Your search keyword '"Vitali, Alberto"' showing total 32 results

1. Liposome Encapsulation of the Palmitoyl–KTTKS Peptide: Structural and Functional Characterization.

Author

Vitali, Alberto, Paolicelli, Patrizia, Bigi, Barbara, Trilli, Jordan, Di Muzio, Laura, Carriero, Vito Cosimo, Casadei, Maria Antonietta, and Petralito, Stefania

Subjects

PEPTIDES, SURFACE charges, VITAMIN C, PHOSPHOLIPIDS, LIPOSOMES, DISPERSION (Chemistry)

Abstract

In this study, the amphiphilic N-palmitoyl–KTTKS peptide was integrated in the bilayer of egg-derived phosphatidylcholine (PC) vesicles using two different preparation methods, namely thin-film evaporation (TLE) and reverse-phase evaporation (REV). Both the REV and TLE methods allowed for the formation of homogeneous liposome dispersions (PdI < 0.20) with mean hydrodynamic diameters of <100 nm and <200 nm, respectively, a net negative surface charge and a percentage of structured phospholipids higher than 90%. The inclusion of the amphiphilic N-palmitoyl–KTTKS peptide within phospholipid-based vesicles could improve peptide stability and skin delivery. Therefore, the obtained liposomes were evaluated via experiments assessing the synthesis of collagen and the ECM in 3T3-NIH fibroblasts. The obtained results showed that, when delivered with PC liposomes, pal-KTTKS stimulated collagen production more than free pentapeptide and 1 mM ascorbic acid, used as a positive control. [ABSTRACT FROM AUTHOR]

Published

2024

2. Disclosing the molecular profile of the human amniotic mesenchymal stromal cell secretome by filter-aided sample preparation proteomic characterization.

Author

Muntiu, Alexandra, Papait, Andrea, Vincenzoni, Federica, Vitali, Alberto, Lattanzi, Wanda, Romele, Pietro, Cargnoni, Anna, Silini, Antonietta, Parolini, Ornella, and Desiderio, Claudia

Subjects

STROMAL cells, AMNION, MULTIOMICS, EXTRACELLULAR matrix, GENE ontology

Abstract

Background: The secretome of mesenchymal stromal cells isolated from the amniotic membrane (hAMSCs) has been extensively studied for its in vitro immunomodulatory activity as well as for the treatment of several preclinical models of immune-related disorders. The bioactive molecules within the hAMSCs secretome are capable of modulating the immune response and thus contribute to stimulating regenerative processes. At present, only a few studies have attempted to define the composition of the secretome, and several approaches, including multi-omics, are underway in an attempt to precisely define its composition and possibly identify key factors responsible for the therapeutic effect. Methods: In this study, we characterized the protein composition of the hAMSCs secretome by a filter-aided sample preparation (FASP) digestion and liquid chromatography-high resolution mass spectrometry (LC–MS) approach. Data were processed for gene ontology classification and functional protein interaction analysis by bioinformatics tools. Results: Proteomic analysis of the hAMSCs secretome resulted in the identification of 1521 total proteins, including 662 unique elements. A number of 157 elements, corresponding to 23.7%, were found as repeatedly characterizing the hAMSCs secretome, and those that resulted as significantly over-represented were involved in immunomodulation, hemostasis, development and remodeling of the extracellular matrix molecular pathways. Conclusions: Overall, our characterization enriches the landscape of hAMSCs with new information that could enable a better understanding of the mechanisms of action underlying the therapeutic efficacy of the hAMSCs secretome while also providing a basis for its therapeutic translation. [ABSTRACT FROM AUTHOR]

Published

2023

3. Cell Penetrating Peptides: Classification, Mechanisms, Methods of Study, and Applications.

Author

Gori, Alessandro, Lodigiani, Giulia, Colombarolli, Stella G., Bergamaschi, Greta, and Vitali, Alberto

Published

2023

4. Novel Arginine- and Proline-Rich Candidacidal Peptides Obtained through a Bioinformatic Approach.

Author

Ciociola, Tecla, Giovati, Laura, De Simone, Tiziano, Bergamaschi, Greta, Gori, Alessandro, Consalvi, Valerio, Conti, Stefania, and Vitali, Alberto

Subjects

ECHINOCANDINS, PROLINE, ANTIMICROBIAL peptides, PEPTIDES, CANDIDA, CANDIDA albicans, SEQUENCE alignment

Abstract

Antimicrobial resistance is a major public health concern worldwide. Albeit to a lesser extent than bacteria, fungi are also becoming increasingly resistant to antifungal drugs. Moreover, due to the small number of antifungal classes, therapy options are limited, complicating the clinical management of mycoses. In this view, antimicrobial peptides (AMPs) are a potential alternative to conventional drugs. Among these, Proline-rich antimicrobial peptides (PrAMPs), almost exclusively of animal origins, are of particular interest due to their peculiar mode of action. In this study, a search for new arginine- and proline-rich peptides from plants has been carried out with a bioinformatic approach by sequence alignment and antimicrobial prediction tools. Two peptide candidates were tested against planktonic cells and biofilms of Candida albicans and Candida glabrata strains, including resistant isolates. These peptides showed similar potent activity, with half-maximal effective concentration values in the micromolar range. In addition, some structural and functional features, revealing peculiar mechanistic behaviors, were investigated. [ABSTRACT FROM AUTHOR]

Published

2023

5. The calcium-antagonist activity of the material released by olive pollen (PMR), tested on Ca2+-cytosolic of PE/CA-PJ15 cells.

Author

Vitali, Alberto, Del Pino, Alberto Marco, Regni, Luca, Costanzi, Eva, Bravi, Elisabetta, Marconi, Ombretta, Proietti, Primo, and Palmerini, Carlo Alberto

Abstract

Inhalation of olive pollen (Olea europaea L.) is one of the main causes of allergy in Mediterranean countries and some areas of North America. The response to allergens consists in the production of inflammatory cytokines which is mediated by the deregulation of Ca2+ signals. In this study, the biological activity of the material released in olive pollen hydration (PMR) was tested on Ca2+ cytosolic of PE/CA-PJ15 cells (PJ-15). Ca2+ cytosolic was determined by fluorometric assay with the cell line PE/CA-PJ15 (PJ-15) labeled with the fluorescent probe FURA 2 AM. The material released in olive pollen hydration (PMR) was analyzed by HPLC for the determination of phenolic acids. PMR was subjected to fractionation by gel filtration, and the fractions with Ca2+-chelating activity were tested with SDS-PAGE and the single bands characterized by proteomic analysis. PMR showed high Ca2+-chelating activity and is able of blocking the increase Ca2+-cytosolic produced by thapsigargin (TG). PMR then restored Ca2+ homeostasis in PJ-15 cells deregulated by the endoplasmic reticulum Ca2+-ATPases inhibitor. It is therefore possible that PMR can antagonize the effects of allergens on Ca2+ cytosolic. The analytical characterization of the material released by the pollen highlighted in the pollen allergen Ole e 3 and in the p-coumaric acid the possible culprits of the Ca2+-antagonist activity of PMR. Furthermore, the sequence of Ole e 3 could provide information for the possible construction of a synthetic peptide to be used in an allergy-targeted Ca2+-antagonist therapy. [ABSTRACT FROM AUTHOR]

Published

2022

6. Peptide-Mediated Targeted Delivery of Aloe-Emodin as Anticancer Drug.

Author

Stringaro, Annarita, Serra, Stefano, Gori, Alessandro, Calcabrini, Annarica, Colone, Marisa, Dupuis, Maria Luisa, Spadaro, Francesca, Cecchetti, Serena, and Vitali, Alberto

Subjects

ANTINEOPLASTIC agents, DRUG accessibility, CELL physiology, AMINO acid sequence, CELL survival, BIOAVAILABILITY

Abstract

Breast cancer is one of the most diffuse cancers in the world and despite the availability of the different drugs employed against it, the need for new and particularly more specific molecules is ever growing. In this framework, natural products are increasingly assuming an important role as new anticancer drugs. Aloe-emodin (AE) is one of the best characterized molecules in this field. The functionalization of bioactive natural products with selected peptide sequences to enhance their bioavailability and specificity of action is a powerful and promising strategy. In this study, we analyzed the cell specificity, cell viability effects, intracellular distribution, and immune cell response of a new peptide conjugate of Aloe-emodin in SKBR3 and A549 cell lines by means of viability tests, flow cytometry, and confocal microscopy. The conjugate proved to be more effective at reducing cell viability than AE in both cell lines. Furthermore, the results showed that it was mainly internalized within the SKBR3 cells, showing a nuclear localization, while A459 cells displayed mainly a cytoplasmic distribution. A preserving effect of the conjugate on NKs' cell function was also observed. The designed conjugate showed a promising specific activity towards HER2-expressing cells coupled with an enhanced water solubility and a higher cytotoxicity; thus, the resulting proof-of-concept molecule can be further improved as an anticancer compound. [ABSTRACT FROM AUTHOR]

Published

2022

7. 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

Subjects

FRAGILE X syndrome, CELL physiology, RNA-binding proteins, CONFOCAL microscopy, REACTIVE oxygen species

Abstract

Fragile X-related disorders are due to a dynamic mutation of the CGG repeat at the 5′ UTR of the FMR1 gene, coding for the RNA-binding protein FMRP. As the CGG sequence expands from premutation (PM, 56-200 CGGs) to full mutation (> 200 CGGs), FMRP synthesis decreases until it is practically abolished in fragile X syndrome (FXS) patients, mainly due to FMR1 methylation. Cells from rare individuals with no intellectual disability and carriers of an unmethylated full mutation (UFM) produce slightly elevated levels of FMR1-mRNA and relatively low levels of FMRP, like in PM carriers. With the aim of clarifying how UFM cells differ from CTRL and FXS cells, a comparative proteomic approach was undertaken, from which emerged an overexpression of SOD2 in UFM cells, also confirmed in PM but not in FXS. The SOD2-mRNA bound to FMRP in UFM more than in the other cell types. The high SOD2 levels in UFM and PM cells correlated with lower levels of superoxide and reactive oxygen species (ROS), and with morphological anomalies and depolarization of the mitochondrial membrane detected through confocal microscopy. The same effect was observed in CTRL and FXS after treatment with MC2791, causing SOD2 overexpression. These mitochondrial phenotypes reverted after knock-down with siRNA against SOD2-mRNA and FMR1-mRNA in UFM and PM. Overall, these data suggest that in PM and UFM carriers, which have high levels of FMR1 transcription and may develop FXTAS, SOD2 overexpression helps to maintain low levels of both superoxide and ROS with signs of mitochondrial degradation. [ABSTRACT FROM AUTHOR]

Published

2020

8. Design of New Nanocarriers for Biomedical Applications.

Author

Colone, Marisa, Angiolella, Letizia, Vitali, Alberto, Serra, Stefano, Gori, Alessandro, Calcabrini, Annarica, and Stringaro, Annarita

Subjects

NANOCARRIERS, BIOMEDICAL materials, DRUG design, NANOMEDICINE, DRUG delivery systems

Abstract

One of the main prerequisite of a therapeutic drug is to overcome a series of physiological barriers and it to be less toxic for the human. To this aim, it is necessary to find a carrying vector able to enhance drug internalization and to improve its therapeutic efficacy. Presently, biocompatible and biodegradable nanoparticles (NPs) as some effective drug delivery devices, are widely studied. In order to increase the antimicrobial and antitumor efficacy of different natural products numerous studies are in progress to evaluate different drug delivery systems (cationic liposomes, lysozymeshelled hollow nano/microbubbles and nano/microcapsules). This delivery system would have a synergistic and additive effect decreasing the drug resistance reactions too. The present article has tried to review some of the latest research on nanocarriers in clinical care. [ABSTRACT FROM AUTHOR]

Published

2018

9. 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, and Vitali, Alberto

Subjects

GRAM-negative bacteria, DRUG resistance in bacteria, PEPTIDES, BIOCHEMICAL mechanism of action, ANTIFUNGAL agents

Abstract

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. [ABSTRACT FROM AUTHOR]

Published

2018

10. Cryptides: latent peptides everywhere.

Author

Iavarone, Federica, Desiderio, Claudia, Vitali, Alberto, Messana, Irene, Martelli, Claudia, Castagnola, Massimo, and Cabras, Tiziana

Subjects

PROTEOMICS, PROTEIN expression, IMMUNOGLOBULINS, MILK proteins, ALBUMINS

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. [ABSTRACT FROM AUTHOR]

Published

2018

11. Cell wall composition and biofilm formation of azoles-susceptible and -resistant Candida glabrata strains.

Author

Vitali, Alberto, Vavala, Elisabetta, Marzano, Valeria, Leone, Claudia, Castagnola, Massimo, Iavarone, Federica, and Angiolella, Letizia

Published

2017

12. The response of Escherichia coli biofilm to salicylic acid.

Author

Cattò, Cristina, Grazioso, Giovanni, Dell’Orto, Silvia, Gelain, Arianna, Villa, Stefania, Marzano, Valeria, Vitali, Alberto, Villa, Federica, Cappitelli, Francesca, and Forlani, Fabio

Subjects

ESCHERICHIA coli, BIOFILMS, SALICYLIC acid, BIOMASS, POLYSACCHARIDES, REACTIVE oxygen species

Abstract

In this research, salicylic acid is proposed as an alternative biocide-free agent suitable for a preventive or integrative anti-biofilm approach. Salicylic acid has been proved to: (1) reduce bacterial adhesion up to 68.1 ± 5.6%; (2) affect biofilm structural development, reducing viable biomass by 97.0 ± 0.7% and extracellular proteins and polysaccharides by 83.9 ± 2.5% and 49.5 ± 5.5% respectively; and (3) promote biofilm detachment 3.4 ± 0.6-fold. Moreover, salicylic acid treated biofilm showed an increased amount of intracellular (2.3 ± 0.2-fold) and extracellular (2.1 ± 0.3-fold) reactive oxygen species, and resulted in increased production of the quorum sensing signal indole (7.6 ± 1.4-fold). For the first time, experiments revealed that salicylic acid interacts with proteins that play a role in quorum sensing, reactive oxygen species accumulation, motility, extracellular polymeric matrix components, transport and metabolism. [ABSTRACT FROM PUBLISHER]

Published

2017

13. 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, and Vitali, Alberto

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-HIVagent. 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. [ABSTRACT FROM AUTHOR]

Published

2016

14. 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

15. Unravelling the Structural and Molecular Basis Responsible for the Anti-Biofilm Activity of Zosteric Acid.

Author

Cattò, Cristina, Dell’Orto, Silvia, Villa, Federica, Villa, Stefania, Gelain, Arianna, Vitali, Alberto, Marzano, Valeria, Baroni, Sara, Forlani, Fabio, and Cappitelli, Francesca

Subjects

BIOFILMS, ZOSTERIN, MOLECULAR biology, CINNAMIC acid, ESCHERICHIA coli, TISSUE scaffolds

Abstract

The natural compound zosteric acid, or p-(sulfoxy)cinnamic acid (ZA), is proposed as an alternative biocide-free agent suitable for preventive or integrative anti-biofilm approaches. Despite its potential, the lack of information concerning the structural and molecular mechanism of action involved in its anti-biofilm activity has limited efforts to generate more potent anti-biofilm strategies. In this study a 43-member library of small molecules based on ZA scaffold diversity was designed and screened against Escherichia coli to understand the structural requirements necessary for biofilm inhibition at sub-lethal concentrations. Considerations concerning the relationship between structure and anti-biofilm activity revealed that i) the para-sulfoxy ester group is not needed to exploit the anti-biofilm activity of the molecule, it is the cinnamic acid scaffold that is responsible for anti-biofilm performance; ii) the anti-biofilm activity of ZA derivatives depends on the presence of a carboxylate anion and, consequently, on its hydrogen-donating ability; iii) the conjugated aromatic system is instrumental to the anti-biofilm activities of ZA and its analogues. Using a protein pull-down approach, combined with mass spectrometry, the herein-defined active structure of ZA was matrix-immobilized, and was proved to interact with the E. coli NADH:quinone reductase, WrbA, suggesting a possible role of this protein in the biofilm formation process. [ABSTRACT FROM AUTHOR]

Published

2015

16. Top-down HPLC- ESI- MS characterization of rat gliadoralin A, a new member of the family of rat submandibular gland glutamine-rich proteins and potential substrate of transglutaminase.

Author

Cabras, Tiziana, Iavarone, Federica, Pirolli, Davide, Cristina De Rosa, Maria, Vitali, Alberto, Faa, Gavino, Cordaro, Massimo, Messana, Irene, Ekström, Jörgen, and Castagnola, Massimo

Subjects

HIGH performance liquid chromatography, SUBMANDIBULAR gland, GLUTAMINE, TRANSGLUTAMINASES, ISOPROTERENOL, NUCLEOTIDE sequence

Abstract

During HPLC- ESI- MS/ MS analysis of rat submandibular saliva secreted under isoprenaline stimulation, a protein with an experimental [M+H]1+ = 10 544.24 m/z was detected (17.5 ± 0.7 min). The MS/ MS fragmentation pattern, manually investigated, allowed establishing an internal sequence in agreement with a DNA-derived sequence of an unknown rat protein coded D3 Z9 M3 ( Swiss- Prot). To match the experimental MS/ MS fragmentation pattern and protein mass with theoretical data, the removal from the N terminus of the signal peptide and from the C terminus of three amino acid (a.a.) residues ( Arg- Ala- Val) and the cyclization of the N-terminal glutamine in pyroglutamic had to be supposed, resulting in a mature protein of 90 a.a. HPLC- ESI- MS/ MS of the trypsin digest ensured 100% sequence coverage. For the high glutamine content (34/90 = 37.8%) we propose to name this protein rat gliadoralin A 1-90. Low amounts of five different isoforms were sporadically detected, which did not significantly change their relative amounts after stimulation. Gliadoralin A is substrate for transglutaminase-2, having Lys 60 and different Gln residues as major determinants for enzyme recognition. In silico investigation of superior structures evidenced that a small part of the protein adopts an α-helical fold, whereas large segments are unfolded, suggesting an unordered conformation. [ABSTRACT FROM AUTHOR]

Published

2013

17. pH-dependent disruption of Escherichia coli ATCC 25922 and model membranes by the human antimicrobial peptides hepcidin 20 and 25.

Author

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

Subjects

PH effect, ESCHERICHIA coli, ANTIMICROBIAL peptides, HEPCIDIN, CYSTEINE, CELL membranes, PROTEIN structure, DRUG activation, FLOW cytometry

Abstract

The human hepcidin 25 (hep-25) and its isoform hepcidin 20 (hep-20) are histidine-containing, cystein rich, β-sheet structured peptides endowed with antimicrobial activity. We previously reported that, similar to other histidine-containing peptides, the microbicidal effects of hep-25 and hep-20 are highly enhanced at acidic pH. In the present study, we investigated whether pH influences the mode of action of hep-25 and hep-20 on Escherichia coli American Type Culture Collection 25922 and model membranes. A striking release of β-galactosidase by hepcidin-treated E. coli was observed at pH 5.0, whereas no inner membrane permeabilization capacity was seen at pH 7.4, even at bactericidal concentrations. Similar results were obtained by flow cytometry when assessing the internalization of propidium iodide by hepcidin-treated E. coli. Scanning electron microscope imaging revealed that both peptides induced the formation of numerous blebs on the surface of bacterial cells at acidic pH but not at neutral pH. Moreover, a phospholipid/polydiacetylene colourimetric vesicle assay revealed a more evident membrane damaging effect at pH 5.0 than at pH 7.4. The leakage of entrapped dextrans of increasing molecular size from liposomes was also assessed at pH 7.4. Consistent with the lack of β-galactosidase release from whole E. coli observed at such a pH value, evident leakage of only the smallest 4-kDa dextran (and not of dextrans of 20 or 70 kDa) was observed, indicating a poor ability of hepcidin peptides to permeabilize liposome vesicles at pH 7.4. Altogether, the data obtained in the present study using different approaches strongly suggest that the ability of hepcidins to perturb bacterial membranes is markedly pH-dependent. [ABSTRACT FROM AUTHOR]

Published

2013

18. Top-down platform for deciphering the human salivary proteome.

Author

Castagnola, Massimo, Cabras, Tiziana, Iavarone, Federica, Vincenzoni, Federica, Vitali, Alberto, Pisano, Elisabetta, Nemolato, Sonia, Scarano, Emanuele, Fiorita, Antonella, Vento, Giovanni, Tirone, Chiara, Romagnoli, Costantino, Cordaro, Massimo, Paludetti, Gaetano, Faa, Gavino, and Messana, Irene

Subjects

PROTEOMICS, DEFENSINS, THYMOSIN, CYSTATINS, HISTATINS

Abstract

Proteomic platforms can be classified in bottom-up strategies, which analyze the sample after proteolytic digestion, and top-down strategies, which analyze the intact naturally occurring proteome. Bottom-up platforms are high-throughput because they can investigate a large number of proteins, regardless of their dimension. Nonetheless, information on post-translational modifications (PTMs) can be lost, especially those regarding naturally occurring cleavages and alternative splicing. Top-down platforms cannot cover vast proteomes, however, they can disclose subtle structural variations occurring during protein maturation and allow label-free relative quantifications in an unlimited number of samples. A repertoire of 256 masses belonging to naturally occurring proteins and peptides consistently detected by RP-HPLC-ESI-MS analysis of the acidic soluble fraction of human whole saliva is presented in this study. Of them, 233 have been identified, while 23 are still pending for the definitive characterization. The present review reports average and mono-isotopic masses of the peptides and proteins detected, RP-HPLC elution times, PTMs, origin and quali-quantitative variations observed in several physiological and pathological conditions. The information reported can be a reference for users of top-down RP-HPLC-ESI-MS proteomic platforms applied to the study of the human salivary proteome as well as of other human bodily fluids. [ABSTRACT FROM AUTHOR]

Published

2012

19. Altered expression level of Escherichia coli proteins in response to treatment with the antifouling agent zosteric acid sodium salt.

Author

Villa, Federica, Remelli, William, Forlani, Fabio, Vitali, Alberto, and Cappitelli, Francesca

Subjects

ESCHERICHIA coli, BACTERIAL proteins, BIOCIDES, SODIUM salts, DRUG activation, BACTERIAL cells, REACTIVE oxygen species, THERAPEUTICS

Abstract

Zosteric acid sodium salt is a powerful antifouling agent. However, the mode of its antifouling action has not yet been fully elucidated. Whole cell proteome of Escherichia coli was analysed to study the different protein patterns expressed by the surface-exposed planktonic cells without and with sublethal concentrations of the zosteric acid sodium salt. Proteomic analysis revealed that at least 27 proteins showed a significant (19 upregulated and 8 downregulated, P < 0.001) altered expression level in response to the antifoulant. The proteomic signatures of zosteric acid sodium salt-treated cells are characterized by stress-associated (e.g. AhpC, OsmC, SodB, GroES, IscU, DnaK), motility-related (FliC), quorum-sensing-associated (LuxS) and metabolism/biosynthesis-related (e.g. PptA, AroA, FabD, FabB, GapA) proteins. Consistent with the overexpression of LuxS enzyme, the antifouling agent increased autoinducer-2 (AI-2) concentration by twofold. Moreover, treated cells experienced a statistically significant but modest increase of reactive oxygen species (+ 23%), tryptophanase (1.2-fold) and indole (1.2-fold) synthesis. Overall, our data suggest that zosteric acid sodium salt acts as environmental cue leading to global stress on E. coli cells, which favours the expression of various protective proteins, the AI-2 production and the synthesis of flagella, to escape from adverse conditions. [ABSTRACT FROM AUTHOR]

Published

2012

20. Structural characterization of a new statherin from pig parotid granules.

Author

Manconi, Barbara, Fanali, Chiara, Cabras, Tiziana, Inzitari, Rosanna, Patamia, Maria, Scarano, Emanuele, Fiorita, Antonella, Vitali, Alberto, Castagnola, Massimo, Messana, Irene, and Teresa Sanna, Maria

Abstract

This study describes the identification and structural characterization of Sus scrofa statherin. HPLC-electrospray ionization mass spectrometry analysis on pig parotid secretory granule extracts evidenced a peptide with a molecular mass value of 5381.1 ± 0.6 Da and its truncated form, devoid of the C-terminal Ala residue, with a molecular mass value of 5310.1 ± 0.6 Da. The complete sequence of pig statherin gene was determined by sequencing the full-length cDNA obtained by rapid amplification of cDNA ends. The gene is 549 base pairs long and contains an open reading frame of 185 nucleotides, encoding a 42-amino acid secretory polypeptide with a signal peptide of 19 residues. This sequence presents some typical features of the four statherins characterized till now, showing the highest degree of amino acid identity with bovine (57%) and human statherin (39%). Pig statherin is mono-phoshorylated on Ser-3, while primate statherins already characterized are di-phosphorylated on Ser-2 and Ser-3. This difference, probably connected to the Asp-4 → Glu substitution, suggests the involvement of the Golgi-casein kinase, which strictly recognizes the SX(E/pS) consensus sequence. Copyright © 2010 European Peptide Society and John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2010

21. Antifungal Carvacrol Loaded Chitosan Nanoparticles.

Author

Vitali, Alberto, Stringaro, Annarita, Colone, Marisa, Muntiu, Alexandra, and Angiolella, Letizia

Subjects

CARVACROL, CHITOSAN, CANDIDA albicans, NANOPARTICLES, MYCOSES, ESSENTIAL oils

Abstract

The increased prevalence and incidence of fungal infections, of which Candida albicans represents one of the most life-threatening organisms, is prompting the scientific community to develop novel antifungal molecules. Many essential oils components are attracting attention for their interesting antifungal activities. Given the chemical and physical characteristics of these compounds, the use of appropriate nanodelivery systems is becoming increasingly widespread. In this study, chitosan nanoparticles were prepared using an ionic gelation procedure and loaded with the phenolic monoterpene carvacrol. After a bioassay guided optimization, the best nanoparticle formulation was structurally characterized by means of different spectroscopic (UV, FTIR and DLS) and microscopy techniques (SEM) and described for their functional features (encapsulation efficiency, loading capacity and release kinetics). The antifungal activity of this formulation was assayed with different Candida spp., both in planktonic and biofilm forms. From these studies, it emerged that the carvacrol loaded nanoparticles were particularly active against planktonic forms and that the antibiofilm activity was highly dependent on the species tested, with the C. tropicalis and C. krusei strains resulting as the most susceptible. [ABSTRACT FROM AUTHOR]

Published

2022

22. 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, Mariagiuseppina, Paludetti, Gaetano, Manni, Armando, Giardina, Bruno, Messana, Irene, and Castagnola, Massimo

Published

2006

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

Author

Vitali, Alberto, Giardina, Bruno, Delle Monache, Giuliano, Rocca, Filippo, Silvestrini, Andrea, Tafi, Andrea, and Botta, Bruno

Subjects

TRANSFERASES, MICROSOMES, CELL culture, ENZYMES

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 Mg2+, to be effective. The apparent Km values for γ,γ-dimethylallyldiphosphate and 2′,4′-dihydroxychalcone were 63 and 142 μM, respectively. The maximum activity of the enzyme was expressed during the first 10 days of cell growth. [Copyright &y& Elsevier]

Published

2004

24. 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, and Messana, Irene

Published

2003

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

Author

Castagnola, Massimo, Zuppi, Cecilia, Rossetti, Diana V., Vincenzoni, Federica, Lupi, Alessandro, Vitali, Alberto, Meucci, Elisabetta, and Messana, Irene

Published

2002

26. Capillary electrophoresis detection of a complex sensitive to electric field.

Author

Messana, Irene, Andreasi Bassi, Francesco, Rossetti, Diana V., Misiti, Francesco, Vincenzoni, Federica, Vitali, Alberto, Zuppi, Cecilia, Giardina, Bruno, and Castagnola, Massimo

Published

2001

27. In vitro plant regeneration of Vismia guianensis through organogenesis.

Author

Monacelli, Barbara, Pasqua, Gabriella, Cuteri, Angelina, and Vitali, Alberto

Published

1999

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

Author

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

Subjects

FIG, ALNUS glutinosa, GLYCERIN, STREPTOCOCCUS pyogenes, HIGH performance liquid chromatography

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. [ABSTRACT FROM AUTHOR]

Published

2020

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

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. [ABSTRACT FROM AUTHOR]

Published

2020

30. A protein chimera self‐assembling unit for drug delivery.

Author

Amalfitano, Adriana, Nocca, Giuseppina, Arcovito, Alessandro, Martini, Cecilia, Sanguinetti, Maurizio, Bugli, Francesca, Vitali, Alberto, Papi, Massimiliano, and De Spirito, Marco

Subjects

PROTEINS, DRUG delivery systems, CHIMERISM, RNA, NANOPARTICLES

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., 35: e2769, 2019. [ABSTRACT FROM AUTHOR]

Published

2019

31. Synthesis and Biosynthesis of Isocordoin.

Author

Vitali, Alberto, Ferrari, Franco, Delle Monache, Giuliano, Bombardelli, Ezio, and Botta, Bruno

Published

2001

32. ChemInform Abstract: β-Glucosyltransferase in Cell Cultures of Verbesina caracasana.

Author

Vitali, Alberto, Delle Monache, Giuliano, Zappia, Giovanni, Misiti, Domenico, Gacs-Baitz, Eszter, and Botta, Bruno

Published

1999