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8. A Case Report of Parental Germline Mosaicism in the PCDH19 Gene of Two Iranian Siblings.

Author

Alijanpour, Sahar, Ghafouri-Fard, Soudeh, Tonekaboni, Seyed Hassan, Karimzadeh, Parvaneh, Ahmadabadi, Farzad, Rahimian, Elham, Panjeshahi, Samareh, and Miryounesi, Mohammad

Subjects
GENETIC variation, GENETIC testing, GENETIC counseling, IRANIANS, MOSAICISM
Abstract

Introduction: Developmental and epileptic encephalopathy 9 (DEE9) is caused by pathogenic variants in the PCDH19 gene. The clinical features include early-onset seizures that are often provoked by fever and display clustered seizures, mild to profound intellectual disability, autistic traits, and behavioral disturbances. DEE9 is characterized by an unusual X-linked pattern where heterozygous females or rarely mosaic hemizygous males are affected, but hemizygous males and homozygous females are asymptomatic. In recent years, an increasing number of female and male patients with PCDH19-related epilepsy and symptoms have been reported. Methods: Here, we report two additional female patients with DEE9 who are siblings. After analyzing karyotype testing results, whole-exome sequencing (WES) was performed for the proband. Then, Sanger sequencing was carried out for proband, her affected sister, and parents. Results: Sequencing results revealed that our two patients had a heterozygous frameshift variant (NM_001184880.2: c.1091delC, p.P364Rfs*4) in the PCDH19 gene. We also reviewed previously reported cases with this mutation in detail. Conclusion: This is the first report of germline mosaicism in the PCDH19 gene in the Iranian population and expanded the phenotypic spectrum of DEE9. Genetic testing has become an effective way of determining the diagnosis. Parental germline mosaicism should be considered when providing genetic counseling for X-linked/autosomal dominant disorders. This report also emphasizes the importance of considering prenatal diagnosis (PND) in such cases. [ABSTRACT FROM AUTHOR]

Published
2024
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9. Novel mutations in the ciliopathy-associated gene CPLANE1 (C5orf42) cause OFD syndrome type VI rather than Joubert syndrome

Author

Bonnard, Carine, Shboul, Mohammad, Tonekaboni, Seyed Hassan, Ng, Alvin Yu Jin, Tohari, Sumanty, Ghosh, Kakaly, Lai, Angeline, Lim, Jiin Ying, Tan, Ene Choo, Devisme, Louise, Stichelbout, Morgane, Alkindi, Adila, Banu, Nazreen, Yüksel, Zafer, Ghoumid, Jamal, Elkhartoufi, Nadia, Boutaud, Lucile, Micalizzi, Alessia, Brett, Maggie Siewyan, Venkatesh, Byrappa, Valente, Enza Maria, Attié-Bitach, Tania, Reversade, Bruno, and Kariminejad, Ariana

Published
2018
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10. Genetics of intellectual disability in consanguineous families

Author

Hu, Hao, Kahrizi, Kimia, Musante, Luciana, Fattahi, Zohreh, Herwig, Ralf, Hosseini, Masoumeh, Oppitz, Cornelia, Abedini, Seyedeh Sedigheh, Suckow, Vanessa, Larti, Farzaneh, Beheshtian, Maryam, Lipkowitz, Bettina, Akhtarkhavari, Tara, Mehvari, Sepideh, Otto, Sabine, Mohseni, Marzieh, Arzhangi, Sanaz, Jamali, Payman, Mojahedi, Faezeh, Taghdiri, Maryam, Papari, Elaheh, Soltani Banavandi, Mohammad Javad, Akbari, Saeide, Tonekaboni, Seyed Hassan, Dehghani, Hossein, Ebrahimpour, Mohammad Reza, Bader, Ingrid, Davarnia, Behzad, Cohen, Monika, Khodaei, Hossein, Albrecht, Beate, Azimi, Sarah, Zirn, Birgit, Bastami, Milad, Wieczorek, Dagmar, Bahrami, Gholamreza, Keleman, Krystyna, Vahid, Leila Nouri, Tzschach, Andreas, Gärtner, Jutta, Gillessen-Kaesbach, Gabriele, Varaghchi, Jamileh Rezazadeh, Timmermann, Bernd, Pourfatemi, Fatemeh, Jankhah, Aria, Chen, Wei, Nikuei, Pooneh, Kalscheuer, Vera M., Oladnabi, Morteza, Wienker, Thomas F., Ropers, Hans-Hilger, and Najmabadi, Hossein

Published
2019
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14. Five patients with spinal muscular atrophy-progressive myoclonic epilepsy (SMA-PME): a novel pathogenic variant, treatment and review of the literature

Author

Karimzadeh, Parvaneh, primary, Najmabadi, Hossein, additional, Lochmuller, Hanns, additional, Babaee, Marzieh, additional, Dehdahsi, Shima, additional, Miryounesi, Mohammad, additional, Amirsalari, Susan, additional, Rayegani, Seyed Mansoor, additional, and Tonekaboni, Seyed Hassan, additional

Published
2022
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15. Epidemiology of Guillain-Barré Syndrome in Iranian Children Aged 0-15 Years (2008-2013)

Author

TONEKABONI, Seyed Hassan, MAHMOUDI, Sussan, ABDOLLAH GORJI, Fatemeh, NEJAD BIGLARI, Habibe, TAGHDIRI, Mohammad Mahdi, ETEMADI, Koroush, GHOFRANI, Mohammad, KARIMI, Abdollah, and REZAEI ZADEH, Mohammad

Subjects
Epidemiology, Incidence, Guillain-Barré Syndrome, Original Article, Iran, Children
Abstract

Objective Guillain-Barré Syndrome (GBS) is an acute inflammatory polyneuropathy characterized by a rapid progressive symmetric weakness. The GBS is the most common cause of acute flaccid paralysis (AFP) in most parts of the world. This study was carried out to investigate the epidemiological features of GBS in Iranian children. Materials & Methods The data were extracted using the AFP surveillance system that is a national screening program to detect all cases of AFP aged 0-15 years around the country. National Population Statistics data and AFP demographic data during 2008-2013 intervals were obtained from the relevant authorities in the Ministry of Health in Iran. The GBS cases were then extracted from the aforementioned database. The Chi-square test and Fisher’s exact test were used for statistical analysis. Results A total of 1884 cases of GBS were identified in the study period, and the average annual incidence rate was 1.72 per 100,000 individuals. The highest incidence rate was within the range of 0-5 years. There was no statistically significant relationship between the incidence of GBS and the season in the whole country. Conclusion High costs of GBS treatment, morbidity and occasional mortality, and number of new cases, which is estimated to be approximately 300 individuals per year, need the particular attention of the health system.

Published
2021

16. Heterogeneous Inheritance in Autism Genes Shared Across Neurodevelopmental and Neuromuscular Disorders in Consanguineous Singlets

Author

Ghasemi, Mohammad-Reza, primary, Sadeghi, Hossein, additional, Hashemi-Gorji, Farzad, additional, Mirfakhraie, Reza, additional, Gupta, Vijay, additional, Ben-Mahmoud, Afif, additional, Razjouyan, Katayoon, additional, Salehpour, Shadab, additional, Tonekaboni, Seyed Hassan, additional, Dianatpour, Mehdi, additional, Omrani, Davood, additional, Layman, Lawrence C., additional, Kim, Hyung-Goo, additional, and Miryounesi, Mohammad, additional

Published
2022
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20. Another Limping Child: An Interesting Diagnosis Journey

Author

HASSAS YEGANEH, Mehrnoush, RAHMANI, Khosro, HASHEMI, Shokuh, TONEKABONI, Seyed Hassan, SINAE, Reza, FATHI, Mohammad reza, and SHIARI, Reza

Subjects
limping child, Weakness, fungi, Hypercalciuria, food and beverages, Case Report
Abstract

Limp is described as any deviation from a normal gait pattern for the child’s age. Limping takes many forms and is one of the most enigmatic complaints in pediatric medicine. It is never normal, and both benign and life-threatening illnesses can present with limp. The provisional diagnosis can be a challenge to establish even after history, physical, and laboratory examinations.

Published
2017

21. Clinical and Epidemiological Aspects of Multiple Sclerosis in Children

Author

Nasehi, Mohammad Mehdi, Sahraian, Mohammad Ali, Moghaddas, Abdorreza Naser, Ghofrani, Mohammad, Ashtari, Fereshteh, Taghdiri, Mohammad Mahdi, Tonekaboni, Seyed Hassan, Karimzadeh, Parvaneh, Afshari, Mahdi, and mahmood moosazadeh

Subjects
Multiple sclerosis, Clinical, Epidemiology, Original Article, Iran, Children
Abstract

Objective Overall, 2%-5% of patients with multiple sclerosis (MS) experienced the first episode of disease before the age 18 years old. Since the age of onset among children is not similar to that in general population, clinicians often fail to early diagnose the disease. This study aimed to determine the epidemiological and clinical patterns of MS among Iranian children. Materials & Methods In this cross-sectional study carried out in Iran in 2014-2015, information was collected using a checklist with approved reliability and validity. Method sampling was consensus. Data were analyzed using frequency, mean and standard deviation indices by means of SPSS ver. 20 software. Results Totally, 177 MS children were investigated. 75.7% of them were female. Mean (SD), minimum and maximum age of subjects were 15.9 (2), 7 and 18 yr, respectively. The most reported symptoms were sensory (28.2%), motor (29.4%), diplopia (20.3%) and visual (32.8%). Primary MRI results showed 91.5% and 53.1% periventricular and spinal cord lesions, respectively. Conclusion MS is significantly more common among women. The most common age of onset is during the second decades. Visual and motor problems are the most symptoms, while, periventricular and spinal cord lesions are the most MRI results.

Published
2017

22. Glutaric AciduriaType 1: Clinical and Molecular Study in Iranian Patients, 3 Novel Mutations

Author

PIRZADEH, Zahra, HOUSHMAND, Massoud, NASIRI, Jafar, MOLLAMOHAMMADI, Mohsen, SEDIGHI, Mostafa, and TONEKABONI, Seyed Hassan

Subjects
GCDH mutation, Glutaricaciduria type1, Original Article, Iran, Glutaryl co-A dehydrogenase
Abstract

Objective Glutaricaciduria type 1 (GA1), is a rare, treatable neuro metabolic disease, due to glutaryl- CoA dehydrogenase (GCDH) gene mutation.In regions without neonatal blood screening (NBS), patients are diagnosed in symptomatic period. This study was carried out to assess patients with GA1 for clinical, biochemical, neuroimaging findings and GCDH gene mutations analysis. Materials & Methods In this cross-sectional study, clinical manifestation, neuroimaging and metabolic findings of eleven Iranian GA1 patients of MofidChildren’s Hospital, Tehran, Iranbetween 2001 and 2011,were evaluated.Mutational analysis of the GCDH gene was performed on genomic DNA. Genomic DNA was extracted from peripheral lymphocytes using QIAamp DNA Micro Kit (Qiagen). All 11 exons and flanking intronic regions of the GCDH gene were amplified by polymerase chain reaction (PCR). Results All patients were diagnosed before 32 months old. Clinical presentations of GA1 include acute encephalopathic crisis and/or developmental delay and macrocephaly. Seven GCDH gene mutations were detected in our patients. The most frequent GCDH mutations occurred in exon7 then exon8, 10 and11. G244 C in exon7, R294 Q in exon8 and N373 S in exon 10 were three novel mutations. There was no correlation between of genotype and phenotype in our patients. Conclusion Physician must remember GA1 in differential diagnosis of acute encephalopathic crisis, macrocephaly, developmental delay, movement disorders such as dystonia and dyskinesia. Early detection, proper treatment and selective screening of patients’ siblings can prevent neurologic disabilities.

Published
2017

23. Demographic, neuroradiological and neuropathological characteristics among children with central nervous system tumors in the iranian referral center for stereotaxis.

Author

Saket, Sasan, Heidari, Atefeh, Zali, Alireza, Nasehi, Mohammad Mehdi, Taghdiri, Mohammad Mehdi, Tonekaboni, Seyed Hassan, Shahzadi, Sohrab, Nilipour, Yalda, and Javadian, Hamed

Subjects
CENTRAL nervous system tumors, STEREOTAXIC techniques, TUMORS in children, CENTRAL nervous system, DEMOGRAPHIC characteristics, TUMOR markers
Abstract

Copyright of Revista Latinoamericana de Hipertension is the property of Revista Latinoamericana de Hipertension and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2021
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24. Comparative Efficacy of Zonisamide and Pregabalin as an Adjunctive Therapy in Children with Refractory Epilepsy

Author

TAGHDIRI, Mohammad Mahdi, BAKHSHANDEH BALI, Mohammad Kazem, KARIMZADEH, Parvaneh, ASHRAFI, Mohammad Reza, TONEKABONI, Seyed Hassan, and GHOFRANI, Mohammad

Subjects
Epileptic children, Zonisamide, Intractable Epilepsy, Antiepileptic drugs, Pregabalin, Original Article
Abstract

Objective Approximately one third of epileptic children are resistant to anticonvulsant drugs. This study evaluates the effectiveness, safety, and tolerability of pregabalin as adjunctive therapy in epileptic children relative to Zonisamide. Materials & Methods From April 2012 to November 2012,121 children were referred to Mofid Children’s Hospital with intractable epilepsy and enrolled in the study. The patients were divided into two groups (A and B) randomly. Group A was treated with Zonisamide and group B was treated with Pregabalin in addition to prior medication. We assessed seizure frequency and severity during a 4-week interval from the beginning of the drug treatment and compared the efficacy of each in these two groups. Results Group A consists of 61 patients, 26 (42.6%) girls, and35 (57.4%) boys with an age range from 1.5 months–14 years (mean, 73.9± 44.04 months). Group B consists of 60 patients, 31(51.7%) girls, 29 (48.3%) boys with an age range from 6 months–16 years (mean, 71±42.9 months). Age, gender, seizure onset, seizure frequency, seizure type, and previous antiepileptic medications showed that there was no significant difference between the groups (P>0.05). Zonisamide and pregabalin reduced more than 50% of seizure intensity in 40.2%; 45.8% of patients also had a seizure frequency decline between35.8–44.4%, respectively and there was no significant superiority between these two novel anticonvulsants (P>0.05). Conclusion In this survey both pregabalin and Zonisamide were impressive for seizure control in children with intractable epilepsy and well sustained with mild complications that were completely reversible.

Published
2015

25. Use of Complementary and Alternative Medicine for Epileptic Children in Tehran: A Cross-Sectional Study (2009-2011)

Author

TONEKABONI, Seyed Hassan, JAFARI NAEINI, Sepideh, KHAJEH, Ali, YAGHINI, Omid, GHAZAVI, Ahad, and ABDOLLAH GORJI, Fatemeh

Subjects
Complementary and Alternative Medicine (CAM), Epilepsy, Original Article, Children
Abstract

Objective Although the use of Complementary and Alternative Medicine (CAM) has been evaluated globally, there are few studies in our country on this subject. The purpose of this study was to determine the prevalence, pattern of use, parental sources of information, and benefits of CAM in epileptic children in Tehran. Materials & Methods One hundred thirty-three parents or relatives of epileptic children who were referred to outpatient clinics or admitted in neurologic ward of four major hospitals in Tehran, were interviewed by our researcher based on a structured questionnaire; from 2009 to 2010. The information obtained comprised the demographic data of patients and their parents, frequency and morphology of convulsions, the type and sources of CAM and finally, the benefits and adverse effects of this practice. Results Forty-four percent of the respondents had used CAM methods either alone or in combination with other methods. The most frequently used CAM was written prayers followed by oral herbs and special diets. CAM was mainly introduced to them by relatives. Only 16.7% of these parents had discussed this matter with their children’s physicians. No efficacy to control seizure was observed for most of these methods. Conclusion This study showed that use of CAM in our study group is relatively common and may have a potentially hazardous role in the treatment process. So, it is necessary for physicians to have enough information about CAM practice in their patients.

Published
2014

26. Ryanodine receptor type 3 (RYR3) as a novel gene associated with a myopathy with nemaline bodies

Author

Nilipour, Yalda, Nafissi, Shahriar, Tjust, Anton E., Ravenscroft, Gianina, Hossein-Nejad Nedai, Hamid, Taylor, Rhonda L., Varasteh, Vahid, Pedrosa Domellöf, Fatima, Zangi, Mahdi, Tonekaboni, Seyed Hassan, Olivé, M., Kiiski, Kirsi, Sagath, L., Davis, Mark R., Laing, Nigel G., Tajsharghi, Homa, Nilipour, Yalda, Nafissi, Shahriar, Tjust, Anton E., Ravenscroft, Gianina, Hossein-Nejad Nedai, Hamid, Taylor, Rhonda L., Varasteh, Vahid, Pedrosa Domellöf, Fatima, Zangi, Mahdi, Tonekaboni, Seyed Hassan, Olivé, M., Kiiski, Kirsi, Sagath, L., Davis, Mark R., Laing, Nigel G., and Tajsharghi, Homa

Abstract

Background: Nemaline myopathy has been associated with mutations in twelve genes to date. However, for some patients diagnosed with nemaline myopathy, definitive mutations are not identified in the known genes, suggesting there are other genes involved. This study describes compound heterozygosity for rare variants in RYR3 in one such patient. Results: Clinical examination of the patient at 22 years of age revealed a long-narrow face, high arched palate and bilateral facial weakness. She had proximal weakness in all four limbs, mild scapular winging but no scoliosis. Muscle biopsy revealed wide variation in fibre size with type 1 fibre predominance and atrophy. Abundant nemaline bodies were located in perinuclear areas, subsarcolemmal and within the cytoplasm. No likely pathogenic mutations in known nemaline myopathy genes were identified. Copy number variation in known nemaline myopathy genes was excluded by nemaline myopathy targeted array-CGH. Next generation sequencing revealed compound heterozygous missense variants in the ryanodine receptor type 3 gene (RYR3). RYR3 transcripts are expressed in human fetal and adult skeletal muscle as well as in human brain or cauda equina samples. Immunofluorescence of human skeletal muscle revealed a "single-row" appearance of RYR3, interspaced between the "double-rows" of RYR1 at each A-I junction. Conclusion: The results suggest that variants in RYR3 may cause a recessive muscle disease with pathological features including nemaline bodies. We characterize the expression pattern of RYR3 in human skeletal muscle and brain and the subcellular localization of RYR1 and RYR3 in human skeletal muscle., © 2018 EAN

Published
2018
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27. Sodium Channel Gene Mutations in Children with GEFS+ and Dravet Syndrome: A Cross Sectional Study

Author

TONEKABONI, Seyed Hassan, EBRAHIMI, Ahmad, BAKHSHANDEH BALI, Mohammad Kazem, TAHERI OTAGHSARA, Seyedeh Mohadeseh, HOUSHMAND, Massoud, NASEHI, Mohammad Mahdi, TAGHDIRI, Mohammad Mahdi, and MOGHADDASI, Mehdi

Subjects
GEFS+, Original Article, SCN1A mutations, Dravet syndrome
Abstract

Objective Dravet syndrome or severe myoclonic epilepsy of infancy (SMEI) is a baleful epileptic encephalopathy that begins in the first year of life. This syndrome specified by febrile seizures followed by intractable epilepsy, disturbed psychomotor development, and ataxia. Clinical similarities between Dravet syndrome and generalized epilepsy with febrile seizure plus (GEFS+) includes occurrence of febrile seizures and joint molecular genetic etiology. Shared features of these two diseases support the idea that these two disorders represent a severity spectrum of the same illness. Nowadays, more than 60 heterozygous pattern SCN1A mutations, which many are de novo mutations, have been detected in Dravet syndrome. Materials & Methods From May 2008 to August 2012, 35 patients who referred to Pediatric Neurology Clinic of Mofid Children Hospital in Tehran were enrolled in this study. Entrance criterion of this study was having equal or more than four criteria for Dravet syndrome. We compared clinical features and genetic findings of the patients diagnosed as Dravet syndrome or GEFS+. Results 35 patients (15 girls and 20 boys) underwent genetic testing. Mean age of them was 7.7 years (a range of 13 months to 15 years). Three criteria that were best evident in SCN1A mutation positive patients are as follows: “Normal development before the onset of seizures, onset of seizure before age of one year, and psychomotor retardation after onset of seizures. Our genetic testing showed that 1 of 3 (33.3%) patients with clinical Dravet syndrome and 3 of 20 (15%) patients that diagnosed as GEFS+, had SCN1A mutation. Conclusion In this study, normal development before seizure onset, seizures beginning before age of one year and psychomotor retardation after age of two years are the most significant criteria in SCN1A mutation positive patients.

Published
2013

28. Prophylaxis of Childhood Migraine: Topiramate Versus Propranolol

Author

TONEKABONI, Seyed Hassan, GHAZAVI, Ahad, FAYYAZI, Afshin, KHAJEH, Ali, TAGHDIRI, Mohammad Mahdi, ABDOLLAH GORJI, Fatemeh, and AZARGHASHB, Eznollah

Subjects
Topiramate, Original Article, Children, Propranolol, Migraine
Abstract

Objective Headache is a common disabling neurological disorder and migraine comprises more than half the causes of recurrent headaches in children. Despite extended prevalence of this type of headache there is lack of evidence about best drug treatment for migraine. So we aimed to compare the therapeutic effects of these drugs on childhood migraine. Materials & Methods In the current study, a randomized clinical trial consisting of 78 patients according to 2004 International Headache Association criteria were randomly assigned to two groups that matched by age and sex. One of these two groups was treated with Topiramate, while the other was given Propranolol. After one and four months, the efficiency of these treatments was measured in terms of frequency, severity and duration of migraine attacks. Results Results obtained from the data collected showed that of these 78 studied patients, 38 patients received Topiramate treatment (group A) and the rest (40 patients; group B) was treated with Propranolol. The average age of group A was 8.5± 2.9 years and that of group B was 8.3 ± 2.8 years. No significant difference was observed between these two groups in terms of reduction in frequency, severity and duration of migraine attacks. Conclusion Results showed that both treatments had the same efficiency in healing migraine headaches and there was no significant difference between their treating results. However, further studies are needed to examine medical effects of these two medicines.

Published
2013

30. Genetics of intellectual disability in consanguineous families

Author

Hu, Hao, primary, Kahrizi, Kimia, additional, Musante, Luciana, additional, Fattahi, Zohreh, additional, Herwig, Ralf, additional, Hosseini, Masoumeh, additional, Oppitz, Cornelia, additional, Abedini, Seyedeh Sedigheh, additional, Suckow, Vanessa, additional, Larti, Farzaneh, additional, Beheshtian, Maryam, additional, Lipkowitz, Bettina, additional, Akhtarkhavari, Tara, additional, Mehvari, Sepideh, additional, Otto, Sabine, additional, Mohseni, Marzieh, additional, Arzhangi, Sanaz, additional, Jamali, Payman, additional, Mojahedi, Faezeh, additional, Taghdiri, Maryam, additional, Papari, Elaheh, additional, Soltani Banavandi, Mohammad Javad, additional, Akbari, Saeide, additional, Tonekaboni, Seyed Hassan, additional, Dehghani, Hossein, additional, Ebrahimpour, Mohammad Reza, additional, Bader, Ingrid, additional, Davarnia, Behzad, additional, Cohen, Monika, additional, Khodaei, Hossein, additional, Albrecht, Beate, additional, Azimi, Sarah, additional, Zirn, Birgit, additional, Bastami, Milad, additional, Wieczorek, Dagmar, additional, Bahrami, Gholamreza, additional, Keleman, Krystyna, additional, Vahid, Leila Nouri, additional, Tzschach, Andreas, additional, Gärtner, Jutta, additional, Gillessen-Kaesbach, Gabriele, additional, Varaghchi, Jamileh Rezazadeh, additional, Timmermann, Bernd, additional, Pourfatemi, Fatemeh, additional, Jankhah, Aria, additional, Chen, Wei, additional, Nikuei, Pooneh, additional, Kalscheuer, Vera M., additional, Oladnabi, Morteza, additional, Wienker, Thomas F., additional, Ropers, Hans-Hilger, additional, and Najmabadi, Hossein, additional

Published
2018
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31. A Novel Homozygous ATP8A2 Variant in a Patient With Phenotypic Features of Dysequilibrium Syndrome.

Author

Saghazadeh, Amene, Tonekaboni, Seyed Hassan, Najmabadi, Hossein, and Rezaei, Nima

Subjects
*SPEECH, *PROTEINS, *DEVELOPMENTAL delay, *CHROMOSOMAL translocation, *SYNDROMES
Abstract

The ATP8A2 protein is mainly located in the brain and takes part in the lipid flipping process. Mutations in the ATP8A2 gene and chromosomal translocations that interfere with the ATP8A2 gene product have been reported in association with global developmental delay and hypotonia. Here, we will report a threeyear- old male presented with major phenotypic features of dysequilibrium syndrome (DES), including severe hypotonia, global developmental delay, speech problem, and strabismus. Whole exome sequencing revealed a homozygous in-frame deletion in the ATP8A2 gene (c.1286_1288delAGA, p.Lys429del). This ATP8A2 variant has not been reported yet and seems to be linked to the phenotypic features of dysequilibrium syndrome. [ABSTRACT FROM AUTHOR]

Published
2018

32. Prediction of Response to Treatment in Children with Epilepsy.

Author

GHOFRANI, Mohammad, NASEHI, Mohammad Mehdi, SAKET, Sasan, MOLLAMOHAMMADI, Mohsen, TAGHDIRI, Mohammad Mahdi, KARIMZADEH, Parvaneh, TONEKABONI, Seyed Hassan, JAVADZADEH, Mohsen, JAFARI, Narjes, ZAVEHZAD, Azadeh, HASANVAND AMOUZADEH, Masoud, BESHRAT, Mahsa, and BABAEI, Meysam

Subjects
ANTICONVULSANTS, DRUG therapy for convulsions, BRAIN diseases, ASPHYXIA, DIAGNOSIS of brain abnormalities, HOSPITAL care of children, CHILDREN'S hospitals, COMPUTED tomography, SEIZURES (Medicine), ELECTROENCEPHALOGRAPHY, EPILEPSY, FEBRILE seizures, FEVER, MAGNETIC resonance imaging, QUESTIONNAIRES, SPASMS, PATIENTS' attitudes, CHILDREN, HISTORY
Abstract

Objective: This study was conducted to predict the response to treatment in patients treated with anti-epilepsy drugs. Material and Methods: This analytical questionnaire-based study was conducted in 2014 among 128 patients with epilepsy admitted to Mofid Children's Hospital, Tehran, Iran. The inclusion criteria were children 2 months to 12 yr of age with epilepsy and patients who experienced fever and seizure attacks at least once were excluded from the study. Patients were followed up for 6 months and the response to their treatment was recorded. The good response to treatment was defined as the absence of seizure with two drugs during follow up. Results: Seventy-two patients (56.3%) were boys. The age of the first seizure was under 2 yr old in 90 patients (70.3%). History of febrile convulsion, family history of epilepsy and history of asphyxia was found in 16 (12.5%), 41 (32%), and 27 (21.1%) patients, respectively. Seizure etiology was idiopathic in 90 patients (70.3%), and the number of seizures was 1-2 in 36 patients (28.1%). Overall, 57 patients (44.5%) had cerebral lesion according to CT scan or MRI, and EEG was abnormal in 101 patients (78.9%). In 6-month follow-up, 40 patients (31.3%) responded well to the treatment and 88 patients (68.8%) responded poorly to the treatment. History of asphyxia (OR = 6.82), neonatal jaundice (OR = 2.81) and abnormal EEG (OR = 0.19) were effective factors in response to treatment. Conclusion: Abnormal EEG is an effective factor in treatment response in the children studied. [ABSTRACT FROM AUTHOR]

Published
2018

34. Exploring the Psychometric Properties of the Farsi Version of Quality of Life Kindl Questionnaire for 4-7 Year-Old Children in Iran.

Author

ROJHANI SHIRAZI, Maryam, TONEKABONI, Seyed Hassan, AZARGASHB, Eznollah, DERAKHSHANNIA, Mehdi, and AGHDASTA, Elham

Abstract

OBJECTIVE: The aim of this study was to translate and validate the psychometric properties of the Quality of Life Kindl questionnaire. MATERIALS & METHODS: Parents of 4-7 yr-old healthy and ill children referred to Mofid Children Hospital in Tehran in 2013, Iran were sampled randomly in two groups each of which 130 people. After translation, the questionnaie's validity and reliability was evaluated and was confirmed for face and content validity. Questionnaire was also completed by two (one healthy and one ill) groups for which inclusion criteria included consent of the parents, age of the children being beween 4 and 7 yr, and presence of the child in a nursery school, kindergarten, school or any class at least for one month. Exclusion criteria were inability of the parents in answering the questions accurately. Inclusion criterion for the ill group was having chronic cardiac, neurologic, hematologic, or respiratory diseases, lasting longer than 3 months for which they were followed up in outpatient clinic in the hospital. The reliability of questionnaire was measured by the Cronbach's alpha. Data were analyzed using factor analysis, Spearman's correlation coefficient, Mann-Whitney and Chi-square test. RESULTS: The reliability was 0.85 and 0.81 in healthy and ill groups, respectively. The results of factor analysis showed that each of eight subscales of questionnaire had acceptable construct validity. Only two of 52 questions of the questionnaire did not have proper correlation coefficient. CONCLUSION: Quality of Life Kindl Questionnaire is a valid and reliable test for assessing healthy and ill children in Iran. [ABSTRACT FROM AUTHOR]

Published
2016

35. Chromosome Structural Alteration an Unusual Abnormality Characterizing Human Neoplasia.

Author

Movafagh, Abolfazl, Zare-Abdollahi, Davood, Emamalizadeh, Babak, Shahvaisizadeh, Farhad, Mansouri, Neda, Hashemi, Mehrdad, Pour, Atefeh Heidary, Heidari, Mohammad Hassan, and Tonekaboni, Seyed Hassan

Subjects
CERVICAL intraepithelial neoplasia, HUMAN chromosome abnormalities
Abstract

Background and Aim: Ring chromosomes are rare cytogenetic abnormalities that occur in less than 10% of hematopoietic malignancies. They are rare in blood disorder. The present review has focused on the ring chromosome associated with oncology malignancies. Materials and Methods: By reviewing the web-based search for all English scientific peer review articles published, was initiated using Medline/PubMed, Mitelman database (http://cgap.nci.nih.gov/Chromosomes/Mitelman), and other pertinent references on websites about ring chromosomes in Oncology. The software program as End Note was used to handle the proper references for instruction to author. Karyotype descriptions were cited according to ISCN. Conclusion: Ring chromosomes are rare chromosomal aberrations, almost many times are of de novo origin, presenting a different phenotype regarding the loss of genetic material. The karyotype represents the main analysis for detection of ring chromosomes, but other molecular technics are necessary for complete characterization. The information of this review article adds to the spectrum of both morphology and genetic rearrangements in the field of oncology malignancies. [ABSTRACT FROM AUTHOR]

Published
2016

36. Effects of Miglustat on Stabilization of Neurological Disorder in Niemann–Pick Disease Type C

Author

Karimzadeh, Parvaneh, primary, Tonekaboni, Seyed Hassan, additional, Ashrafi, Mahmoud Reza, additional, Shafeghati, Yousef, additional, Rezayi, Alireza, additional, Salehpour, Shadab, additional, Ghofrani, Mohammad, additional, Taghdiri, Mohammad Mehdi, additional, Rahmanifar, Ali, additional, Zaman, Talieh, additional, Aryani, Omid, additional, Shoar, Babak Najaf, additional, Shiva, Farideh, additional, Tavasoli, Alireza, additional, and Houshmand, Massoud, additional

Published
2012
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37. Diagnosis and treatment of late-onset Pompe disease in the Middle East and North Africa region: consensus recommendations from an expert group.

Author

Al Jasmi, Fatma, Al Jumah, Mohammed, Alqarni, Fatimah, Al-Sanna'a, Nouriya, Al-Sharif, Fawziah, Bohlega, Saeed, Cupler, Edward J., Fathalla, Waseem, Hamdan, Mohamed A., Makhseed, Nawal, Nafissi, Shahriar, Nilipour, Yalda, Selim, Laila, Shembesh, Nuri, Sunbul, Rawda, Hassan Tonekaboni, Seyed, MENA Pompe Working Group, and Tonekaboni, Seyed Hassan

Subjects
CONSENSUS (Social sciences), MEDICAL protocols, DIAGNOSIS, INBORN errors of carbohydrate metabolism, THERAPEUTICS
Abstract

Background: Pompe disease is a rare autosomal recessive disorder caused by a deficiency of the lysosomal enzyme alpha-glucosidase responsible for degrading glycogen. Late-onset Pompe disease has a complex multisystem phenotype characterized by a range of symptoms.Methods: An expert panel from the Middle East and North Africa (MENA) region met to create consensus-based guidelines for the diagnosis and treatment of late-onset Pompe disease for the MENA region, where the relative prevalence of Pompe disease is thought to be high but there is a lack of awareness and diagnostic facilities.Results: These guidelines set out practical recommendations and include algorithms for the diagnosis and treatment of late-onset Pompe disease. They detail the ideal diagnostic workup, indicate the patients in whom enzyme replacement therapy should be initiated, and provide guidance on appropriate patient monitoring.Conclusions: These guidelines will serve to increase awareness of the condition, optimize patient diagnosis and treatment, reduce disease burden, and improve patient outcomes. [ABSTRACT FROM AUTHOR]

Published
2015
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38. Neurodegeneration with Brain Iron Accumulation: An Overview.

Author

TONEKABONI, Seyed Hassan and MOLLAMOHAMMADI, Mohsen

Subjects
BRAIN anatomy, DIAGNOSIS of brain diseases, SPASTICITY, ENZYMES, DIAGNOSTIC imaging, IRON, NEURODEGENERATION, NEUROLOGY, SERIAL publications, PANTOTHENIC acid, DIAGNOSIS, PHYSIOLOGY, THERAPEUTICS
Abstract

Objective Neurodegeneration with brain iron accumulation (NBIA) is a group of neurodegenerative disorder with deposition of iron in the brain (mainly Basal Ganglia) leading to a progressive Parkinsonism, spasticity, dystonia, retinal degeneration, optic atrophy often accompanied by psychiatric manifestations and cognitive decline. 8 of the 10 genetically defined NBIA types are inherited as autosomal recessive and the remaining two by autosomal dominant and X-linked dominant manner. Brain MRI findings are almost specific and show abnormal brain iron deposition in basal ganglia some other related anatomical locations. In some types of NBIA cerebellar atrophy is the major finding in MRI. [ABSTRACT FROM AUTHOR]

Published
2014

39. Pregabalin in childhood epilepsy: a clinical trial study.

Author

TONEKABONI, Seyed Hassan, MOLLAMOHAMMADI, Mohsen, VAHEDIAN, Mostafa, and PIRZADEH, Zahra

Subjects
SEIZURES diagnosis, DIAGNOSIS of epilepsy, TREATMENT of epilepsy, SPASMS, STATUS epilepticus diagnosis, ANTICONVULSANTS, CLINICAL trials, DRUG prescribing, EVALUATION of medical care, MEDICAL referrals, NEUROLOGY, SERIAL publications, PHYSICIAN practice patterns, DIAGNOSIS, PREGABALIN, THERAPEUTICS
Abstract

Objective The prevalence of active epilepsy is about 0.5-1%, and approximately 70% of patients are cured with first anti-epileptic drugs and the remaining patients need multiple drugs. Pregabalin as an add-on therapy has a postive effect on refractory seizures in adults. To the best of our knowledge, there is no research with this drug in childhood epilepsy. We use pregabalin in children with refractory seizures as an add-on therapy. The objective of this study is to evaluate the effects of pregabalin in the reduction of seizures for refractory epilepsy. Material & Methods Forty patients with refractory seizures who were referred to Mofid Children's Hospital and Hazrat Masoumeh Hospital were selected. A questionnaire based on patient record forms, demographic data (age, gender,…), type of seizure, clinical signs, EEG record, imaging report, drugs that had been used, drugs currently being used, and the number of seizures before and after Pregabalin treatment was completed. We checked the number of seizures after one and four months. Results After one month, 26.8% of patients had more than a 50% reduction in seizures and 14.6% of these patients were seizure-free; 12.2% had a 25-50% reduction; and approximately 61% had less than a 25% reduction or no change in seizures. After the fourth month, 34.1% of patients had more than a 50% reduction in seizures and 24.4% of these patients were seizure-free. Additionally, 65.9% of patients had less than 50% reduction in seizures (9.8% between 25-50% and 56.1% less than 25% or without improvement). Conclusion We recommend Pregabalin as an add-on therapy for refractory seizures (except for myoclonic seizures) for children. [ABSTRACT FROM AUTHOR]

Published
2014

40. The Ketogenic and Atkins Diets Effect on Intractable Epilepsy: A Comparison.

Author

GHAZAVI, Ahad, TONEKABONI, Seyed Hassan, KARIMZADEH, Parvaneh, NIKIBAKHSH, Ahmad Ali, KHAJEH, Ali, and FAYYAZI, Afshin

Subjects
DIAGNOSIS of epilepsy, ANALYSIS of variance, CLINICAL trials, ELECTROENCEPHALOGRAPHY, FISHER exact test, HOSPITALS, KETOGENIC diet, NEUROLOGY, DATA analysis, DATA analysis software, DESCRIPTIVE statistics
Abstract

Objective Intractable epilepsy is a major difficulty in child neurology, because the numbers of drugs that are available for treatment are limited and new treatments such as diets must be tried. Now there are some diets available for treating patients with intractable epilepsy. The oldest diet is the classic ketogenic diet and one of the newest diets is the modified Atkins diet. Patients have a harder time accepting the classic ketogenic diet than the Atkins diet, which is easier to accept because the food tastes better. This study compares the efficacy of the ketogenic diet and the Atkins diet for intractable epilepsy in children. Materials & Methods This study is a clinical trial survey with sample size of 40 children with refractory epilepsy who were patients at Mofid hospital in Tehran, Iran. Initially, from Jan 2005-Oct 2007, 20 children were treated with the Atkins diet, and then from Oct 2007-March 2010, the other group was treated with the classic ketogenic diet and the results were compared. Results In this study, response to treatment was greater than a 50% reduction in seizures and at the end of first, second, and third months for the ketogenic diet were 55%, 30%, and 70% and for the Atkins diet were 50%, 65%, and 70%, respectively. Conclusion The results of this study show that there is no significant difference between the classic Ketogenic diet and the Atkins diet at the end of first, second, and third months and both had similar responses to the treatments. [ABSTRACT FROM AUTHOR]

Published
2014

41. Propionic Acidemia: Diagnosis and Neuroimaging Findings of This Neurometabolic Disorder.

Author

KARIMZADEH, Parvaneh, JAFARI, Narjes, AHMAD ABADI, Farzad, JABBEDARI, Sayena, TAGHDIRI, Mohammad-Mahdi, ALAEE, Mohammad-Reza, GHOFRANI, Mohammad, TONEKABONI, Seyed Hassan, and NEJAD BIGLARI, Habibeh

Subjects
GENETIC disorder diagnosis, DIAGNOSIS of neurological disorders, ACIDOSIS, DIAGNOSIS of developmental disabilities, HOSPITAL care, METABOLISM, NEURORADIOLOGY, NEUROLOGY, PEDIATRICS, PROPIONIC acid, SERIAL publications, EARLY diagnosis, DIAGNOSIS
Abstract

Objective Propionic acidemia is one of the rare congenital neurometabolic disorders with autosomal recessive inheritance. This disorder is caused by a defect in the propionyl-CoA carboxylase enzyme and can be presented with life-threatening ketoacidosis, lethargy, failure to thrive, and developmental delay. Materials & Methods The patients diagnosed as having propionic acidemia in Neurology Department of Mofid Children's Hospital in Tehran, Iran, between 2002 and 2012 were include in our study. This disorder was confirmed by clinical manifestations, neuroimaging findings, and neurometabolic assessment in the reference laboratory in Germany. Our study was conducted to define the sex, age, gender, past medical history, developmental status, clinical findings, and neuroimaging manifestations in 10 patients with propionic acidemia. Results Seventy percent of patients were offspring of consanguineous marriages. In this study, only one patient had microcephaly at birth, but at detection time, 30% of patients had head circumference and weight below the 3rd percentile. The patients were followed for approximately 5 years and this follow-up showed that the patients with early diagnosis had a more favorable clinical response. Neuroimaging findings included brain atrophy, white matter and globus pallidus involvement. Conclusion Finally we suggest that early diagnosis and treatment have an important role in the prevention of disease progression [ABSTRACT FROM AUTHOR]

Published
2014

42. Effects of Miglustat on Stabilization of Neurological Disorder in Niemann–Pick Disease Type C: Iranian Pediatric Case Series.

Author

Karimzadeh, Parvaneh, Tonekaboni, Seyed Hassan, Ashrafi, Mahmoud Reza, Shafeghati, Yousef, Rezayi, Alireza, Salehpour, Shadab, Ghofrani, Mohammad, Taghdiri, Mohammad Mehdi, Rahmanifar, Ali, Zaman, Talieh, Aryani, Omid, Shoar, Babak Najaf, Shiva, Farideh, Tavasoli, Alireza, and Houshmand, Massoud

Subjects
*NIEMANN-Pick diseases, *PSEUDOBULBAR paralysis, *PSYCHOMOTOR disorders, *NEURODEGENERATION, *PEDIATRIC emergencies
Abstract

Niemann–Pick disease type C is a rare neurodegenerative disorder with autosomal recessive inheritance that can be broadly categorized into different forms dependent on age at disease onset: pre-/perinatal, early infantile, late infantile, juvenile, and adolescent/adult. This study was conducted to define the age at onset, clinical manifestations, neuroimaging findings and response to treatment in 21 patients diagnosed with Niemann–Pick disease type C and managed in the neurology departments of hospitals in Tehran, Iran. The effects of miglustat on patient ambulation, fine and gross motor function, swallowing, hearing, speech, seizures, psychomotor development, and ocular movements were evaluated for up to 26 months of treatment. Ambulation, fine and gross motor movements, swallowing, speech, and supranuclear gaze palsy were generally stabilized during therapy, and psychomotor delay appeared to be improved in early- and late-infantile onset patients. However, miglustat had no effect on organomegaly or other systemic manifestations of the disease. Miglustat was well tolerated. [ABSTRACT FROM PUBLISHER]

Published
2013
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43. A Comparison of Buccal Midazolam and Intravenous Diazepam for the Acute Treatment of Seizures in Children.

Author

Tonekaboni, Seyed-Hassan, Shamsabadi, Farhad Mahvelati, Anvari, Seyed-Saeed, Mazrooei, Ali, and Ghofrani, Mohammad

Subjects
*DRUG therapy for convulsions, *CHI-squared test, *COMPARATIVE studies, *DIAZEPAM, *FISHER exact test, *MIDAZOLAM, *SPASMS, *T-test (Statistics), *RANDOMIZED controlled trials, *ACUTE diseases, *DATA analysis software
Abstract

Objective: The purpose of the present study is to compare efficacy and safety of buccal midazolam with intravenous diazepam in control of seizures in Iranian children. Methods: This is a randomized clinical trial. 92 patients with acute seizures, ranging from 6 months to 14 years were randomly assigned to receive either buccal midazolam (32 cases) or intravenous diazepam (60 cases) at the emergency department of a children's hospital. The primary outcome of this study was cessation of visible seizure activity within 5 minutes from administration of the first dosage. The second dosage was used in case the seizure remained uncontrolled 5 minutes after the first one. Findings: In the midazolam group, 22 (68.8%) patients were relieved from seizures in 10 minutes. Meanwhile, diazepam controlled the episodes of 42 (70%) patients within 10 minutes. The difference was, however, not statistically significant (P=0.9). The mean time required to control the convulsive episodes after administration of medications was not statistically significant (P=0.09). No significant side effects were observed in either group. Nevertheless, the risk of respiratory failure in intravenous diazepam is greater than in buccal midazolam. Conclusion: Buccal midazolam is as effective as and safer than intravenous diazepam in control of seizures. [ABSTRACT FROM AUTHOR]

Published
2012

44. Efficacy of the Atkins diet as therapy for intractable epilepsy in children.

Author

Tonekaboni, Seyed Hassan, Mostaghimi, Parvin, Mirmiran, Parvin, Abbaskhanian, Ali, Gorji, Fatemeh Abdollah, Ghofrani, Mohammad, and Azizix, Fereidoun

Abstract

BACKGROUND AND AIMS: The ketogenic diet is an effective medical therapy for intractable childhood epilepsy. However, it has drawbacks in that it restricts calories, fluids and protein. The Atkins diet may also induce ketosis without those restrictions. Our objective was to evaluate the efficacy of a modified Atkins diet in children with intractable childhood epilepsy. METHODS: This clinical trial was conducted in 51 epileptic children aged 1 - 16 years with refractory seizures from Feb. 2004 to Oct. 2006. Outcome measures included seizure frequency and adverse reactions. Twenty-seven patients left the study for various reasons, leaving 24 who continued the Atkins diet for a minimum of three months. Carbohydrates were initially limited to 10 g/day and fats constituted 60% of the total energy requirement. All participants received vitamin and calcium supplementation. RESULTS: Following three months of treatment with the Atkins diet, 16 patients (67%) had >50% decrease in seizure frequency, and 6 (25%) had >90% improvement, of whom 5 were seizure-free. Mean seizure frequency after the first, second and third months of treatment were significantly lower than at baseline (P values <0.001, 0.001 and 0.002, respectively). CONCLUSION: The Atkins diet can be considered as a safe and effective alternative therapy for intractable childhood epilepsy. Atkins diet was well tolerated in our patients with rare complications and it appears to demonstrate preliminary efficacy in childhood refractory epilepsy. [ABSTRACT FROM AUTHOR]

Published
2010

45. THE EFFECT OF THE KETOGENIC DIET ON THE GROWTH AND BIOCHEMICAL PARAMETERS OF THE CHILDREN WITH RESISTANT EPILEPSY.

Author

Alaei, Mohammadreza, Ghazavi, Mohammadreza, Mahvelati, Farhad, Karimzadeh, Parvaneh, Shiva, Mohammadreza, and Tonekaboni, Seyed Hassan

Subjects
CHILDREN with epilepsy, KETOGENIC diet, CHILDHOOD epilepsy, CREATININE, HEMOGLOBINS, CALCIUM, BLOOD sugar monitoring, UNSATURATED fatty acids
Abstract

Objective The aim of this study was to evaluate the effect of the ketogenic diet on the growth parameters of the children with resistant epilepsy. Materials & Methods A total of 36 children with resistant epilepsy who were 2 to 7 year old were put on the ketogenic diet. Their growth and biochemical parameters were studied at the beginning of the study and after 3 months. Results Weight decreased in all patients. Serum levels of hemoglobin, calcium, and blood sugar decreased significantly but remained in the normal range. Creatinine did not change, but BUN showed a significant increase. Conclusion We can lower the complications of ketogenic diets by using more unsaturated fat, more water, and more minerals. [ABSTRACT FROM AUTHOR]

Published
2010

46. HEREDITARY SPASTIC PARAPLEGIA: FROM GENE TO CLINIC.

Author

Tonekaboni, Seyed Hassan

Subjects
PARAPLEGIA, PEOPLE with paraplegia, DEGENERATION (Pathology), PYRAMIDAL tract, SPINAL cord diseases, SPASTICITY, LEG muscles, GENETICS, DISEASES
Abstract

Objective Heredity Spastic Paraplegia (HSP) is a degenerative disease of genetic origin affecting the corticospinal tracts in the spinal cord. There are three forms of inheritance: Autosomal dominant HSP, Autosomal rececive HSP and X-linked HSP. This disease is characterized by progressive spasticity of leg muscles with varying degrees of stiffness and weakness of other muscle groups. In this review, we will discuss the latest findings on the pathophysiology of axonal degeneration and all the responsible genetic defects in HSP. [ABSTRACT FROM AUTHOR]

Published
2010

47. The Effects of Sodium Valproate in Improving Developmental Delay in Seizure-Free Children with Abnormal Electroencephalography.

Author

Karimzadeh, Parvaneh, Tonekaboni, Seyed Hassan, and Shamsabadi, Farhad Mahvelati

Subjects
*PEDIATRIC therapy, *CHILD development, *DEVELOPMENTAL delay, *VALPROIC acid, *REHABILITATION, *ELECTROENCEPHALOGRAPHY, *METABOLIC disorders, *ANTICONVULSANTS, *SEIZURES in children
Abstract

Background: Developmental delay is one of the most common problems of children referred to pediatric neurology clinics. While there are reports on rehabilitation and its effects, limited studies are available to delineate pharmacotherapy of such children. Because many children with developmental delay have abnormal findings in electroencephalography, we aimed to treat a group of these children, who were seizure free with sodium valproate to find the effect of sodium valproate in improving the developmental delay. Methods: We included patients referred to Mofid Children's Hospital for developmental delay who had no organic or brain structural diseases, genetic or metabolic disorders, or intrauterine TORCH infection; however, the patients had abnormal electroencephalograms (without seizure). After clinical, para clinical, and neuroimaging evaluations, the patients were divided into two groups; those receiving treatment with sodium valproate and rehabilitation (experimental group, 25 patients), and those having only rehabilitation (control group, 25 patients). The patients were followed up and assessed at 6, 12, and 18 months after initiation of the study. The data obtained were analyzed using SPSS software. Results: All patients in the experimental group had normal electroencephalograms after 18 months of treatment. Differences in the scores of developmental quotient in both groups, before and after treatment were significant. Conclusion: Sodium valproate along with rehabilitation was very effective in the improvement of speech, mental, and behavioral development. [ABSTRACT FROM AUTHOR]

Published
2009

48. Novel Digital Anomalies, Hippocampal Atrophy, and Mutations Expand the Genotypic and Phenotypic Spectra of CNKSR2 in the Houge Type of X-Linked Syndromic Intellectual Development Disorder (MRXSHG).

Author

Ghasemi MR, Fateh ST, Ben-Mahmoud A, Gupta V, Stühn LG, Lesca G, Chatron N, Platzer K, Edery P, Sadeghi H, Isidor B, Cogné B, Schulz HL, Krauspe-Stübecke I, Periyasamy R, Nampoothiri S, Mirfakhraie R, Alijanpour S, Syrbe S, Pfeifer U, Spranger S, Grundmann-Hauser K, Haack TB, Papadopoulou MT, da Silva Gonçalves T, Panagiotakaki E, Arzimanoglou A, Tonekaboni SH, Rossi M, Korenke GC, Lacassie Y, Jang MH, Layman LC, Miryounesi M, and Kim HG

Abstract

The Houge type of X-linked syndromic intellectual developmental disorder (MRXSHG) encompasses a spectrum of neurodevelopmental disorders characterized by intellectual disability (ID), language/speech delay, attention issues, and epilepsy. These conditions arise from hemizygous or heterozygous deletions, along with point mutations, affecting CNKSR2, a gene located at Xp22.12. CNKSR2, also known as CNK2 or MAGUIN, functions as a synaptic scaffolding molecule within the neuronal postsynaptic density (PSD) of the central nervous system. It acts as a link connecting postsynaptic structural proteins, such as PSD95 and S-SCAM, by employing multiple functional domains crucial for synaptic signaling and protein-protein interactions. Predominantly expressed in dendrites, CNKSR2 is vital for dendritic spine morphogenesis in hippocampal neurons. Its loss-of-function variants result in reduced PSD size and impaired hippocampal development, affecting processes including neuronal proliferation, migration, and synaptogenesis. We present 15 patients including three from the MENA (Middle East and North Africa), a region with no documented mutations in CNKSR2. Each individual displays unique clinical presentations that encompass developmental delay, ID, language/speech delay, epilepsy, and autism. Genetic analyses revealed 14 distinct variants in CNKSR2, comprising five nonsense, three frameshift, two splice, and four missense variants, of which 13 are novel. The ACMG guidelines unanimously interpreted these 14 variants in 15 individuals as pathogenic, highlighting the detrimental impact of these CNKSR2 genetic alterations and confirming the molecular diagnosis of MRXSHG. Importantly, variants Ser767Phe and Ala827Pro may lead to proteasomal degradation or reduced PSD size, contributing to the neurodevelopmental phenotype. Furthermore, these two amino acids, along with another two affected by four missense variants, exhibit complete conservation in nine vertebrate species, illuminating their crucial role in the gene's functionality. Our study revealed unique new digital and brain phenotype, including pointed fingertips (fetal pads of fingertips), syndactyly, tapering fingers, and hippocampal atrophy. These novel clinical features in MRXSHG, combined with 13 novel variants, expand the phenotypic and genotypic spectra of MRXSHG associated with CNKSR2 mutations., (© 2024 The Author(s). American Journal of Medical Genetics Part A published by Wiley Periodicals LLC.)

Published
2024
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49. Biotinidase deficiency: a reversible neurometabolic disorder (an Iranian pediatric case series).

Author

Karimzadeh P, Ahmadabadi F, Jafari N, Jabbehdari S, Alaee MR, Ghofrani M, Taghdiri MM, and Tonekaboni SH

Abstract

Objective: Biotinidase deficiency is one of the rare congenital metabolic disorders with autosomal recessive inheritance. If this disorder is diagnosed in newborn period, could be prevented well from mental and physical developmental delay and most of clinical manifestations., Materials & Methods: The patients were diagnosed as biotinidase deficiency in Neurology Department of Mofid Children's Hospital in Tehran, Iran, between 2009 and 2012 were included in this study. This study was conducted to define the age, gender, past medical history, developmental status, general appearance, clinical manifestations, neuroimaging findings, and response to treatment in 16 patients with biotinidase deficiency in this department., Results: In clinical presentation, cutaneous lesions were not found in 37% of the patients and 43% patients had not alopecia. 75% patients had abnormal neuroimaging that in 56% of them, generalized brain atrophy and myelination delay were found. Results of the present study showed the efficacy of biotin in early diagnosed patients with seizure and dermatological manifestations. The seizure and skin manifestations were improved after biotin therapy., Conclusion: According to the results of this study, we suggest that early assessment and diagnosis have an important role in the prevention of disease progression and clinical signs.

Published
2013

50. Neuroimaging findings in first unprovoked seizures: a multicentric study in tehran.

Author

Molla Mohammadi M, Tonekaboni SH, Khatami A, Azargashb E, Tavasoli A, Javadzadeh M, and Zamani G

Abstract

Objective: Seizure is an emergency in pediatrics. It really matters to the parents of the involved child to have information about the causes, management and prognosis. First unprovoked seizures (FUS) are seizures that occur in patients without fever, trauma or infection. Due to the rapid improvement in diagnostic techniques in the last few decades, the etiology will be revealed and this term will no longer exist. This Study was designed to evaluate brain imaging findings in FUS patients., Materials & Methods: Ninety-six children with FUS, who were admitted in three major children's hospitals in Tehran, underwent brain imaging and were enrolled into the study. The decision about the type of imaging (CT or MRI) was based on the patient's medical and financial conditions. An expert radiologist in the field of pediatric neuroimaging interpreted the images., Results: Altogether, 27.1% had abnormal findings of which 29.2% were in the brain MRI group and 14.3% were in the brain CT scan group. Abnormal results were gliosis (10.4%), hemorrhage (4.2%), dysgenesis (2.1%), dysmyelination (7.3%), encephalomalacy (1%), atrophy (5.2%) and infarction (2.1%). In some patients, the lesions were in 2 or 3 sites and some had more than one type of lesion. There was no association between the duration, age and type of seizure and imaging abnormlities. However, we found an association between the location of the lesion and the type of seizure., Conclusion: We recommend brain imaging in all patients with FUS and apart from some exceptions, brain MRI is superior to CT.

Published
2013

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