Your search keyword '"G. Scarano"' showing total 5 results

1. Paternal mosaicism for a COL1A1 dominant mutation (α1 Ser-415) causes recurrent osteogenesis imperfecta

Author

Maurizia Valli, M. Gomez Lira, G. Scarano, Fortunato Lonardo, Pier Franco Pignatti, Giuseppe Cetta, Monica Mottes, and Antonella Forlino

Subjects

Adult, Male, Proband, DNA Mutational Analysis, Molecular Sequence Data, Biology, Germline, Genetics, medicine, Humans, Point Mutation, Amino Acid Sequence, Allele, Genetics (clinical), Genes, Dominant, Base Sequence, Transition (genetics), Mosaicism, Point mutation, Infant, Newborn, DNA, Osteogenesis Imperfecta, medicine.disease, Molecular biology, Pedigree, Osteogenesis imperfecta, Mutation (genetic algorithm), Female, Collagen, Type I collagen

Abstract

We describe a dominant point mutation in the COL1A1 gene causing extremely severe osteogenesis imperfecta (OI type II/III) which was detected in the dermal fibroblasts of a proband, diagnosed by ultrasonography at 24 weeks of gestation. Type I collagen secretion was reduced and pro alpha 1(I) chains were overmodified. The mutation was localised in one COL1A1 allele by chemical cleavage of mismatched bases in normal cDNA/proband's mRNA heteroduplexes, and identified by cloning and sequencing. A G-to-A transition which causes the substitution of Gly-415 with serine in the alpha 1(I) triple helical domain was found. The same mutation was detected in the father's spermatozoa and lymphocytes. Mosaicism in the father's germline explains the occurrence in the family of two additional OI pregnancies, which were documented by X-ray and ultrasound investigations.

Published

1993

2. Molecular analysis, pathogenic mechanisms, and readthrough therapy on a large cohort of Kabuki syndrome patients.

Author

Micale L, Augello B, Maffeo C, Selicorni A, Zucchetti F, Fusco C, De Nittis P, Pellico MT, Mandriani B, Fischetto R, Boccone L, Silengo M, Biamino E, Perria C, Sotgiu S, Serra G, Lapi E, Neri M, Ferlini A, Cavaliere ML, Chiurazzi P, Monica MD, Scarano G, Faravelli F, Ferrari P, Mazzanti L, Pilotta A, Patricelli MG, Bedeschi MF, Benedicenti F, Prontera P, Toschi B, Salviati L, Melis D, Di Battista E, Vancini A, Garavelli L, Zelante L, and Merla G

Subjects

Abnormalities, Multiple drug therapy, Cell Line, Codon, Nonsense drug effects, Cohort Studies, DNA Mutational Analysis, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Gene Expression, Gene Expression Regulation drug effects, Genetic Association Studies, Gentamicins pharmacology, Gentamicins therapeutic use, Haploinsufficiency, Hematologic Diseases drug therapy, Histone Demethylases genetics, Homeodomain Proteins genetics, Humans, Mutation, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Nonsense Mediated mRNA Decay, Nuclear Proteins genetics, RNA Splice Sites, Sequence Analysis, DNA, Transcription, Genetic, Vestibular Diseases drug therapy, Abnormalities, Multiple genetics, Face abnormalities, Hematologic Diseases genetics, Vestibular Diseases genetics

Abstract

Kabuki syndrome (KS) is a multiple congenital anomalies syndrome characterized by characteristic facial features and varying degrees of mental retardation, caused by mutations in KMT2D/MLL2 and KDM6A/UTX genes. In this study, we performed a mutational screening on 303 Kabuki patients by direct sequencing, MLPA, and quantitative PCR identifying 133 KMT2D, 62 never described before, and four KDM6A mutations, three of them are novel. We found that a number of KMT2D truncating mutations result in mRNA degradation through the nonsense-mediated mRNA decay, contributing to protein haploinsufficiency. Furthermore, we demonstrated that the reduction of KMT2D protein level in patients' lymphoblastoid and skin fibroblast cell lines carrying KMT2D-truncating mutations affects the expression levels of known KMT2D target genes. Finally, we hypothesized that the KS patients may benefit from a readthrough therapy to restore physiological levels of KMT2D and KDM6A proteins. To assess this, we performed a proof-of-principle study on 14 KMT2D and two KDM6A nonsense mutations using specific compounds that mediate translational readthrough and thereby stimulate the re-expression of full-length functional proteins. Our experimental data showed that both KMT2D and KDM6A nonsense mutations displayed high levels of readthrough in response to gentamicin treatment, paving the way to further studies aimed at eventually treating some Kabuki patients with readthrough inducers., (© 2014 The Authors. *Human Mutation published by Wiley Periodicals, Inc.)

Published

2014

3. Disease-associated mutations in the actin-binding domain of filamin B cause cytoplasmic focal accumulations correlating with disease severity.

Author

Daniel PB, Morgan T, Alanay Y, Bijlsma E, Cho TJ, Cole T, Collins F, David A, Devriendt K, Faivre L, Ikegawa S, Jacquemont S, Jesic M, Krakow D, Liebrecht D, Maitz S, Marlin S, Morin G, Nishikubo T, Nishimura G, Prescott T, Scarano G, Shafeghati Y, Skovby F, Tsutsumi S, Whiteford M, Zenker M, and Robertson SP

Subjects

Binding Sites, Dwarfism genetics, Facies, Filamins, Humans, Repetitive Sequences, Nucleic Acid, Severity of Illness Index, Actins metabolism, Contractile Proteins genetics, Contractile Proteins metabolism, Cytoplasm metabolism, Microfilament Proteins genetics, Microfilament Proteins metabolism, Musculoskeletal Abnormalities genetics, Mutation, Osteochondrodysplasias genetics

Abstract

Dominant missense mutations in FLNB, encoding the actin-cross linking protein filamin B (FLNB), cause a broad range of skeletal dysplasias with varying severity by an unknown mechanism. Here these FLNB mutations are shown to cluster in exons encoding the actin-binding domain (ABD) and filamin repeats surrounding the flexible hinge 1 region of the FLNB rod domain. Despite being positioned in domains that bind actin, it is unknown if these mutations perturb cytoskeletal structure. Expression of several full-length FLNB constructs containing ABD mutations resulted in the appearance of actin-containing cytoplasmic focal accumulations of the substituted protein to a degree that was correlated with the severity of the associated phenotypes. In contrast, study of mutations leading to substitutions in the FLNB rod domain that result in the same phenotypes as ABD mutations demonstrated that with only one exception disease-associated substitutions, surrounding hinge 1 demonstrated no tendency to form actin-filamin foci. The exception, a substitution in filamin repeat 6, lies within a region previously implicated in filamin-actin binding. These data are consistent with mutations in the ABD conferring enhanced actin-binding activity but suggest that substitutions affecting repeats near the flexible hinge region of FLNB precipitate the same phenotypes through a different mechanism., (© 2011 Wiley Periodicals, Inc.)

Published

2012

4. Identification of novel mutations in the SLC25A15 gene in hyperornithinemia-hyperammonemia-homocitrullinuria (HHH) syndrome: a clinical, molecular, and functional study.

Author

Tessa A, Fiermonte G, Dionisi-Vici C, Paradies E, Baumgartner MR, Chien YH, Loguercio C, de Baulny HO, Nassogne MC, Schiff M, Deodato F, Parenti G, Rutledge SL, Vilaseca MA, Melone MA, Scarano G, Aldamiz-Echevarría L, Besley G, Walter J, Martinez-Hernandez E, Hernandez JM, Pierri CL, Palmieri F, and Santorelli FM

Subjects

Adult, Amino Acid Transport Systems, Basic chemistry, Biological Transport, Child, Child, Preschool, Citrulline urine, Escherichia coli, Female, Humans, Hyperammonemia epidemiology, Infant, Infant, Newborn, Male, Middle Aged, Mitochondrial Membrane Transport Proteins, Mutant Proteins isolation & purification, Protein Structure, Secondary, Syndrome, Amino Acid Transport Systems, Basic genetics, Citrulline analogs & derivatives, Hyperammonemia genetics, Mutation genetics, Ornithine blood

Abstract

Hyperornithinemia-hyperammonemia-homocitrullinuria (HHH) syndrome is an autosomal recessive disorder of the urea cycle. With the exception of the French-Canadian founder effect, no common mutation has been detected in other populations. In this study, we collected 16 additional HHH cases and expanded the spectrum of SLC25A15/ORC1 mutations. Eleven novel mutations were identified including six new missense and one microrearrangement. We also measured the transport properties of the recombinant purified proteins in reconstituted liposomes for four new and two previously reported missense mutations and proved that the transport activities of these mutant forms of ORC1 were reduced as compared with the wild-type protein; residual activity ranged between 4% and 19%. Furthermore, we designed three-dimensional (3D)-modeling of mutant ORC1 proteins. While modeling the changes in silico allowed us to obtain new information on the pathomechanisms underlying HHH syndrome, we found no clear-cut genotype-phenotype correlations. Although patient metabolic alterations responded well to low-protein therapy, predictions concerning the long-term evolution of HHH syndrome remain uncertain. The preference for a hepatic rather than a neurological presentation at onset also continues, largely, to elude us. Neither modifications in oxidative metabolism-related energy, such as those expected in different mtDNA haplogroups, nor sequence variants in SLC25A2/ORC2 seem to be crucial. Other factors, including protein stability and function, and ORC1-ORC2 structural interactions should be further investigated., (Copyright 2009 Wiley-Liss, Inc.)

Published

2009

5. Paternal mosaicism for a COL1A1 dominant mutation (alpha 1 Ser-415) causes recurrent osteogenesis imperfecta.

Author

Mottes M, Gomez Lira MM, Valli M, Scarano G, Lonardo F, Forlino A, Cetta G, and Pignatti PF

Subjects

Adult, Amino Acid Sequence, Base Sequence, Collagen biosynthesis, DNA genetics, DNA Mutational Analysis, Female, Genes, Dominant, Humans, Infant, Newborn, Male, Molecular Sequence Data, Osteogenesis Imperfecta metabolism, Pedigree, Point Mutation, Collagen genetics, Mosaicism, Osteogenesis Imperfecta genetics

Abstract

We describe a dominant point mutation in the COL1A1 gene causing extremely severe osteogenesis imperfecta (OI type II/III) which was detected in the dermal fibroblasts of a proband, diagnosed by ultrasonography at 24 weeks of gestation. Type I collagen secretion was reduced and pro alpha 1(I) chains were overmodified. The mutation was localised in one COL1A1 allele by chemical cleavage of mismatched bases in normal cDNA/proband's mRNA heteroduplexes, and identified by cloning and sequencing. A G-to-A transition which causes the substitution of Gly-415 with serine in the alpha 1(I) triple helical domain was found. The same mutation was detected in the father's spermatozoa and lymphocytes. Mosaicism in the father's germline explains the occurrence in the family of two additional OI pregnancies, which were documented by X-ray and ultrasound investigations.

Published

1993