原发性铁超载综合征的修订分类。

IF 3.1 3区 医学 Q2 GASTROENTEROLOGY & HEPATOLOGY Journal of Clinical and Translational Hepatology Pub Date : 2024-04-28 Epub Date: 2024-03-19 DOI:10.14218/JCTH.2023.00290
Yasuaki Tatsumi, Motoyoshi Yano, Shinya Wakusawa, Hiroaki Miyajima, Tetsuya Ishikawa, Shinsaku Imashuku, Atsuko Takano, Wataru Nihei, Ayako Kato, Koichi Kato, Hisao Hayashi, Kentaro Yoshioka, Kazuhiko Hayashi
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引用次数: 0

摘要

背景和目的:随着肝磷脂素25(Hep25)在临床上的应用,人们对其与铁蛋白(FP)和二价金属转运体1在原发性铁过载综合征(PIOSs)中的关系有了更详细的了解。2012 年,我们提出了一种基于 Hep25/FP 系统的 PIOSs 分类法,其中包括肝前疟原虫血症、肝血色病(HC)和肝后 FP 病(FP-D)。然而,考虑到有关 PIOSs 的证据不断积累,我们旨在更新该分类:方法:我们回顾了 2012 年的分类,并根据有关 PIOSs 的新信息对其进行了回顾性更新:结果:由于新发现了红铁酮诱导的 Hep25 抑制,铁负荷贫血作为肝前性贫血被纳入 PIOSs,传统 FP-D 的状态被重塑为 BIOIRON 提议。造成肝前型 PIOSs 的关键分子是急性浆细胞性贫血中的低转铁蛋白饱和度和铁负荷性贫血中红细胞产生的更多红铁酮。肝性 PIOS 包括四种 HC 基因型,每种基因型的肝脏中 Hep25 的合成都会不适当地减少。肝后型 PIOS 的肝脏 Hep25 合成充足;然而,两种突变的 FP 分子对 Hep25 的抵抗力不同,分别导致 SLC40A1-HC 和 FP-D。PIOS 表型通过实验室检测(包括循环 Hep25)进行诊断,然后进行适当的治疗。必要时,可将候选基因的直接测序外包给基因中心。C282Y等流行突变的实验室试剂盒可作为白种人HC基因分析的首选:结论:修订后的分类方法可能对全世界都有用。
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A Revised Classification of Primary Iron Overload Syndromes.

Background and aims: The clinical introduction of hepcidin25 (Hep25) has led to a more detailed understanding of its relationship with ferroportin (FP) and divalent metal transporter1 in primary iron overload syndromes (PIOSs). In 2012, we proposed a classification of PIOSs based on the Hep25/FP system, which consists of prehepatic aceruloplasminemia, hepatic hemochromatosis (HC), and posthepatic FP disease (FP-D). However, in consideration of accumulated evidence on PIOSs, we aimed to renew the classification.

Methods: We reviewed the 2012 classification and retrospectively renewed it according to new information on PIOSs.

Results: Iron-loading anemia was included in PIOSs as a prehepatic form because of the newly discovered erythroferrone-induced suppression of Hep25, and the state of traditional FP-D was remodeled as the BIOIRON proposal. The key molecules responsible for prehepatic PIOSs are low transferrin saturation in aceruloplasminemia and increased erythroferrone production by erythroblasts in iron-loading anemia. Hepatic PIOSs comprise four genotypes of HC, in each of which the synthesis of Hep25 is inappropriately reduced in the liver. Hepatic Hep25 synthesis is adequate in posthepatic PIOSs; however, two mutant FP molecules may resist Hep25 differently, resulting in SLC40A1-HC and FP-D, respectively. PIOS phenotypes are diagnosed using laboratory tests, including circulating Hep25, followed by suitable treatments. Direct sequencing of the candidate genes may be outsourced to gene centers when needed. Laboratory kits for the prevalent mutations, such as C282Y, may be the first choice for a genetic analysis of HC in Caucasians.

Conclusions: The revised classification may be useful worldwide.

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来源期刊
Journal of Clinical and Translational Hepatology
Journal of Clinical and Translational Hepatology GASTROENTEROLOGY & HEPATOLOGY-
CiteScore
6.40
自引率
2.80%
发文量
496
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