Measurement of serum hepcidin-25 levels as a potential test for diagnosing hemochromatosis and related disorders

Kaneko, Yoshiaki; Miyajima, Hiroaki; Piperno, Alberto; Tomosugi, Naohisa; Hayashi, Hisao; Morotomi, Natsuko; Tsuchida, Kenichi; Ikeda, Takaaki; Ishikawa, Akihisa; Ota, Yusuke; Wakusawa, Shinya; Yoshioka, Kentaro; Kono, Satoshi; Pelucchi, Sara; Hattori, Ai; Tatsumi, Yasuaki; Okada, Toshihide; Yamagishi, Masakazu

doi:10.1007/s00535-010-0259-8

Cited by 54 publications

(59 citation statements)

References 47 publications

(63 reference statements)

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“…The current observations of circulating hepcidin 25 confirmed the findings previously observed in urine from patients with HFE-hemochromatosis (12). Low levels of serum hepcidin 25 were also found in Japanese patients with non-HFE hemochromatosis (18). In CHC patients, the mechanism of hepatic iron accumulation appears to be more complex and is still not completely understood.…”

Section: Discussionsupporting

confidence: 88%

Patients with Chronic Hepatitis C May be More Sensitive to Iron Hepatotoxicity than Patients with HFE-Hemochromatosis

et al. 2010

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Aim In chronic hepatitis C, iron might play an important role as a hepatotoxic co-factor. Therefore, venesection, a standard treatment for hemochromatosis, has been proposed as an alternative for patients who respond poorly to anti-viral therapy. To improve our understanding of iron-induced hepatotoxicity, we compared the responses to venesection between patients with chronic hepatitis C and those with HFEhemochromatosis. Methods Fourteen Japanese patients with chronic hepatitis C and eight Italian patients with HFEhemochromatosis underwent repeated venesection with a serum ferritin endpoint of 20 and 50 ng/mL, respectively. Serum iron indices and liver function tests were measured in pre-and post treatment blood samples from each patient. Body iron stores were calculated using the removed blood volume. Results In both patients with hepatitis and hemochromatosis, serum ferritin, aminotransferase and hepcidin 25 were reduced after venesection. The serum aminotransferase activity, but not the serum ferritin level, was predictive of effective iron removal treatment. Hepcidin regulation was set at an inappropriately low level in hemochromatosis patients (11.1 ± 9.2 ng/mL), but not so in hepatitis patients (30.7 ± 14.5 ng/mL). Inversely, the estimated body iron stores of hemochromatosis patients were 5,960 ± 2,750 mg, while those of hepatitis patients were 730 ± 560 mg. Judging from the liver enzyme reduction ratio, patients with hepatitis seemed to be more sensitive to iron hepatotoxicity than hemochromatosis patients. Conclusion Even though the threshold of iron hepatotoxicity and benefit of its removal differ between patients with chronic hepatitis C and those with HFE-hemochromatosis, venesection is a valid choice of treatment to reduce liver disease activity in both diseases.

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Section: Discussionsupporting

confidence: 88%

Patients with Chronic Hepatitis C May be More Sensitive to Iron Hepatotoxicity than Patients with HFE-Hemochromatosis

et al. 2010

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“…56 Some data support using hepcidin measurement as a guide for the follow-up genetic testing of IO patients, particularly in populations in whom classical type 1 HFErelated HH is rare. 57 Furthermore, during treatment of type 1 HH, monitoring hepcidin to prevent its complete suppression may curb iron hyperabsorption in the maintenance phase, possibly decreasing the need for phlebotomies. In iron-loading anemias, hepcidin measurement may also be valuable for identifying the most severely affected patients, helping to predict the development of IO and guiding the therapy.…”

Section: Diagnosis Of Io Disordersmentioning

confidence: 99%

Hepcidin in the diagnosis of iron disorders

Girelli

Nemeth

Swinkels

2016

Blood

327

291

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The discovery of the iron-regulatory hormone hepcidin in 2001 has revolutionized our understanding of iron disorders, and its measurement should advance diagnosis/treatment of these conditions. Although several assays have been developed, a gold standard is still lacking, and efforts toward harmonization are ongoing. Nevertheless, promising applications can already be glimpsed, ranging from the use of hepcidin levels for diagnosing iron-refractory iron deficiency anemia to global health applications such as guiding safe iron supplementation in developing countries with high infection burden.

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“…Although not confirmed by liver biopsy, the present case was considered to be H-type because TSAT was found to be elevated. To the best of our knowledge, only three cases of type 4 HH (one M-type and two H-type) have been reported in Japan (3)(4)(5). This is the first Japanese case of p.His507Arg in SLC40A1.…”

Section: Discussionmentioning

confidence: 95%

A Novel Phenotype of a Hereditary Hemochromatosis Type 4 with Ferroportin-1 Mutation, Presenting with Juvenile Cataracts

Yamakawa

Yukawa

et al. 2016

Intern. Med.

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Hereditary hemochromatosis (HH) is an inherited disorder usually seen in Northern Europeans, which results in iron overload syndrome. A few cases have also been reported in Japan. We herein report a Japanese man presenting with fever, arthritis, liver dysfunction, and hyperferritinemia who was diagnosed with type 4 HH. He was heterozygous for the 1520A>G (His507Arg) mutation in the ferroportin-1 gene (SLC40A1). He had a familial cataract as an infant, but hereditary hyperferritinemia cataract syndrome was excluded. This is the first report of type 4 HH with juvenile cataracts and suggests that there is an association between hyperferritinemia and early cataract formation.

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Measurement of serum hepcidin-25 levels as a potential test for diagnosing hemochromatosis and related disorders

Cited by 54 publications

References 47 publications

Patients with Chronic Hepatitis C May be More Sensitive to Iron Hepatotoxicity than Patients with HFE-Hemochromatosis

Patients with Chronic Hepatitis C May be More Sensitive to Iron Hepatotoxicity than Patients with HFE-Hemochromatosis

Hepcidin in the diagnosis of iron disorders

A Novel Phenotype of a Hereditary Hemochromatosis Type 4 with Ferroportin-1 Mutation, Presenting with Juvenile Cataracts

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