Your search keyword '"Cubellis, MARIA VITTORIA"' showing total 36 results

1. Therapy of Fabry disease with pharmacological chaperones: from in silico predictions to in vitro tests

Author

Cammisa Marco, Orlando Pierangelo, De Crescenzo Agostina, Citro Valentina, Andreotti Giuseppina, Correra Antonella, and Cubellis Maria Vittoria

Subjects

Medicine

Abstract

Abstract Background Fabry disease is a rare disorder caused by a large variety of mutations in the gene encoding lysosomal alpha-galactosidase. Many of these mutations are unique to individual families. Fabry disease can be treated with enzyme replacement therapy, but a promising novel strategy relies on small molecules, so called "pharmacological chaperones", which can be administered orally. Unfortunately only 42% of genotypes respond to pharmacological chaperones. Results A procedure to predict which genotypes responsive to pharmacological chaperones in Fabry disease has been recently proposed. The method uses a position-specific substitution matrix to score the mutations. Using this method, we have screened public databases for predictable responsive cases and selected nine representative mutations as yet untested with pharmacological chaperones. Mutant lysosomal alpha galactosidases were produced by site directed mutagenesis and expressed in mammalian cells. Seven out of nine mutations responded to pharmacological chaperones. Nineteen other mutations that were tested with pharmacological chaperones, but were not included in the training of the predictive method, were gathered from literature and analyzed in silico. In this set all five mutations predicted to be positive were responsive to pharmacological chaperones, bringing the percentage of responsive mutations among those predicted to be positive and not used to train the classifier to 86% (12/14). This figure differs significantly from the percentage of responsive cases observed among all the Fabry mutants tested so far. Conclusions In this paper we provide experimental support to an "in silico" method designed to predict missense mutations in the gene encoding lysosomal alpha galactosidase responsive to pharmacological chaperones. We demonstrated that responsive mutations can be predicted with a low percentage of false positive cases. Most of the mutations tested to validate the method were described in the literature as associated to classic or mild classic phenotype. The analysis can provide a guideline for the therapy with pharmacological chaperones supported by experimental results obtained in vitro. We are aware that our results were obtained in vitro and cannot be translated straightforwardly into benefit for patients, but need to be validated by clinical trials.

Published

2011

2. (Epi)genotype-phenotype correlations in Beckwith-Wiedemann syndrome

Author

Giuseppina Baldassarre, Luigi Tarani, Agostina De Crescenzo, Maria Vittoria Cubellis, Silvia Maitz, Maria Francesca Bedeschi, Margherita Silengo, Andrea Freschi, Marina Macchiaiolo, Cristina Molinatto, Silvia Russo, Donatella Milani, Luciano Calzari, Andrea Riccio, Milena Mariani, Giovanni Battista Ferrero, Andrea Bartuli, Lidia Larizza, Daniela Melis, Angelo Selicorni, Alessandro Mussa, A., Mussa, S., Russo, A. D., Crescenzo, A., Freschi, L., Calzari, S., Maitz, M., Macchiaiolo, C., Molinatto, G., Baldassarre, M., Mariani, L., Tarani, M. F., Bedeschi, D., Milani, D., Meli, A., Bartuli, Cubellis, MARIA VITTORIA, A., Selicorni, M. C., Silengo, L., Larizza, A., Riccio, G. B., Ferrero, Mussa, Alessandro, Russo, Silvia, de Crescenzo, Agostina, Freschi, Andrea, Calzari, Luciano, Maitz, Silvia, Macchiaiolo, Marina, Molinatto, Cristina, Baldassarre, Giuseppina, Mariani, Milena, Tarani, Luigi, Bedeschi, Maria Francesca, Milani, Donatella, Melis, Daniela, Bartuli, Andrea, Cubellis, Maria Vittoria, Selicorni, Angelo, Cirillo Silengo, Margherita, Larizza, Lidia, Riccio, Andrea, and Ferrero, Giovanni Battista

Subjects

Male, 0301 basic medicine, Hepatoblastoma, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Beckwith-Wiedemann Syndrome, Genotype, Beckwith–Wiedemann syndrome, genotype-phenotype correlation, 030105 genetics & heredity, Biology, Gastroenterology, Article, Chromosomes, Organomegaly, Genomic Imprinting, 03 medical and health sciences, paternal uniparental disonomy, assisted reproductive technology, Neoplasms, Internal medicine, Genetics, medicine, Macroglossia, Humans, Pair 11, Cyclin-Dependent Kinase Inhibitor p57, Genetic Association Studies, Genetics (clinical), Chromosomes, Human, Pair 11, Cytogenetics, DNA Methylation, Female, Phenotype, medicine.disease, Chromosomal region, Nevus flammeus, medicine.symptom, Human

Abstract

Beckwith-Wiedemann syndrome (BWS) is characterized by cancer predisposition, overgrowth and highly variable association of macroglossia, abdominal wall defects, nephrourological anomalies, nevus flammeus, ear malformations, hypoglycemia, hemihyperplasia, and organomegaly. BWS molecular defects, causing alteration of expression or activity of the genes regulated by two imprinting centres (IC) in the 11p15 chromosomal region, are also heterogeneous. In this paper we define (epi)genotype-phenotype correlations in molecularly confirmed BWS patients. The characteristics of 318 BWS patients with proven molecular defect were compared among the main four molecular subclasses: IC2 loss of methylation (IC2-LoM, n=190), IC1 gain of methylation (IC1-GoM, n=31), chromosome 11p15 paternal uniparental disomy (UPD, n=87), and cyclin-dependent kinase inhibitor 1C gene (CDKN1C) variants (n=10). A characteristic growth pattern was found in each group; neonatal macrosomia was almost constant in IC1-GoM, postnatal overgrowth in IC2-LoM, and hemihyperplasia more common in UPD (P

Published

2015

3. A splicing mutation of the HMGA2 gene is associated with Silver-Russell syndrome phenotype

Author

Massimo Carella, Orazio Palumbo, Agostina De Crescenzo, Andrea Riccio, Maria Vittoria Cubellis, Andrea Freschi, Angela Sparago, Flavia Cerrato, Maria Luigia Cavaliere, Pia Castelluccio, Valentina Citro, De Crescenzo, Agostina, Citro, Valentina, Freschi, Andrea, Sparago, Angela, Palumbo, Orazio, Cubellis, Maria Vittoria, Carella, Massimo, Castelluccio, Pia, Cavaliere, Maria Luigia, Cerrato, Flavia, Riccio, Andrea, A. D., Crescenzo, V., Citro, A., Freschi, A., Sparago, O., Palumbo, Cubellis, MARIA VITTORIA, M., Carella, P., Castelluccio, M. L., Cavaliere, F., Cerrato, and A., Riccio

Subjects

DNA Mutational Analysis, Biology, HMGA2, parasitic diseases, medicine, Genetics, Humans, Gene, Genetic Association Studies, Genetics (clinical), Sequence Deletion, Base Sequence, Silver–Russell syndrome, HMGA2 Protein, medicine.disease, Phenotype, Pedigree, Silver-Russell Syndrome, Case-Control Studies, Child, Preschool, RNA splicing, Mutation (genetic algorithm), biology.protein, Female, RNA Splice Sites

Abstract

Silver-Russell syndrome (SRS) is a heterogeneous disorder characterized by intrauterine and post-natal growth retardation, dysmorphic facial features and body asymmetry. About 50% of the patients carry (epi)genetic alterations involving chromosomes 7 or 11.The high proportion of patients with unidentified molecular etiology suggests the involvement of other genes. Interestingly, SRS patients share clinical features with the 12q14 microdeletion syndrome, characterized by several deletions with a 2.6 Mb region of overlap. Among the genes present in this interval, high mobility AT-hook 2 (HMGA2) appears to be the most likely cause of the growth deficiency, due to its described growth control function. To define the role of HMGA2 in SRS, we looked for 12q14 chromosome imbalances and HMGA2 mutations in a cohort of 45 patients with growth retardation and SRS-like phenotype but no 11p15 (epi)mutations or maternal uniparental disomy of chromosome 7 (matUPD7). We identified a novel 7 bp intronic deletion in HMGA2 present in heterozygosity in the proband and her mother both displaying the typical features of SRS. We demonstrated that the deletion affected normal splicing, indicating that it is a likely cause of HMGA2 deficiency. This study provides the first evidence that a loss-of-function mutation of HMGA2 can be associated with a familial form of SRS. We suggest that HMGA2 mutations leading to haploinsufficiency should be investigated in the SRS patients negative for the typical 11p15 (epi)mutations and matUPD7.

Published

2015

4. D2A-Ala peptide derived from the urokinase receptor exerts anti-tumoural effects in vitro and in vivo

Author

Marco Archinti, Gabriele Eden, Maria Vittoria Cubellis, Ralitsa Arnaudova, Valentina Citro, Giuseppina Andreotti, Federico Furlan, Bernard Degryse, Andrea Motta, Furlan, Federico, Eden, Gabriele, Archinti, Marco, Arnaudova, Ralitsa, Andreotti, Giuseppina, Citro, Valentina, Cubellis, Maria Vittoria, Motta, Andrea, and Degryse, Bernard

Subjects

0301 basic medicine, Physiology, Fibrosarcoma, Mice, Nude, Antineoplastic Agents, Peptide, Biochemistry, Receptors, Urokinase Plasminogen Activator, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, EGF receptor, Endocrinology, In vivo, medicine, Animals, Humans, Neoplasm Invasiveness, Cell migration, Receptor, Cell proliferation, Cancer, chemistry.chemical_classification, Adenosarcoma, Cell growth, Chemotaxis, Tumour growth, medicine.disease, Xenograft Model Antitumor Assays, In vitro, Urokinase receptor, 030104 developmental biology, tumor growth, chemistry, 030220 oncology & carcinogenesis, PEGylation, Cancer research, Female, Colorectal Neoplasms, HT29 Cells, Oligopeptides

Abstract

D2A-Ala is a synthetic peptide that has been created by introducing mutations in the original D2A sequence, 130 IQEGEEGRPKDDR 142 of human urokinase receptor (uPAR). In vitro, D2A-Ala peptide displays strong anti- tumoural properties inhibiting EGF-induced chemotaxis, invasion and proliferation of a human fi brosarcoma cell line, HT 1080, and a human colorectal adenocarcinoma cell line, HT 29. D2A-Ala exerts its e ff ects by preventing EGF receptor (EGFR) phosphorylation. To test D2A-Ala in vivo, this peptide was PEGylated generating polyethyleneglycol (PEG)-D2A-Ala peptide. PEGylation did not alter the inhibitory properties of D2A-Ala. Human tumour xenografts in the immunode fi cient nude mice using HT 1080 and HT 29 cell lines showed that PEG-D2A-Ala signi fi cantly prevents tumour growth decreasing size, weight and density of tumours. The most e ffi cient doses of the peptide were 5 and 10 mg/kg, thereby relevant for possible development of the peptide into a drug against cancer in particular tumours ex- pressing EGFR.

Published

2018

5. The Large Phenotypic Spectrum of Fabry Disease Requires Graduated Diagnosis and Personalized Therapy: A Meta-Analysis Can Help to Differentiate Missense Mutations

Author

Valentina Citro 1, Marco Cammisa 2, Ludovica Liguori 3, Chiara Cimmaruta 1, 3, Jan Lukas 4, Maria Vittoria Cubellis 1, Giuseppina Andreotti 3, Citro, Valentina, Cammisa, Marco, Liguori, Ludovica, Cimmaruta, Chiara, Lukas, Jan, Cubellis, MARIA VITTORIA, and Andreotti, Giuseppina

Subjects

0301 basic medicine, Fabry disease/drug therapy, Mutant, Mutation, Missense, Bioinformatics, Catalysis, Article, α-galactosidase, pharmacological chaperones, 1-deoxynojirimycin, Inorganic Chemistry, Small Molecule Libraries, lcsh:Chemistry, 03 medical and health sciences, ?-galactosidase, Genotype, medicine, Missense mutation, Humans, Physical and Theoretical Chemistry, Precision Medicine, Molecular Biology, lcsh:QH301-705.5, Spectroscopy, Genetics, biology, business.industry, Organic Chemistry, General Medicine, Transfection, medicine.disease, Phenotype, Fabry disease, In vitro, Computer Science Applications, pharmacological chaperone, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Chaperone (protein), alpha-Galactosidase, biology.protein, Fabry Disease, business, Molecular Chaperones

Abstract

Fabry disease is caused by mutations in the GLA gene and is characterized by a large genotypic and phenotypic spectrum. Missense mutations pose a special problem for graduating diagnosis and choosing a cost-effective therapy. Some mutants retain enzymatic activity, but are less stable than the wild type protein. These mutants can be stabilized by small molecules which are defined as pharmacological chaperones. The first chaperone to reach clinical trial is 1-deoxygalactonojirimycin, but others have been tested in vitro. Residual activity of GLA mutants has been measured in the presence or absence of pharmacological chaperones by several authors. Data obtained from transfected cells correlate with those obtained in cells derived from patients, regardless of whether 1-deoxygalactonojirimycin was present or not. The extent to which missense mutations respond to 1-deoxygalactonojirimycin is variable and a reference table of the results obtained by independent groups that is provided with this paper can facilitate the choice of eligible patients. A review of other pharmacological chaperones is provided as well. Frequent mutations can have residual activity as low as one-fourth of normal enzyme in vitro. The reference table with residual activity of the mutants facilitates the identification of non-pathological variants.

Published

2016

6. Identification of an Allosteric Binding Site on Human Lysosomal Alpha-Galactosidase Opens the Way to New Pharmacological Chaperones for Fabry Disease

Author

Horacio Pérez-Sánchez, Ludovica Liguori, Rosita Del Prete, Jan Lukas, Valentina Citro, Giuseppina Andreotti, Maria Vittoria Cubellis, Chiara Cimmaruta, Helena den-Haan, Jorge Peña-García, Citro, Valentina, Peña García, Jorge, den Haan, Helena, Pérez Sánchez, Horacio, Del Prete, Rosita, Liguori, Ludovica, Cimmaruta, Chiara, Lukas, Jan, Cubellis, MARIA VITTORIA, and Andreotti, Giuseppina

Subjects

0301 basic medicine, Luminescence, Missense Mutations, Mutant, High Performance Computing, lcsh:Medicine, Chaperone, medicine.disease_cause, Biochemistry, 1- deoxygalactonojirimycin, silico docking, allosteric hot-spot, 0302 clinical medicine, Computational Chemistry, Catalytic Domain, Drug Discovery, Chlorocebus aethiops, Medicine and Health Sciences, Urea, Drug Interactions, lcsh:Science, Free Energy, Mutation, Multidisciplinary, COS cells, drug-like compound, Drug discovery, Organic Compounds, Physics, Electromagnetic Radiation, Monosaccharides, Biological Sciences, Molecular Docking Simulation, Chemistry, Bioassays and Physiological Analysis, COS Cells, Physical Sciences, Thermodynamics, Medicine, Infectious diseases, allosteric site, Cellular Structures and Organelles, Research Article, Missense Mutation, Allosteric regulation, Ligand Binding, Carbohydrates, Site, Biology, New Pharmacological Chaperones, Research and Analysis Methods, Fluorescence, pharmacological chaperones, 03 medical and health sciences, medicine, Genetics, dithiopurine, Animals, Humans, Enzyme Assays, Pharmacology, Fabry disease, Evolutionary Biology, Alpha-galactosidase, lcsh:R, Organic Chemistry, Chemical Compounds, Fabry Disease Personalized therapies, Active site, Biology and Life Sciences, Galactose, Fabry disease bind, Cell Biology, medicine.disease, lysosomal alpha-galactosidase, pharmacological chaperone, 030104 developmental biology, Fabry, Chemical sciences, Purines, Allosteric Binding Site, alpha-Galactosidase, biology.protein, Human Lysosomal Alpha-Galactosidase Opens, lcsh:Q, Lysosomes, Biochemical Analysis, 030217 neurology & neurosurgery, phenotypic spectrum

Abstract

Personalized therapies are required for Fabry disease due to its large phenotypic spectrum and numerous different genotypes. In principle, missense mutations that do not affect the active site could be rescued with pharmacological chaperones. At present pharmacological chaperones for Fabry disease bind the active site and couple a stabilizing effect, which is required, to an inhibitory effect, which is deleterious. By in silico docking we identified an allosteric hot-spot for ligand binding where a drug-like compound, 2,6-dithiopurine, binds preferentially. 2,6-dithiopurine stabilizes lysosomal alpha-galactosidase in vitro and rescues a mutant that is not responsive to a mono-therapy with previously described pharmacological chaperones, 1-deoxygalactonojirimycin and galactose in a cell based assay. Funding was provided by Telethon - Italy (Grant no. GGP12108). This work was partially supported by the Fundación Séneca del Centro de Coordinación de la Investigación de la Región de Murcia under Project 18946/JLI/13. Powered@NLHPC: This research was partially supported by the supercomputing infrastructure of the NLHPC (ECM-02). Farmacia Medicina

Published

2016

7. Taming molecular flexibility to tackle rare diseases

Author

Maria Vittoria Cubellis, Marc Baaden, Giuseppina Andreotti, Laboratoire de biochimie théorique [Paris] (LBT (UPR_9080)), Université Paris Diderot - Paris 7 (UPD7)-Centre National de la Recherche Scientifique (CNRS)-Institut de biologie physico-chimique (IBPC (FR_550)), Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS)-Institut de Chimie du CNRS (INC), ANR-11-LABX-0011,DYNAMO,Dynamique des membranes transductrices d'énergie : biogénèse et organisation supramoléculaire.(2011), Cubellis, MARIA VITTORIA, M., Baaden, G., Andreotti, Université Paris Diderot - Paris 7 (UPD7)-Institut de biologie physico-chimique (IBPC), Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS)-Centre National de la Recherche Scientifique (CNRS), and ANR-11-LABX-0011/11-LABX-0011,DYNAMO,Dynamique des membranes transductrices d'énergie : biogénèse et organisation supramoléculaire.(2011)

Subjects

Mutant, Cell, Diagnostic use, Disease, Biology, Molecular Dynamics Simulation, Molecular dynamics, Biochemistry, RMSD, Root mean square deviation, RMSF, root mean square fluctuation, AGAL, lysosomal alpha-galactosidase, DGJ, 1-deoxy-galactonojirimycin, Genotype, Protein stability, medicine, Missense mutation, [CHIM]Chemical Sciences, Humans, Genetics, General Medicine, medicine.disease, Fabry disease, Phenotype, Molecular Docking Simulation, Proteostasis, medicine.anatomical_structure, alpha-Galactosidase, Mutation, Fabry Disease, Research Paper

Abstract

Many mutations responsible of Fabry disease destabilize lysosomal alpha-galactosidase, but retain the enzymatic activity. These mutations are associated to a milder phenotype and are potentially curable with a pharmacological therapy either with chaperones or with drugs that modulate proteostasis. We demonstrate the effectiveness of molecular dynamics simulations to correlate the genotype to the severity of the disease. We studied the relation between protein flexibility and residual enzymatic activity of pathological missense mutants in the cell. We found that mutations occurring at flexible sites are likely to retain activity in vivo. The usefulness of molecular dynamics for diagnostic purposes is not limited to lysosomal galactosidase because destabilizing mutations are widely encountered in other proteins, too, and represent a large share of all the ones associated to human diseases., Highlights • Residual alpha-galactosidase activity may relate to mild phenotype in Fabry disease. • Molecular dynamics identifies flexible residues in lysosomal alpha-galactosidase. • Mutations at flexible sites tend to maintain residual alpha-galactosidase activity.

Published

2015

8. Drug repositioning can accelerate discovery of pharmacological chaperones

Author

Giuseppina Andreotti, Bruno Hay Mele, Valentina Citro, Maria Vittoria Cubellis, Mele, B. H., V., Citro, G., Andreotti, and Cubellis, MARIA VITTORIA

Subjects

Medicine(all), Computer science, Drug repositioning, Pharmacology toxicology, Genetic Diseases, Inborn, General Medicine, Computational biology, Pharmacology, Pharmacological chaperone, Drug development, medicine, Drug approval, Humans, Genetics(clinical), Pharmacology (medical), Letter to the Editor, Drug Approval, Genetics (clinical), medicine.drug

Abstract

A promising strategy for the treatment of genetic diseases, pharmacological chaperone therapy, has been proposed recently. It exploits small molecules which can be administered orally, reach difficult tissues such as the brain and have low cost. This strategy has a vast field of application. In order to make drug development as fast as possible, it is important to exploit drug repositioning. We evaluated the impact and limitations of this approach for rare diseases and we provide a shortcut in finding drugs for off-target usage. Electronic supplementary material The online version of this article (doi:10.1186/s13023-015-0273-2) contains supplementary material, which is available to authorized users.

Published

2015

9. CDKN1C mutations: two sides of the same coin

Author

Ignacio Bergadá, Maria Vittoria Cubellis, Eamonn R. Maher, Pablo Lapunzina, Thomas Eggermann, Gerhard Binder, Frédéric Brioude, Dirk Prawitt, Matthias Begemann, Thomas, Eggermann, Gerhard, Binder, Fr?d?ric, Brioude, Eamonn R., Maher, Pablo, Lapunzina, Cubellis, MARIA VITTORIA, Ignacio, Bergad?, Dirk, Prawitt, and Matthias, Begemann

Subjects

CDKN1C Gene, Beckwith-Wiedemann Syndrome, Beckwith–Wiedemann syndrome, Genetic Counseling, Biology, Osteochondrodysplasias, Genomic Imprinting, Cyclin-dependent kinase, medicine, Animals, Humans, Epigenetics, IMAGe Syndrome, Molecular Biology, Cyclin-Dependent Kinase Inhibitor p57, Genetic Association Studies, Genetics, Chromosome Aberrations, Fetal Growth Retardation, Silver–Russell syndrome, Point mutation, Chromosomes, Human, Pair 11, Disease Management, medicine.disease, Phenotype, Urogenital Abnormalities, Mutation, biology.protein, Molecular Medicine, Adrenal Insufficiency

Abstract

Cyclin-dependent kinase (CDK)-inhibitor 1C (CDKN1C) negatively regulates cellular proliferation and it has been shown that loss-of-function mutations in the imprinted CDKN1C gene (11p15.5) are associated with the overgrowth disorder Beckwith–Wiedemann syndrome (BWS). With recent reports of gain-of-function mutations of the PCNA domain of CDKN1C in growth-retarded patients with IMAGe syndrome or Silver–Russell syndrome (SRS), its key role for growth has been confirmed. Thereby, the last gap in the spectrum of molecular alterations in 11p15.5 in growth-retardation and overgrowth syndromes could be closed. Recent functional studies explain the strict association of CDKN1C mutations with clinically opposite phenotypes and thereby contribute to our understanding of the function and regulation of the gene in particular and epigenetic regulation in general.

Published

2014

10. A thermodynamic assay to test pharmacological chaperones for Fabry disease

Author

Giuseppina Andreotti a, Valentina Citro b, Antonella Correra b, c, Maria Vittoria Cubellis c, d, Andreotti, G, Citro, V, Correra, A, and Cubellis, MARIA VITTORIA

Subjects

Protein Folding, Lysosomal storage disorder, Mutant, Biophysics, Biology, medicine.disease_cause, Biochemistry, Article, Limited proteolysis, AGAL, lysosomal alpha-galactosidase, DGJ, 1-deoxy-galactonojirimycin, Chlorocebus aethiops, Pharmacological chaperone, medicine, Animals, Humans, Urea, Cell lysate, CD, circular dichroism, Molecular Biology, Mutation, Protein Stability, HEK 293 cells, Transfection, PC, pharmacological chaperones, medicine.disease, Fabry disease, Urea-induced unfolding, HEK293 Cells, alpha-Galactosidase, COS Cells, Fabry Disease, Thermodynamics, Protein folding, FD, Fabry disease, Function (biology), Molecular Chaperones, medicine.drug

Abstract

Background The majority of the disease-causing mutations affect protein stability, but not functional sites and are amenable, in principle, to be treated with pharmacological chaperones. These drugs enhance the thermodynamic stability of their targets. Fabry disease, a disorder caused by mutations in the gene encoding lysosomal alpha-galactosidase, represents an excellent model system to develop experimental protocols to test the efficiency of such drugs. Methods The stability of lysosomal alpha-galactosidase under different conditions was studied by urea-induced unfolding followed by limited proteolysis and Western blotting. Results We measured the concentration of urea needed to obtain half-maximal unfolding because this parameter represents an objective indicator of protein stability. Conclusions Urea-induced unfolding is a versatile technique that can be adapted to cell extracts containing tiny amounts of wild-type or mutant proteins. It allows testing of protein stability as a function of pH, in the presence or in the absence of drugs. Results are not influenced by the method used to express the protein in transfected cells. General significance Scarce and dispersed populations pose a problem for the clinical trial of drugs for rare diseases. This is particularly true for pharmacological chaperones that must be tested on each mutation associated with a given disease. Diverse in vitro tests are needed. We used a method based on chemically induced unfolding as a tool to assess whether a particular Fabry mutation is responsive to pharmacological chaperones, but, by no means is our protocol limited to this disease., Graphical abstract, Highlights • Pharmacological chaperones stabilize the folded state of proteins. • Only some Fabry mutations can be treated with pharmacological chaperones. • Urea-induced unfolding represents a novel assay to test the efficiency of drugs. • The test with urea can be applied to a tiny amount of mutants in raw extracts. • Responsiveness of Fabry mutations to drugs can be tested with urea-induced unfolding.

Published

2014

11. Functional characterisation of a novel mutation affecting the catalytic domain of MMP2 in siblings with multicentric osteolysis, nodulosis and arthropathy

Author

Maria Vittoria Cubellis, Luca Pietrogrande, Ilaria Parenti, Alessia Fratoni, Cristina Gervasini, Lidia Larizza, Amilcare Cerri, Davide Rovina, Jacopo Azzollini, Jacopo, Azzollini, Davide, Rovina, Cristina, Gervasini, Ilaria, Parenti, Alessia, Fratoni, Cubellis, MARIA VITTORIA, Amilcare, Cerri, Luca, Pietrogrande, and Lidia, Larizza

Subjects

Adult, Male, Models, Molecular, medicine.medical_specialty, Osteolysis, DNA Mutational Analysis, Molecular Sequence Data, Mutant, Mutation, Missense, Biology, medicine.disease_cause, Exon, Catalytic Domain, Molecular genetics, Genetics, medicine, Humans, Missense mutation, Amino Acid Sequence, Genetic Association Studies, Genetics (clinical), Mutation, Sequence Homology, Amino Acid, Siblings, Homozygote, HEK 293 cells, medicine.disease, Molecular biology, Phenotype, Pedigree, Protein Structure, Tertiary, HEK293 Cells, Matrix Metalloproteinase 2, Female

Abstract

Multicentric osteolysis, nodulosis and arthropathy (MONA) is a rare autosomal recessive disorder. To date, 13 mutations of the matrix metalloproteinase 2 (MMP2) gene have been detected in 26 patients with MONA and other osteolytic syndromes. Here, we describe the molecular and functional analysis of a novel MMP2 mutation in two adult Italian siblings with MONA. Both siblings displayed palmar-plantar subcutaneous nodules, tendon retractions, limb arthropathies, osteolysis in the toes and pigmented fibrous skin lesions. Molecular analysis identified a homozygous MMP2 missense mutation in exon 8 c.1228G>C (p.G410R), not detected in 260 controls and predicted by several bioinformatic tools to be pathogenic. By protein modelling, the mutant residue was predicted to affect the main chain conformation of the catalytic domain. Gelatin zymography, the gold standard test for MMP2 function, of serum-free conditioned medium from G410R-MMP2-expressing human embryonic kidney (HEK) cells, showed a complete loss of gelatinolytic activity. The novel mutation is located in the catalytic domain, as are 3 (p.E404K, p.V400del and p.G406D) of the other 13 MMP2 mutations described to date; however, p.G410R underlies a phenotype that is only partially overlapping that of other MMP2 exon 8 mutation carriers. Our results further delineate the complexity of genotype-phenotype correlations in MONA, broaden the repertoire of reported MMP2 mutation and enhance the comprehension of the protein motifs crucial for MMP2 catalytic activity.

Published

2014

12. Biochemical phenotype of a common disease-causing mutation and a possible therapeutic approach for the phosphomannomutase 2-associated disorder of glycosylation

Author

Giuseppina Andreotti1, Emilia Pedone2, Assunta Giordano1, Maria Vittoria Cubellis2, 3, G., Andreotti, E., Pedone, A., Giordano, and Cubellis, MARIA VITTORIA

Subjects

Glycosylation, Protein subunit, Mutant, N-glycosylation, Biology, medicine.disease_cause, chemistry.chemical_compound, phosphomannomutase, glucose 1,6-bisphosphate, N-linked glycosylation, Genetics, medicine, Congenital disorders of glycosylation, Allele, Molecular Biology, Genetics (clinical), chemistry.chemical_classification, Mutation, glucose 1, Original Articles, Enzyme, Biochemistry, chemistry, 6-bisphosphate, Phosphomannomutase

Abstract

Phosphomannomutase 2 (PMM2) deficiency represents the most frequent type of congenital disorders of glycosylation. For this disease there is no cure at present. The complete loss of phosphomannomutase activity is probably not compatible with life and people affected carry at least one allele with residual activity. We characterized wild-type PMM2 and its most common hypomorphic mutant, p.F119L, which is associated with a severe phenotype of the disease. We demonstrated that active species is the dimeric enzyme and that the mutation weakens the quaternary structure and, at the same time, affects the activity and the stability of the enzyme. We demonstrated that ligand binding stabilizes both proteins, wild-type and F119L-PMM2, and promotes subunit association in vitro. The strongest effects are observed with glucose-1,6-bisphosphate (Glc-1,6-P2) or with monophosphate glucose in the presence of vanadate. This finding offers a new approach for the treatment of PMM2 deficiency. We propose to enhance Glc-1,6-P2 concentration either acting on the metabolic pathways that control its synthesis and degradation or exploiting prodrugs that are able to cross membranes.

Published

2013

13. Fabry_CEP: a tool to identify Fabry mutations responsive to pharmacological chaperones

Author

Maria Vittoria Cubellis, Giuseppina Andreotti, Antonella Correra, Marco Cammisa, Cammisa, M, Correra, A, Andreotti, G, and Cubellis, MARIA VITTORIA

Subjects

1-Deoxynojirimycin, Databases, Pharmaceutical, Mutant, Nonsense mutation, Web-application, Bioinformatics, Pharmacological chaperone, medicine, Humans, Missense mutation, Coding region, Genetics(clinical), Pharmacology (medical), Letter to the Editor, Genetics (clinical), Medicine(all), Internet, Fabry disease, business.industry, General Medicine, medicine.disease, Human genetics, Treatment Outcome, alpha-Galactosidase, Mutation, Mutation (genetic algorithm), Therapy, business, Molecular Chaperones, medicine.drug

Abstract

Fabry_CEP is a user-friendly web-application designed to help clinicians Choose Eligible Patients for the therapy with pharmacological chaperones. It provides a database and a predictive tool to evaluate the responsiveness of lysosomal alpha-galactosidase mutants to a small molecule drug, namely 1-Deoxy-galactonojirimycin. The user can introduce any missense/nonsense mutation in the coding sequence, learn whether it is has been tested and gain access to appropriate reference literature. In the absence of experimental data structural, functional and evolutionary analysis provides a prediction and the probability that a given mutation is responsive to the drug.

Published

2013

14. Gain of function in CDKN1C

Author

Andrea Riccio, Maria Vittoria Cubellis, A., Riccio, Cubellis, MARIA VITTORIA, Riccio, Andrea, and Cubellis, Mv

Subjects

Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Kinase, Cancer, Biology, medicine.disease, Gain of function, BECKWITH-WIEDEMANN SYNDROME, E3 UBIQUITIN LIGASE, medicine, Missense mutation, IMAGe Syndrome, Gene, P57(KIP2)

Abstract

Loss-of-function mutations in the gene encoding the cyclin-dependent kinase inhibitor CDKN1C cause Beckwith-Wiedemann syndrome and cancer. A new study now identifies potentially gain-of-function missense mutations in CDKN1C that cause the undergrowth-associated IMAGe syndrome. © 2012 Nature America, Inc. All rights reserved.

Published

2012

15. The urokinase receptor: Structure, regulation and inhibitor-mediated internalization

Author

Pura Muñoz-Cánoves, Francesco Blasi, Leena Riittinen, Ugo Cavallaro, Daniela Talarico, E. Soravia, Lisbeth Birk Møller, Paola Limongi, Massimo Resnati, S. Valcamonica, M P Stoppelli, L. Hemandez-Marrero, Nicolai Sidenius, Marco R. Soria, Tambet Teesalu, F. Fazioli, Maria Vittoria Cubellis, Massimo Conese, N. Pedersen, F., Blasi, M., Conese, L. B., Møller, N., Pedersen, U., Cavallaro, Cubellis, MARIA VITTORIA, F., Fazioli, L., Hemandez Marrero, P., Limongi, P., Munoz Canove, M., Resnati, L., Riittinen, N., Sideniu, E., Soravia, M. R., Soria, M. P., Stoppelli, D., Talarico, T., Teesalu, and S., Valcamonica

Subjects

media_common.quotation_subject, Cell, Hematology, Adhesion, Biology, Molecular biology, In vitro, Cell biology, Urokinase receptor, medicine.anatomical_structure, In vivo, medicine, Receptor, Internalization, Human cancer, media_common

Abstract

The receptor for urokinase plasminogen activator (uPAR) acts as an anchorage site for uPA on the cell surface where it stimulates pro-uPA activation, allows the internalization of uPA:inhibitor and other complexes and sends directly or indirectly signals into the cell that may promote migration, adhesion and growth. It is a GPI-anchored, three-domain protein that belongs to the Ly6 family and is present at the focal and cell-to-cell contacts, where it concentrates uPA activity. Its activity appears to be important to regulate the invasiveness of human cancer cells both in vitro and in vivo, and its inhibition is now a target for antimetastatic therapy.

Published

1994

16. Prediction of the responsiveness to pharmacological chaperones: lysosomal human alpha-galactosidase, a case of study

Author

Marco Cammisa, Mario Rosario Guarracino, Maria Vittoria Cubellis, Antonella Correra, Giuseppina Andreotti, Andreotti, G, Guarracino, M. R., Marco Cammisa, M., Antonella Correra, A., and Cubellis, MARIA VITTORIA

Subjects

Models, Molecular, 1-Deoxynojirimycin, Treatment outcome, lcsh:Medicine, Pharmacology, medicine.disease_cause, chemistry.chemical_compound, Structure-Activity Relationship, Predictive Value of Tests, Catalytic Domain, Genotype, medicine, Humans, Genetics(clinical), Pharmacology (medical), Genetics (clinical), Medicine(all), Mutation, Alpha-galactosidase, biology, lcsh:R, Methodology, General Medicine, medicine.disease, Fabry disease, Human genetics, Clinical trial, Treatment Outcome, chemistry, alpha-Galactosidase, biology.protein, Fabry Disease, Lysosomes, Software, Molecular Chaperones

Abstract

Background The pharmacological chaperones therapy is a promising approach to cure genetic diseases. It relies on substrate competitors used at sub-inhibitory concentration which can be administered orally, reach difficult tissues and have low cost. Clinical trials are currently carried out for Fabry disease, a lysosomal storage disorder caused by inherited genetic mutations of alpha-galactosidase. Regrettably, not all genotypes respond to these drugs. Results We collected the experimental data available in literature on the enzymatic activity of ninety-six missense mutants of lysosomal alpha-galactosidase measured in the presence of pharmacological chaperones. We associated with each mutation seven features derived from the analysis of 3D-structure of the enzyme, two features associated with their thermo-dynamic stability and four features derived from sequence alone. Structural and thermodynamic analysis explains why some mutants of human lysosomal alpha-galactosidase cannot be rescued by pharmacological chaperones: approximately forty per cent of the non responsive cases examined can be correctly associated with a negative prognostic feature. They include mutations occurring in the active site pocket, mutations preventing disulphide bridge formation and severely destabilising mutations. Despite this finding, prediction of mutations responsive to pharmacological chaperones cannot be achieved with high accuracy relying on combinations of structure- and thermodynamic-derived features even with the aid of classical and state of the art statistical learning methods. We developed a procedure to predict responsive mutations with an accuracy as high as 87%: the method scores the mutations by using a suitable position-specific substitution matrix. Our approach is of general applicability since it does not require the knowledge of 3D-structure but relies only on the sequence. Conclusions Responsiveness to pharmacological chaperones depends on the structural/functional features of the disease-associated protein, whose complex interplay is best reflected on sequence conservation by evolutionary pressure. We propose a predictive method which can be applied to screen novel mutations of alpha galactosidase. The same approach can be extended on a genomic scale to find candidates for therapy with pharmacological chaperones among proteins with unknown tertiary structures.

Published

2010

17. Silver-Russell Syndrome and Beckwith-Wiedemann Syndrome Phenotypes Associated with 11p Duplication in a Single Family

Author

Elisa Nalesso, Agostina De Crescenzo, Andrea Riccio, Paola Cavicchioli, Marilena Petrella, Angelo Selicorni, Barbara Zavan, Laura Cardarelli, Maria Vittoria Cubellis, Giovanni Battista Pozzan, Angela Sparago, Cardarelli, L, Sparago, A, De Crescenzo, A, Nalesso, E, Zavan, B, Cubellis, Mv, Selicorni, A, Cavicchioli, P, Pozzan, Gb, Petrella, M, Riccio, Andrea, Cubellis, MARIA VITTORIA, and Riccio, A.

Subjects

Adult, Array-CGH, Genomic imprinting, Beckwith–Wiedemann syndrome, Mothers, Biology, Pathology and Forensic Medicine, Gene Duplication, Gene duplication, medicine, Humans, Epigenetics, Allele, Genetics, Comparative Genomic Hybridization, DNA methylation, Human Growth Hormone, Silver–Russell syndrome, Chromosomes, Human, Pair 11, Chromosome, General Medicine, Uniparental Disomy, medicine.disease, Phenotype, Child, Preschool, Pediatrics, Perinatology and Child Health, Beckwith-Wiedemann syndrome, Female, Silver-Russell syndrome

Abstract

Genomic imprinting is an epigenetic phenomenon resulting in differential expression of maternal and paternal alleles of a subset of genes. In the mouse, mutation of imprinted genes often results in contrasting phenotypes, depending on parental origin. The overgrowth-associated Beckwith-Wiedemann syndrome (BWS) and the growth restriction-associated Silver-Russell syndrome (SRS) have been linked with a variety of epigenetic and genetic defects affecting a cluster of imprinted genes at chromosome 11p15.5. Paternally derived and maternally derived 11p15.5 duplications represent infrequent findings in BWS and SRS, respectively. Here, we report a case in which a 6.5 Mb duplication of 11p15.4-pter resulted in SRS and BWS phenotypes in a child and her mother, respectively. Molecular analyses demonstrated that the duplication involved the maternal chromosome 11p15 in the child and the paternal chromosome 11p15 in the mother. This observation provides a direct demonstration that SRS and BWS represent specular images, both at the clinical and molecular levels. © 2010 Society for Pediatric Pathology.

Published

2010

18. Hypomethylation at multiple maternally methylated imprinted regions including PLAGL1 and GNAS loci in Beckwith-Wiedemann syndrome

Author

Silvia Russo, Rita Fischetto, Faustina Lalatta, Jet Bliek, I. Karen Temple, Flavia Cerrato, Gaetano Verde, Maria Michela Rinaldi, L. Giordano, Marcel M.A.M. Mannens, Jonathan L A Callaway, Serena Ferraiuolo, Paola Ferrari, Agostina De Crescenzo, Deborah J G Mackay, Saskia M. Maas, Maria Vittoria Cubellis, Andrea Riccio, Angela Sparago, Lidia Larizza, Bliek, J., Verde, G., Callaway, J., Maas, S., DE CRESCENZO, A., Sparago, A., Cerrato, F., Russo, S., Ferraiuolo, S., Rinaldi, M. M., Fischetto, R., Lalatta, F., Giordano, L., Ferrari, P., Cubellis, MARIA VITTORIA, Larizza, L., Temple, I. K., Mannens, M., Mackay, D. J. G., Riccio, A., Human Genetics, Paediatric Genetics, ACS - Amsterdam Cardiovascular Sciences, ARD - Amsterdam Reproduction and Development, Cerrato, Flavia, Cubellis, M. V., Temple, K., Mannes, M., Mackay, D., and Riccio, Andrea

Subjects

Male, Candidate gene, Beckwith-Wiedemann Syndrome, Wilms-tumor, animal diseases, Beckwith-Wiedemann syndrome (BWS), KCNQ1OT1, methylation, imprinting, imprinting disorder, hypomethylation of imprinted loci (HIL), neonatal diabetes-mellitus, birth-weight, gene network, growth, establishment, individuals, mutations, defects, DNA Mutational Analysis, Beckwith–Wiedemann syndrome, Cell Cycle Proteins, Polymerase Chain Reaction, Article, Genomic Imprinting, Chromogranins, GTP-Binding Protein alpha Subunits, Gs, Genetics, medicine, GNAS complex locus, Humans, DNA (Cytosine-5-)-Methyltransferases, Epigenetics, Imprinting (psychology), Genetics (clinical), Polymorphism, Genetic, biology, Tumor Suppressor Proteins, DNA Methylation, medicine.disease, Settore MED/03 - Genetica Medica, DNA methylation, biology.protein, Female, Genomic imprinting, Transcription Factors

Abstract

Genomic imprinting is an epigenetic phenomenon restricting gene expression in a manner dependent on parent of origin. Imprinted gene products are critical regulators of growth and development, and imprinting disorders are associated with both genetic and epigenetic mutations, including disruption of DNA methylation within the imprinting control regions (ICRs) of these genes. It was recently reported that some patients with imprinting disorders have a more generalised imprinting defect, with hypomethylation at a range of maternally methylated ICRs. We report a cohort of 149 patients with a clinical diagnosis of Beckwith-Wiedemann syndrome (BWS), including 81 with maternal hypomethylation of the KCNQ1OT1 ICR. Methylation analysis of 11 ICRs in these patients showed that hypomethylation affecting multiple imprinted loci was restricted to 17 patients with hypomethylation of the KCNQ1OT1 ICR, and involved only maternally methylated loci. Both partial and complete hypomethylation was demonstrated in these cases, suggesting a possible postzygotic origin of a mosaic imprinting error. Some ICRs, including the PLAGL1 and GNAS/NESPAS ICRs implicated in the aetiology of transient neonatal diabetes and pseudohypoparathyroidism type 1b, respectively, were more frequently affected than others. Although we did not find any evidence for mutation of the candidate gene DNMT3L, these results support the hypotheses that trans-acting factors affect the somatic maintenance of imprinting at multiple maternally methylated loci and that the clinical presentation of these complex cases may reflect the loci and tissues affected with the epigenetic abnormalities.European Journal of Human Genetics advance online publication, 17 December 2008; doi:10.1038/ejhg.2008.233

Published

2009

19. The pharmacological chaperone 1-deoxynojirimycin increases the activity and lysosomal trafficking of multiple mutant forms of acid alpha-glucosidase

Author

Elfrida R. Benjamin, Maria Rosaria Tuzzi, Katherine Tang, Kenneth J. Valenzano, John J. Flanagan, Federica Fontana, Maria Vittoria Cubellis, David J. Lockhart, Generoso Andria, Giancarlo Parenti, Xiaoyang Wu, Kirsten Mascioli, Hung V. Do, Caterina Porto, Barbara Rossi, Francesca Donaudy, Flanagan, Jj, Rossi, B, Tang, K, Wu, X, Mascioli, K, Donaudy, F, Tuzzi, Mr, Fontana, F, Cubellis, MARIA VITTORIA, Porto, C, Benjamin, E, Lockhart, Dj, Valenzano, Kj, Andria, Generoso, Parenti, Giancarlo, and Do, Hv

Subjects

Adult, Models, Molecular, congenital, hereditary, and neonatal diseases and abnormalities, 1-Deoxynojirimycin, Adolescent, Mutant, Biology, Protein Structure, Secondary, chemistry.chemical_compound, Chlorocebus aethiops, Enzyme Stability, Genetics, medicine, Animals, Humans, Genetics (clinical), Secretory pathway, chemistry.chemical_classification, LAMP2, Glycogen Storage Disease Type II, nutritional and metabolic diseases, Infant, alpha-Glucosidases, Transfection, Fibroblasts, Recombinant Proteins, Pharmacological chaperone, Protein Transport, Enzyme, chemistry, Biochemistry, COS Cells, Acid alpha-glucosidase, Mutant Proteins, Lysosomes, medicine.drug

Abstract

Pompe disease is a lysosomal storage disorder (LSD) caused by mutations in the gene that encodes acid α-glucosidase (GAA). Recently, small molecule pharmacological chaperones have been shown to increase protein stability and cellular levels for mutant lysosomal enzymes and have emerged as a new therapeutic strategy for the treatment of LSDs. In this study, we characterized the pharmacological chaperone 1-deoxynojirimycin (DNJ) on 76 different mutant forms of GAA identified in Pompe disease. DNJ significantly increased enzyme activity and protein levels for 16 different GAA mutants in patient-derived fibroblasts and in transiently transfected COS-7 cells. Additionally, DNJ increased the processing of these GAA mutants to their mature lysosomal forms, suggesting facilitated trafficking through the secretory pathway. Immunofluorescence microscopy studies showed increased colocalization of GAA with the lysosomal marker LAMP2 after incubation with DNJ, confirming increased lysosomal trafficking. Lastly, a GAA structural model was constructed based on the related eukaryotic glucosidase maltase-glucoamylase. The mutated residues identified in responsive forms of GAA are located throughout most of the structural domains, with half of these residues located in two short regions within the catalytic domain. Taken together, these data support further evaluation of DNJ as a potential treatment for Pompe disease in patients that express responsive forms of GAA. Hum Mutat 30:1–10, 2009. © 2009 Wiley-Liss, Inc.

Published

2009

20. Different mechanisms cause imprinting defects at the IGF2/H19 locus in Beckwith-Wiedemann syndrome and Wilms' tumour

Author

Gianfranco Sebastio, Paola Collini, Gaetano Verde, Maria Vittoria Cubellis, Maria Michela Rinaldi, Valentina Citro, Andrea Riccio, Cinzia Magnani, Agostina De Crescenzo, Angela Sparago, Luigi Boccuto, Daniela Perotti, Flavia Cerrato, Paolo D'Angelo, Eamonn R. Maher, Giovanni Neri, Cerrato, Flavia, Sparago, A., Verde, G., DE CRESCENZO, A., Citro, V., Cubellis, M., Rinaldi, M., Boccuto, L., Neri, G., Magnani, C., D'Angelo, P., Collini, P., Perrotti, D., Sebastio, G., Maher, E., Riccio, Andrea, Cerrato, F, Sparago, A, Verde, G, DE CRESCENZO, A, Citro, V, Cubellis, MARIA VITTORIA, Rinaldi, Mm, Boccuto, L, Neri, G, Magnani, C, Dangelo, P, Collini, P, Perotti, D, Sebastio, G, and Maher, E. AND RICCIO A.

Subjects

Male, CCCTC-Binding Factor, Beckwith-Wiedemann Syndrome, RNA, Untranslated, Beckwith–Wiedemann syndrome, Locus (genetics), Biology, Settore MED/03 - GENETICA MEDICA, Wilms Tumor, Insulin-Like Growth Factor II, Chromosome Segregation, Genetics, medicine, Humans, Epigenetics, Allele, Imprinting (psychology), Molecular Biology, Alleles, Genetics (clinical), Chromosomes, Human, Pair 11, human cancer, BWS syndrome, Wilms' tumor, General Medicine, DNA Methylation, medicine.disease, Pedigree, genomic imprinting, DNA-Binding Proteins, Repressor Proteins, Haplotypes, Italy, Mutation, DNA methylation, Female, RNA, Long Noncoding, imprinting, Genomic imprinting, Gene Deletion, epigenetic

Abstract

The parent of origin-dependent expression of the IGF2 and H19 genes is controlled by the imprinting centre 1 (IC1) consisting in a methylation-sensitive chromatin insulator. Deletions removing part of IC1 have been found in patients affected by the overgrowth- and tumour-associated Beckwith - Wiedemann syndrome (BWS). These mutations result in the hypermethylation of the remaining IC1 region, loss of IGF2/H19 imprinting and fully penetrant BWS phenotype when maternally transmitted. We now report that 12 additional cases with IC1 hypermethylation have a similar clinical phenotype but showed neither a detectable deletion nor other mutation in the local vicinity. Likewise, no IC1 deletion was detected in 40 sporadic non-syndromic Wilms' tumours. A detailed analysis of the BWS patients showed that the hypermethylation variably affected the IC1 region and was generally mosaic. We observed that all these cases were sporadic and in at least two families affected and unaffected members shared the same maternal IC1 allele but not the abnormal maternal chromosome epigenotype. Furthermore, the chromosome with the imprinting defect derived from either the maternal grandfather or maternal grandmother. Overall, these results indicate that methylation-imprinting defects at the IGF2-H19 locus can result from inherited mutations of the IC and have high recurrence risk or arise independently from the sequence context and generally not transmitted to the progeny. Despite these differences, the epigenetic abnormalities are usually present in the patients in the mosaic form and probably acquired by post-zygotic de novo methylation. Distinguishing between these two groups of cases is important for genetic counselling. © The Author 2008. Published by Oxford University Press. All rights reserved.

Published

2008

21. Isolation and sequencing of a new β-galactosidase-encoding archaebacterial gene

Author

Piercarlo Montecucchi, Maria Vittoria Cubellis, Mosè Rossi, Carla Rozzo, Cubellis, MARIA VITTORIA, Carla, Rozzo, Piercarlo, Montecucchi, and Mosè, Rossi

Subjects

DNA, Bacterial, Protein subunit, Molecular Sequence Data, Restriction Mapping, ved/biology.organism_classification_rank.species, Biology, medicine.disease_cause, Homology (biology), Genetics, medicine, Amino Acid Sequence, Cloning, Molecular, Codon, Escherichia coli, Gene, Base Sequence, ved/biology, Sulfolobus solfataricus, Nucleic acid sequence, General Medicine, beta-Galactosidase, Archaea, Molecular biology, Genes, Bacterial, Regulatory sequence, Codon usage bias, Oligonucleotide Probes

Abstract

The gene lacS coding for a β-galactosidase (βGal; EC 3.2.1.23) has been cloned from the thermoacidophilic archaebacterium Sulfolobus solfataricus, strain MT-4. It encodes a polypeptide chain of 489 amino acids (aa) (56764 Da) in good agreement with the value directly measured for the enzyme ( 60 ± 2 kDa per subunit). The aa composition of the enzyme and, in particular, its peculiarly low cysteine content (one Cys per subunit) has been confirmed; at the same time, it has been observed that the very low G + C content of the S. solfataricus genome strongly influences the codoon usage preferences in the lacS sequence. There appears to be no evident similarity between this and the Escherichia coli lacZ sequence, thus suggesting that the two enzymes have analogous function, but are not homologous. By comparison with the published sequences of archaebacterial promoters, terminators and ribosome-binding sites, potential regulatory sites have been identified in the flanking regions of the S. solfataricus lacS gene.

Published

1990

22. Heterodimerization of Two Pathological Mutants Enhances the Activity of Human Phosphomannomutase2

Author

Maria Chiara Monti, Giuseppina Andreotti, Valentina Citro, Maria Vittoria Cubellis, Andreotti, Giuseppina, Monti, Maria Chiara, Citro, Valentina, and Cubellis, MARIA VITTORIA

Subjects

Genetics and Molecular Biology (all), Heterozygote, Protein Structure, Glycosylation, Mutant, lcsh:Medicine, Glucose-6-Phosphate, Biology, medicine.disease_cause, Biochemistry, Quaternary, Congenital Disorders of Glycosylation, Protein structure, medicine, Alleles, Dimerization, Humans, Mutation, Phosphorylation, Phosphotransferases (Phosphomutases), Protein Structure, Quaternary, Agricultural and Biological Sciences (all), Biochemistry, Genetics and Molecular Biology (all), Medicine (all), Allele, lcsh:Science, Gene, Multidisciplinary, lcsh:R, Wild type, Molecular biology, Enzyme structure, Proteostasis, heterodimres, lcsh:Q, CDG-PMM2, Research Article

Abstract

The most frequent disorder of glycosylation is due to mutations in the gene encoding phosphomannomutase2 (PMM2-CDG). For this disease, which is autosomal and recessive, there is no cure at present. Most patients are composite heterozygous and carry one allele encoding an inactive mutant, R141H, and one encoding a hypomorphic mutant. Phosphomannomutase2 is a dimer. We reproduced composite heterozygosity in vitro by mixing R141H either with the wild type protein or the most common hypomorphic mutant F119L and compared the quaternary structure, the activity and the stability of the heterodimeric enzymes. We demonstrated that the activity of R141H/F119L heterodimers in vitro, which reproduces the protein found in patients, has the same activity of wild type/R141H, which reproduces the protein found in healthy carriers. On the other hand the stability of R141H/F119L appears to be reduced both in vitro and in vivo. These findings suggest that a therapy designed to enhance protein stability such as those based on pharmacological chaperones or modulation of proteostasis could be beneficial for PMM2-CDG patients carrying R141H/F119L genotype as well as for other genotypes where protein stability rather than specific activity is affected by mutations.

Published

2015

23. Identification of a novel mutation in the myosin VIIA motor domain in a family with autosomal dominant hearing loss (DFNA11)

Author

Pio D'Adamo, Francesca Donaudy, Paolo Gasparini, Elio Marciano, Angela D'Eustacchio, Annamaria Franzè, Maria Vittoria Cubellis, Monica Errichiello, Claudio Saulino, Gennaro Auletta, Pasquale Giannini, Francesca Di Leva, Alfredo Ciccodicola, Di Leva, F, D'Adamo, P, Cubellis, MARIA VITTORIA, D'Eustacchio, A, Errichiello, M, Saulino, C, Auletta, G, Giannini, P, Donaudy, F, Ciccodicola, A, Gasparini, P, Franze', Annamaria, Marciano, Elio, DI LEVA, F, Franz, A, D'Adamo, ADAMO PIO, Cubellis, Mv, Gasparini, Paolo, Franze, A, and Marciano, E.

Subjects

Models, Molecular, Male, Sensorineural: genetics, Physiology, Dyneins: genetics, Chromosome Disorders, Sensorineural, genetic [Myosins], genetic [Sensorineural], Protein structure, Dyneins: chemistry, Myosins: genetics, Models, Myosin, Missense mutation, Vestibular Disease, Genetics, chemistry [Dyneins], Dynein, Chromosome Mapping, Sensory Systems, Pedigree, Vestibular Diseases, Dominant hearing lo, Sensorineural hearing loss, Female, Molecular modelling, medicine.symptom, Vestibular Diseases: complications, Human, Genotype, Myosins: chemistry, Vestibular Diseases: genetics, MYO7A, Hearing loss, Hearing Loss, Sensorineural, Molecular Sequence Data, Mutation, Missense, Locus (genetics), complication [Vestibular Diseases], macromolecular substances, Biology, Myosins, chemistry [Myosins], Missense: genetics, Speech and Hearing, Myosin VIIA, medicine, otorhinolaryngologic diseases, dominant hearing loss, missense mutation, molecular modelling, motor head domain, myosin VIIA, Humans, Amino Acid Sequence, Hearing Loss, Hearing Lo, Base Sequence, genetic [Dyneins], Auditory Threshold, Chromosome Disorders: genetics, Dyneins, Missense, Molecular, Mutation, genetic [Chromosome Disorders], medicine.disease, Chromosome Disorder, Otorhinolaryngology, genetic [Missense], sense organs, genetics [Vestibular Diseases], Motor head domain, Model

Abstract

We ascertained a large Italian family with an autosomal dominant form of non-syndromic sensorineural hearing loss with vestibular involvement. A genome-wide scan found linkage to locus DFNA11. Sequencing of the MYO7A gene in the linked region identified a new missense mutation resulting in an Ala230Val change in the motor domain of the myosin VIIA. Myosin VIIA has already been implicated in several forms of deafness, but this is the third mutation causing a dominant form of deafness, located in the myosin VIIA motor domain in a region never involved in hearing loss until now. A modelled protein structure of myosin VII motor domain provides evidence for a significant functional effect of this missense mutation.

Published

2006

24. Antitumor Action of Seminal Ribonuclease, Its Dimeric Structure, and Its Resistance to the Cytosolic Ribonuclese Inhibitor

Author

and Aniello Russo, Mariarosaria Naddeo, Giuseppe D'Alessio, Maria Vittoria Cubellis, Antonella Antignani, Antignani, A., Naddeo, M., Cubellis, MARIA VITTORIA, Russo, A., D'Alessio, Giuseppe, Antonella, Antignani, Mariarosaria, Naddeo, Aniello, Russo, Giuseppe, D'Alessio, Cubellis, M. V., Russo, Aniello, and D'Alessio, G.

Subjects

RNase P, Drug Resistance, Glutamic Acid, Antineoplastic Agents, Tumor cells, Arginine, Biochemistry, 3T3 cells, Ribonuclese Inhibitor, Mice, Cytosol, Semen, Endoribonucleases, Serine, Tumor Cells, Cultured, medicine, Animals, Cytotoxic T cell, Disulfides, Ribonuclease, Enzyme Inhibitors, chemistry.chemical_classification, Seminal Ribonuclease, biology, Lysine, Mutagenesis, Tryptophan, Proteins, 3T3 Cells, Antitumor, Molecular biology, Growth Inhibitors, Recombinant Proteins, Enzyme, medicine.anatomical_structure, Amino Acid Substitution, chemistry, Mutagenesis, Site-Directed, biology.protein, Cattle, Dimerization

Abstract

Bovine seminal RNase (BS-RNase) is a homodimeric enzyme with a cytotoxic activity selective for tumor cells. In this study, the relationships of its cytotoxic activity to its dimeric structure and its resistance to the cytosolic RNase inhibitor (cRI) are investigated systematically by site-directed mutagenesis. The results show that (1) the dimericity of BS-RNase is essential for its full cytotoxic action; (2) the role of the dimeric structure in the antitumor activity is that of making the enzyme insensitive to the cytosolic RNase inhibitor; (3) a RNase may not be completely insensitive to cRI to exploit a full cytotoxic potential.

Published

2001

25. Relaxation of Insulin-like Growth Factor 2 Imprinting and Discordant Methylation at KvDMR1 in Two First Cousins Affected by Beckwith-Wiedemann and Klippel-Trenaunay-Weber Syndromes

Author

Paola Ungaro, Paolo V. Pedone, Flavia Cerrato, Andrea Riccio, Stefano Casola, Maria Vernucci, Carmelo B. Bruni, Gianfranco Sebastio, Maria Pia Sperandeo, Maria Vittoria Cubellis, Generoso Andria, Lucia Perone, Maria Pia, Sperandeo, Paola, Ungaro, Maria, Vernucci, Paolo V., Pedone, Flavia, Cerrato, Lucia, Perone, Stefano, Casola, Cubellis, MARIA VITTORIA, Carmelo B., Bruni, Generoso, Andria, Gianfranco, Sebastio, Andrea, Riccio, Sperandeo, Mp, Ungaro, P, Vernucci, M, Pedone, Paolo Vincenzo, Cerrato, Flavia, Perone, L, Casola, S, Cubellis, Mv, Bruni, Cb, Andria, G, Sebastio, G, and Riccio, Andrea

Subjects

Proband, Insulin-like growth factor 2, Male, medicine.medical_specialty, Klippel-Trenaunay-Weber Syndrome, Beckwith-Wiedemann Syndrome, Potassium Channels, RNA, Untranslated, Beckwith–Wiedemann syndrome, Mothers, Muscle Proteins, Locus (genetics), Overgrowth syndromes, Biology, Receptor, IGF Type 2, Genomic Imprinting, Insulin-Like Growth Factor II, Internal medicine, Genes, Regulator, Genetics, medicine, Humans, Genetics(clinical), Epigenetics, Allele, Imprinting (psychology), 3' Untranslated Regions, Genetics (clinical), Alleles, KCNQ Potassium Channels, Chromosomes, Human, Pair 11, Articles, DNA Methylation, Fibroblasts, medicine.disease, Introns, Pedigree, Endocrinology, Haplotypes, Potassium Channels, Voltage-Gated, DNA methylation, KCNQ1 Potassium Channel, CpG Islands, Female, RNA, Long Noncoding, Genomic imprinting, Beckwith-Wiedeman syndrome, Polymorphism, Restriction Fragment Length

Abstract

Beckwith-Wiedeman syndrome (BWS) and Klippel-Trenaunay-Weber syndrome (KTWS) are different human disorders characterized, among other features, by tissue overgrowth. Deregulation of one or more imprinted genes located at chromosome 11p15.5, of which insulin-like growth factor 2 (IGF2) is the most likely candidate, is believed to cause BWS, whereas the etiology of KTWS is completely obscure. We report a case of BWS and a case of KTWS in a single family. The probands, sons of two sisters, showed relaxation of the maternal IGF2 imprinting, although they inherited different 11p15.5 alleles from their mothers and did not show any chromosome rearrangement. The patient with BWS also displayed hypomethylation at KvDMR1, a maternally methylated CpG island within an intron of the KvLQT1 gene. The unaffected brother of the BWS proband shared the same maternal and paternal 11p15.5 haplotype with his brother, but the KvDMR1 locus was normally methylated. Methylation of the H19 gene was normal in both the BWS and KTWS probands. Linkage between the insulin-like growth factor 2 receptor (IGF2R) gene and the tissue overgrowth was also excluded. These results raise the possibility that a defective modifier or regulatory gene unlinked to 11p15.5 caused a spectrum of epigenetic alterations in the germ line or early development of both cousins, ranging from the relaxation of IGF2 imprinting in the KTWS proband to disruption of both the imprinted expression of IGF2 and the imprinted methylation of KvDMR1 in the BWS proband. Analysis of these data also indicates that loss of IGF2 imprinting is not necessarily linked to alteration of methylation at the KvDMR1 or H19 loci and supports the notion that IGF2 overexpression is involved in the etiology of the tissue hypertrophy observed in different overgrowth disorders, including KTWS.

Published

2000

26. 'Molecular characterization of G6PD deficiency in Southern Italy: heterogeneity, correlation genotype-phenotype and description of a new variant (G6PD Neapolis)'

Author

Stefania Filosa, Amelia Cimmino, Giuseppe Martini, Maria Vittoria Cubellis, Luigii Vitagliano, Matteo Francese, Adriana Zagari, Brino Rotoli, Filomena Ferraro, Fiorella Alfinito, Alfinito, F., Cimmino, A., Ferraro, F., Cubellis, MARIA VITTORIA, Vitagliano, L., Francese, M., Zagari, Adriana, Rotoli, B., Filosa, S., Martini, G., Alfinito, Fiorella, Cimmino, A, Ferraro, F, Vitagliano, L, Francese, M, Zagari, A, Rotoli, B, Filosa, S, Fiorella, Alfinito, Amelia, Cimmino, Filomena, Ferraro, Luigi, Vitagliano, Matteo, Francese, Adriana, Zagari, Bruno, Rotoli, Stefania, Filosa, and Giuseppe, Martini

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, Genotype, G6PD NEAPOLIS, Glucosephosphate Dehydrogenase, Biology, medicine.disease_cause, Polymerase Chain Reaction, Genotype phenotype, law.invention, Genetic Heterogeneity, law, hemic and lymphatic diseases, parasitic diseases, medicine, Humans, Polymerase chain reaction, Genetics, Mutation, Genetic heterogeneity, nutritional and metabolic diseases, Hematology, New variant, Phenotype, Glucosephosphate Dehydrogenase Deficiency, Italy

Abstract

We report on the molecular basis of glucose-6-phosphate dehydrogenase (G6PD) deficiency in Southern Italy (Campania region). Thirty-one unrelated G6PD-deficient males were analysed at DNA level for the presence of G6PD gene mutations. Nine different G6PD variants were identified, eight of which have already been described (Mediterranean, Seattle, two different A-, Santamaria, Cassano, Union and Cosenza). G6PD Mediterranean, Santamaria, A- and Union were associated with haemolytic episodes. G6PD Seattle, which is polymorphic in several populations, Cassano and Cosenza appeared to be asymptomatic. A new variant (G6PD Neapolis) is reported here. The 467(Pro-->Arg) substitution responsible for G6PD Neapolis is discussed in the light of the current 3D model of human G6PD and in comparison with other natural mutations which occur in the proximity of residue 467.

Published

1997

27. Expression of a hyperthermophilic aspartate aminotransferase in Escherichia coli

Author

Maria Ina Arnone, Leila Birolo, Giovanni Sannia, Gianpaolo Nitti, G. Marino, Maria Vittoria Cubellis, M. I., Arnone, Birolo, Leila, Cubellis, MARIA VITTORIA, G., Nitti, Marino, Gennaro, and Sannia, Giovanni

Subjects

ved/biology.organism_classification_rank.species, Molecular Sequence Data, Biophysics, Oligonucleotides, medicine.disease_cause, Biochemistry, law.invention, Sulfolobus, Structural Biology, law, medicine, Escherichia coli, Aspartate Aminotransferases, Molecular Biology, chemistry.chemical_classification, Expression vector, biology, Base Sequence, ved/biology, Thermophile, Sulfolobus solfataricus, biology.organism_classification, Molecular biology, Recombinant Proteins, Enzyme, chemistry, Recombinant DNA, Bacteria, Plasmids

Abstract

The gene for an archaebacterial hyperthermophilic enzyme, aspartate aminotransferase from Sulfolobus solfataricus (AspAT Ss ), was expressed in Escherichia coli and the enzyme purified to homogencity. A suitable expression vector and host strain were selected and culture conditions were optimized so that 6–7 mg of pure enzyme per litre of culture were obtained repeatedly. The recombinant enzyme and the authentic AspAT Ss are indistinguishable: in fact, they have the same molecular weight, estimated by means of SDS-PAGE and gel filtration, the same K m values for 2-oxo-glutarate and cysteine sulphinate and the same UV-visible spectra. Moreover, recombinant AspAT Ss is thermophilic and thermostable just as the enzyme extracted from Sulfolobus solfataricus . The protocol described may be used to produce thermostable archaebacterial enzymes in mesophilic hosts.

Published

1992

28. Limited proteolysis as a probe of conformational changes in aspartate aminotransferase from Sulfolobus solfataricus

Author

Gianpaolo Nitti, Giovanni Sannia, Maria Vittoria Cubellis, Maria Ina Arnone, Marta Giamberini, Gennaro Marino, Leila Birolo, M. I., Arnone, Birolo, Leila, M., Giamberini, Cubellis, MARIA VITTORIA, G., Nitti, Sannia, Giovanni, and Marino, Gennaro

Subjects

Protein Conformation, Swine, Proteolysis, ved/biology.organism_classification_rank.species, Molecular Sequence Data, Thermolysin, Biology, Biochemistry, Transaminase, Sulfolobus, Structure-Activity Relationship, Cytosol, medicine, Animals, Enzyme kinetics, Amino Acid Sequence, Aspartate Aminotransferases, Enzyme Inhibitors, chemistry.chemical_classification, medicine.diagnostic_test, ved/biology, Myocardium, Sulfolobus solfataricus, Temperature, Trypsin, Arrhenius plot, Enzyme, chemistry, Electrophoresis, Polyacrylamide Gel, medicine.drug, Peptide Hydrolases

Abstract

The analysis of conformational transitions using limited proteolysis was carried out on a hyperthermophilic aspartate aminotransferase isolated from the archaebacterium Sulfolobus solfataricus, in comparison with pig cytosolic aspartate aminotransferase, a thoroughly studied mesophilic aminotransferase which shares about 15% similarity with the archaebacterial protein. Aspartate aminotransferase from S. solfataricus is cleaved at residue 28 by thermolysin and residues 32 and 33 by trypsin; analogously, pig heart cytosolic aspartate aminotransferase is cleaved at residues 19 and 25 [Iriarte, A., Hubert, E., Kraft, K. & Martinez-Carrion, M. (1984) J. Biol. Chem. 259, 723-728] by trypsin. In the case of aspartate aminotransferase from S. solfataricus, proteolytic cleavages also result in transaminase inactivation thus indicating that both enzymes, although evolutionarily distinct, possess a region involved in catalysis and well exposed to proteases which is similarly positioned in their primary structure. It has been reported that the binding of substrates induces a conformational transition in aspartate aminotransferases and protects the enzymes against proteolysis [Gehring, H. (1985) in Transaminases (Christen, P. & Metzler, D. E., eds) pp. 323-326, John Wiley & Sons, New York]. Aspartate aminotransferase from S. solfataricus is protected against proteolysis by substrates, but only at high temperatures (> 60-degrees-C). To explain this behaviour, the kinetics of inactivation caused by thermolysin were measured in the temperature range 25-75-degrees-C. The Arrhenius plot of the proteolytic kinetic constants measured in the absence of substrates is not rectilinear, while the same plot of the constants measured in the presence of substrates is a straight line. Limited proteolysis experiments suggest that aspartate aminotransferase from S. solfataricus undergoes a conformational transition induced by the binding of substrates. Another conformational transition which depends on temperature and occurs in the absence of substrates could explain the non-linear Arrhenius plot of the proteolytic kinetic constants. The latter conformational transition might also be related to the functioning of the archaebacterial aminotransferase since the Arrhenius plot of k(cat) is non-linear as well.

Published

1992

29. Receptor-mediated internalization and degradation of urokinase is caused by its specific inhibitor PAI-1

Author

Maria Vittoria Cubellis, Tze-Chein Wun, Francesco Blasi, Cubellis, MARIA VITTORIA, Wun, Tc, and Blasi, F.

Subjects

Plasmin, media_common.quotation_subject, Receptors, Cell Surface, Biology, Ligands, General Biochemistry, Genetics and Molecular Biology, Cell Line, Receptors, Urokinase Plasminogen Activator, Plasminogen Activators, Cell surface receptor, medicine, Humans, Protein Precursors, Receptor, Internalization, Molecular Biology, media_common, Urokinase, General Immunology and Microbiology, General Neuroscience, Cell Membrane, Biological Transport, Receptor-mediated endocytosis, Ligand (biochemistry), Urokinase-Type Plasminogen Activator, Cell biology, Urokinase receptor, Kinetics, Plasminogen Inactivators, Biochemistry, medicine.drug, Research Article

Abstract

The receptor for urokinase plasminogen activator (uPA) has been previously shown not to internalize its ligand, but rather to focalize its activity at the cell surface, allowing a regulated cell surface plasmin dependent proteolysis. The receptor in fact binds the proenzyme pro-uPA and allows its very efficient conversion to the active two chains form. Receptor bound active uPA can also interact with its specific type 1 inhibiror (PAI-1) which is therefore able to inhibit the cell surface plasmin formation. In this paper we show that the uPA-PAI-1 complex bound to the uPA receptor is internalized and degraded. U937 cells were incubated at 4 degrees C with labeled uPA-PAI-1 (and other ligands), the temperature then raised to 37 degrees C and the fate of the ligand followed for 3 h thereafter. The uPA-PAI-1 complex was internalized into the cells (i.e. could not be dissociated by acid treatment) and thereafter degraded (i.e. appeared in the supernatant in a non TCA-precipitable form). Other ligands (free uPA, ATF and DFP-treated uPA) were not internalized nor degraded. The degradation of the uPA-PAI-1 complex is preceded by internalization and is inhibited by chloroquine, an inhibitor of lysosomal protein degradation. These data suggest the existence of a cellular cycle of uPA. After synthesis pro-uPA is secreted, bound to the receptor and activated to two chain uPA. On the surface, uPA can activate surface bound plasminogen to produce surface bound plasmin. In the presence of PAI-1 uPA activity is inhibited and plasmin production interrupted, while the uPA-PAI-1 complex is internalized and degraded.

Published

1990

30. The urokinase receptor and regulation of cell surface plasminogen activation

Author

Francesco Blasi, Lisbeth Birk Møller, M. Vittoria Cubellis, Nina Pedersen, Vincent Ellis, Michael Ploug, M. Teresa Masucci, David P. Olson, Ebbe Rønne, Niels Behrendt, Keld Danø, Leif R. Lund, Francesco, Blasi, Cubellis, MARIA VITTORIA, M., Teresa Masucci, Lisbeth B., Møller, David P., Olson, Nina, Pedersen, Niels, Behrendt, Vincent, Elli, Leif R., Lund, Michael, Ploug, Ebbe, Rønne, and Keld, Danø

Subjects

Proteolysis, Cell, Receptors, Cell Surface, Biology, Receptors, Urokinase Plasminogen Activator, Mice, medicine, Tumor Cells, Cultured, Animals, Humans, Fibrinolysin, Receptor, chemistry.chemical_classification, medicine.diagnostic_test, Plasminogen, DNA, Urokinase-Type Plasminogen Activator, Endocytosis, Cell biology, Urokinase receptor, Enzyme Activation, Plasminogen Inactivators, Enzyme, medicine.anatomical_structure, chemistry, Gene Expression Regulation, Phospholipases, Cancer cell, biology.protein, Tetradecanoylphorbol Acetate, Vitronectin, Plasminogen activator, Developmental Biology

Abstract

Urokinase-type plasminogen activator (u-PA) is a key enzyme involved in migration and invasiveness of cells, both in cancer and in several normal physiological processes (Reich, 1978; Dana et al., 1985; Saksela and Rifkin, 1988; Blasi and Verde, 1990). The application of modem biochemical and molecular biological techniques has identified some of the steps at which u-PA activity is regulated. A large number of studies have dealt with the biological roles of u-PA catalyzed plasminogen activation. These can be summarized as follows: (1) u-PA-dependent proteolysis can take place on cells with surface-bound reactants; physiologically, this may well be the most relevant form of plasminogen activation; (2) the plasminogen activating system and its regulation are complex and several molecules are known to be involved (activators, substrate, inhibitors, receptors), although other, as yet unidentified, components are also implicated and (3) on a biochemical basis the u-PA system exploited by cancer cells appears to be qualitatively identical to that used in normal

Published

1990

31. The receptor for urokinase-plasminogen activator

Author

Maria Vittoria Cubellis, M P Stoppelli, Francesco Blasi, Francesco, Blasi, M., Patrizia Stoppelli, and Cubellis, MARIA VITTORIA

Subjects

Urokinase, Chemistry, Growth factor, medicine.medical_treatment, Insulin-like growth factor 2 receptor, Cell Differentiation, Receptors, Cell Surface, Cell Biology, Urokinase-Type Plasminogen Activator, Biochemistry, Monocytes, Cell Line, Urokinase receptor, Plasminogen Activators, Growth factor receptor, Epidermal growth factor, Neoplasms, medicine, Humans, Amino Acid Sequence, Receptor, Molecular Biology, A431 cells, medicine.drug

Abstract

Many human cells and cell lines possess a specific receptor that binds urokinase plasminogen activator (uPA) with an affinity of about 10(-10) M. Bound enzyme is not internalized, is slowly dissociated, and retains its enzymatic activity. The amino acid sequence of uPA responsible for receptor binding is located within the first 35 aminoterminal residues, ie, in the growth factor domain. Binding, however, is not competed for by other proteins that contain the growth factor domain (including epidermal growth factor). Cells that produce uPA secrete the pro-uPA form, which subsequently binds to the receptor. A431 cells, in fact, have their receptors completely saturated with pro-uPA. It is proposed that uPA:uPA-receptor interaction plays a direct role in physiological and pathological processes that require cell migration.

Published

1986

32. Accessibility of receptor-bound urokinase to type-1 plasminogen activator inhibitor

Author

M Mayer, Peter A. Andreasen, Pia Ragno, Maria Vittoria Cubellis, Francesco Blasi, Keld Dano, Cubellis, MARIA VITTORIA, Andreasen, P, Ragno, P, Mayer, M, Danø, K, and Blasi, F.

Subjects

Receptors, Cell Surface, Binding, Competitive, Cell Line, Plasminogen Activators, medicine, Humans, Fibrinolysin, Receptor, Binding selectivity, Glycoproteins, Urokinase, Enzyme Precursors, Multidisciplinary, U937 cell, Chemistry, plasminogen activator inhibitor 1, Molecular biology, Urokinase-Type Plasminogen Activator, Urokinase receptor, Molecular Weight, Kinetics, Plasminogen Inactivators, Cell culture, Plasminogen activator, Fibrinolytic agent, medicine.drug, Research Article

Abstract

Urokinase plasminogen activator (uPA) interacts with a surface receptor and with specific inhibitors, such as plasminogen activator inhibitor type 1 (PAI-1). These interactions are mediated by two functionally independent domains of the molecule: the catalytic domain (at the carboxyl terminus) and the growth factor domain (at the amino terminus). We have now investigated whether PAI-1 can bind and inhibit receptor-bound uPA. Binding of 125I-labeled ATF (amino-terminal fragment of uPA) to human U937 monocyte-like cells can be competed for by uPA-PAI-1 complexes, but not by PAI-1 alone. Performed 125I-labeled uPA-PAI-1 complexes can bind to uPA receptor with the same binding specificity as uPA. PAI-1 also binds to, and inhibits the activity of, receptor-bound uPA in U937 cells, as shown in U937 cells by a caseinolytic plaque assay. Plasminogen activator activity of these cells is dependent on exogenous uPA, is competed for by receptor-binding diisopropyl fluorophosphate-treated uPA, and is inhibited by the addition of PAI-1. In conclusion, in U937 cells the binding to the receptor does not shield uPA from the action of PAI-1. The possibility that in adherent cells a different localization of PAI-1 and uPA leads to protection of uPA from PAI-1 is to be considered.

Published

1989

33. Binding of single-chain prourokinase to the urokinase receptor of human U937 cells

Author

Giovanni Cassani, M.L. Nolli, Francesco Blasi, Maria Vittoria Cubellis, Cubellis, MARIA VITTORIA, Nolli, Ml, Cassani, G, and Blasi, F.

Subjects

Plasmin, Receptors, Cell Surface, Biology, Biochemistry, Receptors, Urokinase Plasminogen Activator, Plasminogen Activators, Zymogen, medicine, Humans, Fibrinolysin, Receptor, Molecular Biology, Cells, Cultured, chemistry.chemical_classification, Urokinase, U937 cell, Cell Biology, Urokinase-Type Plasminogen Activator, Cell biology, Urokinase receptor, Kinetics, Enzyme, chemistry, Cell culture, medicine.drug

Abstract

The single-chain form of human urokinase plasminogen activator (uPA) is the major form of the enzyme found in cells, tissues, and extracellular fluids. The protein, called pro-uPA, has high (Kd = 0.5 nM) affinity for the specific uPA receptor of U937 human monocyte-like cells. Its conversion to two-chain uPA by plasmin does not appreciably change the binding parameters. In addition, conversion of pro-uPA to uPA occurs with receptor-bound pro-uPA and does not lead to dissociation from the membrane. These data show that secreted pro-uPA can find its way to the specific surface receptor without previous conversion to the two-chain form and that, once bound, can be activated by plasmin.

Published

1986

34. Cloning and expression of the receptor for human urokinase plasminogen activator, a central molecule in cell surface, plasmin dependent proteolysis

Author

Maria Vittoria Cubellis, Francesco Blasi, Niels Behrendt, Ann Louring Roldan, Keld Danø, Leif R. Lund, Maria Teresa Masucci, Ettore Appella, Roldan, Al, Cubellis, MARIA VITTORIA, Masucci, Mt, Behrendt, N, Lund, Lr, Danø, K, Appella, E, and Blasi, F.

Subjects

Signal peptide, Plasmin, Molecular Sequence Data, Fluorescent Antibody Technique, Gene Expression, Receptors, Cell Surface, Biology, Transfection, General Biochemistry, Genetics and Molecular Biology, Receptors, Urokinase Plasminogen Activator, Mice, Plasminogen Activators, L Cells, Complementary DNA, medicine, Animals, Humans, Amino Acid Sequence, Cloning, Molecular, Molecular Biology, Peptide sequence, Gene Library, Urokinase, Enzyme Precursors, General Immunology and Microbiology, Base Sequence, cDNA library, General Neuroscience, Binding protein, Blotting, Northern, Molecular biology, Urokinase receptor, Kinetics, RNA, Oligonucleotide Probes, medicine.drug, Research Article

Abstract

The surface receptor for urokinase plasminogen activator (uPAR) has been recognized in recent years as a key molecule in regulating plasminogen mediated extracellular proteolysis. Surface plasminogen activation controls the connections between cells, basement membrane and extracellular matrix, and therefore the capacity of cells to migrate and invade neighboring tissues. We have isolated a 1.4 kb cDNA clone coding for the entire human uPAR. An oligonucleotide synthesized on the basis of the N-terminal sequence of the purified protein was used to screen a cDNA library made from SV40 transformed human fibroblasts [Okayama and Berg (1983) Mol. Cell Biol., 3, 280-289]. The cDNA encodes a protein of 313 amino acids, preceded by a 21 residue signal peptide. A hydrophobicity plot suggests the presence of a membrane spanning domain close to the C-terminus. The cDNA hybridizes to a 1.4 kb mRNA from human cells, a size very close to that of the cloned cDNA. Expression of the uPAR cDNA in mouse cells confirms that the clone is complete and expresses a functional uPA binding protein, located on the cell surface and with properties similar to the human uPAR. Caseinolytic plaque assay, immunofluorescence analysis, direct binding studies and cross-linking experiments show that the transfected mouse LB6 cells specifically bind human uPA, which in turn activates plasminogen. The Mr of the mature human receptor expressed in mouse cells is approximately 55,000, in accordance with the naturally occurring, highly glycosylated human uPAR. The Mr calculated on the basis of the cDNA sequence, approximately 35,000, agrees well with that of the deglycosylated receptor.

35. In silico docking of urokinase plasminogen activator and integrins

Author

Francescol Blasi, Bernard Degryse, Maria Vittoria Cubellis, Juan Fernández-Recio, Valentina Citro, Degryse, B, FERNANDEZ RECIO, J, Citro, Valentina, Blasi, F, and Cubellis, MARIA VITTORIA

Subjects

Models, Molecular, Cell signaling, Integrins, Protein Conformation, Integrin, Plasma protein binding, Biochemistry, Protein structure, Structural Biology, Protein Interaction Mapping, medicine, Computer Simulation, Binding site, Receptor, Molecular Biology, Urokinase, Binding Sites, biology, Applied Mathematics, Research, Urokinase-Type Plasminogen Activator, Cell biology, Computer Science Applications, Urokinase receptor, Models, Chemical, biology.protein, medicine.drug, Protein Binding

Abstract

Background Urokinase, its receptor and the integrins are functionally associated and involved in regulation of cell signaling, migration, adhesion and proliferation. No structural information is available on this potential multimolecular complex. However, the tri-dimensional structure of urokinase, urokinase receptor and integrins is known. Results We have modeled the interaction of urokinase on two integrins, αIIbβ3 in the open configuration and αvβ3 in the closed configuration. We have found that multiple lowest energy solutions point to an interaction of the kringle domain of uPA at the boundary between α and β chains on the surface of the integrins. This region is not far away from peptides that have been previously shown to have a biological role in urokinase receptor/integrins dependent signaling. Conclusions We demonstrated that in silico docking experiments can be successfully carried out to identify the binding mode of the kringle domain of urokinase on the scaffold of integrins in the open and closed conformation. Importantly we found that the binding mode was the same on different integrins and in both configurations. To get a molecular view of the system is a prerequisite to unravel the complex protein-protein interactions underlying urokinase/urokinase receptor/integrin mediated cell motility, adhesion and proliferation and to design rational in vitro experiments.

36. Therapy of Fabry disease with pharmacological chaperones: from in silico predictions to in vitro tests

Author

Marco Cammisa, Antonella Correra, Pierangelo Orlando, Agostina De Crescenzo, Giuseppina Andreotti, Maria Vittoria Cubellis, Valentina Citro, Andreotti, G, Citro, V, De Crescenzo, A, Orlando, P, Cammisa, M, Correra, A, and Cubellis, MARIA VITTORIA

Subjects

Male, Models, Molecular, 1-Deoxynojirimycin, In silico, Molecular Sequence Data, Mutant, Mutation, Missense, lcsh:Medicine, Biology, Predictive Value of Tests, genetic disease, Catalytic Domain, Chlorocebus aethiops, Genotype, medicine, Animals, Humans, Missense mutation, Genetics(clinical), Pharmacology (medical), Gene, Genetics (clinical), Genetics, Medicine(all), Base Sequence, Research, lcsh:R, bioinformatics, General Medicine, Enzyme replacement therapy, medicine.disease, Fabry disease, Phenotype, pharmacological chaperone, alpha-Galactosidase, COS Cells, Mutagenesis, Site-Directed, Fabry Disease, Female, Muramidase, Molecular Chaperones

Abstract

Background Fabry disease is a rare disorder caused by a large variety of mutations in the gene encoding lysosomal alpha-galactosidase. Many of these mutations are unique to individual families. Fabry disease can be treated with enzyme replacement therapy, but a promising novel strategy relies on small molecules, so called "pharmacological chaperones", which can be administered orally. Unfortunately only 42% of genotypes respond to pharmacological chaperones. Results A procedure to predict which genotypes responsive to pharmacological chaperones in Fabry disease has been recently proposed. The method uses a position-specific substitution matrix to score the mutations. Using this method, we have screened public databases for predictable responsive cases and selected nine representative mutations as yet untested with pharmacological chaperones. Mutant lysosomal alpha galactosidases were produced by site directed mutagenesis and expressed in mammalian cells. Seven out of nine mutations responded to pharmacological chaperones. Nineteen other mutations that were tested with pharmacological chaperones, but were not included in the training of the predictive method, were gathered from literature and analyzed in silico. In this set all five mutations predicted to be positive were responsive to pharmacological chaperones, bringing the percentage of responsive mutations among those predicted to be positive and not used to train the classifier to 86% (12/14). This figure differs significantly from the percentage of responsive cases observed among all the Fabry mutants tested so far. Conclusions In this paper we provide experimental support to an "in silico" method designed to predict missense mutations in the gene encoding lysosomal alpha galactosidase responsive to pharmacological chaperones. We demonstrated that responsive mutations can be predicted with a low percentage of false positive cases. Most of the mutations tested to validate the method were described in the literature as associated to classic or mild classic phenotype. The analysis can provide a guideline for the therapy with pharmacological chaperones supported by experimental results obtained in vitro. We are aware that our results were obtained in vitro and cannot be translated straightforwardly into benefit for patients, but need to be validated by clinical trials.