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炎症性贫血:铁调素的关联

Anemia of inflammation: the hepcidin link.

作者信息

Roy Cindy N, Andrews Nancy C

机构信息

Children's Hospital, Boston, MA 02115, USA.

出版信息

Curr Opin Hematol. 2005 Mar;12(2):107-11. doi: 10.1097/00062752-200503000-00001.

Abstract

PURPOSE OF REVIEW

The anemia of inflammation has been associated for nearly two decades with elevated cytokine levels, but the primary mediator of this condition was unknown. Recently hepcidin antimicrobial peptide has emerged as the hormone that links the type II acute phase response to iron handling and erythropoiesis.

RECENT FINDINGS

Hepcidin antimicrobial peptide likely modulates iron transport from macrophages and enterocytes to red blood cell precursors as a consequence of its interaction with SLC40A1/ferroportin, the only known transporter that facilitates iron egress. Insights into the regulation of hepcidin antimicrobial peptide expression by known iron metabolic proteins such as HFE, hemojuvelin, and transferrin receptor 2 are expanding the understanding of the genetic circuitry that controls iron absorption and utilization.

SUMMARY

Increasingly, experiments suggest the hepatocyte is not just the iron storage depot but is the 'command central' for the maintenance of iron homeostasis. It receives multiple signals related to iron balance and responds via transcriptional control of hepcidin antimicrobial peptide.

摘要

综述目的

近二十年来,炎症性贫血一直与细胞因子水平升高有关,但这种情况的主要介质尚不清楚。最近,抗菌肽铁调素已成为将II型急性期反应与铁代谢及红细胞生成联系起来的激素。

最新发现

抗菌肽铁调素可能通过与SLC40A1/铁转运蛋白相互作用,调节铁从巨噬细胞和肠细胞向红细胞前体的转运,铁转运蛋白是唯一已知的促进铁流出的转运蛋白。对已知铁代谢蛋白(如HFE、血色素沉着症相关蛋白和转铁蛋白受体2)对抗菌肽铁调素表达调控的深入了解,正在拓展对控制铁吸收和利用的遗传通路的认识。

总结

越来越多的实验表明,肝细胞不仅是铁的储存库,而且是维持铁稳态的“指挥中心”。它接收与铁平衡相关的多种信号,并通过对抗菌肽铁调素的转录控制做出反应。

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