Your search keyword '"Bugiani, O"' showing total 22 results

1. Review: PrP 106-126 - 25 years after.

Author

Forloni G, Chiesa R, Bugiani O, Salmona M, and Tagliavini F

Subjects

Animals, Humans, Peptide Fragments, Prion Diseases, Prions

Abstract

A quarter of a century ago, we proposed an innovative approach to study the pathogenesis of prion disease, one of the most intriguing biomedical problems that remains unresolved. The synthesis of a peptide homologous to residues 106-126 of the human prion protein (PrP106-126), a sequence present in the PrP amyloid protein of Gerstmann-Sträussler-Scheinker syndrome patients, provided a tractable tool for investigating the mechanisms of neurotoxicity. Together with several other discoveries at the beginning of the 1990s, PrP106-126 contributed to underpin the role of amyloid in the pathogenesis of protein-misfolding neurodegenerative disorders. Later, the role of oligomers on one hand and of prion-like spreading of pathology on the other further clarified mechanisms shared by different neurodegenerative conditions. Our original report on PrP106-126 neurotoxicity also highlighted a role for programmed cell death in CNS diseases. In this review, we analyse the prion research context in which PrP106-126 first appeared and the advances in our understanding of prion disease pathogenesis and therapeutic perspectives 25 years later., (© 2019 British Neuropathological Society.)

Published

2019

2. APP mutations in the Aβ coding region are associated with abundant cerebral deposition of Aβ38.

Author

Moro ML, Giaccone G, Lombardi R, Indaco A, Uggetti A, Morbin M, Saccucci S, Di Fede G, Catania M, Walsh DM, Demarchi A, Rozemuller A, Bogdanovic N, Bugiani O, Ghetti B, and Tagliavini F

Subjects

Adult, Aged, Aged, 80 and over, Alzheimer Disease genetics, Alzheimer Disease metabolism, Amyloid beta-Protein Precursor metabolism, Brain metabolism, Brain pathology, Cerebral Amyloid Angiopathy genetics, Cerebral Amyloid Angiopathy metabolism, Humans, Middle Aged, Open Reading Frames, Alzheimer Disease pathology, Amyloid beta-Peptides metabolism, Amyloid beta-Protein Precursor genetics, Cerebral Amyloid Angiopathy pathology, Mutation genetics, Peptide Fragments metabolism

Abstract

Aβ is the main component of amyloid deposits in Alzheimer disease (AD) and its aggregation into oligomers, protofibrils and fibrils is considered a seminal event in the pathogenesis of AD. Aβ with C-terminus at residue 42 is the most abundant species in parenchymal deposits, whereas Aβ with C-terminus at residue 40 predominates in the amyloid of the walls of large vessels. Aβ peptides with other C-termini have not yet been thoroughly investigated. We analysed Aβ38 in the brains of patients with Aβ deposition linked to sporadic and familial AD, hereditary cerebral haemorrhage with amyloidosis, or Down syndrome. Immunohistochemistry, confocal microscopy, immunoelectron microscopy, immunoprecipitation and the electrophoresis separation of low molecular weight aggregates revealed that Aβ38 accumulates consistently in the brains of patients carrying APP mutations in the Aβ coding region, but was not detected in the patients with APP mutations outside the Aβ domain, in the patients with presenilin mutations or in subjects with Down syndrome. In the patients with sporadic AD, Aβ38 was absent in the senile plaques, but it was detected only in the vessel walls of a small subset of patients with severe cerebral amyloid angiopathy. Our results suggest that APP mutations in the Aβ coding region favour Aβ38 accumulation in the brain and that the molecular mechanisms of Aβ deposition in these patients may be different from those active in patients with familial AD associated with other genetic defects and sporadic AD.

Published

2012

3. Structural properties of Gerstmann-Straussler-Scheinker disease amyloid protein.

Author

Salmona M, Morbin M, Massignan T, Colombo L, Mazzoleni G, Capobianco R, Diomede L, Thaler F, Mollica L, Musco G, Kourie JJ, Bugiani O, Sharma D, Inouye H, Kirschner DA, Forloni G, and Tagliavini F

Subjects

Amino Acid Sequence, Amyloid metabolism, Animals, Cell Membrane metabolism, Congo Red pharmacology, Endopeptidases pharmacology, Humans, Microscopy, Electron, Molecular Sequence Data, Neurons metabolism, Peptides chemistry, Protein Isoforms, Protein Structure, Secondary, Protein Structure, Tertiary, Rats, Spectroscopy, Fourier Transform Infrared, Time Factors, X-Ray Diffraction, Amyloid chemistry, Gerstmann-Straussler-Scheinker Disease metabolism, Peptide Fragments chemistry, Prions chemistry

Abstract

Prion protein (PrP) amyloid formation is a central feature of genetic and acquired forms of prion disease such as Gerstmann-Sträussler-Scheinker disease (GSS) and variant Creutzfeldt-Jakob disease. The major component of GSS amyloid is a PrP fragment spanning residues approximately 82-146. To investigate the determinants of the physicochemical properties of this fragment, we synthesized PrP-(82-146) and variants thereof, including entirely and partially scrambled peptides. PrP-(82-146) readily formed aggregates that were partially resistant to protease digestion. Peptide assemblies consisted of 9.8-nm-diameter fibrils having a parallel cross-beta-structure. Second derivative of infrared spectra indicated that PrP-(82-146) aggregates are primarily composed of beta-sheet (54%) and turn (24%) which is consistent with their amyloid-like properties. The peptide induced a remarkable increase in plasma membrane microviscosity of primary neurons. Modification of the amino acid sequence 106-126 caused a striking increase in aggregation rate, with formation of large amount of protease-resistant amorphous material and relatively few amyloid fibrils. Alteration of the 127-146 region had even more profound effects, with the inability to generate amyloid fibrils. These data indicate that the intrinsic properties of PrP-(82-146) are dependent upon the integrity of the C-terminal region and account for the massive deposition of PrP amyloid in GSS.

Published

2003

4. The stimulation of inducible nitric-oxide synthase by the prion protein fragment 106--126 in human microglia is tumor necrosis factor-alpha-dependent and involves p38 mitogen-activated protein kinase.

Author

Fabrizi C, Silei V, Menegazzi M, Salmona M, Bugiani O, Tagliavini F, Suzuki H, and Lauro GM

Subjects

Cells, Cultured, Gene Expression Regulation drug effects, Humans, Nitric Oxide Synthase genetics, Nitric Oxide Synthase Type II, Signal Transduction drug effects, Signal Transduction genetics, p38 Mitogen-Activated Protein Kinases, Microglia metabolism, Mitogen-Activated Protein Kinases metabolism, Nitric Oxide Synthase biosynthesis, Peptide Fragments pharmacology, Prions pharmacology, Tumor Necrosis Factor-alpha metabolism

Abstract

A synthetic peptide consisting of amino acid residues 106-126 of the human prion protein (PrP-(106--126)) has been previously demonstrated to be neurotoxic and to induce microglial activation. The present study investigated the expression of the inducible form of the nitric-oxide synthase (NOS-II) in human microglial cells treated with PrP-(106--126). Using reverse transcriptase-polymerase chain reaction, we found that PrP-(106--126) induces NOS-II gene expression after 24 h of treatment and that this effect is accompanied by a peak of nuclear factor kappa B (NF-kappa B) binding at 30 min as evaluated by electrophoretic mobility shift assay. Since our previous data demonstrated tumor necrosis factor-alpha (TNF-alpha) to be a potent inducer of NOS-II in these cells, we analyzed the expression of this cytokine in PrP-(106--126)-treated microglia. PrP-(106--126) caused the release of TNF-alpha as detected by enzyme-linked immunosorbent assay, and a blocking antibody, anti-TNF-alpha, abolished NOS-II induction elicited by this peptide. Moreover, PrP-(106-126) activates p38 mitogen-activated protein kinase, and the inhibition of this pathway determines the ablation of NF-kappa B binding induced by this fragment peptide.

Published

2001

5. A 7-kDa prion protein (PrP) fragment, an integral component of the PrP region required for infectivity, is the major amyloid protein in Gerstmann-Sträussler-Scheinker disease A117V.

Author

Tagliavini F, Lievens PM, Tranchant C, Warter JM, Mohr M, Giaccone G, Perini F, Rossi G, Salmona M, Piccardo P, Ghetti B, Beavis RC, Bugiani O, Frangione B, and Prelli F

Subjects

Adult, Alleles, Cerebral Cortex pathology, Gerstmann-Straussler-Scheinker Disease genetics, Heterozygote, Humans, Male, Methionine genetics, Prion Proteins, Prions isolation & purification, Sequence Analysis, Protein, Syndrome, Valine genetics, Amyloid genetics, Gerstmann-Straussler-Scheinker Disease etiology, Peptide Fragments isolation & purification, Prions pathogenicity, Protein Precursors genetics

Abstract

Gerstmann-Sträussler-Scheinker disease (GSS) is a cerebral amyloidosis associated with mutations in the prion protein (PrP) gene (PRNP). The aim of this study was to characterize amyloid peptides purified from brain tissue of a patient with the A117V mutation who was Met/Val heterozygous at codon 129, Val(129) being in coupling phase with mutant Val117. The major peptide extracted from amyloid fibrils was a approximately 7-kDa PrP fragment. Sequence analysis and mass spectrometry showed that this fragment had ragged N and C termini, starting mainly at Gly88 and Gly90 and ending with Arg148, Glu152, or Asn153. Only Val was present at positions 117 and 129, indicating that the amyloid protein originated from mutant PrP molecules. In addition to the approximately 7-kDa peptides, the amyloid fraction contained N- and C-terminal PrP fragments corresponding to residues 23-41, 191-205, and 217-228. Fibrillogenesis in vitro with synthetic peptides corresponding to PrP fragments extracted from brain tissue showed that peptide PrP-(85-148) readily assembled into amyloid fibrils. Peptide PrP-(191-205) also formed fibrillary structures although with different morphology, whereas peptides PrP-(23-41) and PrP-(217-228) did not. These findings suggest that the processing of mutant PrP isoforms associated with Gerstmann-Sträussler-Scheinker disease may occur extracellularly. It is conceivable that full-length PrP and/or large PrP peptides are deposited in the extracellular compartment, partially degraded by proteases and further digested by tissue endopeptidases, originating a approximately 7-kDa protease-resistant core that is similar in patients with different mutations. Furthermore, the present data suggest that C-terminal fragments of PrP may participate in amyloid formation.

Published

2001

6. Studies on peptide fragments of prion proteins.

Author

Tagliavini F, Forloni G, D'Ursi P, Bugiani O, and Salmona M

Subjects

Amino Acid Sequence, Animals, Caspases metabolism, Humans, Molecular Sequence Data, Neuroglia drug effects, Neuroglia metabolism, Peptide Fragments pharmacology, Prion Diseases etiology, Prions pharmacology, Protein Conformation, Protein Folding, Sequence Homology, Amino Acid, Peptide Fragments chemistry, Prions chemistry

Published

2001

7. Apoptotic cell death and impairment of L-type voltage-sensitive calcium channel activity in rat cerebellar granule cells treated with the prion protein fragment 106-126.

Author

Thellung S, Florio T, Villa V, Corsaro A, Arena S, Amico C, Robello M, Salmona M, Forloni G, Bugiani O, Tagliavini F, and Schettini G

Subjects

Animals, Apoptosis drug effects, Calcium Channel Blockers pharmacology, Calcium Channels, L-Type physiology, Cell Death drug effects, Cell Death physiology, Cells, Cultured, Cerebellum physiology, Neurons physiology, Nicardipine pharmacology, Rats, Rats, Sprague-Dawley, Apoptosis physiology, Calcium Channels, L-Type drug effects, Cerebellum drug effects, Neurons drug effects, Peptide Fragments pharmacology, Prions pharmacology

Abstract

Prion diseases are neurodegenerative pathologies characterized by the accumulation, in the brain, of altered forms of the prion protein (PrP), named PrP(Sc). A synthetic peptide homologous to residues 106-126 of PrP (PrP106-126) was reported to maintain the neurodegenerative characteristics of PrP(Sc). We investigated the intracellular mechanisms involved in PrP106-126-dependent degeneration of primary cultures of cerebellar granule neurons. Prolonged exposure of such neurons to PrP106-126 induced apoptotic cell death. The L-type voltage-sensitive calcium channel blocker nicardipine reproduced this effect, suggesting that blockade of Ca(2+) entry through this class of calcium channels may be responsible for the granule cell degeneration. Microfluorometric analysis showed that PrP106-126 caused a reduction in cytosolic calcium levels, elicited by depolarizing K(+) concentrations in these neurons. Electrophysiological studies demonstrated that PrP106-126 and nicardipine selectively reduce the L-type calcium channel current. These data demonstrate that PrP106-126 alters the activity of L-type voltage-sensitive calcium channels in rat cerebellar granule cells and suggest that this phenomenon is related to the cell death induced by the peptide., (Copyright 2000 Academic Press.)

Published

2000

8. Intracellular mechanisms mediating the neuronal death and astrogliosis induced by the prion protein fragment 106-126.

Author

Thellung S, Florio T, Corsaro A, Arena S, Merlino M, Salmona M, Tagliavini F, Bugiani O, Forloni G, and Schettini G

Subjects

Amino Acid Sequence, Animals, Astrocytes metabolism, Calcium metabolism, Calcium Channel Blockers pharmacology, Calcium Channels, L-Type metabolism, Cell Death drug effects, Cell Division physiology, Cell Line, Cerebral Cortex cytology, Creutzfeldt-Jakob Syndrome metabolism, DNA biosynthesis, Humans, In Situ Nick-End Labeling, Molecular Sequence Data, Neurons chemistry, Neurons metabolism, Nicardipine pharmacology, Peptide Fragments chemistry, Potassium Chloride pharmacology, Prions chemistry, Rats, Thymidine pharmacokinetics, Tritium, Astrocytes pathology, Cell Death physiology, Gliosis pathology, Neurons pathology, Peptide Fragments toxicity, Prions toxicity

Abstract

Prion encephalopathies include fatal diseases of the central nervous system of men and animals characterized by nerve cell loss, glial proliferation and deposition of amyloid fibrils into the brain. During these diseases a cellular glycoprotein (the prion protein, PrP(C)) is converted, through a not yet completely clear mechanism, in an altered isoform (the prion scrapie, PrP(Sc)) that accumulates within the brain tissue by virtue of its resistance to the intracellular catabolism. PrP(Sc) is believed to be responsible for the neuronal loss that is observed in the prion disease. The PrP 106-126, a synthetic peptide that has been obtained from the amyloidogenic portion of the prion protein, represents a suitable model for studying the pathogenic role of the PrP(Sc), retaining, in vitro, some characteristics of the entire protein, such as the capability to aggregate in fibrils, and the neurotoxicity. In this work we present the results we have recently obtained regarding the action of the PrP 106-126 in different cellular models. We report that the PrP 106-126 induces proliferation of cortical astrocytes, as well as degeneration of primary cultures of cortical neurons or of neuroectodermal stable cell lines (GH(3) cells). In particular, these two opposite effects are mediated by the same attitude of the peptide to interact with the L-type calcium channels: in the astrocytes, the activity of these channels seems to be activated by PrP 106-126, while, in the cortical neurons and in the GH(3) cells, the same treatment causes a blockade of these channels causing a toxic effect.

Published

2000

9. Comment on: Neurotoxicity of prion peptide 106-126 not confirmed, by Beat Kunz, Erika Sandmeier, Philipp Christen. FEBS Letters 485 (1999) 65-68.

Author

Forloni G, Salmona M, Bugiani O, and Tagliavini F

Subjects

Animals, Drug Contamination, Humans, Peptide Fragments chemistry, Peptide Fragments isolation & purification, Prions chemistry, Prions isolation & purification, Protein Conformation, Neurons drug effects, Peptide Fragments toxicity, Prions toxicity

Published

2000

10. Determination of solution conformations of PrP106-126, a neurotoxic fragment of prion protein, by 1H NMR and restrained molecular dynamics.

Author

Ragg E, Tagliavini F, Malesani P, Monticelli L, Bugiani O, Forloni G, and Salmona M

Subjects

Amino Acid Sequence, Animals, Dimethyl Sulfoxide, Humans, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Peptide Fragments genetics, Prions genetics, Protein Conformation, Protein Structure, Secondary, Solutions, Thermodynamics, Trifluoroethanol, Water, Peptide Fragments chemistry, Prions chemistry

Abstract

Experimental two-dimensional 1H NMR data have been obtained for PrP106-128 under the following solvent conditions: deionized water/2, 2,2-trifluoroethanol 50 : 50 (v/v) and dimethylsulfoxide. These data were analyzed by restrained molecular mechanics calculations to determine how changes in solvation affect the conformation of the peptide. In deionized water at pH 3.5, the peptide adopted a helical conformation in the hydrophobic region spanning residues Met112-Leu125, with the most populated helical region corresponding to the Ala115-Ala119 segment ( approximately 10%). In trifluoroethanol/H2O, the alpha-helix increased in population especially in the Gly119-Val122 tract ( approximately 25%). The conformation of this region was found to be remarkably sensitive to pH, as the Ala120-Gly124 tract shifted to an extended conformation at pH 7. In dimethylsulfoxide, the hydrophobic cluster adopted a prevalently extended conformation. For all tested solvents the region spanning residues Asn108-Met112 was present in a 'turn-like' conformation and included His111, situated just before the starting point of the alpha-helix. Rather than by conformational changes, the effect of His111 is exerted by changes in its hydrophobicity, triggering aggregation. The amphiphilic properties and the pH-dependent ionizable side-chain of His111 may thus be important for the modulation of the conformational mobility and heterogeneity of PrP106-126.

Published

1999

11. Molecular determinants of the physicochemical properties of a critical prion protein region comprising residues 106-126.

Author

Salmona M, Malesani P, De Gioia L, Gorla S, Bruschi M, Molinari A, Della Vedova F, Pedrotti B, Marrari MA, Awan T, Bugiani O, Forloni G, and Tagliavini F

Subjects

Amides metabolism, Amino Acid Sequence, Amino Acid Substitution, Animals, Astrocytes cytology, Astrocytes drug effects, Cell Division drug effects, Cell Survival drug effects, Cells, Cultured, Circular Dichroism, Gerstmann-Straussler-Scheinker Disease genetics, Humans, Hydrogen-Ion Concentration, Models, Molecular, Molecular Sequence Data, Neurons cytology, Neurons drug effects, Peptide Fragments genetics, Peptide Fragments pharmacology, Plaque, Amyloid metabolism, Plaque, Amyloid ultrastructure, Polymorphism, Genetic, Prions genetics, Prions pharmacology, Protein Binding, Protein Structure, Secondary, Rats, Static Electricity, Peptide Fragments chemistry, Peptide Fragments metabolism, Prions chemistry, Prions metabolism

Abstract

Prion diseases are marked by the cerebral accumulation of conformationally modified forms of the cellular prion protein (PrP(C)), known as PrP(res). The region comprising the residues 106-126 of human PrP seems to have a key role in this conformational conversion, because a synthetic peptide homologous with this sequence (PrP106-126) adopts different secondary structures in different environments. To investigate the molecular determinants of the physicochemical characteristics of PrP106-126, we synthesized a series of analogues including PrP106-126 H(D), PrP106-126 A and PrP106-126 K, with l-His-->d-His, His-->Ala and His-->Lys substitutions respectively at position 111, PrP106-126 NH(2) with amidation of the C-terminus, PrP106-126 V with an Ala-->Val substition at position 117, and PrP106-126 VNH(2) with an Ala-->Val substitution at position 117 and amidation of the C-terminus. The analysis of the secondary structure and aggregation properties of PrP106-126 and its analogues showed the following. (1) His(111) is central to the conformational changes of PrP peptides. (2) Amidation of the C-terminal Gly(126) yields a predominantly random coil structure, abolishes the molecular polymorphism and decreases the propensity of PrP106-126 to generate amyloid fibrils. (3) PrP106-126 V, carrying an Ala-->Val substitution at position 117, does not demonstrate a fibrillogenic ability superior to that of PrP106-126. However, the presence of Val at position 117 increases the aggregation properties of the amidated peptide. (4) Amyloid fibrils are not required for neurotoxicity because the effects of PrP106-126 NH(2) on primary neuronal cultures were similar to those of the wild-type sequence. Conversely, astroglial proliferation is related to the presence of amyloid fibrils, suggesting that astrogliosis in prion encephalopathies without amyloid deposits is a mediated effect rather than a direct effect of disease-specific PrP isoforms.

Published

1999

12. A betaPP peptide carboxyl-terminal to Abeta is neurotoxic.

Author

Marcon G, Giaccone G, Canciani B, Cajola L, Rossi G, De Gioia L, Salmona M, Bugiani O, and Tagliavini F

Subjects

Animals, Apoptosis, Cell Size drug effects, Cell Survival drug effects, Cells, Cultured, Dose-Response Relationship, Drug, Electrophoresis, Agar Gel, Fetus, Hippocampus drug effects, In Situ Nick-End Labeling, Microscopy, Electron, Mutagenesis, Site-Directed, Neurons cytology, Neurons metabolism, Rats, Amyloid beta-Protein Precursor pharmacology, Amyloid beta-Protein Precursor physiology, Neurons drug effects, Peptide Fragments pharmacology

Abstract

Extracellular Abeta-amyloid and intraneuronal paired helical filaments (PHFs) composed of tau protein are the neuropathological hallmark of Alzheimer's disease. Abeta is a 39- to 43-residue peptide derived by cleavage of a 695- to 770-amino-acid membrane-associate glycoprotein (termed beta-protein precursor, betaPP). Following the observation that an antiserum to an epitope located between residues 713 and 723 of betaPP770 (ie, the transmembrane region of the betaPP distal to Abeta) labels PHFs and that a synthetic peptide homologous to residues 713 to 730 of betaPP770 (betaPP713-730) is highly fibrillogenic and interacts with tau in vitro, it has been hypothesized that betaPP fragments other than Abeta may feature in the pathogenesis of Alzheimer's disease concurring with neuronal degeneration. To investigate this issue, we have analyzed the effects of the exposure of primary neuronal cultures to the synthetic peptide betaPP713-730. Cultures were prepared from rat hippocampus on embryonic day 17 and incubated with the peptide at 2.5 to 30 micromol/L concentration for 1 to 4 days. Cell viability was compared with that of control cultures exposed to a scrambled sequence of the peptide. A 4-day exposure to 20 micromol/L betaPP713-730 resulted in almost complete neuronal loss, whereas no changes were observed with the scrambled peptide. Degenerating neurons showed DNA fragmentation by agarose gel electrophoresis and apoptotic changes by light and electron microscopy. These findings support the view that betaPP sequences other than Abeta may play a role in nerve cell degeneration in Alzheimer's disease.

Published

1999

13. Activation of microglial cells by PrP and beta-amyloid fragments raises intracellular calcium through L-type voltage sensitive calcium channels.

Author

Silei V, Fabrizi C, Venturini G, Salmona M, Bugiani O, Tagliavini F, and Lauro GM

Subjects

Amino Acid Sequence, Amyloid beta-Peptides chemistry, Brain cytology, Brain drug effects, Brain embryology, Calcium Channel Blockers pharmacology, Humans, Membrane Potentials drug effects, Molecular Sequence Data, Amyloid beta-Peptides pharmacology, Calcium metabolism, Calcium Channels drug effects, Microglia drug effects, Peptide Fragments pharmacology, Prions pharmacology

Abstract

The prion protein (PrP) and the amyloid beta (Abeta) precursor protein (APP) are two normal proteins constitutively synthesised in human brain. An altered form of PrP accumulates in Creutzfeldt-Jakob disease, while Abeta is involved in the pathogenesis of Alzheimer's disease. Synthetic fragments of both proteins, PrP106-126 and beta25-35 (beta25-35), have been demonstrated to induce neurodegeneration and microglia activation. This study was undertaken to compare PrP106-126 and beta25-35 capability of activating human resting microglial cells. Our results show that both peptides are able to induce microglial activation and to elicit an increase in [Ca2+]i levels in cells loaded with calcium-green 1. Inhibitors of L-type voltage-sensitive calcium channels (verapamil, nifedipine and diltiazem) prevented the increase in [Ca2+]i concentration as observed after treatment with PrP106-126 and beta25-35, thus indicating a transmembrane calcium influx through these channels. In addition, verapamil abolished the proliferative effect of both PrP106-126 and beta25-35., (Copyright 1999 Elsevier Science B.V.)

Published

1999

14. Prion protein fragment 106-126 induces apoptotic cell death and impairment of L-type voltage-sensitive calcium channel activity in the GH3 cell line.

Author

Florio T, Thellung S, Amico C, Robello M, Salmona M, Bugiani O, Tagliavini F, Forloni G, and Schettini G

Subjects

Amino Acid Sequence, Animals, Cadmium pharmacology, Calcium metabolism, Calcium Channel Blockers pharmacology, Cell Survival drug effects, DNA Fragmentation drug effects, Dose-Response Relationship, Drug, Formazans, In Situ Nick-End Labeling, Membrane Potentials, Molecular Sequence Data, Nicardipine pharmacology, Pituitary Gland, Potassium pharmacology, PrPC Proteins genetics, PrPC Proteins metabolism, Rats, Reverse Transcriptase Polymerase Chain Reaction, Tetrazolium Salts, Tumor Cells, Cultured, Apoptosis, Calcium Channels metabolism, Peptide Fragments pharmacology, Prions pharmacology

Abstract

The prion diseases are transmissible neurodegenerative pathologies characterized by the accumulation of altered forms of the prion protein (PrP), termed PrP(Sc), in the brain. Previous studies have shown that a synthetic peptide homologous to residues 106-126 of PrP (PrP 106-126) maintains many characteristics of PrP(Sc), i.e., the ability to form amyloid fibrils and to induce apoptosis in neurons. We have investigated the intracellular mechanisms involved in the cellular degeneration induced by PrP 106-126, using the GH3 cells as a model of excitable cells. When assayed in serum-deprived conditions (48 hr), PrP 106-126 (50 microM) induced cell death time-dependently, and this process showed the characteristics of the apoptosis. This effect was specific because a peptide with a scrambled sequence of PrP 106-126 was not effective. Then we performed microfluorimetric analysis of single cells to monitor intracellular calcium concentrations and showed that PrP 106-126 caused a complete blockade of the increase in the cytosolic calcium levels induced by K+ (40 mM) depolarization. Conversely, the scrambled peptide was ineffective. The L-type voltage-sensitive calcium channel blocker nicardipine (1 microM) also induced apoptosis in GH3 cells, suggesting that the blockade of Ca2+ entry through this class of calcium channels may cause GH3 apoptotic cell death. We thus analyzed, by means of electrophysiological studies, whether Prp 106-126 modulate L-type calcium channels activity and demonstrated that the apoptotic effect of PrP 106-126 was due to a dose-dependent inactivation of the L-type calcium channels. These data demonstrate that the prion protein fragment 106-126 induces a GH3 apoptotic cell death inducing a selective inhibition of the activity of the L-type voltage-sensitive calcium channels.

Published

1998

15. A neurotoxic and gliotrophic fragment of the prion protein increases plasma membrane microviscosity.

Author

Salmona M, Forloni G, Diomede L, Algeri M, De Gioia L, Angeretti N, Giaccone G, Tagliavini F, and Bugiani O

Subjects

Amino Acid Sequence, Animals, Cell Line, Cell Membrane ultrastructure, HL-60 Cells, Humans, Kinetics, Lipid Bilayers, Liposomes, Mice, Molecular Sequence Data, Peptide Fragments chemistry, Prions chemistry, Rats, Tumor Cells, Cultured, Viscosity, Cell Membrane drug effects, Neurotoxins, Peptide Fragments toxicity, Prions toxicity

Abstract

Prion-related encephalopathies are characterized by astrogliosis and nerve cell degeneration and loss. These lesions might be the consequence of an interaction between the abnormal isoform of the cellular prion protein that accumulates in nervous tissue and the plasma membranes. Previously we found that a synthetic peptide, homologous to residues 106-126 of the human prion protein, is fibrillogenic and toxic to neurons and trophic to astrocytes in vitro. This study dealt with the ability of the peptide to interact with membranes. Accordingly, we compared PrP 106-126 with different synthetic PrP peptides (PrP 89-106, PrP 127-147, a peptide with a scrambled sequences of 106-126, and PrP 106-126 amidated at the C-terminus) as to the ability to increase the microviscosity of artificial and natural membranes. The first three had no effect on nerve and glial cells in vitro, whereas the amidated peptide caused neuronal death. Using a fluorescent probe that becomes incorporated into the hydrocarbon core of the lipid bilayer and records the lipid fluidity, we found PrP 106-126 able to increase significantly the membrane microviscosity of liposomes and of all cell lines investigated. This phenomenon was associated with the distribution of the peptide over the cell surface, but not with changes in the membrane lipid or protein content, or with membrane lipid phase transitions. Accordingly, we deduced that increased membrane microviscosity was unrelated to changes in the membrane native components and was the result of increased lipid density following PrP 106-126 embedding into the lipid bilayer. No control peptides had comparable effects on the membrane microviscosity, except PrP 106-126 amidated at the C-terminus. Since the latter was as neurotoxic, but not as fibrillogenic, as PrP 106-126, we argued that the ability of PrP 106-126 to increase membrane microviscosity was unrelated to the propensity of the peptide to raise fibrils. Rather, it could be connected with the primary structure of PrP 106-126, characterized by two opposing regions, one hydrophilic and the other hydrophobic, that enabled the peptide to interact with the lipid bilayer. Based on these findings, we speculated that the glial and nerve cell involvement occurring in prion-related encephalopathies might be caused by the interaction with the plasma membrane of a PrP 106-126-like fragment or of the sequence spanning residues 106-126 of the abnormal isoform of the prion protein.

Published

1997

16. Activation effects of a prion protein fragment [PrP-(106-126)] on human leucocytes.

Author

Diomede L, Sozzani S, Luini W, Algeri M, De Gioia L, Chiesa R, Lievens PM, Bugiani O, Forloni G, Tagliavini F, and Salmona M

Subjects

Amino Acid Sequence, Calcium blood, Cell Membrane drug effects, Cell Membrane physiology, DNA Primers, Humans, Kinetics, Leukocytes drug effects, Lymphocytes physiology, Molecular Sequence Data, Monocytes physiology, Neutrophils physiology, Polymerase Chain Reaction, Prions blood, Superoxides blood, Actins biosynthesis, Chemotaxis, Leukocyte drug effects, Leukocytes physiology, Peptide Fragments pharmacology, Prions biosynthesis, Prions pharmacology, Transcription, Genetic drug effects

Abstract

Prion-related encephalopathies are characterized by the intracerebral accumulation of an abnormal isoform of the cellular prion protein (PrPC) named scrapie prion protein (PrPSc). The pathological forms of this protein and its cellular precursor are not only expressed in the brain but also, at lower concentrations, in peripheral tissues. We recently showed that a synthetic peptide corresponding to residues 106-126 [PrP-(106-126)] of the human PrP is toxic to neurons and trophic to astrocytes in vitro. Our experiments were aimed at verifying whether PrP-(106-126) and other peptides corresponding to fragments of the amyloid protein purified from brains of patients with Gerstmann-Sträussler-Scheinker disease-namely PrP-(89-106), PrP-(106-114), PrP-(127-147)-were capable of stimulating circulating leucocytes. Native PrP expression in human lymphocytes, monocytes and neutrophils was first confirmed using PCR amplification of total RNA, after reverse transcription, and immunoblot analysis of cell extracts with anti-PrP antibodies. PrP-(106-126), but not the other peptides, increased membrane microviscosity, intracellular Ca2+ concentration and cell migration in circulating leucocytes, and O2-. production in monocytes and neutrophils. Membrane microviscosity was determined by the fluorescence polarization technique, using diphenylhexatriene as a probe, 300 s after the addition of PrP-(106-126) to the cell suspension in the concentration range 5-50 microM. The increase in intracellular Ca2+ elicited by PrP-(106-126) was dose-dependent in the range 5-500 microM. PrP-(106-126) stimulated O2-. production in monocytes and neutrophils in a dose- (10-300 microM) and time-(5-30 min) dependent manner in the presence of 10 microM dihydrocytochalasin B. Both the increase in Ca2+ concentration and the O2-. production were partially sensitive to pertussis toxin. PrP-(106-126) stimulated leucocyte migration in a dose-dependent (30-300 microM) manner and, at the highest concentration used, this migration was comparable with that elicited by 2.5 nM interleukin 8 or 10 nM fMet-Leu-Phe peptide.

Published

1996

17. Intracellular calcium rise through L-type calcium channels, as molecular mechanism for prion protein fragment 106-126-induced astroglial proliferation.

Author

Florio T, Grimaldi M, Scorziello A, Salmona M, Bugiani O, Tagliavini F, Forloni G, and Schettini G

Subjects

Amino Acid Sequence, Animals, Astrocytes cytology, Astrocytes physiology, Binding, Competitive, Calcium Channel Blockers pharmacology, Calcium Channels drug effects, Calcium Channels, L-Type, Cell Division drug effects, Cells, Cultured, DNA biosynthesis, Isradipine metabolism, Kinetics, Molecular Sequence Data, Nicardipine pharmacology, Peptide Fragments chemical synthesis, Peptides chemical synthesis, Peptides pharmacology, Prions chemical synthesis, Rats, Thymidine metabolism, Time Factors, Astrocytes drug effects, Calcium metabolism, Calcium Channels physiology, Cerebral Cortex cytology, Peptide Fragments pharmacology, Prions pharmacology

Abstract

The infectious prion protein (PrPSc) is the etiologic agent of transmissible neurodegenerative conditions such as scrapie or Creutzfeldt-Jakob disease. Its fragment 106-126 (PrP106-126) has been reported to maintain most of the pathological features of PrPSc. We report here the intracellular mechanisms mediating the proliferative effects of PrP106-126 on rat cortical type I astrocytes. The proliferative effects of PrP106-126 started after 24h of treatment and lasted up to 9 days and was antagonized by the L-type voltage-sensitive calcium channel blocker nicardipine. Microfluorimetric studies showed that PrP106-126 caused a rapid increase in the [Ca+2]i. This effect was prevented by nicardipine, or by Ca(+2)-free conditions, showing that the PrP106-126 enhances [Ca+2]i mobilizing Ca+2 from the extracellular environment. Moreover, binding studies demonstrated a direct interference of PrP106-126 with the dihydropyridine binding site. This is the first evidence that a prion protein fragment directly stimulates the proliferation of astrocytes via an increase in [Ca+2]i through the L-type voltage-sensitive calcium channels.

Published

1996

18. Apoptosis-mediated neurotoxicity induced by beta-amyloid and PrP fragments.

Author

Forloni G, Bugiani O, Tagliavini F, and Salmona M

Subjects

Alzheimer Disease pathology, Animals, Apoptosis drug effects, Cell Death drug effects, Cells, Cultured, Fetus, Humans, Neurons cytology, Neurons pathology, Proto-Oncogenes drug effects, RNA, Messenger biosynthesis, Rats, Transcription, Genetic drug effects, Amyloid beta-Peptides toxicity, Hippocampus cytology, Neurons drug effects, Neurotoxins toxicity, Peptide Fragments toxicity, Prions toxicity

Abstract

The neurotoxic activity of beta-amyloid (beta A) and prion protein (PrP) fragments contributed to the hypothesis concerning a causal role of amyloid deposits in Alzheimer disease (AD) and in prion-related encephalopathies. In this study, we investigated some aspects of the molecular mechanisms associated with neurotoxic activity of synthetic peptides homologous to beta A (beta 25-35) or PrP (PrP106-126) fragments. Chronic (5-7 d) exposure to both peptides induced neuronal death by apoptosis, as suggested by biochemical and morphological analysis. The apoptotic mechanism was confirmed by ultrastructural examination. The intracellular cascade of events activated by peptides was investigated by Northern blot and PCR analysis of expression of early genes (c-fos, c-jun, c-myc) and other proteins (p53, SGP-2 bcl-2, HSP70, Ich-1) potentially involved in apoptosis. With the exception of bcl-2 mRNA decrease and a slight increase of SGP-2 in PrP106-126-treated cells, no consistent alterations of these mRNA expressions were found in neuronal cells exposed to beta 25-35 or PrP106-126. Furthermore, we synthesized amidated homologs of both peptides with low amyloidogenic activity to test directly the relationship between amyloid fibrils and cell death. The neurotoxicity exhibited by PrP106-126-NH2 was similar to that observed with original peptide, whereas the amidation of beta 25-35 partially reduced the neurotoxicity of this peptide.

Published

1996

19. Conformational polymorphism of the amyloidogenic and neurotoxic peptide homologous to residues 106-126 of the prion protein.

Author

De Gioia L, Selvaggini C, Ghibaudi E, Diomede L, Bugiani O, Forloni G, Tagliavini F, and Salmona M

Subjects

Amino Acid Sequence, Circular Dichroism, Humans, Liposomes, Molecular Sequence Data, Peptides chemical synthesis, Peptides chemistry, PrPSc Proteins, Neurotoxins chemistry, Peptide Fragments chemistry, Prions chemistry, Protein Conformation, Protein Structure, Secondary

Abstract

Prion-related encephalopathies are characterized by cerebral accumulation of a post-translationally modified form of the cellular prion protein (PrPC), designated PrPSc. Evidence suggests that the conversion from PrPC to PrPSc involves changes in the secondary structure leading to an increase in beta-sheet content. We have previously shown that a synthetic peptide homologous to residues 106-126 of human PrP, belonging to a predicted alpha-helical domain, exhibits a beta-sheet conformation, forms amyloid-like fibrils, and is neurotoxic in vitro. The present study investigated how different chemicophysical conditions such as pH and ionic strength or a membrane-like environment influenced the secondary structure of this peptide. PrP 106-126 exhibited a predominantly beta-sheet structure in 200 mM phosphate buffer, pH 5.0, but a combination of beta-sheet and random coil structure in 200 mM phosphate buffer, pH 7.0, or in deionized water. The addition of trifluoroethanol (50% final concentration) to solutions of peptide in deionized water induced the appearance of an alpha-helical secondary structure, but did not modify the beta-sheet conformation of the peptide dissolved in 200 mM phosphate buffer, pH 5.0. In the presence of micelles formed by a 5% solution of sodium dodecyl sulfate, PrP 106-126 showed a high content of alpha-helix. When the peptide was dissolved in 5 mM phosphate buffer, pH 7.4, and incubated with liposomes, it changed from a prevalently random coil structure to a beta-sheet conformation. The environment-dependent conformational polymorphism of PrP 106-126 and its marked tendency to form stable beta-sheet structures at acidic pH could account for the shift from alpha-helix to beta-sheet associated with the conversion of PrPC to PrPSc, which occurs most likely in the endosomal-lysosomal compartment.

Published

1994

20. Molecular characteristics of a protease-resistant, amyloidogenic and neurotoxic peptide homologous to residues 106-126 of the prion protein.

Author

Selvaggini C, De Gioia L, Cantù L, Ghibaudi E, Diomede L, Passerini F, Forloni G, Bugiani O, Tagliavini F, and Salmona M

Subjects

Amino Acid Sequence, Circular Dichroism, Endopeptidase K, Humans, Molecular Conformation, Molecular Sequence Data, PrPSc Proteins, Pronase metabolism, Protein Structure, Secondary, Sequence Homology, Amino Acid, Serine Endopeptidases metabolism, Solubility, Nerve Tissue Proteins chemistry, Peptide Fragments chemistry, Peptide Fragments metabolism, Prions chemistry, Prions metabolism

Abstract

In the prion-related encephalopathies the prion protein is converted to an altered form, known as PrPSc, that is partially resistant to protease digestion. This abnormal isoform accumulates in the brain and its protease-resistant core aggregates extracellularly into amyloid fibrils. We have investigated the conformational properties, aggregation behaviour and sensitivity to protease digestion of a synthetic peptide homologous to residues 106-126 of human PrP, which was previously found to form amyloid-like fibrils in vitro and displayed neurotoxic activity toward primary cultures of rat hippocampal neurons. A scrambled sequence of peptide PrP 106-126 was used as a control. By circular dichroism, PrP 106-126 exhibited a secondary structure composed largely of beta-sheet, whereas the scrambled sequence of PrP 106-126 showed a random coil structure. The beta-sheet content of PrP 106-126 was much higher in 200 mM phosphate buffer at pH 5.0 than in the same buffer at pH 7.0. Laser light scattering analysis showed that PrP 106-126 aggregated immediately after dissolution in 20 mM or 200 mM phosphate buffer, pH 5.0 and 7.0, whereas scrambled PrP 106-126 did not. PrP 106-126 aggregates had an average hydrodinamic diameter of 100 nm and an average molecular weight of 12 x 10(6) +/- 30% Daltons, corresponding to the aggregation of 6000 +/- 30% molecules. Peptide PrP 106-126 showed partial resistance to digestion with Proteinase K and Pronase, whereas scrambled PrP 106-126 was completely degraded by incubation with the enzymes at 37 degrees C for 30 minutes.

Published

1993

21. Neurotoxicity of a prion protein fragment.

Author

Forloni G, Angeretti N, Chiesa R, Monzani E, Salmona M, Bugiani O, and Tagliavini F

Subjects

Amino Acid Sequence, Animals, Apoptosis, Cells, Cultured, Dose-Response Relationship, Drug, Hippocampus cytology, Hippocampus metabolism, Molecular Sequence Data, Peptide Fragments genetics, Rats, Neurons drug effects, Peptide Fragments toxicity, Prions toxicity

Abstract

The cellular prion protein (PrPC) is a sialoglycoprotein of M(r) 33-35K that is expressed predominantly in neurons. In transmissible and genetic neurodegenerative disorders such as scrapie of sheep, spongiform encephalopathy of cattle and Creutzfeldt-Jakob or Gerstmann-Sträussler-Scheinker diseases of humans, PrPC is converted into an altered form (termed PrPSc) which is distinguishable from its normal homologue by its relative resistance to protease digestion. PrPSc accumulates in the central nervous system of affected individuals, and its protease-resistant core aggregates extracellularly into amyloid fibrils. The process is accompanied by nerve cell loss, whose pathogenesis and molecular basis are not understood. We report here that neuronal death results from chronic exposure of primary rat hippocampal cultures to micromolar concentrations of a peptide corresponding to residues 106-126 of the amino-acid sequence deduced from human PrP complementary DNA. DNA fragmentation of degenerating neurons indicates that cell death occurred by apoptosis. The PrP peptide 106-126 has a high intrinsic ability to polymerize into amyloid-like fibrils in vitro. These findings indicate that cerebral accumulation of PrPSc and its degradation products may play a role in the nerve cell degeneration that occurs in prion-related encephalopathies.

Published

1993

22. Hereditary cerebral hemorrhage with amyloidosis associated with the E693K mutation of APP

Author

Giuseppe Di Fede, Mauro Magoni, Michela Morbin, Fabrizio Tagliavini, Giulia Mazzoleni, Giacomina Rossi, Gianfranco Puoti, Michela Mangieri, Alessandro Padovani, Andrea Salmaggi, Giorgio M. Patruno, Raffaella Capobianco, Alessandro Romorini, Francesco Carella, Chiara Cupidi, Orso Bugiani, Gabriella Marcon, Alberto Bizzi, Annarita Giovagnoli, Giorgio Giaccone, Bugiani, O, Giaccone, G, Rossi, G, Mangieri, M, Capobianco, R, Morbin, M, Mazzoleni, G, Cupidi, C, Marcon, Gabriella, Giovagnoli, A, Bizzi, A, DI FEDE, G, Puoti, G, Carella, F, Salmaggi, A, Romorini, A, Patruno, Gm, Magoni, M, Padovani, A, and Tagliavini, F.

Subjects

Male, Pathology, medicine.medical_specialty, Subarachnoid hemorrhage, Genotype, Apolipoprotein E4, Glutamic Acid, Neuropathology, Amyloid beta-Protein Precursor, Gene Frequency, Arts and Humanities (miscellaneous), medicine, Humans, Genetic Predisposition to Disease, Cognitive decline, Aged, Cerebral Hemorrhage, Family Health, Amyloid beta-Peptides, business.industry, Lysine, Amyloidosis, Leukoaraiosis, Autosomal dominant trait, Middle Aged, medicine.disease, Magnetic Resonance Imaging, Peptide Fragments, Italy, Hemosiderin, Mutation, Hereditary cerebral hemorrhage with amyloidosis, Female, Neurology (clinical), business, Amyloidosis, Familial, Genome-Wide Association Study

Abstract

Objective To report the clinical, genetic, neuroimaging, and neuropathologic studies of patients with the hereditary cerebral hemorrhage with amyloidosis linked to the APP E693K mutation. Design Case series. Clinical details and laboratory results were collected by direct evaluation and previous medical records. DNA analysis was carried out in several affected subjects and healthy individuals. Neuropathologic examination was performed in 2 subjects. Setting Southern Lombardy, Italy. Patients Individuals with and without amyloidosis in 4 unrelated Italian families (N = 37). Main Outcome Measure Genotype-phenotype relationship. Results The affected individuals presented with recurrent headache and multiple strokes, followed by epilepsy and cognitive decline in most of them. The disease was inherited with an autosomal dominant trait and segregated with the APP E693K mutation. Neuroimaging demonstrated small to large hematomas, subarachnoid bleeding, scars with hemosiderin deposits, small infarcts, and leukoaraiosis. Amyloid-β immunoreactivity was detected in the wall of leptomeningeal and parenchymal vessels and in the neuropil, whereas phosphorylated tau, neurofibrillary changes, and neuritic plaques were absent. Conclusions These findings expand the number of APP mutations linked to hereditary cerebral hemorrhage with amyloidosis, reinforcing the link between this phenotype and codon 693 of APP .

Published

2010