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Dive into the research topics where Elisa Peroni is active.

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Featured researches published by Elisa Peroni.


Journal of Neuroimmunology | 2005

The glycopeptide CSF114(Glc) detects serum antibodies in multiple sclerosis

Francesco Lolli; Benedetta Mazzanti; Marta Pazzagli; Elisa Peroni; Maria Claudia Alcaro; Giuseppina Sabatino; Roberta Lanzillo; Vincenzo Morra; Lucio Santoro; Claudio Gasperini; Stefania Galgani; Mario M. D'Elios; Valentina Zipoli; Stefano Sotgiu; Maura Pugliatti; Paolo Rovero; Mario Chelli; Anna Maria Papini

Synthetic glycopeptides have the potential to detect antibodies in multiple sclerosis (MS). In the present study, we analyzed the antibodies (IgM class, IgG class and IgG subclasses) to the synthetic glycopeptide CSF114(Glc) in the serum of 186 MS patients, 166 blood donors (BDs), 25 patients affected by meningitis/encephalitis, 41 affected by systemic lupus erythematosus (SLE) and 49 affected by rheumatoid arthritis (RA). The IgM antibody level to CSF114(Glc) was significantly increased in MS patients versus BDs (p<0.001) or versus other autoimmune diseases (SLE or RA, p<0.001). The IgG response was restricted to the subclass IgG2. IgM antibodies to CSF114(Glc) were found in 30% of relapsing/remitting MS patients and, at lower levels, in subjects affected by meningitis/encephalitis. The study of antibodies to CSF114(Glc) is a new, potential immunological marker of MS.


Current Protein & Peptide Science | 2003

Synthetic Peptides in the Diagnosis of HIV Infection

Maria Claudia Alcaro; Elisa Peroni; Paolo Rovero; Anna Maria Papini

Peptide-based enzyme-linked immunosorbent assays have been found to be enough sensitive and specific for the diagnosis of human immunodeficiency virus specific antibodies in acquired immunodeficiency syndrome patients. This review provides an overview of the most important peptides developed for use as synthetic antigens in immunodiagnosis of HIV-infected patients. In particular, many studies have been devoted to discriminate between the two retroviruses HIV-1 and HIV-2, as well as different subtypes.


Biopolymers | 2008

Ferrocenyl glycopeptides as electrochemical probes to detect autoantibodies in multiple sclerosis patients' sera.

Feliciana Real-Fernández; Amélie Colson; Jérôme Bayardon; Francesca Nuti; Elisa Peroni; Rita Meunier-Prest; Francesco Lolli; Mario Chelli; Christophe Darcel; Sylvain Jugé; Anna Maria Papini

Glycopeptide analogues of CSF114(Glc), modified at N‐terminus with new ferrocenyl carboxylic acid and a new ferrocenyl‐thiphosphino amino acid, were used to implement a new electrochemical biosensor for autoantibody detection in multiple sclerosis. The ferrocenyl moiety of these “electrochemical probes” did not affect autoantibody recognition both in SP‐ELISA and in inhibition experiments. By electrochemical monitoring the interactions of the modified peptides Fc‐CSF114(Glc) and 4‐FcPhP(S)Abu‐CSF114(Glc) with the autoantibodies, we demonstrated that autoantibodies could be detected with a sensitivity comparable to ELISA method. The new electrochemical probes can be proposed to characterize autoantibodies as biomarkers of multiple sclerosis by a simple, rapid, and reproducible cyclic voltammetry‐based diagnostic methodology.


Chemical Physics | 2003

Hydration water dynamics of a completely hydrophobic oligopeptide

Daniela Russo; Piero Baglioni; Elisa Peroni; J. Teixeira

Abstract The dynamics of hydration water of a completely deuterated penta-alanine peptide has been studied by incoherent quasi-elastic neutron scattering. Measurements have been made at different hydration levels (7%, 30%, 50%, 90%), and on the dried powder (0%) which contains one structural water molecule. The dynamical contribution of this first hydration molecule of water is characteristic of a slow rotational motion with a relaxation time, τ1, of 2.2 ps, similar to what is found in supercooled water dynamics. Adding two more hydration water molecules (7%) the rotational motion of the first water is coupled with the new diffusive motion and the dynamics profile can be, in first approximation, described through a rotational jump model. The results suggest a behavior similar to that of bulk water at 2 °C. At higher levels of hydration, the mobility of new molecules of water approaches that of bulk water, with a rotation relaxation time of 1 ps and a confined diffusing motion. However the residence time value, τ0, is of the same order of magnitude as supercooled water at T=−10 ° C.


Bioorganic & Medicinal Chemistry Letters | 2002

A new lipophilic fluorescent probe for interaction studies of bioactive lipopeptides with membrane models

Elisa Peroni; Gabriella Caminati; Piero Baglioni; Francesca Nuti; Mario Chelli; Anna Maria Papini

The new fluorescent lipophilic moiety 11-[(7-amino-4-methyl-2-oxo-2H-1-benzopyran-3-acetyl)amino]undecanoic acid (AMCA-omegaAud-OH) was introduced by SPPS at the N-terminus of the immunodominant epitope GpMBP(74-85). FRET experiments using the new fluorescent lipopeptide demonstrate that the peptide interacts with much more affinity with the membrane compared to the lipid free analogue.


Sensors | 2012

Glycopeptide-Based Antibody Detection in Multiple Sclerosis by Surface Plasmon Resonance

Feliciana Real-Fernández; Irene Passalacqua; Elisa Peroni; Mario Chelli; Francesco Lolli; Anna Maria Papini; Paolo Rovero

In multiple sclerosis (MS) the gold standard for the diagnosis and prognosis is, up to now, the use of magnetic resonance imaging markers. No alternative simpler assays proven of use, except for cerebrospinal fluid analysis, have been provided in MS diagnosis. Therefore, there is a need to develop non-invasive, sensitive, simple new techniques for the clinical routine. Herein we present the evaluation of the feasibility of a glycopeptide-based biosensor to detect MS specific antibodies in sera using the surface plasmon resonance technology. The previously described glycopeptide antigen CSF114(Glc) has been immobilized on a gold sensor chip and the method has been optimized for real-time specific autoantibody detection directly in sera. A population of 60 healthy blood donors and 61 multiple sclerosis patients has been screened. The receiver operating characteristic (ROC)-based analysis has established the optimal diagnostic cut-off value for the method obtaining a sensitivity of 36% and a specificity of 95%. Sample sera have been also screened with a previously validated ELISA.


Journal of Peptide Science | 2015

Synthesis of diastereomerically pure Lys(Nε-lipoyl) building blocks and their use in Fmoc/tBu solid phase synthesis of lipoyl-containing peptides for diagnosis of primary biliary cirrhosis†

Cédric Rentier; Giulia Pacini; Francesca Nuti; Elisa Peroni; Paolo Rovero; Anna Maria Papini

Primary Biliary Cirrhosis is an immune‐mediated disease in which one of the epitopes recognized by antimitochondrial autoantibodies is a lipoylated fragment of the PDC‐E2 protein. Accordingly, the synthesis of lipoylated peptides as diagnostic tools is a relevant target. Up to now, the proper tools for the introduction of lipoylation on building blocks to be used in Fmoc/tBu solid phase peptide synthesis (SPPS) are lacking, and the role of chirality in lipoylation remains poorly studied.


Journal of Neuroimmunology | 2011

IgG and IgM antibodies to the refolded MOG1–125 extracellular domain in humans

Francesca Gori; Barbara Mulinacci; Lara Massai; Carlo Avolio; Mariantonietta Caragnano; Elisa Peroni; S. Lori; Mario Chelli; Anna Maria Papini; Paolo Rovero; Francesco Lolli

Antibodies to MOG in serum have a dubious prognostic value in multiple sclerosis. The MOG recombinant protein conformational properties relevant to the antigenic activity are unknown. We employed a solid-phase ELISA based on a product (rMOG(ED)(His)(6)) expressed in E. coli after subcloning the cDNA of the extracellular domain of rat MOG, performing a refolding procedure on column and affinity purification. The far-UV Circular Dichroism (CD) spectra of rMOG(ED)(His)(6) showed a β-sheet, a characteristic feature of the Ig-fold. However, in MS sera and controls we failed to detected IgM or IgG antibodies.


Bioorganic & Medicinal Chemistry | 2014

Glaser oxidative coupling on peptides: stabilization of β-turn structure via a 1,3-butadiyne constraint.

Nicolas Auberger; Margherita Di Pisa; Maud Larregola; Gérard Chassaing; Elisa Peroni; Solange Lavielle; Anna Maria Papini; Olivier Lequin; Jean-Maurice Mallet

The Glaser-Eglinton reaction between either two C or N propargylglycine (Pra or NPra) amino acids, in the presence of copper(II), led to cyclic hexa- and octapeptides constrained by a butadiyne bridge. The on-resin cyclization conditions were analyzed and optimized. The consequences of this type of constraint on the three dimensional structure of these hexapeptides and octapeptides were analyzed in details by NMR and molecular dynamics. We show that stabilized short cyclic peptides could be readily prepared via the Glaser oxidative coupling either with a chiral (Pra), or achiral (NPra) residue. The 1,3-butadiyne cyclization, along with disulfide bridged and lactam cyclized hexapeptides expands the range of constrained peptides that will allow exploring the breathing of amino acids around a β-turn structure.


Journal of Peptide Science | 2013

Evaluation of new immunological targets in neuromyelitis optica

Jean-Baptiste Chanson; Ilaria Paolini; Nicolas Collongues; Maria Claudia Alcaro; Frédéric Blanc; Francesca Barbetti; Marie Fleury; Elisa Peroni; Paolo Rovero; Gabrielle Rudolf; Francesco Lolli; Elisabeth Trifilieff; Anna Maria Papini; Jérôme De Seze

The detection of reactivity against autoantigens plays a crucial role in the diagnosis of autoimmune diseases. However, only a few autoantibodies are known in each disease, and their precise targets are often not precisely defined. In neuromyelitis optica (NMO), an autoimmune disease of the central nervous system, anti‐aquaporin 4 antibodies are currently the only available immunological markers, although they are not detected in 10–50% of patients. Using enzyme‐linked immunosorbent assays, we evaluated the reactivity against 19 structurally defined peptides in 26 NMO sera compared with 21 healthy subjects. We observed increased levels of IgG against myelin basic protein sequence MBP(156–175), pyruvate dehydrogenase sequence PDH(167–186) and CSF114(Glc), the last of these having a possible correlation with onset of inflammatory relapse. These preliminary results may suggest that the aquaporin 4 is not the unique target in NMO and that the study of reactivity against these peptides would be helpful for the diagnosis and follow‐up of the disease. Complementary studies are however warranted to confirm these results. Copyright

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