Your search keyword '"Riazuddin"' showing total 43 results

1. Investigating the Molecular Basis of Retinal Degeneration in a Familial Cohort of Pakistani Decent by Exome Sequencing.

Author

Maranhao, Bruno, Biswas, Pooja, Gottsch, Alexander DH, Navani, Mili, Naeem, Muhammad Asif, Suk, John, Chu, Justin, Khan, Sheen N, Poleman, Rachel, Akram, Javed, Riazuddin, Sheikh, Lee, Pauline, Riazuddin, S Amer, Hejtmancik, J Fielding, and Ayyagari, Radha

Subjects

Fundus Oculi, Humans, Retinal Degeneration, Eye Proteins, RNA, Messenger, Electroretinography, Pedigree, Sequence Alignment, Sequence Analysis, RNA, Age of Onset, Consanguinity, Genotype, Genes, Recessive, Phenotype, Mutation, Polymorphism, Single Nucleotide, Ethnic Groups, Pakistan, Female, Male, Genetic Association Studies, Exome, RNA, Messenger, Sequence Analysis, Genes, Recessive, Polymorphism, Single Nucleotide, General Science & Technology

Abstract

PurposeTo define the molecular basis of retinal degeneration in consanguineous Pakistani pedigrees with early onset retinal degeneration.MethodsA cohort of 277 individuals representing 26 pedigrees from the Punjab province of Pakistan was analyzed. Exomes were captured with commercial kits and sequenced on an Illumina HiSeq 2500. Candidate variants were identified using standard tools and analyzed using exomeSuite to detect all potentially pathogenic changes in genes implicated in retinal degeneration. Segregation analysis was performed by dideoxy sequencing and novel variants were additionally investigated for their presence in ethnicity-matched controls.ResultsWe identified a total of nine causal mutations, including six novel variants in RPE65, LCA5, USH2A, CNGB1, FAM161A, CERKL and GUCY2D as the underlying cause of inherited retinal degenerations in 13 of 26 pedigrees. In addition to the causal variants, a total of 200 variants each observed in five or more unrelated pedigrees investigated in this study that were absent from the dbSNP, HapMap, 1000 Genomes, NHLBI ESP6500, and ExAC databases were identified, suggesting that they are common in, and unique to the Pakistani population.ConclusionsWe identified causal mutations associated with retinal degeneration in nearly half of the pedigrees investigated in this study through next generation whole exome sequencing. All novel variants detected in this study through exome sequencing have been cataloged providing a reference database of variants common in, and unique to the Pakistani population.

Published

2015

2. Knowledge, attitudes, practices, and its associated factors toward COVID-19 pandemic among Bangladeshi older adults.

Author

Deepa Roy, Suvasish Das Shuvo, Md Sakhawot Hossain, Md Riazuddin, Sanaullah Mazumdar, Bappa Kumar Mondal, and Md Ashrafuzzaman Zahid

Subjects

Medicine, Science

Abstract

BackgroundThe newly emerged COVID-19 has an unprecedented impact on all classes of people, particularly the elderly. The knowledge, attitudes, and practices (KAP) of older adults toward COVID-19 are currently unknown. This study aimed to investigate the KAP and its associated factors toward COVID-19 among older adults in Bangladesh.MethodsA cross-sectional survey was conducted from April to May 2021 among Bangladeshi older adults. Face-to-face interviews were used to collect data from five selected divisions in Bangladesh using simple random sampling. The questionnaire consisted of socio-demographic characteristics, disease conditions, and KAP toward COVID-19. Descriptive statistics, t-tests, one-way analysis of variance (ANOVA), and logistic regression analyses were performed.ResultsOut of 900 respondents, the majority of older adults (82.9%) indicated that COVID-19 is a viral disease and the major clinical symptom of COVID-19 (86.5%). Only 22.1% of participants always washed their hands with soap or hand sanitizer, and 27.6% wore a mask to protect against the virus when going outside the home. Overall, 55.2% had adequate knowledge, 50.2% had positive attitudes toward COVID-19 and only 22.7% had good practices. Out of 30 scores, mean score values were 20.8±6.7 in the knowledge section, 21.2±4.3 in the attitude section, and 11.3±6.7 in the practice section out of 30. In binary logistic regression analysis, factors associated with poor knowledge, and practices were being male, aged >70 years, having a primary education, less income ConclusionThe findings highlight the need for immediate implementation of health education programs and adequate intervention programs for COVID-19 which integrates consideration of associated factors to improve the level of older adults' knowledge, attitudes, and practices.

Published

2022

3. Knowledge, attitudes, practices, and its associated factors toward COVID-19 pandemic among Bangladeshi older adults

Author

Roy, Deepa, primary, Shuvo, Suvasish Das, additional, Hossain, Md. Sakhawot, additional, Riazuddin, Md., additional, Mazumdar, Sanaullah, additional, Mondal, Bappa Kumar, additional, and Zahid, Md. Ashrafuzzaman, additional

Published

2022

4. Factors influencing low-income households’ food insecurity in Bangladesh during the COVID-19 lockdown

Author

Shuvo, Suvasish Das, primary, Hossain, Md. Sakhawot, additional, Riazuddin, Md., additional, Mazumdar, Sanaullah, additional, and Roy, Deepa, additional

Published

2022

5. Factors influencing low-income households' food insecurity in Bangladesh during the COVID-19 lockdown

Author

Suvasish Das Shuvo, Md. Sakhawot Hossain, Md. Riazuddin, Sanaullah Mazumdar, and Deepa Roy

Subjects

Adult, Bangladesh, Food Insecurity, Multidisciplinary, Cross-Sectional Studies, Socioeconomic Factors, Communicable Disease Control, COVID-19, Humans, Middle Aged, Pandemics, Food Supply

Abstract

Background The COVID-19 pandemic and countrywide lockdown could negatively impact household food insecurity among low-income households. This study aimed to investigate the prevalence of household food insecurity and its influencing factors among low-income people in Bangladesh during the lockdown of COVID-19. Methods This cross-sectional study was conducted through face-to-face interviews from 500 low-income households during the countrywide COVID-19 lockdown. A pretested, structured and validated questionnaire was used to collect socioeconomic characteristics, household income conditions, and food accessibility. Household Food Insecurity Access Scale (HFIAS) and Dietary Diversity Score (DDS) were used to measure food insecurity. Multinomial logistic regression models were estimated to evaluate and predict risk factors that influence food insecurity. Results The study found that above 67% of households was mild-to-moderate food insecure while 23% experienced severe food insecurity. Significantly, 88%, 97.4%, and 93.4% of the households had anxiety and uncertainty, inadequate quality, and inadequate quantity of food, respectively. The regression analysis revealed the age 36–50 years (RRR: 4.86; 95% CI: 2.31–7.44, RRR: 4.16; 95% CI: 2.25–6.10) and monthly income Conclusion This study found that households become more susceptible to food insecurity during the COVID-19 pandemic and lockdown period. Based on the findings, we suggest some essential food policies and adequate food assistance to mitigate these negative consequences.

Published

2021

6. Autosomal recessive congenital cataracts linked to HSF4 in a consanguineous Pakistani family

Author

Jiao, Xiaodong, primary, Khan, Shahid Y., additional, Kaul, Haiba, additional, Butt, Tariq, additional, Naeem, Muhammad Asif, additional, Riazuddin, Sheikh, additional, Hejtmancik, J. Fielding, additional, and Riazuddin, S. Amer, additional

Published

2019

7. Autosomal recessive congenital cataracts linked to HSF4 in a consanguineous Pakistani family

Author

Xiaodong Jiao, Shahid Y. Khan, S. Amer Riazuddin, J. Fielding Hejtmancik, Sheikh Riazuddin, Muhammad Asif Naeem, Haiba Kaul, and Tariq M. Butt

Subjects

Male, Genetic Linkage, Gene Expression, Artificial Gene Amplification and Extension, Polymerase Chain Reaction, Biochemistry, Consanguinity, Mice, 0302 clinical medicine, Heat Shock Transcription Factors, Mutant protein, Medicine and Health Sciences, Missense mutation, Pakistan, Sanger sequencing, Genetics, 0303 health sciences, Eye Lens, Multidisciplinary, Pedigree, Congenital cataracts, symbols, Medicine, Female, Anatomy, Genetic Dominance, Research Article, Substitution Mutation, Missense Mutation, Science, Ocular Anatomy, Mutation, Missense, Genes, Recessive, Biology, Research and Analysis Methods, Cataract, 03 medical and health sciences, symbols.namesake, Cataracts, Ocular System, Genetic linkage, Lens, Crystalline, DNA-binding proteins, medicine, Animals, Humans, Gene Regulation, Allele, Molecular Biology Techniques, Molecular Biology, Alleles, Recessive Traits, 030304 developmental biology, Autosomal Recessive Traits, Biology and Life Sciences, Proteins, medicine.disease, eye diseases, Regulatory Proteins, Ophthalmology, Genetic Loci, Lens Disorders, Mutation, 030221 ophthalmology & optometry, Lod Score, Microsatellite Repeats, Transcription Factors

Abstract

PurposeTo investigate the genetic basis of autosomal recessive congenital cataracts (arCC) in a large consanguineous Pakistani family.MethodsAll participating members of family, PKCC074 underwent an ophthalmic examination. Slit-lamp photographs were ascertained for affected individuals that have not been operated for the removal of the cataractous lens. A small aliquot of the blood sample was collected from all participating individuals and genomic DNAs were extracted. A genome-wide scan was performed with polymorphic short tandem repeat (STR) markers and the logarithm of odds (LOD) scores were calculated. All coding exons and exon-intron boundaries of HSF4 were sequenced and expression of Hsf4 in mouse ocular lens was investigated. The C-terminal FLAG-tagged wild-type and mutant HSF4b constructs were prepared to examine the nuclear localization pattern of the mutant protein.ResultsThe ophthalmological examinations suggested that nuclear cataracts are present in affected individuals. Genome-wide linkage analyses localized the critical interval to a 10.95 cM (14.17 Mb) interval on chromosome 16q with a maximum two-point LOD score of 4.51 at θ = 0. Sanger sequencing identified a novel missense mutation: c.433G>C (p.Ala145Pro) that segregated with the disease phenotype in the family and was not present in ethnically matched controls. Real-time PCR analysis identified the expression of HSF4 in mouse lens as early as embryonic day 15 with a steady level of expression thereafter. The immunofluorescence tracking confirmed that both wild-type and mutant HSF4 (p.Ala145Pro) proteins localized to the nucleus.ConclusionHere, we report a novel missense mutation in HSF4 associated with arCC in a familial case of Pakistani descent.

Published

2019

8. Deletion at the GCNT2 Locus Causes Autosomal Recessive Congenital Cataracts

Author

S. Amer Riazuddin, Muhammad Naeem, Bushra Rauf, Sheikh Riazuddin, Muhammad Daud, Allen O. Eghrari, Shahid Y. Khan, Tayyab Husnain, Firoz Kabir, Saif Al Obaisi, Idrees Ahmad Nasir, Shaheen N. Khan, Bushra Irum, Fareeha Fatima, Arif O. Khan, Javed Akram, Hira Iqbal, and Muhammad Ali

Subjects

Male, Genetic Linkage, lcsh:Medicine, Locus (genetics), Biology, N-Acetylglucosaminyltransferases, Cataract, Consanguinity, Mice, medicine, Animals, Humans, Child, lcsh:Science, Sequence Deletion, Genetics, Multidisciplinary, lcsh:R, Correction, Infant, medicine.disease, N-Acetylhexosaminyltransferases, Pedigree, Genetic Loci, Child, Preschool, Congenital cataracts, Female, lcsh:Q, Microsatellite Repeats

Abstract

The aim of this study is to identify the molecular basis of autosomal recessive congenital cataracts (arCC) in a large consanguineous pedigree.All participating individuals underwent a detailed ophthalmic examination. Each patient's medical history, particularly of cataracts and other ocular abnormalities, was compiled from available medical records and interviews with family elders. Blood samples were donated by all participating family members and used to extract genomic DNA. Genetic analysis was performed to rule out linkage to known arCC loci and genes. Whole-exome sequencing libraries were prepared and paired-end sequenced. A large deletion was found that segregated with arCC in the family, and chromosome walking was conducted to estimate the proximal and distal boundaries of the deletion mutation.Exclusion and linkage analysis suggested linkage to a region of chromosome 6p24 harboring GCNT2 (glucosaminyl (N-acetyl) transferase 2) with a two-point logarithm of odds score of 5.78. PCR amplifications of the coding exons of GCNT2 failed in individuals with arCC, and whole-exome data analysis revealed a large deletion on chromosome 6p in the region harboring GCNT2. Chromosomal walking using multiple primer pairs delineated the extent of the deletion to approximately 190 kb. Interestingly, a failure to amplify a junctional fragment of the deletion break strongly suggests an insertion in addition to the large deletion.Here, we report a novel insertion/deletion mutation at the GCNT2 locus that is responsible for congenital cataracts in a large consanguineous family.

Published

2017

9. Correction: Missense Mutations in CRYAB Are Liable for Recessive Congenital Cataracts

Author

Bushra Irum, Asma A. Khan, Tayyab Husnain, Sheikh Riazuddin, Firoz Kabir, Shahid Y. Khan, Javed Akram, S. Amer Riazuddin, J. Fielding Hejtmancik, Xiaodong Jiao, Arif O. Khan, and Qiwei Wang

Subjects

Genetics, Multidisciplinary, business.industry, lcsh:R, Congenital cataracts, medicine, Missense mutation, lcsh:Medicine, lcsh:Q, medicine.disease, business, lcsh:Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0137973.].

Published

2017

10. Deletion at the GCNT2 Locus Causes Autosomal Recessive Congenital Cataracts

Author

Firoz Kabir, Bushra Rauf, Shahid Y. Khan, Shaheen N. Khan, Arif O. Khan, Fareeha Fatima, Idrees Ahmad Nasir, S. Amer Riazuddin, Saif Al Obaisi, Muhammad Daud, Sheikh Riazuddin, Muhammad Ali, Hira Iqbal, Allen O. Eghrari, Bushra Irum, Tayyab Husnain, Muhammad Asif Naeem, and Javed Akram

Subjects

0301 basic medicine, lcsh:Medicine, Artificial Gene Amplification and Extension, Genetic analysis, Polymerase Chain Reaction, Exon, 0302 clinical medicine, Primer walking, Medicine and Health Sciences, Deletions, lcsh:Science, Lens (Anatomy), Genetics, Multidisciplinary, Mammalian Genomics, Chromosome Biology, Nonsense Mutation, Genomics, 16. Peace & justice, Chromosomal Aberrations, Congenital cataracts, Anatomy, Genetic Dominance, Research Article, Ocular Anatomy, Locus (genetics), Biology, Research and Analysis Methods, 03 medical and health sciences, Genetic linkage, Ocular System, medicine, Molecular Biology Techniques, Molecular Biology, Recessive Traits, Autosomal Recessive Traits, Cataracts, lcsh:R, Chromosome, Biology and Life Sciences, Cell Biology, medicine.disease, genomic DNA, Ophthalmology, 030104 developmental biology, Genetic Loci, Animal Genomics, Lens Disorders, Mutation, 030221 ophthalmology & optometry, lcsh:Q

Abstract

PURPOSE The aim of this study is to identify the molecular basis of autosomal recessive congenital cataracts (arCC) in a large consanguineous pedigree. METHODS All participating individuals underwent a detailed ophthalmic examination. Each patient's medical history, particularly of cataracts and other ocular abnormalities, was compiled from available medical records and interviews with family elders. Blood samples were donated by all participating family members and used to extract genomic DNA. Genetic analysis was performed to rule out linkage to known arCC loci and genes. Whole-exome sequencing libraries were prepared and paired-end sequenced. A large deletion was found that segregated with arCC in the family, and chromosome walking was conducted to estimate the proximal and distal boundaries of the deletion mutation. RESULTS Exclusion and linkage analysis suggested linkage to a region of chromosome 6p24 harboring GCNT2 (glucosaminyl (N-acetyl) transferase 2) with a two-point logarithm of odds score of 5.78. PCR amplifications of the coding exons of GCNT2 failed in individuals with arCC, and whole-exome data analysis revealed a large deletion on chromosome 6p in the region harboring GCNT2. Chromosomal walking using multiple primer pairs delineated the extent of the deletion to approximately 190 kb. Interestingly, a failure to amplify a junctional fragment of the deletion break strongly suggests an insertion in addition to the large deletion. CONCLUSION Here, we report a novel insertion/deletion mutation at the GCNT2 locus that is responsible for congenital cataracts in a large consanguineous family.

Published

2016

11. Mutation in LIM2 Is Responsible for Autosomal Recessive Congenital Cataracts

Author

Tayyab Husnain, Muhammad Asif Naeem, Bushra Irum, Bushra Rauf, Javed Akram, Sheikh Riazuddin, Arif O. Khan, Firoz Kabir, Muhammad Ali, S. Amer Riazuddin, Allen O. Eghrari, Haiba Kaul, Shaheen N. Khan, Fareeha Fatima, Shahid Y. Khan, Raheela Nadeem, Idrees Ahmad Nasir, and Saif Al Obaisi

Subjects

Male, 0301 basic medicine, Candidate gene, Heredity, Genetic Linkage, Mutant, lcsh:Medicine, Consanguinity, Mice, Database and Informatics Methods, 0302 clinical medicine, Medicine and Health Sciences, Missense mutation, lcsh:Science, Lens (Anatomy), Genetics, Mammalian Genomics, Multidisciplinary, Genomics, Genomic Databases, Phenotype, Pedigree, 3. Good health, Genetic Mapping, Mutation (genetic algorithm), Congenital cataracts, Linkage Analysis, Female, Anatomy, Genetic Dominance, Research Article, Missense Mutation, Ocular Anatomy, Mutation, Missense, Genes, Recessive, Biology, Research and Analysis Methods, Cataract, 03 medical and health sciences, Genomic Medicine, Cataracts, Ocular System, Genetic linkage, medicine, Animals, Humans, Eye Proteins, Recessive Traits, Autosomal Recessive Traits, lcsh:R, Membrane Proteins, Biology and Life Sciences, Computational Biology, Genome Analysis, medicine.disease, eye diseases, Mice, Inbred C57BL, Ophthalmology, Biological Databases, 030104 developmental biology, Animal Genomics, Lens Disorders, Mutation, 030221 ophthalmology & optometry, lcsh:Q

Abstract

Purpose To identify the molecular basis of non-syndromic autosomal recessive congenital cataracts (arCC) in a consanguineous family. Methods All family members participating in the study received a comprehensive ophthalmic examination to determine their ocular phenotype and contributed a blood sample, from which genomic DNA was extracted. Available medical records and interviews with the family were used to compile the medical history of the family. The symptomatic history of the individuals exhibiting cataracts was confirmed by slit-lamp biomicroscopy. A genome-wide linkage analysis was performed to localize the disease interval. The candidate gene, LIM2 (lens intrinsic membrane protein 2), was sequenced bi-directionally to identify the disease-causing mutation. The physical changes caused by the mutation were analyzed in silico through homology modeling, mutation and bioinformatic algorithms, and evolutionary conservation databases. The physiological importance of LIM2 to ocular development was assessed in vivo by real-time expression analysis of Lim2 in a mouse model. Results Ophthalmic examination confirmed the diagnosis of nuclear cataracts in the affected members of the family; the inheritance pattern and cataract development in early infancy indicated arCC. Genome-wide linkage analysis localized the critical interval to chromosome 19q with a two-point logarithm of odds (LOD) score of 3.25. Bidirectional sequencing identified a novel missense mutation, c.233G>A (p.G78D) in LIM2. This mutation segregated with the disease phenotype and was absent in 192 ethnically matched control chromosomes. In silico analysis predicted lower hydropathicity and hydrophobicity but higher polarity of the mutant LIM2-encoded protein (MP19) compared to the wild-type. Moreover, these analyses predicted that the mutation would disrupt the secondary structure of a transmembrane domain of MP19. The expression of Lim2, which was detected in the mouse lens as early as embryonic day 15 (E15) increased after birth to a level that was sustained through the postnatal time points. Conclusion A novel missense mutation in LIM2 is responsible for autosomal recessive congenital cataracts.

Published

2016

12. Correction: Deletion at the GCNT2 Locus Causes Autosomal Recessive Congenital Cataracts

Author

Irum, Bushra, primary, Khan, Shahid Y., additional, Ali, Muhammad, additional, Daud, Muhammad, additional, Kabir, Firoz, additional, Rauf, Bushra, additional, Fatima, Fareeha, additional, Iqbal, Hira, additional, Khan, Arif O., additional, Obaisi, Saif Al, additional, Naeem, Muhammad Asif, additional, Nasir, Idrees A., additional, Khan, Shaheen N., additional, Husnain, Tayyab, additional, Riazuddin, Sheikh, additional, Akram, Javed, additional, Eghrari, Allen O., additional, and Riazuddin, S. Amer, additional

Published

2017

13. Correction: Missense Mutations in CRYAB Are Liable for Recessive Congenital Cataracts

Author

Jiao, Xiaodong, primary, Khan, Shahid Y., additional, Irum, Bushra, additional, Khan, Arif O., additional, Wang, Qiwei, additional, Kabir, Firoz, additional, Khan, Asma A., additional, Husnain, Tayyab, additional, Akram, Javed, additional, Riazuddin, Sheikh, additional, Hejtmancik, J. Fielding, additional, and Riazuddin, S. Amer, additional

Published

2017

14. Deletion at the GCNT2 Locus Causes Autosomal Recessive Congenital Cataracts

Author

Irum, Bushra, primary, Khan, Shahid Y., additional, Ali, Muhammad, additional, Daud, Muhammad, additional, Kabir, Firoz, additional, Rauf, Bushra, additional, Fatima, Fareeha, additional, Iqbal, Hira, additional, Khan, Arif O., additional, Al Obaisi, Saif, additional, Naeem, Muhammad Asif, additional, Nasir, Idrees A., additional, Khan, Shaheen N., additional, Husnain, Tayyab, additional, Riazuddin, Sheikh, additional, Akram, Javed, additional, Eghrari, Allen O., additional, and Riazuddin, S. Amer, additional

Published

2016

15. Investigating the Molecular Basis of Retinal Degeneration in a Familial Cohort of Pakistani Decent by Exome Sequencing

Author

Sheikh Riazuddin, Muhammad Asif Naeem, Justin Chu, Sheen N. Khan, Alexander D. H. Gottsch, Pooja Biswas, John Suk, Rachel Poleman, S. Amer Riazuddin, Javed Akram, Pauline Lee, Radha Ayyagari, Mili Navani, J. Fielding Hejtmancik, Bruno Maranhao, and Sharon, Dror

Subjects

Retinal degeneration, Male, Messenger, lcsh:Medicine, Pedigree chart, Bioinformatics, Consanguinity, Ethnicity, 2.1 Biological and endogenous factors, Exome, Pakistan, Aetiology, Age of Onset, lcsh:Science, Exome sequencing, Genetics, Multidisciplinary, medicine.diagnostic_test, Retinal Degeneration, Single Nucleotide, 3. Good health, Pedigree, Phenotype, Cohort, Female, Sequence Analysis, Research Article, Genotype, General Science & Technology, Fundus Oculi, Ethnic Groups, Genes, Recessive, Biology, Polymorphism, Single Nucleotide, Clinical Research, otorhinolaryngologic diseases, medicine, Electroretinography, Recessive, Humans, RNA, Messenger, Polymorphism, Eye Proteins, Eye Disease and Disorders of Vision, Genetic Association Studies, Sequence Analysis, RNA, lcsh:R, medicine.disease, Genes, Mutation, RNA, lcsh:Q, Age of onset, Sequence Alignment

Abstract

PURPOSE:To define the molecular basis of retinal degeneration in consanguineous Pakistani pedigrees with early onset retinal degeneration. METHODS:A cohort of 277 individuals representing 26 pedigrees from the Punjab province of Pakistan was analyzed. Exomes were captured with commercial kits and sequenced on an Illumina HiSeq 2500. Candidate variants were identified using standard tools and analyzed using exomeSuite to detect all potentially pathogenic changes in genes implicated in retinal degeneration. Segregation analysis was performed by dideoxy sequencing and novel variants were additionally investigated for their presence in ethnicity-matched controls. RESULTS:We identified a total of nine causal mutations, including six novel variants in RPE65, LCA5, USH2A, CNGB1, FAM161A, CERKL and GUCY2D as the underlying cause of inherited retinal degenerations in 13 of 26 pedigrees. In addition to the causal variants, a total of 200 variants each observed in five or more unrelated pedigrees investigated in this study that were absent from the dbSNP, HapMap, 1000 Genomes, NHLBI ESP6500, and ExAC databases were identified, suggesting that they are common in, and unique to the Pakistani population. CONCLUSIONS:We identified causal mutations associated with retinal degeneration in nearly half of the pedigrees investigated in this study through next generation whole exome sequencing. All novel variants detected in this study through exome sequencing have been cataloged providing a reference database of variants common in, and unique to the Pakistani population.

Published

2015

16. Missense Mutations in CRYAB Are Liable for Recessive Congenital Cataracts

Author

Tayyab Husnain, J. Fielding Hejtmancik, Arif O. Khan, Asma A. Khan, Firoz Kabir, Qiwei Wang, S. Amer Riazuddin, Shahid Y. Khan, Sheikh Riazuddin, Bushra Irum, Xiaodong Jiaox, and Javed Akram

Subjects

Male, Genetic Linkage, DNA Mutational Analysis, Gene Expression, lcsh:Medicine, medicine.disease_cause, Consanguinity, Mice, 0302 clinical medicine, Missense mutation, lcsh:Science, Genetics, 0303 health sciences, Mutation, Multidisciplinary, Slit Lamp, Exons, 3. Good health, Pedigree, Congenital cataracts, Female, Research Article, Mutation, Missense, Genes, Recessive, Biology, Cataract, Evolution, Molecular, 03 medical and health sciences, Cataracts, Genetic linkage, medicine, Animals, Humans, Allele, 030304 developmental biology, Chromosomes, Human, Pair 11, Haplotype, lcsh:R, Computational Biology, alpha-Crystallin B Chain, Correction, medicine.disease, Molecular biology, eye diseases, Disease Models, Animal, Haplotypes, 030221 ophthalmology & optometry, lcsh:Q, Lod Score, Microsatellite Repeats

Abstract

Purpose This study was initiated to identify causal mutations responsible for autosomal recessive congenital cataracts in consanguineous familial cases. Methods Affected individuals underwent a detailed ophthalmological and clinical examination, and slit-lamp photographs were ascertained for affected individuals who have not yet been operated for the removal of the cataractous lens. Blood samples were obtained, and genomic DNA was extracted from white blood cells. A genome-wide scan was completed with short tandem repeat (STR) markers, and the logarithm of odds (LOD) scores were calculated. Protein coding exons of CRYAB were sequenced, bi-directionally. Evolutionary conservation was investigated by aligning CRYAB orthologues, and the expression of Cryab in embryonic and postnatal mice lens was investigated with TaqMan probe. Results The clinical and ophthalmological examinations suggested that all affected individuals had nuclear cataracts. Genome-wide linkage analysis suggested a potential region on chromosome 11q23 harboring CRYAB. DNA sequencing identified a missense variation: c.34C>T (p.R12C) in CRYAB that segregated with the disease phenotype in the family. Subsequent interrogation of our entire cohort of familial cases identified a second familial case localized to chromosome 11q23 harboring a c.31C>T (p.R11C) mutation. In silico analyses suggested that the mutations identified in familial cases, p.R11C and p.R12C will not be tolerated by the three-dimensional structure of CRYAB. Real-time PCR analysis identified the expression of Cryab in mouse lens as early as embryonic day 15 (E15) that increased significantly until postnatal day 6 (P6) with steady level of expression thereafter. Conclusion Here, we report two novel missense mutations, p.R11C and p.R12C, in CRYAB associated with autosomal recessive congenital nuclear cataracts.

Published

2015

17. Mutation in LIM2 Is Responsible for Autosomal Recessive Congenital Cataracts

Author

Irum, Bushra, primary, Khan, Shahid Y., additional, Ali, Muhammad, additional, Kaul, Haiba, additional, Kabir, Firoz, additional, Rauf, Bushra, additional, Fatima, Fareeha, additional, Nadeem, Raheela, additional, Khan, Arif O., additional, Al Obaisi, Saif, additional, Naeem, Muhammad Asif, additional, Nasir, Idrees A., additional, Khan, Shaheen N., additional, Husnain, Tayyab, additional, Riazuddin, Sheikh, additional, Akram, Javed, additional, Eghrari, Allen O., additional, and Riazuddin, S. Amer, additional

Published

2016

18. A Common Ancestral Mutation in CRYBB3 Identified in Multiple Consanguineous Families with Congenital Cataracts

Author

Jiao, Xiaodong, primary, Kabir, Firoz, additional, Irum, Bushra, additional, Khan, Arif O., additional, Wang, Qiwei, additional, Li, David, additional, Khan, Asma A., additional, Husnain, Tayyab, additional, Akram, Javed, additional, Riazuddin, Sheikh, additional, Hejtmancik, J. Fielding, additional, and Riazuddin, S. Amer, additional

Published

2016

19. Correction: A Novel C-Terminal CIB2 (Calcium and Integrin Binding Protein 2) Mutation Associated with Non-Syndromic Hearing Loss in a Hispanic Family

Author

Bernice E. Morrow, Maria Delio, Rashmi S. Hegde, Jinlu Cai, Arnaud P. J. Giese, Joy Samanich, Zubair Ahmed, Kunjan Patel, Jonathan M Grossheim, Saima Riazuddin, and Gregory I. Frolenkov

Subjects

Adult, Male, Models, Molecular, Hearing loss, Mutation, Missense, chemistry.chemical_element, lcsh:Medicine, Calcium, Myosins, Protein Structure, Secondary, Stereocilia, Chlorocebus aethiops, medicine, Animals, Humans, Exome, Amino Acid Sequence, lcsh:Science, Child, Hearing Loss, Integrin binding, Genetics, Multidisciplinary, business.industry, lcsh:R, Calcium-Binding Proteins, Correction, Infant, Membrane Proteins, Hispanic or Latino, Pedigree, HEK293 Cells, chemistry, Mutation (genetic algorithm), COS Cells, lcsh:Q, Female, medicine.symptom, business, Non syndromic

Abstract

Hearing loss is a complex disorder caused by both genetic and environmental factors. Previously, mutations in CIB2 have been identified as a common cause of genetic hearing loss in Pakistani and Turkish populations. Here we report a novel (c.556CT; p.(Arg186Trp)) transition mutation in the CIB2 gene identified through whole exome sequencing (WES) in a Caribbean Hispanic family with non-syndromic hearing loss. CIB2 belongs to the family of calcium-and integrin-binding (CIB) proteins. The carboxy-termini of CIB proteins are associated with calcium binding and intracellular signaling. The p.(Arg186Trp) mutation is localized within predicted type II PDZ binding ligand at the carboxy terminus. Our ex vivo studies revealed that the mutation did not alter the interactions of CIB2 with Whirlin, nor its targeting to the tips of hair cell stereocilia. However, we found that the mutation disrupts inhibition of ATP-induced Ca2+ responses by CIB2 in a heterologous expression system. Our findings support p.(Arg186Trp) mutation as a cause for hearing loss in this Hispanic family. In addition, it further highlights the necessity of the calcium binding property of CIB2 for normal hearing.

Published

2015

20. MARVELD2 (DFNB49) mutations in the hearing impaired Central European Roma population--prevalence, clinical impact and the common origin

Author

Saima Anwar, Saima Riazuddin, Petra Matyas, Ľudevít Kádaši, Judit Bene, Béla Melegh, Andrea Šoltýsová, Slavomír Straka, Daniela Gasperikova, Dana Šafka-Brožková Ph.D, Zubair M. Ahmed, Iwar Klimes, Milan Profant, Lukas Varga, Martina Sůrová, Miloslava Hučková, Ivica Masindova, Andrej Ficek, Pavel Seeman, and Ingrid Janicsek

Subjects

Biallelic Mutation, Pediatrics, medicine.medical_specialty, Slovakia, Roma, Genotype, Hearing loss, Population, lcsh:Medicine, Biology, Polymorphism, Single Nucleotide, Connexins, Gene Frequency, Sequence Homology, Nucleic Acid, medicine, Prevalence, otorhinolaryngologic diseases, Humans, Pakistan, Age of Onset, education, Hearing Loss, lcsh:Science, Allele frequency, Alleles, Czech Republic, Genetics, education.field_of_study, Hungary, Multidisciplinary, Haplotype, lcsh:R, Infant, Exons, medicine.disease, Founder Effect, 3. Good health, Connexin 26, MARVEL Domain Containing 2 Protein, Haplotypes, Mutation (genetic algorithm), Mutation, Sensorineural hearing loss, lcsh:Q, medicine.symptom, Founder effect, Research Article

Abstract

Background In the present study we aimed: 1) To establish the prevalence and clinical impact of DFNB49 mutations in deaf Roma from 2 Central European countries (Slovakia and Hungary), and 2) to analyze a possible common origin of the c.1331+2T>C mutation among Roma and Pakistani mutation carriers identified in the present and previous studies. Methods We sequenced 6 exons of the MARVELD2 gene in a group of 143 unrelated hearing impaired Slovak Roma patients. Simultaneously, we used RFLP to detect the c.1331+2T>C mutation in 85 Hungarian deaf Roma patients, control groups of 702 normal hearing Romanies from both countries and 375 hearing impaired Slovak Caucasians. We analyzed the haplotype using 21 SNPs spanning a 5.34Mb around the mutation c.1331+2T>C. Results One pathogenic mutation (c.1331+2T>C) was identified in 12 homozygous hearing impaired Roma patients. Allele frequency of this mutation was higher in Hungarian (10%) than in Slovak (3.85%) Roma patients. The identified common haplotype in Roma patients was defined by 18 SNP markers (3.89 Mb). Fourteen common SNPs were also shared among Pakistani and Roma homozygotes. Biallelic mutation carriers suffered from prelingual bilateral moderate to profound sensorineural hearing loss. Conclusions We demonstrate different frequencies of the c.1331+2T>C mutation in hearing impaired Romanies from 3 Central European countries. In addition, our results provide support for the hypothesis of a possible common ancestor of the Slovak, Hungarian and Czech Roma as well as Pakistani deaf patients. Testing for the c.1331+2T>C mutation may be recommended in GJB2 negative Roma cases with early-onset sensorineural hearing loss.

Published

2015

21. A Novel C-Terminal CIB2 (Calcium and Integrin Binding Protein 2) Mutation Associated with Non-Syndromic Hearing Loss in a Hispanic Family

Author

Saima Riazuddin, Zubair M. Ahmed, Maria Delio, Jonathan M Grossheim, Joy Samanich, Gregory I. Frolenkov, Arnaud P. J. Giese, Bernice E. Morrow, Jinlu Cai, Rashima S. Hegde, and Kunjan Patel

Subjects

Hearing loss, lcsh:Medicine, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Calcium-binding protein, medicine, otorhinolaryngologic diseases, Missense mutation, lcsh:Science, Exome, Exome sequencing, 030304 developmental biology, Integrin binding, Genetics, 0303 health sciences, Mutation, Multidisciplinary, lcsh:R, Molecular biology, Membrane protein, lcsh:Q, medicine.symptom, 030217 neurology & neurosurgery, Research Article

Abstract

Hearing loss is a complex disorder caused by both genetic and environmental factors. Previously, mutations in CIB2 have been identified as a common cause of genetic hearing loss in Pakistani and Turkish populations. Here we report a novel (c.556C>T; p.(Arg186Trp)) transition mutation in the CIB2 gene identified through whole exome sequencing (WES) in a Caribbean Hispanic family with non-syndromic hearing loss. CIB2 belongs to the family of calcium-and integrin-binding (CIB) proteins. The carboxy-termini of CIB proteins are associated with calcium binding and intracellular signaling. The p.(Arg186Trp) mutation is localized within predicted type II PDZ binding ligand at the carboxy terminus. Our ex vivo studies revealed that the mutation did not alter the interactions of CIB2 with Whirlin, nor its targeting to the tips of hair cell stereocilia. However, we found that the mutation disrupts inhibition of ATP-induced Ca2+ responses by CIB2 in a heterologous expression system. Our findings support p.(Arg186Trp) mutation as a cause for hearing loss in this Hispanic family. In addition, it further highlights the necessity of the calcium binding property of CIB2 for normal hearing.

Published

2015

22. Radioprotective Effect of Aminothiol PrC-210 on Irradiated Inner Ear of Guinea Pig

Author

Zubair M. Ahmed, Daniel I. Choo, Arnaud P. J. Giese, Jess G. Guarnaschelli, Saima Riazuddin, and Jonette A. Ward

Subjects

medicine.medical_specialty, animal structures, Hearing loss, Hearing Loss, Sensorineural, Guinea Pigs, lcsh:Medicine, Radiation-Protective Agents, Diamines, Guinea pig, Hearing, Internal medicine, Hair Cells, Auditory, medicine, Evoked Potentials, Auditory, Brain Stem, otorhinolaryngologic diseases, Animals, Inner ear, Sulfhydryl Compounds, lcsh:Science, Cochlea, Spiral ganglion, Multidisciplinary, medicine.diagnostic_test, Radiotherapy, business.industry, lcsh:R, Dose-Response Relationship, Radiation, Anatomy, medicine.disease, medicine.anatomical_structure, Endocrinology, Organ of Corti, Ear, Inner, Audiometry, Pure-Tone, Sensorineural hearing loss, lcsh:Q, sense organs, Audiometry, medicine.symptom, business, Spiral Ganglion, Injections, Intraperitoneal, Research Article

Abstract

Radiotherapy of individuals suffering with head & neck or brain tumors subserve the risk of sensorineural hearing loss. Here, we evaluated the protective effect of Aminothiol PrC-210 (3-(methyl-amino)-2-((methylamino)methyl)propane-1-thiol) on the irradiated inner ear of guinea pigs. An intra-peritoneal or intra-tympanic dose of PrC-210 was administered prior to receiving a dose of gamma radiation (3000 cGy) to each ear. Auditory Brainstem Responses (ABRs) were recorded one week and two weeks after the radiation and compared with the sham animal group. ABR thresholds of guinea pigs that received an intra-peritoneal dose of PrC-210 were significantly better compared to the non-treated, control animals at one week post-radiation. Morphologic analysis of the inner ear revealed significant inflammation and degeneration of the spiral ganglion in the irradiated animals not treated with PrC-210. In contrast, when treated with PrC-210 the radiation effect and injury to the spiral ganglion was significantly alleviated. PrC-210 had no apparent cytotoxic effect in vivo and did not affect the morphology or count of cochlear hair cells. These findings suggest that aminothiol PrC-210 attenuated radiation-induced cochlea damage for at least one week and protected hearing.

Published

2015

23. A Common Ancestral Mutation in CRYBB3 Identified in Multiple Consanguineous Families with Congenital Cataracts

Author

Xiaodong Jiao, S. Amer Riazuddin, David Li, J. Fielding Hejtmancik, Asma A. Khan, Firoz Kabir, Arif O. Khan, Tayyab Husnain, Bushra Irum, Qiwei Wang, Sheikh Riazuddin, and Javed Akram

Subjects

Male, 0301 basic medicine, Chromosomes, Human, Pair 22, lcsh:Medicine, Database and Informatics Methods, Consanguinity, Mice, 0302 clinical medicine, beta-Crystallin B Chain, Medicine and Health Sciences, Missense mutation, lcsh:Science, Exome, Lens (Anatomy), Genetics, Sanger sequencing, Mammalian Genomics, Slit Lamp, Multidisciplinary, Chromosome Biology, Genomics, Genomic Databases, Pedigree, 3. Good health, Congenital cataracts, symbols, Female, Anatomy, Research Article, Genetic Markers, Ocular Anatomy, Single-nucleotide polymorphism, Biology, Research and Analysis Methods, Polymorphism, Single Nucleotide, Chromosomes, Cataract, 03 medical and health sciences, symbols.namesake, Genomic Medicine, Ocular System, Genetic linkage, Lens, Crystalline, medicine, Animals, Humans, Family, Alleles, Evolutionary Biology, Population Biology, Base Sequence, Cataracts, Gene Expression Profiling, lcsh:R, Haplotype, Biology and Life Sciences, Computational Biology, Cell Biology, Genome Analysis, medicine.disease, eye diseases, Ophthalmology, Biological Databases, 030104 developmental biology, Haplotypes, Animal Genomics, Genetic Loci, Lens Disorders, Mutation, 030221 ophthalmology & optometry, lcsh:Q, Lod Score, Population Genetics, Microsatellite Repeats

Abstract

Purpose This study was performed to investigate the genetic determinants of autosomal recessive congenital cataracts in large consanguineous families. Methods Affected individuals underwent a detailed ophthalmological examination and slit-lamp photographs of the cataractous lenses were obtained. An aliquot of blood was collected from all participating family members and genomic DNA was extracted from white blood cells. Initially, a genome-wide scan was performed with genomic DNAs of family PKCC025 followed by exclusion analysis of our familial cohort of congenital cataracts. Protein-coding exons of CRYBB1, CRYBB2, CRYBB3, and CRYBA4 were sequenced bidirectionally. A haplotype was constructed with SNPs flanking the causal mutation for affected individuals in all four families, while the probability that the four familial cases have a common founder was estimated using EM and CHM-based algorithms. The expression of Crybb3 in the developing murine lens was investigated using TaqMan assays. Results The clinical and ophthalmological examinations suggested that all affected individuals had nuclear cataracts. Genome-wide linkage analysis localized the causal phenotype in family PKCC025 to chromosome 22q with statistically significant two-point logarithm of odds (LOD) scores. Subsequently, we localized three additional families, PKCC063, PKCC131, and PKCC168 to chromosome 22q. Bidirectional Sanger sequencing identified a missense variation: c.493G>C (p.Gly165Arg) in CRYBB3 that segregated with the disease phenotype in all four familial cases. This variation was not found in ethnically matched control chromosomes, the NHLBI exome variant server, or the 1000 Genomes or dbSNP databases. Interestingly, all four families harbor a unique disease haplotype that strongly suggests a common founder of the causal mutation (p

Published

2016

24. Missense Mutations in CRYAB Are Liable for Recessive Congenital Cataracts

Author

Jiaox, Xiaodong, primary, Khan, Shahid Y., additional, Irum, Bushra, additional, Khan, Arif O., additional, Wang, Qiwei, additional, Kabir, Firoz, additional, Khan, Asma A., additional, Husnain, Tayyab, additional, Akram, Javed, additional, Riazuddin, Sheikh, additional, Hejtmancik, J. Fielding, additional, and Riazuddin, S. Amer, additional

Published

2015

25. Replication of TCF4 through association and linkage studies in late-onset Fuchs endothelial corneal dystrophy

Author

Natalie A. Afshari, Gordon K. Klintworth, Simon G. Gregory, Elmer Balajonda, R. Rand Allingham, S. Amer Riazuddin, John D. Gottsch, Nicholas Katsanis, Michael A. Hauser, Bei Zhao, Yi-Ju Li, J. B. Rimmler, Mollie A. Minear, and Allen O. Eghrari

Subjects

Genetic Markers, Genetic Linkage, Fuchs Endothelial Dystrophy, lcsh:Medicine, Genome-wide association study, Single-nucleotide polymorphism, Locus (genetics), Biology, Polymorphism, Single Nucleotide, Transcription Factor 4, Chromosome 18, Genetic linkage, Genome Analysis Tools, Genetic model, Molecular Cell Biology, Genetics, Humans, Genetic Predisposition to Disease, Allele, lcsh:Science, Genetic Association Studies, Linkage Maps, Multidisciplinary, Models, Genetic, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, lcsh:R, Fuchs' Endothelial Dystrophy, Endothelial Cells, Human Genetics, Genomics, Introns, Ophthalmology, Corneal Disorders, Medicine, lcsh:Q, Cellular Types, Chromosomes, Human, Pair 18, Genome-Wide Association Study, Transcription Factors, Research Article

Abstract

Fuchs endothelial corneal dystrophy (FECD) is a common, late-onset disorder of the corneal endothelium. Although progress has been made in understanding the genetic basis of FECD by studying large families in which the phenotype is transmitted in an autosomal dominant fashion, a recently reported genome-wide association study identified common alleles at a locus on chromosome 18 near TCF4 which confer susceptibility to FECD. Here, we report the findings of our independent validation study for TCF4 using the largest FECD dataset to date (450 FECD cases and 340 normal controls). Logistic regression with sex as a covariate was performed for three genetic models: dominant (DOM), additive (ADD), and recessive (REC). We found significant association with rs613872, the target marker reported by Baratz et al.(2010), for all three genetic models (DOM: P = 9.33×10(-35); ADD: P = 7.48×10(-30); REC: P = 5.27×10(-6)). To strengthen the association study, we also conducted a genome-wide linkage scan on 64 multiplex families, composed primarily of affected sibling pairs (ASPs), using both parametric and non-parametric two-point and multipoint analyses. The most significant linkage region localizes to chromosome 18 from 69.94cM to 85.29cM, with a peak multipoint HLOD = 2.5 at rs1145315 (75.58cM) under the DOM model, mapping 1.5 Mb proximal to rs613872. In summary, our study presents evidence to support the role of the intronic TCF4 single nucleotide polymorphism rs613872 in late-onset FECD through both association and linkage studies.

Published

2010

26. Radioprotective Effect of Aminothiol PrC-210 on Irradiated Inner Ear of Guinea Pig

Author

Giese, Arnaud P. J., primary, Guarnaschelli, Jess G., additional, Ward, Jonette A., additional, Choo, Daniel I., additional, Riazuddin, Saima, additional, and Ahmed, Zubair M., additional

Published

2015

27. Correction: A Novel C-Terminal CIB2 (Calcium and Integrin Binding Protein 2) Mutation Associated with Non-Syndromic Hearing Loss in a Hispanic Family

Author

Patel, Kunjan, primary, Giese, Arnaud P., additional, Grossheim, J. M., additional, Hegde, Rashmi S., additional, Delio, Maria, additional, Samanich, Joy, additional, Riazuddin, Saima, additional, Frolenkov, Gregory I., additional, Cai, Jinlu, additional, Ahmed, Zubair M., additional, and Morrow, Bernice E., additional

Published

2015

28. A Novel C-Terminal CIB2 (Calcium and Integrin Binding Protein 2) Mutation Associated with Non-Syndromic Hearing Loss in a Hispanic Family

Author

Patel, Kunjan, primary, Giese, Arnaud P., additional, Grossheim, J. M., additional, Hegde, Rashima S., additional, Delio, Maria, additional, Samanich, Joy, additional, Riazuddin, Saima, additional, Frolenkov, Gregory I., additional, Cai, Jinlu, additional, Ahmed, Zubair M., additional, and Morrow, Bernice E., additional

Published

2015

29. MARVELD2 (DFNB49) Mutations in the Hearing Impaired Central European Roma Population - Prevalence, Clinical Impact and the Common Origin

Author

Mašindová, Ivica, primary, Šoltýsová, Andrea, additional, Varga, Lukáš, additional, Mátyás, Petra, additional, Ficek, Andrej, additional, Hučková, Miloslava, additional, Sůrová, Martina, additional, Šafka-Brožková, Dana, additional, Anwar, Saima, additional, Bene, Judit, additional, Straka, Slavomír, additional, Janicsek, Ingrid, additional, Ahmed, Zubair M., additional, Seeman, Pavel, additional, Melegh, Béla, additional, Profant, Milan, additional, Klimeš, Iwar, additional, Riazuddin, Saima, additional, Kádasi, Ľudevít, additional, and Gašperíková, Daniela, additional

Published

2015

30. Replication of TCF4 through Association and Linkage Studies in Late-Onset Fuchs Endothelial Corneal Dystrophy

Author

Li, Yi-Ju, primary, Minear, Mollie A., additional, Rimmler, Jacqueline, additional, Zhao, Bei, additional, Balajonda, Elmer, additional, Hauser, Michael A., additional, Allingham, R. Rand, additional, Eghrari, Allen O., additional, Riazuddin, S. Amer, additional, Katsanis, Nicholas, additional, Gottsch, John D., additional, Gregory, Simon G., additional, Klintworth, Gordon K., additional, and Afshari, Natalie A., additional

Published

2011

31. Replication of TCF4 through Association and Linkage Studies in Late-Onset Fuchs Endothelial Corneal Dystrophy.

Author

Yi-Ju Li, Minear, Mollie A., Rimmler, Jacqueline, Bei Zhao, Balajonda, Elmer, Hauser, Michael A., Allingham, R. Rand, Eghrari, Allen O., Riazuddin, S. Amer, Katsanis, Nicholas, Gottsch, John D., Gregory, Simon G., Klintworth, Gordon K., and Afshari, Natalie A.

Subjects

DYSTROPHY, ENDOTHELIUM physiology, CORNEA diseases, CHROMOSOME polymorphism, GENETIC polymorphisms, POPULATION genetics, GENETIC models, GENETICS

Abstract

Fuchs endothelial corneal dystrophy (FECD) is a common, late-onset disorder of the corneal endothelium. Although progress has been made in understanding the genetic basis of FECD by studying large families in which the phenotype is transmitted in an autosomal dominant fashion, a recently reported genome-wide association study identified common alleles at a locus on chromosome 18 near TCF4 which confer susceptibility to FECD. Here, we report the findings of our independent validation study for TCF4 using the largest FECD dataset to date (450 FECD cases and 340 normal controls). Logistic regression with sex as a covariate was performed for three genetic models: dominant (DOM), additive (ADD), and recessive (REC). We found significant association with rs613872, the target marker reported by Baratz et al.(2010), for all three genetic models (DOM: P = 9.33×10-35; ADD: P = 7.48×10-30; REC: P = 5.27×10-6). To strengthen the association study, we also conducted a genome-wide linkage scan on 64 multiplex families, composed primarily of affected sibling pairs (ASPs), using both parametric and non-parametric two-point and multipoint analyses. The most significant linkage region localizes to chromosome 18 from 69.94cM to 85.29cM, with a peak multipoint HLOD = 2.5 at rs1145315 (75.58cM) under the DOM model, mapping 1.5 Mb proximal to rs613872. In summary, our study presents evidence to support the role of the intronic TCF4 single nucleotide polymorphism rs613872 in late-onset FECD through both association and linkage studies. [ABSTRACT FROM AUTHOR]

Published

2011

32. Factors influencing low-income households’ food insecurity in Bangladesh during the COVID-19 lockdown

Author

Suvasish Das Shuvo, Md. Sakhawot Hossain, Md. Riazuddin, Sanaullah Mazumdar, and Deepa Roy

Subjects

Medicine, Science

Abstract

Background The COVID-19 pandemic and countrywide lockdown could negatively impact household food insecurity among low-income households. This study aimed to investigate the prevalence of household food insecurity and its influencing factors among low-income people in Bangladesh during the lockdown of COVID-19. Methods This cross-sectional study was conducted through face-to-face interviews from 500 low-income households during the countrywide COVID-19 lockdown. A pretested, structured and validated questionnaire was used to collect socioeconomic characteristics, household income conditions, and food accessibility. Household Food Insecurity Access Scale (HFIAS) and Dietary Diversity Score (DDS) were used to measure food insecurity. Multinomial logistic regression models were estimated to evaluate and predict risk factors that influence food insecurity. Results The study found that above 67% of households was mild-to-moderate food insecure while 23% experienced severe food insecurity. Significantly, 88%, 97.4%, and 93.4% of the households had anxiety and uncertainty, inadequate quality, and inadequate quantity of food, respectively. The regression analysis revealed the age 36–50 years (RRR: 4.86; 95% CI: 2.31–7.44, RRR: 4.16; 95% CI: 2.25–6.10) and monthly income Conclusion This study found that households become more susceptible to food insecurity during the COVID-19 pandemic and lockdown period. Based on the findings, we suggest some essential food policies and adequate food assistance to mitigate these negative consequences.

Published

2022

33. Correction: Missense Mutations in CRYAB Are Liable for Recessive Congenital Cataracts.

Author

Xiaodong Jiao, Shahid Y Khan, Bushra Irum, Arif O Khan, Qiwei Wang, Firoz Kabir, Asma A Khan, Tayyab Husnain, Javed Akram, Sheikh Riazuddin, J Fielding Hejtmancik, and S Amer Riazuddin

Subjects

Medicine, Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0137973.].

Published

2017

34. Correction: Deletion at the GCNT2 Locus Causes Autosomal Recessive Congenital Cataracts.

Author

Bushra Irum, Shahid Y Khan, Muhammad Ali, Muhammad Daud, Firoz Kabir, Bushra Rauf, Fareeha Fatima, Hira Iqbal, Arif O Khan, Saif Al Obaisi, Muhammad Asif Naeem, Idrees A Nasir, Shaheen N Khan, Tayyab Husnain, Sheikh Riazuddin, Javed Akram, Allen O Eghrari, and S Amer Riazuddin

Subjects

Medicine, Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0167562.].

Published

2017

35. Deletion at the GCNT2 Locus Causes Autosomal Recessive Congenital Cataracts.

Author

Bushra Irum, Shahid Y Khan, Muhammad Ali, Muhammad Daud, Firoz Kabir, Bushra Rauf, Fareeha Fatima, Hira Iqbal, Arif O Khan, Saif Al Obaisi, Muhammad Asif Naeem, Idrees A Nasir, Shaheen N Khan, Tayyab Husnain, Sheikh Riazuddin, Javed Akram, Allen O Eghrari, and S Amer Riazuddin

Subjects

Medicine, Science

Abstract

The aim of this study is to identify the molecular basis of autosomal recessive congenital cataracts (arCC) in a large consanguineous pedigree.All participating individuals underwent a detailed ophthalmic examination. Each patient's medical history, particularly of cataracts and other ocular abnormalities, was compiled from available medical records and interviews with family elders. Blood samples were donated by all participating family members and used to extract genomic DNA. Genetic analysis was performed to rule out linkage to known arCC loci and genes. Whole-exome sequencing libraries were prepared and paired-end sequenced. A large deletion was found that segregated with arCC in the family, and chromosome walking was conducted to estimate the proximal and distal boundaries of the deletion mutation.Exclusion and linkage analysis suggested linkage to a region of chromosome 6p24 harboring GCNT2 (glucosaminyl (N-acetyl) transferase 2) with a two-point logarithm of odds score of 5.78. PCR amplifications of the coding exons of GCNT2 failed in individuals with arCC, and whole-exome data analysis revealed a large deletion on chromosome 6p in the region harboring GCNT2. Chromosomal walking using multiple primer pairs delineated the extent of the deletion to approximately 190 kb. Interestingly, a failure to amplify a junctional fragment of the deletion break strongly suggests an insertion in addition to the large deletion.Here, we report a novel insertion/deletion mutation at the GCNT2 locus that is responsible for congenital cataracts in a large consanguineous family.

Published

2016

36. Mutation in LIM2 Is Responsible for Autosomal Recessive Congenital Cataracts.

Author

Bushra Irum, Shahid Y Khan, Muhammad Ali, Haiba Kaul, Firoz Kabir, Bushra Rauf, Fareeha Fatima, Raheela Nadeem, Arif O Khan, Saif Al Obaisi, Muhammad Asif Naeem, Idrees A Nasir, Shaheen N Khan, Tayyab Husnain, Sheikh Riazuddin, Javed Akram, Allen O Eghrari, and S Amer Riazuddin

Subjects

Medicine, Science

Abstract

To identify the molecular basis of non-syndromic autosomal recessive congenital cataracts (arCC) in a consanguineous family.All family members participating in the study received a comprehensive ophthalmic examination to determine their ocular phenotype and contributed a blood sample, from which genomic DNA was extracted. Available medical records and interviews with the family were used to compile the medical history of the family. The symptomatic history of the individuals exhibiting cataracts was confirmed by slit-lamp biomicroscopy. A genome-wide linkage analysis was performed to localize the disease interval. The candidate gene, LIM2 (lens intrinsic membrane protein 2), was sequenced bi-directionally to identify the disease-causing mutation. The physical changes caused by the mutation were analyzed in silico through homology modeling, mutation and bioinformatic algorithms, and evolutionary conservation databases. The physiological importance of LIM2 to ocular development was assessed in vivo by real-time expression analysis of Lim2 in a mouse model.Ophthalmic examination confirmed the diagnosis of nuclear cataracts in the affected members of the family; the inheritance pattern and cataract development in early infancy indicated arCC. Genome-wide linkage analysis localized the critical interval to chromosome 19q with a two-point logarithm of odds (LOD) score of 3.25. Bidirectional sequencing identified a novel missense mutation, c.233G>A (p.G78D) in LIM2. This mutation segregated with the disease phenotype and was absent in 192 ethnically matched control chromosomes. In silico analysis predicted lower hydropathicity and hydrophobicity but higher polarity of the mutant LIM2-encoded protein (MP19) compared to the wild-type. Moreover, these analyses predicted that the mutation would disrupt the secondary structure of a transmembrane domain of MP19. The expression of Lim2, which was detected in the mouse lens as early as embryonic day 15 (E15) increased after birth to a level that was sustained through the postnatal time points.A novel missense mutation in LIM2 is responsible for autosomal recessive congenital cataracts.

Published

2016

37. Missense Mutations in CRYAB Are Liable for Recessive Congenital Cataracts.

Author

Xiaodong Jiao, Shahid Y Khan, Bushra Irum, Arif O Khan, Qiwei Wang, Firoz Kabir, Asma A Khan, Tayyab Husnain, Javed Akram, Sheikh Riazuddin, J Fielding Hejtmancik, and S Amer Riazuddin

Subjects

Medicine, Science

Abstract

This study was initiated to identify causal mutations responsible for autosomal recessive congenital cataracts in consanguineous familial cases.Affected individuals underwent a detailed ophthalmological and clinical examination, and slit-lamp photographs were ascertained for affected individuals who have not yet been operated for the removal of the cataractous lens. Blood samples were obtained, and genomic DNA was extracted from white blood cells. A genome-wide scan was completed with short tandem repeat (STR) markers, and the logarithm of odds (LOD) scores were calculated. Protein coding exons of CRYAB were sequenced, bi-directionally. Evolutionary conservation was investigated by aligning CRYAB orthologues, and the expression of Cryab in embryonic and postnatal mice lens was investigated with TaqMan probe.The clinical and ophthalmological examinations suggested that all affected individuals had nuclear cataracts. Genome-wide linkage analysis suggested a potential region on chromosome 11q23 harboring CRYAB. DNA sequencing identified a missense variation: c.34C>T (p.R12C) in CRYAB that segregated with the disease phenotype in the family. Subsequent interrogation of our entire cohort of familial cases identified a second familial case localized to chromosome 11q23 harboring a c.31C>T (p.R11C) mutation. In silico analyses suggested that the mutations identified in familial cases, p.R11C and p.R12C will not be tolerated by the three-dimensional structure of CRYAB. Real-time PCR analysis identified the expression of Cryab in mouse lens as early as embryonic day 15 (E15) that increased significantly until postnatal day 6 (P6) with steady level of expression thereafter.Here, we report two novel missense mutations, p.R11C and p.R12C, in CRYAB associated with autosomal recessive congenital nuclear cataracts.

Published

2015

38. Investigating the Molecular Basis of Retinal Degeneration in a Familial Cohort of Pakistani Decent by Exome Sequencing.

Author

Bruno Maranhao, Pooja Biswas, Alexander D H Gottsch, Mili Navani, Muhammad Asif Naeem, John Suk, Justin Chu, Sheen N Khan, Rachel Poleman, Javed Akram, Sheikh Riazuddin, Pauline Lee, S Amer Riazuddin, J Fielding Hejtmancik, and Radha Ayyagari

Subjects

Medicine, Science

Abstract

PURPOSE:To define the molecular basis of retinal degeneration in consanguineous Pakistani pedigrees with early onset retinal degeneration. METHODS:A cohort of 277 individuals representing 26 pedigrees from the Punjab province of Pakistan was analyzed. Exomes were captured with commercial kits and sequenced on an Illumina HiSeq 2500. Candidate variants were identified using standard tools and analyzed using exomeSuite to detect all potentially pathogenic changes in genes implicated in retinal degeneration. Segregation analysis was performed by dideoxy sequencing and novel variants were additionally investigated for their presence in ethnicity-matched controls. RESULTS:We identified a total of nine causal mutations, including six novel variants in RPE65, LCA5, USH2A, CNGB1, FAM161A, CERKL and GUCY2D as the underlying cause of inherited retinal degenerations in 13 of 26 pedigrees. In addition to the causal variants, a total of 200 variants each observed in five or more unrelated pedigrees investigated in this study that were absent from the dbSNP, HapMap, 1000 Genomes, NHLBI ESP6500, and ExAC databases were identified, suggesting that they are common in, and unique to the Pakistani population. CONCLUSIONS:We identified causal mutations associated with retinal degeneration in nearly half of the pedigrees investigated in this study through next generation whole exome sequencing. All novel variants detected in this study through exome sequencing have been cataloged providing a reference database of variants common in, and unique to the Pakistani population.

Published

2015

39. MARVELD2 (DFNB49) mutations in the hearing impaired Central European Roma population--prevalence, clinical impact and the common origin.

Author

Ivica Mašindová, Andrea Šoltýsová, Lukáš Varga, Petra Mátyás, Andrej Ficek, Miloslava Hučková, Martina Sůrová, Dana Šafka-Brožková, Saima Anwar, Judit Bene, Slavomír Straka, Ingrid Janicsek, Zubair M Ahmed, Pavel Seeman, Béla Melegh, Milan Profant, Iwar Klimeš, Saima Riazuddin, Ľudevít Kádasi, and Daniela Gašperíková

Subjects

Medicine, Science

Abstract

In the present study we aimed: 1) To establish the prevalence and clinical impact of DFNB49 mutations in deaf Roma from 2 Central European countries (Slovakia and Hungary), and 2) to analyze a possible common origin of the c.1331+2T>C mutation among Roma and Pakistani mutation carriers identified in the present and previous studies.We sequenced 6 exons of the MARVELD2 gene in a group of 143 unrelated hearing impaired Slovak Roma patients. Simultaneously, we used RFLP to detect the c.1331+2T>C mutation in 85 Hungarian deaf Roma patients, control groups of 702 normal hearing Romanies from both countries and 375 hearing impaired Slovak Caucasians. We analyzed the haplotype using 21 SNPs spanning a 5.34Mb around the mutation c.1331+2T>C.One pathogenic mutation (c.1331+2T>C) was identified in 12 homozygous hearing impaired Roma patients. Allele frequency of this mutation was higher in Hungarian (10%) than in Slovak (3.85%) Roma patients. The identified common haplotype in Roma patients was defined by 18 SNP markers (3.89 Mb). Fourteen common SNPs were also shared among Pakistani and Roma homozygotes. Biallelic mutation carriers suffered from prelingual bilateral moderate to profound sensorineural hearing loss.We demonstrate different frequencies of the c.1331+2T>C mutation in hearing impaired Romanies from 3 Central European countries. In addition, our results provide support for the hypothesis of a possible common ancestor of the Slovak, Hungarian and Czech Roma as well as Pakistani deaf patients. Testing for the c.1331+2T>C mutation may be recommended in GJB2 negative Roma cases with early-onset sensorineural hearing loss.

Published

2015

40. Correction: A Novel C-Terminal CIB2 (Calcium and Integrin Binding Protein 2) Mutation Associated with Non-Syndromic Hearing Loss in a Hispanic Family.

Author

Kunjan Patel, Arnaud P Giese, J M Grossheim, Rashmi S Hegde, Maria Delio, Joy Samanich, Saima Riazuddin, Gregory I Frolenkov, Jinlu Cai, Zubair M Ahmed, and Bernice E Morrow

Subjects

Medicine, Science

Published

2015

41. Radioprotective Effect of Aminothiol PrC-210 on Irradiated Inner Ear of Guinea Pig.

Author

Arnaud P J Giese, Jess G Guarnaschelli, Jonette A Ward, Daniel I Choo, Saima Riazuddin, and Zubair M Ahmed

Subjects

Medicine, Science

Abstract

Radiotherapy of individuals suffering with head & neck or brain tumors subserve the risk of sensorineural hearing loss. Here, we evaluated the protective effect of Aminothiol PrC-210 (3-(methyl-amino)-2-((methylamino)methyl)propane-1-thiol) on the irradiated inner ear of guinea pigs. An intra-peritoneal or intra-tympanic dose of PrC-210 was administered prior to receiving a dose of gamma radiation (3000 cGy) to each ear. Auditory Brainstem Responses (ABRs) were recorded one week and two weeks after the radiation and compared with the sham animal group. ABR thresholds of guinea pigs that received an intra-peritoneal dose of PrC-210 were significantly better compared to the non-treated, control animals at one week post-radiation. Morphologic analysis of the inner ear revealed significant inflammation and degeneration of the spiral ganglion in the irradiated animals not treated with PrC-210. In contrast, when treated with PrC-210 the radiation effect and injury to the spiral ganglion was significantly alleviated. PrC-210 had no apparent cytotoxic effect in vivo and did not affect the morphology or count of cochlear hair cells. These findings suggest that aminothiol PrC-210 attenuated radiation-induced cochlea damage for at least one week and protected hearing.

Published

2015

42. A Novel C-Terminal CIB2 (Calcium and Integrin Binding Protein 2) Mutation Associated with Non-Syndromic Hearing Loss in a Hispanic Family.

Author

Kunjan Patel, Arnaud P Giese, J M Grossheim, Rashmi S Hegde, Maria Delio, Joy Samanich, Saima Riazuddin, Gregory I Frolenkov, Jinlu Cai, Zubair M Ahmed, and Bernice E Morrow

Subjects

Medicine, Science

Abstract

Hearing loss is a complex disorder caused by both genetic and environmental factors. Previously, mutations in CIB2 have been identified as a common cause of genetic hearing loss in Pakistani and Turkish populations. Here we report a novel (c.556C>T; p.(Arg186Trp)) transition mutation in the CIB2 gene identified through whole exome sequencing (WES) in a Caribbean Hispanic family with non-syndromic hearing loss. CIB2 belongs to the family of calcium-and integrin-binding (CIB) proteins. The carboxy-termini of CIB proteins are associated with calcium binding and intracellular signaling. The p.(Arg186Trp) mutation is localized within predicted type II PDZ binding ligand at the carboxy terminus. Our ex vivo studies revealed that the mutation did not alter the interactions of CIB2 with Whirlin, nor its targeting to the tips of hair cell stereocilia. However, we found that the mutation disrupts inhibition of ATP-induced Ca2+ responses by CIB2 in a heterologous expression system. Our findings support p.(Arg186Trp) mutation as a cause for hearing loss in this Hispanic family. In addition, it further highlights the necessity of the calcium binding property of CIB2 for normal hearing.

Published

2015

43. Missense Mutations in CRYAB Are Liable for Recessive Congenital Cataracts.

Author

Jiao X, Khan SY, Irum B, Khan AO, Wang Q, Kabir F, Khan AA, Husnain T, Akram J, Riazuddin S, Hejtmancik JF, and Riazuddin SA

Subjects

Animals, Cataract diagnosis, Cataract genetics, Chromosomes, Human, Pair 11, Computational Biology, Consanguinity, DNA Mutational Analysis, Disease Models, Animal, Evolution, Molecular, Exons, Female, Gene Expression, Genes, Recessive, Genetic Linkage, Haplotypes, Humans, Lod Score, Male, Mice, Microsatellite Repeats, Pedigree, Slit Lamp, alpha-Crystallin B Chain chemistry, Cataract congenital, Mutation, Missense, alpha-Crystallin B Chain genetics

Abstract

Purpose: This study was initiated to identify causal mutations responsible for autosomal recessive congenital cataracts in consanguineous familial cases., Methods: Affected individuals underwent a detailed ophthalmological and clinical examination, and slit-lamp photographs were ascertained for affected individuals who have not yet been operated for the removal of the cataractous lens. Blood samples were obtained, and genomic DNA was extracted from white blood cells. A genome-wide scan was completed with short tandem repeat (STR) markers, and the logarithm of odds (LOD) scores were calculated. Protein coding exons of CRYAB were sequenced, bi-directionally. Evolutionary conservation was investigated by aligning CRYAB orthologues, and the expression of Cryab in embryonic and postnatal mice lens was investigated with TaqMan probe., Results: The clinical and ophthalmological examinations suggested that all affected individuals had nuclear cataracts. Genome-wide linkage analysis suggested a potential region on chromosome 11q23 harboring CRYAB. DNA sequencing identified a missense variation: c.34C>T (p.R12C) in CRYAB that segregated with the disease phenotype in the family. Subsequent interrogation of our entire cohort of familial cases identified a second familial case localized to chromosome 11q23 harboring a c.31C>T (p.R11C) mutation. In silico analyses suggested that the mutations identified in familial cases, p.R11C and p.R12C will not be tolerated by the three-dimensional structure of CRYAB. Real-time PCR analysis identified the expression of Cryab in mouse lens as early as embryonic day 15 (E15) that increased significantly until postnatal day 6 (P6) with steady level of expression thereafter., Conclusion: Here, we report two novel missense mutations, p.R11C and p.R12C, in CRYAB associated with autosomal recessive congenital nuclear cataracts.

Published

2015