A R59W mutation in human protoporphyrinogen oxidase results in decreased enzyme activity and is prevalent in South Africans with variegate porphyria

Meissner, Peter N.; Dailey, Tamara A.; Hift, Richard; Ziman, Mel; Corrigall, Anne V.; Roberts, Andrew; Meissner, D.; Kirsch, Ralph E.; Dailey, Harry A.

doi:10.1038/ng0596-95

Cited by 201 publications

(193 citation statements)

References 14 publications

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“…Recently, this mutation has been documented as the first mutation in AIP associated with a founder effect in North America with the identified founding couple (Greene-Davis et al 1997). Such a founder effect has been well documented in variegate porphyria, the other form of acute porphyria (Dean 1971;Meissner et al 1996;Warnich et al 1996;Groenewald et al 1998), and has also been observed in other AIP patients (De Siervi et al 1999). The other mutation in Japan, reported by Morita et al (1995), is a single base substitution C-to-T in exon 8 of the gene, which was the same as a common mutation in the Netherlands (Gu et al 1994).…”

Section: Discussionmentioning

confidence: 99%

Two deletion mutations in the hydroxymethylbilane synthase gene in two unrelated Japanese patients with acute intermittent porphyria

et al. 2000

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Acute intermittent porphyria (AIP) is an autosomal dominant inherited disease caused by a decreased activity of hydroxymethylbilane synthase (HMBS). Regarding the abnormalities of the HMBS gene, many different mutations have been reported worldwide; however, few families from Japan have been studied. In this work, we investigated the presence of mutations in two unrelated Japanese patients with AIP. Mutational analysis was performed using the polymerase chain reaction-single strand conformation polymorphism (SSCP) method, followed by DNA sequencing. Reliable restriction enzyme cleavage assays were also established for the pedigree analyses. Unique SSCP patterns were noted in exons 12 and 15 of the HMBS gene. Sequencing revealed different mutations in each patient: a two-base deletion of CT at nucleotide 730-731 (730delCT), and also a two-base deletion of CA at position 982-983 (982delCA). Both of the deletion mutations lead to truncated proteins with an abnormal C-terminus, which would be expected to decrease the stability and/or activity of HMBS. Using the cleavage assays, we were able to definitively identify gene carriers in the family. This study adds a novel mutation to those that have been previously reported, and emphasizes that molecular analysis would be very useful not only for the identification of asymptomatic gene carriers in the family but also for the detection of ancestral founders in porphyria families.

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Section: Discussionmentioning

confidence: 99%

Two deletion mutations in the hydroxymethylbilane synthase gene in two unrelated Japanese patients with acute intermittent porphyria

et al. 2000

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“…VP mutations also show high heterogeneity with the exception of founder effect mutations e.g. mutation R5 9W in South Africa [7,19].…”

Section: Variegate Porphyriamentioning

confidence: 99%

“…AIP prevalence in Argentina is about 1/125 000 inhabitants [6]. VP is most frequently reported in South African Republic (1/300 inhabitants) due to founder effect [7]. VP prevalence in Finland is estimated at 2/100 000 inhabitants [8]; in Argentina at 1/600 000 [6].…”

Section: Epidemiology Datamentioning

confidence: 99%

Clinical, Biochemical and Molecular Characteristics of the Main Types of Porphyria

2016

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Porphyrias are diverse disorders that arise from various inherited enzyme defects in the heme biosynthesis pathway, except for porphyria cutanea tarda (PCT), in which the enzyme deficiency in most cases is acquired. The biosynthetic blocks resulting from the defective enzymes are largely expressed either in the liver or bone marrow, the sites where the majority of heme is produced. Although the pathophysiologic mechanisms of the clinical manifestations of the porphyrias are not fully understood, two cardinal features prevail: skin photosensitivity and neurologic symptoms of intermittent autonomic neuropathy, acute neurovisceral attacks, and disorders of the nervous system. The primary diagnosis of the proband is based on biochemical testing, which is not always able to identify acute porphyrias, especially in asymptomatic family carriers when heme precursors and porphyrins excretion is normal, low-normal and high-reduced values of enzyme activity overlap, and hematological diseases responsible for abnormal blood cells distribution coexist. Molecular analysis of gene mutations responsible for each type of porphyria is the best diagnostic approach for symptomatic as well as presymptomatic gene carriers (Adv Clin Exp Med 2016, 25, 2, 361-368).

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“…6 Genetic analysis would be the only reliable tool to establish a correct diagnosis of Porphyria even though the high genetic heterogeneity makes this approach difficult. Although restricted geographic areas seem to have a high prevalence of specific molecular abnormality, 7 most of the reported mutations have been detected in a single case or a family. [8][9][10] Moreover, approximately 10% of porphyria cases remain devoid of molecular diagnosis.…”

Section: Introductionmentioning

confidence: 99%

Multiplex ligation-dependent probe amplification: a novel approach for genetic diagnosis of Porphyria

et al. 2009

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Porphyrias are disorders caused by the genetic defects of enzymes of the heme pathway and are characterized by such a wide genetic heterogeneity that even the molecular analysis is not always decisive for a correct diagnosis. In the past few years, deletion with a size range of few kilobase pairs have been reported. These peculiar mutations, missed by both sequencing and cytogenetic techniques, have been identified by time consuming and technically demanding methods. To provide a rapid and sensitive method for the detection of deletions responsible for porphyria, we successfully designed and tested seven chemically synthesized probe sets specific for each heme gene and their flanking regions, to be used in multiplex ligation-dependent probe amplification technique.

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A R59W mutation in human protoporphyrinogen oxidase results in decreased enzyme activity and is prevalent in South Africans with variegate porphyria

Cited by 201 publications

References 14 publications

Two deletion mutations in the hydroxymethylbilane synthase gene in two unrelated Japanese patients with acute intermittent porphyria

Two deletion mutations in the hydroxymethylbilane synthase gene in two unrelated Japanese patients with acute intermittent porphyria

Clinical, Biochemical and Molecular Characteristics of the Main Types of Porphyria

Multiplex ligation-dependent probe amplification: a novel approach for genetic diagnosis of Porphyria

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