Your search keyword '"Maryam Beheshtian"' showing total 43 results

1. Clinical application of next generation sequencing for Mendelian disease diagnosis in the Iranian population

Author

Ayda Abolhassani, Zohreh Fattahi, Maryam Beheshtian, Mahsa Fadaee, Raheleh Vazehan, Fatemeh Ahangari, Shima Dehdahsi, Mehrshid Faraji Zonooz, Elham Parsimehr, Zahra Kalhor, Fatemeh Peymani, Maryam Mozaffarpour Nouri, Mojgan Babanejad, Khadijeh Noudehi, Fatemeh Fatehi, Shima Zamanian Najafabadi, Fariba Afroozan, Hilda Yazdan, Bita Bozorgmehr, Azita Azarkeivan, Shokouh Sadat Mahdavi, Pooneh Nikuei, Farzad Fatehi, Payman Jamali, Mahmoud Reza Ashrafi, Parvaneh Karimzadeh, Haleh Habibi, Kimia Kahrizi, Shahriar Nafissi, Ariana Kariminejad, and Hossein Najmabadi

Subjects

Medicine, Genetics, QH426-470

Abstract

Abstract Next-generation sequencing (NGS) has been proven to be one of the most powerful diagnostic tools for rare Mendelian disorders. Several studies on the clinical application of NGS in unselected cohorts of Middle Eastern patients have reported a high diagnostic yield of up to 48%, correlated with a high level of consanguinity in these populations. We evaluated the diagnostic utility of NGS-based testing across different clinical indications in 1436 patients from Iran, representing the first study of its kind in this highly consanguineous population. A total of 1075 exome sequencing and 361 targeted gene panel sequencing were performed over 8 years at a single clinical genetics laboratory, with the majority of cases tested as proband-only (91.6%). The overall diagnostic rate was 46.7%, ranging from 24% in patients with an abnormality of prenatal development to over 67% in patients with an abnormality of the skin. We identified 660 pathogenic or likely pathogenic variants, including 241 novel variants, associated with over 342 known genetic conditions. The highly consanguineous nature of this cohort led to the diagnosis of autosomal recessive disorders in the majority of patients (79.1%) and allowed us to determine the shared carrier status of couples for suspected recessive phenotypes in their deceased child(ren) when direct testing was not possible. We also highlight the observations of recessive inheritance of genes previously associated only with dominant disorders and provide an expanded genotype–phenotype spectrum for multiple less-characterized genes. We present the largest mutational spectrum of known Mendelian disease, including possible founder variants, throughout the Iranian population, which can serve as a unique resource for clinical genomic studies locally and beyond.

Published

2024

2. P483: A comprehensive study of spinal muscular atrophy testing referrals’ data among the Iranian population since 2006

Author

Ali Khanbazi, Maryam Beheshtian, Maryam Azad, Masoume Akbari, Fariba Afrozan, Fatemeh Fatehi, Khadijeh Noudehi, Shima Zamanian Najafabadi, Ariana Kariminejad, Kimia Kahrizi, and Hossein Najmabadi

Subjects

Genetics, QH426-470, Medicine

Published

2024

3. P604: Diagnostic utility of NGS testing in a highly consanguineous population: Findings from 1400+ Iranian patients with Mendelian disorders

Author

Ayda Abolhassani, Zohreh Fattahi, Maryam Beheshtian, Mahsa Fadaee, Raheleh Vazehan, Fatemeh Ahangari, Shima Dehdahsi, Mehrshid Faraji Zonooz, Elham Parsimehr, Zahra Kalhor, Fatemeh Peymani, Maryam Mozaffarpour Nouri, Mojgan Babanejad, Khadijeh Noudehi, Fatemeh Fatehi, Shima Zamanian Najafabadi, Fariba Afroozan, Hilda Yazdan, Bita Bozorgmehr, Azita Azarkeivan, Shokouh Sadat Mahdavi, Pooneh Nikuei, Farzad Fatehi, Payman Jamali, Mahmoud Reza Ashrafi, Parvaneh Karimzadeh, Haleh Habibi, Kimia Kahrizi, Shahriar Nafissi, Ariana Kariminejad, and Hossein Najmabadi

Subjects

Genetics, QH426-470, Medicine

Published

2024

4. Phenotype and genotype spectrum of variants in guanine nucleotide exchange factor genes in a broad cohort of Iranian patients

Author

Meysam Mosallaei, Naeim Ehtesham, Maryam Beheshtian, Shahrouz Khoshbakht, Behzad Davarnia, Kimia Kahrizi, and Hossein Najmabadi

Subjects

developmental delay, guanine nucleotide exchange factors, intellectual disability, Iranian families, Genetics, QH426-470

Abstract

Abstract Background Guanine nucleotide exchange factors (GEFs) play pivotal roles in neuronal cell functions by exchanging GDP to GTP nucleotide and activation of GTPases. We aimed to determine the genotype and phenotype spectrum of GEF mutations by collecting data from a large Iranian cohort with intellectual disability (ID) and/or developmental delay (DD). Methods We collected data from nine families with 20 patients extracted from Iranian cohort of 640 families with ID and/or DD. Next‐generation sequencing (NGS) was used to identify the causing variants in recruited families. We also compared our clinical and molecular findings with previously reported patients carrying mutations in these GEF genes in the literature published until mid‐2021. Results We identified disease‐causing variants in eight GEF genes including ALS2, IQSEC2, MADD, RAB3GAP1, RAB3GAP2, TRIO, ITSN1, and DENND2A. The major clinical manifestations in 203 previously reported cases along with our 20 patients with disease causing variants in eight GEF genes were as follow; speech disorder (85.2%), ID (81.6%), DD (81.1%), inability to walk (71.3%), facial dysmorphisms features (52.4%), abnormalities in skull morphology (55.6%), hypotonia and muscle weakness (47%), and brain MRI abnormalities (43.4%). Conclusion Our study provides new insights into the genotype and phenotype spectrum of mutations in GEF genes.

Published

2022

5. Whole genome sequencing identifies a duplicated region encompassing Xq13.2q13.3 in a large Iranian family with intellectual disability

Author

Sepideh Mehvari, Farzaneh Larti, Hao Hu, Zohreh Fattahi, Maryam Beheshtian, Seyedeh Sedigheh Abedini, Sanaz Arzhangi, Hans‐Hilger Ropers, Vera M. Kalscheuer, Daniel Auld, Kimia Kahrizi, Yasser Riazalhosseini, and Hossein Najmabadi

Subjects

intellectual disability, whole genome sequencing, Xq duplication, Xq13.2q13.3, Genetics, QH426-470

Abstract

Abstract Background The X chromosome has historically been one of the most thoroughly investigated chromosomes regarding intellectual disability (ID), whose etiology is attributed to many factors including copy number variations (CNVs). Duplications of the long arm of the X chromosome have been reported in patients with ID, short stature, facial anomalies, and in many cases hypoplastic genitalia and/or behavioral abnormalities. Methods Here, we report on a large Iranian family with X‐linked ID caused by a duplication on the X chromosome identified by whole genome sequencing in combination with linkage analysis. Results Seven affected males in different branches of the family presented with ID, short stature, seizures, facial anomalies, behavioral abnormalities (aggressiveness, self‐injury, anxiety, impaired social interactions, and shyness), speech impairment, and micropenis. The duplication of the region Xq13.2q13.3, which is ~1.8 Mb in size, includes seven protein‐coding OMIM genes. Three of these genes, namely SLC16A2, RLIM, and NEXMIF, if impaired, can lead to syndromes presenting with ID. Of note, this duplicated region was located within a linkage interval with a LOD score >3. Conclusion Our report indicates that CNVs should be considered in multi‐affected families where no candidate gene defect has been identified in sequencing data analysis.

Published

2020

6. Brief Report of Variants Detected in Hereditary Hearing Loss Cases in Iran over a 3-Year Period

Author

Niloofar BAZAZZADEGAN, Raheleh VAZEHAN, Mahsa FADAEE, Zohreh FATTAHI, Ayda ABOLHASSANI, Elham PARSIMEHR, Zahra KALHOR, Mehrshid FARAJI ZONOOZ, Fatemeh AHANGARI, Shima DEHDAHSI, Farshide SAMIEE, Payman JAMALI, Haleh HABIBI, Younes NOURIZADEH, Shokouh MAHDAVI, Maryam BEHESHTIAN, Ariana KARIMINEJAD, Richard JH SMITH, and Hossein NAJMABADI

Subjects

OtoSCOPE, Hereditary hearing loss, Novel variant, Known variant, Public aspects of medicine, RA1-1270

Abstract

Background: Diagnosis of hereditary hearing loss (HHL) as a heterogeneous disorder is very important espe-cially in countries with high rates of consanguinity where the autosomal recessive pattern of inheritance is preva-lent. Techniques such as next-generation sequencing, a comprehensive genetic test using targeted genomic en-richment and massively parallel sequencing (TGE + MPS), have made the diagnosis more cost-effective. The aim of this study was to determine HHL variants with comprehensive genetic testing in our country. Methods: Fifty GJB2 negative individuals with HHL were referred to the Kariminejad-Najmabadi Pathology and Genetics Center, Tehran, one of the reference diagnostic genetic laboratories in Iran, during a 3-year period between 2014 and 2017. They were screened with the OtoSCOPE test, the targeted genomic enrichment and massively parallel sequencing (TGE + MPS) platform after a detailed history had been taken along with clinical evaluation. Results: Among 32 out of 50 GJB2 negative patients (64%), 34 known pathogenic and novel variants were de-tected of which 16 (47%) were novel, identified in 10 genes of which the most prevalent were CDH23, MYO7A and MYO15A. Conclusion: These results provide a foundation from which to make appropriate recommendations for the use of comprehensive genetic testing in the evaluation of Iranian patients with hereditary hearing loss.

Published

2019

7. Distinct genetic variation and heterogeneity of the Iranian population.

Author

Zohreh Mehrjoo, Zohreh Fattahi, Maryam Beheshtian, Marzieh Mohseni, Hossein Poustchi, Fariba Ardalani, Khadijeh Jalalvand, Sanaz Arzhangi, Zahra Mohammadi, Shahrouz Khoshbakht, Farid Najafi, Pooneh Nikuei, Mohammad Haddadi, Elham Zohrehvand, Morteza Oladnabi, Akbar Mohammadzadeh, Mandana Hadi Jafari, Tara Akhtarkhavari, Ehsan Shamsi Gooshki, Aliakbar Haghdoost, Reza Najafipour, Lisa-Marie Niestroj, Barbara Helwing, Yasmina Gossmann, Mohammad Reza Toliat, Reza Malekzadeh, Peter Nürnberg, Kimia Kahrizi, Hossein Najmabadi, and Michael Nothnagel

Subjects

Genetics, QH426-470

Abstract

Iran, despite its size, geographic location and past cultural influence, has largely been a blind spot for human population genetic studies. With only sparse genetic information on the Iranian population available, we pursued its genome-wide and geographic characterization based on 1021 samples from eleven ethnic groups. We show that Iranians, while close to neighboring populations, present distinct genetic variation consistent with long-standing genetic continuity, harbor high heterogeneity and different levels of consanguinity, fall apart into a cluster of similar groups and several admixed ones and have experienced numerous language adoption events in the past. Our findings render Iran an important source for human genetic variation in Western and Central Asia, will guide adequate study sampling and assist the interpretation of putative disease-implicated genetic variation. Given Iran's internal genetic heterogeneity, future studies will have to consider ethnic affiliations and possible admixture.

Published

2019

8. Iran′s Multiple Indicator Demographic and Health Survey - 2010: Study Protocol

Author

Arash Rashidian, Akram Karimi-Shahanjarini, Ardeshir Khosravi, Elham Elahi, Maryam Beheshtian, Elham Shakibazadeh, Roghayeh Khabiri, Mohammad Arab, and Mohammad-Reza Zakeri

Subjects

National survey, quality assurance, sampling, survey design, Medicine

Abstract

Background: There is an international emphasis on providing timely and high quality data to monitor progress of countries toward Millennium Development Goals. Iran′s Multiple Indicator Demographic and Health Survey (IrMIDHS) aimed to provide valid information on population and health outcomes to monitor progress in achieving national priorities and health programs and to assist policy makers to design effective strategies for improving health outcomes and equity in access to care. Methods: A cross-sectional multi-stage stratified cluster-random survey is conducted through face-to-face household interviews. The sampling frame is developed using Iran′s 2006 population and housing census. Provincial samples ranging are from a minimum of 400 households per province to 6400 households in Tehran province. Cluster size is 10 households. The target sample includes 3096 clusters: 2187 clusters in urban and 909 clusters in rural areas. IrMIDHS instruments include three questionnaires: Household questionnaire, women aged 15-54 questionnaire, children under five questionnaire, supervision and quality assessment checklists and data collection sheets and standard weight and height measurement tools for under-five children. A cascading decentralized training method is used for training data collection and supervision teams. Quality assurance procedures are defined for the five steps of conducting the survey including: Sampling, training data collection and training teams, survey implementation, data entry and analysis. A multi-layer supervision and monitoring procedure is established. All the questionnaires are double entered. Conclusions: IrMIDHS will provide valuable data for policymakers in Iran. Designing and implementation of the study involve contributions from academics as well as program managers and policy makers. The collaborative nature of the study may facilitate better usage of its results.

Published

2014

9. Characterizing Genotypes and Phenotypes Associated with Dysfunction of Channel-Encoding Genes in a Cohort of Patients with Intellectual Disability

Author

Naeim Ehtesham, Meysam Mosallaei, Maryam Beheshtian, Shahrouz Khoshbakht, Mahsa Fadaee, Raheleh Vazehan, Mehrshid Faraji Zonooz, Parvaneh Karimzadeh, Kimia Kahrizi, and Hossein Najmabadi

Subjects

General Medicine

Abstract

Background: Ion channel dysfunction in the brain can lead to impairment of neuronal membranes and generate several neurological diseases, especially neurodevelopmental disorders. Methods: In this study, we set out to delineate the genotype and phenotype spectrums of 14 Iranian patients from 7 families with intellectual disability (ID) and/or developmental delay (DD) in whom genetic mutations were identified by next-generation sequencing (NGS) in 7 channel-encoding genes: KCNJ10, KCNQ3, KCNK6, CACNA1C, CACNA1G, SCN8A, and GRIN2B. Moreover, the data of 340 previously fully reported ID and/or DD cases with a mutation in any of these seven genes were combined with our patients to clarify the genotype and phenotype spectrum in this group. Results: In total, the most common phenotypes in 354 cases with ID/DD in whom mutation in any of these 7 channel-encoding genes was identified were as follows: ID (77.4%), seizure (69.8%), DD (59.8%), behavioral abnormality (29.9%), hypotonia (21.7%), speech disorder (21.5%), gait disturbance (20.9%), and ataxia (20.3%). Electroencephalography abnormality (33.9%) was the major brain imaging abnormality. Conclusion: The results of this study broaden the molecular spectrum of channel pathogenic variants associated with different clinical presentations in individuals with ID and/or DD.

Published

2022

10. Targeted Next Generation Sequencing Revealed Novel Variants in the PKD1 and PKD2 Genes of Iranian Patients with Autosomal Dominant Polycystic Kidney Disease

Author

Maryam Hosseinpour, Fariba Ardalani, Marzieh Mohseni, Maryam Beheshtian, Sanaz Arzhangi, Shahrzad Ossareh, Hossein Najmabadi, Ali Nobakht, Kimia Kahrizi, and Behrooz Broumand

Subjects

General Medicine

Abstract

Background: Autosomal dominant polycystic kidney disease (ADPKD), one of the common inherited disorders in humans, is characterized by the development and enlargement of renal cysts, often leading to end-stage renal disease (ESRD). In this study, Iranian ADPKD families were subjected to high-throughput DNA sequencing to find potential causative variants facilitating the way toward risk assessment and targeted therapy. Methods: Our protocol was based on the targeted next generation sequencing (NGS) panel previously developed in our center comprising 12 genes involved in PKD. This panel has been applied to investigate the genetic causes of 32 patients with a clinical suspicion of ADPKD. Results: We identified a total of 31 variants for 32 individuals, two of which were each detected in two individuals. Twenty-seven out of 31 detected variants were interpreted as pathogenic/likely pathogenic and the remaining 4 of uncertain significance with a molecular diagnostic success rate of 87.5%. Among these variants, 25 PKD1/2 pathogenic/likely pathogenic variants were detected in 32 index patients (78.1%), and variants of uncertain significance in four individuals (12.5% in PKD1/2). The majority of variants was identified in PKD1 (74.2%). Autosomal recessive PKD was identified in one patient, indicating the similarities between recessive and dominant PKD. In concordance with earlier studies, this biallelic PKD1 variant, p.Arg3277Cys, leads to rapidly progressive and severe disease with very early-onset ADPKD. Conclusion: Our findings suggest that targeted gene panel sequencing is expected to be the method of choice to improve diagnostic and prognostic accuracy in PKD patients with heterogeneity in genetic background.

Published

2022

11. Disease Waves of SARS-CoV-2 in Iran Closely Mirror Global Pandemic Trends

Author

Hanieh Behravan, Ahmad Piroozmand, Azam Ghaziasadi, Khadijeh Jalalvand, Mahdieh Koshki, Fatemeh Tavangar, Angila Ataei-Pirkooh, Farid Yousefi, Masoumeh Bayani, Zohreh Fattahi, Hamed Fakhim, Mojtaba Varshochi, Mohammad Khazeni, Zakiye Mokhames, Fariba Shahraki-Sanavi, Reza Malekzadeh, Maryam Beheshtian, Yousef Yahyapour, Seyed Jalal Kiani, Fariba Keramat, Shokouh Ghafari, Behrooz Ataei, Alireza Abdollahi, Afagh Moattari, Fatemeh Keshavarzi, Mohammad Reza Haghshenas, Alireza AnsariMoghaddam, Maryam Azad, Mohammad Hassan Pouriayevali, Mohsen Moghadami, Azarakhsh Azaran, Zohreh Elahi, Farhang Babamahmoodi, Mohamad Soveyzi, Kimia Kahrizi, Hamid Reza Khorram Khorshid, Vahdat Poortahmasebi, Reza Najafipour, Farzane Zare Ashrafi, Akram Ezani, Farid Azizi Jalilian, Mostafa Salehi-Vaziri, Seyed Mohammad Jazayeri, Seyed Mohammad Hashemi-Shahri, Abdolvahab Moradi, Ali Mojtahedi, Fatemeh Ghodratpour, Marzieh Mohseni, Davod Javanmard, Mahsa Tavakoli, Ali Jafarpour, Hossein Najmabadi, Alijan Tabarraei, Alireza Soleimani, Tahmineh Jalali, Elahe Nasri, Mahmood Yaghoubi, Marzieh Kalhor, Farah Bokharaei-Salim, Iman Rezaeiazhar, and Masood Ziaee

Subjects

Genetics, Whole genome sequencing, education.field_of_study, Mutation, Genetic diversity, Lineage (genetic), Population, Outbreak, General Medicine, Biology, medicine.disease_cause, Genome, medicine, education, Clade

Abstract

SARS-CoV-2 genome surveillance projects provide a good measure of transmission and monitor the circulating SARS-CoV-2 variants at regional and global scales. Iran is one of the most affected countries still involved with the virus circulating in at least five significant disease waves, as of September 2021. Complete genome sequencing of 50 viral isolates in an early phase of outbreak in Iran, shed light on the origins and circulating lineages at that time. As part of a genomic surveillance program, we provided an additional 319 complete genomes from October 2020 onwards. The current study is the report of complete SARS-CoV-2 genome sequences of Iran in the March 2020-May 2021 time interval. We aimed to characterize the genetic diversity of SARS-CoV-2 in Iran over one year. Overall, 35 different lineages and 8 clades were detected. Temporal dynamics of the prominent SARS-CoV-2 clades/lineages circulating in Iran is comparable to the global perspective and introduces the 19A clade (B.4) dominating the first disease wave, followed by 20A (B.1.36), 20B (B.1.1.413), 20I (B.1.1.7) clades, dominating second, third and fourth disease waves, respectively. We observed a mixture of circulating 20A (B.1.36), 20B (B.1.1.413), 20I (B.1.1.7) clades in winter 2021, paralleled in a diminishing manner for 20A/20B and a growing rise for 20I, eventually prompting the 4th outbreak peak. Furthermore, our study provides evidence on the entry of the Delta variant in April 2021, leading to the 5th disease wave in summer 2021. Three lineages are highlighted as hallmarks of SARS-CoV-2 outbreak in Iran; B4, dominating early periods of the epidemic, B.1.1.413 (specific B.1.1 lineage carrying a combination of [D138Y-S477N-D614G] spike mutations) in October 2020-February 2021, and the co-occurrence of [I100T-L699I] spike mutations in half of B.1.1.7 sequences mediating the fourth peak. Continuous monthly monitoring of SARS-CoV-2 genome mutations led to the detection of 1577 distinct nucleotide mutations, in which the top recurrent mutations were D614G, P323L, R203K/G204R, 3037C>T, and 241C>T; the renowned combination of mutations in G and GH clades. The most frequent spike mutation is D614G followed by 13 other frequent mutations based on the prominent circulating lineages; B.1.1.7 (H69_V70del, Y144del, N501Y, A570D, P681H, T716I, S982A, D1118H, I100T, and L699I), B.1.1.413 (D138Y, S477N) and B.1.36 (I210del). In brief, mutation surveillance in this study provided a real-time comprehensive picture of the SARS-CoV-2 mutation profile in Iran, which is beneficial for evaluating the magnitude of the epidemic and assessment of vaccine and therapeutic efficiency in this population.

Published

2022

12. Genetic etiology of hearing loss in Iran

Author

Mojgan Babanejad, Maryam Beheshtian, Fereshteh Jamshidi, Marzieh Mohseni, Kevin T. Booth, Kimia Kahrizi, and Hossein Najmabadi

Subjects

Hearing Loss, Sensorineural, Mutation, Genetics, Humans, Deafness, Iran, Hearing Loss, Genetics (clinical), Pedigree

Abstract

Hearing loss (HL) is an etiologically heterogeneous disorder that affects around 5% of the world's population. There has been an exponential increase in the identification of genes and variants responsible for hereditary HL over recent years. Iran, a country located in the Middle East, has a high prevalence of consanguineous marriages, so heterogeneous diseases such as HL are more common. Comprehensive studies using different strategies from linkage analysis to next-generation sequencing, especially exome-sequencing, have achieved significant success in identifying possible pathogens in deaf Iranian families. About 12% of non-syndromic autosomal recessive HL genes investigated to date, were first identified in families from Iran. Variations of 56 genes have been observed in families with NSHL in Iran. Variants in GJB2, SLC26A4, MYO15A, MYO7A, CDH23, and TMC1 account for 16.5%, 16.25%, 13.5%, 9.35%, 6.9% and 4.92%, cases of NSHL, respectively. In summary, there are also different diagnostic rates between studies conducted in Iran. In the comprehensive investigations conducted by the Genetic Research Center of the University of Social Welfare and Rehabilitation Sciences over the past 20 years, the overall diagnosis rate is about 80% while there are other studies with lower diagnostic rates which could reflect differences in project designs, sampling, and accuracy and validity of the methods used. Furthermore, there are several syndromic HHLs in Iran including, Waardenburg syndrome, BOR syndrome, Brown-Vialetto-Van Laere syndrome, Wolfram syndrome, among which Pendred and Usher syndromes are well-studied. These results are of importance for further investigation and elucidation of the molecular basis of HHL in Iran.

Published

2022

13. CEP104 and CEP290; Genes with Ciliary Functions Cause Intellectual Disability in Multiple Families

Author

Kimia Kahrizi, Mahsa Fadaee, Zohreh Fattahi, Maryam Beheshtian, Shahrouz Khoshbakht, Raheleh Vazehan, Ayda Abolhassani, Arzu Celik, Ariana Kariminejad, Mina Makvand, Mehrshid Faraji Zonooz, Hossein Najmabadi, Niloofar Bazazzadegan, and Elham Parsimehr

Subjects

Genetics, medicine.diagnostic_test, Cilium, General Medicine, Biology, medicine.disease, Phenotype, Ciliopathies, Western blot, Intellectual disability, medicine, Exome, Gene, Exome sequencing

Abstract

Background Neurodevelopmental and intellectual impairments are extremely heterogeneous disorders caused by a diverse variety of genes involved in different molecular pathways and networks. Genetic alterations in cilia, highly-conserved organelles with sensorineural and signal transduction roles can compromise their proper functions and lead to so-called "ciliopathies" featuring intellectual disability (ID) or neurodevelopmental disorders as frequent clinical manifestations. Here, we report several Iranian families affected with ID and other ciliopathy-associated features carrying known and novel variants in two ciliary genes; CEP104 and CEP290. Methods Whole exome and Targeted exome sequencing were carried out on affected individuals. Lymphoblastoid cell lines (LCLs) derived from the members of affected families were established for two families carrying CEP104 mutations. RNA and protein expression studies were carried out on these cells using qPCR and Western blot, respectively. Results A novel homozygous variant; NM_025114.3:c.7341_7344dupACTT p.(Ser2449Thrfs*8) and four previously reported homozygous variants; NM_025114.3:c.322C>T p.(Arg108*), NM_025114.3:c.4393C>T p.(Arg1465*), NM_025114.3:c.5668G>T p.(Gly1890*) and NM_025114.3:c.1666dupA p.(Ile556Asnfs*20) were identified in CEP290. In two other families, two novel homozygous variants; NM_014704:c.2356_2357insTT p.(Cys786Phefs*11) and NM_014704:c.1901_1902insT p.(Leu634Phefs*33) were identified in CEP104, another ciliary gene. qPCR and Western blot analyses showed significantly lower levels of CEP104 transcripts and protein in patients compared to heterozygous or normal family members. Conclusion We emphasize on the clinical variability and pleiotropic phenotypes due to variants of these genes. In conclusion, our findings support the pivotal role of these genes resulting in cognitive and neurodevelopmental features.

Published

2021

14. Molecular Diagnosis of Hereditary Neuropathies by Whole Exome Sequencing and Expanding the Phenotype Spectrum

Author

Raheleh Vazehan, Kimia Kahrizi, Hossein Najmabadi, Farnaz Sadeghinia, Sara Taghizadeh, Shahriar Nafissi, Zohreh Fattahi, Maryam Beheshtian, Sanaz Arzhangi, Ariana Kariminejad, and Marzieh Mohseni

Subjects

Adult, Male, Adolescent, Hereditary spastic paraplegia, Disease, Iran, Biology, Young Adult, Charcot-Marie-Tooth Disease, Exome Sequencing, medicine, Humans, Child, Clinical phenotype, Gene, Exome sequencing, Genetics, Hereditary neuropathies, Genetic Variation, Infant, General Medicine, Middle Aged, medicine.disease, Phenotype, Child, Preschool, Mutation, Spinocerebellar ataxia, Female, Myelin Proteins

Abstract

Background: Inherited peripheral neuropathies (IPNs) are a group of neuropathies affecting peripheral motor and sensory neurons. Charcot-Marie-Tooth (CMT) disease is the most common disease in this group. With recent advances in next-generation sequencing (NGS) technologies, more than 100 genes have been implicated for different types of CMT and other clinically and genetically inherited neuropathies. There are also a number of genes where neuropathy is a major feature of the disease such as spinocerebellar ataxia (SCA) and hereditary spastic paraplegia (HSP). We aimed to determine the genetic causes underlying IPNs in Iranian families. Methods: We performed whole exome sequencing (WES) for 58 PMP22 deletion-/duplication-negative unrelated Iranian patients with a spectrum of phenotypes and with a preliminary diagnosis of hereditary neuropathies. Results: Twenty-seven (46.6%) of the cases were genetically diagnosed with pathogenic or likely pathogenic variants. In this study, we identified genetically strong variants within genes not previously linked to any established disease phenotype in five (8.6%) patients. Conclusion: Our results highlight the advantage of using WES for genetic diagnosis in highly heterogeneous diseases such as IPNs. Moreover, functional analysis is required for novel and uncertain variants.

Published

2020

15. The Role of ATP-Binding Cassette Transporters in the Chemoresistance of Anaplastic Thyroid Cancer: A Systematic Review

Author

Bagher Larijani, Maryam Beheshtian, Hilda Samimi, Sayed Mahmoud Sajjadi-Jazi, Vahid Haghpanah, and Elnaz Abbasifarid

Subjects

0301 basic medicine, medicine.medical_specialty, Abcg2, MEDLINE, ATP-binding cassette transporter, Drug resistance, Cochrane Library, Thyroid Carcinoma, Anaplastic, Bioinformatics, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Internal medicine, medicine, Animals, Humans, ATP Binding Cassette Transporter, Subfamily B, Member 1, Anaplastic thyroid cancer, Thyroid cancer, biology, business.industry, medicine.disease, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, biology.protein, ABCC1, ATP-Binding Cassette Transporters, business, Signal Transduction

Abstract

Anaplastic thyroid cancer (ATC) is an aggressive type of thyroid cancer with a high mortality rate. Cytotoxic drugs are among the treatment modalities usually used for ATC treatment. However, systemic chemotherapies for ATC have not been shown to have remarkable efficacy. ATP-binding cassette (ABC) transporters have been suggested as a possible mechanism in ATC resistance to chemotherapy. This systematic review was aimed to define the possible roles of ABC transporters in ATC resistance to chemotherapy. Numerous databases, including Scopus, Web of Science, PubMed, Cochrane Library, Ovid, ProQuest, and EBSCO, were searched for papers published since 1990, with predefined keywords. The literature searches were updated twice, in 2015 and 2017. All identified articles were reviewed, and 14 papers that met the inclusion criteria were selected. In the eligible studies, the roles of 10 out of 49 ABC transporters were evaluated; among them, three pumps (ABCB1, ABCC1, and ABCG2) were the most studied transporters in ATC samples. ABCC1 and ABCG2 had the highest expression rates in ATC, and ABCB1 ranked second among the inspected transporters. In conclusion, ABC transporters are the major determinants of ATC resistance to chemotherapy. By identifying these transporters, we can tailor the best treatment approach for patients with ATC. Additional studies are needed to define the exact role of each ABC transporter and other mechanisms in ATC drug resistance.

Published

2019

16. Effects of cerebrolysin on functional outcome of patients with traumatic brain injury: a systematic review and meta-analysis

Author

Ali Rasti, Reza Tabrizi, Fariborz Ghaffarpasand, Saeed Torabi, Fatemeh Pakzad, Maryam Beheshtian, Sara Aghabaklou, and Mohammad Hadi Niakan

Subjects

modified Rankin Scale, medicine.medical_specialty, Neuropsychiatric Disease and Treatment, education, cerebrolysin, Cochrane Library, functional outcome, law.invention, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Randomized controlled trial, law, Modified Rankin Scale, Internal medicine, TBI, medicine, Glasgow Coma Scale, 030212 general & internal medicine, Original Research, mRS, business.industry, traumatic brain injury, Glasgow Outcome Scale, GOS, chemistry, Cerebrolysin, Meta-analysis, business, 030217 neurology & neurosurgery, Cohort study

Abstract

Fariborz Ghaffarpasand,1 Saeed Torabi,2 Ali Rasti,3 Mohammad Hadi Niakan,4 Sara Aghabaklou,5 Fatemeh Pakzad,6 Maryam Sadat Beheshtian,7 Reza Tabrizi8 1Research Center for Neuromodulation and Pain, Shiraz University of Medical Sciences, Shiraz, Iran; 2Department of Anesthesiology and Intensive Care Medicine, University Hospital of Cologne, Cologne, Germany; 3Poostchi Ophthalmology Research Center, Shiraz University of Medical Sciences, Shiraz, Iran; 4Trauma Research Center, Rajaei Trauma Hospital, Shiraz University of Medical Sciences, Shiraz, Iran; 5Department of Neurosurgery, Tehran University of Medical Sciences, Tehran, Iran; 6Department of Anesthesiology, Shiraz University of Medical Sciences, Shiraz, Iran; 7Department of Neurosurgery, Shahid Beheshti University of Medical Sciences, Tehran, Iran; 8Health Policy Research Center, Institute of Health, Student Research Committee, Shiraz University of Medical Sciences, Shiraz, Iran Background: Traumatic brain injury (TBI) remains a main public health problem being associated with high mortality and morbidity. The functional outcome of TBI remains unfavorable despite several surgical and medical therapies. Cerebrolysin is a neuropeptide with potential neuroregenerative entities. Objective: The aim of the current systematic review and meta-analysis was to investigate the effects of cerebrolysin on functional outcome in patients with moderate and severe TBI. Data sources: Online databases used included Medline, Scopus, EMBASE, Google Scholar, Web of Science, and Cochrane Library. Study eligibility criteria: All the relevant studies with randomized clinical trial and cohort design evaluating the effects of intravenous cerebrolysin vs placebo on functional outcome of patients with TBI within the English literature up to October 2018 were included. Study appraisal and synthesis methods: The articles were reviewed by two independent authors and the data were extracted to a data sheet. I2 and Cochran’s Q-statistics were used to assess heterogeneity. Based on the presence of significant heterogeneity across included studies, data were pooled using random-effects model with Dersimonian–Laird method and presented as standardized mean differences (SMDs) and corresponding 95% CI. Results: Five articles (5,685 participants) were included in the current meta-analysis. The overall pooled findings using random-effects models among patients with TBI indicated that intravenous administration of cerebrolysin significantly increased Glasgow Outcome Scale score (SMD =0.30; 95% CI: 0.18 to 0.42; P

Published

2018

17. Exome sequencing utility in defining the genetic landscape of hearing loss and novel-gene discovery in Iran

Author

Marzieh Mohseni, Kevin T. Booth, Atefeh Khoshaeen, Fatemeh Bahrami, Payman Jamali, Hossein Najmabadi, Niloofar Bazazzadegan, Kimia Kahrizi, Nooshin Nikzat, Farkhonde Habibi, Richard J.H. Smith, Fariba Ardalani, Mojgan Babanejad, Hanieh Behravan, Fatemeh Keshavarzi, Michael Nothnagel, Faezeh Jahanshad, Seyed Morteza Seifati, Fatemeh Ghodratpour, Sanaz Arzhangi, Behzad Davarnia, Zohreh Mehrjoo, Holger Thiele, Khadijeh Jalalvand, Maryam Beheshtian, Hela Azaiez, Sepide Mirzaei, and Hasan Otukesh

Subjects

0301 basic medicine, Adult, Male, Candidate gene, Adolescent, Hearing loss, Consanguinity, 030105 genetics & heredity, Biology, Iran, DNA sequencing, Article, Cohort Studies, 03 medical and health sciences, Young Adult, Locus heterogeneity, Exome Sequencing, Genetics, medicine, Humans, Exome, Genetic Predisposition to Disease, Child, Hearing Loss, Gene, Genetics (clinical), Exome sequencing, Genetic heterogeneity, High-Throughput Nucleotide Sequencing, Middle Aged, medicine.disease, Pedigree, 030104 developmental biology, Child, Preschool, Mutation, Female, medicine.symptom

Abstract

Hearing loss (HL) is one of the most common sensory defects affecting more than 466 million individuals worldwide. It is clinically and genetically heterogeneous with over 120 genes causing non-syndromic HL identified to date. Here, we performed exome sequencing (ES) on a cohort of Iranian families with no disease-causing variants in known deafness-associated genes after screening with a targeted gene panel. We identified likely causal variants in 20 out of 71 families screened. Fifteen families segregated variants in known deafness-associated genes. Eight families segregated variants in novel candidate genes for HL: DBH, TOP3A, COX18, USP31, TCF19, SCP2, TENM1, and CARMIL1. In the three of these families, intrafamilial locus heterogeneity was observed with variants in both known and novel candidate genes. In aggregate, we were able to identify the underlying genetic cause of HL in nearly 30% of our study cohort using ES. This study corroborates the observation that high-throughput DNA sequencing in populations with high rates of consanguineous marriages represents a more appropriate strategy to elucidate the genetic etiology of heterogeneous conditions such as HL.

Published

2021

18. Author response for 'Exome sequencing utility in defining the genetic landscape of hearing loss and novel‐gene discovery in Iran'

Author

Seyed Morteza Seifati, Maryam Beheshtian, Kevin T. Booth, Behzad Davarnia, Faezeh Jahanshad, Farkhonde Habibi, Michael Nothnagel, Atefeh Khoshaeen, Hanieh Behravan, K. Kahrizi, Fatemeh Ghodratpour, Sanaz Arzhangi, Fatemeh Bahrami, Hossein Najmabadi, Payman Jamali, Marzieh Mohseni, Fariba Ardalani, Mojgan Babanejad, Khadijeh Jalalvand, Hela Azaiez, Sepide Mirzaei, Holger Thiele, Zohreh Mehrjoo, Hasan Otukesh, Nooshin Nikzat, Richard J.H. Smith, Fatemeh Keshavarzi, and Niloofar Bazazzadegan

Subjects

Novel gene, Hearing loss, medicine, Computational biology, Biology, medicine.symptom, Exome sequencing

Published

2021

19. Whole genome sequencing identifies a duplicated region encompassing Xq13.2q13.3 in a large Iranian family with intellectual disability

Author

Hans-Hilger Ropers, Sepideh Mehvari, Zohreh Fattahi, Maryam Beheshtian, Daniel Auld, Hossein Najmabadi, Yasser Riazalhosseini, Kimia Kahrizi, Farzaneh Larti, Vera M. Kalscheuer, Sanaz Arzhangi, Seyedeh Sedigheh Abedini, and Hao Hu

Subjects

0301 basic medicine, Male, Monocarboxylic Acid Transporters, Candidate gene, lcsh:QH426-470, Ubiquitin-Protein Ligases, Nerve Tissue Proteins, 030105 genetics & heredity, Biology, Short stature, Clinical Reports, 03 medical and health sciences, Genetic linkage, Intellectual disability, Gene duplication, Chromosome Duplication, Genetics, medicine, Humans, Copy-number variation, Genetic Testing, Molecular Biology, Genetics (clinical), X chromosome, Whole genome sequencing, Chromosomes, Human, X, whole genome sequencing, Clinical Report, Symporters, Xq13.2q13.3, Genetic Diseases, X-Linked, Xq duplication, medicine.disease, Pedigree, lcsh:Genetics, 030104 developmental biology, intellectual disability, medicine.symptom

Abstract

Background The X chromosome has historically been one of the most thoroughly investigated chromosomes regarding intellectual disability (ID), whose etiology is attributed to many factors including copy number variations (CNVs). Duplications of the long arm of the X chromosome have been reported in patients with ID, short stature, facial anomalies, and in many cases hypoplastic genitalia and/or behavioral abnormalities. Methods Here, we report on a large Iranian family with X‐linked ID caused by a duplication on the X chromosome identified by whole genome sequencing in combination with linkage analysis. Results Seven affected males in different branches of the family presented with ID, short stature, seizures, facial anomalies, behavioral abnormalities (aggressiveness, self‐injury, anxiety, impaired social interactions, and shyness), speech impairment, and micropenis. The duplication of the region Xq13.2q13.3, which is ~1.8 Mb in size, includes seven protein‐coding OMIM genes. Three of these genes, namely SLC16A2, RLIM, and NEXMIF, if impaired, can lead to syndromes presenting with ID. Of note, this duplicated region was located within a linkage interval with a LOD score >3. Conclusion Our report indicates that CNVs should be considered in multi‐affected families where no candidate gene defect has been identified in sequencing data analysis., We report a duplication on the X chromosome encompassing Xq13.2q13.3 in a large Iranian family with X‐linked intellectual disability. There are seven affected males in ones and twos within two generations of the pedigree who presented with a similar phenotype, including ID, short stature, seizures, facial anomalies, behavioral abnormalities, speech impairment, and micropenis.

Published

2020

20. Author response for 'Comprehensive genotype-phenotype correlation in AP-4 deficiency syndrome; Adding data from a large cohort of Iranian patients'

Author

Seyedeh Sedigheh Abedini, Vera M. Kalscheuer, Sanaz Arzhangi, Hossein Najmabadi, Zohreh Fattahi, Maryam Beheshtian, Reza Najafipour, Hao Hu, K. Kahrizi, Mahsa Fadaee, Hans-Hilger Ropers, Payman Jamali, Sepideh Mehvari, Tara Akhtarkhavari, and Marzieh Mohseni

Subjects

Oncology, Correlation, medicine.medical_specialty, Deficiency syndrome, business.industry, Internal medicine, medicine, business, Genotype phenotype, Large cohort

Published

2020

21. Comprehensive genotype-phenotype correlation in AP-4 deficiency syndrome; Adding data from a large cohort of Iranian patients

Author

Seyedeh Sedigheh Abedini, Zohreh Fattahi, Kimia Kahrizi, Maryam Beheshtian, Hossein Najmabadi, Marzieh Mohseni, Sepideh Mehvari, Payman Jamali, Tara Akhtarkhavari, Hans-Hilger Ropers, Vera M. Kalscheuer, Hao Hu, Sanaz Arzhangi, Mahsa Fadaee, and Reza Najafipour

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Microcephaly, Adolescent, Adaptor Protein Complex 4, Consanguinity, 030105 genetics & heredity, Iran, Quadriplegia, Corpus Callosum, Cohort Studies, 03 medical and health sciences, Internal medicine, Intellectual Disability, Intellectual disability, Genetics, medicine, Humans, Spasticity, Global developmental delay, Child, Spastic tetraplegia, Genetics (clinical), Genetic Association Studies, business.industry, Brain, medicine.disease, Phenotype, Pedigree, 030104 developmental biology, Child, Preschool, Mutation, Female, medicine.symptom, business, Ventriculomegaly

Abstract

Mutations in adaptor protein complex‐4 (AP‐4) genes have first been identified in 2009, causing a phenotype termed as AP‐4 deficiency syndrome. Since then several patients with overlapping phenotypes, comprised of intellectual disability (ID) and spastic tetraplegia have been reported. To delineate the genotype‐phenotype correlation of the AP‐4 deficiency syndrome, we add the data from 30 affected individuals from 12 out of 640 Iranian families with ID in whom we detected disease‐causing variants in AP‐4 complex subunits, using next‐generation sequencing. Furthermore, by comparing genotype‐phenotype findings of those affected individuals with previously reported patients, we further refine the genotype‐phenotype correlation in this syndrome. The most frequent reported clinical findings in the 101 cases consist of ID and/or global developmental delay (97%), speech disorders (92.1%), inability to walk (90.1%), spasticity (77.2%), and microcephaly (75.2%). Spastic tetraplegia has been reported in 72.3% of the investigated patients. The major brain imaging findings are abnormal corpus callosum morphology (63.4%) followed by ventriculomegaly (44.5%). Our result might suggest the AP‐4 deficiency syndrome as a major differential diagnostic for unknown hereditary neurodegenerative disorders.

Published

2020

22. Effect of inbreeding on intellectual disability revisited by trio sequencing

Author

Payman Jamali, Zhila Ghaderi, Hans-Hilger Ropers, Haleh Habibi, Fatemeh Pourfatemi, Farahnaz Sabbagh Kermani, Zohreh Mehrjoo, Kimia Kahrizi, Farnaz Sadeghinia, Hao Hu, Vera M. Kalscheuer, Bettina Lipkowitz, Reza Najafipour, Sanaz Arzhangi, Maryam Rahimi, Pooneh Nikuei, Atefeh Khoshaeen, Marzieh Mohseni, Masoumeh Hosseini, Hossein Najmabadi, Vanessa Suckow, Milad Falahat Chian, Faezeh Mojahedi, Sepideh Mehvari, Zohreh Fattahi, Maryam Beheshtian, Roshanak Jazayeri, Mohammad-Reza Khodaie-Ardakani, S. Hassan Tonekaboni, Tara Akhtarkhavari, and Thomas F. Wienker

Subjects

Male, 0301 basic medicine, Genes, Recessive, Iran, 030105 genetics & heredity, Biology, Carrier testing, Consanguinity, Middle East, 03 medical and health sciences, Intellectual Disability, Exome Sequencing, Intellectual disability, Genetics, medicine, Humans, Exome, Family, Inbreeding, Genetics (clinical), De novo mutations, Exome sequencing, High rate, Homozygote, Disease gene identification, medicine.disease, Pedigree, 030104 developmental biology, Parental consanguinity, Mutation, Female

Abstract

In outbred Western populations, most individuals with intellectual disability (ID) are sporadic cases, dominant de novo mutations (DNM) are frequent, and autosomal recessive ID (ARID) is very rare. Due to the high rate of parental consanguinity which raises the risk for ARID and other recessive disorders, the prevalence of ID is significantly higher in Near- and Middle-East countries. Indeed, homozygosity mapping and sequencing in consanguineous families have already identified a plethora of ARID genes, but due to the design of these studies, DNMs could not be systematically assessed, and the proportion of cases that are potentially preventable by avoiding consanguineous marriages or through carrier testing is hitherto unknown. This prompted us to perform whole exome sequencing in 100 sporadic ID patients from Iran and their healthy consanguineous parents. In 61 patients, we identified apparently causative changes in known ID genes. Of these, 44 were homozygous recessive and 17 dominant de novo mutations. Assuming that the DNM rate is stable, these results suggest that parental consanguinity raises the ID risk about 3.6-fold, and about 4.1-4.25-fold for children of first-cousin unions. These results do not rhyme with recent opinions that consanguinity-related health risks are generally small and have been 'overstated' in the past. This article is protected by copyright. All rights reserved.

Published

2018

23. SLC52A2 mutations cause SCABD2 phenotype: A second report

Author

Hakimeh Azarafra, Marzieh Mohseni, Omid Ali Adeli, Kimia Kahrizi, Maryam Beheshtian, Farnaz Sadeghnia, Nooshin Nikzat, Mojgan Babanejad, and Hossein Najmabadi

Subjects

Adult, Male, 0301 basic medicine, Ataxia, Adolescent, Mutation, Missense, Iran, 030105 genetics & heredity, Receptors, G-Protein-Coupled, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Atrophy, Exome Sequencing, medicine, Humans, Spinocerebellar Ataxias, Missense mutation, Young adult, Child, Hearing Loss, Gene, Genetic Association Studies, Exome sequencing, Genetics, business.industry, General Medicine, medicine.disease, Phenotype, Pedigree, Otorhinolaryngology, Pediatrics, Perinatology and Child Health, Spinocerebellar ataxia, Female, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Introduction Autosomal recessive cerebellar ataxias (ARCAs) are a large group of neurodegenerative disorders that manifest mainly in children and young adults. Most ARCAs are heterogeneous with respect to age at onset, severity of disease progression, and frequency of extracerebellar and systemic signs. Methods The phenotype of a consanguineous Iranian family was characterized using clinical testing and pedigree analysis. Whole-exome sequencing was used to identify the disease-causing gene in this family. Results and conclusion Using whole exome sequencing (WES), a novel missense mutation in SLC52A2 gene is reported in a consanguineous Iranian family with progressive severe hearing loss, optic atrophy and ataxia. This is the second report of the genotype-phenotype correlation between this syndrome named spinocerebellar ataxia with blindness and deafness type 2 (SCABD2) and SLC52A2 gene.

Published

2018

24. Author response for 'Identification of disease causing variants in the EXOSC gene family underlying autosomal recessive intellectual disability in Iranian families'

Author

Raheleh Vazehan, Hans-Hilger Ropers, Elham Parsimehr, Zahra Kalhor, Seyedeh Sedighe Abedini, Mahboubeh Kamgar, Faezeh Mojahedi, K. Kahrizi, Ariana Kariminejad, Farahnaz Sabbagh Kermani, Mahsa Fadaee, Zohreh Fattahi, Vera M. Kalscheuer, Mehrshid Faraji Zonooz, Maryam Beheshtian, Sanaz Arzhangi, Shokouh Sadat Mahdavi, Payman Jamali, and Hossein Najmabadi

Subjects

Genetics, Intellectual disability, medicine, Gene family, Identification (biology), Disease, Biology, medicine.disease

Published

2019

25. Iranome: A catalog of genomic variations in the Iranian population

Author

Mohammad Shekari, Peyman Jamali, Akbar Mohammadzadeh, Kimia Kahrizi, Behzad Davarnia, Bernd Timmermann, Hamid Reza Khorram Khorshid, Marzieh Mohseni, Erin Sellars, Morteza Oladnabi, Reza Najafipour, Khadijeh Jalalvand, Sayyed Hossein Nezhadi, Ali Akbar Haghdoost, Hossein Poustchi, Zahra Mohammadi, Hossein Najmabadi, Elham Zohrehvand, Azim Nejatizadeh, Pooneh Nikuei, Amir Amini, Sanaz Arzhangi, Mohammad R. Akbari, Maryam Bagherzadeh, Zohreh Fattahi, Reza Malekzadeh, Maryam Beheshtian, Stefan T. Börno, and Ehsan Shamsi-Gooshki

Subjects

Genotype, Population, Ethnic group, Biology, Iran, Web Browser, Iranian population, 03 medical and health sciences, Middle East, Databases, Genetic, Genetics, Ethnicity, Humans, education, Genetics (clinical), Exome sequencing, 030304 developmental biology, 0303 health sciences, education.field_of_study, Geography, Genome, Human, 030305 genetics & heredity, Computational Biology, Genetic Variation, Molecular Sequence Annotation, Genome project, Genomics, Variome, Genetics, Population, Evolutionary biology, Human genome

Abstract

Considering the application of human genome variation databases in precision medicine, population-specific genome projects are continuously being developed. However, the Middle Eastern population is underrepresented in current databases. Accordingly, we established Iranome database (www.iranome.com) by performing whole exome sequencing on 800 individuals from eight major Iranian ethnic groups representing the second largest population of Middle East. We identified 1,575,702 variants of which 308,311 were novel (19.6%). Also, by presenting higher frequency for 37,384 novel or known rare variants, Iranome database can improve the power of molecular diagnosis. Moreover, attainable clinical information makes this database a good resource for classifying pathogenicity of rare variants. Principal components analysis indicated that, apart from Iranian-Baluchs, Iranian-Turkmen, and Iranian-Persian Gulf Islanders, who form their own clusters, rest of the population were genetically linked, forming a super-population. Furthermore, only 0.6% of novel variants showed counterparts in "Greater Middle East Variome Project", emphasizing the value of Iranome at national level by releasing a comprehensive catalog of Iranian genomic variations and also filling another gap in the catalog of human genome variations at international level. We introduce Iranome as a resource which may also be applicable in other countries located in neighboring regions historically called Greater Iran (Persia).

Published

2019

26. Contribution of Iran in Elucidating the Genetic Causes of Autosomal Recessive Intellectual Disability

Author

Reza, Ataei, Shahrouz, Khoshbakht, Maryam, Beheshtian, Seyedeh Sedigheh, Abedini, Hanieh, Behravan, Saeed, Esmaeili Dizghandi, Fatemeh, Godratpour, Sepide, Mirzaei, Fatemeh, Bahrami, Mojdeh, Akbari, Fatemeh, Keshavarzi, Kimia, Kahrizi, and Hossein, Najmabadi

Subjects

Consanguinity, Intellectual Disability, Mutation, High-Throughput Nucleotide Sequencing, Humans, Exome, Family, Genes, Recessive, Iran, Pedigree

Abstract

Many genes with different inheritance modes contribute to the pathogenicity of intellectual disability (ID) making it the most known genetically heterogeneous disorder. Advanced next-generation sequencing (NGS) technologies have helped researchers identify genes underlying ID at an exponential pace. As a consanguineous country, Iran is a hotspot for discovering novel autosomal recessive intellectual disability (ARID) genes. Here, we aimed to review and compare reported ARID gene discovery both in Iran and globally, and pinpoint the research areas that need to be developed in future. We studied published articles and reviews on all known ID genes. In parallel, the gene-discovery research carried out on the Iranian population were also reviewed to determine the contribution of Iran to identifying novel ID genes. Also we tried to find supporting evidence on the causative role of novel genes identified in Iran including confirmatory functional studies and existence of more affected families. We also briefly reviewed the current therapeutic approaches under development for a subset of eligible ID cases. In total, 8% of all ID and 11.5% of all ARID genes described so far have been identified via studies on Iranian population. Functional studies have been performed on 29% of the genes identified in Iran. More than one affected family has been reported for many of these genes, supporting their causative role in ID pathogenesis. Despite the notable contribution of Iran in gene-discovery research, further functional studies on the identified genes are required.

Published

2019

27. Identification of disease-causing variants in the EXOSC gene family underlying autosomal recessive intellectual disability in Iranian families

Author

Shokouh Sadat Mahdavi, Ariana Kariminejad, Hossein Najmabadi, Raheleh Vazehan, Kimia Kahrizi, Payman Jamali, Seyedeh Sedigheh Abedini, Faezeh Mojahedi, Mehrshid Faraji Zonooz, Hans-Hilger Ropers, Vera M. Kalscheuer, Sanaz Arzhangi, Mahsa Fadaee, Zohreh Fattahi, Maryam Beheshtian, Zahra Kalhor, Mahboubeh Kamgar, Farahnaz Sabbagh Kermani, and Elham Parsimehr

Subjects

0301 basic medicine, Male, Genes, Recessive, Disease, 030105 genetics & heredity, Biology, Iran, Cohort Studies, 03 medical and health sciences, Consanguinity, Intellectual Disability, Clinical information, Intellectual disability, Exome Sequencing, Genetics, medicine, Gene family, Humans, Family, Child, Genetics (clinical), Rna processing, Exosome Multienzyme Ribonuclease Complex, fungi, Infant, medicine.disease, Phenotype, humanities, Pedigree, 030104 developmental biology, Child, Preschool, Mutation, Neurodevelopmental delay, Identification (biology), Female, geographic locations

Abstract

Neurodevelopmental delay and intellectual disability (ID) can arise from numerous genetic defects. To date, variants in the EXOSC gene family have been associated with such disorders. Using next-generation sequencing (NGS), known and novel variants in this gene family causing autosomal recessive ID (ARID) have been identified in five Iranian families. By collecting clinical information on these families and comparing their phenotypes with previously reported patients, we further describe the clinical variability of ARID resulting from alterations in the EXOSC gene family, and emphasize the role of RNA processing dysregulation in ARID.

Published

2019

28. Genetics of intellectual disability in consanguineous families

Author

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

Subjects

Adult, Male, 0301 basic medicine, Medizin, Genes, Recessive, Consanguinity, Iran, Biology, DNA sequencing, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Intellectual Disability, Exome Sequencing, Intellectual disability, medicine, Humans, Exome, Family, Protein Interaction Maps, Molecular Biology, Gene, De novo mutations, Affected offspring, Whole genome sequencing, Genetics, Whole Genome Sequencing, Homozygote, High-Throughput Nucleotide Sequencing, Middle Aged, medicine.disease, Pedigree, Psychiatry and Mental health, 030104 developmental biology, Mutation, Female, 030217 neurology & neurosurgery

Abstract

Autosomal recessive (AR) gene defects are the leading genetic cause of intellectual disability (ID) in countries with frequent parental consanguinity, which account for about 1/7th of the world population. Yet, compared to autosomal dominant de novo mutations, which are the predominant cause of ID in Western countries, the identification of AR-ID genes has lagged behind. Here, we report on whole exome and whole genome sequencing in 404 consanguineous predominantly Iranian families with two or more affected offspring. In 219 of these, we found likely causative variants, involving 77 known and 77 novel AR-ID (candidate) genes, 21 X-linked genes, as well as 9 genes previously implicated in diseases other than ID. This study, the largest of its kind published to date, illustrates that high-throughput DNA sequencing in consanguineous families is a superior strategy for elucidating the thousands of hitherto unknown gene defects underlying AR-ID, and it sheds light on their prevalence.

Published

2019

29. Prevalence of common MEFV mutations and carrier frequencies in a large cohort of Iranian populations

Author

Christian Oberkanins, Nasim Izadi, Maryam Beheshtian, Stefan Németh, Maryam Rostami, Elham Parsi Mehr, Hossein Najmabadi, Gernot Kriegshäuser, Mona Montajabiniat, Maryam Azad, Ariana Kariminejad, Masoumeh Hosseini, and Kimia Kahrizi

Subjects

Adult, Male, 0301 basic medicine, Heterozygote, Adolescent, DNA Mutational Analysis, Gene Expression, Familial Mediterranean fever, Disease, Iran, Biology, Asymptomatic, Cohort Studies, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Gene Frequency, Ethnicity, Prevalence, Genetics, medicine, Humans, Genetic Predisposition to Disease, Allele, Child, Allele frequency, Alleles, Aged, 030203 arthritis & rheumatology, Sanger sequencing, Infant, Exons, Middle Aged, Pyrin, medicine.disease, MEFV, Familial Mediterranean Fever, Phenotype, 030104 developmental biology, Child, Preschool, Mutation, Cohort, symbols, Female, medicine.symptom

Abstract

Familial Mediterranean fever (FMF) is a hereditary autoinflammatory disorder caused by mutations in the MEFV gene. The disease is especially common among Armenian, Turkish, Jewish and Middle East Arab populations. To identify the frequency and the spectrum of common MEFV mutations in different Iranian populations, we investigated a cohort of 208 unselected asymptomatic individuals and 743 FMF patients. Nine hundred and fifty-one samples were analysed for the presence of 12 MEFV mutations by PCR and reverse-hybridization (FMF StripAssay, ViennaLab, Vienna, Austria). Confirmatory dideoxy sequencing of all MEFV gene exons was performed for 39 patients. Fifty-seven (27.4%) healthy individual carried mutant MEFV alleles. Three hundred and ninety-one (52.6%) FMF patients were found positive for either one (172/743; 23.1%), two or three MEFV mutations. Using dideoxy sequencing, three novel variants, A66P, R202W and H300Q, could be identified. Our analysis revealed an allele frequency and carrier rate of 15.6 and 27.4%, respectively, among healthy Iranians. Still moderate compared to neighbouring Armenia, but higher than in Turkey or Iraq, these data suggest that FMF is remarkably common among Iranian populations. E148Q was most frequent in the group of healthy individuals, whereas M694V was the most common mutation among FMF patients, thereby corroborating previous studies on MEFV mutational spectra in the Middle East. Accordingly, MEFV mutations are frequent in healthy Iranian individuals across different ethnic groups. Based on this finding, the awareness for FMF and the implementation of augmented carrier screening programmes considering the multiethnic nature of the Iranian population should be promoted.

Published

2016

30. Improved diagnostic yield of neuromuscular disorders applying clinical exome sequencing in patients arising from a consanguineous population

Author

Mahsa Fadaee, Gholamreza Zamani, Hossein Najmabadi, Elham Parsimehr, Ayda Abolhassani, Mohammad R. Akbari, Kimia Kahrizi, Zahra Kalhor, Ariana Kariminejad, Shahriar Nafissi, Zohreh Fattahi, Maryam Beheshtian, Raheleh Vazehan, and Yalda Nilipour

Subjects

Male, 0301 basic medicine, Population, Consanguinity, Bioinformatics, LMNA, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, Exome, Family, Genetic Testing, education, Genetics (clinical), Exome sequencing, SGCA, Genetic testing, education.field_of_study, Massive parallel sequencing, medicine.diagnostic_test, business.industry, High-Throughput Nucleotide Sequencing, Neuromuscular Diseases, Pedigree, Biotechnology, Phenotype, 030104 developmental biology, Female, business, 030217 neurology & neurosurgery

Abstract

Neuromuscular diseases (NMDs) include a broad range of disorders affecting muscles, nerves and neuromuscular junctions. Their overlapping phenotypes and heterogeneous genetic nature have created challenges in diagnosis which calls for the implementation of massive parallel sequencing as a candidate strategy to increase the diagnostic yield. In this study, total of 45 patients, mostly offspring of consanguineous marriages were examined using whole exome sequencing. Data analysis was performed to identify the most probable pathogenic rare variants in known NMD genes which led to identification of causal variants for 33 out of 45 patients (73.3%) in the following known genes: CAPN3, Col6A1, Col6A3, DMD, DYSF, FHL1, GJB1, ISPD, LAMA2, LMNA, PLEC1, RYR1, SGCA, SGCB, SYNE1, TNNT1 and 22 novel pathogenic variants were detected. Today, the advantage of whole exome sequencing in clinical diagnostic strategies of heterogeneous disorders is clear. In this cohort, a diagnostic yield of 73.3% was achieved which is quite high compared to the overall reported diagnostic yield of 25% to 50%. This could be explained by the consanguineous background of these patients and is another strong advantage of offering clinical exome sequencing in diagnostic laboratories, especially in populations with high rate of consanguinity.

Published

2016

31. Autosomal recessive mutations inTHOC6cause intellectual disability: syndrome delineation requiring forward and reverse phenotyping

Author

Jean-Baptiste Rivière, Wendy Alcaraz, Sha Tang, Zohreh Fattahi, Maryam Beheshtian, A. Kariminedjad, Laurence Faivre, A.M. Innes, Hossein Najmabadi, Robert Roger Lebel, Katherine L. Helbig, Julien Thevenon, Seyed Hassan Tonekaboni, Chandree L. Beaulieu, Alice Masurel-Paulet, J.S. Amos, Lijia Huang, and Kym M. Boycott

Subjects

0301 basic medicine, Genetics, education.field_of_study, Microcephaly, business.industry, Population, Transcription export complex, 030105 genetics & heredity, Compound heterozygosity, medicine.disease, 03 medical and health sciences, 030104 developmental biology, Intellectual disability, Medicine, Missense mutation, business, education, Exome, Genetics (clinical), Exome sequencing

Abstract

THOC6 is a part of the THO complex, which is involved in coordinating mRNA processing with export. The THO complex interacts with additional components to form the larger TREX complex (transcription export complex). Previously, a homozygous missense mutation in THOC6 in the Hutterite population was reported in association with syndromic intellectual disability. Using exome sequencing, we identified three unrelated patients with bi-allelic mutations in THOC6 associated with intellectual disability and additional clinical features. Two of the patients were compound heterozygous for a stop and a missense mutation, and the third was homozygous for a missense mutation; the missense mutations were predicted to be pathogenic by in silico analysis and modeling. Clinical features of the three newly identified patients and those previously reported are reviewed; intellectual disability is moderate to severe, and malformations are variable including renal and heart defects, cleft palate, microcephaly, and corpus callosum dysgenesis. Facial features are variable and include tall forehead, short upslanting palpebral fissures +/- deep set eyes, and a long nose with overhanging columella. These subtle facial features render the diagnosis difficult to make in isolation with certainty. Our results expand the mutational and clinical spectrum of this rare disease, confirm that THOC6 is an intellectual disability causing gene, while providing insight into the importance of the THO complex in neurodevelopment.

Published

2016

32. Author response for 'Effect of inbreeding on intellectual disability revisited by Trio sequencing'

Author

Mohammad-Reza Khodaie-Ardakani, Farahnaz Sabbagh Kermani, K. Kahrizi, Roshanak Jazayeri, Pooneh Nikuei, Payman Jamali, Masoumeh Hosseini, Faezeh Mojahedi, Tara Akhtarkhavari, Zhila Ghaderi, Sepideh Mehvari, Atefeh Khoshaeen, Zohreh Fattahi, Marzieh Mohseni, Maryam Beheshtian, Zohreh Mehrjoo, Haleh Habibi, Vera M. Kalscheuer, Hao Hu, Bettina Lipkowitz, Hossein Najmabadi, Sanaz Arzhangi, Fatemeh Pourfatemi, Thomas F. Wienker, Vanessa Suckow, Seyed Hassan Tonekaboni, Hans-Hilger Ropers, Farnaz Sadeghinia, Reza Najafipour, Maryam Rahimi, and Milad Falahat Chian

Subjects

Intellectual disability, medicine, Psychology, medicine.disease, Inbreeding, Genealogy

Published

2018

33. Social Determinants of Health and Health Equity: Islamic Republic of Iran’s Executive Actions and Monitoring System

Author

Maryam Beheshtian, Mohammadreza Zakeri, and Ardeshir Khosravi

Subjects

Expectancy theory, Government, Economic growth, 030505 public health, Monitoring system, General Medicine, Affect (psychology), Health indicator, Health equity, 03 medical and health sciences, 0302 clinical medicine, Nomination, 030212 general & internal medicine, Social determinants of health, Business, 0305 other medical science

Abstract

Background and Objectives: Increasing evidence leaves no doubt that significant disparity in health arises from uneven distribution of wealth across populations. Diverse patterns in pervasiveness of social factors eventually become manifest in heterogeneous face of disease prevalence, morbidity, and mortality rate within and between communities and remarkably affect expectancy of human life. Here, we presented the formulation and implementation of executive actions as well as a monitoring system for social determinants of health (SDH) initiated by the Ministry of Health and Medical Education (MOHME) since 2006. Methods: This was a descriptive review of various actions performed by MOHME on social elements to reduce health disparities. Results: Nomination of national think tank committee and sensitizing and mobilizing sectors other than health in all policies resulted in approval of 52 health indicators at the government level. Emphasis was placed on the collaborative efforts particularly on developing a monitoring system which could show the distance between achievements and goals and assure the effectiveness of implemented actions on reducing health inequities. Conclusions: We pictured the road which was paved by MOHME on social determinants of health (SDH) to facilitate the evaluation and formulation of the future actions to reduce health disparities in a more effective manner.

Published

2018

34. In Reply to 'Noncoding Ribonucleic Acid Studies of Lumbar Disk Disease: Decade Retrospect'

Author

Masih Sherafatian, Maryam Beheshtian, and Fariborz Ghaffarpasand

Subjects

Lumbar, business.industry, Medicine, RNA, Surgery, Neurology (clinical), Disease, business, Bioinformatics

Published

2019

35. Characterising the spectrum of autosomal recessive hereditary hearing loss in Iran

Author

Nooshin Nikzat, Kevin T. Booth, Richard J.H. Smith, Allen C. Simpson, Kimia Kahrizi, Maryam Beheshtian, Reza Mozafari, Fariba Ardalani, Mojgan Babanejad, Farahnaz Sabbagh, Kathy L. Frees, Nicole C. Meyer, Leila Jamali, Zohreh Mehrjoo, Niloofar Bazazzadegan, Sanaz Arzhangi, Hossein Khodaei, Christina M. Sloan-Heggen, Tara Akhtarkhavari, Maryam Taghdiri, Hela Azaiez, Mohammad Farhadi, Marzieh Mohseni, Hasan Otukesh, Seyed Morteza Seifati, Hossein Najmabadi, Saeideh Vaziri, and Ahmad Daneshi

Subjects

MYO15A, medicine.medical_specialty, Hearing loss, Genes, Recessive, Consanguinity, Iran, Biology, Connexins, Article, Gene Frequency, Molecular genetics, otorhinolaryngologic diseases, Genetics, medicine, Humans, Genetic Predisposition to Disease, Hearing Loss, Genetic Association Studies, Genetics (clinical), Massive parallel sequencing, Genetic heterogeneity, Founder Effect, Connexin 26, Medical genetics, medicine.symptom, Founder effect

Abstract

Background Countries with culturally accepted consanguinity provide a unique resource for the study of rare recessively inherited genetic diseases. Although hereditary hearing loss (HHL) is not uncommon, it is genetically heterogeneous, with over 85 genes causally implicated in non-syndromic hearing loss (NSHL). This heterogeneity makes many gene-specific types of NSHL exceedingly rare. We sought to define the spectrum of autosomal recessive HHL in Iran by investigating both common and rarely diagnosed deafness-causing genes. Design Using a custom targeted genomic enrichment (TGE) panel, we simultaneously interrogated all known genetic causes of NSHL in a cohort of 302 GJB2 -negative Iranian families. Results We established a genetic diagnosis for 67% of probands and their families, with over half of all diagnoses attributable to variants in five genes: SLC26A4 , MYO15A , MYO7A , CDH23 and PCDH15 . As a reflection of the power of consanguinity mapping, 26 genes were identified as causative for NSHL in the Iranian population for the first time. In total, 179 deafness-causing variants were identified in 40 genes in 201 probands, including 110 novel single nucleotide or small insertion–deletion variants and three novel CNV. Several variants represent founder mutations. Conclusion This study attests to the power of TGE and massively parallel sequencing as a diagnostic tool for the evaluation of hearing loss in Iran, and expands on our understanding of the genetics of HHL in this country. Families negative for variants in the genes represented on this panel represent an excellent cohort for novel gene discovery.

Published

2015

36. De novo Mutation in CACNA1S Gene in a 20-Year-Old Man Diagnosed with Metabolic Myopathy

Author

Masoud, Edizadeh, Raheleh, Vazehan, Fatemeh, Javadi, Shima, Dehdahsi, Mahsa, Fadaee, Mehrshid, Faraji Zonooz, Elham, Parsimehr, Fatemeh, Ahangari, Ayda, Abolhassani, Zahra, Kalhor, Zohreh, Fattahi, Maryam, Beheshtian, Ariana, Kariminejad, Mohammad Reza, Akbari, Hossein, Najmabadi, and Shahriar, Nafissi

Subjects

Male, Young Adult, Calcium Channels, L-Type, Muscular Diseases, DNA Mutational Analysis, Mutation, Exome Sequencing, Humans, Calcium Channels, Creatine Kinase

Abstract

The calcium channel, voltage-dependent, L-type, alpha 1S subunit (CACNA1S) gene encodes a skeletal Ca2+ channel which is involved in calcium-dependent processes such as muscle contraction and neurotransmitter release. Mutations in this gene have been accompanied by hypo- and normokalemic periodic paralysis, thyrotoxic periodic paralysis, and susceptibility to malignant hyperthermia. We report the clinical and genetic findings in a patient diagnosed with metabolic myopathy who had episodic attacks of muscle pain and weakness but with no family background of the disease. Next-generation sequencing (NGS) using a panel targeting metabolic myopathy and myotonia genes identified a de novo heterozygous pathogenic variant c.3724AG, p.Arg1242Gly, in exon 30 of CACNA1S. As the second report of this variant, this case may broaden the CACNA1S-related disease spectrum to include normokalemic periodic paralysis.

Published

2017

37. Distinct genetic variation and heterogeneity of the Iranian population

Author

Zahra Mohammadi, Zohreh Mehrjoo, Reza Najafipour, Shahrouz Khoshbakht, Mohammad R. Toliat, Marzieh Mohseni, Pooneh Nikuei, Akbar Mohammadzadeh, Kimia Kahrizi, Mohammad Haddadi, Fariba Ardalani, Zohreh Fattahi, M. Jafari, Khadijeh Jalalvand, Ali Akbar Haghdoost, Reza Malekzadeh, Peter Nürnberg, Lisa-Marie Niestroj, Maryam Beheshtian, Elham Zohrehvand, Hossein Najmabadi, Barbara Helwing, Yasmina Gossmann, Hossein Poustchi, Farid Najafi, Sanaz Arzhangi, Michael Nothnagel, Tara Akhtarkhavari, Ehsan Shamsi Gooshki, and Morteza Oladnabi

Subjects

Male, Cancer Research, Arabic People, Ethnic group, Social Sciences, Population genetics, Human genetic variation, Iran, QH426-470, Biochemistry, Geographical Locations, Consanguinity, 0302 clinical medicine, Ethnicity, Ethnicities, Psychology, Genetics (clinical), Language, 0303 health sciences, education.field_of_study, Ancient DNA, Paleogenetics, Middle Aged, Nucleic acids, Female, Research Article, Adult, Asia, Population, Genomics, Biology, 03 medical and health sciences, Genetic variation, Genetics, Humans, education, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Persian People, Aged, 030304 developmental biology, Evolutionary Biology, Population Biology, Genetic heterogeneity, Cognitive Psychology, Biology and Life Sciences, Paleontology, Genetic Variation, DNA, Genetics, Population, Evolutionary biology, People and Places, Earth Sciences, Cognitive Science, Population Groupings, Population Genetics, 030217 neurology & neurosurgery, Neuroscience, Genome-Wide Association Study

Abstract

Iran, despite its size, geographic location and past cultural influence, has largely been a blind spot for human population genetic studies. With only sparse genetic information on the Iranian population available, we pursued its genome-wide and geographic characterization based on 1021 samples from eleven ethnic groups. We show that Iranians, while close to neighboring populations, present distinct genetic variation consistent with long-standing genetic continuity, harbor high heterogeneity and different levels of consanguinity, fall apart into a cluster of similar groups and several admixed ones and have experienced numerous language adoption events in the past. Our findings render Iran an important source for human genetic variation in Western and Central Asia, will guide adequate study sampling and assist the interpretation of putative disease-implicated genetic variation. Given Iran’s internal genetic heterogeneity, future studies will have to consider ethnic affiliations and possible admixture., Author summary Based on genome-wide genotype data on over 1000 samples from eleven ethnic groups present in Iran and by comparison to reference data sets of both extant populations and ancient DNA samples, we show that the Iranian population comprises distinct genetic variation with respect to populations in close geographic proximity, a cluster of genetically largely overlapping ethnic groups as well as a number of strongly admixed groups. These observations, also corroborated by f3 migration statistics and other approaches, indicate genetic continuity of and limited influx into the cluster groups over several millennia, despite Iran’s geographic position at a crossroads in West Asia. They also suggest, correspondingly, several instances of language adoption instead of demic replacement in the past. Future human genetic studies, both with a focus on population and medical genetics, will have to consider differences in heterogeneity, consanguinity and degree of admixture between the ethnic groups for an adequate design and interpretation.

Published

2019

38. Heterogeneity of Hereditary Hearing Loss in Iran: a Comprehensive Review

Author

Maryam, Beheshtian, Mojgan, Babanejad, Hela, Azaiez, Niloofar, Bazazzadegan, Diana, Kolbe, Christina, Sloan-Heggen, Sanaz, Arzhangi, Kevin, Booth, Marzieh, Mohseni, Kathy, Frees, Mohammad Hossein, Azizi, Ahmad, Daneshi, Mohammad, Farhadi, Kimia, Kahrizi, Richard Jh, Smith, and Hossein, Najmabadi

Subjects

Hearing Loss, Sensorineural, Membrane Transport Proteins, Iran, Myosins, Connexins, Article, Connexin 26, Consanguinity, Sulfate Transporters, Myosin VIIa, Mutation, otorhinolaryngologic diseases, Humans, Genetic Testing, Delivery of Health Care

Abstract

A significant contribution to the causes of hereditary hearing impairment comes from genetic factors. More than 120 genes and 160 loci have been identified to be involved in hearing impairment. Given that consanguine populations are more vulnerable to most inherited diseases, such as hereditary hearing loss (HHL), the genetic picture of HHL among the Iranian population, which consists of at least eight ethnic subgroups with a high rate of intermarriage, is expected to be highly heterogeneous. Using an electronic literature review through various databases such as PubMed, MEDLINE, and Scopus, we review the current picture of HHL in Iran. In this review, we present more than 39 deafness genes reported to cause non-syndromic HHL in Iran, of which the most prevalent causative genes include GJB2, SLC26A4, MYO15A, and MYO7A. In addition, we highlight some of the more common genetic causes of syndromic HHL in Iran. These results are of importance for further investigation and elucidation of the molecular basis of HHL in Iran and also for developing a national diagnostic tool tailored to the Iranian context enabling early and efficient diagnosis of hereditary hearing impairment.

Published

2016

39. Novel CFTR Mutations in Two Iranian Families with Severe Cystic Fibrosis

Author

Marzieh, Mohseni, Mohammad, Razzaghmanesh, Elham, Parsi Mehr, Hanieh, Zare, Maryam, Beheshtian, and Hossein, Najmabadi

Subjects

Adult, Male, Base Sequence, Cystic Fibrosis, Full Length, Mutation, Missense, Sequence analysis, Cystic Fibrosis Transmembrane Conductance Regulator, Cystic fibrosis transmembrane conductance regulator protein, Sequence Analysis, DNA, Iran, Child, Preschool, Mutation, Humans, Female, Genetic Predisposition to Disease, Genetic Testing

Abstract

Background: Cystic fibrosis (CF) is a common autosomal recessive disorder that affects many body systems and is produced by mutations in the cystic fibrosis transmembrane conductance regulator (CFTR) gene. CF is also the most frequently inherited disorder in the West. The aim of this study was to detect the mutations in the CFTR gene in two Iranian families with CF. Methods: After DNA extraction using the salting out method, a mutation panel consisting of 35 common mutations was tested by PCR, followed by reverse hybridization Strip Assay. To confirm the mutations, we have also performed Sanger sequencing for all 27 exons, intronic flanking regions, and 5’ and 3’ UTRs of the CFTR gene. Results: Carrier testing in a spouse revealed a novel nonsense mutation in the CFTR gene (c.2777 T>A (p.L926X)) in exon 17 for husband and a previously described heterozygous splice site pathogenic mutation (c.1393-1G>A) in his wife. The other novel compound heterozygous missense mutation (c.3119 T>A (p.L1040H)), which was previously reported as nonsense c.3484C>T (p.R1162X) mutation, was found in exon 19 in patient screening. Conclusion: Two novel CFTR mutations in exons 17 and 19 are responsible for CF with severe phenotypes in two Iranian families. These two mutations supplement the mutation spectrum of CFTR and may contribute to a better understanding of CFTR protein function.

Published

2016

40. Impact of whole exome sequencing among Iranian patients with autosomal recessive retinitis pigmentosa

Author

Maryam, Beheshtian, Samira, Saee Rad, Mojgan, Babanejad, Marzieh, Mohseni, Hassan, Hashemi, Arash, Eshghabadi, Fedra, Hajizadeh, Mohammad Reza, Akbari, Kimia, Kahrizi, Mohammad, Riazi Esfahani, and Hossein, Najmabadi

Subjects

Adult, Male, Cyclic Nucleotide Phosphodiesterases, Type 6, Adolescent, DNA Mutational Analysis, Homozygote, Mutation, Missense, Membrane Proteins, Nerve Tissue Proteins, Iran, Middle Aged, Pedigree, Young Adult, Phenotype, Humans, ATP-Binding Cassette Transporters, Exome, Female, Eye Proteins, Retinitis Pigmentosa

Abstract

Non-syndromic autosomal recessive Retinitis Pigmentosa (arRP) is a highly heterogeneous genetic visual disorder with a large number of causative genes. We aimed to determine the power of Whole Exome Sequencing (WES) in the identification of the genes responsible for non-syndromic arRP among Iranian patients.We used WES, followed by the Sanger sequencing to identify the underlying gene mutations causing non-syndromic arRP.Our study revealed disease-causing mutations in known arRP genes for 10 of the 13 families studied (76.9%). These mutations included two-frameshift insertion/deletion in CRB1 and ABCA4, one splicing mutation in PDE6B, four missense mutations in RP1, CRB1, PANK2 and IFT140, as well as three stop codon mutations in RDH12, PRCD, and C2orf71. Three remaining families harbored no mutation in previously known RP genes. Of the 10 diseases causing mutations identified among the investigated Iranian patients with non-syndromic arRP, eight variants had not been reported previously. We confirmed segregation of all 10 mutations with disease phenotypes in our studied population.This study supports the genetic heterogeneity of non-syndromic arRP in Iranian patients, and provides an opportunity to show the effectiveness of WES in the identification of pathogenic mutations among patients with non-syndromic arRP born to consanguineous parents.

Published

2015

41. Report of limb girdle muscular dystrophy type 2a in 6 Iranian patients, one with a novel deletion in CAPN3 gene

Author

Hamed Reza Godarzi, Hossein Najmabadi, Kimia Kahrizi, Mohammad R. Akbari, Ariana Kariminejad, Raheleh Vazehan, Shahriar Nafissi, Zohreh Fattahi, Maryam Beheshtian, and Mahsa Fadaee

Subjects

0301 basic medicine, Adult, Male, Weakness, Adolescent, DNA Mutational Analysis, Muscle Proteins, Limb girdle, Biology, Iran, Genetic analysis, 03 medical and health sciences, Exon, Young Adult, 0302 clinical medicine, medicine, Humans, Family, Muscular dystrophy, Gene, Genetics (clinical), Exome sequencing, Sequence Deletion, Genetics, Base Sequence, Calpain, Exons, medicine.disease, Pedigree, 030104 developmental biology, medicine.anatomical_structure, Neurology, Muscular Dystrophies, Limb-Girdle, Pediatrics, Perinatology and Child Health, Shoulder girdle, Female, Neurology (clinical), medicine.symptom, 030217 neurology & neurosurgery

Abstract

Calpain3 is a calcium-dependent intracellular protease involved in an autosomal recessive form of muscular dystrophy known as limb-girdle muscular dystrophy type 2A. Many pathogenic mutations have been identified in calpain3, encoded by the CAPN3 gene, which leads to weakness of the pelvic and shoulder girdle muscles. In the present study, whole exome sequencing was performed on six unrelated Iranian families who presented with progressive muscle weakness, with a strong suspicion of Calpainopathies. Genetic analysis of CAPN3 gene revealed five causative variants which had not been reported in the Iranian population before including a novel 6 bp deletion (c.795_800delCATTGA) and four previously reported mutations (c.1939G > T, c.2243G > A, c.2257delGinsAA, and c.2380 + 2T > G). Our findings indicate that exome sequencing can be a very effective and affordable method to diagnose heterogeneous muscular dystrophies, especially in consanguineous populations such as Iran.

Published

2015

42. Iran's Multiple Indicator Demographic and Health Survey - 2010: Study Protocol

Author

Arash, Rashidian, Akram, Karimi-Shahanjarini, Ardeshir, Khosravi, Elham, Elahi, Maryam, Beheshtian, Elham, Shakibazadeh, Roghayeh, Khabiri, Mohammad, Arab, and Mohammad-Reza, Zakeri

Subjects

National survey, survey design, sampling, Original Article, quality assurance

Abstract

Background: There is an international emphasis on providing timely and high quality data to monitor progress of countries toward Millennium Development Goals. Iran's Multiple Indicator Demographic and Health Survey (IrMIDHS) aimed to provide valid information on population and health outcomes to monitor progress in achieving national priorities and health programs and to assist policy makers to design effective strategies for improving health outcomes and equity in access to care. Methods: A cross-sectional multi-stage stratified cluster-random survey is conducted through face-to-face household interviews. The sampling frame is developed using Iran's 2006 population and housing census. Provincial samples ranging are from a minimum of 400 households per province to 6400 households in Tehran province. Cluster size is 10 households. The target sample includes 3096 clusters: 2187 clusters in urban and 909 clusters in rural areas. IrMIDHS instruments include three questionnaires: Household questionnaire, women aged 15-54 questionnaire, children under five questionnaire, supervision and quality assessment checklists and data collection sheets and standard weight and height measurement tools for under-five children. A cascading decentralized training method is used for training data collection and supervision teams. Quality assurance procedures are defined for the five steps of conducting the survey including: Sampling, training data collection and training teams, survey implementation, data entry and analysis. A multi-layer supervision and monitoring procedure is established. All the questionnaires are double entered. Conclusions: IrMIDHS will provide valuable data for policymakers in Iran. Designing and implementation of the study involve contributions from academics as well as program managers and policy makers. The collaborative nature of the study may facilitate better usage of its results.

Published

2013

43. Brief Report of Variants Detected in Hereditary Hearing Loss Cases in Iran over a 3-Year Period

Author

Shima Dehdahsi, Ayda Abolhassani, Raheleh Vazehan, Mehrshid Faraji Zonooz, Zohreh Fattahi, Maryam Beheshtian, Shokouh Sadat Mahdavi, Hossein Najmabadi, Mahsa Fadaee, Payman Jamali, Elham Parsimehr, Richard J.H. Smith, Younes Nourizadeh, Ariana Kariminejad, Fatemeh Ahangari, Farshide Samiee, Zahra Kalhor, Niloofar Bazazzadegan, and Haleh Habibi

Subjects

High rate, Genetics, Massive parallel sequencing, medicine.diagnostic_test, MYO7A, Hearing loss, business.industry, Short Communication, lcsh:Public aspects of medicine, Public Health, Environmental and Occupational Health, lcsh:RA1-1270, Consanguinity, Novel variant, OtoSCOPE, Hereditary hearing loss, CDH23, Known variant, medicine, otorhinolaryngologic diseases, medicine.symptom, business, Heterogeneous disorder, Genetic testing

Abstract

Background: Diagnosis of hereditary hearing loss (HHL) as a heterogeneous disorder is very important especially in countries with high rates of consanguinity where the autosomal recessive pattern of inheritance is prevalent. Techniques such as next-generation sequencing, a comprehensive genetic test using targeted genomic enrichment and massively parallel sequencing (TGE + MPS), have made the diagnosis more cost-effective. The aim of this study was to determine HHL variants with comprehensive genetic testing in our country. of this study was to determine HHL variants with comprehensive genetic testing in our country. Methods: Fifty GJB2 negative individuals with HHL were referred to the Kariminejad-Najmabadi Pathology and Genetics Center, Tehran, one of the reference diagnostic genetic laboratories in Iran, during a 3-year period between 2014 and 2017. They were screened with the OtoSCOPE test, the targeted genomic enrichment and massively parallel sequencing (TGE + MPS) platform after a detailed history had been taken along with clinical evaluation. Results: Among 32 out of 50 GJB2 negative patients (64%), 34 known pathogenic and novel variants were detected of which 16 (47%) were novel, identified in 10 genes of which the most prevalent were CDH23, MYO7A and MYO15A. Conclusion: These results provide a foundation from which to make appropriate recommendations for the use of comprehensive genetic testing in the evaluation of Iranian patients with hereditary hearing loss.