Current Biology

Current Biology

Volume 10, Issue 16, 14 August 2000, Pages 1001-1004
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Brief Communication
Zebrafish dracula encodes ferrochelatase and its mutation provides a model for erythropoietic protoporphyria

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Abstract

Exposure to light precipitates the symptoms of several genetic disorders that affect both skin and internal organs. It is presumed that damage to non-cutaneous organs is initiated indirectly by light, but this is difficult to study in mammals. Zebrafish have an essentially transparent periderm for the first days of development. In a previous large-scale genetic screen we isolated a mutation, dracula (drc), which manifested as a light-dependent lysis of red blood cells [1]. We report here that protoporphyrin IX accumulates in the mutant embryos, suggesting a deficiency in the activity of ferrochelatase, the terminal enzyme in the pathway for heme biosynthesis. We find that homozygous drcm248 mutant embryos have a G→T transversion at a splice donor site in the ferrochelatase gene, creating a premature stop codon. The mutant phenotype, which shows light-dependent hemolysis and liver disease, is similar to that seen in humans with erythropoietic protoporphyria, a disorder of ferrochelatase.

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These authors contributed equally to this work.

Present address: Laboratory of Molecular Genetics, National Institute of Child Health and Development, Maryland 20892, USA.

§

Present address: Jake Gittlen Cancer Research Institute, The Pennsylvania State University College of Medicine, Hershey, Pennsylvania 17033, USA.

Present address: The Center for Study of Disorders of Iron and Porphyrin Metabolism and The Division of Digestive Disease and Nutrition, University of Massachusetts Medical School, Worcester, Massachusetts 01655, USA.

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