Your search keyword '"Saadet Mercimek-Mahmutoglu"' showing total 7 results

1. Variable expressivity of a likely pathogenic variant in KCNQ2 in a three-generation pedigree presenting with intellectual disability with childhood onset seizures

Author

Stacy Hewson, Saadet Mercimek-Mahmutoglu, and Klajdi Puka

Subjects

Adult, Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Encephalopathy, 03 medical and health sciences, 0302 clinical medicine, Seizures, Intellectual Disability, Intellectual disability, Genetics, medicine, Humans, KCNQ2 Potassium Channel, Genetic Predisposition to Disease, Benign familial neonatal seizures, Global developmental delay, Genetics (clinical), Likely pathogenic, Exome sequencing, Aged, business.industry, Cognition, Middle Aged, medicine.disease, Pedigree, 030104 developmental biology, Child, Preschool, Mutation, Female, Differential diagnosis, business, Spasms, Infantile, 030217 neurology & neurosurgery

Abstract

KCNQ2 has been reported as a frequent cause of autosomal dominant benign familial neonatal seizures. De novo likely pathogenic variants in KCNQ2 have been described in neonatal or early infantile onset epileptic encephalopathy patients. Here, we report a three-generation family with six affected patients with a novel likely pathogenic variant (c.628C>T; p.Arg210Cys) in KCNQ2. Four family members, three adults and a child, presented with a childhood seizure onset with variability in the severity of seizures and response to treatment, intellectual disability (ID) as well as behavioral problems. The two youngest affected patients had a variable degree of global developmental delay with no seizures at their current age. This three-generation family with six affected members expands the phenotypic spectrum of KCNQ2 associated encephalopathy to KCNQ2 associated ID and or childhood onset epileptic encephalopathy. We think that KCNQ2 associated epileptic encephalopathy should be included in the differential diagnosis of childhood onset epilepsy and early onset global developmental delay, cognitive dysfunction, or ID. Furthermore, whole exome sequencing in families with ID and history of autosomal dominant inheritance pattern with or without seizures, may further broaden the phenotypic spectrum of KCNQ2 associated epileptic encephalopathy or encephalopathy.

Published

2017

2. BCAP31- associated encephalopathy and complex movement disorder mimicking mitochondrial encephalopathy

Author

Saadet Mercimek-Mahmutoglu, Saleh Albanyan, Nasim Monfared, and Amal Al Teneiji

Subjects

Male, 0301 basic medicine, Heterozygote, Microcephaly, Pathology, medicine.medical_specialty, Hearing Loss, Sensorineural, Encephalopathy, Choreoathetosis, 03 medical and health sciences, Mitochondrial Encephalomyopathies, otorhinolaryngologic diseases, Genetics, medicine, Humans, Global developmental delay, Genetics (clinical), Exome sequencing, Dystonia, Movement Disorders, Muscle biopsy, medicine.diagnostic_test, business.industry, Membrane Proteins, medicine.disease, 030104 developmental biology, Child, Preschool, Mutation, Sensorineural hearing loss, medicine.symptom, business

Abstract

BCAP31, encoded by BCAP31, is involved in the export of transmembrane proteins from the endoplasmic reticulum. Pathogenic variants in BCAP31 results in global developmental delay, dystonia, deafness and dysmorphic features in males, called deafness, dystonia, and cerebral hypomyelination (DDCH) syndrome. We report a new patient with BCAP3-associated encephalopathy, DDCH syndrome, sensorineural hearing loss, generalized dystonia, and choreoathetosis. This 3.5-year-old boy had microcephaly and failure to thrive within the first 3 months of life. His brain MRI showed bilateral increased signal intensity in globus pallidus at age 3 months raising the suspicion of mitochondrial encephalopathy. His muscle biopsy revealed pleomorphic subsarcolemmal mitochondria collection in electron microscopy. Respiratory chain enzyme activities were normal in muscle. He was enrolled to a whole exome sequencing research study, which identified a hemizygous likely pathogenic truncating variant (c.533_536dup; p.Ser180AlafsX6) in BCAP31, inherited from his mother, who had sensorineural hearing loss and normal cognitive functions. We report a new patient with BCAP31-associated encephalopathy, DDCH syndrome, mimicking mitochondrial encephalopathy. We also report a heterozygous mother who has bilateral sensorineural hearing loss. This patient's clinical features, muscle histopathology, brain MRI features, and family history were suggestive of mitochondrial encephalopathy. Whole exome sequencing research study confirmed the diagnosis of BCAP31-associated encephalopathy, DDCH syndrome.

Published

2017

3. MED23-associated refractory epilepsy successfully treated with the ketogenic diet

Author

Saadet Mercimek-Mahmutoglu, Anath C. Lionel, Nasim Monfared, Stephen W. Scherer, and Christian R. Marshall

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Microcephaly, Genotype, medicine.medical_treatment, Energy homeostasis, 03 medical and health sciences, Epilepsy, 0302 clinical medicine, Internal medicine, Genetics, medicine, Humans, Global developmental delay, Allele, Child, Alleles, Genetic Association Studies, Genetics (clinical), Exome sequencing, Mediator Complex, business.industry, Brain, Electroencephalography, medicine.disease, Magnetic Resonance Imaging, Phenotype, Treatment Outcome, 030104 developmental biology, Endocrinology, Gluconeogenesis, Mutation, Diet, Ketogenic, business, 030217 neurology & neurosurgery, Ketogenic diet

Abstract

We report a new patient with refractory epilepsy associated with a novel pathogenic homozygous MED23 variant. This 7.5-year-old boy from consanguineous parents had infantile onset global developmental delay and refractory epilepsy. He was treated with the ketogenic diet at 2.5 years of age and became seizure free on the first day. He had microcephaly and truncal hypotonia. His brain MRI showed delayed myelination and thin corpus callosum. He was enrolled in a whole exome sequencing research study, which identified a novel, homozygous, likely pathogenic (c.1937A>G; p.Gln646Arg) variant in MED23. MED23 is a regulator of energy homeostasis and glucose production. Liver-specific Med23-knockout mice showed reduced liver gluconeogenesis and lower blood glucose levels compared to control mice. This is the first patient with documented refractory epilepsy caused by a novel homozygous pathogenic variant in MED23 expanding the phenotypic spectrum. Identification of the underlying genetic defect in MED23 sheds light on the possible mechanism of complete response to the ketogenic diet in this child. © 2016 Wiley Periodicals, Inc.

Published

2016

4. Nomenclature of genetic movement disorders: Recommendations of the international Parkinson and movement disorder society task force

Author

Sarah J. Tabrizi, Vladimir S. Kostic, Bart P.C. van de Warrenburg, Katja Lohmann, Birgit Assmann, Thomas T. Warner, Connie Marras, Darius Ebrahimi-Fakhari, Saadet Mercimek-Mahmutoglu, Anthony E. Lang, Lars Bertram, Carolyn M. Sue, Alexandra Durr, and Christine Klein

Subjects

0301 basic medicine, Dystonia, Ataxia, Movement disorders, Hereditary spastic paraplegia, Neurodegeneration with brain iron accumulation, Parkinsonism, Chorea, medicine.disease, 3. Good health, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Neurology, medicine, Neurology (clinical), medicine.symptom, Psychology, Neuroscience, Machado–Joseph disease, 030217 neurology & neurosurgery

Abstract

The system of assigning locus symbols to specify chromosomal regions that are associated with a familial disorder has a number of problems when used as a reference list of genetically determined disorders,including (I) erroneously assigned loci, (II) duplicated loci, (III) missing symbols or loci, (IV) unconfirmed loci and genes, (V) a combination of causative genes and risk factor genes in the same list, and (VI) discordance between phenotype and list assignment. In this article, we report on the recommendations of the International Parkinson and Movement Disorder Society Task Force for Nomenclature of Genetic Movement Disorders and present a system for naming genetically determined movement disorders that addresses these problems. We demonstrate how the system would be applied to currently known genetically determined parkinsonism, dystonia, dominantly inherited ataxia, spastic paraparesis, chorea, paroxysmal movement disorders, neurodegeneration with brain iron accumulation, and primary familial brain calcifications. This system provides a resource for clinicians and researchers that, unlike the previous system, can be considered an accurate and criterion-based list of confirmed genetically determined movement disorders at the time it was last updated.

Published

2016

5. Diagnostic yield of genetic testing in epileptic encephalopathy in childhood

Author

O. Carter Snead, Jeff Kobayashi, Berge A. Minassian, Dawn Cordeiro, David F. Callen, Cecil D. Hahn, Stacy Hewson, Saadet Mercimek-Mahmutoglu, Jaina Patel, Mahendranath Moharir, Rosanna Weksberg, Komudi Siriwardena, Shelly K. Weiss, Elizabeth J. Donner, and Peter Kannu

Subjects

Male, Pathology, medicine.medical_specialty, Sodium-Hydrogen Exchangers, Adolescent, Methylenetetrahydrofolate reductase deficiency, Developmental Disabilities, Biology, Glycine encephalopathy, Bioinformatics, Cohort Studies, Epilepsy, Munc18 Proteins, Molecular genetics, medicine, Humans, KCNQ2 Potassium Channel, Genetic Predisposition to Disease, Global developmental delay, Child, Pyridoxine-dependent epilepsy, Genetic testing, NAV1.2 Voltage-Gated Sodium Channel, medicine.diagnostic_test, Infant, Cadherins, medicine.disease, Protocadherins, Neurology, Child, Preschool, Mutation, Female, Menkes disease, Neurology (clinical), Cognition Disorders, Spasms, Infantile

Abstract

SummaryObjective Epilepsy is a common neurologic disorder of childhood. To determine the genetic diagnostic yield in epileptic encephalopathy, we performed a retrospective cohort study in a single epilepsy genetics clinic. Methods We included all patients with intractable epilepsy, global developmental delay, and cognitive dysfunction seen between January 2012 and June 2014 in the Epilepsy Genetics Clinic. Electronic patient charts were reviewed for clinical features, neuroimaging, biochemical investigations, and molecular genetic investigations including targeted next-generation sequencing of epileptic encephalopathy genes. Results Genetic causes were identified in 28% of the 110 patients: 7% had inherited metabolic disorders including pyridoxine dependent epilepsy caused by ALDH7A1 mutation, Menkes disease, pyridox(am)ine-5-phosphate oxidase deficiency, cobalamin G deficiency, methylenetetrahydrofolate reductase deficiency, glucose transporter 1 deficiency, glycine encephalopathy, and pyruvate dehydrogenase complex deficiency; 21% had other genetic causes including genetic syndromes, pathogenic copy number variants on array comparative genomic hybridization, and epileptic encephalopathy related to mutations in the SCN1A, SCN2A, SCN8A, KCNQ2, STXBP1, PCDH19, and SLC9A6 genes. Forty-five percent of patients obtained a genetic diagnosis by targeted next-generation sequencing epileptic encephalopathy panels. It is notable that 4.5% of patients had a treatable inherited metabolic disease. Significance To the best of our knowledge, this is the first study to combine inherited metabolic disorders and other genetic causes of epileptic encephalopathy. Targeted next-generation sequencing panels increased the genetic diagnostic yield from 25% in patients with epileptic encephalopathy.

Published

2015

6. Reply letter to Jinnah 'Locus pocus' and Albanese 'Complex dystonia is not a category in the new 2013 consensus classification': Necessary evolution, no magic!

Author

Saadet Mercimek-Mahmutoglu, Connie Marras, Lars Bertram, Thomas T. Warner, Birgit Assmann, Sarah J. Tabrizi, Katja Lohmann, B.P.C. van de Warrenburg, Carolyn M. Sue, Christine Klein, Anthony E. Lang, Alexandra Durr, Darius Ebrahimi-Fakhari, and Vladimir S. Kostic

Subjects

0301 basic medicine, Dystonia, Cognitive science, business.industry, Locus (genetics), medicine.disease, Clinical neurology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Neurology, medicine, Neurology (clinical), business, 030217 neurology & neurosurgery

Published

2016

7. Pseudohypoparathyroidism type 1a and the GNAS p.R231H mutation: Somatic mosaicism in a mother with two affected sons

Author

Siu-Li Yong, Laura Stewart, William T. Gibson, Chieko Chijiwa, Wendy P. Robinson, Ying Fai Ngai, and Saadet Mercimek-Mahmutoglu

Subjects

Adult, Male, musculoskeletal diseases, Heterozygote, medicine.medical_specialty, Adolescent, Somatic cell, Germline mosaicism, Molecular cloning, Pregnancy, Internal medicine, Chromogranins, GTP-Binding Protein alpha Subunits, Gs, Genetics, medicine, GNAS complex locus, Humans, Child, Genetics (clinical), Pseudohypoparathyroidism, biology, Mosaicism, Infant, Newborn, Middle Aged, medicine.disease, Phenotype, Osteochondrodysplasia, Endocrinology, Amino Acid Substitution, Child, Preschool, Mutation, Mutation (genetic algorithm), biology.protein, Female

Abstract

Pseudohypoparathyrodism (PHP) is a disorder caused by mutations in the guanine nucleotide-binding α-subunit (GNAS). We sought to determine the genetic origin of PHP1a in one affected family. We identified the previously reported Gsα R231H mutation in family members affected with PHP1a. DNA analysis found that the two clinically affected sons are heterozygous for the mutation. The sons have PHP1a, manifesting obesity, intellectual disability, hypogonadism, hypothyroidism and elevated PTH levels. Initial DNA sequencing did not detect the mutation in either parent. However, their mother displayed some features of PHP, including elevated PTH levels and asymmetrical metacarpal shortening. Using molecular cloning, we detected the mutation at low levels in the mother's leukocyte DNA, consistent with somatic mosaicism and her mildly affected status. Thus, we have identified additional cases of PHP1a caused by the Gsα R231H mutation. In this family, the mother has a milder phenotype due in part to somatic mosaicism, whereas the two affected sons have full PHP1a. Though somatic mosaicism for activating GNAS mutations is known to occur in McCune–Albright syndrome, this is the first report confirming somatic mosaicism for a hypofunctioning GNAS mutation in a PHP kindred. © 2010 Wiley-Liss, Inc.

Published

2010