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6. Altered mitochondrial function in cells carrying a premutation or unmethylated full mutation of the FMR1 gene

Author

Nobile, Veronica, Palumbo, Federica, Lanni, Stella, Ghisio, Valentina, Vitali, Alberto, Castagnola, Massimo, Marzano, Valeria, Maulucci, Giuseppe, De Angelis, Claudio, De Spirito, Marco, Pacini, Laura, D’Andrea, Laura, Ragno, Rino, Stazi, Giulia, Valente, Sergio, Mai, Antonello, Chiurazzi, Pietro, Genuardi, Maurizio, Neri, Giovanni, and Tabolacci, Elisabetta

Published
2020
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11. Cryptides: latent peptides everywhere.

Author

Iavarone, Federica, Desiderio, Claudia, Vitali, Alberto, Messana, Irene, Martelli, Claudia, Castagnola, Massimo, Cabras, Tiziana, Iavarone Federica (ORCID:0000-0002-2074-5531), Desiderio Claudia, Vitali Alberto, Messana Irene (ORCID:0000-0002-1436-6105), Martelli Claudia, Castagnola Massimo (ORCID:0000-0002-0959-7259), Cabras Tiziana., Iavarone, Federica, Desiderio, Claudia, Vitali, Alberto, Messana, Irene, Martelli, Claudia, Castagnola, Massimo, Cabras, Tiziana, Iavarone Federica (ORCID:0000-0002-2074-5531), Desiderio Claudia, Vitali Alberto, Messana Irene (ORCID:0000-0002-1436-6105), Martelli Claudia, Castagnola Massimo (ORCID:0000-0002-0959-7259), and Cabras Tiziana.

Abstract

Proteomic surveys with top-down platforms are today revealing thousands of naturally occurring fragments of bigger proteins. Some of them have not functional meaning because they derive from pathways responsible for protein degradation, but many have specific functions, often completely different from that one of the parent proteins. These peptides encrypted in the protein sequence are nowadays called cryptides. They are frequent in the animal and plant kingdoms and represent a new interesting -omic field of investigation. To point out how much widespread is their presence, we describe here the most studied cryptides from very common sources such as serum albumin, immunoglobulins, hemoglobin, and from saliva and milk proteins. Given its vastness, it is unfeasible to cover the topic exhaustively, therefore only several selected examples of cryptides from other sources are thereafter reported. Demanding is the development of new -omic platforms for the functional screening of new cryptides, which could provide suggestion for peptides and peptido-mimetics with variegate fields of application.

Published
2018

12. Potent in vitro activity of citrus aurantium essential oil and vitis vinifera hydrolate against gut yeast isolates from irritable bowel syndrome patients—the right mix for potential therapeutic use

Author

Di Vito, Maura, Grazia Bellardi, M., Sanguinetti, Maurizio, Mondello, F., Girolamo, A., Barbanti, L., Garzoli, S., Sabatino, M., Ragno, R., Vitali, Alberto, Palucci, Ivana, Posteraro, Brunella, Gasbarrini, Antonio, Maria Prati, G., Aragona, G., Mattarelli, P., Bugli, Francesca, Di Vito M. (ORCID:0000-0002-2991-0855), Sanguinetti M. (ORCID:0000-0002-9780-7059), Vitali A., Palucci I., Posteraro B. (ORCID:0000-0002-1663-7546), Gasbarrini A. (ORCID:0000-0002-7278-4823), Bugli F. (ORCID:0000-0001-9038-3233), Di Vito, Maura, Grazia Bellardi, M., Sanguinetti, Maurizio, Mondello, F., Girolamo, A., Barbanti, L., Garzoli, S., Sabatino, M., Ragno, R., Vitali, Alberto, Palucci, Ivana, Posteraro, Brunella, Gasbarrini, Antonio, Maria Prati, G., Aragona, G., Mattarelli, P., Bugli, Francesca, Di Vito M. (ORCID:0000-0002-2991-0855), Sanguinetti M. (ORCID:0000-0002-9780-7059), Vitali A., Palucci I., Posteraro B. (ORCID:0000-0002-1663-7546), Gasbarrini A. (ORCID:0000-0002-7278-4823), and Bugli F. (ORCID:0000-0001-9038-3233)

Abstract

Background: Irritable bowel syndrome (IBS) is a functional disorder without any pathological alteration, in which the alterations of the Candida/Saccharomyces ratio of the gut microbiota, the balance of pro and anti-inflammatory cytokines and the brain-gut-microbiome axis are important for the development and progression of IBS. The aim of the study was to identify natural products, including essential oils or hydrolates, which were contextually harmless for the gut beneficial strains (e.g. Saccharomyces spp.) but inhibitory for the pathogenic ones (Candida spp.). Methods: The effectiveness of 6 essential oils and 2 hydrolates was evaluated using microbiological tests, carried out on 50 clinical isolates (Candida, Saccharomyces and Galattomyces species) and 9 probiotic strains (Saccharomyces cerevisiae, Lactobacillus species, Akkermansia muciniphila and Faecalibacterium prausnitzii) and immunological and antioxidant assays. Results: The study led to a mixture based on a 1/100 ratio of Citrus aurantium var. amara essential oil/Vitis vinifera cv Italia hydrolate able to contextually reduce, in a concentration-dependent manner, the ability of Candida species to form hyphal filaments and have an interesting immunomodulatory and anti-oxidant action. This mixture can potentially be useful in the IBS treatment promoting the restoration of the intestinal microbial and immunological balance.

Published
2020

13. Phytocomplex influences antimicrobial and health properties of concentrated glycerine macerates

Author

Di Vito, Maura, Gentile, M., Mattarelli, P., Barbanti, L., Micheli, L., Mazzuca, C., Garzoli, S., Titubante, M., Vitali, Alberto, Cacaci, Margherita, Sanguinetti, Maurizio, Bugli, Francesca, Di Vito M. (ORCID:0000-0002-2991-0855), Vitali A., Cacaci M. (ORCID:0000-0002-5433-9400), Sanguinetti M. (ORCID:0000-0002-9780-7059), Bugli F. (ORCID:0000-0001-9038-3233), Di Vito, Maura, Gentile, M., Mattarelli, P., Barbanti, L., Micheli, L., Mazzuca, C., Garzoli, S., Titubante, M., Vitali, Alberto, Cacaci, Margherita, Sanguinetti, Maurizio, Bugli, Francesca, Di Vito M. (ORCID:0000-0002-2991-0855), Vitali A., Cacaci M. (ORCID:0000-0002-5433-9400), Sanguinetti M. (ORCID:0000-0002-9780-7059), and Bugli F. (ORCID:0000-0001-9038-3233)

Abstract

The purpose of this study was to correlate the chemical composition of four commercial concentrated glycerine macerates (C-GMs), produced through the same extraction method, with their in vitro antimicrobial, antioxidant, and immunomodulatory properties, in order to evaluate their potential for healing upper airway diseases. C-GMs of Carpinus betulus (CB), Ficus carica (FC), Alnus glutinosa (AG) and Ribes nigrum (RN) were studied. The quality was evaluated using HPLC and IM-SPME/GC-MS systems; anti-oxidant and anti-microbial activities were assessed by the respective DPPH test, and micro-broth dilution test performed against 10 strains of Streptococcus pyogenes and 10 probiotic strains. ELISA and MTT tests were used to assess the immunomodulatory activity and the cytotoxicity of C-GMs, respectively. A significant correlation was found between the number of active compounds and the in vitro C-GMs effectiveness. Furthermore, the C-GMs of AG showed the best anti-microbial activity on pathological strains and, together with CB, the best anti-oxidant activity. The ELISA test exhibited a good immunomodulatory activity of RN. In vitro data support the integrated use of C-GMs of CB, AG, and RN in presence of airway diseases, and highlight the importance of standard procedures in cultivation, harvest and post-harvest treatments, as a premise for C-GMs with consistent characteristics.

Published
2020

14. Phytocomplex Influences Antimicrobial and Health Properties of Concentrated Glycerine Macerates

Author

Di Vito, Maura, primary, Gentile, Margherita, additional, Mattarelli, Paola, additional, Barbanti, Lorenzo, additional, Micheli, Laura, additional, Mazzuca, Claudia, additional, Garzoli, Stefania, additional, Titubante, Mattia, additional, Vitali, Alberto, additional, Cacaci, Margherita, additional, Sanguinetti, Maurizio, additional, and Bugli, Francesca, additional

Published
2020
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16. Potent In Vitro Activity of Citrus aurantium Essential Oil and Vitis vinifera Hydrolate Against Gut Yeast Isolates from Irritable Bowel Syndrome Patients—The Right Mix for Potential Therapeutic Use

Author

Di Vito, Maura, primary, Bellardi, Maria Grazia, additional, Sanguinetti, Maurizio, additional, Mondello, Francesca, additional, Girolamo, Antonietta, additional, Barbanti, Lorenzo, additional, Garzoli, Stefania, additional, Sabatino, Manuela, additional, Ragno, Rino, additional, Vitali, Alberto, additional, Palucci, Ivana, additional, Posteraro, Brunella, additional, Gasbarrini, Antonio, additional, Prati, Gian Maria, additional, Aragona, Giovanni, additional, Mattarelli, Paola, additional, and Bugli, Francesca, additional

Published
2020
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18. Nanomedicine Approaches for the Pulmonary Treatment of Cystic Fibrosis

Author

Velino, Cecilia, Carella, Francesca, Adamiano, Alessio, Sanguinetti, Maurizio, Vitali, Alberto, Catalucci, Daniele, Bugli, Francesca, Iafisco, Michele, Sanguinetti, Maurizio (ORCID:0000-0002-9780-7059), Bugli, Francesca (ORCID:0000-0001-9038-3233), Velino, Cecilia, Carella, Francesca, Adamiano, Alessio, Sanguinetti, Maurizio, Vitali, Alberto, Catalucci, Daniele, Bugli, Francesca, Iafisco, Michele, Sanguinetti, Maurizio (ORCID:0000-0002-9780-7059), and Bugli, Francesca (ORCID:0000-0001-9038-3233)

Abstract

N/A

Published
2019

19. A protein chimera self-assembling unit for drug delivery

Author

Amalfitano, Adriana, Martini, Cecilia, Nocca, Giuseppina, Papi, Massimiliano, De Spirito, Marco, Sanguinetti, Maurizio, Vitali, Alberto, Bugli, Francesca, Arcovito, Alessandro, Nocca, Giuseppina (ORCID:0000-0002-2799-4557), Papi, Massimiliano (ORCID:0000-0002-0029-1309), De Spirito, Marco (ORCID:0000-0003-4260-5107), Sanguinetti, Maurizio (ORCID:0000-0002-9780-7059), Bugli, Francesca (ORCID:0000-0001-9038-3233), Arcovito, Alessandro (ORCID:0000-0002-8384-4844), Amalfitano, Adriana, Martini, Cecilia, Nocca, Giuseppina, Papi, Massimiliano, De Spirito, Marco, Sanguinetti, Maurizio, Vitali, Alberto, Bugli, Francesca, Arcovito, Alessandro, Nocca, Giuseppina (ORCID:0000-0002-2799-4557), Papi, Massimiliano (ORCID:0000-0002-0029-1309), De Spirito, Marco (ORCID:0000-0003-4260-5107), Sanguinetti, Maurizio (ORCID:0000-0002-9780-7059), Bugli, Francesca (ORCID:0000-0001-9038-3233), and Arcovito, Alessandro (ORCID:0000-0002-8384-4844)

Abstract

In the modern view of selective drug delivery of bioactive molecules, the attention is moving onto the setup of the perfect carrier more than in the optimization of the active compound. In this respect, virus-like particles constitute bioinspired nanodevices with the intrinsic ability to transport a large class of molecules, ranging from smart drugs to small interfering RNAs. In this work, we demonstrate the efficacy of a novel construct obtained by fusing a self-assembling protein from the human Rotavirus A, VP6, with the Small Ubiquitin Modifier domain, which maintains the ability to form nanoparticles and nanotubes and is able to be used as a drug carrier, even without specific targeting epitopes. The high expression and purification yield, combined with low toxicity of the empty particles, clearly indicate a good candidate for future studies of selective drug delivery. © 2018 American Institute of Chemical Engineers Biotechnol. Prog., 2018.

Published
2019

20. The activity of a mammalian proline-rich peptide against Gram-negative bacteria, including drug-resistant strains, relies on a nonmembranolytic mode of action

Author

Ciociola,Tecla, Giovati,Laura, Giovannelli,Angela, Conti,Stefania, Castagnola,Massimo, Vitali,Alberto, Ciociola,Tecla, Giovati,Laura, Giovannelli,Angela, Conti,Stefania, Castagnola,Massimo, and Vitali,Alberto

Abstract

Tecla Ciociola,1 Laura Giovati,1 Angela Giovannelli,2 Stefania Conti,1 Massimo Castagnola,2,3 Alberto Vitali3 1Department of Medicine and Surgery, University of Parma, Parma, 2Institute of Biochemistry and Clinical Biochemistry, Catholic University, Rome, 3Institute for the Chemistry of Molecular Recognition, C.N.R., c/o Institute of Biochemistry and Clinical Biochemistry, Catholic University, Rome, Italy Background: A peptide of 2,733 Da named SP-E, previously isolated from pig saliva and already described for its antifungal activity and absence of toxicity against mammalian cells, is characterized by a high content of proline residues (70% of entire sequence), that confer structural features probably related to peptide activity. Purpose: The aim of this study was to evaluate the activity of SP-E against Gram-negative bacteria, including drug-resistant clinical isolates. Methods: SP-E and shorter fragments of the same peptide were tested in vitro against the selected bacteria by colony forming unit assays. Scanning electron microscopy and confocal microscopy were also applied. SP-E potential therapeutic activity was evaluated in vivo in a Galleria mellonella model of bacterial infection. Results: SP-E proved to be active against the tested bacteria with EC50 values in the micromolar range. Though maintaining antibacterial properties, the shorter peptides showed lower activity in respect to the parental molecule. Kinetics of killing action and nonmembranolytic internalization within Escherichia coli and Pseudomonas aeruginosa cells strongly suggested a cytosolic mechanism of action involving one or more intracellular molecular targets. A single injection of SP-E exerted a therapeutic effect in G. mellonella larvae infected with P. aeruginosa. Conclusion: The biological properties of SP-E strongly back this peptide as a new promising multitasking antimicrobial molecule. Keywords: antimicrobial peptide, proline-rich peptides, drug-resistant bacteria, confocal microsco

Published
2018

21. Curcumin-loaded graphene oxide flakes as an effective antibacterial system against methicillin-resistant staphylococcus aureus

Author

Bugli, Francesca, Cacaci, Margherita, Palmieri, Valentina, Di Santo, R., Torelli, Riccardo, Ciasca, Gabriele, Di Vito, Maura, Vitali, Alberto, Conti, C., Sanguinetti, Maurizio, De Spirito, Marco, Papi, Massimiliano, Bugli, F. (ORCID:0000-0001-9038-3233), Cacaci, M. (ORCID:0000-0002-5433-9400), Palmieri, V., Torelli, R., Ciasca, G. (ORCID:0000-0002-3694-8229), Di Vito, M. (ORCID:0000-0002-2991-0855), Vitali, A., Sanguinetti, M. (ORCID:0000-0002-9780-7059), De Spirito, M. (ORCID:0000-0003-4260-5107), Papi, M. (ORCID:0000-0002-0029-1309), Bugli, Francesca, Cacaci, Margherita, Palmieri, Valentina, Di Santo, R., Torelli, Riccardo, Ciasca, Gabriele, Di Vito, Maura, Vitali, Alberto, Conti, C., Sanguinetti, Maurizio, De Spirito, Marco, Papi, Massimiliano, Bugli, F. (ORCID:0000-0001-9038-3233), Cacaci, M. (ORCID:0000-0002-5433-9400), Palmieri, V., Torelli, R., Ciasca, G. (ORCID:0000-0002-3694-8229), Di Vito, M. (ORCID:0000-0002-2991-0855), Vitali, A., Sanguinetti, M. (ORCID:0000-0002-9780-7059), De Spirito, M. (ORCID:0000-0003-4260-5107), and Papi, M. (ORCID:0000-0002-0029-1309)

Abstract

Methicillin-resistant Staphylococcus aureus (MRSA) is responsible for serious hospital infections worldwide and represents a global public health problem. Curcumin, the major constituent of turmeric, is effective against MRSA but only at cytotoxic concentrations or in combination with antibiotics. The major issue in curcumin-based therapies is the poor solubility of this hydrophobic compound and the cytotoxicity at high doses. In this paper, we describe the efficacy of a composite nanoparticle made of curcumin (CU) and graphene oxide (GO), hereafter GOCU, in MRSA infection treatment. GO is a nanomaterial with a large surface area and high drug-loading capacity. GO has also antibacterial properties due mainly to a mechanical cutting of the bacterial membranes. For this physical mechanism of action, microorganisms are unlikely to develop resistance against this nanomaterial. In this work, we report the capacity of GO to support and stabilize curcumin molecules in a water environment and we demonstrate the efficacy of GOCU against MRSA at a concentration below 2 mg ml21. Further, GOCU displays low toxicity on fibroblasts cells and avoids haemolysis of red blood cells. Our results indicate that GOCU is a promising nanomaterial against antibiotic-resistant MRSA.

Published
2018

23. Antibacterial Properties of Curcumin Loaded Graphene Oxide Flakes

Author

Palmieri, Valentina, primary, Bugli, Francesca, additional, Cacaci, Margherita, additional, Di Santo, Riccardo, additional, Vitali, Alberto, additional, Torelli, Riccardo, additional, Di Vito, Maura, additional, Conti, Claudio, additional, Sanguinetti, Maurizio, additional, De Spirito, Marco, additional, and Papi, Massimiliano, additional

Published
2018
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24. Cell wall composition and biofilm formation of azoles-susceptible and -resistant Candida glabrata strains.

Author

Vitali, Alberto, Vavala, E, Marzano, Valeria, Leone, C, Castagnola, Massimo, Iavarone, Federica, Angiolella, L., Castagnola, Massimo (ORCID:0000-0002-0959-7259), Iavarone, Federica (ORCID:0000-0002-2074-5531), Vitali, Alberto, Vavala, E, Marzano, Valeria, Leone, C, Castagnola, Massimo, Iavarone, Federica, Angiolella, L., Castagnola, Massimo (ORCID:0000-0002-0959-7259), and Iavarone, Federica (ORCID:0000-0002-2074-5531)

Abstract

In the present study, three strains of Candida glabrata have been investigated to shed light on the mechanisms involved in azole resistance during adherence and biofilm formation. In particular, a clinical isolate, susceptible to azole-based drugs, DSY562 and two different resistant mutagenic strains deriving from DSY562, SFY114 and SFY115, have been analysed with different approaches for their cell wall composition and properties. A proteomic analysis revealed that the expression of six cell wall-related proteins and biofilm formation varied between the strains. The SFY114 and SFY115 strains resulted to be less hydrophobic than the susceptible parental counterpart DSY562, on the other hand they showed a higher amount in total cell wall polysaccharides fraction in the total cell wall. Accordingly to the results obtained from the hydrophobicity and adherence assays, in the resistant strain SFY115 the biofilm formation decreased compared to the parental strain DSY562. Finally, the total glucose amount in resistant SFY115 was about halved in comparison to other strains. Taken together all these data suggest that azole drugs may affect the cell wall composition of C. glabrata, in relation to the different pathogenic behaviours.

Published
2017

25. Antagonistic Effect of a Salivary Proline-Rich Peptide on the Cytosolic Ca2+ Mobilization Induced by Progesterone in Oral Squamous Cancer Cells.

Author

Palmerini, Carlo Alberto, Mazzoni, Manuela, Radicioni, Giorgia, Marzano, Valeria, Granieri, Letizia, Iavarone, Federica, Longhi, R, Messana, Irene, Cabras, Tiziana, Sanna, Maria Teresa, Castagnola, Massimo, Vitali, Alberto, Iavarone, Federica (ORCID:0000-0002-2074-5531), Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Sanna , Maria Teresa, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Palmerini, Carlo Alberto, Mazzoni, Manuela, Radicioni, Giorgia, Marzano, Valeria, Granieri, Letizia, Iavarone, Federica, Longhi, R, Messana, Irene, Cabras, Tiziana, Sanna, Maria Teresa, Castagnola, Massimo, Vitali, Alberto, Iavarone, Federica (ORCID:0000-0002-2074-5531), Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Sanna , Maria Teresa, and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

A salivary proline-rich peptide of 1932 Da showed a dose-dependent antagonistic effect on the cytosolic Ca2+ mobilization induced by progesterone in a tongue squamous carcinoma cell line. Structure-activity studies showed that the activity of the peptide resides in the C-terminal region characterized by a proline stretch flanked by basic residues. Furthermore, lack of activity of the retro-inverso peptide analogue suggested the involvement of stereospecific recognition. Mass spectrometry-based shotgun analysis, combined with Western blotting tests and biochemical data obtained with the Progesterone Receptor Membrane Component 1 (PGRMC1) inhibitor AG205, showed strong evidence that p1932 performs its modulatory action through an interaction with the progesterone receptor PGRMC1, which is predominantly expressed in this cell line and, clearly, plays a role in progesterone induced Ca2+ response. Thus, our results point to p1932 as a modulator of the transduction signal pathway mediated by this protein and, given a well-established involvement of PGRMC1 in tumorigenesis, highlight a possible therapeutic potential of p1932 for the treatment of oral cancer.

Published
2016

26. Structural studies and SH3 domain binding properties of a human antiviral salivary proline-rich peptide

Author

Righino, Benedetta, Pirolli, Davide, Radicioni, Giorgia, Marzano, Valeria, Longhi, Renato, Arcovito, Alessandro, Sanna, Maria Teresa, De Rosa, Maria Cristina, Paoluzi, Serena, Cesareni, Gianni, Messana, Irene, Castagnola, Massimo, Vitali, Alberto, Pirolli, Davide (ORCID:0000-0003-2303-2577), Arcovito, Alessandro (ORCID:0000-0002-8384-4844), Sanna , Maria Teresa, Messana, Irene (ORCID:0000-0002-1436-6105), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Righino, Benedetta, Pirolli, Davide, Radicioni, Giorgia, Marzano, Valeria, Longhi, Renato, Arcovito, Alessandro, Sanna, Maria Teresa, De Rosa, Maria Cristina, Paoluzi, Serena, Cesareni, Gianni, Messana, Irene, Castagnola, Massimo, Vitali, Alberto, Pirolli, Davide (ORCID:0000-0003-2303-2577), Arcovito, Alessandro (ORCID:0000-0002-8384-4844), Sanna , Maria Teresa, Messana, Irene (ORCID:0000-0002-1436-6105), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

Human saliva contains hundreds of small proline-rich peptides originated by the proteolytic cleavage of the salivary basic Proline-Rich Proteins. Nevertheless only for few of them a specific biological activity has been assigned to date. Among them, the 1932 Da peptide (p1932) has been patented as an anti-HIV agent. In order to shed light on the possible mechanism of action of this peptide, we assessed in this study, by means of molecular dynamics calculations, circular dichroism and FTIR spectroscopic techniques, that p1932 has an intrinsic propensity to adopt a polyproline-II helix arrangement. This structural feature combined with the presence of PxxP motifs in its primary structure, represents an essential property for the exploitation of several biological activities. Next to these findings, we recently demonstrated the ability of this peptide to be internalized within cells of the oral mucosa, thus we focused onto a possible intracellular target, represented by the SH3 domains family. Its ability to interact with selected SH3 domains was finally assayed by Surface Plasmon Resonance spectroscopy. As a result, only Fyn, Hck and c-Src SH3 domains gave positive results in terms of interaction, showing dissociation constants ranging from nanomolar to micromolar values having the best performer a KD of 148 nM. It is noteworthy that all the interacting domains belong to the Src kinases family, suggesting a role for p1932 as a modulator of the signal transduction pathways mediated by these kinases.

Published
2016

27. Antagonistic Effect of a Salivary Proline-Rich Peptide on the Cytosolic Ca2+ Mobilization Induced by Progesterone in Oral Squamous Cancer Cells

Author

Palmerini, Carlo Alberto, primary, Mazzoni, Michela, additional, Radicioni, Giorgia, additional, Marzano, Valeria, additional, Granieri, Letizia, additional, Iavarone, Federica, additional, Longhi, Renato, additional, Messana, Irene, additional, Cabras, Tiziana, additional, Sanna, Maria Teresa, additional, Castagnola, Massimo, additional, and Vitali, Alberto, additional

Published
2016
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28. Characterization of the cell penetrating properties of a human salivary proline-rich peptide

Author

Radicioni, Giorgia, Stringaro, Annarita, Molinari, Agnese, Nocca, Giuseppina, Longhi, R, Pirolli, Davide, Scarano, Emanuele, Iavarone, Federica, Manconi, Barbara, Cabras, Tiziana, Messana, Irene, Castagnola, Massimo, Vitali, Alberto, Nocca, Giuseppina (ORCID:0000-0002-2799-4557), Pirolli, Davide (ORCID:0000-0003-2303-2577), Scarano, Emanuele (ORCID:0000-0003-2570-1121), Iavarone, Federica (ORCID:0000-0002-2074-5531), Manconi , Barbara, Cabras , Tiziana, Messana, Irene (ORCID:0000-0002-1436-6105), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Radicioni, Giorgia, Stringaro, Annarita, Molinari, Agnese, Nocca, Giuseppina, Longhi, R, Pirolli, Davide, Scarano, Emanuele, Iavarone, Federica, Manconi, Barbara, Cabras, Tiziana, Messana, Irene, Castagnola, Massimo, Vitali, Alberto, Nocca, Giuseppina (ORCID:0000-0002-2799-4557), Pirolli, Davide (ORCID:0000-0003-2303-2577), Scarano, Emanuele (ORCID:0000-0003-2570-1121), Iavarone, Federica (ORCID:0000-0002-2074-5531), Manconi , Barbara, Cabras , Tiziana, Messana, Irene (ORCID:0000-0002-1436-6105), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

Saliva contains hundreds of small proline-rich peptides most of which derive from the post-translational and post-secretory processing of the acidic and basic salivary proline-rich proteins. Among these peptides we found that a 20 residue proline-rich peptide (p1932), commonly present in human saliva and patented for its antiviral activity, was internalized within cells of the oral mucosa. The cell-penetrating properties of p1932 have been studied in a primary gingival fibroblast cell line and in a squamous cancer cell line, and compared to its retro-inverso form. We observed by mass-spectrometry, flow cytometry and confocal microscopy that both peptides were internalized in the two cell lines on a time scale of minutes, being the natural form more efficient than the retro-inverso one. The cytosolic localization was dependent on the cell type: both peptide forms were able to localize within nuclei of tumoral cells, but not in the nuclei of gingival fibroblasts. The uptake was shown to be dependent on the culture conditions used: peptide internalization was indeed effective in a complete medium than in a serum-free one allowing the hypothesis that the internalization could be dependent on the cell cycle. Both peptides were internalized likely by a lipid raft-mediated endocytosis mechanism as suggested by the reduced uptake in the presence of methyl-ß-cyclodextrin. These results suggest that the natural peptide may play a role within the cells of the oral mucosa after its secretion and subsequent internalization. Furthermore, lack of cytotoxicity of both peptide forms highlights their possible application as novel drug delivery agents.

Published
2015

29. Chrono-proteomics of human saliva: variations of the salivary proteome during human development

Author

Messana, Irene, Cabras, Tiziana, Iavarone, Federica, Manconi, Barbara, Huang, Liling, Martelli, Claudia, Olianas, Alessandra, Sanna, Mt, Pisano, Elisabetta, Sanna, M, Arba, M, D'Alessandro, A, Desiderio, Claudia, Vitali, Alberto, Pirolli, Davide, Tirone, Chiara, Lio, Alessandra, Vento, Giovanni, Romagnoli, Costantino, Cordaro, Massimo, Manni, Armando, Gallenzi, Patrizia, Fiorita, Antonella, Scarano, Emanuele, Calo', Lea, Passali, Giulio Cesare, Picciotti, Pasqualina Maria, Paludetti, Gaetano, Fanos, V, Faa, G, Castagnola, Massimo, Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Iavarone, Federica (ORCID:0000-0002-2074-5531), Manconi , Barbara, Olianas , Alessandra, Pisano , Elisabetta, Pirolli, Davide (ORCID:0000-0003-2303-2577), Vento, Giovanni (ORCID:0000-0002-8132-5127), Romagnoli, Costantino (ORCID:0000-0003-1176-2943), Cordaro, Massimo (ORCID:0000-0002-0797-5172), Manni, Armando (ORCID:0000-0002-7784-1911), Gallenzi, Patrizia (ORCID:0000-0001-9805-4522), Scarano, Emanuele (ORCID:0000-0003-2570-1121), Calo', Lea (ORCID:0000-0003-2671-336X), Passali, Giulio Cesare (ORCID:0000-0002-8176-0962), Picciotti, Pasqualina Maria (ORCID:0000-0002-1502-6508), Paludetti, Gaetano (ORCID:0000-0003-2480-1243), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Messana, Irene, Cabras, Tiziana, Iavarone, Federica, Manconi, Barbara, Huang, Liling, Martelli, Claudia, Olianas, Alessandra, Sanna, Mt, Pisano, Elisabetta, Sanna, M, Arba, M, D'Alessandro, A, Desiderio, Claudia, Vitali, Alberto, Pirolli, Davide, Tirone, Chiara, Lio, Alessandra, Vento, Giovanni, Romagnoli, Costantino, Cordaro, Massimo, Manni, Armando, Gallenzi, Patrizia, Fiorita, Antonella, Scarano, Emanuele, Calo', Lea, Passali, Giulio Cesare, Picciotti, Pasqualina Maria, Paludetti, Gaetano, Fanos, V, Faa, G, Castagnola, Massimo, Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Iavarone, Federica (ORCID:0000-0002-2074-5531), Manconi , Barbara, Olianas , Alessandra, Pisano , Elisabetta, Pirolli, Davide (ORCID:0000-0003-2303-2577), Vento, Giovanni (ORCID:0000-0002-8132-5127), Romagnoli, Costantino (ORCID:0000-0003-1176-2943), Cordaro, Massimo (ORCID:0000-0002-0797-5172), Manni, Armando (ORCID:0000-0002-7784-1911), Gallenzi, Patrizia (ORCID:0000-0001-9805-4522), Scarano, Emanuele (ORCID:0000-0003-2570-1121), Calo', Lea (ORCID:0000-0003-2671-336X), Passali, Giulio Cesare (ORCID:0000-0002-8176-0962), Picciotti, Pasqualina Maria (ORCID:0000-0002-1502-6508), Paludetti, Gaetano (ORCID:0000-0003-2480-1243), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

An important contribution to the variability of any proteome is given by the time dimension that should be carefully considered to define physiological modifications. To this purpose, whole saliva proteome was investigated in a wide age range. Whole saliva was collected from 17 preterm newborns with a postconceptional age at birth of 178-217 days. In these subjects sample collection was performed serially starting immediately after birth and within about 1 year follow-up, gathering a total of 111 specimens. Furthermore, whole saliva was collected from 182 subjects aged between 0 and 17 years and from 23 adults aged between 27 and 57 years. The naturally occurring intact salivary proteome of the 316 samples was analyzed by low- and high-resolution HPLC-ESI-MS platforms. Proteins peculiar of the adults appeared in saliva with different time courses during human development. Acidic proline-rich proteins encoded by PRH2 locus and glycosylated basic proline-rich proteins encoded by PRB3 locus appeared following 180 days of postconceptional age, followed at 7 months (±2 weeks) by histatin 1, statherin, and P-B peptide. The other histatins and acidic proline-rich proteins encoded by PRH1 locus appeared in whole saliva of babies from 1 to 3 weeks after the normal term of delivery, S-type cystatins appeared at 1 year (±3 months), and basic proline-rich proteins appeared at 4 years (±1 year) of age. All of the proteinases involved in the maturation of salivary proteins were more active in preterm than in at-term newborns, on the basis of the truncated forms detected. The activity of the Fam20C kinase, involved in the phosphorylation of various proteins, started around 180 days of postconceptional age, slowly increased reaching values comparable to adults at about 2 years (±6 months) of age. Instead, MAPK14 involved in the phosphorylation of S100A9 was fully active since birth also in preterm newborns.

Published
2015

30. Characterization of the cell penetrating properties of a human salivary proline-rich peptide

Author

Radicioni, Giorgia, primary, Stringaro, Annarita, additional, Molinari, Agnese, additional, Nocca, Giuseppina, additional, Longhi, Renato, additional, Pirolli, Davide, additional, Scarano, Emanuele, additional, Iavarone, Federica, additional, Manconi, Barbara, additional, Cabras, Tiziana, additional, Messana, Irene, additional, Castagnola, Massimo, additional, and Vitali, Alberto, additional

Published
2015
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32. Expression, purification, phosphorylation and characterization of recombinant human statherin.

Author

Manconi, Barbara, Cabras, Tiziana, Vitali, Alberto, Fanali, Chiara, Fiorita, Antonella, Inzitari, Rosanna, Castagnola, Massimo, Messana, Irene, Sanna, Maria Teresa, Manconi , Barbara, Cabras , Tiziana, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Messana, Irene (ORCID:0000-0002-1436-6105), Sanna , Maria Teresa, Manconi, Barbara, Cabras, Tiziana, Vitali, Alberto, Fanali, Chiara, Fiorita, Antonella, Inzitari, Rosanna, Castagnola, Massimo, Messana, Irene, Sanna, Maria Teresa, Manconi , Barbara, Cabras , Tiziana, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Messana, Irene (ORCID:0000-0002-1436-6105), and Sanna , Maria Teresa

Abstract

This work reports the successful recombinant expression of human statherin in Escherichia coli, its purification and in vitro phosphorylation. Human statherin is a 43-residue peptide, secreted by parotid and submandibular glands and phosphorylated on serine 2 and 3. The codon-optimized statherin gene was synthesized and cloned into commercial pTYB11 plasmid to allow expression of statherin as a fusion protein with intein containing a chitin-binding domain. The plasmid was transformed into E. coli strains and cultured in Luria-Bertani medium, which gave productivity of soluble statherin fusion protein of up to 47 mg per liter of cell culture, while 112 mg of fusion protein were in the form of inclusion bodies. No significant refolded target protein was obtained from inclusion bodies. The amount of r-h-statherin purified by RP-HPLC corresponded to 0.6 mg per liter of cell culture. Attenuated total reflection-Fourier transform infrared spectroscopy experiments performed on human statherin isolated from saliva and r-h-statherin assessed the correct folding of the recombinant peptide. Recombinant statherin was transformed into the diphosphorylated biologically active form by in vitro phosphorylation using the Golgi-enriched fraction of pig parotid gland containing the Golgi-casein kinase. (C) 2009 Elsevier Inc. All rights reserved.

Published
2009

33. A proteomic approach to characterizing ciglitazone-induced cancer cell differentiation in Hep-G2 cell line

Author

Bottoni, Patrizia, Giardina, Bruno, Vitali, Alberto, Boninsegna Lucarelli, Alma, Scatena, Roberto, Scatena, Roberto (ORCID:0000-0002-9425-8293), Bottoni, Patrizia, Giardina, Bruno, Vitali, Alberto, Boninsegna Lucarelli, Alma, Scatena, Roberto, and Scatena, Roberto (ORCID:0000-0002-9425-8293)

Abstract

Drug induced cell differentiation represents a promising experimental model for proteomic analysis of cancer cells. In fact, by modulating and monitoring neoplastic cell differentiation it could be possible to identify cytodifferentiation related protein expression changes that can be subsequently utilized in vivo as potential cancer biomarkers. One main advantage of this approach is the significant reduction of biological variability normally observed in clinical biomarker research, with important implications also in prognosis and therapy. At this regard, a new class of differentiating agents is emerging, the so called PPAR-ligands. which however are characterized by a debated mechanism of action that has not been yet studied through a proteomic approach. To this aim, we investigated ciglitazone-induced differentiation of a human hepatocarcinoma HepG2 cell line, by monitoring biochemical and cellular parameters of cytodifferentiation and modifications of cellular protein profiles through 2-DE and MALDI-TOF analysis. Independent of the hypothesized mechanism of action of this intriguing PPAR gamma agonist, results indicated that ciglitazone is a strong differentiating agent for the HepG2 cell line and that this process is associated with modifications of protein expression related to cell antioxidant systems, the cell cycle apparatus, signal transduction pathways, cellular stress and invasiveness. At last, considering these and other published data, a proteomic profile related to the cancer aggressiveness is beginning to emerge

Published
2009

34. Structural and functional characterization of the porcine proline-rich antifungal peptide SP-B isolated from salivary gland granules.

Author

Cabras, Tiziana, Longhi, Renato, Secundo, Francesco, Nocca, Giuseppina, Conti, Salvatore, Polonelli, Luciano, Fanali, Chiara, Inzitari, Rosanna, Petruzzelli, Raffaele, Messana, Irene, Castagnola, Massimo, Vitali, Alberto, Cabras , Tiziana, Nocca, Giuseppina (ORCID:0000-0002-2799-4557), Messana, Irene (ORCID:0000-0002-1436-6105), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Cabras, Tiziana, Longhi, Renato, Secundo, Francesco, Nocca, Giuseppina, Conti, Salvatore, Polonelli, Luciano, Fanali, Chiara, Inzitari, Rosanna, Petruzzelli, Raffaele, Messana, Irene, Castagnola, Massimo, Vitali, Alberto, Cabras , Tiziana, Nocca, Giuseppina (ORCID:0000-0002-2799-4557), Messana, Irene (ORCID:0000-0002-1436-6105), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

A 1905-Da cationic proline-rich peptide, named SP-B, was recently isolated by our group as the main component of salivary gland granules, and its primary sequence fully characterized by means of automated Edman sequencing and LC-MS/MS tools. In the present study SP-B is shown to possess antifungal activity when challenged with strains of Cryptococcus neoformans, Candida albicans and Aspergillus fumigatus, while only negligible antibacterial activity was detected. Furthermore, SP-B was found to be non-cytotoxic when tested on fibroblast cell lines. To obtain information regarding its structure affinity, capillary electrophoresis (CE), circular dichroism (CD) and attenuated total reflection (ATR)-FT/IR experiments were performed. CE revealed a pH dependence of the hydrodynamic radial dimensions both in aqueous and 2,2,2-trifluoroethanol solutions. CD and ATR-FT/IR measurements confirmed the structure-pH relationship, revealing a secondary structure composed of mixed proportions of polyproline-II, unordered and turn motifs, the last being more evident in the zwitterionic form of the peptide. From these findings SP-B peptide could be classified as a new member of the proline-rich antimicrobial peptide family. Copyright (C) 2007 European Peptide Society and John Wiley & Sons, Ltd.

Published
2008

35. Different structural behaviors evidenced in thaumatin-like proteins: A spectroscopic study

Author

Perri, Fabio, Romitelli, Federica, Rufini, F, Secundo, F, Di Stasio, Enrico, Giardina, Bruno, Vitali, Alberto, Di Stasio, Enrico (ORCID:0000-0003-1047-4261), Perri, Fabio, Romitelli, Federica, Rufini, F, Secundo, F, Di Stasio, Enrico, Giardina, Bruno, Vitali, Alberto, and Di Stasio, Enrico (ORCID:0000-0003-1047-4261)

Abstract

Three proteins belonging to the thaumatin-like proteins family were compared in this study from a structural point of view: zeamatin, a new recently isolated PR-5 from Cassia didymobotrya and the commercial sweet-thaumatin. The former two proteins possess antifungal activities while commercial thaumatin is well known to be a natural sweetener. Intrinsic fluorescence studies have evidenced that the three proteins behave differently in unfolding experiments showing different structural rigidity. All the three proteins are more stable at slight acidic buffers, but sweet-thaumatin has a major tendency to destructurate itself. Similar observations were made from circular dichroism studies where a structural dependence relationship from the pH and the solvent used confirmed a hierarchic scale of stability for the three proteins. These structural differences should be considered to be significant for a functional role

Published
2008

36. Trafficking and post-secretory events responsible for the formation of secreted human salivary peptides. A proteomic approach

Author

Messana, Irene, Cabras, Tiziana, Pisano, Elisabetta, Sanna, Maria Teresa, Olianas, Alessandra, Manconi, Barbara, Pellegrini, Magi, Paludetti, Gaetano, Scarano, Emanuele, Fiorita, Antonella, Agostino, Stefania, Contucci, Alessia Maria, Calo', Lea, Picciotti, Pasqualina Maria, Manni, Armando, Bennick, Ander, Vitali, Alberto, Fanali, Chiara, Inzitari, Rosanna, Castagnola, Massimo, Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Pisano , Elisabetta, Sanna , Maria Teresa, Olianas , Alessandra, Manconi , Barbara, Pellegrini , Magi, Paludetti, Gaetano (ORCID:0000-0003-2480-1243), Scarano, Emanuele (ORCID:0000-0003-2570-1121), Calo', Lea (ORCID:0000-0003-2671-336X), Picciotti, Pasqualina Maria (ORCID:0000-0002-1502-6508), Manni, Armando (ORCID:0000-0002-7784-1911), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Messana, Irene, Cabras, Tiziana, Pisano, Elisabetta, Sanna, Maria Teresa, Olianas, Alessandra, Manconi, Barbara, Pellegrini, Magi, Paludetti, Gaetano, Scarano, Emanuele, Fiorita, Antonella, Agostino, Stefania, Contucci, Alessia Maria, Calo', Lea, Picciotti, Pasqualina Maria, Manni, Armando, Bennick, Ander, Vitali, Alberto, Fanali, Chiara, Inzitari, Rosanna, Castagnola, Massimo, Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Pisano , Elisabetta, Sanna , Maria Teresa, Olianas , Alessandra, Manconi , Barbara, Pellegrini , Magi, Paludetti, Gaetano (ORCID:0000-0003-2480-1243), Scarano, Emanuele (ORCID:0000-0003-2570-1121), Calo', Lea (ORCID:0000-0003-2671-336X), Picciotti, Pasqualina Maria (ORCID:0000-0002-1502-6508), Manni, Armando (ORCID:0000-0002-7784-1911), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

To elucidate the localization of post-translational modifications of different classes of human salivary proteins and peptides (acidic and basic proline-rich proteins (PRPs), Histatins, Statherin, P-B peptide, and "S type" Cystatins) a comparative reversed phase HPLC-ESI-MS analysis on intact proteins of enriched granule preparations from parotid and submandibular glands as well as parotid, submandibular/sublingual (Sm/SI), and whole saliva was performed. The main results of this study indicate the following. (1) Phosphorylation of all salivary peptides, sulfation of Histatin 1, proteolytic cleavages of acidic and precursor basic PRPs occur before granule storage. (ii) In agreement with previous studies, basic PRPs are secreted by the parotid gland only, whereas all isoforms of acidic PRPs (aPRPs) are secreted by both parotid and Sm/SI glands. (iii) Phosphorylation levels of aPRPs, Histatin 1, and Statherin are higher in the parotid gland, whereas the extent of cleavage of aPRP is higher in Sm/SI glands. (iv) O-Sulfation of tyrosines of Histatin 1 is a posttranslational modification specific for the submandibular gland. (v) The concentration of Histatin 3, Histatin 5, and Histatin 6, but not Histatin 1, is higher in parotid saliva. (vi) Histatin 3 is submitted to the first proteolytic cleavage (generating Histatins 6 and 5) during granule maturation, and it occurs to the same relative extent in both glands. (vii) The proteolytic cleavages of Histatin 5 and 6, generating a cascade of Histatin 3 fragments, take place after granule secretion and are more extensive in parotid secretion. (viii) Basic PRPs are cleaved in the oral cavity by unknown peptidases, generating various small proline-rich peptides. (ix) C-terminal removal from Statherin is more extensive in parotid saliva. (x) P-B peptide is secreted by both glands, and its relative quantity is higher in submandibular/sublingual secretion. (xi) In agreement with previous studies, S type Cystatins are mainly the pr

Published
2008

37. pH-dependent disruption ofEscherichia coliATCC 25922 and model membranes by the human antimicrobial peptides hepcidin 20 and 25

Author

Maisetta, Giuseppantonio, primary, Vitali, Alberto, additional, Scorciapino, Mariano A., additional, Rinaldi, Andrea C., additional, Petruzzelli, Raffaele, additional, Brancatisano, Franca L., additional, Esin, Semih, additional, Stringaro, Annarita, additional, Colone, Marisa, additional, Luzi, Carla, additional, Bozzi, Argante, additional, Campa, Mario, additional, and Batoni, Giovanna, additional

Published
2013
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38. Structural and functional studies on a proline-rich peptide isolated from swine saliva endowed with antifungal activity towards Cryptococcus neoformans

Author

Conti, Stefania, primary, Radicioni, Giorgia, additional, Ciociola, Tecla, additional, Longhi, Renato, additional, Polonelli, Luciano, additional, Gatti, Rita, additional, Cabras, Tiziana, additional, Messana, Irene, additional, Castagnola, Massimo, additional, and Vitali, Alberto, additional

Published
2013
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39. Antagonistic Effect of a Salivary Proline-Rich Peptide on the Cytosolic Ca2+ Mobilization Induced by Progesterone in Oral Squamous Cancer Cells.

Author

Palmerini, Carlo Alberto, Mazzoni, Michela, Radicioni, Giorgia, Marzano, Valeria, Granieri, Letizia, Iavarone, Federica, Longhi, Renato, Messana, Irene, Cabras, Tiziana, Sanna, Maria Teresa, Castagnola, Massimo, and Vitali, Alberto

Subjects
SALIVARY glands, PROLINE, DRUG efficacy, CYTOSOL, PEPTIDES, PROGESTERONE, SQUAMOUS cell carcinoma, PHYSIOLOGY
Abstract

A salivary proline-rich peptide of 1932 Da showed a dose-dependent antagonistic effect on the cytosolic Ca2+ mobilization induced by progesterone in a tongue squamous carcinoma cell line. Structure-activity studies showed that the activity of the peptide resides in the C-terminal region characterized by a proline stretch flanked by basic residues. Furthermore, lack of activity of the retro-inverso peptide analogue suggested the involvement of stereospecific recognition. Mass spectrometry-based shotgun analysis, combined with Western blotting tests and biochemical data obtained with the Progesterone Receptor Membrane Component 1 (PGRMC1) inhibitor AG205, showed strong evidence that p1932 performs its modulatory action through an interaction with the progesterone receptor PGRMC1, which is predominantly expressed in this cell line and, clearly, plays a role in progesterone induced Ca2+ response. Thus, our results point to p1932 as a modulator of the transduction signal pathway mediated by this protein and, given a well-established involvement of PGRMC1 in tumorigenesis, highlight a possible therapeutic potential of p1932 for the treatment of oral cancer. [ABSTRACT FROM AUTHOR]

Published
2016
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40. Detection in human saliva of different statherin and P-B fragments and derivatives

Author

Inzitari, Rosanna, Cabras, Tiziana, Rossetti, Diana Valeria, Fanali, Chiara, Vitali, Alberto, Pellegrini, Magi, Paludetti, Gaetano, Manni, Armando, Giardina, Bruno, Messana, Irene, Castagnola, Massimo, Cabras , Tiziana, Paludetti, Gaetano (ORCID:0000-0003-2480-1243), Manni, Armando (ORCID:0000-0002-7784-1911), Messana, Irene (ORCID:0000-0002-1436-6105), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Inzitari, Rosanna, Cabras, Tiziana, Rossetti, Diana Valeria, Fanali, Chiara, Vitali, Alberto, Pellegrini, Magi, Paludetti, Gaetano, Manni, Armando, Giardina, Bruno, Messana, Irene, Castagnola, Massimo, Cabras , Tiziana, Paludetti, Gaetano (ORCID:0000-0003-2480-1243), Manni, Armando (ORCID:0000-0002-7784-1911), Messana, Irene (ORCID:0000-0002-1436-6105), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Published
2006

41. Chalcone inhibition of anthracycline secondary alcohol metabolite formation in rabbit and human heart cytosol.

Author

Silvestrini, Andrea, Meucci Calabrese, Elisabetta, Vitali, Alberto, Giardina, Bruno, Mordente, Alvaro, Silvestrini, Andrea (ORCID:0000-0002-2005-3746), Meucci, Elisabetta (ORCID:0000-0002-8821-8041), Mordente, Alvaro (ORCID:0000-0003-3260-9796), Silvestrini, Andrea, Meucci Calabrese, Elisabetta, Vitali, Alberto, Giardina, Bruno, Mordente, Alvaro, Silvestrini, Andrea (ORCID:0000-0002-2005-3746), Meucci, Elisabetta (ORCID:0000-0002-8821-8041), and Mordente, Alvaro (ORCID:0000-0003-3260-9796)

Abstract

Antineoplastic therapy with anthracyclines like doxorubicin (DOX) and daunorubicin (DNR) is limited by the possible development of a dose-related cardiomyopathy. Secondary alcohol metabolites like doxorubicinol (DOXol) and daunorubicinol (DNRol), formed by cytoplasmic two-electron reductases, have been implicated as potential mediators of anthracycline-induced cardiomyopathy. In the present study, we characterized the effects of 12 chalcones on the formation of anthracycline secondary alcohol metabolites by rabbit or human heart cytosol and compared them with those of quercetin and other flavonoids. Both chalcones and flavonoids inhibited DOXol or DNRol formation in isolated rabbit heart cytosol. Structure--activity relationships showed that inhibition by chalcones was determined primarily by the position of hydroxyl groups in their phenolic A and B rings. In particular, the presence of a hydroxyl group at C-4' in the A ring was an important determinant of the inhibitory activity of chalcones. Among chalcones, 2',4',2-trihydroxychalcone exhibited the highest inhibition of both DOXol and DRNol formation, but it proved less efficient than quercetin. Different results were obtained with isolated human heart cytosol: in the latter, 2',4',2-trihydroxychalcone and other hydroxychalcones inhibited both DOXol and DNRol formation, whereas quercetin and other flavonoids inhibited DNRol formation but failed to inhibit or slightly stimulated DOXol formation. These results identify chalcones as versatile inhibitors of the cytoplasmic reductases that convert anthracyclines to cardiotoxic secondary alcohol metabolites.

Published
2006

42. Prenylated flavonoids: pharmacology and biotechnology

Author

Botta, Bruno, Vitali, Alberto, Menendez, Pilar, Misiti, Donatello, Delle Monache, Giuliano, Castagnola, Massimo, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Botta, Bruno, Vitali, Alberto, Menendez, Pilar, Misiti, Donatello, Delle Monache, Giuliano, Castagnola, Massimo, and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

NO ABSTRACT

Published
2005

43. Two proline-rich peptides from pig (Sus scrofa) salivary glands generated by a pre-secretory pathway underlying the action of a proteinase cleaving Pro-Ala bonds

Author

Patamia, Maria, Messana, Irene, Petruzzelli, Raffaele, Vitali, Alberto, Inzitari, Rosanna, Cabras, Tiziana, Fanali, Chiara, Scarano, Emanuele, Contucci, Alessia Maria, Galtieri, Antonio, Castagnola, Massimo, Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Scarano, Emanuele (ORCID:0000-0003-2570-1121), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Patamia, Maria, Messana, Irene, Petruzzelli, Raffaele, Vitali, Alberto, Inzitari, Rosanna, Cabras, Tiziana, Fanali, Chiara, Scarano, Emanuele, Contucci, Alessia Maria, Galtieri, Antonio, Castagnola, Massimo, Messana, Irene (ORCID:0000-0002-1436-6105), Cabras , Tiziana, Scarano, Emanuele (ORCID:0000-0003-2570-1121), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

The primary structures of two salivary proline-rich peptides (PRP-SP-A, M 6156.0 amu and PRP-SP-B, M 1905.0 amu), from pig (Sus scrofa) were determined. The PRP-SP-B peptide, 21 residues long, overlaps with a sequence repeated 43 times in three deposited cDNAs coding for PRP proteins cloned from porcine parotid glands (Swiss-Prot codes: Q95JC9, Q95JD1, Q95JD0). PRP-SP-A peptide, 56 amino acid residues long, overlaps with the N-terminus repeats of Q95JC9 and Q95JD1 and it is phosphorylated at Ser 12 and 14. The two peptides were found both in whole saliva and in granules from pig parotid glands. The biosynthesis of the two peptides implies the action of a proteinase responsible for Pro down arrow Ala cleavage in the pre-secretory process. (c) 2005 Elsevier Inc. All rights reserved.

Published
2005

44. Chalcone dimethylallyltransferase from Morus nigra cell cultures. Substrate specificity studies.

Author

Vitali, Alberto, Giardina, Bruno, Delle Monache, Giuliano, Rocca, Fabrizio, Silvestrini, Andrea, Tafi, Andrea, Botta, Bruno, Silvestrini, Andrea (ORCID:0000-0002-2005-3746), Vitali, Alberto, Giardina, Bruno, Delle Monache, Giuliano, Rocca, Fabrizio, Silvestrini, Andrea, Tafi, Andrea, Botta, Bruno, and Silvestrini, Andrea (ORCID:0000-0002-2005-3746)

Abstract

A new prenyltransferase (PT) enzyme derived from the microsomal fractions of cell cultures of Morus nigra was shown to be able to prenylate exclusively chalcones with a 2',4'-dihydroxy substitution and the isoflavone genistein. Computational studies were performed to shed some light on the relationship between the structure of the substrate and the enzymatic activity. PT requires divalent cations, particularly Mg(2+), to be effective. The apparent K(m) values for gamma,gamma-dimethylallyldiphosphate and 2',4'-dihydroxychalcone were 63 and 142 microM, respectively. The maximum activity of the enzyme was expressed during the first 10 days of cell growth.

Published
2004

45. The Surprising Composition of the Salivary Proteome of Preterm Human Newborn

Author

Castagnola, Massimo, primary, Inzitari, Rosanna, additional, Fanali, Chiara, additional, Iavarone, Federica, additional, Vitali, Alberto, additional, Desiderio, Claudia, additional, Vento, Giovanni, additional, Tirone, Chiara, additional, Romagnoli, Costantino, additional, Cabras, Tiziana, additional, Manconi, Barbara, additional, Teresa Sanna, Maria, additional, Boi, Roberto, additional, Pisano, Elisabetta, additional, Olianas, Alessandra, additional, Pellegrini, Mariagiuseppina, additional, Nemolato, Sonia, additional, Wilhelm Heizmann, Claus, additional, Faa, Gavino, additional, and Messana, Irene, additional

Published
2011
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46. Determination of urinary hippuric acid by micellar electrokinetic chromatography.

Author

Zuppi, Cecilia, Rossetti, Diana Valeria, Vitali, Alberto, Vincenzoni, Federica, Giardina, Bruno, Castagnola, Massimo, Messana, I., Zuppi, Cecilia (ORCID:0000-0003-4710-4934), Castagnola, Massimo (ORCID:0000-0002-0959-7259), Zuppi, Cecilia, Rossetti, Diana Valeria, Vitali, Alberto, Vincenzoni, Federica, Giardina, Bruno, Castagnola, Massimo, Messana, I., Zuppi, Cecilia (ORCID:0000-0003-4710-4934), and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

no abstract

Published
2003

47. Affinity capillary electrophoresis study of the linkage existing between proton and zinc ion binding to bacitracin A1

Author

Castagnola, Massimo, Rossetti, Diana Valeria, Inzitari, Rosanna, Vitali, Alberto, Lupi, Alessandro, Zuppi, Cecilia, Cabras, Tiziana, Fadda, Maria Benedetta, Petruzzelli, Raffaele, Giardina, Bruno, Messana, Irene, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Zuppi, Cecilia (ORCID:0000-0003-4710-4934), Castagnola, Massimo, Rossetti, Diana Valeria, Inzitari, Rosanna, Vitali, Alberto, Lupi, Alessandro, Zuppi, Cecilia, Cabras, Tiziana, Fadda, Maria Benedetta, Petruzzelli, Raffaele, Giardina, Bruno, Messana, Irene, Castagnola, Massimo (ORCID:0000-0002-0959-7259), and Zuppi, Cecilia (ORCID:0000-0003-4710-4934)

Abstract

Measurements by capillary electrophoresis (CE) of bacitracin A(1) effective mobility at different pH values permitted to estimate the five acidic dissociation constants and the Stokes radii at different protonation stages of the macrocyclic dodecapeptide. The pK(a) values were 3.6 and 4.4 for the two carboxylic groups of the lateral chains of D-Asp-11 and D-Glu-4, respectively, 6.4 for the aza-atom of the imidazole ring of His-10, 7.6 for the amino group of N-terminal Ile-1 and 9.7 for the delta-amino group of D-Orn-7, very close to the values obtained by other researchers by titration experiments. In agreement with a rigid macrocyclic structure the Stokes radii of different protonated forms ranged only between 14.3 and 14.8 Angstrom. Best fitting procedures performed on experimental mobility measured at two different pH values (5.50 and 6.72) in the presence of increasing Zn+2 concentration allowed confirming the model that assumes the binding of Zn+2 to P-0 peptide form with a 1.5 x 10(3) M-1 intrinsic association constant. Following to Zn+2 binding, the pK(a) of the amino group of N-terminal Ile-1 is shifted from 7.6 to 5.9 and the Stokes radius is reduced of about 3 Angstrom. The mean charge of the bacitracin A(1)-Zn+2 complex resulted +1.67 and +1.12 at pH 5.50 and 6.72, respectively. These results suggest that the amino group of N-terminal Ile-1 is not essential for Zn+2 binding.

Published
2003

48. Capillary electrophoretic study of the binding of Zn(II) ion to bacitracin A1 in water-2,2,2-trifluoroethanol

Author

Castagnola, Massimo, Rossetti, Diana Valeria, Inzitari, Rosanna, Vitali, Alberto, Lupi, Alessandro, Zuppi, Cecilia, Cabras, Tiziana, Fadda, Maria Benedetta, Podda, Ilaria, Petruzzelli, Raffaele, Giardina, Bruno, Messana, Irene, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Zuppi, Cecilia (ORCID:0000-0003-4710-4934), Castagnola, Massimo, Rossetti, Diana Valeria, Inzitari, Rosanna, Vitali, Alberto, Lupi, Alessandro, Zuppi, Cecilia, Cabras, Tiziana, Fadda, Maria Benedetta, Podda, Ilaria, Petruzzelli, Raffaele, Giardina, Bruno, Messana, Irene, Castagnola, Massimo (ORCID:0000-0002-0959-7259), and Zuppi, Cecilia (ORCID:0000-0003-4710-4934)

Abstract

Binding of Zn2+ to bacitracin A(1) was studied by capillary electrophoresis in water/2,2,2-trifluoroethanol (70/30 v/v) at different apparent pH values in order to estimate the association constant of metal, the acidic dissociation constants and the Stokes radii of both free and bounded peptide in apolar environment. The Stokes radii of the free peptide species were compared with those in aqueous solution, as obtained in a recent study performed by our group, indicating that apolar environment stabilizes bacitracin A(1) in a conformational structure with the lateral chain of apolar amino acids exposed on the external surface. This conformation of the macrocyclic dodecapeptide is ready to interact with Zn2+ ion, as pointed out by the strong increase of the association constant measured in water/2,2,2-trifluoroethanol with respect to the value obtained in aqueous solution. In addition, whereas Zn2+ ion binding in aqueous solution provides a sensible reduction of peptide Stokes radius, no sensible variations following to ion binding were observed in hydro-organic solution. The present results suggest that the apolar environment, rather than the metal ion binding, could be responsible for the conformational transition that brings bacitracin A(1) towards its biologically active structure*.

Published
2003

49. Characterization of dendrimer properties by capillary electrophoresis and their use as pseudostationary phases

Author

Castagnola, Massimo, Zuppi, Cecilia, Rossetti, Diana Valeria, Vincenzoni, Federica, Vitali, Alberto, Meucci, Elisabetta, Messana, Irene, A., Lupi, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Zuppi, Cecilia (ORCID:0000-0003-4710-4934), Meucci, Elisabetta (ORCID:0000-0002-8821-8041), A. Lupi, Castagnola, Massimo, Zuppi, Cecilia, Rossetti, Diana Valeria, Vincenzoni, Federica, Vitali, Alberto, Meucci, Elisabetta, Messana, Irene, A., Lupi, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Zuppi, Cecilia (ORCID:0000-0003-4710-4934), Meucci, Elisabetta (ORCID:0000-0002-8821-8041), and A. Lupi

Abstract

The general properties of dendrimers and in particular their electrolytic characteristics that are relevant in electrokinetic separations, are described. In order to confirm theoretical considerations on commercial dendrimer charge and hydrodynamic radius, several capillary zone electrophoresis (CZE) experiments were performed. Electrophoretic mobilities measured at different pH values indicated a sensible increase of dendrimer hydrodynamic radius at pH values lower than 2.5. This was probably due to the Coulombic repulsion of charged amine groups of the inner dendrimer shells. The principal reasons that should address the use of dendrimers as pseudostationary phases in micellar electrokinetic chromatography (MEKC) are discussed. Moreover, a survey of different separations performed utilizing dendrimers in MEKC as well as of several future plausible uses of various classes of dendrimers is presented.

Published
2002

50. Aryltetralin lignans: chemistry, pharmacology and biotransformations

Author

Botta, Bruno, Delle Monache, Giuliano, Misiti, Domenico, Vitali, Alberto, Zappia, Giovanni, Castagnola, Massimo, Castagnola, Massimo (ORCID:0000-0002-0959-7259), Botta, Bruno, Delle Monache, Giuliano, Misiti, Domenico, Vitali, Alberto, Zappia, Giovanni, Castagnola, Massimo, and Castagnola, Massimo (ORCID:0000-0002-0959-7259)

Abstract

NO ABSTRACT

Published
2001

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