Your search keyword '"Geracitano, Silvana"' showing total 7 results

1. A Novel Pathogenic PSEN1 Mutation in a Family with Alzheimer's Disease: Phenotypical and Neuropathological Features.

Author

Gallo, Maura, Marcello, Norina, Curcio, Sabrina A.M., Colao, Rosanna, Geracitano, Silvana, Bernardi, Livia, Anfossi, Maria, Puccio, Gianfranco, Frangipane, Francesca, Clodomiro, Alessandra, Mirabelli, Maria, Vasso, Franca, Smirne, Nicoletta, Muraca, Gabriella, Di Lorenzo, Raffaele, Maletta, Raffaele, Ghidoni, Enrico, Bugiani, Orso, Tagliavini, Fabrizio, and Giaccone, Giorgio

Subjects

ALZHEIMER'S disease, DISEASES in older people, GENETIC mutation, NEURODEGENERATION, PHENOTYPES

Abstract

We report a novel presenilin1 (PSEN1) gene mutation (I143 V) in a four-generation family with Alzheimer's disease. Clinical, molecular, and neuropathological examinations were performed on index patient; thirteen affected subjects were also identified. The index patient presented at 55 with personality changes, apathy, reduction of verbal fluency, and temporal and spatial disorientation. At 68, she showed visual hallucinations; blurred language, and rigidity. She became bedridden and died at 75. A novel mutation at codon 143 was found in PSEN1 gene, changing isoleucine to valine. The brain showed severe atrophy of the frontal and temporal lobes. Parenchymal amyloid-β (Aβ) deposits were abundant, diffuse to grey structures and contained Aβ42, but very few Aβ40. Amyloid angiopathy was absent. Neurofibrillary changes were severe. Our study confirms that PSEN1 mutations can be associated with unusual phenotypes. The peculiarity of the age at onset (not very early), the long course, and the frontal involvement, together with the rather complete absence of Aβ40 and of amyloid angiopathy, widen the spectrum of PSEN1-linked phenotypes. [ABSTRACT FROM AUTHOR]

Published

2011

2. PSEN1 and PRNP Gene Mutations Co-occurrence Makes Onset Very Early in a Family with FTD Phenotype.

Author

Bernardi, Livia, Anfossi, Maria, Gallo, Maura, Geracitano, Silvana, Colao, Rosanna, Puccio, Gianfranco, Curcio, Sabrina A. M., Frangipane, Francesca, Mirabelli, Maria, Clodomiro, Alessandra, Di Lorenzo, Raffaele, Smirne, Nicoletta, Maletta, Raffaele, Iapaolo, David, and Bruni, Amalia C.

Subjects

DEMENTIA, GENETIC polymorphisms, GENETIC mutation, PRIONS, PROTEINS, PRESENILINS

Abstract

Prion protein (PRNP) gene mutations have recently been associated with clinical pictures resembling Frontotemporal dementia (FTD). We describe a novel seven extra-repeat insertional mutation in the PRNP gene in a family affected by early-onset autosomal dominant FTD previously reported as caused by a PSEN1 mutation in which there was inconsistency between clinical picture and genotype. Both mutations were pathogenic and showed a variable penetrance when present separately; when occurring together, the onset was very early, within the third decade of life. Genetic screening of the PRNP gene becomes of major importance in early onset autosomal dominant dementia. [ABSTRACT FROM AUTHOR]

Published

2011

3. Novel MAPT Val75Ala mutation and PSEN2 Arg62Hys in two siblings with frontotemporal dementia.

Author

Gallo, Maura, Tomaino, Carmine, Puccio, Gianfranco, Frangipane, Francesca, Curcio, Sabrina A. M., Bernardi, Livia, Geracitano, Silvana, Anfossi, Maria, Mirabelli, Maria, Colao, Rosanna, Vasso, Franca, Smirne, Nicoletta, Maletta, Raffaele G., and Bruni, Amalia Cecilia

Subjects

ALZHEIMER'S disease, FRONTOTEMPORAL dementia, DEMENTIA, PRESENILINS, MEMBRANE proteins, GENETIC mutation

Abstract

A clinical and molecular overlap between Alzheimer’s disease (AD) and frontotemporal dementia (FTD) has been reported. Presenilins have been associated with FTD or with FTD-like phenotype, while mutations in the MAPT gene have been linked to a clinical phenotype of AD. We performed a clinical and genetic examination in two FTD siblings and their family tree has been reconstructed. We identified a novel Val75Ala MAPT mutation in one patient and in the other the Arg62His Presenilin2 mutation. The DNA variations identified, defined mutations by frequency, per se are not causative of the disease. These mutations, possibly in association with other unknown environmental and genetic factors, may contribute to neurodegeneration. In this family, the disease might result from a genetically interconnected spectrum of altered pathways that could link most neurodegenerative disorders. Moreover, the novel mutation identified merits further functional studies that would contribute to the unravelling of such a complex field. [ABSTRACT FROM AUTHOR]

Published

2010

4. AβPP A713T Mutation in Late Onset Alzheimer's Disease with Cerebrovascular Lesions.

Author

Bernardi, Livia, Geracitano, Silvana, Colao, Rosanna, Puccio, Gianfranco, Gallo, Maura, Anfossi, Maria, Frangipane, Francesca, Curcio, Sabrina A. M., Mirabelli, Maria, Tomaino, Carmine, Vasso, Franca, Smirne, Nicoletta, Maletta, Raffaele, and Bruni, Amalia C.

Subjects

*ALZHEIMER'S disease, *DISEASES in older people, *GENETIC mutation, *PRECANCEROUS conditions, *MEDICAL genetics, *MEDICAL care

Abstract

Mutations in the amyloid-β protein precursor (AβPP) gene can cause autosomal dominant early-onset Alzheimer's disease, or Alzheimer's disease (AD) associated with cerebral amyloid angiopathy (CAA), cerebral hemorrhage, or both. We have previously reported that the AβPP A713T mutation is associated with AD and subcortical ischemic lesions at magnetic resonance imaging in a large family which neuropathology confirmed CAA, stroke, and AD lesions. The objective of this clinical and molecular study was to investigate AβPP gene mutations in 59 patients affected by AD with cerebrovascular lesions (CVLs) and a family history of dementia. We identified three affected subjects with the AβPP A713T mutation. Since the prevalence of this mutation worldwide is very low, a common founder could exist in southern Italy. The pathogenicity of this mutation was confirmed and the clinical AD phenotype with CVLs seems to be a distinctive feature in the southern Italian population. The identification of these patients suggests that genetic epidemiology in large cohorts of familial late onset AD with CVLs would increase the probability of identifying AβPP mutations. [ABSTRACT FROM AUTHOR]

Published

2009

5. Novel PSEN1 and PGRN mutations in early-onset familial frontotemporal dementia

Author

Bernardi, Livia, Tomaino, Carmine, Anfossi, Maria, Gallo, Maura, Geracitano, Silvana, Costanzo, Angela, Colao, Rosanna, Puccio, Gianfranco, Frangipane, Francesca, Curcio, Sabrina A.M., Mirabelli, Maria, Smirne, Nicoletta, Iapaolo, David, Maletta, Raffaele Giovanni, and Bruni, Amalia C.

Subjects

*NEUROGENETICS, *NEUROLOGICAL disorders, *DEMENTIA, *GENETIC mutation, *PRESENILINS, *MOLECULAR pathology

Abstract

Abstract: Background: Frontotemporal dementia is a clinically and genetically heterogeneous syndrome. Mutations in two genes, Microtubule Associated Protein Tau (MAPT) and Progranulin (PGRN), and rarely Presenilin mutations, have been causally linked to this disorder. Objective: To investigate the presence of PGRN, PSEN1, PSEN2 and APP mutations in a group of familial early-onset frontotemporal dementia (f-EOFTD) patients negative for MAPT gene mutations. Subjects and methods: We prospectively studied 17 unrelated subjects diagnosed with f-EOFTD (one case neuropathologically confirmed as FTD-Ub+). Among these subjects eight belonged to eight autosomal dominant families unrelated to each other, and nine had at least one first degree relative affected by dementia. Results: We identified two novel heterozygous mutations in two unrelated patients, Cys139Arg in the PGRN gene and Val412Ile in the PSEN1 gene. Conclusions: Early-onset f-FTD remains a heterogeneous disorder from a genetic point of view. PGRN mutation frequency was low in our sample. The presence of a novel PSEN1 mutation suggests that presenilin molecular studies should be performed when screening for MAPT and PGRN genes is negative. [Copyright &y& Elsevier]

Published

2009

6. Epidemiology and genetics of frontotemporal dementia: a door-to-door survey in Southern Italy

Author

Bernardi, Livia, Frangipane, Francesca, Smirne, Nicoletta, Colao, Rosanna, Puccio, Gianfranco, Curcio, Sabrina A.M., Mirabelli, Maria, Maletta, Raffaele, Anfossi, Maria, Gallo, Maura, Geracitano, Silvana, Conidi, Maria Elena, Di Lorenzo, Raffale, Clodomiro, Alessandra, Cupidi, Chiara, Marzano, Sandra, Comito, Francesco, Valenti, Vincenzo, Zirilli, Maria Angela, and Ghani, Mahdi

Subjects

*FRONTOTEMPORAL dementia, *EPIDEMIOLOGY, *SURVEYS, *GENETIC mutation, *ALZHEIMER'S disease

Abstract

Abstract: The objectives of this study were to estimate frontotemporal dementia (FTD) prevalence, identify FTD-related mutations, and correlate FTD phenotype with mutations in a Southern Italian population. The study population consisted of subjects ≥ 50 years of age residing in the Community of Biv. on January 1, 2004, and a door-to-door 2-phase design was used. Genetic and biochemical analyses were done on samples collected from 32 patients. Prevalence rates were 0.6 for Alzheimer''s disease, 0.4 for vascular dementia (VD), 3.5 for FTD, 0.2 for Parkinson dementia, and 1.2 for unspecified dementia. Three GRN (1 known and 2 novel) mutations with reduced plasma protein levels were found associated to 3 distinct phenotypes (behavioral, affective, and delirious type). We report an unusually high FTD prevalence in the investigated population, but a low prevalence of Alzheimer''s disease. We confirm the heterogeneity of FTD phenotype associated with different GRN mutations. [Copyright &y& Elsevier]

Published

2012

7. Compound heterozygosity of 2 novel MAPT mutations in frontotemporal dementia

Author

Anfossi, Maria, Vuono, Romina, Maletta, Raffaele, Virdee, Kanwar, Mirabelli, Maria, Colao, Rosanna, Puccio, Gianfranco, Bernardi, Livia, Frangipane, Francesca, Gallo, Maura, Geracitano, Silvana, Tomaino, Carmine, Curcio, Sabrina Anna Maria, Zannino, Giuseppa, Lamenza, Francesco, Duyckaerts, Charles, Spillantini, Maria Grazia, Losso, Maria Adele, and Bruni, Amalia C.

Subjects

*HETEROZYGOSITY, *GENETIC mutation, *REVERSE transcriptase polymerase chain reaction, *FRONTOTEMPORAL dementia, *NEURODEGENERATION, *IMMUNOHISTOCHEMISTRY, *PRESENILE dementia

Abstract

Abstract: Intronic MAPT mutations altering exon 10 splicing lead mainly to an increase of 4Rtau. The objective of this study is to report clinical, genetic, and neuropathological data of an apparently sporadic early onset frontotemporal dementia (FTD) case associated with 2 novel intronic MAPT gene mutations IVS10+4A > C and IVS9−15T > C that increase 3Rtau. Methods and subjects used are clinical, neuroradiological, and neuropathological examination; molecular genetics of MAPT, PGRN, and other relevant genes. Exon 10 splicing tested with minigene constructs. Tau deposits detected by immunohistochemistry. Sarkosyl-insoluble and soluble tau investigated by immunoblotting. Two novel MAPT mutations IVS10+4A > C and the IVS9−15T > C transmitted by the unaffected parents were identified. Semiquantitative reverse transcription polymerase chain reaction (RT-PCR) analyses on minigenes and in brain tissue showed that both mutations cause an increase of tau mRNA (messenger ribonucleic acid) transcripts lacking exon 10 only in the patient. Immunohistochemistry and immunoblotting of the patient''s brain revealed tau deposits composed mostly of 3Rtau isoforms with a predominance of the shorter 3Rtau isoforms. The compound heterozygosity of the patient increasing 3Rtau seems to be responsible for the disease and furthermore suggests that sporadic cases can be caused by genetic mutations. [Copyright &y& Elsevier]

Published

2011