Your search keyword '"Houda Nehdi"' showing total 7 results

1. Clinical features and molecular genetics of two Tunisian families with abetalipoproteinemia

Author

Ghada El Euch-Fayache, Moncef Feki, Rim Amouri, Houda Nehdi, Wieme Maamouri-Hicheri, Monia B. Hammer, and Fayçal Hentati

Subjects

Foot Deformities, Male, medicine.medical_specialty, Tunisia, Adolescent, Apolipoprotein B, Nonsense mutation, Acanthocytes, medicine.disease_cause, Microsomal triglyceride transfer protein, Young Adult, symbols.namesake, Physiology (medical), Molecular genetics, medicine, Humans, Family, Child, Genetics, Sanger sequencing, Mutation, ABL, Base Sequence, biology, Foot, Abetalipoproteinemia, Sequence Analysis, DNA, General Medicine, medicine.disease, Pedigree, Neurology, Codon, Nonsense, Child, Preschool, biology.protein, symbols, Female, lipids (amino acids, peptides, and proteins), Surgery, Neurology (clinical), Carrier Proteins

Abstract

Abetalipoproteinemia (ABL) is a rare monogenic disease characterized by very low plasma levels of cholesterol and triglyceride and almost complete absence of apolipoprotein B (apoB)-containing lipoproteins. Typically, patients present with failure to thrive, acanthocytosis, pigmented retinopathy and neurological features. It has been shown that ABL results from mutations in the gene encoding the microsomal triglyceride transfer protein (MTTP). Sanger sequencing of MTTP was performed for two unrelated consanguineous Tunisian families with two affected individuals each, presenting a more severe ABL phenotype than previously reported in the literature. The patients were found to be homozygous for two novel mutations. In the first family, a nonsense mutation, c.2313T>A, leading to a truncated protein (p.Y771X) was identified. In the second family, a splice mutation, IVS 9+2T>G, was found. These mutations are believed to abolish the assembly and secretion of apoB-containing lipoproteins.

Published

2014

2. SLC25A46 Mutations Associated with Autosomal Recessive Cerebellar Ataxia in North African Families

Author

Alexandra Durr, Monia B. Hammer, Rim Amouri, Ghada Eleuch-Fayache, Sean B. Chong, Jinhui Ding, Steven J. Clipman, Andrew B. Singleton, Fanny Mochel, Perrine Charles, Houda Nehdi, Giovanni Stevanin, Marie Coutelier, Dena G. Hernandez, Elisa Majounie, J. Raphael Gibbs, Alexis Brice, Fayçal Hentati, Yosr Bouhlal, and Sampath Arepalli

Subjects

0301 basic medicine, Adult, Male, genetic structures, Cerebellar Ataxia, DNA Mutational Analysis, Biology, Article, Mitochondrial Proteins, 03 medical and health sciences, Consanguinity, 0302 clinical medicine, medicine, Humans, Phosphate Transport Proteins, Genetics, Family Health, Genetic heterogeneity, Autosomal recessive cerebellar ataxia, medicine.disease, Magnetic Resonance Imaging, eye diseases, 030104 developmental biology, Neurology, Mutation, North America, North african, Female, sense organs, Neurology (clinical), human activities, 030217 neurology & neurosurgery

Abstract

Background: Autosomal recessive cerebellar ataxias (ARCA) are a complex group of neurodegenerative disorders with high clinical and genetic heterogeneity. In most cases, the cerebellar ataxia is not pure, and complicating clinical features such as pyramidal signs or extraneurological features are found. Objective: To identify the genetic origin of the cerebellar ataxia for 3 consanguineous North African families presenting with ARCA. Methods: Genome-wide high-density SNP genotyping and whole-exome sequencing were performed followed by Sanger sequencing for mutation confirmation. Results: Two variants were identified in SLC25A46. Mutations in this gene have been previously associated with Charcot-Marie-Tooth type 2 and optic atrophy. While the previously reported variant p.Arg340Cys seems to be consistently associated with the same clinical features such as childhood onset, optic atrophy, gait and speech difficulties, and wasting of the lower limbs, the patient with the novel mutation p.Trp160Ser did not present with optic atrophy and his ocular abnormalities were limited to nystagmus and saccadic pursuit. Conclusion: In this study, we report a novel variant (p.Trp160Ser) in SLC25A46 and we broaden the phenotypic spectrum associated with mutations in SLC25A46.

Published

2016

3. Spinal Muscular Atrophy Due to Double Gene Conversion Event

Author

Yosr Bouhlel, Najla Khmiri, Sihem Souilem, Rim Amouri, Houda Nehdi, Monia B. Hammer, Fayçal Hentati, and Wiéme Maamouri

Subjects

Male, Sequence analysis, animal diseases, Gene Conversion, Spinal Muscular Atrophies of Childhood, Biology, Exon, medicine, Humans, Multiplex ligation-dependent probe amplification, Gene conversion, Gene, Base Sequence, General Neuroscience, Infant, Exons, General Medicine, Spinal muscular atrophy, SMA, medicine.disease, Spinal cord, Survival of Motor Neuron 1 Protein, Molecular biology, nervous system diseases, Survival of Motor Neuron 2 Protein, medicine.anatomical_structure, nervous system, Gene Deletion

Abstract

Spinal muscular atrophy (SMA) is an autosomal recessive disease characterized by degeneration of the anterior horn cells of the spinal cord. The survival motor neuron (SMN) gene has been identified as an SMA-determining gene. SMN exists as two copies in 5q13, and deletions in exons 7 and 8 of the telomeric copy (SMN(T)) occur in 95% of patients, regardless of disease severity. In a minority of patients, exon 7 but not exon 8 of SMN(T) appears deleted. We now report a patient with typical features of SMA type II who carried homozygous deletions of SMN(T) exon 7 and centromeric SMN (SMN(C)) exon 8 but retained SMN(T) exon 8 and SMN(C) exon 7. Sequence analysis demonstrated that SMN(C) exon 7 was adjacent to SMN(T) exon 8 on both SMN copies, indicating a double conversion. We confirm that sequence conversion is a common event in SMA and is associated with the milder form of the disease. The severity, however, can be modified in either positive or negative direction by other factors.

Published

2010

4. Clinical and molecular findings of ataxia with oculomotor apraxia type 2 (AOA2) in 5 Tunisian families

Author

Fatma Nabli, Ghada El Euch-Fayache, Yosr Bouhlal, Monia B. Hammer, Amira Nasri, Houda Nehdi, Fayçal Hentati, Wieme Maamouri-Hicheri, Dalel Saidi, and Rim Amouri

Subjects

Male, Ataxia, Tunisia, Adolescent, Nonsense mutation, DNA Mutational Analysis, Mutation, Missense, Consanguinity, Biology, Gene mutation, medicine.disease_cause, Pathology and Forensic Medicine, Young Adult, medicine, Missense mutation, Humans, Spinocerebellar Ataxias, Oculomotor apraxia, Age of Onset, Child, Molecular Biology, Spinocerebellar Degenerations, Genetics, Family Health, Mutation, DNA Helicases, Autosomal recessive cerebellar ataxia, Cell Biology, medicine.disease, Multifunctional Enzymes, Codon, Nonsense, Female, medicine.symptom, RNA Helicases

Abstract

Ataxia with oculomotor apraxia type 2 (AOA2) is a recently described autosomal recessive cerebellar ataxia caused by mutations in the SETX gene. It is a rare monogenic disease characterized by progressive cerebellar ataxia, oculomotor apraxia, axonal sensorimotor neuropathy, and an elevated serum α-fetoprotein level. To date, >100 AOA2 patients have been described and 75 different mutations in the SETX gene have been identified. We report here the clinical and genetic findings of 13 AOA2 patients from 5 unrelated Tunisian consanguineous families. DNA was collected from probands and available family members, and the 24 SETX exons were screened by direct sequencing. Four different homozygous SETX gene mutations were identified. The missense mutation 915G>T [W305C] has been described previously in Algeria. The 3 other SETX mutations are novel, including a missense mutation c.7231C>T [R 2380 W], a nonsense mutation c.6475 C>T [R2098X], and a deletion c.7180-7183delAAAA [D2332fsX2343]. More extensive screening by molecular genetic analysis of SETX in patients with Friedreich ataxia-like phenotype may show that AOA2 is more common in Tunisia than previously thought.

Published

2012

5. Allelic ROBO3 heterogeneity in Tunisian patients with horizontal gaze palsy with progressive scoliosis

Author

Houda Nehdi, Fayçal Hentati, M. Kefi, A. Larnaout, Yosr Bouhlal, and Rim Amouri

Subjects

Adult, Genetic Markers, Male, medicine.medical_specialty, Neurology, Tunisia, Adolescent, DNA Mutational Analysis, Receptors, Cell Surface, Scoliosis, Gene mutation, Biology, Allelic Imbalance, medicine.disease_cause, Nervous System Malformations, Cellular and Molecular Neuroscience, Young Adult, Ocular Motility Disorders, Cerebellum, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Allele, Receptors, Immunologic, Child, Gene, Genetics, Mutation, Chromosome Mapping, Genetic Variation, Horizontal gaze palsy, General Medicine, medicine.disease, Gaze, Magnetic Resonance Imaging, Disease Progression, Female, Brain Stem

Abstract

Horizontal gaze palsy with progressive scoliosis (HGPPS) is a rare autosomal recessive disorder characterized by the congenital absence of horizontal gaze, progressive scoliosis, and failure of the corticospinal and somatosensory axon tracts to decussate in the medulla. HGPPS is caused by mutations of the ROBO3 gene, which encodes a protein that shares homology with the roundabout family of transmembrane receptors that are important in axon guidance and neuronal migration. To date, over 15 mutations have been found in consanguineous families of Greek, Italian, Turkish, Pakistani, Saudi Arabian, and Indian descent. To detail clinical, cerebral magnetic resonance imaging (MRI) and genetic findings of ten HGPPS patients from four unrelated Tunisian families. Four unrelated consanguineous Tunisian families with a total of ten patients suffering from horizontal gaze palsy with progressive scoliosis. Genetic linkage analysis and direct sequencing of the ROBO3 gene. All patients shared similar clinical gaze movement abnormalities and variable degrees of scoliosis. Four distinct homozygous mutations were identified. This study extends the molecular spectrum of the ROBO3 gene and the geographic origin of patients with ROBO3 gene mutations, and underlines the homogeneity of the motor ocular syndrome whatever type of mutation is encountered.

Published

2009

6. Front & Back Matter

Author

Hana Stufkova, Jessica Mandrioli, Amelia Conte, Federica Violi, Elmar H. Pinkhardt, Takahiro Fukuda, Maria Carmela Tartaglia, Yosr Bouhlal, Hans-Jürgen Huppertz, Andrew B. Singleton, Daniela Vidinska, Marie Coutelier, Carla Sanchis-Segura, Ai-Ling Shen, David S. Howland, Margot Samson, María Sol Fittipaldi-Márquez, Alexis Brice, Jos Prinzen, Marco Vinceti, Francesco Curcio, Sean B. Chong, Mario Sabatelli, Chien-Yeh Hsu, Satz Mengensatzproduktion, Nuno Sousa, Giovanni Stevanin, Samir Abu-Rumeileh, Peter Grill, Che-Yi Chou, Ricardo Taipa, Valeria A. Sansone, Monika Macakova, Daniela Berg, Rob van Lummel, Rim Amouri, Antonio Baldi, Hsiu-Chen Lin, Hisashi Hashimoto, Olga Vintonyak, Jiri Klima, Perrine Charles, Nova Sanvilli, Jinhui Ding, Yuan-Fu Tseng, Daniel O. Claassen, Antonio Belenguer, Jana Krizova, Sampath K. Arepalli, Marie Rodinova, Manuel Melo Pires, Christian Lunetta, Cristina Forn, Alexandra Durr, Elisa Majounie, Markus A. Hobert, Gian Luigi Gigli, Silvia Del Din, Martina Fabris, Andrew C Robinson, Ghada Eleuch-Fayache, Jan Motlik, Steven J. Clipman, Inga Liepelt-Scarfone, Faycal Hentati, Dominik Blum, Zdenka Ellederova, Bernhard Cerff, Druckerei Stückle, J. Raphael Gibbs, Bernhard Michalke, Hana Hansikova, Hsiu-Li Lin, Sebastiano D'Anna, Cassandra Jessica Anor, Hans-Peter Müller, Dena G. Hernandez, Malte Kampmeyer, Tomonori Kawabe, César Ávila, Lucio D'Anna, Fanny Mochel, Houda Nehdi, Bozena Bohuslavova, Monia B. Hammer, Paulo Brochado, Mariarosaria Valente, David M. A. Mann, Nikolay Solovyev, Patrício Costa, Walter Maetzler, David F. Tang-Wai, Álvaro Javier Cruz-Gómez, Ron Keren, Cinzia Pistis, Albert C. Ludolph, Martin Gorges, Patricia Sulzer, Antonin Pavlok, Moriaki Kusakabe, Susanne Gräber, Sean O'Connor, Jiri Zeman, Amardeep Saund, Inês Reis, and Jan Kassubek

Subjects

Optics, Neurology, business.industry, Neurology (clinical), Dermatology, business, Geology, Front (military)

Published

2012

7. Mutations in GBA2 Cause Autosomal-Recessive Cerebellar Ataxia with Spasticity

Author

Henry Houlden, Monia B. Hammer, Rim Amouri, A Sailer, Sean B. Chong, J. Raphael Gibbs, Huaibin Cai, Houda Nehdi, Lucia Schottlaender, Celeste Sassi, Yosr Bouhlal, Pramod K. Mistry, Sampath Arepalli, Ghada Eleuch-Fayache, Ginamarie Shrader, Guoxiang Liu, Andrew B. Singleton, Dena G. Hernandez, and Fayçal Hentati

Subjects

Adult, Male, Tunisia, Ataxia, Adolescent, Cerebellar Ataxia, DNA Mutational Analysis, Molecular Sequence Data, Nonsense mutation, Genes, Recessive, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Report, Genetics, medicine, Lysosomal storage disease, Humans, Family, Genetics(clinical), Amino Acid Sequence, Child, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Mutation, Base Sequence, Cerebellar ataxia, beta-Glucosidase, Glucosylceramidase activity, Autosomal recessive cerebellar ataxia, Disease gene identification, medicine.disease, Pedigree, 3. Good health, Muscle Spasticity, Child, Preschool, Glucosylceramidase, Female, medicine.symptom, 030217 neurology & neurosurgery

Abstract

Autosomal-recessive cerebellar ataxia (ARCA) comprises a large and heterogeneous group of neurodegenerative disorders with more than 20 different forms currently recognized, many of which are also associated with increased tone and some of which have limb spasticity. Gaucher disease is a lysosomal storage disease resulting from a defect in the enzyme acid β-glucosidase 1. β-glucosidase 2 is an enzyme with similar glucosylceramidase activity but to date has not been associated with a monogenic disorder. We studied four unrelated consanguineous families of Tunisian decent diagnosed with cerebellar ataxia of unknown origin. We performed homozygosity mapping and whole-exome sequencing in an attempt to identify the genetic origin of their disorder. We were able to identify mutations responsible for autosomal-recessive ataxia in these families within the gene encoding β-glucosidase 2, GBA2. Two nonsense mutations (c.363CA [p.Tyr121(∗)] and c.1018CT [p.Arg340(∗)]) and a substitution (c.2618GA [p.Arg873His]) were identified, probably resulting in nonfunctional enzyme. This study suggests GBA2 mutations are a cause of recessive spastic ataxia and responsible for a form of glucosylceramide storage disease in humans.