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2. Expanding the knowledge around antitubercular 5-(2-aminothiazol-4-yl)isoxazole-3-carboxamides: Hit–to–lead optimization and release of a novel antitubercular chemotype via scaffold derivatization

Author

Girardini, Miriam, Ferlenghi, Francesca, Annunziato, Giannamaria, Degiacomi, Giulia, Papotti, Bianca, Marchi, Cinzia, Sammartino, José Camilla, Rasheed, Sari S., Contini, Anna, Pasca, Maria Rosalia, Vacondio, Federica, Evans, Joanna C., Dick, Thomas, Müller, Rolf, Costantino, Gabriele, and Pieroni, Marco

Published
2023
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4. Towards the sustainable discovery and development of new antibiotics

Author

Miethke, Marcus, Pieroni, Marco, Weber, Tilmann, Brönstrup, Mark, Hammann, Peter, Halby, Ludovic, Arimondo, Paola B., Glaser, Philippe, Aigle, Bertrand, Bode, Helge B., Moreira, Rui, Li, Yanyan, Luzhetskyy, Andriy, Medema, Marnix H., Pernodet, Jean-Luc, Stadler, Marc, Tormo, José Rubén, Genilloud, Olga, Truman, Andrew W., Weissman, Kira J., Takano, Eriko, Sabatini, Stefano, Stegmann, Evi, Brötz-Oesterhelt, Heike, Wohlleben, Wolfgang, Seemann, Myriam, Empting, Martin, Hirsch, Anna K. H., Loretz, Brigitta, Lehr, Claus-Michael, Titz, Alexander, Herrmann, Jennifer, Jaeger, Timo, Alt, Silke, Hesterkamp, Thomas, Winterhalter, Mathias, Schiefer, Andrea, Pfarr, Kenneth, Hoerauf, Achim, Graz, Heather, Graz, Michael, Lindvall, Mika, Ramurthy, Savithri, Karlén, Anders, van Dongen, Maarten, Petkovic, Hrvoje, Keller, Andreas, Peyrane, Frédéric, Donadio, Stefano, Fraisse, Laurent, Piddock, Laura J. V., Gilbert, Ian H., Moser, Heinz E., and Müller, Rolf

Published
2021
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11. Roadmap towards the sustainable discovery and development of new antibiotics

Author

Miethke, Marcus, Pieroni, Marco, Weber, Tilmann, Brönstrup, Mark, Hammann, Peter, Halby, Ludovic, Arimondo, Paola, GLASER, Philippe, Aigle, Bertrand, Bode, Helge, Moreira, Rui, Li, Yanyan, Luzhetskyy, Andriy, Medema, Marnix, Pernodet, Jean-Luc, Stadler, Marc, Tormo, José Rubén, Genilloud, Olga, Truman, Andrew, Weissman, Kira, Takano, Eriko, Sabatini, Stefano, Stegmann, Evi, Brötz-Oesterhelt, Heike, Wohlleben, Wolfgang, Seemann, Myriam, Empting, Martin, Hirsch, Anna, Loretz, Brigitta, Lehr, Claus-Michael, Titz, Alexander, Herrmann, Jennifer, Jaeger, Timo, Alt, Silke, Hesterkamp, Thomas, Winterhalter, Mathias, Schiefer, Andrea, Pfarr, Kenneth, Hoerauf, Achim, Graz, Heather, Graz, Michael, Lindvall, Mika, Ramurthy, Savithri, Karlén, Anders, van Dongen, Maarten, Petkovic, Hrvoje, Keller, Andreas, Peyrane, Frédéric, Donadio, Stefano, Fraisse, Laurent, Piddock, Laura, Gilbert, Ian, Moser, Heinz, Müller, Rolf, Molécules de Communication et Adaptation des Micro-organismes (MCAM), and Muséum national d'Histoire naturelle (MNHN)-Centre National de la Recherche Scientifique (CNRS)

Subjects
[CHIM]Chemical Sciences, ComputingMilieux_MISCELLANEOUS
Abstract

International audience

Published
2021

13. Inhibitors of O -Acetylserine Sulfhydrylase with a Cyclopropane-Carboxylic Acid Scaffold Are Effective Colistin Adjuvants in Gram Negative Bacteria.

Author

Annunziato, Giannamaria, Spadini, Costanza, Marchetti, Marialaura, Franko, Nina, Pavone, Marialaura, Iannarelli, Mattia, Bruno, Agostino, Pieroni, Marco, Bettati, Stefano, Cabassi, Clotilde Silvia, Campanini, Barbara, and Costantino, Gabriele

Subjects
GRAM-negative bacteria, COLISTIN, SALMONELLA enterica serovar typhimurium, SALMONELLA enterica, SALMONELLA enterica serovar Typhi, PATHOGENIC bacteria, KLEBSIELLA pneumoniae
Abstract

Antibacterial adjuvants are of great significance, since they allow one to downscale the therapeutic dose of conventional antibiotics and reduce the insurgence of antibacterial resistance. Herein, we report that O-acetylserine sulfhydrylase (OASS) inhibitors could be used as colistin adjuvants to treat infections caused by critical pathogens spreading worldwide, Escherichia coli, Salmonella enterica serovar Typhimurium, and Klebsiella pneumoniae. Starting from a hit compound endowed with a nanomolar dissociation constant, we have rationally designed and synthesized a series of derivatives to be tested against S. Typhimurium OASS isoenzymes, StOASS-A and StOASS-B. All acidic derivatives have shown good activities in the nanomolar range against both OASS isoforms in vitro. Minimal Inhibitory Concentrations (MICs) were then evaluated, as well as compounds' toxicity. The compounds endowed with good activity in vitro and low cytotoxicity have been challenged as a potential colistin adjuvant against pathogenic bacteria in vitro and the fractional inhibitory concentration (FIC) index has been calculated to define additive or synergistic effects. Finally, the target engagement inside the S. Typhimurium cells was confirmed by using a mutant strain in which the OASS enzymes were inactivated. Our results provide a robust proof of principle supporting OASS as a potential nonessential antibacterial target to develop a new class of adjuvants. [ABSTRACT FROM AUTHOR]

Published
2022
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16. Crystal structure of Aspergillus fumigatusAroH, an aromatic amino acid aminotransferase.

Author

Spizzichino, Sharon, Pampalone, Gioena, Dindo, Mirco, Bruno, Agostino, Romani, Luigina, Cutruzzolà, Francesca, Zelante, Teresa, Pieroni, Marco, Cellini, Barbara, and Giardina, Giorgio

Abstract

Aspergillus fumigatus is a saprophytic ubiquitous fungus whose spores can trigger reactions such as allergic bronchopulmonary aspergillosis or the fatal invasive pulmonary aspergillosis. To survive in the lungs, the fungus must adapt to a hypoxic and nutritionally restrictive environment, exploiting the limited availability of aromatic amino acids (AAAs) in the best possible way, as mammals do not synthesize them. A key enzyme for AAAs catabolism in A. fumigatus is AroH, a pyridoxal 5′‐phosphate‐dependent aromatic aminotransferase. AroH was recently shown to display a broad substrate specificity, accepting L‐kynurenine and α‐aminoadipate as amino donors besides AAAs. Given its pivotal role in the adaptability of the fungus to nutrient conditions, AroH represents a potential target for the development of innovative therapies against A. fumigatus‐related diseases. We have solved the crystal structure of Af‐AroH at 2.4 Å resolution and gained new insight into the dynamics of the enzyme's active site, which appears to be crucial for the design of inhibitors. The conformational plasticity of the active site pocket is probably linked to the wide substrate specificity of AroH. [ABSTRACT FROM AUTHOR]

Published
2022
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17. Challenging the drug-likeness dogma for new drug discovery in Tuberculosis

Author

Machado, Diana, Girardini, Miriam, Viveiros, Miguel, Pieroni, Marco, TB, HIV and opportunistic diseases and pathogens (THOP), Global Health and Tropical Medicine (GHTM), and Instituto de Higiene e Medicina Tropical (IHMT)

Subjects
Microbiology (medical), Infectious Diseases, SDG 3 - Good Health and Well-being, Proton motive force, Rule of five, Lipophilicity, Drug Discovery, Tuberculosis, Medicinal chemistry, Efflux inhibitors, Microbiology
Abstract

The emergence of multi- and extensively drug resistant tuberculosis worldwide poses a great threat to human health and highlight the need to discover and develop new, effective and inexpensive antituberculosis agents. High-throughput screening assays against well-validated drug targets and structure based drug design have been employed to discover new lead compounds. However, the great majority fail to demonstrate any antimycobacterial activity when tested against Mycobacterium tuberculosis in whole-cell screening assays. This is mainly due to some of the intrinsic properties of the bacilli, such as the extremely low permeability of its cell wall, slow growth, drug resistance, drug tolerance, and persistence. In this sense, understanding the pathways involved in M. tuberculosis drug tolerance, persistence, and pathogenesis, may reveal new approaches for drug development. Moreover, the need for compounds presenting a novel mode of action is of utmost importance due to the emergence of resistance not only to the currently used antituberculosis agents, but also to those in the pipeline. Cheminformatics studies have shown that drugs endowed with antituberculosis activity have the peculiarity of being more lipophilic than many other antibacterials, likely because this leads to improved cell penetration through the extremely waxy mycobacterial cell wall. Moreover, the interaction of the lipophilic moiety with the membrane alters its stability and functional integrity due to the disruption of the proton motive force, resulting in cell death. When a ligand-based medicinal chemistry campaign is ongoing, it is always difficult to predict whether a chemical modification or a functional group would be suitable for improving the activity. Nevertheless, in the "instruction manual" of medicinal chemists, certain functional groups or certain physicochemical characteristics (i.e., high lipophilicity) are considered red flags to look out for in order to safeguard drug-likeness and avoid attritions in the drug discovery process. In this review, we describe how antituberculosis compounds challenge established rules such as the Lipinski's "rule of five" and how medicinal chemistry for antituberculosis compounds must be thought beyond such dogmatic schemes. publishersversion published

Published
2018

19. Cycloserine enantiomers are reversible inhibitors of human alanine: glyoxylate aminotransferase: implications for Primary Hyperoxaluria type 1.

Author

Dindo, Mirco, Grottelli, Silvia, Annunziato, Giannamaria, Giardina, Giorgio, Pieroni, Marco, Pampalone, Gioena, Faccini, Andrea, Cutruzzolà, Francesca, Laurino, Paola, Costantino, Gabriele, and Cellini, Barbara

Subjects
ALANINE aminotransferase, MULTIDRUG-resistant tuberculosis, PROTEOLYSIS, ENANTIOMERS, CALCIUM oxalate, CYCLOSERINE, MOLECULAR chaperones
Abstract

Peroxisomal alanine:glyoxylate aminotransferase (AGT) is responsible for glyoxylate detoxification in human liver and utilizes pyridoxal 50-phosphate (PLP) as coenzyme. The deficit of AGT leads to Primary Hyperoxaluria Type I (PH1), a rare disease characterized by calcium oxalate stones deposition in the urinary tract as a consequence of glyoxylate accumulation. Most missense mutations cause AGT misfolding, as in the case of the G41R, which induces aggregation and proteolytic degradation. We have investigated the interaction of wild-type AGT and the pathogenic G41R variant with D-cycloserine (DCS, commercialized as Seromycin), a natural product used as a second-line treatment of multidrug-resistant tuberculosis, and its synthetic enantiomer L-cycloserine (LCS). In contrast with evidences previously reported on other PLP-enzymes, both ligands are AGT reversible inhibitors showing inhibition constants in the micromolar range. While LCS undergoes half-transamination generating a ketimine intermediate and behaves as a classical competitive inhibitor, DCS displays a time-dependent binding mainly generating an oxime intermediate. Using a mammalian cellular model, we found that DCS, but not LCS, is able to promote the correct folding of the G41R variant, as revealed by its increased specific activity and expression as a soluble protein. This effect also translates into an increased glyoxylate detoxification ability of cells expressing the variant upon treatment with DCS. Overall, our findings establish that DCS could play a role as pharmacological chaperone, thus suggesting a new line of intervention against PH1 based on a drug repositioning approach. To a widest extent, this strategy could be applied to other diseasecausing mutations leading to AGT misfolding. [ABSTRACT FROM AUTHOR]

Published
2019
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20. Refining the structure−activity relationships of 2-phenylcyclopropane carboxylic acids as inhibitors of O-acetylserine sulfhydrylase isoforms.

Author

Magalhães, Joana, Franko, Nina, Annunziato, Giannamaria, Pieroni, Marco, Benoni, Roberto, Nikitjuka, Anna, Mozzarelli, Andrea, Bettati, Stefano, Karawajczyk, Anna, Jirgensons, Aigars, Campanini, Barbara, and Costantino, Gabriele

Subjects
STRUCTURE-activity relationships, CARBOXYLIC acids, SALMONELLA enterica serovar typhimurium, MULTIDRUG resistance in bacteria, PHARMACEUTICAL chemistry
Abstract

The lack of efficacy of current antibacterials to treat multidrug resistant bacteria poses a life-threatening alarm. In order to develop enhancers of the antibacterial activity, we carried out a medicinal chemistry campaign aiming to develop inhibitors of enzymes that synthesise cysteine and belong to the reductive sulphur assimilation pathway, absent in mammals. Previous studies have provided a novel series of inhibitors for O-acetylsulfhydrylase – a key enzyme involved in cysteine biosynthesis. Despite displaying nanomolar affinity, the most active representative of the series was not able to interfere with bacterial growth, likely due to poor permeability. Therefore, we rationally modified the structure of the hit compound with the aim of promoting their passage through the outer cell membrane porins. The new series was evaluated on the recombinant enzyme from Salmonella enterica serovar Typhimurium, with several compounds able to keep nanomolar binding affinity despite the extent of chemical manipulation. [ABSTRACT FROM AUTHOR]

Published
2019
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21. Discovering a new class of antifungal agents that selectively inhibits microbial carbonic anhydrases.

Author

Annunziato, Giannamaria, Giovati, Laura, Angeli, Andrea, Pavone, Marialaura, Del Prete, Sonia, Pieroni, Marco, Capasso, Clemente, Bruno, Agostino, Conti, Stefania, Magliani, Walter, Supuran, Claudiu T., and Costantino, Gabriele

Subjects
ANTIFUNGAL agents, CARBONIC anhydrase, CRYPTOCOCCUS neoformans, ANTI-infective agents, DRUG development, DRUG design
Abstract

Infections caused by pathogens resistant to the available antimicrobial treatments represent nowadays a threat to global public health. Recently, it has been demonstrated that carbonic anhydrases (CAs) are essential for the growth of many pathogens and their inhibition leads to growth defects. Principal drawbacks in using CA inhibitors (CAIs) as antimicrobial agents are the side effects due to the lack of selectivity toward human CA isoforms. Herein we report a new class of CAIs, which preferentially interacts with microbial CA active sites over the human ones. The mechanism of action of these inhibitors was investigated against an important fungal pathogen, Cryptococcus neoformans, revealing that they are also able to inhibit CA in microbial cells growing in vitro. At our best knowledge, this is the first report on newly designed synthetic compounds selectively targeting β-CAs and provides a proof of concept of microbial CAs suitability as an antimicrobial drug target. [ABSTRACT FROM AUTHOR]

Published
2018
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22. Discovery of novel fragments inhibiting O-acetylserine sulphhydrylase by combining scaffold hopping and ligand-based drug design.

Author

Magalhães, Joana, Franko, Nina, Annunziato, Giannamaria, Welch, Martin, Dolan, Stephen K., Bruno, Agostino, Mozzarelli, Andrea, Armao, Stefano, Jirgensons, Aigars, Pieroni, Marco, Costantino, Gabriele, and Campanini, Barbara

Subjects
DRUG development, CYSTEINE synthase, LIGANDS (Biochemistry), DRUG design, PHARMACOLOGY, VIRULENCE of bacteria
Abstract

Several bacteria rely on the reductive sulphur assimilation pathway, absent in mammals, to synthesise cysteine. Reduction of virulence and decrease in antibiotic resistance have already been associated with mutations on the genes that codify cysteine biosynthetic enzymes. Therefore, inhibition of cysteine biosynthesis has emerged as a promising strategy to find new potential agents for the treatment of bacterial infection. Following our previous efforts to explore OASS inhibition and to expand and diversify our library, a scaffold hopping approach was carried out, with the aim of identifying a novel fragment for further development. This novel chemical tool, endowed with favourable pharmacological characteristics, was successfully developed, and a preliminary Structure-Activity Relationship investigation was carried out. [ABSTRACT FROM AUTHOR]

Published
2018
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25. Efflux Activity Differentially Modulates the Levels of Isoniazid and Rifampicin Resistance among Multidrug Resistant and Monoresistant Mycobacterium tuberculosis Strains.

Author

Machado, Diana, Perdigão, João, Portugal, Isabel, Pieroni, Marco, Silva, Pedro A., Couto, Isabel, and Viveiros, Miguel

Subjects
MULTIDRUG resistance in bacteria, EFFLUX (Microbiology), ISONIAZID, RIFAMPIN, BACTERIAL growth, MYCOBACTERIUM tuberculosis
Abstract

With the growing body of knowledge on the contribution of efflux activity to Mycobacterium tuberculosis drug resistance, increased attention has been given to the use of efflux inhibitors as adjuvants of tuberculosis therapy. Here, we investigated how efflux activity modulates the levels of efflux between monoresistant and multi- and extensively drug resistant (M/XDR) M. tuberculosis clinical isolates. The strains were characterized by antibiotic susceptibility testing in the presence/absence of efflux inhibitors, molecular typing, and genetic analysis of drug-resistance-associated genes. Efflux activity was quantified by real-time fluorometry. The results demonstrated that all the M. tuberculosis clinical strains, susceptible or resistant, presented a faster, rapid, and non-specific efflux-mediated short-term response to drugs. The synergism assays demonstrated that the efflux inhibitors were more effective in reducing the resistance levels in the M/XDR strains than in the monoresistant strains. This indicated that M/XDR strains presented a more prolonged response to drugs mediated by efflux compared to the monoresistant strains, but both maintain it as a long-term stress response. This work shows that efflux activity modulates the levels of drug resistance between monoresistant and M/XDR M. tuberculosis clinical strains, allowing the bacteria to survive in the presence of noxious compounds. [ABSTRACT FROM AUTHOR]

Published
2018
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30. Accepting the Invitation to Open Innovation in Malaria Drug Discovery: Synthesis, Biological Evaluation, and Investigation on the Structure-Activity Relationships of Benzo[b]thiophene-2-carboxamides as Antimalarial Agents.

Author

Pieroni, Marco, Azzali, Elisa, Basilico, Nicoletta, Parapini, Silvia, Zolkiewski, Michal, Beato, Claudia, Annunziato, Giannamaria, Bruno, Agostino, Vacondio, Federica, and Costantino, Gabriele

Subjects
*MALARIA treatment, *DRUG development, *STRUCTURE-activity relationship in pharmacology, *ANTIMALARIALS, *COMBINATION drug therapy
Abstract

Malaria eradication is a global health priority, but current therapies are not always suitable for providing a radical cure. Artemisinin has paved the way for the current malaria treatment, the so-called Artemisinin-based Combination Therapy (ACT). However, with the detection of resistance to ACT, innovative compounds active against multiple parasite species and at multiple life stages are needed. GlaxoSmithKline has recently disclosed the results of a phenotypic screening of an internal library, publishing a collection of 400 antimalarial chemotypes, termed the "Malaria Box". After analysis of the data set, we have carried out a medicinal chemistry campaign in order to define the structure-activity relationships for one of the released compounds, which embodies a benzothiophene-2-carboxamide core. Thirty-five compounds were prepared, and a description of the structural features responsible for the in vitro activity against different strains of P. falciparum, the toxicity, and the metabolic stability is herein reported. [ABSTRACT FROM AUTHOR]

Published
2017
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31. Discovery of Multitarget Agents Active as Broad-Spectrum Antivirals and Correctors of Cystic Fibrosis Transmembrane Conductance Regulator for Associated Pulmonary Diseases.

Author

Tassini, Sabrina, Liang Sun, Lanko, Kristina, Crespan, Emmanuele, Langron, Emily, Falchi, Federico, Kissova, Miroslava, Armijos-Rivera, Jorge I., Delang, Leen, Mirabelli, Carmen, Neyts, Johan, Pieroni, Marco, Cavalli, Andrea, Costantino, Gabriele, Maga, Giovanni, Vergani, Paola, Leyssen, Pieter, and Radi, Marco

Published
2017
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32. Cyclopropane-1,2-dicarboxylic acids as new tools for the biophysical investigation of O -acetylserine sulfhydrylases by fluorimetric methods and saturation transfer difference (STD) NMR.

Author

Annunziato, Giannamaria, Pieroni, Marco, Benoni, Roberto, Campanini, Barbara, Pertinhez, Thelma A., Pecchini, Chiara, Bruno, Agostino, Magalhães, Joana, Bettati, Stefano, Franko, Nina, Mozzarelli, Andrea, and Costantino, Gabriele

Subjects
*CYCLOPROPANE, *DICARBOXYLIC acids, *PHYSICAL biochemistry, *NUCLEAR magnetic resonance, *DRUG resistance
Abstract

Cysteine is a building block for many biomolecules that are crucial for living organisms.O-Acetylserine sulfhydrylase (OASS), present in bacteria and plants but absent in mammals, catalyzes the last step of cysteine biosynthesis. This enzyme has been deeply investigated because, beside the biosynthesis of cysteine, it exerts a series of “moonlighting” activities in bacteria. We have previously reported a series of molecules capable of inhibiting Salmonella typhimurium (S. typhymurium) OASS isoforms at nanomolar concentrations, using a combination of computational and spectroscopic approaches. The cyclopropane-1,2-dicarboxylic acids presented herein provide further insights into the binding mode of small molecules to OASS enzymes. Saturation transfer difference NMR (STD-NMR) was used to characterize the molecule/enzyme interactions for both OASS-A and B. Most of the compounds induce a several fold increase in fluorescence emission of the pyridoxal 5′-phosphate (PLP) coenzyme upon binding to either OASS-A or OASS-B, making these compounds excellent tools for the development of competition-binding experiments. [ABSTRACT FROM PUBLISHER]

Published
2016
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34. An Experimental Model for the Rapid Screening of Compounds with Potential Use Against Mycobacteria.

Author

Costa, Sofia Santos, Lopes, Elizeth, Azzali, Elisa, Machado, Diana, Coelho, Tatiane, da Silva, Pedro Eduardo Almeida, Viveiros, Miguel, Pieroni, Marco, and Couto, Isabel

Subjects
BIOACTIVE compounds, MYCOBACTERIA, ANTIBACTERIAL agents
Abstract

Infections caused by Mycobacterium tuberculosis and other mycobacteria are major challenges for global public health. Particularly worrisome are infections caused by multidrug-resistant bacteria, which are increasingly difficult to treat because of the loss of efficacy of the current antibacterial agents, a problem that continues to escalate worldwide. There has been a limited interest and investment on the development of new antibacterial agents in the past decades. This has led to the current situation, in which there is an urgent demand for innovative therapeutic alternatives to fight infections caused by multidrug-resistant pathogens, such as multidrug-resistant tuberculosis. The identification of compounds that can act as adjuvants in antimycobacterial therapeutic regimens is an appealing strategy to restore the efficacy lost by some of the antibiotics currently used and shorten the duration of the therapeutic regimen. In this work, by setting Mycobacterium smegmatis as a model organism, we have developed a methodological strategy to identify, in a fast and simple approach, compounds with antimycobacterial activity or with potential adjuvant properties, by either inhibition of efflux or other unrelated mechanisms. Such an approach may increase the rate of identification of promising molecules, to be further explored in pathogenic models for their potential use either as antimicrobials or as adjuvants, in combination with available therapeutic regimens for the treatment of mycobacterial infections. This method allowed us to identify a new molecule that shows promising activity as an efflux inhibitor in M. smegmatis. [ABSTRACT FROM AUTHOR]

Published
2016
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36. Cyclopropane derivatives as potential human serine racemase inhibitors: unveiling novel insights into a difficult target.

Author

Beato, Claudia, Pecchini, Chiara, Cocconcelli, Chiara, Campanini, Barbara, Marchetti, Marialaura, Pieroni, Marco, Mozzarelli, Andrea, and Costantino, Gabriele

Subjects
CYCLOPROPANE, ENZYME inhibitors, RACEMASES, SERINE, METHYL aspartate receptors, NEURODEGENERATION, MOLECULAR docking
Abstract

d-Serine is the co-agonist of NMDA receptors and binds to the so-called glycine site.d-Serine is synthesized by human serine racemase (SR). Over activation of NMDA receptors is involved in many neurodegenerative diseases and, therefore, the inhibition of SR might represent a novel strategy for the treatment of these pathologies. SR is a very difficult target, with only few compounds so far identified exhibiting weak inhibitory activity. This study was aimed at the identification of novel SR inhibitor by mimicking malonic acid, the best-known SR inhibitor, with a cyclopropane scaffold. We developed, synthesized, and tested a series of cyclopropane dicarboxylic acid derivatives, complementing the synthetic effort with molecular docking. We identified few compounds that bind SR in high micromolar range with a lack of significant correlation between experimental and predicted binding affinities. The thorough analysis of the results can be exploited for the development of more potent SR inhibitors. [ABSTRACT FROM AUTHOR]

Published
2016
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37. Rational Design, Synthesis, and Preliminary Structure-Activity Relationships of α-Substituted-2-Phenylcyclopropane Carboxylic Acids as Inhibitors of Salmonella typhimurium O-Acetylserine Sulfhydrylase.

Author

Pieroni, Marco, Annunziato, Giannamaria, Beato, Claudia, Wouters, Randy, Benoni, Roberto, Campanini, Barbara, Pertinhez, Thelma A., Bettati, Stefano, Mozzarelli, Andrea, and Costantino, Gabriele

Subjects
*DRUG design, *DRUG synthesis, *CYCLOPROPANE, *ENZYME inhibitors, *CARBOXYLIC acids, *STRUCTURE-activity relationship in pharmacology, *SALMONELLA typhimurium, *SERINE, *THERAPEUTICS
Abstract

Cysteine is a building block for several biomolecules that are crucial for living organisms. The last step of cysteine biosynthesis is catalyzed by O-acetylserine sulfydrylase (OASS), a highly conserved pyridoxal 5'-phosphate (PLP)-dependent enzyme, present in different isoforms in bacteria, plants, and nematodes, but absent in mammals. Beside the biosynthesis of cysteine, OASS exerts a series of "moonlighting" activities in bacteria, such as transcriptional regulation, contact-dependent growth inhibition, swarming motility, and induction of antibiotic resistance. Therefore, the discovery of molecules capable of inhibiting OASS would be a valuable tool to unravel how this protein affects the physiology of unicellular organisms. As a continuation of our efforts toward the synthesis of OASS inhibitors, in this work we have used a combination of computational and spectroscopic approaches to rationally design, synthesize, and test a series of substituted 2-phenylcyclopropane carboxylic acids that bind to the two S. typhymurium OASS isoforms at nanomolar concentrations. [ABSTRACT FROM AUTHOR]

Published
2016
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38. PreliminaryStructure–Activity Relationships and Biological Evaluationof Novel Antitubercular Indolecarboxamide Derivatives Against Drug-Susceptibleand Drug-Resistant Mycobacterium tuberculosisStrains.

Author

Onajole, Oluseye K., Pieroni, Marco, Tipparaju, Suresh K., Lun, Shichun, Stec, Jozef, Chen, Gang, Gunosewoyo, Hendra, Guo, Haidan, Ammerman, Nicole C., Bishai, William R., and Kozikowski, Alan P.

Subjects
*INDOLE compounds, *CARBOXAMIDES, *ANTITUBERCULAR agents, *MICROBIAL sensitivity tests, *DRUG resistance in bacteria, *MYCOBACTERIUM tuberculosis, *TUBERCULOSIS treatment, *THERAPEUTICS
Abstract

Tuberculosis(TB) remains one of the leading causes of mortality and morbidityworldwide, with approximately one-third of the world’s populationinfected with latent TB. This is further aggravated by HIV coinfectionand the emergence of multidrug- and extensively drug-resistant (MDRand XDR, respectively) TB; hence the quest for highly effective antituberculardrugs with novel modes of action is imperative. We report herein thediscovery of an indole-2-carboxamide analogue, 3, asa highly potent antitubercular agent, and the subsequent chemicalmodifications aimed at establishing a preliminary body of structure–activityrelationships (SARs). These efforts led to the identification of threemolecules (12–14) possessing an exceptionalactivity in the low nanomolar range against actively replicating Mycobacterium tuberculosis, with minimum inhibitoryconcentration (MIC) values lower than those of the most prominentantitubercular agents currently in use. These compounds were alsodevoid of apparent toxicity to Vero cells. Importantly, compound 12was found to be active against the tested XDR-TB strainsand orally active in the serum inhibition titration assay. [ABSTRACT FROM AUTHOR]

Published
2013
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42. From 6-Aminoquinolone Antibacterials to 6-Amino-7-thiopyranopyridinylquinolone Ethyl Esters as Inhibitors of Staphylococcus aureusMultidrug Efflux Pumps.

Author

Pieroni, Marco, Dimovska, Mirjana, Brincat, Jean Pierre, Sabatini, Stefano, Carosati, Emanuele, Massari, Serena, Kaatz, Glenn W., and Fravolini, Arnaldo

Subjects
*QUINOLONE antibacterial agents, *ESTERS, *STAPHYLOCOCCUS aureus, *MULTIDRUG resistance, *PYRIDINE, *ORGANIC synthesis, *HETEROCYCLIC compounds, *ANTI-infective agents, *THERAPEUTICS
Abstract

The thiopyranopyridine moiety was synthesized as a new heterocyclic base to be inserted at the C-7 position of selected quinolone nuclei followed by a determination of antibacterial activity against strains of Staphylococcus aureus. Selected thiopyranopyridinylquinolones showed significant antimicrobial activity, including strains having mutations in gyrAand grlAas well as other strains overexpressing the NorA multidrug (MDR) efflux pump. Most derivatives did not appear to be NorA substrates. The effect of the thiopyranopyridinyl substituent on making these quinolones poor substrates for NorA was investigated further. Several quinolone ester intermediates, devoid of any intrinsic antibacterial activity, were tested for their abilities to inhibit the activities of NorA (MFS family) and MepA (MATE family) S. aureusMDR efflux pumps. Selected quinolone esters were capable of inhibiting both MDR pumps more efficiently than the reference compound reserpine. Moreover, they also were able to restore, and even enhance, the activity of ciprofloxacin toward some genetically modified resistant S. aureusstrains. [ABSTRACT FROM AUTHOR]

Published
2010
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43. A Competitive O- Acetylserine Sulfhydrylase Inhibitor Modulates the Formation of Cysteine Synthase Complex.

Author

Marchetti, Marialaura, De Angelis, Francesco Saverio, Annunziato, Giannamaria, Costantino, Gabriele, Pieroni, Marco, Ronda, Luca, Mozzarelli, Andrea, Campanini, Barbara, Cannistraro, Salvatore, Bizzarri, Anna Rita, and Bettati, Stefano

Subjects
CYSTEINE, ESSENTIAL amino acids, SURFACE plasmon resonance, BIOMOLECULES, SALMONELLA typhimurium, GLUTAMINE synthetase
Abstract

Cysteine is the main precursor of sulfur-containing biological molecules in bacteria and contributes to the control of the cell redox state. Hence, this amino acid plays an essential role in microbial survival and pathogenicity and the reductive sulfate assimilation pathway is considered a promising target for the development of new antibacterials. Serine acetyltransferase (SAT) and O-acetylserine sulfhydrylase (OASS-A), the enzymes catalyzing the last two steps of cysteine biosynthesis, engage in the formation of the cysteine synthase (CS) complex. The interaction between SAT and OASS-A finely tunes cysteine homeostasis, and the development of inhibitors targeting either protein–protein interaction or the single enzymes represents an attractive strategy to undermine bacterial viability. Given the peculiar mode of interaction between SAT and OASS-A, which exploits the insertion of SAT C-terminal sequence into OASS-A active site, we tested whether a recently developed competitive inhibitor of OASS-A exhibited any effect on the CS stability. Through surface plasmon resonance spectroscopy, we (i) determined the equilibrium constant for the Salmonella Typhimurium CS complex formation and (ii) demonstrated that the inhibitor targeting OASS-A active site affects CS complex formation. For comparison, the Escherichia coli CS complex was also investigated, with the aim of testing the potential broad-spectrum activity of the candidate antimicrobial compound. [ABSTRACT FROM AUTHOR]

Published
2021
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44. Discovery of Substituted (2-Aminooxazol-4-yl)Isoxazole-3-carboxylic Acids as Inhibitors of Bacterial Serine Acetyltransferase in the Quest for Novel Potential Antibacterial Adjuvants.

Author

Magalhães, Joana, Franko, Nina, Raboni, Samanta, Annunziato, Giannamaria, Tammela, Päivi, Bruno, Agostino, Bettati, Stefano, Armao, Stefano, Spadini, Costanza, Cabassi, Clotilde Silvia, Mozzarelli, Andrea, Pieroni, Marco, Campanini, Barbara, Costantino, Gabriele, and Meegan, Mary J.

Subjects
ACETYLTRANSFERASES, PHARMACEUTICAL chemistry, SERINE, CYSTEINE, DRUG resistance in microorganisms
Abstract

Many bacteria and actinomycetales use L-cysteine biosynthesis to increase their tolerance to antibacterial treatment and establish a long-lasting infection. In turn, this might lead to the onset of antimicrobial resistance that currently represents one of the most menacing threats to public health worldwide. The biosynthetic machinery required to synthesise L-cysteine is absent in mammals; therefore, its exploitation as a drug target is particularly promising. In this article, we report a series of inhibitors of Salmonella thyphimurium serine acetyltransferase (SAT), the enzyme that catalyzes the rate-limiting step of L-cysteine biosynthesis. The development of such inhibitors started with the virtual screening of an in-house library of compounds that led to the selection of seven structurally unrelated hit derivatives. A set of molecules structurally related to hit compound 5, coming either from the original library or from medicinal chemistry efforts, were tested to determine a preliminary structure–activity relationship and, especially, to improve the inhibitory potency of the derivatives, that was indeed ameliorated by several folds compared to hit compound 5 Despite these progresses, at this stage, the most promising compound failed to interfere with bacterial growth when tested on a Gram-negative model organism, anticipating the need for further research efforts. [ABSTRACT FROM AUTHOR]

Published
2021
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45. Aspergillus fumigatus tryptophan metabolic route differently affects host immunity.

Author

Zelante, Teresa, Choera, Tsokyi, Beauvais, Anne, Fallarino, Francesca, Paolicelli, Giuseppe, Pieraccini, Giuseppe, Pieroni, Marco, Galosi, Claudia, Beato, Claudia, De Luca, Antonella, Boscaro, Francesca, Romoli, Riccardo, Liu, Xin, Warris, Adilia, Verweij, Paul E., Ballard, Eloise, Borghi, Monica, Pariano, Marilena, Costantino, Gabriele, and Calvitti, Mario

Abstract

Indoleamine 2,3-dioxygenases (IDOs) degrade l -tryptophan to kynurenines and drive the de novo synthesis of nicotinamide adenine dinucleotide. Unsurprisingly, various invertebrates, vertebrates, and even fungi produce IDO. In mammals, IDO1 also serves as a homeostatic regulator, modulating immune response to infection via local tryptophan deprivation, active catabolite production, and non-enzymatic cell signaling. Whether fungal Idos have pleiotropic functions that impact on host-fungal physiology is unclear. Here, we show that Aspergillus fumigatus possesses three ido genes that are expressed under conditions of hypoxia or tryptophan abundance. Loss of these genes results in increased fungal pathogenicity and inflammation in a mouse model of aspergillosis, driven by an alternative tryptophan degradation pathway to indole derivatives and the host aryl hydrocarbon receptor. Fungal tryptophan metabolic pathways thus cooperate with the host xenobiotic response to shape host-microbe interactions in local tissue microenvironments. • Aspergillus Idos contribute to de novo NAD+ biosynthesis and fungal growth • In conditions of tryptophan abundance, Aspergillus releases indole derivatives via Aro • Activation of lung AhR enhances harmful lung inflammation during fungal infection • Pharmacological induction of Ido in Aspergillus improves infection outcome Mammalians use the kynurenine pathway for tryptophan degradation inducing tolerogenic immune responses. Zelante et al. report that similarly, the fungus Aspergillus fumigatus uses the kynurenine pathway. Pathogenic immune response occurs when the fungus catabolizes tryptophan via the indolepyruvate pathway, which targets host AhR. Administration of Ido inducers ameliorates infection outcome. [ABSTRACT FROM AUTHOR]

Published
2021
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46. Sodium Hyaluronate Nanocomposite Respirable Microparticles to Tackle Antibiotic Resistance with Potential Application in Treatment of Mycobacterial Pulmonary Infections.

Author

Rossi, Irene, Buttini, Francesca, Sonvico, Fabio, Affaticati, Filippo, Martinelli, Francesco, Annunziato, Giannamaria, Machado, Diana, Viveiros, Miguel, Pieroni, Marco, and Bettini, Ruggero

Subjects
MYCOBACTERIAL diseases, LUNG infections, THERAPEUTICS, RESPIRATORY infections, ALVEOLAR macrophages, SPRAYING & dusting in agriculture, TUBERCULOSIS in cattle
Abstract

Tuberculosis resistant cases have been estimated to grow every year. Besides Mycobacterium tuberculosis, other mycobacterial species are responsible for an increasing number of difficult-to-treat infections. To increase efficacy of pulmonary treatment of mycobacterial infections an inhalable antibiotic powder targeting infected alveolar macrophages (AMs) and including an efflux pump inhibitor was developed. Low molecular weight sodium hyaluronate sub-micron particles were efficiently loaded with rifampicin, isoniazid and verapamil, and transformed in highly respirable microparticles (mean volume diameter: 1 μm) by spray drying. These particles were able to regenerate their original size upon contact with aqueous environment with mechanical stirring or sonication. The in vitro drugs release profile from the powder was characterized by a slow release rate, favorable to maintain a high drug level inside AMs. In vitro antimicrobial activity and ex vivo macrophage infection assays employing susceptible and drug resistant strains were carried out. No significant differences were observed when the powder, which did not compromise the AMs viability after a five-day exposure, was compared to the same formulation without verapamil. However, both preparations achieved more than 80% reduction in bacterial viability irrespective of the drug resistance profile. This approach can be considered appropriate to treat mycobacterial respiratory infections, regardless the level of drug resistance. [ABSTRACT FROM AUTHOR]

Published
2019
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49. Investigational Studies on a Hit Compound Cyclopropane-Carboxylic Acid Derivative Targeting O -Acetylserine Sulfhydrylase as a Colistin Adjuvant.

Author

Annunziato G, Spadini C, Franko N, Storici P, Demitri N, Pieroni M, Flisi S, Rosati L, Iannarelli M, Marchetti M, Magalhaes J, Bettati S, Mozzarelli A, Cabassi CS, Campanini B, and Costantino G

Subjects
Animals, Carboxylic Acids, Colistin pharmacology, Cyclopropanes, Sheep, Staphylococcus, Cysteine Synthase, Methicillin-Resistant Staphylococcus aureus
Abstract

Antibacterial adjuvants are of great significance, since they allow the therapeutic dose of conventional antibiotics to be lowered and reduce the insurgence of antibiotic resistance. Herein, we report that an O- acetylserine sulfhydrylase (OASS) inhibitor can be used as a colistin adjuvant to treat infections caused by Gram-positive and Gram-negative pathogens. A compound that binds OASS with a nM dissociation constant was tested as an adjuvant of colistin against six critical pathogens responsible for infections spreading worldwide, Escherichia coli , Salmonella enterica serovar Typhimurium, Klebisiella pneumoniae , Staphylococcus aureus , methicillin-resistant Staphylococcus aureus , and Staphylococcus pseudintermedius . The compound showed promising synergistic or additive activities against all of them. Knockout experiments confirmed the intracellular target engagement supporting the proposed mechanism of action. Moreover, compound toxicity was evaluated by means of its hemolytic activity against sheep defibrinated blood cells, showing a good safety profile. The 3D structure of the compound in complex with OASS was determined at 1.2 Å resolution by macromolecular crystallography, providing for the first time structural insights about the nature of the interaction between the enzyme and this class of competitive inhibitors. Our results provide a robust proof of principle supporting OASS as a potential nonessential antibacterial target to develop a new class of adjuvants and the structural basis for further structure-activity relationship studies.

Published
2021
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50. Nitric oxide-releasing cyclodextrins as biodegradable antibacterial scaffolds: a patent evaluation of US2019343869(A1).

Author

Pieroni M

Subjects
A549 Cells, Anti-Bacterial Agents pharmacology, Antineoplastic Agents pharmacology, Biofilms drug effects, Drug Delivery Systems, Drug Resistance, Bacterial, Humans, Neoplasms drug therapy, Neoplasms pathology, Patents as Topic, Anti-Bacterial Agents administration & dosage, Antineoplastic Agents administration & dosage, Cyclodextrins chemistry, Nitric Oxide metabolism
Abstract

Introduction: Antimicrobial resistance is one of the major scourges for health care worldwide; therefore, novel investigational approaches are needed to potentiate and preserve the current antibacterial arsenal. Cyclodextrins are known to improve the formulability of several different therapeutic agents. When functionalized with nitric oxide (NO) releasing groups, and suitably loaded with an antibacterial or antitumoral agents, they can exert additive activity, especially toward certain bacterial strains and cell cancer lines., Areas Covered: US2019343869 describes NO-releasing cyclodextrins, a method for their synthesis, a composition that is based on them, and their application as anticancer or antibacterial agents, especially toward planktonic P. aeruginosa and the biofilm resulting from infection. Anticancer activity is measured against A549 cells. The amount of NO released is in the range of 0.5 μmol to 2.5 μmol per milligram of functionalized cyclodextrin with a half-life for NO release in a range of between about 0.7-4.2 hours., Expert Opinion: The results support the use of NO-releasing cyclodextrins as a matrix for the delivery of antibacterial and anticancer drugs in a suitable formulation. However, antibacterial activity seems to be weak, and more focused studies are needed.

Published
2020
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