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转铁蛋白受体2的功能多样性及其治疗价值。

The Functional Versatility of Transferrin Receptor 2 and Its Therapeutic Value.

作者信息

Roetto Antonella, Mezzanotte Mariarosa, Pellegrino Rosa Maria

机构信息

Department of Clinical and Biological Sciences, University of Torino, 10043 Orbassano, Torino, Italy.

出版信息

Pharmaceuticals (Basel). 2018 Oct 23;11(4):115. doi: 10.3390/ph11040115.

Abstract

Iron homeostasis is a tightly regulated process in all living organisms because this metal is essential for cellular metabolism, but could be extremely toxic when present in excess. In mammals, there is a complex pathway devoted to iron regulation, whose key protein is hepcidin (Hepc), which is a powerful iron absorption inhibitor mainly produced by the liver. Transferrin receptor 2 (Tfr2) is one of the hepcidin regulators, and mutations in gene are responsible for type 3 hereditary hemochromatosis (HFE3), a genetically heterogeneous disease characterized by systemic iron overload. It has been recently pointed out that Hepc production and iron regulation could be exerted also in tissues other than liver, and that Tfr2 has an extrahepatic role in iron metabolism as well. This review summarizes all the most recent data on Tfr2 extrahepatic role, taking into account the putative distinct roles of the two main Tfr2 isoforms, Tfr2α and Tfr2β. Representing Hepc modulation an effective approach to correct iron balance impairment in common human diseases, and with Tfr2 being one of its regulators, it would be worthwhile to envisage Tfr2 as a therapeutic target.

摘要

铁稳态在所有生物体内都是一个受到严格调控的过程,因为这种金属对细胞代谢至关重要,但过量存在时可能具有极高的毒性。在哺乳动物中,存在一条专门用于铁调节的复杂途径,其关键蛋白是铁调素(Hepc),它是一种主要由肝脏产生的强大的铁吸收抑制剂。转铁蛋白受体2(Tfr2)是铁调素的调节因子之一,该基因突变会导致3型遗传性血色素沉着症(HFE3),这是一种以全身铁过载为特征的遗传异质性疾病。最近有研究指出,铁调素的产生和铁调节也可能在肝脏以外的组织中发挥作用,并且Tfr2在铁代谢中也具有肝外作用。本综述总结了关于Tfr2肝外作用的所有最新数据,同时考虑了两种主要Tfr2亚型Tfr2α和Tfr2β假定的不同作用。鉴于调节铁调素是纠正常见人类疾病中铁平衡受损的有效方法,而Tfr2是其调节因子之一,将Tfr2设想为治疗靶点是值得的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0ce3/6316356/d47a925511b2/pharmaceuticals-11-00115-g001.jpg

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