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We are analyzing https://link.springer.com/article/10.1007/s10571-007-9192-7.

Title:
Molecular Pathogenesis of Wilson Disease Among Indians: A Perspective on Mutation Spectrum in ATP7B gene, Prevalent Defects, Clinical Heterogeneity and Implication Towards Diagnosis | Cellular and Molecular Neurobiology
Description:
Aims We aim to identify the molecular defects in the ATP7B, the causal gene for Wilson disease (WD), in eastern Indian patients and attempt to assess the overall mutation spectrum in India for detection of mutant allele for diagnostic purposes. Methods Patients from 109 unrelated families and their first-degree relatives comprising 400 individuals were enrolled in this study as part of an ongoing project. Genomic DNA was prepared from the peripheral blood of Indian WD patients. PCR was done to amplify the exons and flanking regions of the WD gene followed by sequencing, to identify the nucleotide variants. Results In addition to previous reports, we recently identified eight mutations including three novel (c.3412 + 1G > A, c.1771 G > A, c.3091 A > G) variants, and identified patients with variable phenotype despite similar mutation background suggesting potential role of modifier locus. Conclusions So far we have identified 17 mutations in eastern India including five common mutations that account for 44% of patients. Comparative study on WD mutations between different regions of India suggests high genetic heterogeneity and the absence of a single or a limited number of common founder mutations. Genotype–phenotype correlation revealed that no particular phenotype could be assigned to a particular mutation and even same set of mutations in different patients showed different phenotypes.
Website Age:
28 years and 1 months (reg. 1997-05-29).

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  • Science
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🌠 Phenomenal Traffic: 5M - 10M visitors per month


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Keywords {🔍}

disease, article, google, scholar, wilson, pubmed, cas, mutations, patients, gene, atpb, molecular, indian, mutation, analysis, wilsons, ray, india, genet, privacy, cookies, content, research, gupta, study, correlation, access, publish, search, spectrum, prevalent, clinical, september, prasad, author, data, including, information, log, journal, pathogenesis, defects, heterogeneity, arnab, chattopadhyay, dey, gangopadhyay, kunal, detection, variants,

Topics {✒️}

genotype/phenotype/copper atpase activity human genetics division month download article/chapter glucose-6-phosphate dehydrogenase deficiency genotype–phenotype correlation revealed related subjects full article pdf privacy choices/manage cookies wilson disease gene familial nervous disease article gupta molecular neurobiology aims wilson disease mutations eastern indian patients european economic area thomas gr cold spring harbor progressive lenticular degeneration pre-doctoral fellowship post-doctoral fellowship indian wd patients article cellular clinical heterogeneity conditions privacy policy nucleotide variants clinical phenotype eastern india including genotype–phenotype correlation accepting optional cookies poonam nasipuri oral zinc therapy similar content walshe jm wilson disease article log atp7b gene mutations common founder mutations common mutations r778g das sk author correspondence kunal ray disease patients journal finder publish indian institute genomic dna check access instant access mutation analysis article cite variants

Schema {🗺️}

WebPage:
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         headline:Molecular Pathogenesis of Wilson Disease Among Indians: A Perspective on Mutation Spectrum in ATP7B gene, Prevalent Defects, Clinical Heterogeneity and Implication Towards Diagnosis
         description:Aims We aim to identify the molecular defects in the ATP7B, the causal gene for Wilson disease (WD), in eastern Indian patients and attempt to assess the overall mutation spectrum in India for detection of mutant allele for diagnostic purposes. Methods Patients from 109 unrelated families and their first-degree relatives comprising 400 individuals were enrolled in this study as part of an ongoing project. Genomic DNA was prepared from the peripheral blood of Indian WD patients. PCR was done to amplify the exons and flanking regions of the WD gene followed by sequencing, to identify the nucleotide variants. Results In addition to previous reports, we recently identified eight mutations including three novel (c.3412 + 1G > A, c.1771 G > A, c.3091 A > G) variants, and identified patients with variable phenotype despite similar mutation background suggesting potential role of modifier locus. Conclusions So far we have identified 17 mutations in eastern India including five common mutations that account for 44% of patients. Comparative study on WD mutations between different regions of India suggests high genetic heterogeneity and the absence of a single or a limited number of common founder mutations. Genotype–phenotype correlation revealed that no particular phenotype could be assigned to a particular mutation and even same set of mutations in different patients showed different phenotypes.
         datePublished:2007-09-02T00:00:00Z
         dateModified:2007-09-02T00:00:00Z
         pageStart:1023
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             K-F ring
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            Neurosciences
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      headline:Molecular Pathogenesis of Wilson Disease Among Indians: A Perspective on Mutation Spectrum in ATP7B gene, Prevalent Defects, Clinical Heterogeneity and Implication Towards Diagnosis
      description:Aims We aim to identify the molecular defects in the ATP7B, the causal gene for Wilson disease (WD), in eastern Indian patients and attempt to assess the overall mutation spectrum in India for detection of mutant allele for diagnostic purposes. Methods Patients from 109 unrelated families and their first-degree relatives comprising 400 individuals were enrolled in this study as part of an ongoing project. Genomic DNA was prepared from the peripheral blood of Indian WD patients. PCR was done to amplify the exons and flanking regions of the WD gene followed by sequencing, to identify the nucleotide variants. Results In addition to previous reports, we recently identified eight mutations including three novel (c.3412 + 1G > A, c.1771 G > A, c.3091 A > G) variants, and identified patients with variable phenotype despite similar mutation background suggesting potential role of modifier locus. Conclusions So far we have identified 17 mutations in eastern India including five common mutations that account for 44% of patients. Comparative study on WD mutations between different regions of India suggests high genetic heterogeneity and the absence of a single or a limited number of common founder mutations. Genotype–phenotype correlation revealed that no particular phenotype could be assigned to a particular mutation and even same set of mutations in different patients showed different phenotypes.
      datePublished:2007-09-02T00:00:00Z
      dateModified:2007-09-02T00:00:00Z
      pageStart:1023
      pageEnd:1033
      sameAs:https://doi.org/10.1007/s10571-007-9192-7
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         WD
         Wilson Disease
          K-F ring
         SNP
         ATP7B
         Neurosciences
         Cell Biology
         Neurobiology
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               name:Bangur Institute of Neuroscience and Psychiatry, Kolkata, India
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      affiliation:
            name:Bangur Institute of Neuroscience and Psychiatry
            address:
               name:Bangur Institute of Neuroscience and Psychiatry, Kolkata, India
               type:PostalAddress
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      affiliation:
            name:Indian Institute of Chemical Biology
            address:
               name:Molecular and Human Genetics Division, Indian Institute of Chemical Biology, Kolkata, India
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      name:Bangur Institute of Neuroscience and Psychiatry, Kolkata, India
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