<i>GALNS</i> mutations in Indian patients with mucopolysaccharidosis IVA

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

doi:10.1002/ajmg.a.36735

Cited by 34 publications

(48 citation statements)

References 49 publications

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“…We hypothesize that the high rate of homozygous biallelic mutations (6/9; 67%) in the absence of consanguinity is due to the endogamous marriages within the same caste or community. Similar trends are also reported in other recessive disorders in India [Dalal et al, ; Bidchol et al, ].…”

Section: Discussionsupporting

confidence: 85%

KCNQ1 mutations associated with Jervell and Lange–Nielsen syndrome and autosomal recessive Romano–Ward syndrome in India—expanding the spectrum of long QT syndrome type 1

Vyas

Puri

Namboodiri

et al. 2016

American J of Med Genetics Pt A

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Long QT syndrome type 1 (LQT1) is the most common type of all Long QT syndromes (LQTS) and occurs due to mutations in KCNQ1. Biallelic mutations with deafness is called Jervell and Lange-Nielsen syndrome (JLNS) and without deafness is autosomal recessive Romano-Ward syndrome (AR RWS). In this prospective study, we report biallelic mutations in KCNQ1 in Indian patients with LQT1 syndrome. Forty patients with a clinical diagnosis of LQT1 syndrome were referred for molecular testing. Of these, 18 were excluded from the analysis as they did not fulfill the inclusion criteria of broad T wave ECG pattern of the study. Direct sequencing of KCNQ1 was performed in 22 unrelated probands, parents and at-risk family members. Mutations were identified in 17 patients, of which seven had heterozygous mutations and were excluded in this analysis. Biallelic mutations were identified in 10 patients. Five of 10 patients did not have deafness and were categorized as AR RWS, the rest being JLNS. Eight mutations identified in this study have not been reported in the literature and predicted to be pathogenic by in silico analysis. We hypothesize that the homozygous biallelic mutations identified in 67% of families was due to endogamous marriages in the absence of consanguinity. This study presents biallelic gene mutations in KCNQ1 in Asian Indian patients with AR JLNS and RWS. It adds to the scant worldwide literature of mutation studies in AR RWS. © 2016 Wiley Periodicals, Inc.

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Section: Discussionsupporting

confidence: 85%

KCNQ1 mutations associated with Jervell and Lange–Nielsen syndrome and autosomal recessive Romano–Ward syndrome in India—expanding the spectrum of long QT syndrome type 1

Vyas

Puri

Namboodiri

et al. 2016

American J of Med Genetics Pt A

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“…It is known that even in the absence of actual consanguinity, inbreeding can lead to homozygosity for recessive mutations and thereby result in disease in the offspring [Pemberton et al, ]. This is not an uncommon phenomenon in many regions of India where inbreeding within small communities in quite prevalent and similar findings have been documented in previous molecular genetic studies from India [Dalal et al, ; Bidchol et al, ].…”

Section: Discussionmentioning

confidence: 59%

Spectrum of SMPD1 mutations in Asian‐Indian patients with acid sphingomyelinase (ASM)‐deficient Niemann–Pick disease

Ranganath

Matta

Wangnekar

et al. 2016

American J of Med Genetics Pt A

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Acid sphingomyelinase (ASM)-deficient Niemann-Pick disease is an autosomal recessive lysosomal storage disorder caused by biallelic mutations in the SMPD1 gene. To date, around 185 mutations have been reported in patients with ASM-deficient NPD world-wide, but the mutation spectrum of this disease in India has not yet been reported. The aim of this study was to ascertain the mutation profile in Indian patients with ASMdeficient NPD. We sequenced SMPD1 in 60 unrelated families affected with ASM-deficient NPD. A total of 45 distinct pathogenic sequence variants were found, of which 14 were known and 31 were novel. The variants included 30 missense, 4 nonsense, and 9 frameshift (7 single base deletions and 2 single base insertions) mutations, 1 indel, and 1 intronic duplication. The pathogenicity of the novel mutations was inferred with the help of the mutation prediction software MutationTaster, SIFT, Polyphen-2, PROVEAN, and HANSA. The effects of the identified sequence variants on the protein structure were studied using the structure modeled with the help of the SWISS-MODEL workspace program. The p. (Arg542 Ã ) (c.1624C>T) mutation was the most commonly identified mutation, found in 22% (26 out of 120) of the alleles tested, but haplotype analysis for this mutation did not identify a founder effect for the Indian population. To the best of our knowledge, this is the largest study on mutation analysis of patients with Festschrift honoring John C. Carey

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“…Recent years have seen publication of genetic and mutation profiles for large case series of osteogenesis imperfecta, skeletal dysplasias, and lysosomal storage disorders. These studies have revealed the unique molecular profile of patients from the India with identification of many novel mutations not previously reported in other populations (Gorospe et al 2004;Pathak et al 2010;Sachdeva et al 2011Sachdeva et al , 2012Shukla et al 2011;Bashyam et al 2012;Dalal et al 2012;Mistri et al 2012;Bidchol et al 2014;Ankala et al 2015;Stephen et al 2015; A. Uttarilli, P. Ranganath, S.J.M. Nurul Jain, K.P.…”

Section: Academic Programs In Medical Geneticsmentioning

confidence: 93%

“…Use of SNP microarray to identify regions of homozygosity and candidate genes in these regions is a strategy which can be successfully used in the consanguineous families (Stephen et al 2015). Some conditions found to be relatively common have been Van Der Knaap disease with a founder mutation in the Agarwal community from north western India, calpainopahy, recessive forms of Osteogenesis imperfecta, Progressive pseudorheumatoid arthropthy of childhood and Handigodu disease from a specific community in South India (Gorospe et al 2004;Pathak et al 2010;Sachdeva et al 2011Sachdeva et al , 2012Shukla et al 2011;Bashyam et al 2012;Dalal et al 2012;Bidchol et al 2014;Ankala et al 2015). However, the available data on monogenic malformation syndromes and metabolic disorders from India though extensive, represents only tip of the iceberg as a large population still does not have access to the clinical genetics services due to cost and limited number of genetic centers.…”

Section: Spectrum Of Genetic Disordersmentioning

confidence: 99%

Medical genetics and genomic medicine in India: current status and opportunities ahead

Aggarwal

Phadke

2015

Molec Gen & Gen Med

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GALNS mutations in Indian patients with mucopolysaccharidosis IVA

Cited by 34 publications

References 49 publications

KCNQ1 mutations associated with Jervell and Lange–Nielsen syndrome and autosomal recessive Romano–Ward syndrome in India—expanding the spectrum of long QT syndrome type 1

KCNQ1 mutations associated with Jervell and Lange–Nielsen syndrome and autosomal recessive Romano–Ward syndrome in India—expanding the spectrum of long QT syndrome type 1

Spectrum of SMPD1 mutations in Asian‐Indian patients with acid sphingomyelinase (ASM)‐deficient Niemann–Pick disease

Medical genetics and genomic medicine in India: current status and opportunities ahead

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