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BRIEF REPORT
From Department of Pediatrics and the Department of
Pediatric Urology, Nagoya Daini Red Cross Hospital, Japan; the
Department of Nutrition and Biochemistry, National Institute of Public
Health, Tokyo, Japan; the Third Department of Internal Medicine,
Yamagata University School of Medicine, Japan; and the Department of
Pediatrics, Nagoya City University, Japan.
The appearance of hereditary coproporphyria (HCP) before puberty is
very rare, and all reported cases of early-onset HCP have been in the
homozygous or the compound heterozygous state. Some have been
identified as harderoporphyria, which is a rare erythropoietic variant form of HCP. These conditions can be differentiated by molecular analysis because the gene abnormality responsible for harderoporphyria seems to be unique (K404E). Early-onset HCP, not harderoporphyria, is reported with a gene mutation in the heterozygous state and male pseudohermaphrodism. It was shown that
adrenal gland hypofunction resulted in male pseudohermaphrodism. This
case demonstrates the possibility that abnormalities of steroid metabolism influence porphyria.
(Blood. 2001;98:3871-3873) Hereditary coproporphyria (HCP) is a hereditary
autosomal-dominant disease of heme biosynthesis resulting from a
partial deficiency of coproporphyrinogen oxidase (CPO). It is
clinically characterized by neurologic dysfunction attacks and
occasional photosensitivity.1 HCP is rare before
puberty,2 and all reported early-onset cases have been in
the homozygous3-8 or the compound heterozygous
state.9 Harderoporphyria, a rare erythropoietic variant
form of HCP, is characterized by neonatal hyperbilirubinemia and
hemolytic anemia, hepatosplenomegaly, and sometimes
photosensitivity.6-9 To date, 3 families with
harderoporphyria have been reported. Molecular analysis indicates that
a CPO gene abnormality, K404E, was unique for the
disease.9 Therefore, HCP can be differentially diagnosed from harderoporphyria by both clinical and laboratory examinations and
molecular analysis. Here, we describe a first case of neonatal-onset HCP in the heterozygous state with male pseudohermaphrodism.
Patient history
Molecular and DNA analysis
Hereditary coproporphyria in the heterozygous state Clinical symptoms, an increase of coproporphyrin III excretion in the stool, and increases of -aminolevulinic acid, porphobilinogen, and coproporphyrin III excretion in the urine indicated that the patient had HCP. Mostly, fecal porphyrin excretion showed increased coproporphyrin III (60%-70% in total porphyrin) (Table
1). Genetic molecular analysis confirmed
the diagnosis. The nucleotide sequence of the DNA fragment containing
exon 6 revealed a heterozygous mutation, a G-to-A transition at the
last nucleotide of exon 6 (Figure 1A).
This mutation was identical to that reported in another patient with
HCP,15 which was responsible for exon 6 skipping. We also
examined the nucleotide sequence of all PCR-amplified fragments and
found no mutation, indicating that no other abnormality of the CPO gene
was responsible for his disease. PCR products were also subjected to
restriction analysis with MspI from family members and a
healthy control (Figure 1B). These studies showed that the father was
heterozygous for the mutation and a normal allele, whereas the
mother's findings were normal. This, however, seemed confusing because
the mother showed a slight elevation of coproporphyrin and
protoporphyrin (Table 1). Psychological stress might
have been the cause of the elevation. It is also possible that she had
a mutation of the CPO gene in lariat branch sites in the intron or the
promoter region or that she had gene rearrangements because not
all of these kinds of gene mutations could be detected by the methods
used here. Alternatively, she might have had a gene abnormality
responsible for another type of porphyria such as acute intermittent
porphyria (AIP), variegate porphyria, or -aminolevulinic acid
dehydratase-deficient porphyria.
The clinical features of our patient were significantly different from those of a reported Czech patient,15 who repeatedly had neurologic symptoms including paresis. In contrast, our patient never exhibited neurologic symptoms. Except for the ambiguous external genitalia and adrenal hypofunction, the clinical features of our patient resembled those of harderoporphyria. However, the excretion of harderoporphyrin in feces was not high (7%-10%) enough to be constitute harderoporphyria (Table 1). Furthermore, his gene abnormality was different from that reportedly responsible for harderoporphyria (K404E) (Figure 1C). Therefore, it was considered that our patient had HCP in the heterozygous state, not harderoporphyria. Steroid hormone abnormalities may aggravate porphyria We examined the pathogenesis of his male pseudohermaphrodism. His karyotype was 46,XY and his testosterone level was low for his age (45 ng/dL). Administration of 5000 U human chorionic gonadotropin intramuscularly for 3 days was ineffective in elevating serum testosterone and 5 -dehydrotestosterone levels. Hepatic
5-reductase deficiency was ruled out by a urinary steroid profile
(5THF/5 THF = 0.66).16 Concerning adrenal
function, the patient's adrenocorticotropic hormone (ACTH) level
was high (1800 pg/mL), whereas his cortisol level was within normal
range (7.6 g/dL) (Table 2). We found no significant change in
levels of serum steroid metabolites before and after a rapid ACTH test
done at 16 months of age. Abdominal magnetic resonance imaging and
ultrasonography showed no adrenal tumor or hypertrophy. Therefore, he
had adrenal gland hypofunction with an abnormality in testosterone
biosynthesis. Skin pigmentation was markedly decreased after
corticosteroid substitution therapy. He had no problems except for
chronic anemia, requiring periodic blood transfusions, until he was 8 months old. At age 2, despite having mild anemia and photosensitivity,
he showed normal growth and mental development. No skin pigmentation,
hypertrichosis, or symptoms of rickets were observed. The patient is
now receiving oral -carotene17,18 and cortisone
acetate daily.
The natural history of AIP provides strong suggestive evidence of the significant interplay of endocrine and genetic factors in the clinical expression of porphyria.19,20 Savage et al21 reported successful treatment of active AIP with a testosterone implant in women, suggesting that an androgenic environment partially protects against porphyria attacks. They also speculated that androgens might act later in the porphyrin-heme pathway to stimulate heme production, which is necessary to maintain intracellular levels of cytochromes. Steroid hormone metabolism depends on the heme enzyme cytochrome P450, especially in the liver. It is unclear why this heterozygous mutation presents such an early onset and severe clinical features as in homozygous patients. Our patient exhibited male pseudohermaphrodism. This indicates that a relative lack of androgen and estrogen of maternal origin may aggravate the dysfunction of heme biosynthesis caused by porphyria. Further investigations are necessary to clarify the cause of steroid hormone abnormalities, which, in our patient, may be linked with the clinical expression of HCP.
We thank Dr K. Honma, Prof N. Matsuo (Department of Pediatrics, Keio University) for urinary steroid profile analyses, Dr T. Yanase (The Third Department of Internal Medicine, Kyushu University), and Dr Y. Horie (The Second Department of Internal Medicine, Tottori University) for valuable comments.
Submitted April 11, 2001; accepted August 13, 2001.
The publication costs of this article were defrayed in part by page charge payment. Therefore, and solely to indicate this fact, this article is hereby marked "advertisement" in accordance with 18 U.S.C. section 1734.
Reprints: Harue Takeuchi, Department of Pediatrics, Nagoya Daini Red Cross Hospital, 2-9 Myokencho, Showaku, Nagoya, 466-8650, Japan; e-mail address: takeuchi{at}freesurf.ch.
1. Kappas A, Sassa S, Galbraith RA, Nordmann Y. The porphyrias. In: Scriver CR,Beaudet AL,Sly WS,Valle D, eds. The Metabolic and Molecular Bases of Inherited Disease. Vol 2. 7th ed. New York, NY: McGraw-Hill; 1995:2103-2159. 2. Elder GH. Hepatic porphyrias in children. J Inherit Metab Dis. 1997;20:237-246[CrossRef][Medline] [Order article via Infotrieve]. 3. Berger H, Goldberg A. Hereditary coproporphyria. BMJ. 1955;ii:85-88. 4. Grandchamp B, Phung N, Nordmann Y. Homozygous case of hereditary coproporphyria [letter]. Lancet. 1977;2:1348-1349[Medline] [Order article via Infotrieve].
5.
Martasek P, Nordmann Y, Grandchamp B.
Homozygous hereditary coproporphyria caused by an arginine to tryptophane substitution in coproporphyrinogen oxidase and common intragenic polymorphisms.
Hum Mol Genet.
1994;3:477-480 6. Doss M, von Tiepermann R, Köpp W. Harderoporphyrin coproporphyria [letter]. Lancet. 1984;1:292[Medline] [Order article via Infotrieve]. 7. Nordmann Y, Grandchamp B, Verneuil H, Phung L, Cartigny B, Fontaine G. Harderoporphyria: a variant hereditary coproporphyria. J Clin Invest. 1983;72:1139-1149.
8.
Lamoril J, Martasek P, Deybach JC, Da Silva V, Grandchamp B, Nordmann Y.
A molecular defect in coproporphyrinogen oxidase gene causing harderoporphyria, a variant form of hereditary coproporphyria.
Hum Mol Genet.
1995;4:275-278
9.
Lamoril J, Puy H, Gouya L, et al.
Neonatal hemolytic anemia due to inherited harderoporphyria: clinical characteristics and molecular basis.
Blood.
1998;91:1453-1457
10.
Kaiser IH.
Brown amniotic fluid in congenital erythropoietic porphyria.
Obstet Gynecol.
1980;56:383-384 11. Huang JL, Zaider E, Roth P, Garcia O, Pollack S, Poh-Fitzpatrick MB. Congenital erythropoietic porphyria: clinical, biochemical, and enzymatic profile of a severely affected infant. J Am Acad Dermatol. 1996;34:924-927[CrossRef][Medline] [Order article via Infotrieve]. 12. Xie Y, Kondo M, Koga H, Miyamoto H, Chiba M. Urinary porphyrins in patients with endemic chronic arsenic poisoning caused by burning coal in China. Environ Health Prev Med. 2001;5:180-185[CrossRef]. 13. Susa S, Daimon M, Kondo H, Kondo M, Yamatani K, Sasaki H. Identification of a novel mutation of the CPO gene in a Japanese hereditary coproporphyria family. Am J Med Genet. 1998;80:204-206[CrossRef][Medline] [Order article via Infotrieve]. 14. Daimon M, Gojyou E, Sugawara M, Yamatani K, Tominaga M, Sasaki H. A novel missense mutation in exon 4 of the human coproporphyrinogen oxidase gene in two patients with hereditary coproporphyria. Hum Genet. 1997;99:199-201[CrossRef][Medline] [Order article via Infotrieve].
15.
Delfau-Larue M-H, Martasek P, Grandchamp B.
Coproporphyrinogen oxidase: gene organization and description of a mutation leading to exon 6 skipping.
Hum Mol Genet.
1994;3:1325-1330 16. Miller JA, Levene GM. Congenital erythropoietic porphyria and congenital adrenal hyperplasia with evidence for hepatic delta-5 alpha-reductase deficiency. J R Soc Med. 1989;82:107-108[Medline] [Order article via Infotrieve].
17.
Mathews-Roth MM.
Erythropoietic protoporphyria 18. Seip M, Thune PO, Eriksen L. Treatment of photosensitivity in congenital erythropoietic porphyria (CEP) with beta-carotene. Acta Dermatol Venereol. 1974;54:239-240[Medline] [Order article via Infotrieve]. 19. Krsnjavi H, Milkovic-Kraus S, Prpic-Majic D. Acute intermittent porphyria and hormone disbalance. Med Hypotheses. 1991;34:141-143[CrossRef][Medline] [Order article via Infotrieve]. 20. Anderson KE, Bradlow HL, Sassa S, Kappas A. Studies in porphyria, VIII: relationship of the 5 alpha-reductive metabolism of steroid hormones to clinical expression of the genetic defect in acute intermittent porphyria. Am J Med. 1979;66:644-650[CrossRef][Medline] [Order article via Infotrieve]. 21. Savage MW, Reed P, Orrman-Rossiter SL, Weinkove C, Anderson DC. Acute intermittent porphyria treated by testosterone implant. Postgrad Med J. 1992;68:479-481[Abstract].
© 2001 by The American Society of Hematology.
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Top
Abstract
Introduction
diagnosis and treatment.
N Engl J Med.
1977;297:98-100