Your search keyword '"Neerja Gupta"' showing total 80 results

1. Late onset Pompe Disease in India – Beyond the Caucasian phenotype

Author

Madhulika Kabra, Ratna Dua Puri, Ishwar C. Verma, Sheela Nampoothiri, Katta M. Girisha, Neerja Gupta, Ishpreet K. Biji, Priya S. Kishnani, Mamta N. Muranjan, Sujatha Jagadeesh, N Vinu, Jyotsna Verma, Jayarekha Raja, Ravinder Makkar, Divya C. Thomas, Nitika Setia, and Meenakshi Bhat

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Genotype, Cardiomyopathy, India, Late onset, Disease, Compound heterozygosity, Left ventricular hypertrophy, Cohort Studies, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Missense mutation, Age of Onset, Child, Genetics (clinical), Retrospective Studies, Glycogen Storage Disease Type II, business.industry, Homozygote, Muscle weakness, medicine.disease, Cross-Sectional Studies, Phenotype, 030104 developmental biology, Neurology, Mutation, Pediatrics, Perinatology and Child Health, Cohort, Disease Progression, Female, RNA Splice Sites, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

We evaluated the clinical histories, motor and pulmonary functions, cardiac phenotypes and GAA genotypes of an Indian cohort of twenty patients with late onset Pompe disease (LOPD) in this multi-centre study. A mean age at onset of symptoms and diagnosis of 9.9 ±9.7 years and 15.8 ±12.1 years respectively was identified. All patients had lower extremity limb-girdle muscle weakness. Seven required ventilatory support and seven used mobility assists. Of the four who used both assists, two received ventilatory support prior to wheelchair use. Cardiac involvement was seen in eight patients with various combinations of left ventricular hypertrophy, tricuspid regurgitation, cardiomyopathy,dilated ventricles with biventricular dysfunction and aortic regurgitation. Amongst 20 biochemically diagnosed patients (low residual GAA enzyme activity) GAA genotypes of 19 patients identified homozygous variants in eight and compound heterozygous in 11: 27 missense, 3 nonsense, 2 initiator codon, 3 splice site and one deletion. Nine variants in 7 patients were novel. The leaky Caucasian, splice site LOPD variant, c. −32 −13T > G mutation was absent. This first study from India provides an insight into a more severe LOPD phenotype with earlier disease onset at 9.9 years compared to 33.3 years in Caucasian patients, and cardiac involvement more than previously reported. The need for improvement in awareness and diagnosis of LOPD in India is highlighted

Published

2021

2. Association of Sleep Apnea With Development and Behavior in Down Syndrome: A Prospective Clinical and Polysomnographic Study

Author

Madhulika Kabra, Savita Sapra, Neerja Gupta, Garima Shukla, Anupama Gupta, Shivam Pandey, Vaishakh Anand, Ravindra Mohan Pandey, and Sheffali Gulati

Subjects

Male, Pediatrics, medicine.medical_specialty, Down syndrome, Polysomnography, Child Behavior, CBCL, Comorbidity, Severity of Illness Index, 03 medical and health sciences, Child Development, 0302 clinical medicine, Developmental Neuroscience, 030225 pediatrics, Humans, Medicine, Prospective Studies, Child, Child Behavior Checklist, Prospective cohort study, Sleep Apnea, Obstructive, medicine.diagnostic_test, business.industry, Sleep apnea, medicine.disease, respiratory tract diseases, Obstructive sleep apnea, Neurology, Child, Preschool, Pediatrics, Perinatology and Child Health, Breathing, Female, Neurology (clinical), Down Syndrome, business, 030217 neurology & neurosurgery

Abstract

Background The prevalence of sleep-disordered breathing is high in children with Down syndrome. Although the association between sleep-disordered breathing and developmental delay and behavioral abnormalities are proven among typically developing children, there are few such studies of children with Down syndrome. This study assesses the relationship between the severity of sleep apnea and development and behavioral abnormalities in individuals with Down syndrome. Methods In a cross-sectional prospective study, 53 children with Down syndrome were assessed for sleep-disordered breathing by overnight polysomnography. Behavior was assessed using Child Behavior Checklist (CBCL) and developmental quotient (DQ) using Developmental Profile 3. The association between various domains of behavior and development with the Apnea-Hypopnea Index (AHI) was assessed using Spearman rank correlation. Multiple linear regression assessed the independent effects of various factors on development and behavior. Results Of 53 subjects (three to 11.8 years), 51 (96%) were found to have obstructive sleep apnea (OSA). In both three to five year and six to 12 year age groups, there was a statistically significant positive correlation between the CBCL scores and the AHI (rho = 0.77 and 0.83, respectively). There was a statistically significant negative correlation between the DQ and the AHI (rho = −0.62). In multiple linear regression, AHI was the only independent variable that was associated with CBCL and DQ. Conclusions This study provides robust evidence that OSA can negatively influence the development and behavior in children with Down syndrome as in typically developing children. Moreover, with increasing severity of OSA, children with Down syndrome have more behavioral abnormalities, especially attention deficit and hyperactivity, and also have poorer development scores.

Published

2021

3. Spectrum of amyloglucosidase mutations in Asian Indian patients with Glycogen storage disease type III

Author

Neerja Gupta, Manoj Kumar, Punit Kaur, Madhumita Roy Chowdhury, Madhulika Kabra, and Shama Perveen

Subjects

Male, Biology, medicine.disease_cause, Glycogen storage disease type III, Glycogen debranching enzyme, Glycogen Storage Disease Type III, Exon, chemistry.chemical_compound, Asian People, Gene Frequency, Genetics, medicine, Humans, Missense mutation, Genetic Predisposition to Disease, Allele, Child, Allele frequency, Alleles, Genetics (clinical), Mutation, Glycogen, Exons, medicine.disease, Liver, chemistry, Child, Preschool, Female, Glucan 1,4-alpha-Glucosidase

Abstract

Glycogen storage disease type III (GSD III) is a rare autosomal recessive inborn error of glycogen degradation pathway due to deficiency or reduced activity of glycogen debranching enzyme (GDE) that results in accumulation of abnormal glycogen in the liver, muscle, and heart. The cardinal hallmarks are hepatomegaly, fasting hypoglycemia, seizures, growth retardation, progressive skeletal myopathy, and cardiomyopathy in few. To date, 258 mutations in amyloglucosidase (AGL) gene have been identified worldwide. However, the mutation spectrum in the Asian Indian region is yet to be well characterized. We investigated 24 patients of Asian origin from 21 unrelated families with a provisional diagnosis of GSD III based on clinical and biochemical criteria. Molecular diagnosis was assessed by bidirectional sequencing and the impact of novel missense variants on the tertiary (three-dimensional) structure of GDE was evaluated by molecular modeling approach. Eighteen different pathogenic variants were identified, out of which 78% were novel. Novel variants included five nonsense, three small duplications and two small deletions, a splice site variant, and three missense variants. Variations in Exons 4, 14, 19, 24, 27, and 33 accounted for 61% of the total pathogenic variants identified and Allele p.Gly798Alafs*3 showed a high allele frequency of 11%. Molecular modeling study of novel pathogenic missense variants indicated the probable underlying molecular mechanism of adverse impact of variations on the structure and catalytic function of human GDE. Our study is the first large study on GSD III from the Asian subcontinent, which further expands the mutation spectrum of AGL.

Published

2020

4. Newborn Screening and Diagnosis of Infants with Congenital Adrenal Hyperplasia

Author

Seema Kapoor, Neerja Gupta, B.K. Thelma, Rajni Sharma, Aashima Dabas, Sunil Kumar Polipalli, Vandana Jain, Preeti Singh, Prerna Batra, Pallavi Vats, Ravindra Kumar, Madhulika Kabra, Sangeeta Yadav, and Anju Seth

Subjects

Male, Pediatrics, medicine.medical_specialty, Hydrocortisone, Genetic counseling, Fluorescent Antibody Technique, Genetic Counseling, Prenatal diagnosis, 03 medical and health sciences, Neonatal Screening, 0302 clinical medicine, Tandem Mass Spectrometry, 030225 pediatrics, Pediatric surgery, Humans, Medicine, Congenital adrenal hyperplasia, 030212 general & internal medicine, Genetic testing, Pregnancy, Newborn screening, Adrenal Hyperplasia, Congenital, medicine.diagnostic_test, business.industry, 17-alpha-Hydroxyprogesterone, Infant, Newborn, Gestational age, medicine.disease, Pediatrics, Perinatology and Child Health, Female, Dried Blood Spot Testing, business

Abstract

Congenital adrenal hyperplasia (CAH) is an autosomal recessive endocrine disorder which can manifest after birth with ambiguous genitalia and salt-wasting crisis. However, genital ambiguity is not seen in male babies and may be mild in female babies, leading to a missed diagnosis of classical CAH at birth. In this review, we provide a standard operating protocol for routine newborn screening for CAH in Indian settings. A standardization of first tier screening tests with a single consistent set of cut-off values stratified by gestational age is also suggested. The protocol also recommends a two-tier protocol of initial immunoassay/time resolved fluoroimmunoassay followed by liquid chromatography tandem mass spectrometry for confirmation of screen positive babies, wherever feasible. Routine molecular and genetic testing is not essential for establishing the diagnosis in all screen positive babies, but has significant utility in prenatal diagnosis and genetic counseling for future pregnancy.

Published

2020

5. Post-mortem MRI in stillbirth: Normal imaging appearances

Author

Neerja Gupta, Amit Gupta, Atin Kumar, Madhulika Kabra, Raju Sharma, Arun Kumar Gupta, and Manisha Jana

Subjects

Fetus, Pregnancy, Humans, Radiology, Nuclear Medicine and imaging, Female, General Medicine, Autopsy, Stillbirth, Fetal Death, Magnetic Resonance Imaging

Abstract

Post-mortem MRI (PMMRI) can reliably detect most major organ malformations in cases of stillbirth. However, variable normal post-mortem changes mimicking pathology make the interpretation difficult. Varying morphological appearances of internal organs could be due to differences in gestational age of the fetuses being evaluated or the presence of maceration changes which occur after fetal demise in-utero. Final differentiation and detection of abnormality require a close interaction and inputs from the geneticist regarding clinical examination of the fetus and thorough evaluation of intranatal imaging records. With the increasing use of PMMRI in cases of fetal demise, it is prudent for the radiologists to be aware of normal post-mortem findings to avoid misdiagnosis.

Published

2021

6. Skeletal abnormalities are common features in Aymé‐Gripp syndrome

Author

Bruno Dallapiccola, Carlos Ruggiero, Fermina López-Grondona, Domenico Barbuti, Marcello Niceta, Giuseppe Zampino, Eduardo F. Tizzano, Christiane Zweier, Emilia Stellacci, Luitgard Graul-Neumann, Paula Fernández-Álvarez, Neerja Gupta, Marco Tartaglia, Andreas Tzschach, Gen Nishimura, Chiara Leoni, Andrea Del Fattore, Irene Valenzuela, and Sabina Barresi

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Hearing Loss, Sensorineural, Long bone, Mutation, Missense, bone defects, skeletal dysplasia, 030105 genetics & heredity, Cataract, AYME-GRIPP SYNDROME, Young Adult, 03 medical and health sciences, Intellectual Disability, Intellectual disability, Genetics, medicine, Humans, Missense mutation, Genetic Predisposition to Disease, Child, Growth Disorders, Genetics (clinical), Hip dysplasia, MAF, Aymé-Gripp syndrome, business.industry, Facies, Infant, medicine.disease, Dermatology, Musculoskeletal Abnormalities, 030104 developmental biology, medicine.anatomical_structure, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Child, Preschool, Proto-Oncogene Proteins c-maf, Congenital cataracts, Female, Sensorineural hearing loss, Skeletal abnormalities, business

Abstract

Aymé-Gripp syndrome (AYGRPS) is a recognizable condition caused by a restricted spectrum of dominantly acting missense mutations affecting the transcription factor MAF. Major clinical features of AYGRPS include congenital cataracts, sensorineural hearing loss, intellectual disability, and a distinctive flat facial appearance. Skeletal abnormalities have also been observed in affected individuals, even though these features have not been assessed systematically. Expanding the series with four additional patients, here we provide a more accurate delineation of the molecular aspects and clinical phenotype, particularly focusing on the skeletal features characterizing this disorder. Apart from previously reported malar flattening and joint limitations, we document that carpal/tarsal and long bone defects, and hip dysplasia occur in affected subjects more frequently than formerly appreciated.

Published

2019

7. Functional characterization of novel variants in SMPD1 in Indian patients with acid sphingomyelinase deficiency

Author

Prajnya Ranganath, Ashwin Dalal, Akash Ranjan, S Jamal Md Nurul Jain, Sunita Bijarnia-Mahay, Dipti Deshpande, Jayesh Sheth, Madhulika Kabra, Shagun Aggarwal, Katta M. Girisha, Asodu Sandeep Sarma, Kausik Mandal, Mehul Mistri, Mamta N. Muranjan, Preetha Tilak, Naresh B. Tayade, Ratna Dua Puri, Neerja Gupta, A Radha Rama Devi, Shailesh Kumar Gupta, Shubha R. Phadke, and Chaitanya Datar

Subjects

medicine.medical_specialty, In silico, Biology, symbols.namesake, Pregnancy, Genetics, Lysosomal storage disease, medicine, Missense mutation, Humans, Child, Genetics (clinical), Sanger sequencing, Niemann-Pick Diseases, Molecular pathology, Exons, Niemann-Pick Disease, Type A, medicine.disease, HEK293 Cells, Sphingomyelin Phosphodiesterase, Mutation, symbols, Medical genetics, Female, Acid sphingomyelinase, Niemann–Pick disease, medicine.drug

Abstract

Pathogenic variations in SMPD1 lead to acid sphingomyelinase deficiency (ASMD), that is, Niemann-Pick disease (NPD) type A and B (NPA, NPB), which is a recessive lysosomal storage disease. The knowledge of variant spectrum in Indian patients is crucial for early and accurate NPD diagnosis and genetic counseling of families. In this study, we recruited 40 unrelated pediatric patients manifesting symptoms of ASMD and subnormal ASM enzyme activity. Variations in SMPD1 were studied using Sanger sequencing for all exons, followed by interpretation of variants based on American College of Medical Genetics and Genomics & Association for Molecular Pathology (ACMG/AMP) criteria. We identified 18 previously unreported variants and 21 known variants, including missense, nonsense, deletions, duplications, and splice site variations with disease-causing potential. Eight missense variants were functionally characterized using in silico molecular dynamic simulation and in vitro transient transfection in HEK293T cells, followed by ASM enzyme assay, immunoblot, and immunofluorescence studies. All the variants showed reduced ASM activity in transfected cells confirming their disease-causing potential. The study provides data for efficient prenatal diagnosis and genetic counseling of families with NPD type A and B.

Published

2021

8. Utility of fetal whole exome sequencing in the etiological evaluation and outcome of nonimmune hydrops fetalis

Author

Ramesh Agarwal, Madhulika Kabra, Kamal Naini, Alec Reginald Errol Correa, Vatsla Dadhwal, Pallavi Mishra, Neerja Gupta, and Rashmi Shukla

Subjects

Adult, medicine.medical_specialty, Hydrops Fetalis, Aneuploidy, India, Consanguinity, Cohort Studies, Fetus, Predictive Value of Tests, Pregnancy, Hydrops fetalis, Exome Sequencing, medicine, Humans, Prospective Studies, Prospective cohort study, Genetics (clinical), Exome sequencing, Obstetrics, business.industry, Obstetrics and Gynecology, medicine.disease, RAPSN, Cohort, Etiology, Female, business

Abstract

Introduction Nonimmune hydrops fetalis (NIHF) has varied etiology. We assessed the etiological spectrum and evaluated the utility of fetal whole exome sequencing (fWES) for the diagnosis of NIHF. Methods In this prospective cohort study, we evaluated antenatally diagnosed fetuses with NIHF between July 2018 and December 2019 according to the routine diagnostic algorithm. Fetuses that remained undiagnosed after routine NIHF workup were subjected to fetal chromosomal microarray and/or WES. Pregnancies were followed up for clinical outcomes. Results Of the 45 fetuses, consanguinity and recurrent hydrops fetalis were observed in 13.3% (6/45) and 28.8% (13/45), respectively. Overall, an etiological diagnosis was possible in 75.5% (34/45) of fetuses, while the cause remained unknown in 24.4% (11/45). A genetic etiology was identified in 46.6% (21/45): aneuploidy and monogenic disorders in 28.8% (13/45) and 17.8% (8/45), respectively. fWES on 19 fetuses detected disease-causing variants in 42.1% (8/19). Nine novel variants were detected in RAPSN, ASCC1, NEB, PKD1L1, GUSB, and PIEZO1. Only 8.8% (4/45) of the cohort survived without morbidity. Conclusions This study describes the etiological spectrum and the disease-causing variants in an Indian cohort of hydropic fetuses.

Published

2021

9. Combined Methylmalonic Aciduria and Homocystinuria Presenting as Pulmonary Hypertension

Author

Madhulika Kabra, Neerja Gupta, and A. Gupta

Subjects

medicine.medical_specialty, Hypertension, Pulmonary, Homocystinuria, Compound heterozygosity, Cobalamin, Gastroenterology, chemistry.chemical_compound, Internal medicine, medicine, Humans, Amino Acid Metabolism, Inborn Errors, business.industry, Metabolic disorder, Infant, Vitamin B 12 Deficiency, medicine.disease, MMACHC, Pulmonary hypertension, Vitamin B 12, Methylmalonic aciduria, chemistry, Pediatrics, Perinatology and Child Health, Mutation, Female, CBLC, business, Oxidoreductases

Abstract

Combined methylmalonic aciduria and homocystinuria, cblC type, (MAHCC) is a rare autosomal recessive metabolic disorder of remethylation caused due to mutations in the MMACHC (metabolism of cobalamin associated C) gene with predominant neurological involvement. Microvascular, renal, and cardiovascular complications are also known to occur. However, the disease presenting primarily with a cardiovascular phenotype without any neurological involvement is a rare entity. We report a case of developmentally normal 23-mo-old female child, who presented with pulmonary arterial hypertension (PAH) and succumbed to cardiac failure. Extensive workup for PAH was inconclusive. Posthumous trio whole-exome sequencing revealed pathogenic compound heterozygous variants in the MMACHC. Diagnosis of MAHCC should be considered as a differential diagnosis for unexplained PAH in children. An elevated plasma homocysteine level can serve as a simple screening modality for this disorder. Accurate diagnosis has paramount therapeutic implications, as management with hydroxocobalamin and betaine may lead to partial or complete remission of PAH in these patients.

Published

2021

10. 50 Years Ago in TheJournalofPediatrics: Syndromic Intellectual Disability: A Never-Ending Genomic Odyssey

Author

Mounika, Endrakanti, Neerja, Gupta, and Piyush, Gupta

Subjects

Genetic Markers, Phenotype, Intellectual Disability, Humans, Female, Genetic Testing, Genomics, Syndrome, Oligonucleotide Array Sequence Analysis

Published

2021

11. Phenotypic and genotypic spectrum of CTSK variants in a cohort of twenty-five Indian patients with pycnodysostosis

Author

Deepti Saxena, Haseena Sait, Prajnya Ranganath, Priyanka Srivastava, Seema Kapoor, Madhulika Kabra, Ashwin Dalal, Ajitesh Roy, Kausik Mandal, Shubha R. Phadke, Neerja Gupta, Ikrormi Rungsung, and Jayalakshmi Pabbati

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Pycnodysostosis, Cathepsin K, Hepatosplenomegaly, Consanguinity, 030105 genetics & heredity, Short stature, Frameshift mutation, Cohort Studies, 03 medical and health sciences, symbols.namesake, Gene Frequency, Internal medicine, Genotype, Genetics, medicine, Humans, Family history, Child, Genetics (clinical), Sanger sequencing, business.industry, Homozygote, General Medicine, medicine.disease, 030104 developmental biology, Phenotype, Mutation, symbols, Female, medicine.symptom, business

Abstract

Background Pycnodysostosis is an autosomal recessive skeletal dysplasia with easily recognizable clinical features and marked molecular heterogeneity. In this study, we explored the clinical and molecular spectrum of 25 Indian patients with pycnodysostosis from 20 families. Methods Clinical information was collected on a predesigned clinical proforma. Sanger method was employed to sequence all the exons and exon/intron boundaries of the CTSK gene. Novel variants were systematically assessed by prediction softwares and protein modelling. The pathogenicity of variant was established based on ACMG-AMP criteria. An attempt was also made to establish a genotype-phenotype correlation and devise a diagnostic scoring system based on clinical and radiological findings. Results Consanguinity and positive family history were present in 65% (13/20) and 45% (9/20) of the families respectively. Short stature and fractures were the predominant presenting complaints and was evident in 96% (24/25) and 32% (8/25) of affected individuals respectively. Gestalt facial phenotype and acro-osteolysis were present in 76% (19/25) and 82.6% (19/23) of the individuals respectively. Hepatosplenomegaly was present in 15% (3/20) of the individuals with one of them having severe anaemia. Causative sequence variations were identified in all of them. A total of 19 variants were identified from 20 families amongst which 10 were novel. Homozygous variants were identified in 90% (18/20) families. Amongst the novel variants, there was a considerable proportion (40%) of frameshift variants (4/10). No significant genotype-phenotype correlation was noted. Scoring based on clinical and radiological findings led to the proposal that a minimum of 2 scores in each category is required in addition to high bone density to diagnose pycnodysostosis with certainty. Conclusion This study delineated the genotypic and phenotypic characterisation of Indian patients with pycnodysostosis with identification of 10 novel variants. We also attempted to develop a clinically useful diagnostic scoring system which requires further validation.

Published

2020

12. Rubinstein-Taybi syndrome in diverse populations

Author

Leah Dowsett, Omar A. Abdul-Rahman, Kelly L. Jones, Nicole Fleischer, Leon Mutesa, Babajide Owosela, María Gabriela Obregon, Victoria Huckstadt, Ebenezer Badoe, Bryan Malonga, Ekanem N. Ekure, Neerja Gupta, Ho Ming Luk, Gerarda Cappuccio, Engy A. Ashaat, Alicia Diaz-Kuan, Mona O. El Ruby, Jasmine L.F. Fung, Paul Kruszka, Stephanie Lotz-Esquivel, Nirmala D. Sirisena, Monica Penon Portmann, Carolyn Sian Kitchin, Cedrik Tekendo-Ngongang, Ifeanyi Kanayo Ifeorah, Meow-Keong Thong, Annette Uwineza, Sansan Lee, Yonit A. Addissie, Brian H.Y. Chung, Ivan F M Lo, Dalia Farouk Hussen, Angélica Moresco, Vajira H. W. Dissanayake, Maximilian Muenke, Nicola Brunetti-Pierri, Eloise J. Prijoles, Ramses Badilla-Porras, Roger E. Stevenson, Leticia Cassimiro Batista, Manuel Saborio-Rocafort, Danilo Moretti-Ferreira, Arianne Llamos Paneque, Tekendo-Ngongang, Cedrik, Owosela, Babajide, Fleischer, Nicole, Addissie, Yonit A, Malonga, Bryan, Badoe, Ebenezer, Gupta, Neerja, Moresco, Angélica, Huckstadt, Victoria, Ashaat, Engy A, Hussen, Dalia Farouk, Luk, Ho-Ming, Lo, Ivan F M, Hon-Yin Chung, Brian, Fung, Jasmine L F, Moretti-Ferreira, Danilo, Batista, Letícia Cassimiro, Lotz-Esquivel, Stephanie, Saborio-Rocafort, Manuel, Badilla-Porras, Ramse, Penon Portmann, Monica, Jones, Kelly L, Abdul-Rahman, Omar A, Uwineza, Annette, Prijoles, Eloise J, Ifeorah, Ifeanyi Kanayo, Llamos Paneque, Arianne, Sirisena, Nirmala D, Dowsett, Leah, Lee, Sansan, Cappuccio, Gerarda, Kitchin, Carolyn Sian, Diaz-Kuan, Alicia, Thong, Meow-Keong, Obregon, María Gabriela, Mutesa, Leon, Dissanayake, Vajira H W, El Ruby, Mona O, Brunetti-Pierri, Nicola, Ekure, Ekanem Nsikak, Stevenson, Roger E, Muenke, Maximilian, Kruszka, Paul, The National Institutes of Health, FDNA Inc., College of Health Sciences, All India Institute of Medical Sciences, Hospital de Pediatría Garrahan, National Research Centre, Hong Kong Special Administrative Region, Universidade Estadual Paulista (Unesp), Hospital San Juan de Dios (CCSS), National Children's Hospital Dr. Carlos Sáenz Herrera (CCSS), University of California San Francisco, Children's Hospital of The King's Daughters, University of Nebraska Medical Center, University of Rwanda, Greenwood Genetic Center, Nigerian Air Force, School of Dentistry, University of Colombo, Kapi'olani Medical Center and University of Hawai'i, Federico II University, Telethon Institute of Genetics and Medicine (TIGEM), University of Cape Town, Instituto de Medicina Genética, University of Malaya, University of Lagos, and American College of Medical Genetics and Genomics

Subjects

Adult, Male, Rubinstein–Taybi syndrome, Pediatrics, medicine.medical_specialty, Asia, Adolescent, Population, facial analysis technology, Physical examination, African Group, European descent, Cohort Studies, Middle East, Young Adult, Intellectual disability, Genetics, medicine, Ethnicity, Humans, Craniofacial, education, Child, Genetics (clinical), Genetic Association Studies, Rubinstein-Taybi Syndrome, education.field_of_study, medicine.diagnostic_test, Receiver operating characteristic, business.industry, Infant, International Agencies, Middle Aged, medicine.disease, Prognosis, Latin America, Genetics, Population, Case-Control Studies, Child, Preschool, Face, Africa, Mutation, Female, business, E1A-Associated p300 Protein

Abstract

Made available in DSpace on 2021-06-25T10:11:48Z (GMT). No. of bitstreams: 0 Previous issue date: 2020-12-01 National Human Genome Research Institute Rubinstein–Taybi syndrome (RSTS) is an autosomal dominant disorder, caused by loss-of-function variants in CREBBP or EP300. Affected individuals present with distinctive craniofacial features, broad thumbs and/or halluces, and intellectual disability. RSTS phenotype has been well characterized in individuals of European descent but not in other populations. In this study, individuals from diverse populations with RSTS were assessed by clinical examination and facial analysis technology. Clinical data of 38 individuals from 14 different countries were analyzed. The median age was 7 years (age range: 7 months to 47 years), and 63% were females. The most common phenotypic features in all population groups included broad thumbs and/or halluces in 97%, convex nasal ridge in 94%, and arched eyebrows in 92%. Face images of 87 individuals with RSTS (age range: 2 months to 47 years) were collected for evaluation using facial analysis technology. We compared images from 82 individuals with RSTS against 82 age- and sex-matched controls and obtained an area under the receiver operating characteristic curve (AUC) of 0.99 (p

Published

2020

13. Identification and characterization of 30 novel pathogenic variations in 69 unrelated Indian patients with Mucolipidosis Type II and Type III

Author

Divya, Pasumarthi, Neerja, Gupta, Jayesh, Sheth, S Jamal Md Nurul, Jain, Ikrormi, Rungsung, Madhulika, Kabra, Prajnya, Ranganath, Shagun, Aggarwal, Shubha R, Phadke, Katta M, Girisha, Anju, Shukla, Chaitanya, Datar, Ishwar C, Verma, Ratna Dua, Puri, Riddhi, Bhavsar, Mehul, Mistry, V H, Sankar, Kalpana, Gowrishankar, Divya, Agrawal, Mohandas, Nair, Sumita, Danda, Jai Prakash, Soni, and Ashwin, Dalal

Subjects

Adult, Male, Mannosephosphates, Adolescent, Genotype, Mutation, Missense, India, Transferases (Other Substituted Phosphate Groups), Exons, Young Adult, Asian People, Mucolipidoses, Child, Preschool, Gene Duplication, Humans, Protein Isoforms, Female, Child, Frameshift Mutation, Lysosomes, Gene Deletion

Abstract

Mucolipidosis (ML) (OMIM 607840607838) is a rare autosomal recessive inherited disorder that occurs due to the deficiency of golgi enzyme uridine diphosphate (UDP)- N-acetylglucosamine-1-phosphotransferase (GlcNAc-phosphotransferase) responsible for tagging mannose-6-phosphate for proper trafficking of lysosomal enzymes to lysosomes. Variants in GlcNAc-phosphotransferase (GNPTAB (α, β subunits) and GNPTG (γ subunits) are known to result in impaired targeting of lysosomal enzymes leading to Mucolipidosis (ML) Type II or Type III. We analyzed 69 Indian families of MLII/III for clinical features and molecular spectrum and performed in silico analysis for novel variants. We identified 38 pathogenic variants in GNPTAB and 5 pathogenic variants in GNPTG genes including missense, frame shift, deletion, duplication and splice site variations. A total of 26 novel variants were identified in GNPTAB and 4 in GNPTG gene. In silico studies using mutation prediction software like SIFT, Polyphen2 and protein structure analysis further confirmed the pathogenic nature of the novel sequence variants detected in our study. Except for a common variant c.3503_3504delTC in early onset MLII, we could not establish any other significant genotype and phenotype correlation. This is one of the largest studies reported till date on Mucolipidosis II/III in order to identify mutation spectrum and any recurrent mutations specific to the Indian ethnic population. The mutational spectrum information in Indian patients will be useful in better genetic counselling, carrier detection and prenatal diagnosis for patients with ML II/III.

Published

2020

14. High burden of cardiometabolic risk factors in spouses of Indian women with hyperglycaemia in pregnancy

Author

Neerja Bhatla, Nikhil Tandon, Alpesh Goyal, Neerja Gupta, Seema Singhal, Yashdeep Gupta, and Mani Kalaivani

Subjects

Adult, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Pregnancy in Diabetics, India, 030209 endocrinology & metabolism, Overweight, Prediabetic State, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Pregnancy, Diabetes mellitus, Internal Medicine, medicine, Diabetes Mellitus, Humans, 030212 general & internal medicine, Prediabetes, Obesity, Spouses, Metabolic Syndrome, Obstetrics, business.industry, Cardiometabolic Risk Factors, Odds ratio, medicine.disease, Gestational diabetes, Diabetes, Gestational, Cross-Sectional Studies, Female, medicine.symptom, Metabolic syndrome, business

Abstract

AIM To evaluate the burden and association of cardiometabolic risk factors in the spouses of women with and without hyperglycaemia in pregnancy. METHODS Women with (n = 204) and without (n = 197) hyperglycaemia in pregnancy, along with their spouses, participated in this cross-sectional study. The hyperglycaemia in pregnancy group included women with gestational diabetes and diabetes in pregnancy. A detailed questionnaire was completed for all participants (men and women), documenting relevant personal and medical history, along with biochemical investigations (men). RESULTS A total of 401 couples were evaluated at the time point during the pregnancy of 24.7 ± 5.2 gestational weeks (mean ± sd). Dysglycaemia (prediabetes or diabetes), overweight/obesity (BMI ≥25 kg/m2 ) and metabolic syndrome were detected in 120 (58.9%), 123 (60.3%) and 98 spouses (48.3%) of women with hyperglycaemia in pregnancy, respectively. In the fully adjusted model, an increased risk of dysglycaemia [odds ratio 1.43 (95% CI 0.95-2.17); P = 0.088], overweight/obesity [odds ratio 1.49 (95% CI 0.98-2.27); P = 0.064] and metabolic syndrome [odds ratio 2.00 (95% CI 1.30-3.07); P = 0.001] was seen in the spouses of women with hyperglycaemia in pregnancy. The prevalence of these metabolic conditions was higher in spouses of women with diabetes in pregnancy compared to spouses of women with gestational diabetes mellitus. CONCLUSIONS A high burden of cardiometabolic risk factors was observed in the spouses of women with hyperglycaemia in pregnancy. The opportunity provided by pregnancy could be used by the healthcare system not only to improve the health of the woman and her offspring, but also her spouse.

Published

2020

15. Management of Infants with Congenital Adrenal Hyperplasia

Author

Aashima Dabas, Seema Kapoor, Vandana Jain, Prerna Batra, Ravindra Kumar, Pallavi Vats, Neerja Gupta, Anju Seth, Madhulika Kabra, Preeti Singh, Sangeeta Yadav, and Rajni Sharma

Subjects

Male, medicine.medical_specialty, Pediatrics, endocrine system diseases, Fludrocortisone, Administration, Oral, India, Context (language use), Disease, urologic and male genital diseases, Early initiation, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, 030225 pediatrics, Mineralocorticoids, Pediatric surgery, medicine, Humans, Congenital adrenal hyperplasia, 030212 general & internal medicine, Glucocorticoids, Adrenal Hyperplasia, Congenital, business.industry, Virilization, Infant, medicine.disease, Prenatal Exposure Delayed Effects, Pediatrics, Perinatology and Child Health, Female, Steroids, medicine.symptom, business, medicine.drug

Abstract

Treatment of congenital adrenal hyperplasia (CAH) requires lifelong replacement of glucocorticoids with regular follow up to manage associated morbidities. The current review focuses on follow-up and management of infants diagnosed with classical CAH pertinent to Indian context. Early initiation of oral hydrocortisone in divided doses is recommended after diagnosis in newborn period, infancy and childhood. Fludrocortisone is recommended for all infants with classical CAH. All infants should be monitored as per protocol for disease and treatment related complications. The role of prenatal steroids to pregnant women with previous history of CAH affected infant for prevention of virilization of female fetus is controversial.

Published

2020

16. Turner syndrome in diverse populations

Author

Joanna Y.L. Tung, Katta M. Girisha, Paul Kruszka, Nicole Fleischer, Engy A. Ashaat, E.V. Badoe, Dalia Farouk Hussen, Neer Shoba Chitrakar, Angélica Moresco, Neveen A. Ashaat, Olufemi Fasanmade, Siddaramappa J. Patil, Mona O. El Ruby, André Mégarbané, Johnathan Watts, Karen Fieggen, Gary T. K. Mok, Dhanya Yesodharan, Milagros M. Dueñas-Roque, Ezana Lulseged, Cedrik Tekendo-Ngongang, Sarah Savage, Saumya Shekhar Jamuar, Vajira H. W. Dissanayake, Nirmala D. Sirisena, Sultana M.H. Faradz, Antonio Richieri-Costa, Kelly L. Jones, Jasmine Chew Yin Goh, Brenda C. Iriele, María Beatriz de Herreros, Brian H.Y. Chung, Godfrey Mutashambara Rwegerera, María Gabriela Obregon, Yonit A. Addissie, Nydia Rena Benita Sihombing, Teresa Aravena, Shubha R. Phadke, Victoria Huckstadt, C. Sampath Paththinige, Meow-Keong Thong, Neerja Gupta, Agustini Utari, Sheela Nampoothiri, Elizabeth Eberechi Oyenusi, Ekanem N. Ekure, Maximilian Muenke, Rupesh Mishra, Oluwarotimi Bolaji Olopade, Annette Uwineza, Vorasuk Shotelersuk, and Ambroise Wonkam

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Adolescent, Population, Cubitus valgus, Turner Syndrome, Physical examination, Short stature, Article, White People, Young Adult, Asian People, Turner syndrome, Genetics, medicine, Humans, Abnormalities, Multiple, SÍNDROME DE NOONAN, Child, education, Genetics (clinical), X chromosome, Chromosomes, Human, X, education.field_of_study, medicine.diagnostic_test, business.industry, Noonan Syndrome, Infant, Newborn, Area under the curve, Infant, Hispanic or Latino, Middle Aged, medicine.disease, Phenotype, Child, Preschool, Face, Population Surveillance, Noonan syndrome, Female, medicine.symptom, business, Facial Recognition

Abstract

Turner syndrome (TS) is a common multiple congenital anomaly syndrome resulting from complete or partial absence of the second X chromosome. TS presents with short stature, infertility secondary to ovarian dysgenesis, cardiac and renal anomalies, characteristic exam findings such as cubitus valgus, normal intelligence, and specific neurocognitive profile which includes visual spacial deficits and math difficulties. Clinical studies of TS have predominantly focused on individuals of European descent. In this study, we explore the phenotype of TS in diverse populations using clinical examination and facial analysis technology. Clinical data from 70 individuals and images from 108 individuals with TS from 18 different countries were analyzed. Individuals were grouped into categories of African descent (African), Asian, Latin American, Caucasian (European descent), and Middle Eastern. The most common phenotype features across all population groups were short stature (85%), cubitus valgus (77%) and, low posterior hair line 70%. Other phenotype features found in over half included small mandible (63%), narrow hyperconvex and deep set fingernails (56%), narrow maxilla (53%), and short fourth metacarpals (50%). Congenital heart disease was found in 32% of the cohort. Two facial analysis technology experiments were conducted: TS vs. general population and TS vs. Noonan syndrome. Across all ethnicities, facial analysis was very accurate in diagnosing TS from frontal facial images as measured by the area under the curve (AUC). An AUC of 0.903 (p

Published

2020

17. Molecular Testing of MECP2 Gene in Rett Syndrome Phenotypes in Indian Girls

Author

Shubha R. Phadke, Meenakshi Lallar, Archana Rai, Madhulika Kabra, Kausik Mandal, Priyanka Srivastava, and Neerja Gupta

Subjects

Genetic Markers, 0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Methyl-CpG-Binding Protein 2, DNA Mutational Analysis, India, Rett syndrome, Postnatal microcephaly, MECP2, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Rett Syndrome, medicine, Humans, Atypical Rett syndrome, Genetic Testing, Multiplex ligation-dependent probe amplification, Child, Sequence Deletion, Sanger sequencing, Base Sequence, business.industry, Infant, medicine.disease, Cross-Sectional Studies, Phenotype, 030104 developmental biology, Child, Preschool, Mutation, Pediatrics, Perinatology and Child Health, Mutation (genetic algorithm), symbols, Medical genetics, Female, business, 030217 neurology & neurosurgery

Abstract

OBJECTIVE To assess yield of MECP2 gene sequence variations analysis and large deletions in suspected cases of Rett syndrome. DESIGN Descriptive study. SETTING Tertiary-care medical genetics center. PATIENTS Girls with neuroregression, postnatal microcephaly and signs and symptoms suggestive of classical and atypical Rett syndrome were classified into two groups. Group I consisted of girls with Classical and atypical Rett syndrome on basis on the Revised Rett Syndrome diagnostic criteria, 2010. Group II included girls with neuroregression and postnatal microcephaly and other Rett like features but not fulfilling the above criteria. PROCEDURE Sanger sequencing of coding regions and large deletional analysis of MECP2 gene. OUTCOME MEASURES Identification of mutation in MECP2 gene. RESULTS Mutation in MECP2 gene was identified in 74% (14/19) in group I and none (0/17) in group II. The mutation detection rate was 93% (13/14) in group I classical Rett syndrome girls (2 with large deletions identified with Multiplex ligation dependent probe amplification) and 20% (1/5) in group I atypical Rett syndrome girls. One novel MECP2 sequence variation was identified in group I classical Rett syndrome. CONCLUSIONS The yield of the mutation detection in MECP2 is higher in classical Rett syndrome. In girls with some Rett like features, but not fulfilling revised Rett syndrome diagnostic criteria, mutation testing for MECP2 gene has a low yield.

Published

2018

18. Apert syndrome with congenital diaphragmatic hernia: another case report and review of the literature

Author

Mari Jeeva Sankar, Ravneet Kaur, Puneeta Mishra, Neerja Gupta, Surjeet Kumar, and Madhulika Kabra

Subjects

medicine.medical_specialty, business.industry, Infant, Newborn, MEDLINE, Diaphragmatic breathing, Congenital diaphragmatic hernia, General Medicine, Apert syndrome, Acrocephalosyndactylia, medicine.disease, Pathology and Forensic Medicine, Surgery, Pediatrics, Perinatology and Child Health, Humans, Medicine, Abnormalities, Multiple, Female, Receptor, Fibroblast Growth Factor, Type 2, Anatomy, Hernias, Diaphragmatic, Congenital, business, Genetics (clinical)

Published

2019

19. Homozygosity for a nonsense variant in AIMP2 is associated with a progressive neurodevelopmental disorder with microcephaly, seizures, and spastic quadriparesis

Author

Anju Shukla, Malavika Hebbar, Aneek Das Bhowmik, Katta M. Girisha, K V Rajagopal, Neerja Gupta, and Ashwin Dalal

Subjects

0301 basic medicine, Microcephaly, Pathology, medicine.medical_specialty, Quadriplegia, Corpus callosum, Cisterna magna, 03 medical and health sciences, Neurodevelopmental disorder, Atrophy, Seizures, Genetics, medicine, Humans, Exome, Child, Genetics (clinical), Chromosome 7 (human), business.industry, Cerebrum, Homozygote, Genetic Diseases, Inborn, Nuclear Proteins, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Codon, Nonsense, Neurodevelopmental Disorders, Female, business, Chromosomes, Human, Pair 7

Abstract

We ascertained two unrelated consanguineous families with two affected children each having microcephaly, refractory seizures, intellectual disability, and spastic quadriparesis. Magnetic resonance imaging showed atrophy of cerebrum, cerebellum and spinal cord, prominent cisterna magna, symmetric T2 hypo-intensities in the bilateral basal ganglia and thinning of corpus callosum. Whole-exome sequencing of three affected individuals revealed c.105C>A [p.(Tyr35Ter)] variant in AIMP2. The variant lies in a common homozygous region of 940 kb on chromosome 7 and is likely to have been inherited from a common ancestor. The phenotype noted in our subjects' shares marked similarity with that of hypomyelinating leukodystrophy-3 caused by mutations in closely related gene AIMP1. We hereby report the first human disease associated with deleterious mutations in AIMP2.

Published

2017

20. Asparagine Synthetase deficiency-report of a novel mutation and review of literature

Author

Manoj Kumar, Punit Kaur, Madhulika Kabra, Vishal Vishnu Tewari, Reema Kumar, Vedam Laxmi Ramprasad, Sakthivel Murugan, Neerja Gupta, Aditi Gupta, Pallavi Mishra, Nitika Langeh, and Manisha Jana

Subjects

0301 basic medicine, Microcephaly, Developmental Disabilities, Nonsense mutation, Asparagine synthetase, Biology, Compound heterozygosity, Biochemistry, 03 medical and health sciences, Cellular and Molecular Neuroscience, Exon, 0302 clinical medicine, medicine, Humans, Missense mutation, Exome sequencing, Genetics, Epilepsy, Aspartate-Ammonia Ligase, medicine.disease, 030104 developmental biology, Inborn error of metabolism, Child, Preschool, Mutation, Female, Neurology (clinical), 030217 neurology & neurosurgery

Abstract

Asparagine synthetase deficiency is a rare inborn error of metabolism caused by a defect in ASNS, a gene encoding asparagine synthetase. It manifests with a severe neurological phenotype manifesting as severe developmental delay, congenital microcephaly, spasticity and refractory seizures. To date, nineteen patients from twelve unrelated families have been identified. Majority of the mutations are missense and nonsense mutations in homozygous or compound heterozygous state. We add another case from India which harbored a novel homozygous missense variation in exon 11 and compare the current case with previously reported cases.

Published

2017

21. Epigenetic Abnormalities of 11p15.5 Region in Beckwith-Wiedemann Syndrome - A Report of Eight Indian Cases

Author

Puneeta Mishra, Alec Reginald Errol Correa, Madhulika Kabra, and Neerja Gupta

Subjects

Male, Pathology, medicine.medical_specialty, Beckwith-Wiedemann Syndrome, Genotype, Beckwith–Wiedemann syndrome, India, Epigenesis, Genetic, Abdominal wall, 03 medical and health sciences, Genomic Imprinting, 0302 clinical medicine, Genotype-phenotype distinction, Macroglossia, 030225 pediatrics, medicine, Humans, Epigenetics, Multiplex ligation-dependent probe amplification, Genetic testing, medicine.diagnostic_test, business.industry, Chromosomes, Human, Pair 11, Infant, DNA Methylation, medicine.disease, medicine.anatomical_structure, Phenotype, Pediatrics, Perinatology and Child Health, DNA methylation, Female, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

To report a phenotypic series of eight patients of Beckwith-Wiedemann Syndrome (BWS) with abnormalities of 11p15.5 region to highlight the spectrum of phenotypic manifestations. All the cases were evaluated using Methylation Specific Multiplex Ligation Dependent Probe Amplification (MS-MLPA) of 11p15.5 region to detect the abnormal methylation status of ICR1 (H19DR) and ICR2 (KvDMR) regions. The median age at diagnosis was 5.7 mo (range 1.5–13 mo) with female preponderance. Macroglossia, ear creases and abdominal wall defects were the major features. Hypomethylation at ICR2 and hypermethylation at ICR1 was observed in 6/8 and 2/8 patients respectively. No specific genotype and phenotype correlation was observed. This report highlights the major clinical features of BWS that should prompt pediatricians to offer genetic testing to evaluate the epigenetic abnormalities using MS-MLPA, as it not only helps in appropriate counseling but also provides further guidance about the tumor risk surveillance.

Published

2019

22. Application of chromosomal microarrays in the evaluation of intellectual disability/global developmental delay patients – A study from a tertiary care genetic centre in India

Author

Manju Ghosh, Pankaj Sharma, Madhumita Roy Chowdhury, Sheffali Gulati, Savita Sapra, Madhulika Kabra, and Neerja Gupta

Subjects

Male, 0301 basic medicine, DNA Copy Number Variations, Developmental Disabilities, India, Prenatal diagnosis, 030105 genetics & heredity, Biology, Genome, Tertiary Care Centers, 03 medical and health sciences, Intellectual Disability, mental disorders, Intellectual disability, Genetics, medicine, Humans, Global developmental delay, Copy-number variation, Child, Chromosome Aberrations, Genome, Human, Microarray analysis techniques, Chromosome Mapping, Infant, Chromosome, General Medicine, Microarray Analysis, medicine.disease, Child, Preschool, Etiology, Female

Abstract

Intellectual disability (ID)/Global developmental delay (GDD) is a diverse group of disorders in terms of cognitive and non-cognitive functions and can occur with or without associated co-morbidities. It affects 1–3% of individuals globally and in at least 30–50% of cases the etiology remains unexplained. The widespread use of chromosomal microarray analysis (CMA) in a clinical setting has allowed the identification of submicroscopic copy number variations (CNVs), throughout the genome, associated with neurodevelopmental phenotypes including ID/GDD. In this study we investigated the utility of CMA in the detection of CNVs in 106 patients with unexplained ID/DD, dysmorphism with or without multiple congenital anomalies (MCA). CMA study was carried out using Agilent 8 × 60 K chips and Illumina Human CytoSNP-12 chips. Pathogenic CNVs were found in 15 (14.2%) patients. In these patients, CNVs on single chromosome were detected in 10 patients while 5 patients showed co-occurrence CNVs on two chromosomes. The size of these CNVs ranged between 322 kb to 13 Mb. The yield of pathogenic CNVs was similar for both mild and severe ID/GDD cases. One patient described in this paper is considered to harbour a likely pathogenic CNV with deletion in 17q22 region. Only few cases have been described in literature for 17q22 deletion and patient reported here was found to have an atypical deletion in 17q22 region (Case 90). This study re-affirms the view point that CMA is a powerful diagnostic tool in the evaluation of idiopathic ID/GDD patients irrespective of the degree of severity. Identifying pathogenic CNVs helps in counseling and prenatal diagnosis if desired.

Published

2016

23. Seventeen Novel Mutations in PCCA and PCCB Genes in Indian Propionic Acidemia Patients, and Their Outcomes

Author

Renu Saxena, Roumi Deb, Sunita Bijarnia-Mahay, Neerja Gupta, Yosuke Shigematsu, Ishwar Chander Verma, Deepti Gupta, Madhulika Kabra, Seiji Yamaguchi, Ratna Dua Puri, Osamu Sakamoto, Sudha Kohli, and Seema Thakur

Subjects

Male, 0301 basic medicine, Methylmalonyl-CoA Decarboxylase, Propionic Acidemia, India, 030105 genetics & heredity, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, 03 medical and health sciences, symbols.namesake, Asian People, Polymorphism (computer science), medicine, Humans, Genetic Predisposition to Disease, Propionic acidemia, Allele, Gene, Alleles, Genetics (clinical), Sequence Deletion, G alpha subunit, Genetics, Sanger sequencing, Mutation, Infant, Newborn, Infant, General Medicine, medicine.disease, Protein Subunits, 030104 developmental biology, Child, Preschool, symbols, Female, Methylmalonyl-CoA decarboxylase

Abstract

The goal of this study was to identify mutations in the propionyl-CoA carboxylase alpha subunit (PCCA) and propionyl-CoA carboxylase beta subunit (PCCB) genes, and to assess their effects on propionic academia (PA) patients.Twenty-five Indian children with PA were enrolled in this study. Bidirectional Sanger sequencing was performed on both the coding and flanking regions of the PCCA and PCCB genes and the chromatograms were analyzed. Bioinformatic tools were used to classify novel variations into pathogenic or benign.The majority of the cases (19/25, 76%) were of the early-onset (90 days of age) type and 5 were of the late-onset type. The majority of patients had mutations in the PCCA gene (18/25). A total of 26 mutations were noted: 20 in the PCCA gene and 6 in PCCB gene. Seventeen mutations were novel (14 in PCCA and 3 in PCCB). The SNP c.937CT (p.Arg313Ter), was noted in 9/36 (25%) alleles in the PCCA gene. All of the children were symptomatic and only three survived who are doing well with no major disabilities.The spectrum of mutations in the PCCA and PCCB genes among Indians is distinct from other populations. The absence of a common mutation signifies the heterogeneity and admixture of various subpopulations. These findings also suggest that individuals of Indian origin may not benefit from the mutation-based "carrier screening panels" offered by many genetic laboratories.

Published

2016

24. Chanarin Dorfman syndrome: a case report with novel nonsense mutation

Author

Neerja Gupta, Prasenjit Das, Sunil Gothwal, Madhulika Kabra, Daniela Tavian, Amit Kumar Satpathy, Sara Missaglia, and Dipsal Timila

Subjects

0301 basic medicine, medicine.medical_specialty, Congenital ichthyosiform erythroderma, Lipid storage disorder, Nonsense mutation, Erythroderma, Biology, CHANARIN-DORFMAN SYNDROME, Lipid Metabolism, Inborn Errors, 03 medical and health sciences, Settore BIO/12 - BIOCHIMICA CLINICA E BIOLOGIA MOLECOLARE CLINICA, 0302 clinical medicine, Muscular Diseases, Internal medicine, Genetics, medicine, Humans, In patient, Ichthyosis, lipid storage disorder, General Medicine, 1-Acylglycerol-3-Phosphate O-Acyltransferase, Ichthyosiform Erythroderma, Congenital, medicine.disease, Dermatology, Peripheral blood, 030104 developmental biology, Endocrinology, Codon, Nonsense, Child, Preschool, Female, Chanarin Dorfman Syndrome, liver involvement, 030217 neurology & neurosurgery

Abstract

Chanarin Dorfman syndrome (CDS) is a very rare neutral lipid metabolism disorder with multisystem involvement. It is inherited as an autosomal recessive manner. It is characterized with congenital ichthyosiform erythroderma and involvement of liver, muscle, and central nervous system. Demonstration of lipid vacuoles in neutrophils from peripheral blood smears in patients with ichthyosiform erythroderma leads to the diagnosis. We report a novel ABHD5 truncating variant in a twenty nine month old female child, who presented with icthyosiform erythroderma.

Published

2016

25. Clinical and Molecular Disease Spectrum and Outcomes in Patients with Infantile-Onset Pompe Disease

Author

Catherine Rehder, Madhulika Kabra, Priya S. Kishnani, Neerja Gupta, Mamta N. Muranjan, Mani Kalaivani, Deeksha Bali, Ratna Dua Puri, Sheela Nampoothiri, Sujatha Jagdeesh, Ishwar C. Verma, and Zoheb B. Kazi

Subjects

Male, Pediatrics, medicine.medical_specialty, India, Molecular Disease, Disease, 03 medical and health sciences, 0302 clinical medicine, 030225 pediatrics, medicine, Humans, Missense mutation, In patient, 030212 general & internal medicine, Age of Onset, Alglucosidase alfa, Retrospective Studies, Glycogen Storage Disease Type II, business.industry, Infant, Newborn, Infant, Respiratory infection, Enzyme replacement therapy, medicine.disease, Malnutrition, Cross-Sectional Studies, Phenotype, Treatment Outcome, Pediatrics, Perinatology and Child Health, Female, business, medicine.drug

Abstract

Objectives To evaluate the clinical and molecular spectrum, and factors affecting clinical outcome of patients in India diagnosed with infantile-onset Pompe disease (IOPD). Study design In this multicenter, cross-sectional study, we evaluated the records of 77 patients with IOPD to analyze their clinical course, outcomes, and factors influencing the outcomes. Results Of the 77 patients with IOPD, phenotype data were available in 59; 46 (78%) had the classic phenotype. Overall, 58 of 77 (75%) and 19 of 77 (25%) patients were symptomatic before and after age 6 months, respectively. Alpha-glucosidase gene variant analysis available for 48 patients (96 alleles) showed missense variants in 49 alleles. Cross-reactive immunologic material (CRIM) status could be determined or predicted in 44 of 48 patients. In total, 32 of 44 patients (72%) were CRIM-positive, and 12 of 44 patients (27%) were CRIM-negative. Thirty-nine cases received enzyme-replacement therapy (ERT), alglucosidase alfa, and 38 patients never received ERT. Median age at initiation of ERT was 6.5 months. Response to ERT was better in babies who had CRIM-positive, non-classic IOPD. Conclusions This study highlights the clinical spectrum of IOPD in India and provides an insight on various factors, such as undernutrition, feeding difficulties, and recurrent respiratory infection, as possible factors influencing clinical outcomes in these patients. The study also reiterates the importance of raising awareness among clinicians about the need for early diagnosis and timely treatment of IOPD.

Published

2020

26. Batten disease: biochemical and molecular characterization revealing novel PPT1 and TPP1 gene mutations in Indian patients

Author

Arpita Thakker, Sanjiv Mehta, Jayesh Sheth, Vivek Jain, Madhulika Kabra, Frenny Sheth, Sheela Nampoothiri, Raju C Shah, Dhairya Pancholi, Riddhi Bhavsar, Mehul Mistri, Mahesh Kamate, and Neerja Gupta

Subjects

Male, 0301 basic medicine, Batten disease, India, Gene mutation, Aminopeptidases, lcsh:RC346-429, Frameshift mutation, PPT1, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Asian People, Neuronal Ceroid-Lipofuscinoses, Gene duplication, Humans, Medicine, Missense mutation, Genetic Testing, Dipeptidyl-Peptidases and Tripeptidyl-Peptidases, Gene, lcsh:Neurology. Diseases of the nervous system, TPP1, Neuronal ceroid lipofuscinoses (NCL), Genetics, Sanger sequencing, Tripeptidyl-Peptidase 1, business.industry, Infant, Membrane Proteins, General Medicine, medicine.disease, 030104 developmental biology, Child, Preschool, Mutation, symbols, Female, Thiolester Hydrolases, Neurology (clinical), Serine Proteases, business, 030217 neurology & neurosurgery, Research Article

Abstract

Background Neuronal ceroid lipofuscinoses type I and type II (NCL1 and NCL2) also known as Batten disease are the commonly observed neurodegenerative lysosomal storage disorder caused by mutations in the PPT1 and TPP1 genes respectively. Till date, nearly 76 mutations in PPT1 and approximately 140 mutations, including large deletion/duplications, in TPP1 genes have been reported in the literature. The present study includes 34 unrelated Indian patients (12 females and 22 males) having epilepsy, visual impairment, cerebral atrophy, and cerebellar atrophy. Methods The biochemical investigation involved measuring the palmitoyl protein thioesterase 1 and tripeptidy peptidase l enzyme activity from the leukocytes. Based on the biochemical analysis all patients were screened for variations in either PPT1 gene or TPP1 gene using bidirectional Sanger sequencing. In cases where Sanger sequencing results was uninformative Multiplex Ligation-dependent Probe Amplification technique was employed. The online tools performed the protein homology modeling and orthologous conservation of the novel variants. Results Out of 34 patients analyzed, the biochemical assay confirmed 12 patients with NCL1 and 22 patients with NCL2. Molecular analysis of PPT1 gene in NCL1 patients revealed three known mutations (p.Val181Met, p.Asn110Ser, and p.Trp186Ter) and four novel variants (p.Glu178Asnfs*13, p.Pro238Leu, p.Cys45Arg, and p.Val236Gly). In the case of NCL2 patients, the TPP1 gene analysis identified seven known mutations and eight novel variants. Overall these 15 variants comprised seven missense variants (p.Met345Leu, p.Arg339Trp, p.Arg339Gln, p.Arg206Cys, p.Asn286Ser, p.Arg152Ser, p.Tyr459Ser), four frameshift variants (p.Ser62Argfs*19, p.Ser153Profs*19, p.Phe230Serfs*28, p.Ile484Aspfs*7), three nonsense variants (p.Phe516*, p.Arg208*, p.Tyr157*) and one intronic variant (g.2023_2024insT). No large deletion/duplication was identified in three NCL1 patients where Sanger sequencing study was normal. Conclusion The given study reports 34 patients with Batten disease. In addition, the study contributes four novel variants to the spectrum of PPT1 gene mutations and eight novel variants to the TPP1 gene mutation data. The novel pathogenic variant p.Pro238Leu occurred most commonly in the NCL1 cohort while the occurrence of a known pathogenic mutation p.Arg206Cys dominated in the NCL2 cohort. This study provides an insight into the molecular pathology of NCL1 and NCL2 disease for Indian origin patients. Electronic supplementary material The online version of this article (10.1186/s12883-018-1206-1) contains supplementary material, which is available to authorized users.

Published

2018

27. Identification of novel variants in a large cohort of children with Tay-Sachs disease: An initiative of a multicentric task force on lysosomal storage disorders by Government of India

Author

Katta M. Girisha, Sankar V. Hariharan, Frenny Sheth, Mehul Mistri, Dhaval Solanki, Madhulika Kabra, Sanjeev Mehta, Neerja Gupta, Ratna Dua Puri, Sheela Nampoothiri, Mahesh Kamate, and Jayesh Sheth

Subjects

0301 basic medicine, Male, beta-Hexosaminidase alpha Chain, media_common.quotation_subject, Nonsense, Mutation, Missense, India, 030105 genetics & heredity, Biology, medicine.disease_cause, 03 medical and health sciences, Genotype, Genetics, medicine, Missense mutation, Humans, Allele, Genetics (clinical), Alleles, Genetic Association Studies, media_common, Demography, Sequence Deletion, Mutation, Tay-Sachs Disease, Tay-Sachs disease, Infant, medicine.disease, HEXA, Phenotype, 030104 developmental biology, Codon, Nonsense, Child, Preschool, Female

Abstract

Tay–Sachs disease (TSD) (OMIM) is a neurodegenerative lysosomal storage disorder caused due to mutations in the HEXA gene. To date, nearly 190 mutations have been reported in HEXA gene. Here, we have characterized 34 enzymatically confirmed TSD families to investigate the presence of novel as well as known variants in HEXA gene. Overall study detected 25 variants belonging to 31 affected TSD patients and 3 carrier couples confirmed by enzyme study. Of these 17 patients harbors 15 novel variants, including seven missense variants [p.V206L, p.Y213H, p.R252C, p.F257S, p.C328G, p.G454R, and p.P475R], four nonsense variant [p.S9X, p.E91X, p.W420X, and p.W482X], two splice site variants [c.347–1G>A and c.460–1G>A], and two small deletion [c.1349delC (p.A450VfsX3) and c.52delG (p.G18Dfs*82)]. While remaining 17 patients harbors 10 previously reported variants that includes six missense variants [p.M1T, p.R170Q, p.D322Y, p.D322N, p.E462V, and p.R499C], one nonsense variant [p.Q106X], two splice site variants [c.1073+1G>A and c.459+4A>G] and one 4 bp insertion [c.1278insTATC (p.Y427IfsX5)]. In conclusion, Indian infantile TSD patients provide newer insight into the molecular heterogeneity of the TSD. Combining present study and our earlier studies, we have observed that 67% genotypes found in Indian TSD patients are novel, which are associated with severe infantile phenotypes, while rest 33% genotypes found in our cohort were previously reported in various populations. In addition, higher frequency of the p.E462V and c.1278insTATC mutations in the present study further support and suggest the prevalence of p.E462V mutation in the Indian population.

Published

2018

28. Spectrum of ARSA variations in Asian Indian patients with Arylsulfatase A deficient metachromatic leukodystrophy

Author

Ashwin Dalal, Mahesh Kamate, Shubha R. Phadke, Divya Matta, Shagun Aggarwal, Jamal Mohammed Nurul Jain, Madhulika Kabra, Chaitanya Datar, Neerja Gupta, Kalpana Gowrishankar, Prajnya Ranganath, and Dhanya Lakshmi Narayanan

Subjects

0301 basic medicine, Adult, Male, Arylsulfatase A, Adolescent, Genotype, RNA Splicing, India, 030105 genetics & heredity, Biology, Frameshift mutation, 03 medical and health sciences, Young Adult, Asian People, Genetics, medicine, Missense mutation, Humans, Allele, Indel, Child, Genetics (clinical), Alleles, Cerebroside-Sulfatase, Leukodystrophy, Infant, Leukodystrophy, Metachromatic, medicine.disease, Metachromatic leukodystrophy, 030104 developmental biology, Child, Preschool, Mutation, Female

Abstract

Metachromatic leukodystrophy due to Arylsulfatase A enzyme deficiency is an autosomal recessive disorder caused by biallelic variations in ARSA gene. Till date 186 variations have been reported in ARSA gene worldwide, but the variation spectrum in India is not known. The aim of this study was to identify the variation profile in Indian patients presenting with features of Arylsulfatase A deficient metachromatic leukodystrophy. We sequenced the ARSA gene in 51 unrelated families and identified 36 variants out of which 16 were novel. The variations included 23 missense, 3 nonsense, and 6 frameshift variants (3 single-base deletions and 3 single-base duplications), 1 indel, one 3 bp deletion, and 2 splice site variations. The pathogenicity of the novel variations was inferred with the help of mutation prediction softwares like MutationTaster, SIFT, Polyphen-2, PROVEAN, and HANSA. The effects of the identified sequence variants on the protein structure were studied using in silico methods. The most common variation was c.931 C > T(p.Arg311*), found in 11.4% (14 out of 122 alleles) of the tested individuals. To the best of our knowledge, this study is the first of its kind in India with respect to the size of the cohort and the molecular diagnostic method used and one of the largest cohorts of metachromatic leukodystrophy studied till date.

Published

2018

29. Locus and allelic heterogeneity and phenotypic variability in Waardenburg syndrome

Author

Katta M. Girisha, Anju Shukla, Neerja Gupta, Leslie Lewis, Sheela Nampoothiri, Anupriya Kaur, Kalpana Gowrishankar, Puneeth H. Somashekar, Dhanya Lakshmi Narayanan, Sujatha Jagadeesh, Radha Devi, Shenoy Shailaja, and Shruti Bajaj

Subjects

0301 basic medicine, Male, DNA Copy Number Variations, Quantitative Trait Loci, Locus (genetics), 030105 genetics & heredity, Biology, 03 medical and health sciences, Genetic Heterogeneity, Gene Frequency, Exome Sequencing, Genetics, medicine, Humans, Waardenburg Syndrome, Allele, Genetics (clinical), Alleles, Phenocopy, integumentary system, Waardenburg syndrome, Genetic heterogeneity, medicine.disease, Penetrance, Pedigree, 030104 developmental biology, Phenotype, Biological Variation, Population, Allelic heterogeneity, Female, Neural crest cell migration

Abstract

Waardenburg syndrome (WS) is a disorder of neural crest cell migration characterized by auditory and pigmentary abnormalities. We investigated a cohort of 14 families (16 subjects) either by targeted sequencing or whole-exome sequencing. Thirteen of these families were clinically diagnosed with WS and one family with isolated non-syndromic hearing loss (NSHL). Intra-familial phenotypic variability and non-penetrance were observed in families diagnosed with WS1, WS2 and WS4 with pathogenic variants in PAX3, MITF and EDNRB, respectively. We observed gonosomal mosaicism for a variant in PAX3 in an asymptomatic father of two affected siblings. For the first time, we report a biallelic pathogenic variant in MITF in a subject with WS2 and a biallelic variant in EDNRB was noted in a subject with WS2. An individual with isolated NSHL carried a pathogenic variant in MITF. Blended phenotype of NSHL and albinism was observed in a subject clinically diagnosed to have WS2. A phenocopy of WS1 was observed in a subject with a reported pathogenic variant in GJB2, known to cause isolated NSHL. These novel and infrequently reported observations exemplify the allelic and genetic heterogeneity and show phenotypic diversity of WS.

Published

2018

30. An immune tolerance approach using transient low-dose methotrexate in the ERT-naïve setting of patients treated with a therapeutic protein: experience in infantile-onset Pompe disease

Author

R. Bradley Troxler, Marta Sabbadini, Neerja Gupta, David Kronn, Ankit K. Desai, Katalin Scherer, Susan M. Richards, Alison McVie-Wylie, Priya S. Kishnani, Reeval Segel, Langston Sherry, Alexandra Joseph, Pranoot Tanpaiboon, William B. Rizzo, Crystal Sung, Seymour Packman, Sheela Nampoothiri, Zoheb B. Kazi, Omar A. Abdul-Rahman, Annette Feigenbaum, and Dmitriy Niyazov

Subjects

0301 basic medicine, Male, medicine.medical_specialty, alglucosidase alfa, Disease, 030105 genetics & heredity, Cross Reactions, Low dose methotrexate, Gastroenterology, Article, methotrexate, Immune tolerance, 03 medical and health sciences, Internal medicine, medicine, Immune Tolerance, Humans, prophylactic immune tolerance induction, Enzyme Replacement Therapy, Age of Onset, Alglucosidase alfa, Genetics (clinical), business.industry, Glycogen Storage Disease Type II, Infant, Newborn, Therapeutic protein, Infant, Pompe disease, alpha-Glucosidases, 3. Good health, Titer, 030104 developmental biology, anti-drug antibodies, Methotrexate, Female, Infantile onset, business, medicine.drug

Abstract

Purpose: To investigate immune tolerance induction with transient low-dose methotrexate (TLD-MTX) initiated with recombinant human acid α-glucosidase (rhGAA), in treatment-naïve cross-reactive immunologic material (CRIM)-positive infantile-onset Pompe disease (IOPD) patients. Methods: Newly-diagnosed IOPD patients received subcutaneous or oral 0.4 mg/kg TLD-MTX for 3 cycles (3 doses/cycle) with the first 3 rhGAA infusions. Anti-rhGAA IgG titers, classified as high-sustained (HSAT; ≥51,200, ≥2 times after 6 months), sustained intermediate (SIT; ≥12,800 and

Published

2018

31. A novel homozygous mutation in POLR3A gene causing 4H syndrome: a case report

Author

C. M. Sreedhar, Vishal Vishnu Tewari, Sheffali Gulati, Akbar Mohammad, Madhulika Kabra, Neerja Gupta, Kunal Tewari, and Ritu Mehta

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Ataxia, Mutation, Missense, Case Report, Clitoromegaly, Hypogonadotropic hypogonadism, 03 medical and health sciences, 4H syndrome, 0302 clinical medicine, Leukoencephalopathies, Medicine, Humans, Exome sequencing, Low-set ears, Anodontia, Dystonia, business.industry, Hypodontia, Hypogonadism, lcsh:RJ1-570, Infant, RNA Polymerase III, lcsh:Pediatrics, Congenital hypomyelinating leukodystrophy, medicine.disease, White Matter, Hyperintensity, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Female, medicine.symptom, business, POLR3A gene, 030217 neurology & neurosurgery

Abstract

Background 4H syndrome is a congenital hypomyelinating leukodystrophy characterized by hypodontia, hypomyelination and hypogonadotropic hypogonadism belonging to the Pol III-related leukodystrophies which arise due to mutations in the POLR3A or POLR3B gene. The clinical presentation is of neurodevelopmental delay or regression with ataxia, dystonia, nystagmus, delayed deciduous dentition and abnormal order of eruption of teeth. MRI brain shows a characteristic hypomyelination pattern. Several mutations have been described in the implicated genes but there are no reports on mutations seen in patients from India. Case presentation We report a 1½ year old girl, only child of a non-consanguinous couple who presented with delayed developmental milestones and delayed dentition. On physical examination she had downward slanting palpebral fissures, low set ears, smooth philtrum, hypodontia, prominent body hair and clitoromegaly. There was prominent horizontal nystagmus, hypertonia of both upper and lower limbs, exaggerated deep tendon jerks and flexor planter response. She had not attained complete head control and required support to sit. She showed absent waves on brainstem evoked response audiometry and her fundus examination showed bilateral optic atrophy with prolongation of P100 latencies on visual evoked potentials. MRI Brain showed hyperintensity of entire white matter with involvement of the internal and external capsule, frontal deep white matter and corpus callosum. Her karyotype was 46 XX and her endocrinal profile was unremarkable. Clinical exome sequencing identified an unreported mutation in the POLR3A gene. The same mutation was identified by Sanger sequencing in heterozygous state in both parents. The child is being managed with physiotherapy and developmental therapy. She has been provided with hearing aids and started on speech therapy. Parents were provided anticipatory guidance and genetic counselling about autosomal recessive nature of inheritance, risk of recurrence and need for follow-up. Conclusion 4H syndrome is a rare congenital hypomyelinating leukodystrophy inherited as an autosomal recessive disorder due to mutations in the POLR3A and POLR3B gene. Delay or regression of milestones, abnormalities in dentition and endocrinal perturbations are its hallmark. A novel mutation in the POLR3A gene resulting in amino acid substitution of arginine for glutamine at codon 808 (p.R808Q) was detected in exon 18 in our case. Electronic supplementary material The online version of this article (10.1186/s12887-018-1108-9) contains supplementary material, which is available to authorized users.

Published

2018

32. Recurrent and novel GLB1 mutations in India

Author

Prajnya Ranganath, Hitesh Shah, Shrikiran Hebbar, Divya Matta, Neerja Gupta, Anju Shukla, Ishwar C. Verma, Ashwin Dalal, Shuba Krishna, P. M. Gopinath, Abdul Mueed Bidchol, Kalpana Gowrishankar, Katta M. Girisha, Shagun Aggarwal, Alka V. Ekbote, Ratna Dua Puri, Shubha R. Phadke, Rakesh Trivedi, Mahesh Kamate, Chaitanya Datar, Sheela Nampoothiri, Ramesh Y Bhat, Kamalakshi G. Bhat, Madhulika Kabra, Nutan Kamath, Hampapathalu A. Nagarajaram, Sheetal Sharda, Kapaettu Satyamoorthy, V.H. Sankar, and Sumita Danda

Subjects

Male, Models, Molecular, Heterozygote, DNA Mutational Analysis, Nonsense mutation, Mutation, Missense, India, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, Exon, Genetics, medicine, Humans, Missense mutation, Gene, Allele frequency, Genetic Association Studies, Mutation, Gangliosidosis, GM1, Infant, Newborn, Infant, General Medicine, beta-Galactosidase, GLB1, Child, Preschool, RNA splicing, Female

Abstract

GM1 gangliosidosis is a lysosomal storage disorder caused by mutations in the GLB1 gene, leading to the deficiency of the enzyme β-d-galactosidase. In this study, we report molecular findings in 50 Asian Indian families with GM1 gangliosidosis. We sequenced all the exons and flanking intronic sequences of GLB1 gene. We identified 33 different mutations (20 novel and 13 previously reported). The novel mutations include 12 missense (p.M1?, p.E129Q, p.G134R, p.L236P, p.G262E, p.L297F, p.Y331C, p.G414V, p.K493N, p.L514P, p.P597L, p.T600I), four splicing (c.246-2A>G, c.397-2A>G, c.552+1G>T, c.956-2A>G), three indels (p.R22Qfs*8, p.L24Cfs*47, p.I489Qfs*4) and one nonsense mutation (p.Q452*). Most common mutations identified in this study were c.75+2InsT (14%) and p.L337P (10%). Known mutations accounted for 67% of allele frequency in our cohort of patients, suggesting that these mutations in GLB1 are recurrent across different populations. Twenty three mutations were localized in the TIM barrel domain, β-domain 1 and β-domain 2. In silico sequence and structure analysis of GLB1 reveal that all the novel mutations affect the function and structure of the protein. We hereby report on the largest series of patients with GM1 gangliosidosis and the first from India.

Published

2015

33. Novel and recurrent mutations in WISP3 and an atypical phenotype

Author

Sankar V. Hariharan, Kalpana Gowrishankar, M. L. Kulkarni, Anju Shukla, Kavitha Mohanasundaram, Ashwin Dalal, Meenakshi Bhat, Sumita Danda, Anju Gupta, A. Radha Ramadevi, Shubha R. Phadke, Shagun Aggarwal, Katta M. Girisha, Prajnya Ranganath, Akhil Muralidhar Kulkarni, Gandham SriLakshmi Bhavani, Hitesh Shah, Neerja Gupta, Sunita Bijarnia-Mahay, Madhulika Kabra, Sankaralingam Rajeswari, Ratna Dua Puri, and Sheela Nampoothiri

Subjects

Adult, Cartilage, Articular, Male, Heterozygote, Adolescent, Gene Expression, India, Biology, CCN Intercellular Signaling Proteins, Text mining, Genetics, Humans, Atypical phenotype, Family, Genetics (clinical), business.industry, Homozygote, Exons, Introns, Phenotype, Amino Acid Substitution, Mutation, Female, Joint Diseases, business

Published

2015

34. Williams-Beuren Syndrome: Experience of 43 Patients and a Report of an Atypical Case from a Tertiary Care Center in India

Author

Manju Ghosh, Pankaj Sharma, Madhulika Kabra, Shubha R. Phadke, Ashutosh Halder, Savita Sapra, Neerja Gupta, and Madhumita Roy Chowdhury

Subjects

Male, Williams Syndrome, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Adolescent, Microarray, India, Biology, Gene duplication, Intellectual disability, Genetics, medicine, Humans, Multiplex ligation-dependent probe amplification, Child, Molecular Biology, Genetics (clinical), Breakpoint, Infant, medicine.disease, Phenotype, Child, Preschool, Microsatellite, Female, Williams syndrome, Chromosome Deletion, Supravalvular aortic stenosis, Chromosomes, Human, Pair 7

Abstract

Williams-Beuren syndrome (WBS) or Williams syndrome (OMIM 194050) is a multisystem disorder manifested by neurodevelopmental delay and is caused by a hemizygous deletion of ∼1.5-1.8 Mb in the 7q11.23 region. Clinical features include cardiovascular anomalies (mainly supravalvular aortic stenosis), peripheral pulmonary stenosis, distinctive facies, intellectual disability (usually mild), unique personality characteristics, and growth and endocrine abnormalities. Clinical diagnostic criteria are available for WBS; however, the mainstay of diagnosis is the detection of the contiguous gene deletion. Although FISH remains the most widely used laboratory test, the diagnosis can also be established by means of qPCR, MLPA, microsatellite marker analysis, and chromosomal microarray (CMA). We evaluated the utility of MLPA to detect deletion/duplication in the 7q11.23 region in 43 patients suspected to have WBS using MLPA kits for microdeletion syndromes. A hemizygous deletion in the 7q11.23 region was found in 41 (95.3%) patients using MLPA. One patient had an atypical deletion detected by CMA. During the initial period of this study, the results of 12 patients tested by MLPA were also confirmed by FISH. Compared to FISH and CMA, MLPA is a cheaper, high-throughput, less labor-intensive and less time-consuming technique for the diagnosis of WBS. Although CMA is expensive and labor-intensive, its effectiveness is demonstrated to detect an atypical deletion and to delineate the breakpoints.

Published

2015

35. Identification of a novel homozygous mutation in transmembrane channel like 1 (

Author

Pawan Kumar, Singh, Manju, Ghosh, Shipra, Sharma, Shivaram, Shastri, Neerja, Gupta, Madhumita Roy, Chowdhury, Anuranjan, Anand, and Madhulika, Kabra

Subjects

Male, Genotype, Genetic Linkage, Homozygote, India, Membrane Proteins, hearing impairment, Deafness, Connexins, Pedigree, short tandem repeat markers, Connexin 26, Haplotypes, Mutation, transmembrane channel like 1 gene, otorhinolaryngologic diseases, Humans, Female, Original Article, DNA sequencing, DFNB7/11 locus, linkage study

Abstract

Background & objectives: Hearing impairment is a common and heterogeneous sensory disorder in humans. Among about 90 genes, which are known to be associated with hearing impairment, mutations in the GJB2 (gap junction protein beta 2) gene are the most prevalent in individuals with hereditary hearing loss. Contribution of the other deafness-causing genes is relatively poorly understood. Here, we present our findings on two families with transmembrane channel like 1 (TMC1) gene variants of the 47 families with nonsyndromic hearing loss (NSHL) studied. Methods: Forty seven families including 26 consanguineous families with at least two hearing impaired children and one normal hearing child and 21 non-consanguineous families having at least three hearing impaired children and one normal hearing child were enrolled for this study. Genetic linkage studies were carried out in 41 families that were GJB2 (Connexin 26) negative. Seven polymorphic short tandem repeat markers at the DFNB7/11 locus were studied employing fluorescently labelled markers. Results: A novel homozygous missense mutation c.1283C>A (p.Ala428Asp) was identified co-segregating with hearing loss. This change results in substitution of a highly conserved polar alanine to a charged aspartic acid and is predicted to be deleterious. In addition, a previously reported nonsense mutation, p.R34X in TMC1, was found. Interpretation & conclusions: While mutations in TMC1 are not as common a cause of NSHL as those in GJB2, TMC1 should be considered for diagnostic investigations in cases of NSHL in GJB2-negative families.

Published

2017

36. Validation of Polymerase Chain Reaction-Based Assay to Detect Actual Number of CGG Repeats in FMR1 Gene in Indian Fragile X Syndrome Patients

Author

Neerja Gupta, Madhulika Kabra, Sandeepa Chauhan, Anjali Dabral, B.K. Thelma, and Madhumita Roy Chowdhury

Subjects

0301 basic medicine, Male, Offspring, Intermediate region, India, Genetic Counseling, 030105 genetics & heredity, Biology, Polymerase Chain Reaction, law.invention, 03 medical and health sciences, Fragile X Mental Retardation Protein, Asian People, law, medicine, Humans, Family, Genetic Predisposition to Disease, Allele, Polymerase chain reaction, Genetics, Molecular genetic testing, medicine.disease, FMR1, Fragile X syndrome, Fmr1 gene, Blotting, Southern, Fragile X Syndrome, Pediatrics, Perinatology and Child Health, Female, Neurology (clinical), Trinucleotide Repeat Expansion

Abstract

Molecular genetic testing for fragile X (FX) is complicated due to the large variation in the size of CGG expansion. The aim of this study was to apply this new technique using AmplideX FMR1 PCR assay, which is considered a better diagnostic tool for detecting expanded alleles in Indian population. The primary objective was to identify the carrier status of females and to correlate the instability of premutation alleles in females with the repeat sizes. 24 children with FX based on rapid PCR and 29 female relatives of these patients were included. Out of the 29 females screened, those whose child (or children) was affected by FX, were all premutation carriers confirming their role in transmission. The smallest PM allele that expanded into FM in the next generation was 78 repeats and the smallest PM allele detected was 63 repeats, and when transmitted from mother to offspring remained in the premutation range. In 4 families, the repeat size of the allele reduced from PM to normal repeat numbers in their daughters and in 1 case to borderline PM range. Thus, apart from the reduced turnaround time, this PCR based assay offers advantage by its sensitivity to detect CGG repeats in the intermediate region and lower range of premutation alleles. It also provides added information of AGG interruptions, which may have an impact on the counseling of women with intermediate and PM alleles.

Published

2017

37. Threshold levels of 25-hydroxyvitamin D and parathyroid hormone for impaired bone health in children with congenital ichthyosis and type IV and V skin

Author

Madhulika Kabra, Mohammad Irshad, Neetu Bhari, Raman K. Marwaha, Vinod Sharma, Neerja Gupta, Vamsi K Yenamandra, V Sreenivas, Sanjay Thulkar, and Gomathy Sethuraman

Subjects

Male, medicine.medical_specialty, Adolescent, Parathyroid hormone, Rickets, Dermatology, vitamin D deficiency, Blood serum, Internal medicine, Congenital ichthyosis, medicine, Vitamin D and neurology, Humans, Vitamin D, Child, Hyperparathyroidism, Ichthyosis, business.industry, Infant, Vitamin D Deficiency, medicine.disease, Cross-Sectional Studies, Endocrinology, Parathyroid Hormone, Case-Control Studies, Child, Preschool, Female, business, Ichthyosis, Lamellar

Abstract

Summary Background Patients with congenital ichthyosis, especially those with darker skin types, are at increased risk of developing vitamin D deficiency and rickets. The relationships between 25-hydroxyvitamin D [25(OH)D], parathyroid hormone (PTH) and bone health have not been studied previously, in ichthyosis. Objectives To determine the threshold levels of 25(OH)D and PTH for impaired bone health in children with congenital ichthyosis. Methods In this cross-sectional study, 119 children with ichthyosis and 168 controls were recruited. Serum 25(OH)D, PTH, calcium, phosphate and alkaline phosphatase (ALP) were measured. Radiological screening for rickets was carried out only in children with ichthyosis. Results Forty-seven children with ichthyosis had either clinical or radiological evidence of rickets. The correlation between serum 25(OH)D and PTH showed that a serum level of 25(OH)D 8 ng mL−1 was associated with a significant increase in PTH. The correlation between PTH and ALP showed that a serum PTH level of 75 pg mL−1 was associated with a significant increase in ALP levels. Of the different clinical phenotypes of ichthyosis, both autosomal recessive congenital ichthyosis (ARCI) and epidermolytic ichthyosis (EI) were found to have significantly increased PTH, ALP and radiological rickets scores compared with common ichthyosis. Conclusions Serum levels of 25(OH)D ≤ 8 ng mL−1 and PTH ≥ 75 pg mL−1 significantly increases the risk for development of rickets [odds ratio (OR) 2·8; 95% confidence interval (CI) 1·05–7·40; P = 0·04] in ichthyosis. Among the different types, patients with ARCI (OR 4·83; 95% CI 1·74–13·45; P

Published

2014

38. GALNSmutations in Indian patients with mucopolysaccharidosis IVA

Author

Kapaettu Satyamoorthy, V.H. Sankar, Sumita Danda, Abdul Mueed Bidchol, Katta M. Girisha, Hampapathalu A. Nagarajaram, S.J. Patil, Hitesh Shah, Kalpana Gowrishankar, Madhulika Kabra, Shubha R. Phadke, Pallavi Mishra, Seema Kapoor, Ratna Dua Puri, Neerja Gupta, Suryanarayana S, Ashwin Dalal, S Jamal Md Nurul Jain, Sheela Nampoothiri, Meenal Agarwal, Parag M Tamhankar, I. C. Verma, Prajnya Ranganath, A. Radha Rama Devi, Mahesh Kamate, Ankur Singh, and P. M. Gopinath

Subjects

Adult, Male, Morquio syndrome, Adolescent, Mucopolysaccharidosis, DNA Mutational Analysis, Nonsense mutation, India, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, White People, Frameshift mutation, Young Adult, Exon, Gene Frequency, Pregnancy, Prenatal Diagnosis, Gene Order, Genetics, medicine, Humans, Missense mutation, Child, Alleles, Genetics (clinical), Mutation, Computational Biology, Infant, Mucopolysaccharidosis IV, medicine.disease, Chondroitinsulfatases, Enzyme Activation, Amino Acid Substitution, Child, Preschool, Female

Abstract

Mucopolysaccharidosis IV A (Morquio syndrome A, MPS IVA) is a lysosomal storage disease caused by the deficiency of N-acetylgalactosamine-6-sulfatase (GALNS). The mutation spectrum in this condition is yet to be determined in Indians. We aimed to analyze the mutations in the GALNS gene in Asian Indians with MPS IVA. All the exons and the adjacent intronic regions of the gene were amplified and sequenced in sixty-eight unrelated Indian families. We identified 136 mutant alleles comprising of 40 different mutations. We report twenty-two novel mutations that comprise of seventeen missense (p.Asn32Thr, p.Leu36Arg, p.Pro52Leu, p.Pro77Ser, p.Cys79Arg, p.His142Pro, p.Tyr191Asp, p.Asn204Thr, p.Gly188Ser, p.Phe216Ser, p.Trp230Cys, p.Ala291Ser, p.Gly317Arg, p.His329Pro, p.Arg386Ser, p.Glu450Gly, p.Cys501Ser), three splice-site variants (c.120+1G>C, c.1003-3C>G, c.1139+1G>A), one nonsense mutation (p.Gln414*) and one frameshift mutation (p.Pro420Leufs*440). Eighteen mutations have been reported earlier. Among these p.Ser287Leu (8.82%), p.Phe216Ser (7.35%), p.Asn32Thr (6.61%) and p.Ala291Ser (5.88%) were the most frequent mutations in Indian patients but were rare in the mutational profiles reported in other populations. These results indicate that the Indian patients may have a distinct mutation spectrum compared to those of other populations. Mutant alleles in exon 1, 7 and 8 accounted for 44.8% of the mutations, and sequencing of these exons initially may be a cost-effective approach in Asian Indian patients. This is the largest study on molecular analysis of patients with MPS IVA reported in the literature, and the first report from India. (c) 2014 Wiley Periodicals, Inc.

Published

2014

39. Mutation spectrum ofCOL1A1andCOL1A2genes in Indian patients with osteogenesis imperfecta

Author

Joshi Stephen, Shubha R. Phadke, Hitesh Shah, Neerja Gupta, Kosei Hasegawa, Katta M. Girisha, Preeti Dabadghao, Ashwin Dalal, Madhulika Kabra, Anju Shukla, and Hiroyuki Tanaka

Subjects

Adult, Male, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, DNA Mutational Analysis, India, Consanguinity, Biology, medicine.disease_cause, Collagen Type I, Fractures, Bone, Young Adult, Exon, Genetics, medicine, Humans, Coding region, Mutation detection, Child, skin and connective tissue diseases, Gene, Genetics (clinical), Mutation, Polymorphism, Genetic, Base Sequence, Sequence Analysis, DNA, Osteogenesis Imperfecta, medicine.disease, Collagen Type I, alpha 1 Chain, Phenotype, Osteogenesis imperfecta, Child, Preschool, Mutation (genetic algorithm), Etiology, Female

Abstract

Osteogenesis imperfecta (OI) is a condition of decreased bone density with heterogeneous etiologies. Most of the cases are inherited in an autosomal dominant fashion and are caused by mutations in the COL1A1 or COL1A2 genes. Since these two genes are very large, there are no data about mutations in Indian patients with OI. We selected 35 Indian patients who were clinically diagnosed with OI and all exons of both the genes were sequenced. Mutations in COL1A1 (14 cases, 6 novel) and COL1A2 (11 cases, 7 novel) were identified in 25 patients. A total of 55 polymorphisms were identified in both the genes with eight novel variants in the coding region, and nine novel variants in the non-coding regions. No mutation was detected in 10 patients. Six of them were from consanguineous families, with one or two similarly affected siblings suggesting possible autosomal recessive inheritance. If we exclude families with consanguinity, mutations were identified in 25 out of 29 families giving 86% mutation detection rate. Mutations in COL1A1 accounted for 56% of the cases and COL1A2 44%, which is similar to the reported rate worldwide.

Published

2014

40. Severe neuronopathic autosomal recessive osteopetrosis due to homozygous deletions affecting OSTM1

Author

Madhulika Kabra, Heidemarie Neitzel, Phillipe Schröter, Uwe Kornak, Anna Rajab, Neerja Gupta, Claus-Eric Ott, Björn Fischer, Stefan Mundlos, Reyk Richter, and Nishant Verma

Subjects

Male, Pathology, medicine.medical_specialty, Histology, Physiology, Ubiquitin-Protein Ligases, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Molecular Sequence Data, Hematopoietic stem cell transplantation, Real-Time Polymerase Chain Reaction, Sepsis, Consanguinity, Skeletal disorder, Osteoclast, Humans, Medicine, Base Sequence, business.industry, Genetic heterogeneity, Homozygote, Infant, Newborn, Bone marrow failure, Infant, Membrane Proteins, Increased Bone Density, medicine.disease, Pedigree, medicine.anatomical_structure, Osteopetrosis, Female, business, Gene Deletion, Infantile malignant osteopetrosis

Abstract

Autosomal recessive osteopetrosis (ARO, MIM 259700) is a genetically heterogeneous rare skeletal disorder characterized by failure of osteoclast resorption leading to pathologically increased bone density, bone marrow failure, and fractures. In the neuronopathic form neurological complications are especially severe and progressive. An early identification of the underlying genetic defect is imperative for assessment of prognosis and treatment by hematopoietic stem cell transplantation. Here we describe for the first time homozygous microdeletions of different sizes affecting the OSTM1 gene in two unrelated consanguineous families with children suffering from neuronopathic infantile malignant osteopetrosis. Patients showed an exceptionally severe phenotype with variable CNS malformations, seizures, blindness, and deafness. Multi-organ failure due to sepsis led to early death between six weeks and five months of age in spite of intensive care treatment. Analysis of the breakpoints revealed different mechanisms underlying both rearrangements. Microdeletions seem to represent a considerable portion of OSTM1 mutations and should therefore be included in a sufficient diagnostic screening.

Published

2013

41. Cardiovascular Autonomic Dysfunction in Children and Adolescents With Rett Syndrome

Author

Ajay Kumar, Savita Sapra, Akanksha Singh, Biswaroop Chakrabarty, R.M. Pandey, Kishore Kumar Deepak, Neerja Gupta, Rajni Khajuria, Madhulika Kabra, Ashok Kumar Jaryal, and Sheffali Gulati

Subjects

Male, Sympathetic nervous system, Adolescent, Methyl-CpG-Binding Protein 2, India, Rett syndrome, Blood Pressure, 030204 cardiovascular system & hematology, MECP2, 03 medical and health sciences, 0302 clinical medicine, Developmental Neuroscience, Heart Rate, Hyperventilation, medicine, Rett Syndrome, Heart rate variability, Humans, Aerophagia, Child, Retrospective Studies, business.industry, Cold pressor test, medicine.disease, Blood pressure, medicine.anatomical_structure, Neurology, Autonomic Nervous System Diseases, Cardiovascular Diseases, Anesthesia, Case-Control Studies, Child, Preschool, Pediatrics, Perinatology and Child Health, Mutation, Female, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Background Autonomic dysfunction is common in children with Rett syndrome. They usually manifest with agitation, persistent screaming, constipation, gastroesophageal reflux, aerophagia, hyperventilation, and breath-holding episodes. Cardiovascular autonomic dysfunction may result in fatal a arrhythmia. Many of these events are mistaken for seizures and treated with antiepileptics. Methods The present study was conducted in a tertiary care teaching hospital in north India for more than a six month period. MeCP2 mutation positive, 24 cases with Rett syndrome and 24 age-matched healthy girls were evaluated for cardiovascular autonomic dysfunction (heart rate variability, head-up tilt test, and cold pressor test). Results The mean age was 9.06 years (±3.4) and 9.75 years (±3.13) for patients and control subjects, respectively. The heart rate variability contributed independently by parasympathetic and sympathetic nervous system was significantly reduced in cases compared with control subjects ( P = 0.033 and P = 0.001, respectively). There was significant sympathovagal imbalance with sympathetic overactivity in cases compared with control subjects ( P = 0.001). The mean longest QT c interval was significantly prolonged in cases compared with control subjects ( P = 0.001). Cold pressor test and head-up tilt test could be done in 16 Rett syndrome patients (because of poor cooperation) and in all 24 control subjects. The change in blood pressure during cold pressor test and head-up tilt test was not significantly different in cases and control subjects. Conclusions Children with Rett syndrome exhibited significant cardiovascular autonomic dysfunction in the form of sympathetic overactivity, parasympathetic underactivity, and sympathovagal imbalance. These findings have potentially important therapeutic- and outcome-related implications.

Published

2016

42. Prevalence of neural tube defects in a rural area of north india from 2001 to 2014: A population-based survey

Author

Shashi, Kant, Sumit, Malhotra, Arvind Kumar, Singh, Partha, Haldar, Ravneet, Kaur, Puneet, Misra, and Neerja, Gupta

Subjects

Adult, Rural Population, Anencephaly, Pregnancy Outcome, India, Stillbirth, Community Health Planning, Cross-Sectional Studies, Pregnancy, Surveys and Questionnaires, Prevalence, Humans, Female, Neural Tube Defects, Live Birth, Spinal Dysraphism, Encephalocele

Abstract

Neural tube defects (NTDs) are one of the commonest birth defects. There was paucity of community-based data on occurrence of NTDs in India, especially from rural parts of the country. Against this background, the current study was carried out with main objectives to determine the prevalence of NTDs and its specific types (anencephaly, spina bifida and encephalocele) in a rural community setting over the time period 2001 to 2014.This was a community-based cross-sectional study carried out in 28 villages of Ballabgarh Tehsil of Faridabad district in north India (population ∼ 96,000). A household survey was undertaken by trained multi-purpose workers who enquired ever-married women about history of conception with outcome as NTD during the study period. The probable case of NTD was determined using a colored pictorial card with photographs of different types of NTDs. These cases were confirmed by doctors.A total of 26,946 live births occurred during the years 2001 to 2014. A total of 140 confirmed cases of NTDs were identified. The live birth prevalence of NTDs was 24.1 per 10,000 live births (95% confidence interval, 18.8-30.6). The birth prevalence of NTDs for the years 2008 to 2014 was 50.8 (95% confidence interval, 39.9-63.8) per 10,000 live and stillbirths. The most common type of NTD was found to be spina bifida followed by anencephaly and encephalocele.We found high prevalence of NTDs in rural community settings from north India for years 2001 to 2014.Birth Defects Research 109:203-210, 2017.© 2016 Wiley Periodicals, Inc.

Published

2016

43. Novel Genetic, Clinical, and Pathomechanistic Insights into TFG-Associated Hereditary Spastic Paraplegia

Author

Gaurav V, Harlalka, Meriel E, McEntagart, Neerja, Gupta, Anna E, Skrzypiec, Mariusz W, Mucha, Barry A, Chioza, Michael A, Simpson, Ajith, Sreekantan-Nair, Anthony, Pereira, Sven, Günther, Amir, Jahic, Hamid, Modarres, Heather, Moore-Barton, Richard C, Trembath, Madhulika, Kabra, Emma L, Baple, Seema, Thakur, Michael A, Patton, Christian, Beetz, Robert, Pawlak, and Andrew H, Crosby

Subjects

Male, Neurons, Spastic Paraplegia, Hereditary, Mutation, Missense, Proteins, Sequence Analysis, DNA, Magnetic Resonance Imaging, Mitochondria, Pedigree, Mice, Animals, Humans, Female, Genetic Predisposition to Disease, Cells, Cultured

Abstract

Hereditary spastic paraplegias (HSPs) are genetically and clinically heterogeneous axonopathies primarily affecting upper motor neurons and, in complex forms, additional neurons. Here, we report two families with distinct recessive mutations in TFG, previously suggested to cause HSP based on findings in a single small family with complex HSP. The first carried a homozygous c.317GA (p.R106H) variant and presented with pure HSP. The second carried the same homozygous c.316CT (p.R106C) variant previously reported and displayed a similarly complex phenotype including optic atrophy. Haplotyping and bisulfate sequencing revealed evidence for a c.316CT founder allele, as well as for a c.316_317 mutation hotspot. Expression of mutant TFG proteins in cultured neurons revealed mitochondrial fragmentation, the extent of which correlated with clinical severity. Our findings confirm the causal nature of bi-allelic TFG mutations for HSP, broaden the clinical and mutational spectra, and suggest mitochondrial impairment to represent a pathomechanistic link to other neurodegenerative conditions.

Published

2016

44. Pycnodysostosis: mutation spectrum in five unrelated Indian children

Author

Prajnya Ranganath, Madhulika Kabra, Satinath Mukhopadhyay, Kausik Mandal, Deepti Saxena, Neerja Gupta, Priyanka Srivastava, Sayantan Ray, Shubha R. Phadke, and Amita Moirangthem

Subjects

0301 basic medicine, Male, Adolescent, Genotype, Pycnodysostosis, Cathepsin K, DNA Mutational Analysis, India, Bioinformatics, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Child, Genetics (clinical), Alleles, Genetics, Base Sequence, business.industry, Infant, General Medicine, medicine.disease, 030104 developmental biology, Phenotype, Child, Preschool, Pediatrics, Perinatology and Child Health, Mutation (genetic algorithm), Mutation, Female, Anatomy, business, 030217 neurology & neurosurgery

Published

2016

45. Biologicals in Juvenile Idiopathic Arthritis

Author

Isha, Saini, Lesa, Dawman, Neerja, Gupta, and S K, Kabra

Subjects

Abatacept, Male, Treatment Outcome, Adolescent, Antirheumatic Agents, Child, Preschool, Humans, Infant, Female, Antibodies, Monoclonal, Humanized, Child, Arthritis, Juvenile, Etanercept

Abstract

We share our experience with biological agents in children with juvenile idiopathic arthritis with an aim to highlight the adverse events and response to treatment. Out of a total of 10 children treated with biological agents, one patient had serious infection, all showed good response and none had tuberculosis. High cost was limiting factor for their use.

Published

2016

46. Report of four new patients with protein-truncating mutations in C6orf221/KHDC3L and colocalization with NLRP7

Author

William Daley, Elie Akoury, Rima Slim, Neerja Gupta, Isabelle Touitou, Christine Dery, Ramesh Reddy, Rosemary A. Fisher, Asangla Ao, Hanène Landolsi, Omar A. Abdul-Rahman, and Ngoc Minh Phuong Nguyen

Subjects

Male, DNA Mutational Analysis, Biology, Immunofluorescence, Article, Frameshift mutation, Gene Frequency, Pregnancy, Genetics, medicine, Humans, Frameshift Mutation, Allele frequency, Gene, Genetic Association Studies, Genetics (clinical), Adaptor Proteins, Signal Transducing, Sequence Deletion, Base Sequence, medicine.diagnostic_test, HEK 293 cells, Haplotype, Pregnancy Outcome, Proteins, Colocalization, Hydatidiform Mole, Molecular biology, NLRP7, Pedigree, Abortion, Spontaneous, Protein Transport, HEK293 Cells, Haplotypes, Case-Control Studies, Uterine Neoplasms, Female, Chorionic Villi

Abstract

To date, two maternal-effect genes have been shown to have causative roles in recurrent hydatidiform moles (RHMs); NLRP7 that is mutated in 48-60% of patients with RHMs and C6orf221 (HUGO-approved nomenclature is now KHDC3L), a recently identified gene, that is mutated in 14% of patients with RHMs who are negative for NLRP7 mutations. We sequenced KHDC3L in 97 patients with RHMs and reproductive loss who are mostly negative for NLRP7 mutations. We identified three unrelated patients, each homozygous for one of the two protein-truncating mutations, a novel 4-bp deletion resulting in a frameshift, c.299_302delTCAA, p.Ile100Argfs*2, and a previously described 4-bp deletion, c.322_325delGACT, p.Asp108Ilefs*30, transmitted on a shared haplotype to three patients from different populations. We show that five HM tissues from one of these patients are diploid and biparental similar to HMs from patients with two defective NLRP7 mutations. Using immunofluorescence, we show that KHDC3L protein displays a juxta perinuclear signal and colocalizes with NLRP7 in lymphoblastoid cell lines from normal subjects. Using cell lines from patients, we demonstrate that the KHDC3L mutations do not change the subcellular localization of the protein in hematopoietic cells. Our data highlight the similarities between the two causative genes for RHMs, KHDC3L and NLRP7, in their subcellular localization, the parental contribution to the HM tissues caused by them, and the presence of several founder mutations and variants in both of them indicating positive selection and adaptation.

Published

2012

47. Brachytelephalangic chondrodysplasia punctata

Author

Manju Ghosh, Ganesh Prasad Das, Rashmi Shukla, Neerja Gupta, and Madhulika Kabra

Subjects

Heart Defects, Congenital, Male, Chondrodysplasia Punctata, Chondrodystrophy, Developmental Disabilities, Pathology and Forensic Medicine, Finger Phalanges, medicine, Humans, Chondrodysplasia punctata, Child, Arylsulfatase E, Genetics (clinical), Optic nerve hypoplasia, business.industry, Brachydactyly, Infant, Newborn, Infant, Genetic Diseases, X-Linked, Bone age, General Medicine, Anatomy, medicine.disease, Radiography, Phenotype, Facial Asymmetry, Dysplasia, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, business, Epiphyseal stippling

Abstract

Chondrodysplasia punctata (CDP) is a heterogenous group of skeletal dysplasias characterized by aberrant bone mineralization, manifesting radiologically as epiphyseal stippling. Among this group, brachytelephalangic dysplasia, a benign form of CDP (CDPX1), is probably under-reported. It is an X-linked recessive disorder and is characterized by a flat nasal tip, short columella and maxillary hypoplasia, involvement of terminal phalanges, and stippled chondrodystrophy. This paper presents a clinical series of 13 patients with brachytelephalangic dysplasia. These patients enrolled during 2002-2006 were re-evaluated and their dysmorphic features were compiled in a predesigned proforma. Skeletal survey, karyotype, cardiac evaluation, and ophthalmic evaluation were planned for all the cases. Out of 13 patients, 10 were males and three were females. All patients had flat facies, a depressed nasal bridge, a hypoplastic nose, a short philtrum, notched alae nasi, brachydactyly, and hypoplastic terminal phalanges. In addition, congenital heart disease, optic nerve hypoplasia, and developmental delay were found in a few patients. Radiography showed hypoplastic terminal phalanges, delayed bone age (1/13), epiphyseal stippling in carpal (3/13) and tarsal bones (2/13), sacral bone (1/13), and bullet-shaped lumbar vertebra (1/13). Cranial neuroimaging, thyroid profile, and karyotype carried out in a few were normal. The present paper discusses various clinical features and associated abnormalities in patients with brachytelephalangic dysplasia (CDPX1) to further delineate the phenotype. The presence of a similar phenotype in females suggests the possibility of another locus or manifestation of disease in heterozygous females. Arylsulfatase E gene analysis would further help in establishing the genotype-phenotype correlation.

Published

2012

48. Novel non-identical MECP2 mutations in Rett syndrome family: A rare presentation

Author

Rajni Khajuria, Sheffali Gulati, Neerja Gupta, Manju Ghosh, Savita Sapra, Madhulika Kabra, and Veena Kalra

Subjects

Male, Proband, Methyl-CpG-Binding Protein 2, Genetic counseling, DNA Mutational Analysis, Rett syndrome, Biology, Gene mutation, MECP2, Frameshift mutation, Developmental Neuroscience, Rett Syndrome, medicine, Humans, Missense mutation, Family, Genetics, Base Sequence, General Medicine, medicine.disease, Pedigree, Child, Preschool, Mutation, Pediatrics, Perinatology and Child Health, Mutation (genetic algorithm), Female, Neurology (clinical)

Abstract

Introduction Rett syndrome (RS), an X-linked neurodevelopmental disorder and the common cause of mental retardation in females, is caused by methyl CpG binding protein 2 ( MECP2 ) gene mutations with a frequency of more than 95% in classical Rett patients. Majority of RS cases are sporadic but few familial cases caused by either skewed X-chromosome inactivation in healthy female carriers or mosaicism in male carriers are also reported. Most of the times, the mutation carried in a family is the same as found in affected child. Methods and results Here we report a unique family carrying non-identical MECP2 mutations in exon 2 wherein the proband with classical RS was carrying a de-novo early truncating frameshift mutation while her asymptomatic mother was carrying a missense mutation, both predicted as pathogenic mutations. Conclusions These findings further validate the importance of MECP2 mutation screening in parents of all mutation positive patients and careful evaluation of the pathogenicity of the mutation found in asymptomatic carriers before providing genetic counseling to the family. The results also propose the role of other factors including other gene mutations, environmental and epigenetics factors in modifying the expression of MECP2 mutations.

Published

2012

49. Molecular analysis of ABCD1 gene in Indian patients with X-linked Adrenoleukodystrophy

Author

Arun Gupta, Raju Sharma, Manju Ghosh, Neerja Gupta, Sheffali Gulati, Madhulika Kabra, Pallavi Shukla, Veena Kalra, and S. Vasisht

Subjects

Genetics, Gel electrophoresis, Pregnancy, Genetic counseling, Biochemistry (medical), Clinical Biochemistry, India, Prenatal diagnosis, General Medicine, Biology, medicine.disease, ATP Binding Cassette Transporter, Subfamily D, Member 1, Biochemistry, medicine.anatomical_structure, Prenatal Diagnosis, medicine, Humans, Chorionic villi, ATP-Binding Cassette Transporters, Female, Adrenoleukodystrophy, Abnormality, Gene

Abstract

Background X-linked Adrenoleukodystrophy (X-ALD), with an incidence of 1:14,000 is the most frequent monogenic demyelinating disorder worldwide. The principal biochemical abnormality in X-ALD is the increased levels of saturated, unbranched very long chain fatty acids (VLCFA). It is caused by mutations in ABCD1 gene. No molecular data on X-ALD is available in India and mutational spectrum in Indian patients is not known. Methods We standardized conformation sensitive gel electrophoresis (CSGE) method to detect mutations in ABCD1 gene in twenty Indian patients with X-ALD. The results were confirmed by sequencing. Genotype–phenotype correlation was also attempted. Prenatal diagnosis (PND) in one family was done using chorionic villi (CV) sample at 12 weeks of gestation. Results Out of twenty, causative mutations could be identified in twelve patients (60%). Six reported and four novel mutations were identified. Three polymorphisms were also observed. No hot spot was found. No significant genotype–phenotype correlation could be established. Conclusions The study identified the mutation spectrum of Indian X-ALD patients, which enabled us to offer accurate genetic counseling, carrier detection and prenatal diagnosis where needed.

Published

2011

50. Recombinant macrophage targeted enzyme replacement therapy for Gaucher disease in India

Author

Neerja Gupta, Aabha Nagral, Pramod K. Mistry, Ishwar C. Verma, Ratna Dua Puri, Madhulika Kabra, Prerna Mewawalla, Shubha R. Phadke, Sujatha Jagadeesh, and Priya S. Kishnani

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Adolescent, Imiglucerase, Treatment outcome, India, Disease, law.invention, law, Humans, Medicine, Macrophage, Enzyme Replacement Therapy, Child, Retrospective Studies, Gaucher Disease, business.industry, Maternal and child health, Macrophages, Infant, nutritional and metabolic diseases, Retrospective cohort study, Enzyme replacement therapy, Recombinant Proteins, nervous system diseases, Surgery, Treatment Outcome, Child, Preschool, Pediatrics, Perinatology and Child Health, Immunology, Recombinant DNA, Glucosylceramidase, Female, business, medicine.drug

Abstract

Gaucher disease in India has been reported only in a few case reports from India. The aim of the study was to assess the response to enzyme replacement therapy in Indian patients with Gaucher disease.Retrospective analysis of patients receiving CHO-derived recombinant macrophage-targetted glucocorebrosidase.Five centers from India with experience in treating lysosomal storage disorders.The diagnosis of Gaucher disease was confirmed by low glucocerebrosidase levels, though it was first made on splenectomy in 8 and on bone marrow examination in 9 patients. Twenty five of 52 patients diagnosed with Gaucher disease (17 Type I, 8 mild Type III) received treatment for6 months. Indications for treatment included symptomatic anemia, thrombo-cytopenia, organomegaly, bone disease or mild neurological symptoms leading to impairment of quality of life. Patients with significant neurological involvement were excluded. The drug infusions were given intravenously every 15 days.Hemoglobin, platelet counts, liver and spleen volumes and growth parameters.22 of the 25 children who survived were analyzed. After 6 months of treatment, the mean (range) increase in hemoglobin was 1.5 (-3.4 to 6.1) g/dL (P=0.01) and in platelet count was 32 x 10(9)/L (-98.5 x 109 to 145.5 x10(9))/L (P=0.02). The mean (range) increase in weight was 3 kg (-5.6 to 10.5) (P=0.04) and in height was 7.1 cm (0 to 26.5) (P=0.0003). Liver size decreased by a mean (range) of 38.5% (- 5.5 to 86.7) (P=0.0003) and the spleen size by 34.8% (0 to 91.7) (P=0.004). All patients had improvement in bone pains and in 2 patients, neurological symptoms improved with others remaining static.This is the first reported cohort of patients in India reporting our experience with imiglucerase enzyme replacement therapy for treatment of Gaucher Disease in India.

Published

2011