Publications by authors named "Francesca Nuti"

Article Synopsis
  • A study under the European LIFE project is investigating the presence of endocrine-disrupting chemicals (EDCs) in 20 types of infant formulas and in baby bottles and teats, highlighting the risks posed by these chemicals, especially during pregnancy and infancy.* -
  • The study used advanced analytical methods to test for 85 different chemicals, finding low levels of certain harmful substances like phthalates and PAHs in baby products, raising concerns about exposure.* -
  • While some chemicals were absent in accordance with EU regulations in baby bottles, significant levels of EDCs were found in infant formulas, signaling a need for ongoing monitoring and public health measures to protect young children.*
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A gel that exhibits intrinsically multiple-responsive behavior was prepared from an oligopeptide and studied. ACP(65-74) is an active decapeptide fragment of acyl carrier protein. We investigated 3% w/v ACP(65-74)-NH self-healing physical gels in water, glycerol carbonate (GC), and their mixtures.

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Oxytocin (OT) is a neurohypophyseal peptide hormone containing a disulphide-bridged pseudocyclic conformation. The biomedical use of OT peptides is limited amongst others by disadvantageous pharmacokinetic parameters. To increase the stability of OT by replacing the disulphide bridge with the stable and more rigid [1,2,3]triazol-1-yl moiety, we employed the Cu-catalysed side chain-to-side chain azide-alkyne 1,3-cycloaddition.

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  • Multiple sclerosis (MS) is an autoimmune disorder characterized by inflammation and the damaging of myelin due to antibody activity.
  • Researchers created two glucosylated peptides from human myelin proteins, which possess similar structures to a specific antigen recognized by MS patient antibodies, to study their immune response.
  • The findings indicate that these peptides are recognized by antibodies in MS patients and share immunological similarities with both human and bacterial proteins, suggesting a possible link between these proteins that might contribute to the onset of MS.
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Peptide fragments of glycoproteins containing multiple -glycosylated sites are essential biochemical tools not only to investigate protein-protein interactions but also to develop glycopeptide-based diagnostics and immunotherapy. However, solid-phase synthesis of glycopeptides containing multiple -glycosylated sites is hampered by difficult couplings, which results in a substantial drop in yield. To increase the final yield, large amounts of reagents but also time-consuming steps are required.

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Article Synopsis
  • The study focuses on Myelin Basic Protein (MBP) and its role in Multiple Sclerosis, particularly how its α-helix structure affects antibody recognition.
  • Researchers synthesized and tested two different lengths of MBP peptides, finding that elongating the peptide improves antibody recognition but destabilizes its helical structure.
  • Results indicate that the original shorter peptide (MBP 81-106) is better recognized by IgM antibodies in competitive ELISA due to its stable helical form, highlighting the complexity of antibody-antigen interactions in different testing conditions.
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Article Synopsis
  • - The study focuses on creating tentacle-like polymers that can enhance the capture of antibodies in patient sera, specifically targeting those found in multiple sclerosis (MS) patients.
  • - Researchers identified a specific peptide epitope from a protein associated with a bacteria (NTHi) that MS antibodies recognize and developed a multivalent dextran conjugate to increase antibody binding.
  • - The new polymer effectively captured both IgG and IgM antibodies from MS patients, demonstrating potential for selectively isolating high-affinity autoantibodies, which could improve diagnostics and treatment for autoimmune conditions.
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Diagnosis of Latent Autoimmune Diabetes in Adults (LADA) is based on the adult-age, anti-islet autoantibodies, and temporary insulin-independence. As in Type-1-Diabetes (T1DM), autoimmunity may trigger LADA and enteroviruses-infections can play a role. Anti-human Glutamic-Acid-Decarboxylase (hGAD) autoantibodies are accepted clinical biomarkers, but do not discriminate LADA T1DM.

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Article Synopsis
  • The study investigates the diagnostic potential of antibodies against human glutamic acid decarboxylase (hGAD) peptides in diagnosing latent autoimmune diabetes in adults (LADA) and type 1 diabetes mellitus (T1DM), focusing on their relation to Enterovirus Coxsackie B4.
  • It involved testing serum samples from 27 LADA patients, 23 T1DM patients, and 24 controls using ELISA, and found significant differences in antibody responses between the patient groups and the controls.
  • The results showed that IgM antibodies had high diagnostic power for LADA (sensitivity over 85%, specificity 95.8%), highlighting the importance of peptide antigens in distinguishing between T1DM and L
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  • - Peptides that mimic the specific parts targeted by antibodies can be useful for diagnosing and treating autoimmune diseases like multiple sclerosis (MS) by acting as antigen substitutes.
  • - Research focused on synthesizing peptides derived from the Haemophilus influenzae adhesin, particularly those containing N-linked glucopyranosyl moieties, which were found crucial for strong antibody binding in certain MS patients.
  • - The best-performing synthetic peptide, Ac-KAN (Glc)VTLN (Glc)TT-NH, exhibited effective binding to IgG antibodies, but its binding characteristics didn't rely on the sugar's placement or the peptide's structure in solution, indicating complexity in how these interactions occur.
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  • The diagnosis of Multiple Sclerosis (MS) mainly relies on magnetic resonance imaging (MRI), but few simple tests are available to monitor disease activity over time.
  • Researchers found that antibodies against a specific type of sugar-modified peptide (anti--Glc) can be detected in the blood of MS patients and may serve as useful biomarkers.
  • They developed a new set of multiple-glucosylated peptide epitopes (known as -Glc MEPs) for a diagnostic test, utilizing a specific structure to enhance the detection of these antibodies efficiently in patients' serum.
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We report herein a novel ChemMatrix Rink resin functionalised with two phenylboronate (PhB) moieties linked on the -α and -ε amino functions of a lysine residue to specifically capture deoxyfructosylated peptides, compared to differently glycosylated peptides in complex mixtures. The new PhB-Lys(PhB)-ChemMatrix Rink resin allows for exploitation of the previously demonstrated ability of diols to form phenylboronic esters. The optimised capturing and cleavage procedure from the novel functionalised resin showed that only the peptides containing deoxyfructosyl-lysine moieties can be efficiently and specifically detected by HR-MS and MS/MS experiments.

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The insertion of azobenzene moiety in complex molecular protein or peptide systems can lead to molecular switches to be used to determine kinetics of folding/unfolding properties of secondary structures, such as α-helix, β-turn, or β-hairpin. In fact, in azobenzene, absorption of light induces a reversible trans ↔ cis isomerization, which in turns generates a strain or a structure relaxation in the chain that causes peptide folding/unfolding. In particular azobenzene may permit reversible conformational control of hairpin formation.

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Article Synopsis
  • Mitochondrial proteins are significant in type 1 diabetes (T1D), offering potential targets for studying antigens related to the disease.
  • The study evaluated immune responses in T1D patients using synthetic peptides with specific post-translational modifications (PTMs), like lipoylation and phosphorylation.
  • Findings revealed that specific PTMs in the mitochondrial peptide are important for IgM antibody recognition, suggesting potential new diagnostic markers for T1D.
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  • * A cyclic heptapeptide was developed that binds well to an anti-HNK1 mouse monoclonal antibody, demonstrating promising affinity through structure-activity relationship studies.
  • * However, initial tests reveal that human sera do not specifically recognize this peptide, suggesting that mouse antibodies are not reliable for selecting probes to detect human auto-antibodies.
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Article Synopsis
  • Autoimmune diseases, like multiple sclerosis (MS), may be triggered by specific non-self antigens from infections, potentially leading to immune system dysfunction.
  • Research indicates that exposure to certain bacteria, such as Haemophilus influenzae, could be linked to MS, as these bacteria produce antigens that resemble human cell markers.
  • A unique protein from H. influenzae that undergoes hyperglucosylation was found to be recognized by antibodies in some MS patients, suggesting it might play a role in triggering autoimmune responses in the disease.
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The role of pathologic auto-antibodies against myelin oligodendrocyte glycoprotein (MOG) in multiple sclerosis is a highly controversial matter. As the use of animal models may enable to unravel the molecular mechanisms of the human disorder, numerous studies on multiple sclerosis are carried out using experimental autoimmune encephalomyelitis (EAE). In particular, the most extensively used EAE model is obtained by immunizing C57BL/6 mice with the immunodominant peptide MOG(35-55).

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The modulation of collagen turnover can be a relevant pharmacological target in the context of treating either pathological or pathophysiological conditions, such as collagen-related diseases and skin aging. Our recent work has focused on the search for short-chain peptides as lead compounds for further development of compounds that enhance the production of type I collagen. In this study we selected and synthesized overlapping peptides of the C-terminal portion of serpin A1 (residues 393-418), the impact of which on collagen production has been reported previously, in order to identify shorter and still active fragments and to provide insight on the mechanisms involved.

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  • The study explores how lipid environments interact with the β-turn peptide CSF114 and its modified version, CSF114(Glc), which serves as a synthetic probe for identifying specific autoantibodies in multiple sclerosis patients.
  • Using techniques like fluorescence spectroscopy and electrochemical measurements, the researchers found that CSF114(Glc) interacts with lipid structures, particularly those made from dioleoylphosphatidylcholine, especially under certain electrical conditions.
  • The research indicates that CSF114(Glc) can affect lipid membranes by creating defects that increase permeability, but it does not significantly alter tethered bilayer lipid membranes (tBLMs).
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Primary biliary cirrhosis is an immune-mediated chronic liver disease whose diagnosis relies on the detection of serum antimitochondrial antibodies directed against a complex set of proteins, among which pyruvate dehydrogenase complex is considered the main autoantigen. We studied the immunological role of the lipoyl domain of this protein using synthetic lipoylated peptides, showing that the lipoyl chain chirality does not affect autoantibody recognition and, most importantly, confirming that both lipoylated and unlipoylated peptides are able to recognize specific autoantibodies in patients sera. In fact, 74% of patients sera recognize at least one of the tested peptides but very few positive sera recognized exclusively the lipoylated peptide, suggesting that the lipoamide moiety plays a marginal role within the autoreactive epitope.

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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.

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Objectives: Phthalates might be implicated with obesity and insulin sensitivity. We evaluated the levels of primary and secondary metabolites of Di-(2-ethylhexyl) phthalate (DEHP) in urine in obese and normal-weight subjects both before and during puberty, and investigated their relationships with auxological parameters and indexes of insulin sensitivity.

Design And Methods: DEHP metabolites (MEHP, 6-OH-MEHP, 5-oxo-MEHP, 5-OH-MEHP, and 5-CX-MEHP), were measured in urine by RP-HPLC-ESI-MS.

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Rett syndrome (RTT), a neurodevelopmental disorder affecting exclusively (99%) female infants, is associated with loss-of-function mutations in the gene encoding methyl-CpG binding protein 2 (MECP2) and, more rarely, cyclin-dependent kinase-like 5 (CDKL5) and forkhead box protein G1 (FOXG1). In this study, we aimed to evaluate the function of the immune system by measuring serum immunoglobulins (IgG and IgM) in RTT patients (n = 53) and, by comparison, in age-matched children affected by non-RTT pervasive developmental disorders (non-RTT PDD) (n = 82) and healthy age-matched controls (n = 29). To determine immunoglobulins we used both a conventional agglutination assay and a novel ELISA based on antibody recognition by a surrogate antigen probe, CSF114(Glc), a synthetic N-glucosylated peptide.

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