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2. Clinical heterogeneity of Kabuki syndrome in a cohort of Italian patients and review of the literature

Author

Di Candia, Francesca, Fontana, Paolo, Paglia, Pamela, Falco, Mariateresa, Rosano, Carmen, Piscopo, Carmelo, Cappuccio, Gerarda, Siano, Maria Anna, De Brasi, Daniele, Mandato, Claudia, De Maggio, Ilaria, Squeo, Gabriella Maria, Monica, Matteo Della, Scarano, Gioacchino, Lonardo, Fortunato, Strisciuglio, Pietro, Merla, Giuseppe, and Melis, Daniela

Published
2022
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4. RASopathies and hemostatic abnormalities: key role of platelet dysfunction

Author

Di Candia, Francesca, Marchetti, Valeria, Cirillo, Ferdinando, Di Minno, Alessandro, Rosano, Carmen, Pagano, Stefano, Siano, Maria Anna, Falco, Mariateresa, Assunto, Antonia, Boccia, Giovanni, Magliacane, Gerardo, Pinna, Valentina, De Luca, Alessandro, Tartaglia, Marco, Di Minno, Giovanni, Strisciuglio, Pietro, and Melis, Daniela

Published
2021
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5. Herpeticum

Author

Bove, Martina, primary, Iannaccone, Diletta, additional, Timpone, Laura, additional, Iannicelli, Gennaro, additional, Falco, Mariateresa, additional, and Ferrara, Giovanni, additional

Published
2023
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6. Genotype-phenotype spectrum and correlations in Xia-Gibbs syndrome: Report of five novel cases and literature review

Author

Romano, Ferruccio, Falco, Mariateresa, Cappuccio, Gerarda, Brunetti-Pierri, Nicola, Lonardo, Fortunato, Torella, Annalaura, Digilio, Maria Cristina, Dentici, Maria Lisa, Alfieri, Paolo, Agolini, Emanuele, Novelli, Antonio, Garavelli, Livia, Accogli, Andrea, Striano, Pasquale, Scarano, Gioacchino, Nigro, Vincenzo, Scala, Marcello, Capra, Valeria, Romano, Ferruccio, Falco, Mariateresa, Cappuccio, Gerarda, Brunetti-Pierri, Nicola, Lonardo, Fortunato, Torella, Annalaura, Digilio, Maria Cristina, Dentici, Maria Lisa, Alfieri, Paolo, Agolini, Emanuele, Novelli, Antonio, Garavelli, Livia, Accogli, Andrea, Striano, Pasquale, Scarano, Gioacchino, Nigro, Vincenzo, Scala, Marcello, and Capra, Valeria

Subjects
Embryology, AHDC1, loss-of-function variant, Genotype, Xia-Gibbs syndrome, Health, Toxicology and Mutagenesis, DNA-Binding Protein, DNA repair, DNA, genotype-phenotype correlation, Toxicology, neurodevelopmental syndrome, Epigenesis, Genetic, Musculoskeletal Abnormalities, Phenotype, Intellectual Disability, Pediatrics, Perinatology and Child Health, Abnormalities, Multiple, Developmental Biology, Human
Abstract

Background Xia-Gibbs syndrome (XGS) is a rare neurodevelopmental disorder caused by pathogenic variants in the AT-hook DNA-binding motif-containing 1 gene (AHDC1), encoding a protein with a crucial role in transcription and epigenetic regulation, axonogenesis, brain function, and neurodevelopment. AHDC1 variants possibly act through a dominant-negative mechanism and may interfere with DNA repair processes, leading to genome instability and impaired DNA translesion repair. Variants affecting residues closer to the N-terminal are thought to determine a milder phenotype with better cognitive performances. However, clean-cut genotype-phenotype correlations are still lacking. Cases In this study, we investigated five subjects with XGS in whom exome sequencing led to the identification of five novel de novo pathogenic variants in AHDC1. All variants were extremely rare and predicted to cause a loss of protein function. The phenotype of the reported patients included developmental delay, hypotonia, and distinctive facial dysmorphisms. Additionally, uncommon clinical features were observed, including congenital hypothyroidism and peculiar skeletal abnormalities. Conclusions In this study, we report uncommon XGS features associated with five novel truncating variants in AHDC, thus expanding the genotype and phenotypic spectrum of this complex condition. We also compared our cases to previously reported cases, discussing the current status of genotype-phenotype correlations in XGS.

Published
2022

7. Clinical and molecular characterization of patients affected by Beckwith‐Wiedemann spectrum conceived through assisted reproduction techniques

Author

Carli, Diana, primary, Operti, Matteo, additional, Russo, Silvia, additional, Cocchi, Guido, additional, Milani, Donatella, additional, Leoni, Chiara, additional, Prada, Elisabetta, additional, Melis, Daniela, additional, Falco, Mariateresa, additional, Spina, Jennifer, additional, Uliana, Vera, additional, Sara, Osimani, additional, Sirchia, Fabio, additional, Tarani, Luigi, additional, Macchiaiolo, Marina, additional, Cerrato, Flavia, additional, Sparago, Angela, additional, Pignata, Laura, additional, Tannorella, Pierpaola, additional, Cardaropoli, Simona, additional, Bartuli, Andrea, additional, Riccio, Andrea, additional, Ferrero, Giovanni Battista, additional, and Mussa, Alessandro, additional

Published
2022
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8. Bone Metabolism In Patients With Type 1 Neurofibromatosis: Key Role of Sun Exposure and Physical Activity

Author

Ferrara, Ursula Pia, primary, Tortora, Cristina, additional, BD, Carmen Rosano, additional, BD, Antonia Assunto, additional, Rossi, Alessandro, additional, Pagano, Stefano, additional, Falco, Mariateresa, additional, Simeoli, Chiara, additional, Ferrigno, Rosario, additional, D’Amico, Alessandra, additional, Salvio, Dario, additional, Cangemi, Giuliana, additional, Pivonello, Rosario, additional, Strisciuglio, Pietro, additional, and Melis, Daniela, additional

Published
2021
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9. Clinical heterogeneity of Kabuki syndrome in a cohort of Italian patients and review of the literature

Author

Di Candia, Francesca, primary, Fontana, Paolo, additional, Paglia, Pamela, additional, Falco, Mariateresa, additional, Rosano, Carmen, additional, Piscopo, Carmelo, additional, Cappuccio, Gerarda, additional, Siano, Maria Anna, additional, De Brasi, Daniele, additional, Mandato, Claudia, additional, De Maggio, Ilaria, additional, Squeo, Gabriella Maria, additional, Monica, Matteo Della, additional, Scarano, Gioacchino, additional, Lonardo, Fortunato, additional, Strisciuglio, Pietro, additional, Merla, Giuseppe, additional, and Melis, Daniela, additional

Published
2021
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10. Novel INF2 mutations in an Italian cohort of patients with focal segmental glomerulosclerosis, renal failure and Charcot-Marie-Tooth neuropathy

Author

Caridi, Gianluca, Lugani, Francesca, Dagnino, Monica, Gigante, Maddalena, Iolascon, Achille, Falco, Mariateresa, Graziano, Claudio, Benetti, Elisa, Dugo, Mauro, Del Prete, Dorella, Granata, Antonio, Borracelli, Donella, Moggia, Elisabetta, Quaglia, Marco, Rinaldi, Rita, Gesualdo, Loreto, and Ghiggeri, Gian Marco

Published
2014
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14. De Novo Inverted Duplication Deletion of 4p in a 14-Week-Old Male Fetus Aborted Due to Multiple Anomalies

Author

Fontana, Paolo, additional, Bernardini, Laura, additional, Lombardi, Cinzia, additional, Giuffrida, Maria Grazia, additional, Ciavarella, Maria, additional, Capalbo, Anna, additional, Maioli, Marianna, additional, Scarano, Francesca, additional, Cantalupo, Giuseppina, additional, Falco, Mariateresa, additional, Scarano, Gioacchino, additional, and Lonardo, Fortunato, additional

Published
2020
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15. M170. GENETIC CHARACTERIZATION OF A COHORT OF PATIENTS AFFECTED BY SCHIZOPHRENIA. THE ROLE FOR RARE STRUCTURAL VARIANTS IN MODULATING TREATMENT RESISTANT ENDOPHENOTYPES: PRELIMINARY DATA

Author

Barone, Annarita, primary, Iasevoli, Felice, primary, Matrone, Marta, primary, Filomena Buonaguro, Elisabetta, primary, Falco, Mariateresa, primary, Genesio, Rita, primary, Pignataro, Piero, primary, Capasso, Mario, primary, Gambale, Antonella, primary, Avagliano, Camilla, primary, Razzino, Eugenio, primary, Notar Francesco, Danilo, primary, Ciccarelli, Mariateresa, primary, Vitiello, Giuseppina, primary, Andolfo, Immacolata, primary, Nitsch, Lucio, primary, Iolascon, Achille, primary, and de Bartolomeis, Andrea, primary

Published
2020
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16. RAI1 gene mutations: mechanisms of Smith–Magenis syndrome

Author

Falco, Mariateresa, Amabile, Sonia, and Acquaviva, Fabio

Subjects
neurogenesis, sleep disorders, Review, 17p11.2, syndromic obesity, craniofacial abnormalities
Abstract

Smith–Magenis syndrome (SMS; OMIM #182290) is a complex genetic disorder characterized by distinctive physical features, developmental delay, cognitive impairment, and a typical behavioral phenotype. SMS is caused by interstitial 17p11.2 deletions, encompassing multiple genes and including the retinoic acid-induced 1 gene (RAI1), or by mutations in RAI1 itself. About 10% of all the SMS patients, in fact, carry an RAI1 mutation responsible for the phenotype. RAI1 (OMIM *607642) is a dosage-sensitive gene expressed in many tissues and highly conserved among species. Over the years, several studies have demonstrated that RAI1 (or its homologs in animal models) acts as a transcriptional factor implicated in embryonic neurodevelopment, neuronal differentiation, cell growth and cell cycle regulation, bone and skeletal development, lipid and glucose metabolisms, behavioral functions, and circadian activity. Patients with RAI1 pathogenic variants show some phenotypic differences when compared to those carrying the typical deletion. They usually have lower incidence of hypotonia and less cognitive impairment than those with 17p11.2 deletions but more frequently show the behavioral characteristics of the syndrome and overeating issues. These differences reflect the primary pathogenetic role of RAI1 without the pathogenetic contribution of the other genes included in the typical 17p11.2 deletion. The better comprehension of physiological roles of RAI1, its molecular co-workers and interactors, and its contribution in determining the typical SMS phenotype will certainly open a new path for therapeutic interventions.

Published
2017

17. Clinical report of a brain magnetic resonance imaging finding in Noonan syndrome.

Author

D'Amico, Alessandra, Cipullo, Maria Brunella, Falco, Mariateresa, Ugga, Lorenzo, and Melis, Daniela

Subjects
MAGNETIC resonance imaging, NOONAN syndrome, CONGENITAL heart disease, RAS proteins, DISABILITIES, RIB cage
Abstract

Noonan syndrome (NS) is an autosomal dominant disease caused by aberrant up-regulated signaling through RAS GTPase. It is characterized by facial dysmorphisms, short stature, congenital heart defects, malformations of rib cage bones, bleeding problems, learning difficulties, or mild intellectual disability. Additional intracranial findings in NS patients include tumors, midline anomalies, and malformations of cortical development. In this report, we present the case of a young female patient, with a known diagnosis of Noonan syndrome that in complete well being developed two brain lesions, in the right nucleus pallidus and in the left cerebellar hemisphere respectively, whose location and signal on MRI looked similar to neurofibromatosis type 1 unidentified bright objects (UBOs), and whose spectroscopic characteristics excluded neoplasms. [ABSTRACT FROM AUTHOR]

Published
2021
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18. Celiac disease in type 1 diabetes mellitus

Author

Camarca Maria, Mozzillo Enza, Nugnes Rosa, Zito Eugenio, Falco Mariateresa, Fattorusso Valentina, Mobilia Sara, Buono Pietro, Valerio Giuliana, Troncone Riccardo, and Franzese Adriana

Subjects
Diabetes, Celiac disease, Genetic background, HLA, Dietetic compliance, Glycaemic index, Gluten free diet, Quality of life, Pediatrics, RJ1-570
Abstract

Abstract Celiac Disease (CD) occurs in patients with Type 1 Diabetes (T1D) ranging the prevalence of 4.4-11.1% versus 0.5% of the general population. The mechanism of association of these two diseases involves a shared genetic background: HLA genotype DR3-DQ2 and DR4-DQ8 are strongly associated with T1D, DR3-DQ2 with CD. The classical severe presentation of CD rarely occurs in T1D patients, but more often patients have few/mild symptoms of CD or are completely asymptomatic (silent CD). In fact diagnosis of CD is regularly performed by means of the screening in T1D patients. The effects of gluten-free diet (GFD) on the growth and T1D metabolic control in CD/T1D patient are controversial. Regarding of the GFD composition, there is a debate on the higher glycaemic index of gluten-free foods respect to gluten-containing foods; furthermore GFD could be poorer of fibers and richer of fat. The adherence to GFD by children with CD-T1D has been reported generally below 50%, lower respect to the 73% of CD patients, a lower compliance being more frequent among asymptomatic patients. The more severe problems of GFD adherence usually occur during adolescence when in GFD non compliant subjects the lowest quality of life is reported. A psychological and educational support should be provided for these patients.

Published
2012
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20. RAI1 gene mutations: mechanisms of Smith–Magenis Syndrome

Author

Falco,Mariateresa, Amabile,Sonia, Acquaviva,Fabio, Falco,Mariateresa, Amabile,Sonia, and Acquaviva,Fabio

Abstract

Mariateresa Falco,1,* Sonia Amabile,1,* Fabio Acquaviva2 1Department of Molecular Medicine and Medical Biotechnology, University of Naples “Federico II”, Naples, Italy; 2Department of Translational Medical Sciences (DISMET), Section of Pediatric Clinical Genetics, University of Naples “Federico II”, Naples, Italy *These authors contributed equally to this work Abstract: Smith–Magenis syndrome (SMS; OMIM #182290) is a complex genetic disorder characterized by distinctive physical features, developmental delay, cognitive impairment, and a typical behavioral phenotype. SMS is caused by interstitial 17p11.2 deletions, encompassing multiple genes and including the retinoic acid-induced 1 gene (RAI1), or by mutations in RAI1 itself. About 10% of all the SMS patients, in fact, carry an RAI1 mutation responsible for the phenotype. RAI1 (OMIM *607642) is a dosage-sensitive gene expressed in many tissues and highly conserved among species. Over the years, several studies have demonstrated that RAI1 (or its homologs in animal models) acts as a transcriptional factor implicated in embryonic neurodevelopment, neuronal differentiation, cell growth and cell cycle regulation, bone and skeletal development, lipid and glucose metabolisms, behavioral functions, and circadian activity. Patients with RAI1 pathogenic variants show some phenotypic differences when compared to those carrying the typical deletion. They usually have lower incidence of hypotonia and less cognitive impairment than those with 17p11.2 deletions but more frequently show the behavioral characteristics of the syndrome and overeating issues. These differences reflect the primary pathogenetic role of RAI1 without the pathogenetic contribution of the other genes included in the typical 17p11.2 deletion. The better comprehension of physiological roles of RAI1, its molecular co-workers and interactors, and its contribution in determining the typical SMS phenotyp

Published
2017

29. GENETIC CHARACTERIZATION OF A COHORT OF PATIENTS AFFECTED BY SCHIZOPHRENIA. THE ROLE FOR RARE STRUCTURAL VARIANTS IN MODULATING TREATMENT RESISTANT ENDOPHENOTYPES: PRELIMINARY DATA.

Author

Barone, Annarita, Iasevoli, Felice, Matrone, Marta, Buonaguro, Elisabetta Filomena , Falco, Mariateresa, Genesio, Rita, Pignataro, Piero, Capasso, Mario, Gambale, Antonella, Avagliano, Camilla, Razzino, Eugenio, Notar Francesco, Danilo, Ciccarelli, Mariateresa, Vitiello, Giuseppina, Andolfo, Immacolata, Nitsch, Lucio, Iolascon, Achille, and de Bartolomeis, Andrea

Subjects
GENETICS of schizophrenia, CONFERENCES & conventions, GENETIC polymorphisms, RARE diseases, PHENOTYPES
Abstract

Background: Schizophrenia (SCZ) is a debilitating mental illness characterized by a highly complex, heterogeneous, non-mendelian genetic background. Recent progress in dissecting genetic architecture of SCZ has accelerated over the last decade due to new advanced technologies. Genome-Wide Association Studies (GWAS) on extremely large samples of patients identified and replicated hundreds of Single-Nucleotide Polymorphism (SNPs), each exhibiting only a modest effect. The analysis of genomic Copy Number Variations (CNVs) clarified the role of rare structural variants conferring significant risk by disrupting multiple genes involved in neurodevelopmental pathways, and linked to SCZ. In this scenario, the aim of our study is to carry out a genetic characterization of a cohort of patients affected by SCZ, in order to assess the risk of recurrence, to elucidate putative pathogenetic mechanisms and, whenever possible, to conceive tailored interventions and therapies. Methods: 34 patients (8 women and 26 men) affected by SCZ and admitted to Day Hospital at Psychiatric Division for Treatment Resistant Psychosis of the University of Naples Federico II were recruited, and underwent: i) psychopathological evaluation and assessment of clinical response to antipsychotics; ii) genetic counseling; iii) further diagnostic investigation by using Comparative Genomic Hybridization (CGH) + Single Nucleotide Polymorphism (SNP) microarray with 2x400k Agilent’s platform “GenetiSure” for detecting unbalanced chromosomal abnormalities and regions of homozygosity (ROHs). Results: Structural pathogenetic rearrangements resulted in 9 (27%) patients. Those identified were the following: 15q13.3 deletion, 16p13.11 duplication, 22q11.22 deletion (TOP3B), 22q11.22 (PRODH, DGCR5, DGCR6), RBFOX1 deletion, TCF4 deletion, derivative X chromosome (X;Y translocation). Potentially pathogenic rearrangements, involving genes associated with psychiatric disorders or implicated in neurodevelopment, resulted in 15 patients (44%). No relevant CNVs were detected in 10 patients (29%), although they showed the presence of ROHs that may contain susceptibility loci, since many neurodevelopmental genes map onto or near these specific regions. Certain of these rearrangements occur in many patients, and certain patients showed likewise multiple rearrangements. Discussion: The analysis of CNVs and SNPs allowed us to characterize the genetic disease structure in the whole cohort of patients and helped to refine the diagnosis in a few cases, thereby ascertaining an underlying specific genetic condition. A further extension of the study, in terms of sample size and more accurate investigations (i.e genetic mapping of ROHs) is underway. According to literature, rare risk-associated CNVs account for 2% of SCZ cases, but their higher prevalence (27%) in our sample may be influenced by a larger percentage of Treatment Resistant and more severely ill patients (since they were recruited in a highly specialized Unit for Treatment Resistant Psychosis). Therefore, our future purpose is to demonstrate a robust genetic modulation of Treatment Resistant endophenotypes of SCZ. Moreover, we believe that the role of genetic counseling in psychiatric services should be emphasized, and that genetic testing in this field should not be restricted to suspected childhood neuropsychiatric disorders. According to the neurodevelopmental hypothesis of SCZ, that suggests a brain development disruption in early life (due to genetic and early environmental factors), prompting to a subsequent later emergence of the disease in adulthood, even chronic complex adult mental illness, such as SCZ, deserves detailed investigations and a more exhaustive genetic evaluation [ABSTRACT FROM AUTHOR]

Published
2020
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30. Clinical heterogeneity of Kabuki syndrome in a cohort of Italian patients and review of the literature

Author

Mariateresa Falco, Pietro Strisciuglio, Ilaria De Maggio, Fortunato Lonardo, Daniela Melis, Gabriella Maria Squeo, Giuseppe Merla, Gerarda Cappuccio, Gioacchino Scarano, Carmen Rosano, Maria Siano, Claudia Mandato, Carmelo Piscopo, Paolo Fontana, Francesca Di Candia, P. Paglia, Daniele De Brasi, Matteo Della Monica, Di Candia, Francesca, Fontana, Paolo, Paglia, Pamela, Falco, Mariateresa, Rosano, Carmen, Piscopo, Carmelo, Cappuccio, Gerarda, Siano, Maria Anna, De Brasi, Daniele, Mandato, Claudia, De Maggio, Ilaria, Squeo, Gabriella Maria, Monica, Matteo Della, Scarano, Gioacchino, Lonardo, Fortunato, Strisciuglio, Pietro, Merla, Giuseppe, and Melis, Daniela

Subjects
0301 basic medicine, Adult, Male, Microcephaly, Pediatrics, medicine.medical_specialty, Adolescent, Neurological features, Autoimmunity, Vitiligo, 030105 genetics & heredity, Brain anomalie, 03 medical and health sciences, Young Adult, Intellectual disability, Medicine, Humans, Brain anomalies, Kabuki syndrome, Child, Face, Female, Retrospective Studies, Abnormalities, Multiple, Hematologic Diseases, Vestibular Diseases, Hypertelorism, Strabismus, Immunodeficiency, business.industry, medicine.disease, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Cohort, Original Article, medicine.symptom, Abnormalities, business, Multiple
Abstract

Kabuki syndrome (KS) is a well-recognized disorder characterized by postnatal growth deficiency, dysmorphic facial features, skeletal anomalies, and intellectual disability. The syndrome is caused by KMT2D gene mutations or less frequently KDM6A gene mutations or deletions. We report a systematic evaluation of KS patients from Campania region of Italy; data were also compared with literature ones. We collected data of 15 subjects (8 males and 7 females with age range 10–26 years; mean age 16.9 years) with confirmed diagnosis of KS, representing the entire cohort of patients from Campania Region. Each patient performed biochemical testing and instrumental investigation. Neuro-intellectual development, cranio-facial dysmorphisms, and multisystem involvement data were collected retrospectively. For each category, type of defects and frequency of the anomalies were analyzed. Our observation shows that KS patients from Campania region have some particular and previously underscored, neurological and immunological findings. We found high prevalence of EEG’s abnormalities (43%) and MRI brain abnormalities (60%). Microcephaly resulted more common in our series (33%), if compared with major cohorts described in literature. Biochemical features of immunodeficiency and autoimmune diseases including thyroid autoimmunity, polyserositis, and vitiligo were observed with high prevalence (54.5%). Low immunoglobulins levels were a frequent finding. Lymphocyte class investigation showed significantly reduced CD8 levels in one patient.Conclusions: These data confirm great heterogeneity of clinical manifestations in KS and suggest to introduce further clinical diagnostic criteria in order to perform a correct and precocious diagnosis. What is Known• Kabuki syndrome is characterized by growth deficiency, dysmorphic facial features, skeletal anomalies, and intellectual disability• Immune dysfunction is a common finding but autoimmune diseases are rarely seen• Neurological features are common What is New• Some particular facial features could help gestalt diagnosis (hypertelorism, broad nasal bridge, micrognathia, tooth agenesis, cutaneous haemangiomas and strabismus)• Higher prevalence of autoimmune disorders than previously reported• Particular neurological features are present in this cohort (EEG and MRI brain abnormalities)

Published
2021

31. Clinical and molecular characterization of patients affected by Beckwith-Wiedemann spectrum conceived through assisted reproduction techniques

Author

Diana Carli, Matteo Operti, Silvia Russo, Guido Cocchi, Donatella Milani, Chiara Leoni, Elisabetta Prada, Daniela Melis, Mariateresa Falco, Jennifer Spina, Vera Uliana, Osimani Sara, Fabio Sirchia, Luigi Tarani, Marina Macchiaiolo, Flavia Cerrato, Angela Sparago, Laura Pignata, Pierpaola Tannorella, Simona Cardaropoli, Andrea Bartuli, Andrea Riccio, Giovanni Battista Ferrero, Alessandro Mussa, Carli, Diana, Operti, Matteo, Russo, Silvia, Cocchi, Guido, Milani, Donatella, Leoni, Chiara, Prada, Elisabetta, Melis, Daniela, Falco, Mariateresa, Spina, Jennifer, Uliana, Vera, Sara, Osimani, Sirchia, Fabio, Tarani, Luigi, Macchiaiolo, Marina, Cerrato, Flavia, Sparago, Angela, Pignata, Laura, Tannorella, Pierpaola, Cardaropoli, Simona, Bartuli, Andrea, Riccio, Andrea, Ferrero, Giovanni Battista, and Mussa, Alessandro

Subjects
imprinting disorder, assisted reproductive technologies, Beckwith-Wiedemann Syndrome, uniparental disomy, Reproductive Techniques, Assisted, Beckwith-Wiedemann spectrum, hypomethylation, imprinting disorders, DNA Methylation, Female, Fertilization, Humans, Pregnancy, Genomic Imprinting, assisted reproductive technologie, Reproductive Techniques, Assisted, Genetics, Genetics (clinical), Human
Abstract

The prevalence of Beckwith-Wiedemann spectrum (BWSp) is tenfold increased in children conceived through assisted reproductive techniques (ART). More than 90% of ART-BWSp patients reported so far display imprinting center 2 loss-of-methylations (IC2-LoM), versus 50% of naturally conceived BWSp patients. We describe a cohort of 74 ART-BWSp patients comparing their features with a cohort of naturally conceived BWSp patients, with the ART-BWSp patients previously described in literature, and with the general population of children born from ART. We found that the distribution of UPD(11)pat was not significantly different in ART and naturally conceived patients. We observed 68.9% of IC2-LoM and 16.2% of mosaic UPD(11)pat in our ART cohort, that strongly differ from the figure reported in other cohorts so far. Since UPD(11)pat likely results from post-fertilization recombination events, our findings allows to hypothesize that more complex molecular mechanisms, besides methylation disturbances, may underlie BWSp increased risk in ART pregnancies. Moreover, comparing the clinical features of ART and non-ART BWSp patients, we found that ART-BWSp patients might have a milder phenotype. Finally, our data show a progressive increase in the prevalence of BWSp over time, paralleling that of ART usage in the last decades.

Published
2022

32. M170. GENETIC CHARACTERIZATION OF A COHORT OF PATIENTS AFFECTED BY SCHIZOPHRENIA. THE ROLE FOR RARE STRUCTURAL VARIANTS IN MODULATING TREATMENT RESISTANT ENDOPHENOTYPES: PRELIMINARY DATA

Author

Andrea de Bartolomeis, Lucio Nitsch, Piero Pignataro, Mariateresa Ciccarelli, Camilla Avagliano, Mario Capasso, Marta Matrone, Achille Iolascon, Elisabetta F. Buonaguro, Danilo Notar Francesco, Eugenio Razzino, Mariateresa Falco, Rita Genesio, Immacolata Andolfo, Giuseppina Vitiello, Felice Iasevoli, Annarita Barone, Antonella Gambale, de Bartolomeis, Andrea, Iolascon, Achille, Nitsch, Lucio, Andolfo, Immacolata, Vitiello, Giuseppina, Ciccarelli, Mariateresa, Notar Francesco, Danilo, Razzino, Eugenio, Avagliano, Camilla, Gambale, Antonella, Capasso, Mario, Pignataro, Piero, Genesio, Rita, Falco, Mariateresa, Filomena Buonaguro, Elisabetta, Matrone, Marta, Iasevoli, Felice, and Barone, Annarita

Subjects
Psychiatry and Mental health, Poster Session II, AcademicSubjects/MED00810, business.industry, Schizophrenia (object-oriented programming), Endophenotype, Cohort, Medicine, business, Bioinformatics, Treatment resistant
Abstract

Background Schizophrenia (SCZ) is a debilitating mental illness characterized by a highly complex, heterogeneous, non-mendelian genetic background. Recent progress in dissecting genetic architecture of SCZ has accelerated over the last decade due to new advanced technologies. Genome-Wide Association Studies (GWAS) on extremely large samples of patients identified and replicated hundreds of Single-Nucleotide Polymorphism (SNPs), each exhibiting only a modest effect. The analysis of genomic Copy Number Variations (CNVs) clarified the role of rare structural variants conferring significant risk by disrupting multiple genes involved in neurodevelopmental pathways, and linked to SCZ. In this scenario, the aim of our study is to carry out a genetic characterization of a cohort of patients affected by SCZ, in order to assess the risk of recurrence, to elucidate putative pathogenetic mechanisms and, whenever possible, to conceive tailored interventions and therapies. Methods 34 patients (8 women and 26 men) affected by SCZ and admitted to Day Hospital at Psychiatric Division for Treatment Resistant Psychosis of the University of Naples Federico II were recruited, and underwent: i) psychopathological evaluation and assessment of clinical response to antipsychotics; ii) genetic counseling; iii) further diagnostic investigation by using Comparative Genomic Hybridization (CGH) + Single Nucleotide Polymorphism (SNP) microarray with 2x400k Agilent’s platform “GenetiSure” for detecting unbalanced chromosomal abnormalities and regions of homozygosity (ROHs). Results Structural pathogenetic rearrangements resulted in 9 (27%) patients. Those identified were the following: 15q13.3 deletion, 16p13.11 duplication, 22q11.22 deletion (TOP3B), 22q11.22 (PRODH, DGCR5, DGCR6), RBFOX1 deletion, TCF4 deletion, derivative X chromosome (X;Y translocation). Potentially pathogenic rearrangements, involving genes associated with psychiatric disorders or implicated in neurodevelopment, resulted in 15 patients (44%). No relevant CNVs were detected in 10 patients (29%), although they showed the presence of ROHs that may contain susceptibility loci, since many neurodevelopmental genes map onto or near these specific regions. Certain of these rearrangements occur in many patients, and certain patients showed likewise multiple rearrangements. Discussion The analysis of CNVs and SNPs allowed us to characterize the genetic disease structure in the whole cohort of patients and helped to refine the diagnosis in a few cases, thereby ascertaining an underlying specific genetic condition. A further extension of the study, in terms of sample size and more accurate investigations (i.e genetic mapping of ROHs) is underway. According to literature, rare risk-associated CNVs account for 2% of SCZ cases, but their higher prevalence (27%) in our sample may be influenced by a larger percentage of Treatment Resistant and more severely ill patients (since they were recruited in a highly specialized Unit for Treatment Resistant Psychosis). Therefore, our future purpose is to demonstrate a robust genetic modulation of Treatment Resistant endophenotypes of SCZ. Moreover, we believe that the role of genetic counseling in psychiatric services should be emphasized, and that genetic testing in this field should not be restricted to suspected childhood neuropsychiatric disorders. According to the neurodevelopmental hypothesis of SCZ, that suggests a brain development disruption in early life (due to genetic and early environmental factors), prompting to a subsequent later emergence of the disease in adulthood, even chronic complex adult mental illness, such as SCZ, deserves detailed investigations and a more exhaustive genetic evaluation.

Published
2020

33. Novel compound heterozygous mutations in BCS1L gene causing Bjornstad syndrome in two siblings

Author

Sandra Iossa, Luigia De Falco, Elio Marciano, Antonella Gambale, Annamaria Franzè, Achille Iolascon, Mariateresa Falco, Falco, Mariateresa, Franzè, Annamaria, Iossa, Sandra, De Falco, Luigia, Gambale, Antonella, Marciano, Elio, and Iolascon, Achille

Subjects
Hair Disease, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Mitochondrial Diseases, Sibling, BCS1L, Hearing loss, Hearing Loss, Sensorineural, GRACILE syndrome, Mutation, Missense, Compound heterozygosity, Electron Transport Complex III, 03 medical and health sciences, 0302 clinical medicine, Genetic, Mitochondrial Disease, Genetics, medicine, Humans, Genetics (clinical), Bjornstad syndrome, Pili torti, business.industry, Siblings, pili torti, Björnstad syndrome, ATPases Associated with Diverse Cellular Activitie, hearing lo, medicine.disease, Pedigree, 030104 developmental biology, Hair disease, ATPases Associated with Diverse Cellular Activities, Female, Sensorineural hearing loss, novel mutation, medicine.symptom, Hair Diseases, business, 030217 neurology & neurosurgery, Human
Abstract

Bjornstad syndrome is a rare condition characterized by pili torti and sensorineural hearing loss associated with pathological variations in BCS1L. Mutations in this gene are also associated with the more severe complex III deficiency and GRACILE syndrome. We report the first Italian patients with Bjornstad syndrome, two siblings with pili torti and sensorineural hearing loss, in whom we detected two novel compound heterozygous mutations in BCS1L. A thorough clinical evaluation did not reveal any features consistent with complex III deficiency or GRACILE syndrome.

Published
2017

34. Cerebral Accidents in Pediatric Diabetic Ketoacidosis: Different Complications and Different Evolutions

Author

Enza Mozzillo, Elena De Nitto, Barbara Carotenuto, Adriana Franzese, Alessandra D'Amico, P Buono, Valentina Fattorusso, Mariateresa Falco, Mozzillo, Enza, D'Amico, Alessandra, Fattorusso, Valentina, Carotenuto, Barbara, Buono, Pietro, De Nitto, Elena, Falco, Mariateresa, and Franzese, Adriana

Subjects
Male, Venous stroke, medicine.medical_specialty, Pediatrics, Extrapontine myelinolysis, endocrine system diseases, Diabetic ketoacidosis, Endocrinology, Diabetes and Metabolism, Venous Stroke, Brain Edema, Cerebral accident, Medical care, Diabetic Ketoacidosis, Cerebral edema, Diabetic Ketoacidosi, Endocrinology, Edema, medicine, Humans, Child, Intensive care medicine, Stroke, medicine.diagnostic_test, business.industry, Medicine (all), Infant, nutritional and metabolic diseases, Magnetic resonance imaging, Arterial stroke, medicine.disease, Magnetic Resonance Imaging, Treatment Outcome, Pediatrics, Perinatology and Child Health, Disease Progression, Fluid Therapy, Female, medicine.symptom, business, Human
Abstract

Diabetic ketoacidosis (DKA) may be associated with neurologic complications: the most common is cerebral edema while the risk of venous and arterial stroke is rare. There is a pathogenetic link between DKA, hypercoagulability and stroke, whose risk is underestimated by clinicians. Our cases present a wide spectrum of cerebral accidents during DKA, the first one being diffuse cerebral edema, the second one venous stroke after 5 days of DKA resolution, while the third one multifocal edema suspected to be extrapontine myelinolysis although without electrolyte imbalance. Our cases suggest that DKA requires very accurate treatment, particularly at an early age, and it can be complicated by cerebral accidents even with appropriate medical care.

Published
2015

35. Constitutional chromothripsis involving the critical region of 9q21.13 microdeletion syndrome

Author

Angela Mormile, Anna Conti, Paolo Fontana, Mariateresa Falco, Daniela Melis, Lucio Nitsch, Adriana Franzese, Enza Mozzillo, Alberto Casertano, Rita Genesio, Genesio, Rita, Fontana, Paolo, Mormile, Angela, Casertano, Alberto, Falco, Mariateresa, Conti, Anna, Franzese, Adriana, Mozzillo, Enza, Nitsch, Lucio, and Melis, Daniela

Subjects
medicine.medical_specialty, Chromothripsi, Platelet disorder, Chromosome 9, Case Report, Biology, Biochemistry, GNAQ, Genetic, Genetics, medicine, Genetics(clinical), Molecular Biology, Genetics (clinical), Biochemistry, medical, Chromothripsis, Biochemistry (medical), Cytogenetics, Chromosome, Microdeletion syndrome, 9q21.13 deletion syndrome, Human genetics, Molecular Medicine
Abstract

BACKGROUND: The chromothripsis is a biological phenomenon, first observed in tumors and then rapidly described in congenital disorders. The principle of the chromothripsis process is the occurrence of a local shattering to pieces and rebuilding of chromosomes in a random order. Congenital chromothripsis rearrangements often involve reciprocal rearrangements on multiple chromosomes and have been described as cause of contiguous gene syndromes. We hypothesize that chromothripsis could be responsible for known 9q21.13 microdeletion syndrome, causing a composite phenotype with additional features. CASE PRESENTATION: The case reported is a 16- years-old female with a complex genomic rearrangement of chromosome 9 including the critical region of 9q21.13 microdeletion syndrome. The patient presents with platelet disorder and thyroid dysfunction in addition to the classical neurobehavioral phenotype of the syndrome. CONCLUSIONS: The presence of multiple rearrangements on the same chromosome 9 and the rebuilding of chromosome in a random order suggested that the rearrangement could origin from an event of chromthripsis. To our knowledge this is the first report of congenital chromothripsis involving chromosome 9. Furthermore this is the only case of 9q21.13 microdeletion syndrome due to chromothripsis.

Published
2015

36. Celiac disease in type 1 diabetes mellitus

Author

Enza Mozzillo, P Buono, M.E. Camarca, Rosa Nugnes, Adriana Franzese, Giuliana Valerio, Valentina Fattorusso, Mariateresa Falco, Sara Mobilia, Eugenio Zito, Riccardo Troncone, Erminia Camarca, Maria, Mozzillo, Enza, Nugnes, Rosa, Zito, Eugenio, Falco, Mariateresa, Fattorusso, Valentina, Mobilia, Sara, Buono, Pietro, Valerio, Giuliana, Troncone, Riccardo, and Franzese, Adriana

Subjects
Quality of life, medicine.medical_specialty, endocrine system diseases, Population, Glycaemic index, Disease, Human leukocyte antigen, Review, Dietetic compliance, Global Health, Asymptomatic, immune system diseases, Internal medicine, Diabetes mellitus, Gluten free diet, HLA-DQ Antigens, medicine, Humans, education, education.field_of_study, Type 1 diabetes, Immunity, Cellular, celiachia, business.industry, Diabetes, lcsh:RJ1-570, nutritional and metabolic diseases, lcsh:Pediatrics, diabete di tipo 1, medicine.disease, Genetic background, HLA, Celiac Disease, Diabetes Mellitus, Type 1, Metabolic control analysis, Population Surveillance, Immunology, medicine.symptom, Morbidity, business, dieta senza glutine
Abstract

Celiac Disease (CD) occurs in patients with Type 1 Diabetes (T1D) ranging the prevalence of 4.4-11.1% versus 0.5% of the general population. The mechanism of association of these two diseases involves a shared genetic background: HLA genotype DR3-DQ2 and DR4-DQ8 are strongly associated with T1D, DR3-DQ2 with CD. The classical severe presentation of CD rarely occurs in T1D patients, but more often patients have few/mild symptoms of CD or are completely asymptomatic (silent CD). In fact diagnosis of CD is regularly performed by means of the screening in T1D patients. The effects of gluten-free diet (GFD) on the growth and T1D metabolic control in CD/T1D patient are controversial. Regarding of the GFD composition, there is a debate on the higher glycaemic index of gluten-free foods respect to gluten-containing foods; furthermore GFD could be poorer of fibers and richer of fat. The adherence to GFD by children with CD-T1D has been reported generally below 50%, lower respect to the 73% of CD patients, a lower compliance being more frequent among asymptomatic patients. The more severe problems of GFD adherence usually occur during adolescence when in GFD non compliant subjects the lowest quality of life is reported. A psychological and educational support should be provided for these patients.

Published
2012

37. Genotype-phenotype spectrum and correlations in Xia-Gibbs syndrome: Report of five novel cases and literature review.

Author

Romano F, Falco M, Cappuccio G, Brunetti-Pierri N, Lonardo F, Torella A, Digilio MC, Dentici ML, Alfieri P, Agolini E, Novelli A, Garavelli L, Accogli A, Striano P, Scarano G, Nigro V, Scala M, and Capra V

Subjects
DNA, DNA-Binding Proteins genetics, Epigenesis, Genetic, Genotype, Humans, Phenotype, Abnormalities, Multiple genetics, Abnormalities, Multiple pathology, Intellectual Disability genetics, Musculoskeletal Abnormalities genetics
Abstract

Background: Xia-Gibbs syndrome (XGS) is a rare neurodevelopmental disorder caused by pathogenic variants in the AT-hook DNA-binding motif-containing 1 gene (AHDC1), encoding a protein with a crucial role in transcription and epigenetic regulation, axonogenesis, brain function, and neurodevelopment. AHDC1 variants possibly act through a dominant-negative mechanism and may interfere with DNA repair processes, leading to genome instability and impaired DNA translesion repair. Variants affecting residues closer to the N-terminal are thought to determine a milder phenotype with better cognitive performances. However, clean-cut genotype-phenotype correlations are still lacking., Cases: In this study, we investigated five subjects with XGS in whom exome sequencing led to the identification of five novel de novo pathogenic variants in AHDC1. All variants were extremely rare and predicted to cause a loss of protein function. The phenotype of the reported patients included developmental delay, hypotonia, and distinctive facial dysmorphisms. Additionally, uncommon clinical features were observed, including congenital hypothyroidism and peculiar skeletal abnormalities., Conclusions: In this study, we report uncommon XGS features associated with five novel truncating variants in AHDC, thus expanding the genotype and phenotypic spectrum of this complex condition. We also compared our cases to previously reported cases, discussing the current status of genotype-phenotype correlations in XGS., (© 2022 The Authors. Birth Defects Research published by Wiley Periodicals LLC.)

Published
2022
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