Studies in porphyria: functional evidence for a partial deficiency of ferrochelatase activity in mitogen-stimulated lymphocytes from patients with erythropoietic protoporphyria.

Sassa, Shigeru; Zalar, Gregory L.; Poh–Fitzpatrick, Maureen B.; Anderson, Karl E.; Kappas, Attallah

doi:10.1172/jci110520

Cited by 30 publications

(12 citation statements)

References 24 publications

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“…Although the parents were available for ferrochelatase assays in an early study, they and several other members of this family were no longer available for the molecular studies on the ferrochelatase defect, for reasons beyond our control. Partial ferrochelatase deficiency (-50%) is also known to occur in both asymptomatic carriers and clinically affected patients in other EPP families (6,14). Thus the occurrence of '50% ferrochelatase deficiency both in the father and in the daughter is similar to that in other EPP families and is compatible with an autosomal dominant inheritance of EPP in this family.…”

supporting

confidence: 68%

“…In humans, EPP is thought to be an autosomal dominant disease, but the frequency of its clinical expression is highly variable (2). Previous studies have shown that, in patients with EPP, the activity of ferrochelatase (protoheme ferro-lyase, EC 4.99.1.1) is decreased to -50% compared with normal levels, in all tissues and isolated cell preparations so far examined: e.g., bone marrow (3), liver (4), cultured skin fibroblasts (5), and lymphoblasts (6). A deficiency of ferrochelatase activity is consistent with the marked increase in protoporphyrin IX, a substrate for the enzyme, observed in erythrocytes, plasma, and liver of patients with EPP, and accounts for cutaneous photosensitivity in this disorder.…”

mentioning

confidence: 99%

“…Protoporphyrin concentrations in her erythrocytes, plasma, and stool were markedly elevated (Table 1), and erythrocyte porphyrins consisted almost exclusively of free, not Zn-chelated, protoporphyrin (13). Ferrochelatase activity, as determined by an assay based on the ability of lymphocytes to form protoporphyrin from its precursor, 6-aminolevulinic acid (6), indicated that the proband's enzyme activity was about one-half (46.5%) the normal level (Table 1). These findings in the proband's cells are compatible with the diagnosis of EPP.…”

mentioning

confidence: 99%

“…(mean + SEM, n = 8) (mean ± SEM, n = 9) As an indirect assay for ferrochelatase, protoporphyrin IX formation by lymphocytes was determined as described previously (6). Lymphocytes were incubated with phytohemagglutinin (PHA) and pokeweed mitogen (PWM) for 3 days and then with 0.6 mM 8-aminolevulinic acid (ALA) for 24 h. Protoporphyrin IX accumulation found by this assay has been shown to be inversely correlated with ferrochelatase activity (6). Both PHA/PWM-stimulated lymphocytes and Epstein-Barr virus-transformed lymphoblastoid cells give similar results with this assay (unpublished observation).…”

mentioning

confidence: 99%

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The molecular defect of ferrochelatase in a patient with erythropoietic protoporphyria.

Nakahashi¹,

Fujita²,

Taketani³

et al. 1992

Proc. Natl. Acad. Sci. U.S.A.

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The molecular basis of an inherited defect of ferrochelatase in a patient with erythropoietic protoporphyria (EPP) was investigated. Ferrochelatase is the terminal enzyme in the heme biosynthetic pathway and catalyzes the insertion of ferrous iron into protoporphyrin IX to form heme. In EpsteinBarr virus-transformed lymphoblastoid cells from a proband with EPP, enzyme activity, an immunochemically quantifiable protein, and mRNA content of ferrochelatase were about one-half the normal level. In contrast, the rate of ftrnription of ferrochelatase mRNA in the proband's cells was normal, suggesting that decreased ferrochelatase mRNA is due to an unstable transcript. cDNA clones encoding ferrochelatase in the proband, isolated by amplification using the polymerase chain reaction, were found to be classifid either into those encoding the normal protein or into those encoding an abnormal protein that lacked exon 2 of the ferrochelatase gene, indicating that the proband is heterozygous for the ferrochelatase defect. Genomic DNA analysis revealed that the abnormal allele had a point mutation, C -* T, near the acceptor site of intron 1. This point mutation appears to be responsible for the post-transcriptional splicing abnormality resulting in an aberrant transcript of ferrochelatase in this patient.

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supporting

confidence: 68%

mentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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The molecular defect of ferrochelatase in a patient with erythropoietic protoporphyria.

Nakahashi¹,

Fujita²,

Taketani³

et al. 1992

Proc. Natl. Acad. Sci. U.S.A.

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“…The former is a spe cific inhibitor of ferrochelatase in various types of cultured cells [7,9,11], while the lat-ter is one of the two substrates of ferrochelatase; the other substrate of the enzyme is pro toporphyrin. Our results indicate that iron decreased porphyrin levels, and this decrease was partially reversed by CaMg EDTA (fig.…”

Section: Discussionmentioning

confidence: 99%

Porphyrin Synthesis by Murine Epidermal Cells

Karas²,

Sassa³

et al. 1993

Skin Pharmacol Physiol

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Incubation of murine epidermal cells with delta-aminolevulinic acid (ALA) resulted in a dose- and time-dependent accumulation of porphyrins, predominantly of protoporphyrin. Porphyrin accumulation decreased in the presence of iron, and the iron-mediated decrease was partially reversed by CaMg EDTA (1.25–10.0 mM), suggesting that there is functionally active ferrochelatase in these cells. This study suggests that these cells may be a useful model for the study of cutaneous porphyrin metabolism involving ferrochelatase activity.

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