respectively).

Published

1990

30. Poliovirus morphogenesis. I. Identification of 80S dissociable particles and evidence for the artifactual production of procapsids.

Author

Marongiu ME, Pani A, Corrias MV, Sau M, and La Colla P

Subjects

Cell Line, Humans, Hydrogen-Ion Concentration, Morphogenesis, Poliovirus metabolism, Sodium Dodecyl Sulfate, Temperature, Capsid metabolism, Poliovirus growth & development, Viral Proteins metabolism, Virion metabolism

Abstract

The current model of poliovirus morphogenesis postulates a fundamental role for procapsid, 80S shells that, upon interaction with viral RNA and subsequent proteolytic cleavage, give rise to complete virus particles. Although 80S sedimenting particles can, indeed, be isolated from cytoplasmic extracts of infected cells, their physical properties differ from those reported for procapsids. Far from being stable structures, they can be dissociated by pH 8.5 and 0.1% sodium dodecyl sulfate into slower-sedimenting subunits. The reasons for this discrepancy were investigated, and two main modalities leading to the appearance of procapsids in vitro were identified. The first involves a temperature-mediated conversion of dissociable 80S particles into stable 80S procapsids, and the second involves the self-assembly of endogenous 14S subunits, also primed by an increase in the temperature of cytoplasmic extracts.

Published

1981

31. [Models for resistance and dependence in viruses].

Author

Pani A, Marongiu ME, Corrias MV, and La Colla P

Subjects

Amantadine analogs & derivatives, Animals, Aphthovirus drug effects, Drug Resistance, Microbial, Guanidine, Humans, Amantadine pharmacology, Guanidines pharmacology, Influenza A virus drug effects, Picornaviridae drug effects

Published

1987

32. On the importance of thiols and disulphides and the antiviral action of dichloropyrimidines.

Author

Pompei R, Marcialis MA, Flore O, Marongiu ME, and Garzia A

Subjects

Disulfides pharmacology, Structure-Activity Relationship, Viruses drug effects, Antiviral Agents, Pyrimidines pharmacology, Sulfhydryl Compounds pharmacology, Sulfhydryl Reagents pharmacology

Published

1977

33. Approaches to antiviral drug development.

Author

Prusoff WH, Lin TS, August EM, Wood TG, and Marongiu ME

Subjects

Binding Sites, Drug Design, Genes, Viral, Structure-Activity Relationship, Thymidine Kinase antagonists & inhibitors, United States, United States Food and Drug Administration, Virus Replication drug effects, Antiviral Agents pharmacology, Virus Diseases therapy

Abstract

At present, only a few drugs have been approved by the FDA for therapy of viral infections in humans. There is a great need for antiviral drugs with increased potency and decreased toxicity, as well as drugs to treat viral diseases for which no drug or vaccine is currently available. Two approaches for development of antiviral drugs are described--an empirical strategy and a rational strategy--with several examples of each. Although many compounds have potent antiviral activity in cell culture, only a small fraction of these will go on to become antiviral drugs for use in humans. At this time, only seven synthetic compounds and alpha interferon have been approved by the FDA for therapy of viral infections in humans. None of these approved drugs are without toxicities, however, and hence there is a great need for antiviral drugs with increased potency and decreased toxicity, as well as for drugs to treat viral diseases for which no drug or vaccine is currently available. Two approaches for the development of antiviral drugs--the empirical and the rational strategies--and their applications and future directions are discussed.

Published

1989

34. 5-(2-bromoethyl)-2'-deoxyuridine: a selective inhibitor of herpes simplex viruses in vitro.

Author

La Colla P, Pani A, Marongiu ME, Corrias MV, Flore O, Marcello C, and Lecca U

Subjects

Bromodeoxyuridine pharmacology, Humans, Antiviral Agents pharmacology, Bromodeoxyuridine analogs & derivatives, Herpes Simplex drug therapy

Abstract

A new pyrimidine analog, 5-(2-bromoethyl)-2'-deoxyuridine (BEUdR), was tested in vitro for antiviral activity on Herpes simplex virus types 1 and 2. As reference compounds, ACG, BVUdR and PAA were used. Compared to ACG and BVUdR, BEUdR resulted less potent on both HSV-1 and HSV-2. However, a 50% inhibition of the multiplication of uninfected cells could be obtained only at very high BEUdR concentration (ID50 = 8500 microM). This makes BEUdR the least toxic analog known and gives it a selective index comparable to, if not better, than of ACG and BVUdR.

Published

1989

35. [Analogs of pyrimidine nucleosides with selective antiherpetic activity].

Author

La Colla P, Pani A, Corrias MV, and Marongiu ME

Subjects

DNA Replication drug effects, Enzyme Induction drug effects, Herpesviridae Infections enzymology, Humans, Structure-Activity Relationship, Virus Replication drug effects, Herpesviridae Infections drug therapy, Pyrimidine Nucleosides therapeutic use

Published

1985

36. Initial studies on the cellular pharmacology of 3'-deoxythymidin-2'-ene (d4T): a potent and selective inhibitor of human immunodeficiency virus.

Author

August EM, Marongiu ME, Lin TS, and Prusoff WH

Subjects

Cell Division drug effects, Cell Line, Chromatography, High Pressure Liquid, Dideoxynucleosides pharmacokinetics, Humans, Stavudine, Virus Replication drug effects, Dideoxynucleosides pharmacology, HIV drug effects

Published

1988

37. Characterization and role in morphogenesis of a new subviral particle (55S) isolated from poliovirus-infected cells.

Author

Corrias MV, Flore O, Broi E, Marongiu ME, Pani A, Torelli S, and La Colla P

Subjects

Cell Line, HeLa Cells cytology, Humans, Hydrogen-Ion Concentration, Molecular Weight, Osmolar Concentration, Peptides analysis, Poliovirus ultrastructure, Viral Proteins analysis, Morphogenesis, Poliovirus isolation & purification

Abstract

A previously undetected subviral particle, designated the 55S particle because of its position in sucrose density gradients, has been found in cytoplasmic extracts of poliovirus-infected cells. It contains no RNA, is composed of equimolar amounts of the structural polypeptides P1AB, P1C, and P1D, and is stable in vitro under a variety of conditions: presence or absence of EDTA, dilution in low- or high-ionic-strength buffers, suspension in buffers up to pH 10, incubation at 37 degrees C, and centrifugation to equilibrium in CsCl gradients (where it bands at a density of 1.285 g/cm3). Conventional pulse-chase experiments show that 55S particles are the products of the assembly of 14S subunits and the precursors of virions. These data led to the formulation of a model of poliovirus morphogenesis in which the conversion of capsomers into 73S empty capsids does not occur directly, but through the formation of an intermediate structure, the 55S particle.

Published

1987

38. Metabolic changes induced by 15(S) 15-methyl prostaglandin F2 alpha in tumoral cells.

Author

Caminiti F, De Murtas M, Parodo G, Lecca U, Marongiu ME, La Colla P, and Nasi A

Subjects

Cell Division drug effects, Cell Line, DNA, Neoplasm biosynthesis, Dinoprost, Humans, Neoplasm Proteins biosynthesis, Neoplasms physiopathology, RNA, Neoplasm biosynthesis, Carboprost pharmacology, Neoplasms metabolism, Prostaglandins F pharmacology, Prostaglandins F, Synthetic pharmacology

Published

1980

39. Influence of hydrocortisone on cytopathic effect of Newcastle disease virus and stability to freezing of vescicular stomatitis virus.

Author

Pompei R, Marcialis MA, Flore O, Pani A, Marongiu ME, and Manconi PE

Subjects

Cells, Cultured, Cytopathogenic Effect, Viral drug effects, Freezing, Vesicular stomatitis Indiana virus drug effects, Vesicular stomatitis Indiana virus pathogenicity, Hydrocortisone pharmacology, Newcastle disease virus drug effects

Abstract

The presence of hydrocortisone in virus-infected cell cultures leads to enhancement of the syncytia forming ability of Newcastle disease virus and to production of vescicular stomatitis virus particles which loose their infectivity upon storage below 0 degrees C.

Published

1978

40. Antiherpes activity of 5-(2-bromoethyl)-2'-deoxyuridine.

Author

La Colla P, Gelli G, Mura L, Landini MP, Corrias MV, Pani A, and Marongiu ME

Subjects

Acyclovir pharmacology, Animals, Bromodeoxyuridine pharmacology, Cell Division drug effects, Cell Line, Cytomegalovirus drug effects, Cytomegalovirus genetics, Cytomegalovirus growth & development, DNA, Viral biosynthesis, DNA-Directed DNA Polymerase, Humans, Idoxuridine pharmacology, Mutation, Phosphonoacetic Acid pharmacology, Phosphorylation, Simplexvirus genetics, Simplexvirus growth & development, Thymidine Kinase metabolism, Viral Plaque Assay, Antiviral Agents pharmacology, Bromodeoxyuridine analogs & derivatives, Simplexvirus drug effects

Published

1985

41. Dichloropyrimidines: specific inhibitors of virus growth.

Author

Flore O, Marcialis MA, Marongiu ME, Pompei R, La Colla P, and Loddo B

Subjects

Cysteine pharmacology, Glutamine pharmacology, Mercaptoethanol pharmacology, Pyrimidines antagonists & inhibitors, Structure-Activity Relationship, Virus Replication drug effects, Viruses, Antiviral Agents antagonists & inhibitors, Pyrimidines pharmacology

Published

1977

42. Enhancement of virus growth produced by thiols and disulphides.

Author

Marcialis MA, Flore O, Marongiu ME, Pompei R, La Colla P, and Loddo B

Subjects

Encephalomyocarditis virus drug effects, Encephalomyocarditis virus growth & development, Poliovirus drug effects, Poliovirus growth & development, Simplexvirus drug effects, Simplexvirus growth & development, Stimulation, Chemical, Vaccinia virus drug effects, Vaccinia virus growth & development, Vesicular stomatitis Indiana virus drug effects, Vesicular stomatitis Indiana virus growth & development, Viruses drug effects, Disulfides pharmacology, Sulfhydryl Compounds pharmacology, Viruses growth & development

Abstract

Several thiols and disulphides have been found able both to shorten the latency phase and to increase the growth of several virus strains in cell cultures.

Published

1977

43. Evaluation of the toxicity of the dopaminergic neurotoxins MPTP and MPP+ in PC12 pheochromocytoma cells: binding and biological studies.

Author

Marongiu ME, Piccardi MP, Bernardi F, Corsini GU, and Del Zompo M

Subjects

1-Methyl-4-phenyl-1,2,3,6-tetrahydropyridine, 1-Methyl-4-phenylpyridinium, Adrenal Gland Neoplasms metabolism, Animals, Binding Sites, Cell Division drug effects, Cell Line, Cell Survival drug effects, Dose-Response Relationship, Drug, Macromolecular Substances, Monoamine Oxidase Inhibitors pharmacology, Pheochromocytoma metabolism, Pyridines antagonists & inhibitors, Pyridines metabolism, Pyridinium Compounds metabolism, Rats, Tumor Cells, Cultured cytology, Tumor Cells, Cultured drug effects, Tumor Cells, Cultured metabolism, Dopamine physiology, Neurotoxins toxicity, Pyridines toxicity, Pyridinium Compounds toxicity

Abstract

This study was designed to investigate the toxicity of both MPTP and MPP+ using some simple cell systems, such as PC12 and C6 cultures, as models. Exposure of PC12 cells to 0.5 mM MPTP for 72 h resulted in a 50% cell loss with respect to the control cells, and clorgyline, a MAO-A inhibitor, antagonized this toxic effect. Higher concentrations of MPTP demonstrated only a weak cytostatic effect on C6 cells. Moreover, MPP+ showed a toxic effect which was 100 times more evident than MPTP toxicity in the PC12. We found a single, saturable class of [3H]MPP+ binding sites with a relatively high affinity both in PC12 and C6 cell lines. Moreover, the most susceptible cell line towards the toxic effects of both MPTP and MPP+, i.e. PC12, has the higher number of MPP+ binding sites. Our results suggest that MPTP can be toxic not only via MAO-B, but also via MAO-A activity and we propose PC12 as a model to study the intracellular mechanisms of MPTP and MPP+ toxicity.

Published

1988

44. On the inhibitory effect of 2-amino-4,6-dichloropyrimidine on growth of vaccinia virus.

Author

Marcialis MA, Flore O, Marongiu ME, Pompei R, Pani A, and Manconi PE

Subjects

DNA, Viral biosynthesis, Vaccinia virus growth & development, Vaccinia virus metabolism, Viral Proteins metabolism, Pyrimidines pharmacology, Vaccinia virus drug effects

Abstract

2-Amino-4,6-dichloropyrimidine prevents maturation of Vaccinia virus. Proteins synthesized in the presence of the drug are not assembled into virions.

Published

1979