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8. Pendred Syndrome: study of three families

Author

Bigozzi, M, Melchionda, S, Casano, R, Palladino, T, and Gitti, G

Subjects
Connexin 26, Goiter, otorhinolaryngologic diseases, Humans, sense organs, Syndrome, Deafness, Polymerase Chain Reaction, Severity of Illness Index, Article, Connexins, DNA Primers, Pedigree
Abstract

Although the textbook view of the Pendred syndrome is that of an autosomal recessive condition characterised by deafness and goitre, it is increasingly clear that not all patients present this classical clinical description. Malform-ations of the inner ear, specifically, enlargement of the vestibular aqueduct, are common in the Pendred syndrome. Mutations in the Pendred syndrome gene have been observed in patients with deafness and vestibular aqueduct dilatation, in the absence of other Pendred syndrome features. In our study, all patients with congenital profound or severe sensory-neural deafness were evaluated using computed tomography and magnetic resonance imaging, followed by genetic examinations and blood tests. The procedure followed was the sensory-neural child deafness protocol elaborated by the Joint Committee for Infant Hearing based on skull and petrous bone. In 3 families, the computed tomography scans (performed on 7 out of 8 of these deaf subjects) showed enlarged vestibular aqueducts. The present study evaluates whether or not enlargement of the vestibular aqueduct should be considered as the most likely presentation of the Pendred syndrome.

Published
2005

10. Calcium-sensing-related gene mutations in hypercalcaemic hypocalciuric patients as differential diagnosis from primary hyperparathyroidism: detection of two novel inactivating mutations in an Italian population

Author

Stratta, P., primary, Merlotti, G., additional, Musetti, C., additional, Quaglia, M., additional, Pagani, A., additional, Izzo, C., additional, Radin, E., additional, Airoldi, A., additional, Baorda, F., additional, Palladino, T., additional, Leone, M. P., additional, and Guarnieri, V., additional

Published
2014
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12. Effect of hippocampal and amygdala volumes on clinical outcomes in major depression: a 3-year prospective magnetic resonance imaging study.

Author

Frodl T, Jäger M, Smajstrlova I, Born C, Bottlender R, Palladino T, Reiser M, Möller H, and Meisenzahl EM

Abstract

OBJECTIVE: According to the stress-toxicity hypothesis of depression, hippocampal volumes may diminish as the disease progresses. We sought to examine the changes in hippocampal and amygdala volumes at baseline and at 3 years after an acute depressive episode, and the impact of reduced hippocampal volumes on the outcome. METHODS: In a prospective, longitudinal study, we examined the hippocampus and amygdala of 30 inpatients with major depression from the Department of Psychiatry and Psychotherapy and 30 healthy participants from the community (control group) using high-resolution magnetic resonance images at baseline and after 3 years. Psychopathology was assessed at baseline, weekly during the inpatient phase and then after 1, 2 and 3 years. RESULTS: During the 3-year follow-up period, neither hippocampal nor amygdala volumes changed significantly among patients or participants in the control group. However, in the subgroup of patients who took antidepressants over the full 3 years, the left hippocampal volumes increased significantly. Patients with small hippocampal volumes and previous depressive episodes had a worse clinical outcome compared with patients with large hippocampal volumes and previous depressive episodes. CONCLUSION: Overall, our results suggest that a relatively small hippocampal volume may be a vulnerability factor for a bad treatment response in major depression. Subtle changes in hippocampal volumes may be detectable during continuous antidepressant therapy. Such changes may be the result of neuroplastic processes. [ABSTRACT FROM AUTHOR]

Published
2008

13. A Power Line Signaling Based Scheme for Anti-Islanding Protection of Distributed Generators—Part II: Field Test Results

Author

Wang, Wencong, Kliber, J., Zhang, Guibin, Xu, Wilsun, Howell, B., and Palladino, T.

Abstract

Anti-islanding protection of distributed generators (DG) is a significant technical barrier to the emerging DG industry. In response to this challenge, a power line signaling based anti-islanding protection scheme has been proposed in a companion paper. The scheme broadcasts a signal from a substation to the DG sites using the distribution feeders as signal paths. A DG is considered as islanded from the upstream system if the signal is not detected at the DG site. This paper presents extensive field test results and experiences obtained for the proposed scheme. The results confirm that the proposed scheme is a very promising and economical method to satisfy anti-islanding protection requirements for synchronous DG interconnections.

Published
1995
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15. A novel deletion in 2q24.1q24.2 in a girl with mental retardation and generalized hypotonia: a case report

Author

Palumbo Orazio, Palumbo Pietro, Palladino Teresa, Stallone Raffaella, Zelante Leopoldo, and Carella Massimo

Subjects
mental retardation, 2q24.1q24.2, array comparative genomic hybridization, Genetics, QH426-470
Abstract

Abstract Background Chromosomal imbalances, recognized as the major cause of mental retardation, are often due to submicroscopic deletions or duplications not evidenced by conventional cytogenetic methods. To date, interstitial deletion of long arm of chromosome 2 have been reported for more than 100 cases, although studies reporting small interstitial deletions involving the 2q24.1q24.2 region are rare. With the widespread clinical use of comparative genomic hybridization chromosomal microarray technology, several cryptic chromosome imbalances have outlined new genotype-phenotype correlations and isolated a number of distinctive clinical conditions. Results here we report on a girl with mental retardation and generalized hypotonia. A genome-wide screen for copy number variations (CNVs) using single nucleotide polymorphisms (SNPs) array revealed a 7.5 Mb interstitial deletion of chromosome region 2q24.1q24.2 encompassing 59 genes, which was absent in parents. The gene content analysis of the deleted region and review of the literature revealed the presence of some genes that may be indicated as good candidate in generating the main clinical features of the patient. Discussion the present case represents a further patient described in the literature with an interstitial deletion of chromosome 2q24.1q24.2. Our patient shares some clinical features with the previously reported patients carriers of overlapping 2q24 deletion. Although more cases are needed to delineate the full-blown phenotype of 2q24.1q24.2 deletion syndrome, published data and present observation suggest that hemizygosity of this region results in a clinically recognizable phenotype. Considering these clinical and cytogenetic similarities, we suggest the existence of an emerging syndrome associated to 2q24.1q24.2 region.

Published
2012
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17. Unilateral inguinal hernia: laparoscopic or inguinal approach. Decision making strategy: a prospective study

Author

Marianna Iaquinto, Ciro Esposito, Francesca Alicchio, T. Palladino, S. Scermino, I. Giurin, Alessandro Settimi, Alessandra Farina, Esposito, Ciro, Giurin, I., Alicchio, Francesca, Farina, Alessandra, Iaquinto, M., Scermino, Silvia, Palladino, T., and Settimi, Alessandro

Subjects
Male, Parents, Surgical results, medicine.medical_specialty, Inguinal approach, Hernia, Inguinal, Choice Behavior, Surgical technology, medicine, Humans, Unilateral inguinal hernia, Prospective Studies, Child, Laparoscopy, Prospective cohort study, Herniorrhaphy, Paediatric patients, medicine.diagnostic_test, business.industry, General surgery, Infant, medicine.disease, Surgery, Inguinal hernia, Treatment Outcome, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, business, Attitude to Health, Follow-Up Studies
Abstract

The management of the contralateral region in a child with a known unilateral inguinal hernia is a debated issue among paediatric surgeons. The available literature indicates that the perspective of the child's parents is seldom. This study was performed to evaluate parents' views on this topic. After the Ethical Committee's approval, 100 consecutive patients under 12 years of age with a unilateral inguinal hernia were studied prospectively from March 2010 to September 2010. After an oral interview, a study form was given to the parents about the nature of an inguinal hernia, the incidence of 20 to 90% of a contralateral patency of the peritoneal-vaginal duct and the possible surgical options (inguinal repair or laparoscopic repair). The parents' decision and surgical results were analyzed. Eighty-nine parents chose laparoscopic approach, and 11 parents preferred inguinal exploration. Regarding their motives, all 89 parents requesting laparoscopic approach indicated that the convenience and risk to have a second anaesthesia was the primary reason of their decision. The 11 parents who preferred inguinal approach indicated that the fear of a new surgical technology was their primary reason. Conclusion There is no consensus about the management of paediatric patients with a unilateral inguinal hernia. We believe that a correct decision-making strategy for parents' choice is to propose them the both procedures. Our study shows that parents prefer laparoscopic inspection and repair in the vast majority of cases.

Published
2012
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20. The effect of aortic coarctation surgical repair on QTc and JTc dispersion in severe aortic coarctation newborns: A short-term follow-up study

Author

Berardo Sarubbi, Giuseppe Caianiello, N. D. Cioppa, Maria Giovanna Russo, Anna Rago, Andrea Antonio Papa, Giovanni Nigro, Vincenzo Russo, T. Palladino, A. Corcione, C. Scarpati, Nigro, Gerardo, Russo, V, Rago, A, Papa, A. A., Cioppa, N. D., Scarpati, C, Palladino, T, Corcione, A, Sarubbi, B, Caianiello, G, and Russo, Maria Giovanna

Subjects
Male, Time Factors, Physiology, QT interval, Sudden death, Severity of Illness Index, Aortic Coarctation, Heart Rate, Heart rate, Medicine, Humans, cardiovascular diseases, Electrical instability, Ultrasonography, Surgical repair, business.industry, Follow up studies, Infant, Newborn, General Medicine, Surgical correction, Anesthesia, cardiovascular system, Female, business, Congenital cardiac malformations, Follow-Up Studies
Abstract

Sudden death is a possible occurrence for newborns younger than 1 year with severe aortic coarctation (CoA) before surgical correction. In our previous study, we showed a significant increase of QTc-D and JTc-D in newborns with isolated severe aortic coarctation, electrocardiographic parameters that clinical and experimental studies have suggested could reflect the physiological variability of regional and ventricular repolarization and could provide a substrate for life-threatening ventricular arrhythmias. The aim of the current study was to evaluate the effect of surgical repair of CoA on QTc-d, JTc-d in severe aortic coarctation newborns with no associated congenital cardiac malformations. The study included 30 newborns (18M; 70±12 h old) affected by severe congenital aortic coarctation, without associated cardiac malformations. All newborns underwent to classic extended end-to-end repair. Echocardiographic and electrocardiographic measurements were performed in each patient 24 h before and 24 h after the interventional procedure and at the end of the follow-up period, 1 month after the surgical correction. All patients at baseline, 24 h and one month after CoA surgical repair did not significantly differ in terms of heart rate, weight, height, and echocardiographic parameters. There were no statistically significant differences in QTc-D (111.7±47.4 vs 111.9±63.8 ms vs 108.5±55.4 ms; P=0.4) and JTc-D (98.1±41.3 vs 111.4±47.5 vs 105.1±33.4 ms; P=0.3) before, 24 h and 1 month after CoA surgical correction. In conclusions, our study did not show a statistically significant decrease in QTc-D and JTc-D, suggesting the hypothesis that the acute left ventricular afterload reduction, related to successful CoA surgical correction, may not reduce the ventricular electrical instability in the short-term follow-up.

21. The Telematic solutions in plastic surgery during COVID-19 pandemic.

Author

De Santis G, Palladino T, Leti Acciaro A, and Starnoni M

Subjects
COVID-19, Coronavirus Infections transmission, Humans, Pandemics, Pneumonia, Viral transmission, SARS-CoV-2, Betacoronavirus, Coronavirus Infections epidemiology, Disease Transmission, Infectious prevention & control, Pneumonia, Viral epidemiology, Plastic Surgery Procedures methods, Risk Management methods, Surgery, Plastic organization & administration, Telemedicine methods
Abstract

During the COVID-19 pandemic, surgical elective procedures were stopped in our plastic surgery unit. Limitations for consultations and for follow-up of previous surgical procedures were imposed in order to minimize the risk of contagion in waiting rooms and outpatient clinics. We have identified telemedicine as an alternative way to follow patients during the lockdown. Nevertheless, we have experienced different difficulties. We have not had the possibility to use a secure teleconferencing software. In our unit we had not technological devices. Surgeons in our department were not able to use remote video technology for patient management. Guidelines for an appropriate selection of patients which could be served via telemedicine had to be created. Telemedicine must be regulated by healthcare organizations for legal, ethical, medico-legal and risk management aspects. Even if we have experienced an important need to use telematic solutions during the COVID-19 lockdown, liability and risk management issues has greatly limited this possibility in our unit. The need of telemedicine in the time of COVID-19 pandemic has encouraged us to implement future virtual encounters in order to reduce unnecessary in-person visits by taking into consideration all legal, ethical and medico-legal aspects.

Published
2020
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22. Differentiating False Loss of Resistance from True Loss of Resistance While Performing the Epidural Block with the CompuFlo® Epidural Instrument.

Author

Vaira P, Camorcia M, Palladino T, Velardo M, and Capogna G

Abstract

Background: The occurrence of false losses of resistance may be one of the reasons for inadequate or failed epidural block. A CompuFlo® epidural instrument has been introduced to measure the pressure of human tissues in real time at the orifice of a needle and has been used as a tool to identify the epidural space. The aim of this study was to investigate the sensitivity and the specificity of the ability of CompuFlo® to differentiate the false loss of resistance from the true loss of resistance encountered during the epidural space identification procedure., Method: We performed epidural block with the CompuFlo® epidural instrument in 120 healthy women who requested labor epidural analgesia. The epidural needle was considered to have reached the epidural space when an increase in pressure (accompanied by an increase in the pitch of the audible tone) was followed by a sudden and sustained drop in pressure for more than 5 seconds accompanied by a sudden decrease in the pitch of the audible tone, resulting in the formation of a low and stable pressure plateau. We evaluate the sensitivity, specificity, and positive and negative predictive values of the ability of CompuFlo® recordings to correctly identify the true LOR from the false LOR., Results: The drop in pressure associated with the epidural space identification was significantly greater than that recorded after the false loss of resistance (73% vs 33%) ( P =0.000001). The sensitivity was 0.83, and the AUC was 0.82., Discussion: We have confirmed the ability of CompuFlo® to differentiate the false loss of resistance from the true loss of resistance and established its specificity and sensitivity., Conclusion: An easier identification of dubious losses of resistance during the epidural procedure is essential to reduce the number of epidural attempts and/or needle reinsertions with the potential of a reduced risk of accidental dural puncture especially in difficult cases or when the procedure is performed by trainees.

Published
2019
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23. Refinement of the critical 7p22.1 deletion region: Haploinsufficiency of ACTB is the cause of the 7p22.1 microdeletion-related developmental disorders.

Author

Palumbo O, Accadia M, Palumbo P, Leone MP, Scorrano A, Palladino T, Stallone R, Bonaglia MC, and Carella M

Subjects
Craniofacial Abnormalities pathology, Developmental Disabilities pathology, Female, Haploinsufficiency, Humans, Infant, Phenotype, Syndrome, Actins genetics, Chromosome Deletion, Chromosomes, Human, Pair 22 genetics, Craniofacial Abnormalities genetics, Developmental Disabilities genetics
Abstract

Non-recurrent microdeletion (≤2 Mb in size) in 7p22.1 is a rarely described cytogenetic aberration, only recently reported in patients with developmental delay/intellectual disability, short stature and microcephaly. The size of the deletions ranged from 0.37 to 1.5 Mb, and reported genotype-phenotype correlations identified a minimum deleted region of 0.37 Mb involving the FBLX18, ACTB, FSCN1, RNF216 and ZNF815P genes. The authors suggested that deletion of ACTB, which encodes β-actin, an essential component of the cytoskeleton, could be responsible for the clinical features observed in the patients with a 7p22.1 microdeletion. Here, we describe a 23-month-old child displaying developmental delay, short stature, microcephaly and distinctive facial features. Chromosomal microarray analysis performed using high-resolution SNP-array platform revealed a de novo interstitial 60 Kb microdeletion in the 7p22.1 region (from 5,509,127 bp to 5,569,096 bp, hg19) encompassing only two genes: FBXL18 and ACTB. To the best of our knowledge, this is the smallest deletion at 7p22.1 to date reported in medical literature (Pubmed). Combining our data with phenotypic and genotypic data of cases from literature, we were able to narrow the minimal critical region, which contained only two genes, i.e., FBXL18 and ACTB. Our finding is useful to perform a more accurate genotype-phenotype correlation and strongly strengthen the hypothesis that haploinsufficiency of ACTB is the main cause of the clinical phenotype observed in the patients with 7p22.1 microdeletions, facilitating genetic diagnosis and counseling., (Copyright © 2017 Elsevier Masson SAS. All rights reserved.)

Published
2018
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24. Clinical and molecular characterization of an emerging chromosome 22q13.31 microdeletion syndrome.

Author

Palumbo P, Accadia M, Leone MP, Palladino T, Stallone R, Carella M, and Palumbo O

Subjects
Adolescent, Ataxin-10 genetics, Cadherins genetics, Calcium-Binding Proteins genetics, Chromosome Deletion, Chromosome Disorders physiopathology, Chromosomes, Human, Pair 22 genetics, Comparative Genomic Hybridization, Developmental Disabilities physiopathology, Genetic Association Studies, Humans, Male, Neurodevelopmental Disorders physiopathology, Phenotype, Polymorphism, Single Nucleotide genetics, Uroplakin III genetics, Chromosome Disorders genetics, Developmental Disabilities genetics, Neurodevelopmental Disorders genetics
Abstract

Microdeletion of chromosome 22q13.31 is a very rare condition. Fourteen patients have been annotated in public databases but, to date, a clinical comparison has not been done and, consequently, a specific phenotype has not been delineated yet. We describe a patient showing neurodevelopmental disorders, dysmorphic features, and multiple congenital anomalies in which SNP array analysis revealed an interstitial 3.15 Mb de novo microdeletion in the 22q13.31 region encompassing 21 RefSeq genes and seven non-coding microRNAs. To perform an accurate phenotype characterization, clinical features observed in previously reported cases of 22q13.31 microdeletions were reviewed and compared to those observed in our patient. To the best of our knowledge, this is the first time that a comparison between patients carrying overlapping 22q13.31 deletions has been done. This comparison allowed us to identify a distinct spectrum of clinical manifestations suggesting that patients with a de novo interstitial microdeletion involving 22q13.31 have an emerging syndrome characterized by developmental delay/intellectual disability, speech delay/language disorders, behavioral problems, hypotonia, urogenital, and hands/feet anomalies. The microdeletion identified in our patient is the smallest reported so far and, for this reason, useful to perform a detailed genotype-phenotype correlation. In particular, we propose the CELSR1, ATXN10, FBLN1, and UPK3A as candidate genes in the onset of the main clinical features of this contiguous gene syndrome. Thus, the patient reported here broadens our knowledge of the phenotypic consequences of 22q13.31 microdeletions facilitating genotype-phenotype correlations. Additional cases are needed to corroborate our hypothesis and confirm genotype-phenotype correlations of this emerging syndrome., (© 2017 Wiley Periodicals, Inc.)

Published
2018
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25. [OssERvare Project: direct observation of use of the Safety Surgery CheckList in the operating room.]

Author

Bentivegna R, Caminati A, Agnoletti V, Bonilauri S, Buonaccorso S, Campaniello G, Dovani A, Lanciotti G, Maselli V, Mastrangelo S, Montella MT, Palladino T, Pelati C, Sciolino L, Zoni E, Porcu E, Campagna A, and Nicastro O

Subjects
Checklist, Humans, Patient Care Team standards, Patient Safety, Operating Rooms standards, Patient Care Team organization & administration, Surgical Procedures, Operative standards
Abstract

Introduction: Safety Surgery CheckList (SSCL) is a support tool for operating teams, used to carry out safety checks while also encouraging compliance with the implementation of recommended quality and safety standards. In Emilia-Romagna it was deemed appropriate to check actual surgical team compliance with correct checklist application in the operating theatre, through a project called "OssERvare"., Methods: Direct observation was identified as the preferred inspection method. With the use of special report sheets, observers proceeded with the guided observation of behaviour in the operating room, recording any inconsistencies with correct SSCL use methods. The project began in January 2017 and all observations were carried out from 1st January-15th April 2017., Results: In 43% of observed operation sign in, all three team members were not present, whereas in 7% of observed cases, sign out was not carried out. All three team members were present in 88% of observed operation time out. There are two evidently critical phases: sign in and sign out. Results obtained for time out were better., Discussion and Conclusion: Compliance data collected from observations differed markedly from reported compliance in administrative flow records. The results of the observational study indicate that the SSCL is not properly filled in many times; there is also a great possibility to improve the correct use of this tool. In conclusion, we think that the combined approach of use of administrative data and assessing compliance appeared to be a useful instrument to investigate the implementation and to promote the real utilization of safety tools such as the SSCL.

Published
2017
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26. Putative TMPRSS3/GJB2 digenic inheritance of hearing loss detected by targeted resequencing.

Author

Leone MP, Palumbo P, Ortore R, Castellana S, Palumbo O, Melchionda S, Palladino T, Stallone R, Mazza T, Cocchi R, and Carella M

Subjects
Adolescent, Child, Connexin 26, Female, Hearing Loss, Sensorineural physiopathology, Heterozygote, Humans, Male, Mutation, Sequence Analysis, DNA, Siblings, Connexins genetics, Genetic Predisposition to Disease, Hearing Loss, Sensorineural genetics, Membrane Proteins genetics, Neoplasm Proteins genetics, Serine Endopeptidases genetics
Abstract

The paper describes a putative digenic form of deafness in two siblings affected by non-syndromic hereditary hearing loss, detected by a Targeted resequencing approach. Given that a previous paper suggested TMPRSS3 and GJB2 genes as responsible for a digenic form of hearing loss, our data support and reinforce this hypothesis., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published
2017
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27. [Percutaneous treatment of complex post-myocardial infarction ventricular septal defect: case report and literature review].

Author

Moscarella E, Santoro G, Gaio G, Palladino T, D'Aiello AF, Mahmoud HT, Cappelli Bigazzi M, and Russo MG

Subjects
Female, Heart Septal Defects, Ventricular etiology, Humans, Middle Aged, Myocardial Infarction complications, Prosthesis Implantation methods, Heart Septal Defects, Ventricular surgery, Septal Occluder Device
Abstract

Post-myocardial infarction (MI) ventricular septal defects (VSD) are a rare but life-threatening complication of acute MI, with very high mortality rates even if timely approached by surgical repair. Transcatheter closure is an attractive alternative to surgery. However, this option is currently deemed challenging and often unsuitable in complex VSD. We report the case of a young woman in poor hemodynamic conditions due to a complex post-MI VSD. A two-step percutaneous VSD closure was successfully performed adopting a patient-tailored approach based on a throughout knowledge of the anatomic and functional picture using both commercially available dedicated and off-label devices.

Published
2017
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28. PARK2 Microduplication: Clinical and Molecular Characterization of a Further Case and Review of the Literature.

Author

Palumbo O, Palumbo P, Leone MP, Stallone R, Palladino T, Vendemiale M, Palladino S, Papadia F, Carella M, and Fischetto R

Abstract

We report on a patient with psychomotor deficits, language delay, dyspraxia, skeletal anomalies, and facial dysmorphisms (hirsutism, right palpebral ptosis, a bulbous nasal tip with enlarged and anteverted nares, and a mild prominent antihelix stem). Using high-resolution SNP array analysis, we identified a 0.49-Mb microduplication in chromosome 6q26 inherited from the mother involving the PARK2 gene: arr[hg19] 6q26(162,672,821-163,163,143)×3 mat. To the best of our knowledge, this is the third patient to date described in whom a 6q26 microduplication encompassing only the PARK2 gene has been reported in medical literature. The PARK2 gene is a neurodevelopmental gene that was initially discovered as one of the causes of autosomal recessive juvenile Parkinson disease and subsequently reported to be linked to autism spectrum disorders and attention-deficit hyperactivity disorders. We provide an overview of the literature on PARK2 microduplications and further delineate the associated phenotype. Taken together, our findings confirm the involvement of this gene in neurodevelopmental disorders and are useful to strengthen the hypothesis that, although with variable expressivity and incomplete penetrance, the PARK2 microduplication is associated with a new emerging neurodevelopmental delay syndrome. However, clinical and molecular evaluations of more patients with the microduplication are needed for full delineation of this syndrome.

Published
2016
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29. Expanding the mutation spectrum in 130 probands with ARPKD: identification of 62 novel PKHD1 mutations by sanger sequencing and MLPA analysis.

Author

Melchionda S, Palladino T, Castellana S, Giordano M, Benetti E, De Bonis P, Zelante L, and Bisceglia L

Subjects
Adolescent, Adult, Alleles, Amino Acid Substitution, Child, Child, Preschool, DNA Mutational Analysis, Female, Genotype, Humans, Infant, Male, Middle Aged, Multiplex Polymerase Chain Reaction, Polycystic Kidney, Autosomal Recessive diagnosis, Sequence Analysis, DNA, Young Adult, Mutation, Polycystic Kidney, Autosomal Recessive genetics, Receptors, Cell Surface genetics
Abstract

Autosomal recessive polycystic kidney disease (ARPKD) is a rare severe genetic disorder arising in the perinatal period, although a late-onset presentation of the disease has been described. Pulmonary hypoplasia is the major cause of morbidity and mortality in the newborn period. ARPKD is caused by mutations in the PKHD1 (polycystic kidney and hepatic disease 1) gene that is among the largest human genes. To achieve a molecular diagnosis of the disease, a large series of Italian affected subjects were recruited. Exhaustive mutation analysis of PKHD1 gene was carried out by Sanger sequencing and multiple ligation probe amplification (MLPA) technique in 110 individuals. A total of 173 mutations resulting in a detection rate of 78.6% were identified. Additional 20 unrelated patients, in whom it was not possible to analyze the whole coding sequence, have been included in this study. Taking into account the total number (n=130) of this cohort of patients, 107 different types of mutations have been detected in 193 mutated alleles. Out of 107 mutations, 62 were novel: 11 nonsense, 6 frameshift, 7 splice site mutations, 2 in-frame deletions and 2 multiexon deletion detected by MLPA. Thirty-four were missense variants. In conclusion, our report expands the spectrum of PKHD1 mutations and confirms the heterogeneity of this disorder. The population under study represents the largest Italian ARPKD cohort reported to date. The estimated costs and the time invested for molecular screening of genes with large size and allelic heterogeneity such as PKHD1 demand the use of next-generation sequencing (NGS) technologies for a faster and cheaper screening of the affected subjects.

Published
2016
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30. Clinical and molecular characterization of a de novo 19p13.3 microdeletion.

Author

Palumbo P, Palumbo O, Leone MP, Stallone R, Palladino T, Zelante L, and Carella M

Abstract

Background: Structural rearrangements of chromosome 19p13.3 are a rare condition, and their phenotypic consequences remain not well defined, because of the variability of clinical manifestations. Increasing knowledge of new 19p13.3 microdeletion is useful to clarify the phenotypic variability observed in some patients. In a small number of recent papers, patients with intellectual disabilities, multiple congenital anomalies and microdeletion of the chromosome band 19p13.3 have been described. However, little is known about genes responsible for clinical features in patients carriers of 19p13.3 microdeletion; thus, increasing number of reported cases will be helpful to investigate the contribution of candidate genes, providing bases for future investigations., Case Presentation: Here, we report on a 10-years-old girl referred to our genetics clinic due to intellectual disability, attention deficit, behavioral and speech delay, hypotonia, facial dysmorphisms, eye anomalies and congenital malformations. Using an high resolution SNP array, we identified a de novo microdeletion of chromosome 19p13.3, resulting in the heterozygous loss of 27 RefSeq genes and a miRNA, partially overlapping with three others deletions already reported in literature, but extending downstream (centromeric) for additional 386 Kb. This chromosomal region includes 13 genes amongst of which we suggest for the first time the APC2, PLK5 and MBD3 genes as potential functional candidates for neurodevelopmental and behavioral phenotypes observed., Conclusions: Here we describe a patient with a 19p13.3 microdeletion that spans to the downstream chromosomal region with respect to the overlapping deletions previously reported in several other cases. The neurobehavioral features observed in our case has extended the phenotypic spectrum associated with the 19p13.3 microdeletion. New candidate genes are proposed for the neurobehavioral phenotype observed in our case.

Published
2016
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32. Microdeletion of 12q24.31: report of a girl with intellectual disability, stereotypies, seizures and facial dysmorphisms.

Author

Palumbo O, Palumbo P, Delvecchio M, Palladino T, Stallone R, Crisetti M, Zelante L, and Carella M

Subjects
Child, Preschool, Chromosome Mapping, Comparative Genomic Hybridization, DNA Copy Number Variations, Facies, Female, Humans, Intellectual Disability diagnosis, Phenotype, Seizures diagnosis, Chromosome Deletion, Chromosomes, Human, Pair 12, Facial Bones abnormalities, Intellectual Disability genetics, Seizures genetics, Stereotyped Behavior
Abstract

We provide a detailed clinical and molecular characterization of an 11-year-old female patient presenting with neurodevelopmental delay (NDD), intellectual disability (ID), seizures, stereotypies and dysmorphic features. Chromosomal microarrays analysis (CMA) detected a small, rare de novo deletion on chromosome 12q24.31 encompassing 31 protein-coding RefSeq genes and a microRNA. Phenotypic comparison with molecularly well-defined cases previously reported in the literature harboring an overlapping 12q24.31 microdeletion indicate that these patients shared common clinical features including neurodevelopmental delay, intellectual disability and behavioral problems. Also, seizures and dysmorphic features are frequent and a consistent pattern was recognized. Since there are remarkable resemblance between the patient described here and at least another one previously reported, our report is provides supportive evidence for the existence of an emerging syndrome caused by a microdeletion in 12q24.31. We propose a minimal region shared among patients contributing to the etiology of the common clinical features observed suggesting as candidate, for the first time, the gene SETD1B which is a component of a histone methyltransferase complex. In addition, we speculate on the possible contributive role of the MIR4304 to some clinical features observed in our patient. Evaluation of more patients with well-characterized deletions within 12q24.31, as well as careful clinical assessment of them, is needed to corroborate our hypothesis, to perform a more detailed genotype-phenotype correlation and, finally, to fully delineate this emerging microdeletion syndrome., (© 2014 Wiley Periodicals, Inc.)

Published
2015
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33. 3p14.1 de novo microdeletion involving the FOXP1 gene in an adult patient with autism, severe speech delay and deficit of motor coordination.

Author

Palumbo O, D'Agruma L, Minenna AF, Palumbo P, Stallone R, Palladino T, Zelante L, and Carella M

Subjects
Abnormalities, Multiple genetics, Adult, Forkhead Transcription Factors metabolism, Haploinsufficiency, Humans, Karyotype, Magnetic Resonance Imaging, Male, Motor Activity genetics, Pedigree, Phenotype, Polymorphism, Single Nucleotide, Repressor Proteins metabolism, Sequence Analysis, DNA, Young Adult, Autistic Disorder genetics, Forkhead Transcription Factors genetics, Gene Deletion, Language Development Disorders genetics, Repressor Proteins genetics
Abstract

Interstitial deletion of chromosome region 3p14.1, including FOXP1 gene, is relatively rare and, until recently, there were no strong evidences to support the hypothesis that this microdeletion could play a role in the etiology of genomic disorders. Here, we report on an adult patient with a recognizable phenotype of autism, severe speech delay, deficit of motor coordination and typical dysmorphic features. Analysis of a dense whole genome single-nucleotide polymorphism (SNP) array showed a 1Mb interstitial deletion of chromosome region 3p14.1 including the entire coding region of FOXP1 (MIM 605515) gene. In order to study the parental origin of the deletion, we analyzed selected SNPs in the deleted area in the proband and his parents showing Mendelian incompatibilities suggesting a de novo deletion on the chromosome of paternal origin. Despite the frequency of this genomic alteration has not been estimated, our patient confirm the hypothesis that microdeletion of 3p14.1 seems to be a rare cause of cognitive disorders and that haploinsufficiency of FOXP1 may play a role in neurological and language deficits in patients carrying a 3p14.1 deletion. Finally, our patient is also important because useful to further delineate the clinical spectrum secondary to the 3p14.1 microdeletions., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published
2013
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34. 8q12.1q12.3 de novo microdeletion involving the CHD7 gene in a patient without the major features of CHARGE syndrome: case report and critical review of the literature.

Author

Palumbo O, Palumbo P, Stallone R, Palladino T, Zelante L, and Carella M

Subjects
Base Sequence, Child, Female, Humans, Polymorphism, Single Nucleotide, Severity of Illness Index, CHARGE Syndrome genetics, Chromosomes, Human, Pair 8 genetics, DNA Helicases genetics, DNA-Binding Proteins genetics, Sequence Deletion
Abstract

CHARGE syndrome is an autosomal dominant inherited disorder characterized by a specific and recognizable pattern of anomalies. De novo mutations or deletions of the gene encoding chromodomain helicase DNA binding protein 7 (CHD7) are the major cause of CHARGE syndrome. In this report, we describe a patient with a typical phenotype characterized by psychomotor retardation, hypertrichosis, facial asymmetry, synophria, failure to thrive, developmental delay and gastro-esophageal reflux, carrying a de novo 6.04Mb interstitial deletion in 8q12.1q12.3 detected by single nucleotide polymorphism (SNP) array analysis. Despite the deletion includes CHD7 and although the patient shares some of the clinical features of the CHARGE syndrome, she does not fulfill the clinical criteria for this syndrome. To the best of our knowledge, this is the second case with an entire deletion of the CHD7 gene not leading to CHARGE syndrome and, for this reason, useful to expand and further delineate the clinical features associated with the 8q12.1q12.3 deletion. Furthermore, the literature review revealed that the phenotype secondary to duplications of the same region partially overlaps with the phenotype reported in this study. Selected genes that are present in the hemizygous state and which might be important for the phenotype of this patient, are discussed in context of the clinical features., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published
2013
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35. An emerging phenotype of interstitial 15q25.2 microdeletions: clinical report and review.

Author

Palumbo O, Palumbo P, Palladino T, Stallone R, Miroballo M, Piemontese MR, Zelante L, and Carella M

Subjects
Abnormalities, Multiple genetics, Child, Female, Humans, Phenotype, Chromosome Deletion, Chromosomes, Human, Pair 15, Developmental Disabilities genetics, Sequence Deletion
Abstract

Interstitial deletions of chromosome 15q25.2 are rare. To date, only nine patients with microdeletions within this chromosomal region have been described. Here, we report on a girl with severe speech and psychomotor delay, behavioral problems and mild dysmorphic features with a 1.6 Mb deletion in 15q25.2 region. In order to study the parental origin of the rearrangement, we analyzed selected SNPs in the deleted area in the patient and her parents, showing Mendelian incompatibilities suggesting a de novo deletion on the chromosome of maternal origin. By comparing the clinical and molecular features of our patient with five previously reported cases of an overlapping deletion, we suggest that 15q25.2 deletion is an emerging syndrome characterized by a distinct although variable spectrum of clinical manifestations, including mild dysmorphic features, neurodevelopmental delay, and a recognizable pattern of congenital malformation. Furthermore, our patient is the second one in which a behavioral phenotype characterized by hyperactivity, anxiety, and autistic features was reported, indicating that these features might be part of this new syndromic condition. Breakpoints of the deletion in the patient reported here are useful to better define the smallest region of overlap (SRO) among all the patients. Selected genes that are present in the hemizygous state and which might be important for the phenotype of these patients, are discussed in context of the clinical features. In conclusion, our patient increases the knowledge about the molecular and phenotypic consequences of interstitial 15q25.2 deletions, highlighting that deletions of this region may be responsible for a new microdeletion syndrome., (Copyright © 2012 Wiley Periodicals, Inc.)

Published
2012
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36. Identification of a novel mutation in the SLC26A4 gene in an Italian with fluctuating sensorineural hearing loss.

Author

Cama E, Alemanno MS, Bellacchio E, Santarelli R, Carella M, Zelante L, Palladino T, Inches I, di Paola F, Arslan E, and Melchionda S

Subjects
Adolescent, Female, Follow-Up Studies, Goiter, Nodular diagnosis, Goiter, Nodular genetics, Hearing Loss, Sensorineural physiopathology, Humans, Italy, Magnetic Resonance Imaging methods, Mutation, Severity of Illness Index, Sulfate Transporters, Tomography, X-Ray Computed methods, Hearing Loss, Sensorineural diagnosis, Hearing Loss, Sensorineural genetics, Membrane Transport Proteins genetics
Abstract

Pendred syndrome is an autosomal recessive disorder characterized by congenital sensorineural deafness, goitre and defective iodide organification. Congenital and profound hearing loss is the hallmark of the syndrome, while goitre and thyroid dysfunction are highly variable even within the same family. Clinical features are due to altered formation of pendrin, a chloride/iodide transporter protein expressed in the inner ear, thyroid gland and kidney. A novel substitution was found in exon 7 of the pendrin encoding gene (SLC26A4) that leads to a stop codon, S314X. The new variation was found in compound heterozygosity with L445W mutation in a hearing impaired patient with bilateral Mondini's dysplasia and goitre.

Published
2009
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37. A novel missense mutation in the Connexin 26 gene associated with autosomal recessive nonsyndromic sensorineural hearing loss in a consanguineous Tunisian family.

Author

Alemanno MS, Cama E, Santarelli R, Carella M, Zelante L, Toffolatti L, Palladino T, Melchionda S, and Arslan E

Subjects
Child, Preschool, Connexin 26, Consanguinity, Female, Hearing Loss, Sensorineural congenital, Hearing Loss, Sensorineural diagnosis, Humans, Pedigree, Tunisia, Connexins genetics, Hearing Loss, Sensorineural genetics, Inheritance Patterns genetics, Mutation, Missense genetics
Abstract

Nonsyndromic sensorineural hearing impairment is inherited in a predominantly autosomal recessive manner in up to 70% of cases. The gene more often involved is GJB2, encoding the gap junction protein Connexin 26. We report here a novel missense mutation in the GJB2 gene found in a Tunisian family. A homozygous change C/G at nucleotide 263 was detected in the 4-year-old girl of this family, affected by congenital moderate hearing loss. This transversion leads to the replacement of a highly conserved alanine with glycine at codon 88 (A88G). The consanguineous parents of the child are healthy carriers of the mutation.

Published
2009
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38. Hearing loss features in GJB2 biallelic mutations and GJB2/GJB6 digenic inheritance in a large Italian cohort.

Author

Cama E, Melchionda S, Palladino T, Carella M, Santarelli R, Genovese E, Benettazzo F, Zelante L, and Arslan E

Subjects
Acoustic Impedance Tests, Adolescent, Adult, Aged, Alleles, Audiometry, Pure-Tone, Auditory Perception, Child, Child, Preschool, Cohort Studies, Connexin 26, Connexin 30, Disease Progression, Female, Genetic Predisposition to Disease, Hearing Loss, Sensorineural physiopathology, Heterozygote, Homozygote, Humans, Infant, Inheritance Patterns, Italy, Male, Middle Aged, Otoscopy, Phenotype, Reflex, Acoustic, Retrospective Studies, Young Adult, Connexins genetics, Hearing Loss, Sensorineural genetics, Mutation
Abstract

The aim of this study was to describe the clinical features of hearing loss due to mutations on connexin 26/30 coding genes (GJB2/GJB6). Mutations in the GJB2 gene are found to account for approximately 50% of cases of autosomal recessive non-syndromic deafness. Several European studies have estimated that the GJB2 healthy carrier condition involves about 2-4% of the population, with the 35delG mutations being the most common. A 342-kb deletion truncating the GJB6 gene (encoding connexin-30) has been associated with autosomal recessive non-syndromic deafness, mostly as digenic inheritance of the Cx30 deletion/Cx26 mutation. The following retrospective study describes audiological features and genotypes of a large cohort of 376 Italian hearing-impaired patients who underwent genetic screening for the GJB2/GJB6 genes and received follow-up care at our centre between January 2002 and October 2006. Sixteen different genotypes causing deafness in more than 27% of patients with either biallelic mutations or digenic inheritance GJB2/GJB6 were identified. The most frequent mutations were 35delG, M34T, L90P, and R184P.

Published
2009
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39. Pendred syndrome: study of three families.

Author

Bigozzi M, Melchionda S, Casano R, Palladino T, and Gitti G

Subjects
Connexin 26, DNA Primers genetics, Humans, Pedigree, Polymerase Chain Reaction, Severity of Illness Index, Syndrome, Connexins genetics, Deafness complications, Deafness genetics, Goiter complications, Goiter genetics
Abstract

Although the textbook view of the Pendred syndrome is that of an autosomal recessive condition characterised by deafness and goitre, it is increasingly clear that not all patients present this classical clinical description. Malform-ations of the inner ear, specifically, enlargement of the vestibular aqueduct, are common in the Pendred syndrome. Mutations in the Pendred syndrome gene have been observed in patients with deafness and vestibular aqueduct dilatation, in the absence of other Pendred syndrome features. In our study, all patients with congenital profound or severe sensory-neural deafness were evaluated using computed tomography and magnetic resonance imaging, followed by genetic examinations and blood tests. The procedure followed was the sensory-neural child deafness protocol elaborated by the Joint Committee for Infant Hearing based on skull and petrous bone. In 3 families, the computed tomography scans (performed on 7 out of 8 of these deaf subjects) showed enlarged vestibular aqueducts. The present study evaluates whether or not enlargement of the vestibular aqueduct should be considered as the most likely presentation of the Pendred syndrome.

Published
2005

40. Breast fibroadenoma in a male-to-female transsexual patient after hormonal treatment.

Author

Lemmo G, Garcea N, Corsello S, Tarquini E, Palladino T, Ardito G, and Garcea R

Subjects
Adult, Humans, Male, Androgen Antagonists administration & dosage, Breast Neoplasms, Male pathology, Cyproterone Acetate administration & dosage, Ethinyl Estradiol administration & dosage, Fibroadenoma pathology, Transsexualism pathology
Published
2003

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