A novel point mutation in an acceptor splice site of intron 32 (IVS32 A -12 →G) but no exon 3 mutations in the glycogen debranching enzyme gene in a homozygous patient with glycogen storage disease type IIIb

Okubo, Minoru; Horinishi, Asako; Nakamura, Norimasa; Aoyama, Yoshiko; Hashimoto, Masaji; Endo, Yuzo; Murase, Toshio

doi:10.1007/s004390050646

Cited by 28 publications

(20 citation statements)

References 15 publications

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“…Patient 12 (female, age 41 years) had type IIIb and was compound heterozygous for the novel p.Arg343Trp mutation and c.4260-12A>G in intron 32. c.4260-12A>G was previously described and associated with IIIb as well as IIIa (Okubo et al 1998;Shaiu et al 2000). This patients' phenotype was severe IIIb and a case report on her was published after she received an orthotopic liver transplantation after being diagnosed with liver cirrhosis (Haagsma et al 1997).…”

Section: Discussionmentioning

confidence: 79%

Mutation Analysis in Glycogen Storage Disease Type III Patients in the Netherlands: Novel Genotype-Phenotype Relationships and Five Novel Mutations in the AGL Gene

et al. 2012

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Section: Discussionmentioning

confidence: 79%

Mutation Analysis in Glycogen Storage Disease Type III Patients in the Netherlands: Novel Genotype-Phenotype Relationships and Five Novel Mutations in the AGL Gene

et al. 2012

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“…We have reported the heterogeneity of AGL mutations in Japan. Eleven different mutations have been identified in our studies (Horinishi et al 2002;Okubo et al 1996Okubo et al , 1998Okubo et al , 1999Okubo et al , 2000a. Lucchiari et al (2002) discovered genetic heterogeneity in Italian patients also, although one splicing mutation (IVS21+1G>A) accounts for 28%.…”

Section: Introductionmentioning

confidence: 68%

Molecular characterization of Egyptian patients with glycogen storage disease type IIIa

Endo¹,

Fateen

Aoyama³

et al. 2005

J Hum Genet

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Glycogen storage disease type IIIa (GSD IIIa) is an autosomal recessive disorder characterized by excessive accumulation of abnormal glycogen in the liver and muscles and caused by a deficiency in the glycogen debranching enzyme. The spectrum of AGL mutations in GSD IIIa patients depends on ethnic group-prevalent mutations have been reported in the North African Jewish population and in an isolate such as the Faroe islands, because of the founder effect, whereas heterogeneous mutations are responsible for the pathogenesis in Japanese patients. To shed light on molecular characteristics in Egypt, where high rate of consanguinity and large family size increase the frequency of recessive genetic diseases, we have examined three unrelated patients from the same area in Egypt. We identified three different individual AGL mutations; of these, two are novel deletions [4-bp deletion (750-753delAGAC) and 1-bp deletion (2673delT)] and one the nonsense mutation (W1327X) previously reported. All are predicted to lead to premature termination, which completely abolishes enzyme activity. Three consanguineous patients are homozygotes for their individual mutations. Haplotype analysis of mutant AGL alleles showed that each mutation was located on a different haplotype. Our results indicate the allelic heterogeneity of the AGL mutation in Egypt. This is the first report of AGL mutations in the Egyptian population.

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“…Those studies revealed that the spectrum of AGL mutations in GSD III patients depends on ethnic grouping. For example, specific mutations were prevalent in Jewish GSD III patients (Parvari et al 1997) and in an isolated region such as the Faroe Islands (Santer et al 2001) because of founder effect, while heterogeneous mutations were found in Japanese patients (Horinishi et al 2002;Okubo et al 1996Okubo et al , 1998Okubo et al , 1999Okubo et al , 2000a. In Caucasian and Italian populations a few mutations accounted for a quarter of GSD III patients, but the rest of the mutations were heterogeneous (Lucchiari et al 2002a, b;Shen and Chen 2002).…”

Section: Introductionmentioning

confidence: 99%

Molecular analysis of the AGL gene: heterogeneity of mutations in patients with glycogen storage disease type III from Germany, Canada, Afghanistan, Iran, and Turkey

Endo¹,

Horinishi²,

Vorgerd

et al. 2006

J Hum Genet

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Glycogen storage disease type III (GSD III) is an autosomal recessive disorder characterized by excessive accumulation of abnormal glycogen in the liver and/or muscles and caused by deficiency in the glycogen debranching enzyme (AGL). Previous studies have revealed that the spectrum of AGL mutations in GSD III patients depends on ethnic grouping. We investigated nine GSD III patients from Germany, Canada, Afghanistan, Iran, and Turkey and identified six novel AGL mutations: one nonsense (W255X), three deletions (1019delA, 3202-3203delTA, and 1859-1869del11-bp), and two splicing mutations (IVS7 + 5G > A and IVS21 + 5insA), together with three previously reported ones (R864X, W1327X, and IVS21 + 1G > A). All mutations are predicted to lead to premature termination, which abolishes enzyme activity. Our molecular study on GSD III patients of different ethnic ancestry showed allelic heterogeneity of AGL mutations. This is the first AGL mutation report for German, Canadian, Afghan, Iranian and Turkish populations.

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A novel point mutation in an acceptor splice site of intron 32 (IVS32 A -12 →G) but no exon 3 mutations in the glycogen debranching enzyme gene in a homozygous patient with glycogen storage disease type IIIb

Cited by 28 publications

References 15 publications

Mutation Analysis in Glycogen Storage Disease Type III Patients in the Netherlands: Novel Genotype-Phenotype Relationships and Five Novel Mutations in the AGL Gene

Mutation Analysis in Glycogen Storage Disease Type III Patients in the Netherlands: Novel Genotype-Phenotype Relationships and Five Novel Mutations in the AGL Gene

Molecular characterization of Egyptian patients with glycogen storage disease type IIIa

Molecular analysis of the AGL gene: heterogeneity of mutations in patients with glycogen storage disease type III from Germany, Canada, Afghanistan, Iran, and Turkey

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