Your search keyword '"Alice Triveri"' showing total 10 results

1. Effects of the Combined Treatment with a G-Quadruplex-Stabilizing Ligand and Photon Beams on Glioblastoma Stem-like Cells: A Magnetic Resonance Study

Author

Alessandra Palma, Sveva Grande, Anna Maria Luciani, Lucia Ricci-Vitiani, Mariachiara Buccarelli, Roberto Pallini, Alice Triveri, Valentina Pirota, Filippo Doria, Quintino Giorgio D’Alessandris, Francesco Berardinelli, Antonio Antoccia, and Antonella Rosi

Subjects

glioblastoma, stem cells, metabolism, magnetic resonance spectroscopy, photon beams, G4-quadruplex ligand, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Glioblastoma multiforme is a malignant primary brain tumor with a poor prognosis and high rates of chemo-radiotherapy failure, mainly due to a small cell fraction with stem-like properties (GSCs). The mechanisms underlying GSC response to radiation need to be elucidated to enhance sensitivity to treatments and to develop new therapeutic strategies. In a previous study, two GSC lines, named line #1 and line #83, responded differently to carbon ions and photon beams, with the differences likely attributable to their own different metabolic fingerprint rather than to radiation type. Data from the literature showed the capability of RHPS4, a G-quadruplex stabilizing ligand, to sensitize the glioblastoma radioresistant U251MG cells to X-rays. The combined metabolic effect of ligand #190, a new RHPS4-derivative showing reduced cardiotoxicity, and a photon beam has been monitored by magnetic resonance (MR) spectroscopy for the two GSC lines, #1 and #83, to reveal whether a synergistic response occurs. MR spectra from both lines were affected by single and combined treatments, but the variations of the analysed metabolites were statistically significant mainly in line #1, without synergistic effects due to combination. The multivariate analysis of ten metabolites shows a separation between control and treated samples in line #1 regardless of treatment type, while separation was not detected in line #83.

Published

2021

2. Conformational Behavior of SARS-Cov-2 Spike Protein Variants: Evolutionary Jumps in Sequence Reverberate in Structural Dynamic Differences

Author

Alice Triveri, Emanuele Casali, Elena Frasnetti, Filippo Doria, Francesco Frigerio, Fabrizio Cinquini, Silvia Pavoni, Elisabetta Moroni, Filippo Marchetti, Stefano A. Serapian, and Giorgio Colombo

Subjects

Physical and Theoretical Chemistry, Computer Science Applications

Published

2023

3. Selective light-up of dimeric G-quadruplex forming aptamers for efficient VEGF165 detection

Author

Ettore Napolitano, Claudia Riccardi, Rosa Gaglione, Angela Arciello, Valentina Pirota, Alice Triveri, Filippo Doria, Domenica Musumeci, Daniela Montesarchio, Napolitano, Ettore, Riccardi, Claudia, Gaglione, Rosa, Arciello, Angela, Pirota, Valentina, Triveri, Alice, Doria, Filippo, Musumeci, Domenica, and Montesarchio, Daniela

Subjects

Structural Biology, Aptamers, Fluorescence light up recognition, G quadruplex, General Medicine, Molecular Biology, Biochemistry

Abstract

To develop efficient anticancer theranostic systems, we studied the interaction between a cyanine dye, analogue of thiazole orange (named CyOH), and two G-quadruplex-forming aptamers, V7t1 and 3R02, recognizing the Vascular Endothelial Growth Factor 165 (VEGF165) - an angiogenic protein overexpressed in cancer cells, responsible for the rapid growth and metastases of solid tumours. We demonstrated, by exploiting different biophysical techniques - i.e. gel electrophoresis, circular dichroism (CD), UV-vis and fluorescence spectroscopy - that this cyanine interacted with both aptamers giving a marked fluorescence light-up only when bound to their dimeric forms. Interestingly, both oligonucleotides recognized VEGF165 with higher affinity when adopting dimeric G-quadruplexes, largely prevalent over their monomeric forms in pseudo-physiological conditions. Notably, the fluorescence light-up produced by the probe was maintained when the dimeric aptamer-CyOH complexes bound to the target protein. These complexes, tested on MCF-7 cancer cells using non-tumorigenic MCF-10A cells as control, were effectively internalized in cells and colocalized with a fluorescently-labelled anti-VEGF-A antibody, allowing both recognition and detection of the target. Our experiments showed that the studied systems are promising tools for anticancer theranostic strategies, combining the therapeutic potential of the G4-forming anti-VEGF aptamers with the diagnostic efficacy of the cyanine selective fluorescence light-up.

Published

2023

4. Selective light-up of dimeric G-quadruplex forming aptamers for efficient VEGF

Author

Ettore, Napolitano, Claudia, Riccardi, Rosa, Gaglione, Angela, Arciello, Valentina, Pirota, Alice, Triveri, Filippo, Doria, Domenica, Musumeci, and Daniela, Montesarchio

Abstract

To develop efficient anticancer theranostic systems, we studied the interaction between a cyanine dye, analogue of thiazole orange (named CyOH), and two G-quadruplex-forming aptamers, V7t1 and 3R02, recognizing the Vascular Endothelial Growth Factor 165 (VEGF

Published

2022

5. Protein Allostery and Ligand Design: Computational Design Meets Experiments to Discover Novel Chemical Probes

Author

Alice Triveri, Carlos Sanchez-Martin, Luca Torielli, Stefano A. Serapian, Filippo Marchetti, Giovanni D'Acerno, Valentina Pirota, Matteo Castelli, Elisabetta Moroni, Mariarosaria Ferraro, Paolo Quadrelli, Andrea Rasola, and Giorgio Colombo

Subjects

Hsp90, Ligands, TRAP1, Small Molecule Libraries, Allosteric Regulation, Structural Biology, protein folding, Drug Design, allosteric regulation, molecular chaperones, Humans, HSP90 Heat-Shock Proteins, allosteric regulation Hsp90 molecular chaperones protein folding TRAP1, Molecular Biology, Allosteric Site, Molecular Chaperones

Abstract

Herein we examine the determinants of the allosteric inhibition of the mitochondrial chaperone TRAP1 by a small molecule ligand. The knowledge generated is harnessed into the design of novel derivatives with interesting biological properties. TRAP1 is a member of the Hsp90 family of proteins, which work through sequential steps of ATP processing coupled to client-protein remodeling. Isoform selective inhibition of TRAP1 can provide novel information on the biomolecular mechanisms of molecular chaperones, as well as new insights into the development of small molecules with therapeutic potential. Our analysis of the interactions between an active first-generation allosteric ligand and TRAP1 shows how the small molecule induces long-range perturbations that influence the attainment of reactive poses in the active site. At the same time, the dynamic adaptation of the allosteric binding pocket to the presence of the first-generation compound sets the stage for the design of a set of second-generation ligands: the characterization of the formation/disappearance of pockets around the allosteric site that is used to guide optimize the ligands' fit for the allosteric site and improve inhibitory activities. The effects of the newly designed molecules are validated experimentally in vitro and in vivo. We discuss the implications of our approach as a promising strategy towards understanding the molecular determinants of allosteric regulation in chemical and molecular biology, and towards speeding up the design of allosteric small molecule modulators.

Published

2022

6. SARS-CoV-2 Spike Protein Mutations and Escape from Antibodies: a Computational Model of Epitope Loss in Variants of Concern

Author

Andrea Rasola, Alice Triveri, Stefano A. Serapian, Francesco Frigerio, Elisabetta Moroni, Filippo Doria, Fabrizio Cinquini, Giorgio L Colombo, Silvia Pavoni, and Filippo Marchetti

Subjects

COVID-19 Vaccines, Coronavirus disease 2019 (COVID-19), General Chemical Engineering, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, Mutant, Peptides and proteins, Computational biology, Library and Information Sciences, Biology, Antibodies, Viral, medicine.disease_cause, Article, Virus, Epitope, Epitopes, Biopolymers, Genetics, medicine, Humans, Antigens, Sequence (medicine), Mutation, SARS-CoV-2, COVID-19, General Chemistry, Vaccine efficacy, Antibodies, Neutralizing, Computer Science Applications, Spike Glycoprotein, Coronavirus, biology.protein, Antibody

Abstract

The SARS-CoV-2 spike (S) protein is exposed on the viral surface and is the first point of contact between the virus and the host. For these reasons it represents the prime target for Covid-19 vaccines. In recent months, variants of this protein have started to emerge. Their ability to reduce or evade recognition by S-targeting antibodies poses a threat to immunological treatments and raises concerns for their consequences on vaccine efficacy.To develop a model able to predict the potential impact of S-protein mutations on antibody binding sites, we performed unbiased multi-microsecond molecular dynamics of several glycosylated S-protein variants and applied a straightforward structure-dynamics-energy based strategy to predict potential changes in immunogenic regions on each variant. We recover known epitopes on the reference D614G sequence. By comparing our results, obtained on isolated S-proteins in solution, to recently published data on antibody binding and reactivity in new S variants, we directly show that modifications in the S-protein consistently translate into the loss of potentially immunoreactive regions. Our findings can thus be qualitatively reconnected to the experimentally characterized decreased ability of some of the Abs elicited against the dominant S-sequence to recognize variants. While based on the study of SARS-CoV-2 Spike variants, our computational epitope-prediction strategy is portable and could be applied to study immunoreactivity in mutants of proteins of interest whose structures have been characterized, helping the development/selection of vaccines and antibodies able to control emerging variants.

Published

2021

7. New perspectives in cancer drug development: computational advances with an eye to design

Author

Luca Torielli, Alice Triveri, Filippo Marchetti, Matteo Castelli, Filippo Doria, Simona Collina, Stefano A. Serapian, Mauro Freccero, Giorgio Colombo, and Valentina Pirota

Subjects

Pharmacology, 0303 health sciences, Drug discovery, Computer science, Organic Chemistry, Cancer drugs, Pharmaceutical Science, Future application, Computational biology, 010402 general chemistry, 01 natural sciences, Biochemistry, 0104 chemical sciences, 03 medical and health sciences, Chemistry, Drug Discovery, Molecular Medicine, Identification (biology), 030304 developmental biology

Abstract

Computational chemistry has come of age in drug discovery. Indeed, most pharmaceutical development programs rely on computer-based data and results at some point. Herein, we discuss recent applications of advanced simulation techniques to difficult challenges in drug discovery. These entail the characterization of allosteric mechanisms and the identification of allosteric sites or cryptic pockets determined by protein motions, which are not immediately evident in the experimental structure of the target; the study of ligand binding mechanisms and their kinetic profiles; and the evaluation of drug-target affinities. We analyze different approaches to tackle challenging and emerging biological targets. Finally, we discuss the possible perspectives of future application of computation in drug discovery.

Published

2021

8. Effects of the combined treatment with a g‐quadruplex‐stabilizing ligand and photon beams on glioblastoma stem‐like cells: A magnetic resonance study

Author

Filippo Doria, Quintino Giorgio D'Alessandris, Anna Maria Luciani, Alice Triveri, Mariachiara Buccarelli, Antonella Rosi, Francesco Berardinelli, Roberto Pallini, Alessandra Palma, Antonio Antoccia, Valentina Pirota, Lucia Ricci-Vitiani, Sveva Grande, Palma, A., Grande, S., Luciani, A. M., Ricci-vitiani, L., Buccarelli, M., Pallini, R., Triveri, A., Pirota, V., Doria, F., D'Alessandris, Q. G., Berardinelli, F., Antoccia, A., and Rosi, A.

Subjects

Radiation-Sensitizing Agents, QH301-705.5, Cell Survival, Settore MED/27 - NEUROCHIRURGIA, Brain tumor, G4-quadruplex ligand, G4‐quadruplex ligand, Stem cells, Ligands, Radiation Tolerance, Article, Catalysis, Spectral line, Inorganic Chemistry, Radioresistance, Magnetic resonance spectroscopy, medicine, Humans, Biology (General), Physical and Theoretical Chemistry, QD1-999, Molecular Biology, Spectroscopy, Photons, Cardiotoxicity, medicine.diagnostic_test, Brain Neoplasms, Chemistry, Organic Chemistry, glioblastoma, stem cells, metabolism, magnetic resonance spectroscopy, photon beams, Magnetic resonance imaging, General Medicine, Nuclear magnetic resonance spectroscopy, Ligand (biochemistry), medicine.disease, Computer Science Applications, G-Quadruplexes, Photon beams, Metabolism, Neoplastic Stem Cells, Biophysics, Acridines, Photon beam, Stem cell, Glioblastoma

Abstract

Glioblastoma multiforme is a malignant primary brain tumor with a poor prognosis and high rates of chemo-radiotherapy failure, mainly due to a small cell fraction with stem-like properties (GSCs). The mechanisms underlying GSC response to radiation need to be elucidated to enhance sensitivity to treatments and to develop new therapeutic strategies. In a previous study, two GSC lines, named line #1 and line #83, responded differently to carbon ions and photon beams, with the differences likely attributable to their own different metabolic fingerprint rather than to radiation type. Data from the literature showed the capability of RHPS4, a G-quadruplex stabilizing ligand, to sensitize the glioblastoma radioresistant U251MG cells to X-rays. The combined metabolic effect of ligand #190, a new RHPS4-derivative showing reduced cardiotoxicity, and a photon beam has been monitored by magnetic resonance (MR) spectroscopy for the two GSC lines, #1 and #83, to reveal whether a synergistic response occurs. MR spectra from both lines were affected by single and combined treatments, but the variations of the analysed metabolites were statistically significant mainly in line #1, without synergistic effects due to combination. The multivariate analysis of ten metabolites shows a separation between control and treated samples in line #1 regardless of treatment type, while separation was not detected in line #83.

Published

2021

9. Exploiting Folding and Degradation Machineries To Target Undruggable Proteins: What Can a Computational Approach Tell Us?

Author

Matteo Castelli, Filippo Marchetti, Giorgio Colombo, Alice Triveri, and Stefano A. Serapian

Subjects

Models, Molecular, Proteasome Endopeptidase Complex, Protein Folding, Computer science, Genomics, Computational biology, Proteomics, 01 natural sciences, Biochemistry, Structure-Activity Relationship, Drug Discovery, Humans, General Pharmacology, Toxicology and Pharmaceutics, Clinical phenotype, Pharmacology, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Ubiquitin, Organic Chemistry, 0104 chemical sciences, Folding (chemistry), 010404 medicinal & biomolecular chemistry, Proteasome, Molecular Medicine, Function (biology), Protein Binding

Abstract

Advances in genomics and proteomics have unveiled an ever-growing number of key proteins and provided mechanistic insights into the genesis of pathologies. This wealth of data showed that changes in expression levels of specific proteins, mutations, and post-translational modifications can result in (often subtle) perturbations of functional protein-protein interaction networks, which ultimately determine disease phenotypes. Although many such validated pathogenic proteins have emerged as ideal drug targets, there are also several that escape traditional pharmacological regulation; these proteins have thus been labeled "undruggable". The challenges posed by undruggable targets call for new sorts of molecular intervention. One fascinating solution is to perturb a pathogenic protein's expression levels, rather than blocking its activities. In this Concept paper, we shall discuss chemical interventions aimed at recruiting undruggable proteins to the ubiquitin proteasome system, or aimed at disrupting protein-protein interactions in the chaperone-mediated cellular folding machinery: both kinds of intervention lead to a decrease in the amount of active pathogenic protein expressed. Specifically, we shall discuss the role of computational strategies in understanding the molecular determinants characterizing the function of synthetic molecules typically designed for either type of intervention. Finally, we shall provide our perspectives and views on the current limitations and possibilities to expand the scope of rational approaches to the design of chemical regulators of protein levels.

Published

2020

10. The Answer Lies in the Energy: How Simple Atomistic Molecular Dynamics Simulations May Hold the Key to Epitope Prediction on the Fully Glycosylated SARS-CoV-2 Spike Protein

Author

Massimiliano Meli, Stefano A. Serapian, Filippo Marchetti, Andrea Rasola, Giuseppe A. Sautto, Alice Triveri, Giulia Morra, Elisabetta Moroni, and Giorgio L Colombo

Subjects

Models, Molecular, 0301 basic medicine, Glycan, Letter, Glycosylation, Peptidomimetic, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Molecular Conformation, Computational biology, Molecular Dynamics Simulation, 01 natural sciences, Epitope, Betacoronavirus, Epitopes, 03 medical and health sciences, chemistry.chemical_compound, Molecular dynamics, epitope prediction, Polysaccharides, Humans, General Materials Science, Physical and Theoretical Chemistry, Binding site, biology, SARS-CoV-2, 010405 organic chemistry, Binding properties, Spike Protein, Antigen binding, atomistic molecular dynamics simulations, 0104 chemical sciences, SARS-CoV-2 spike protein, 030104 developmental biology, chemistry, Spike Glycoprotein, Coronavirus, biology.protein, Binding Sites, Antibody, Peptides, Algorithms

Abstract

Betacoronavirus SARS-CoV-2 is posing a major threat to human health and its diffusion around the world is having dire socioeconomical consequences. Thanks to the scientific community’s unprecedented efforts, the atomic structure of several viral proteins has been promptly resolved. As the crucial mediator of host cell infection, the heavily glycosylated trimeric viral Spike protein (S) has been attracting the most attention and is at the center of efforts to develop antivirals, vaccines, and diagnostic solutions.Herein, we use an energy-decomposition approach to identify antigenic domains and antibody binding sites on the fully glycosylated S protein. Crucially, all that is required by our method are unbiased atomistic molecular dynamics simulations; no prior knowledge of binding properties or ad hoc combinations of parameters/measures extracted from simulations is needed. Our method simply exploits the analysis of energy interactions between all intra-protomer aminoacid and monosaccharide residue pairs, and cross-compares them with structural information (i.e., residueresidue proximity), identifying potential immunogenic regions as those groups of spatially contiguous residues with poor energetic coupling to the rest of the protein.Our results are validated by several experimentally confirmed structures of the S protein in complex with anti- or nanobodies. We identify poorly coupled sub-domains: on the one hand this indicates their role in hosting (several) epitopes, and on the other hand indicates their involvement in large functional conformational transitions. Finally, we detect two distinct behaviors of the glycan shield: glycans with stronger energetic coupling are structurally relevant and protect underlying peptidic epitopes; those with weaker coupling could themselves be poised for antibody recognition. Predicted Immunoreactive regions can be used to develop optimized antigens (recombinant subdomains, synthetic (glyco)peptidomimetics) for therapeutic applications.

Published

2020