Your search keyword '"NILIPOUR, Yalda"' showing total 10 results

1. Description of clinical features and genetic analysis of one ultra-rare (SPG64) and two common forms (SPG5A and SPG15) of hereditary spastic paraplegia families.

Author

Pashaei, Mahdieh, Davarzani, Atefeh, Hajati, Reza, Zamani, Babak, Nafissi, Shahriar, Larti, Farzaneh, Nilipour, Yalda, Rohani, Mohammad, and Alavi, Afagh

Subjects

FAMILIAL spastic paraplegia, PHENOTYPES, FAMILIES, GENETIC mutation, NEURODEGENERATION

Abstract

Hereditary spastic paraplegia (HSP) is a clinically and genetically heterogeneous neurodegenerative disorder, characterized by lower-limb spasticity and weakness. To date, more than 82 loci/genes (SPG1-SPG82) have been identified that contribute to the cause of HSP. Despite the use of next-generation sequencing-based methods, genetic-analysis has failed in the finding of causative genes in more than 50% of HSP patients, indicating a more significant heterogeneity and absence of a given phenotype-genotype correlation. Here, we performed whole-exome sequencing (WES) to identify HSP-causing genes in three unrelated-Iranian probands. Candidate variants were detected and confirmed in the probands and co-segregated in the family members. The phenotypic data gathered and compared with earlier cases with the same sub-types of disease. Three novel homozygous variants, c.978delT; p.Q327Kfs*39, c.A1208G; p.D403G and c.3811delT; p.S1271Lfs*44, in known HSP-causing genes including ENTPD1, CYP7B1, and ZFYVE26 were identified, respectively. Intra and interfamilial clinical variability were observed among affected individuals. Mutations in CYP7B1 and ZFYVE26 are relatively common causes of HSP and associated with SPG5A and SPG15, respectively. However, mutations in ENTPD1 are related to SPG64 which is an ultra-rare form of HSP. The research affirmed more complexities of phenotypic manifestations and allelic heterogeneity in HSP. Due to these complexities, it is not feasible to show a clear phenotype-genotype correlation in HSP cases. Identification of more families with mutations in HSP-causing genes may help the establishment of this correlation, further understanding of the molecular basis of the disease, and would provide an opportunity for genetic-counseling in these families. [ABSTRACT FROM AUTHOR]

Published

2021

2. Reporting a rare form of myopathy, myopathy with extrapyramidal signs, in an Iranian family using next generation sequencing: a case report.

Author

Mojbafan, Marzieh, Nojehdeh, Somayeh Takrim, Rahiminejad, Faezeh, Nilipour, Yalda, Tonekaboni, Seyed Hasan, and Zeinali, Sirous

Subjects

MICROSATELLITE repeats, MEDICAL genetics, MUSCLE diseases, GENETIC mutation, LIMB-girdle muscular dystrophy

Abstract

Background: Myopathy with extrapyramidal signs (MPXPS) is an autosomal recessive mitochondrial disorder which is caused by mutation in mitochondrial calcium uptake 1 (MICU1) gene located on chromosome 10q22.1. Next Generation Sequencing (NGS) technology is the most effective method for identification of pathogenic variants with the ability to overcome some limitations which Sanger sequencing may encountered. There are few reports on this rare disease around the world and here in this study we first revealed genetic identification of two affected individuals in an Iranian family with a novel mutation. Case presentation: The proband was a 5-year-old girl from consanguenous parents. She was first clinically suspicious of affected with limb-girdle muscular dystrophy (LGMD). Muscle biopsy studies and autozygosity mapping, using four short tandem repeat (STR) markers linked to 6 genes of the most prevalent forms of LGMD, ruled out calpainopathy, dysferlinopathy, and sarcoglycanopathis. DNA sample of the proband was sent for NGS. Whole exome sequencing (WES) revealed a novel mutation c.1295delA in exon 13 of MICU1 gene. This homozygous deletion creates a frameshift and a premature stop codon downstream of canonical EF4 calcium binding motif of MICU1. According to the American College of Medical Genetics and Genomics (ACMG) guidline for sequence interpretation, this variant was a pathogenic one. Sanger sequencing in all family members confirmed the results of the WES. Conclusions: This study was the first report of MPXPS in Iranian population which also revealed a novel mutation in the MICU1 gene. [ABSTRACT FROM AUTHOR]

Published

2020

3. Late-onset pompe disease in Iran: A clinical and genetic report.

Author

Nazari, Ferdos, Sinaei, Farnaz, Nilipour, Yalda, Fatehi, Farzad, Streubel, Berthold, Ashrafi, Mahmoud Reza, Aryani, Omid, and Nafissi, Shahriar

Subjects

CONSANGUINITY, DISEASE susceptibility, ELECTROMYOGRAPHY, EVOKED potentials (Electrophysiology), FAMILY health, GLYCOSIDASES, GENETIC mutation, RESPIRATORY diseases, SKELETAL muscle, GENOTYPES, INBORN errors of carbohydrate metabolism, DIAGNOSIS, THERAPEUTICS

Abstract

Introduction: Pompe disease is characterized by absence or deficiency of acid α-glucosidase, and several causative mutations are known. In this study we report clinical and laboratory data in Iranian patients with late-onset Pompe disease (LOPD), focusing on population-specific mutations.Methods: Clinical and laboratory data of 14 patients from 10 families with the diagnosis of LOPD were recorded. All had reduced enzyme activity on dried blood spot (DBS) analysis. Genetic investigation was performed to identify the underlying mutations.Results: The age of onset ranged from <2 to 38 years. The clinical presentations were heterogeneous. Two siblings presented with foot drop. The most common mutation was c.(-32-13T>G). There were 4 novel mutations: c.(2040 + 2dup); c.(1650delG); c.(1837T>G); and c.(2596delG).Conclusion: This is a comprehensive report of LOPD in Iranian patients. Distinct phenotypic and genotypic features in this population are highlighted. Muscle Nerve 55: 835-840, 2017. [ABSTRACT FROM AUTHOR]

Published

2017

4. A novel mutation in alpha sarcoglycan gene in an Iranian family with limb girdle muscular dystrophy 2D.

Author

Mojbafan, Marzieh, Nilipour, Yalda, Tonekaboni, Seyed Hasan, Tavakkoly-Bazzaz, Javad, and Zeinali, Sirous

Subjects

MUSCULAR dystrophy, GENETIC mutation, SARCOGLYCANS, PHENOTYPES, IMMUNOHISTOCHEMISTRY, GENE expression, GENETIC disorders

Abstract

Objective and importance: The sarcoglycanopathies (SGPs) are a subgroup of autosomal recessive limb girdle muscular dystrophies. They are caused by mutations in gamma, alpha, beta, and delta sarcoglycans (SGs) genes. Alpha-SGPs are the most frequent form of SGPs. Muscle biopsy studies in patients with SGPs have indicated that loss of one SG subunit leads to instability of whole SG complex. Autozygosity mapping is a powerful gene mapping approach for rare recessive inherited disorders in consanguineous families. Clinical presentation: In the present study, proband was a 9 year old girl from consanguineous parents. She was diagnosed at the age of 5 when she had problems climbing stairs. Her creatine kinase level was 16428 U/L. Proximal weakness and ankle contracture were also observed in the patient. Techniques: Autozygosity mapping, using short tandem repeat (STR) markers linked to the SG genes, showed co-segregation of the phenotype with STR markers linked to the SGCA (Alpha-sarcoglycan) gene. Her muscle biopsy also suggested alpha sarcoglycanopathy. Mutation analyses revealed a novel homozygous deletion of 11 base pairs in exon 4 of this gene. This deletion introduces a premature termination codon after the 4th amino acid. This will eliminate the expression of the downstream part of the extracellular domain of the protein. This domain has a critical role by associating with other molecules of dystrophin-glycoprotein complexes. Conclusion: IHC (Immunohistochemistry) studies combined with autozygosity mapping and mutation screening is an efficient diagnostic method in the SGPs. [ABSTRACT FROM AUTHOR]

Published

2016

5. Analysis of dystrophin gene in Iranian Duchenne and Becker muscular dystrophies patients and identification of a novel mutation.

Author

Zamani, Gholam, Karami, Fatemeh, Mehdizadeh, Mahshid, Movafagh, Abolfazl, Nilipour, Yalda, Zamani, Mahdi, and Zamani, Gholam Reza

Subjects

DYSTROPHIN genetics, GENETIC mutation, DUCHENNE muscular dystrophy, MUSCULAR dystrophy genetics, NUCLEOTIDE sequencing, EXONS (Genetics), DELETION mutation, IRANIANS, GENES, RETROSPECTIVE studies, SEQUENCE analysis

Abstract

Duchenne muscular dystrophy (DMD) and Becker muscular dystrophy (BMD) are the most frequent muscular dystrophies. Present study aimed to determine the frequency of dystrophin gene alterations in Iranian DMD/BMD patients using molecular techniques. 146 Iranian DMD/BMD patients have been analyzed using two devised sets of multiplex polymerase chain reaction (M-PCR) followed by multiple ligation-dependent probe amplification (MLPA). Two isolated DMD and BMD patients were analyzed by DNA sequencing. 30.9 % of patients had single-exon deletion while group and contiguous exon deletions were identified in 41 % of the patients. The most numerous exon deletions included exons 45-50 and were identified in the first M-PCR set. Deletion detection rate was 99 % in first M-PCR set and remaining deletions (1 %) were identified in the second M-PCR set. MLPA analysis showed that there were two exons 3-5 and 41-43 duplications (1.4 %) in a BMD and a DMD patient, respectively. Two nonsense mutations including c.633dupA and c.6283 C>T were, respectively, found in a DMD and BMD patient in which c.633dupA has not ever been reported in DMD mutation database and was pathogenic mutation. Besides the report of frequency of dystrophin gene alteration in a subset of Iranian DMD/BMD patients, it was revealed that the proposed M-PCR protocol can be useful in the initial step of molecular diagnosis of DMD/BMD. Exon sequencing would be the final step in determining the mutation status of DMD/BMD patients following MLPA. [ABSTRACT FROM AUTHOR]

Published

2015

6. Congenital myasthenic syndrome with tubular aggregates caused by GFPT1 mutations.

Author

Guergueltcheva, Velina, Müller, Juliane, Dusl, Marina, Senderek, Jan, Oldfors, Anders, Lindbergh, Christopher, Maxwell, Susan, Colomer, Jaume, Mallebrera, Cecilia, Nascimento, Andres, Vilchez, Juan, Muelas, Nuria, Kirschner, Janbernd, Nafissi, Shahriar, Kariminejad, Ariana, Nilipour, Yalda, Bozorgmehr, Bita, Najmabadi, Hossein, Rodolico, Carmelo, and Sieb, Jörn

Subjects

CONGENITAL myasthenic syndromes, MYONEURAL junction, GENETIC mutation, PROTEIN kinases, GLUTAMINE, AMINOTRANSFERASES

Abstract

Congenital myasthenic syndrome (CMS) is a clinically and genetically heterogeneous group of inherited disorders of the neuromuscular junction. A difficult to diagnose subgroup of CMS is characterised by proximal muscle weakness and fatigue while ocular and facial involvement is only minimal. DOK7 mutations have been identified as causing the disorder in about half of the cases. More recently, using classical positional cloning, we have identified mutations in a previously unrecognised CMS gene, GFPT1, in a series of DOK7-negative cases. However, detailed description of clinical features of GFPT1 patients has not been reported yet. Here we describe the clinical picture of 24 limb-girdle CMS (LG-CMS) patients and pathological findings of 18 of them, all carrying GFPT1 mutations. Additional patients with CMS, but without tubular aggregates, and patients with non-fatigable weakness with tubular aggregates were also screened. In most patients with GFPT1 mutations, onset of the disease occurs in the first decade of life with characteristic limb-girdle weakness and fatigue. A common feature was beneficial and sustained response to acetylcholinesterase inhibitor treatment. Most of the patients who had a muscle biopsy showed tubular aggregates in myofibers. Analysis of endplate morphology in one of the patients revealed unspecific abnormalities. Our study delineates the phenotype of CMS associated with GFPT1 mutations and expands the understanding of neuromuscular junction disorders. As tubular aggregates in context of a neuromuscular transmission defect appear to be highly indicative, we suggest calling this condition congenital myasthenic syndrome with tubular aggregates (CMS-TA). [ABSTRACT FROM AUTHOR]

Published

2012

7. A novel missense mutation in the GNE gene in an Iranian patient with hereditary inclusion body myopathy.

Author

Behnam, Mahdiyeh, Shin Jin-Hong, Dae-Seong Kim, Basiri, Keivan, Nilipour, Yalda, and Sedghi, Maryam

Subjects

MUSCLE diseases, GENES, GENETIC mutation, GENETICS

Abstract

Hereditary inclusion body myopathy (hIBM) is an adult-onset hereditary myopathy, usually with distal onset and quadriceps sparing. This myopathy is autosomal recessive and associated to UPD-N-acetylglucosamine-2-epimerase/N-acetylmannosamine kinase (GNE) gene mutations. In this study, we report a novel GNE homozygous point mutation c.1834T>G that results in amino acid substitution of cysteine 612 to glutamine in an Iranian patient. This mutation is located in exon 10 within the kinase domain of the protein. [ABSTRACT FROM AUTHOR]

Published

2014

8. Multiple acyl-coenzyme A dehydrogenase deficiency shows a possible founder effect and is the most frequent cause of lipid storage myopathy in Iran.

Author

Nilipour, Yalda, Fatehi, Farzad, Sanatinia, Saleheh, Bradshaw, Anna, Duff, Jennifer, Lochmüller, Hanns, Horvath, Rita, and Nafissi, Shahriar

Subjects

*GENETIC mutation, *MUSCLE strength, *GLUCOSE-6-phosphate dehydrogenase deficiency, *MUSCLE diseases, *METABOLIC disorders, *LIPIDS

Abstract

Multiple acyl-coenzyme A dehydrogenase deficiency disorder (MADD) is a relatively rare disorders of lipid metabolism. This study aimed to investigate the demographic, clinical, and genetic features of MADD in Iran. Twenty-nine patients with a definite diagnosis of lipid storage myopathy were recruited. All patients were tested for mutation in the ETFDH gene, and 19 had a biallelic mutation in this gene. Of 19 patients with definite mutations, 11 (57.9%) were female, and the median age was 31 years. Twelve patients had c.1130 T > C (p.L377P) mutation in exon 10. Two patients had two novel heterozygote pathogenic variants (c.679C > T (p.P227S) in exon 6 and c.814G > A (p.G272R) in exon 7) and two patients had c.1699G > A (p.E567K) in exon 13. Before treatment, the median muscle power was 4.6 (IQR: 4–4.7) that increased to 5 (IQR: 5–5) after treatment (Z = −3.71, p =.000). The median CK was 1848 U/l (IQR: 1014–3473) before treatment, which declined to 188 U/l (IQR: 117–397) after treatment (Z = −3.41, p =.001). Sixteen patients (84.2%) had full recovery after the treatment. The disease onset was earlier (12 years of age; IQR: 6–18) in patients with homozygous c.1130 T > C; p.(L377P) mutation compared to other ETFDH mutations (30 years of age; IQR: 20–35) (p =.00). MADD has different clinical presentations. As the patients respond favorably to treatment, early diagnosis and treatment may prevent the irreversible complications of the disease. Unlabelled Image • MADDs are rare disorders of lipid metabolism due to mutation in the ETFDH gene. • We describe 19 Iranian patients with a biallelic mutation in the ETFDH. • We found two patients with two novel heterozygote pathogenic variants. • The patients had different clinical presentations. • Early diagnosis and treatment may prevent irreversible complications. [ABSTRACT FROM AUTHOR]

Published

2020

9. Hexosamine Biosynthetic Pathway Mutations Cause Neuromuscular Transmission Defect

Author

Senderek, Jan, Müller, Juliane S., Dusl, Marina, Strom, Tim M., Guergueltcheva, Velina, Diepolder, Irmgard, Laval, Steven H., Maxwell, Susan, Cossins, Judy, Krause, Sabine, Muelas, Nuria, Vilchez, Juan J., Colomer, Jaume, Mallebrera, Cecilia Jimenez, Nascimento, Andres, Nafissi, Shahriar, Kariminejad, Ariana, Nilipour, Yalda, Bozorgmehr, Bita, and Najmabadi, Hossein

Subjects

*HEXOSAMINES, *AMINE synthesis, *BIOSYNTHESIS, *GENETIC mutation, *NEUROMUSCULAR transmission, *MOTOR neurons, *ZEBRA danio

Abstract

Neuromuscular junctions (NMJs) are synapses that transmit impulses from motor neurons to skeletal muscle fibers leading to muscle contraction. Study of hereditary disorders of neuromuscular transmission, termed congenital myasthenic syndromes (CMS), has helped elucidate fundamental processes influencing development and function of the nerve-muscle synapse. Using genetic linkage, we find 18 different biallelic mutations in the gene encoding glutamine-fructose-6-phosphate transaminase 1 (GFPT1) in 13 unrelated families with an autosomal recessive CMS. Consistent with these data, downregulation of the GFPT1 ortholog gfpt1 in zebrafish embryos altered muscle fiber morphology and impaired neuromuscular junction development. GFPT1 is the key enzyme of the hexosamine pathway yielding the amino sugar UDP-N-acetylglucosamine, an essential substrate for protein glycosylation. Our findings provide further impetus to study the glycobiology of NMJ and synapses in general. [ABSTRACT FROM AUTHOR]

Published

2011

10. BVVL/ FL: features caused by SLC52A3 mutations; WDFY4 and TNFSF13B may be novel causative genes.

Author

Khani, Marzieh, Shamshiri, Hosein, Taheri, Hanieh, Hardy, John, Bras, Jose Tomas, Carmona, Susana, Moazzeni, Hamidreza, Alavi, Afagh, Heshmati, Ali, Taghizadeh, Peyman, Nilipour, Yalda, Ghazanfari, Tooba, Shahabi, Majid, Okhovat, Ali Asghar, Rohani, Mohammad, Valle, Giorgio, Boostani, Reza, Abdi, Siamak, Eshghi, Shaghayegh, and Nafissi, Shahriar

Subjects

*GENES, *AMYOTROPHIC lateral sclerosis, *MAGNETIC resonance imaging, *GENETIC mutation, *SELF-expression

Abstract

Brown-Vialetto-Van Laere (BVVL) and Fazio-Londe are disorders with amyotrophic lateral sclerosis–like features, usually with recessive inheritance. We aimed to identify causative mutations in 10 probands. Neurological examinations, genetic analysis, audiometry, magnetic resonance imaging, biochemical and immunological testings, and/or muscle histopathology were performed. Mutations in known causative gene SLC52A3 were found in 7 probands. More importantly, only 1 mutated allele was observed in several patients, and variable expressivity and incomplete penetrance were clearly noted. Environmental insults may contribute to variable presentations. Putative causative mutations in other genes were identified in 3 probands. Two of the genes, WDFY4 and TNFSF13B , have immune-related functions. Inflammatory responses were implicated in the patient with the WDFY4 mutation. Malfunction of the immune system and mitochondrial anomalies were shown in the patient with the TNFSF13B mutation. Prevalence of heterozygous SLC52A3 BVVL causative mutations and notable variability in expressivity of homozygous and heterozygous genotypes are being reported for the first time. Identification of WDFY4 and TNFSF13B as candidate causative genes supports conjectures on involvement of the immune system in BVVL and amyotrophic lateral sclerosis. • Only one mutated SLC52A3 allele found in several BVVL patients. • Variable expressivity and penetrance are associated with SLC52A3 mutations. • Environmental insults may contribute to presentations of BVVL pathology. • WDFY4 and TNFSF13B are candidate BVVL-causative genes. • Malfunction of the immune system may contribute to BVVL etiology. [ABSTRACT FROM AUTHOR]

Published

2021