Matriptase-2 regulates iron homeostasis primarily by setting the basal levels of hepatic hepcidin expression through a nonproteolytic mechanism.

The Journal of Biological Chemistry Pub Date : 2023-10-01 Epub Date: 2023-09-09 DOI:10.1016/j.jbc.2023.105238
Caroline A Enns, Tyler Weiskopf, Richard H Zhang, Jeffrey Wu, Shall Jue, Makiko Kawaguchi, Hiroaki Kataoka, An-Sheng Zhang
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Abstract

Matriptase-2 (MT2), encoded by TMPRSS6, is a membrane-anchored serine protease. It plays a key role in iron homeostasis by suppressing the iron-regulatory hormone, hepcidin. Lack of functional MT2 results in an inappropriately high hepcidin and iron-refractory iron-deficiency anemia. Mt2 cleaves multiple components of the hepcidin-induction pathway in vitro. It is inhibited by the membrane-anchored serine protease inhibitor, Hai-2. Earlier in vivo studies show that Mt2 can suppress hepcidin expression independently of its proteolytic activity. In this study, our data indicate that hepatic Mt2 was a limiting factor in suppressing hepcidin. Studies in Tmprss6-/- mice revealed that increases in dietary iron to ∼0.5% were sufficient to overcome the high hepcidin barrier and to correct iron-deficiency anemia. Interestingly, the increased iron in Tmprss6-/- mice was able to further upregulate hepcidin expression to a similar magnitude as in wild-type mice. These results suggest that a lack of Mt2 does not impact the iron induction of hepcidin. Additional studies of wild-type Mt2 and the proteolytic-dead form, fMt2S762A, indicated that the function of Mt2 is to lower the basal levels of hepcidin expression in a manner that primarily relies on its nonproteolytic role. This idea is supported by the studies in mice with the hepatocyte-specific ablation of Hai-2, which showed a marginal impact on iron homeostasis and no significant effects on iron regulation of hepcidin. Together, these observations suggest that the function of Mt2 is to set the basal levels of hepcidin expression and that this process is primarily accomplished through a nonproteolytic mechanism.

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基质蛋白酶-2主要通过非促细胞分裂机制调节肝铁调素表达的基础水平来调节铁稳态。
基质蛋白酶-2(MT2)由TMPRSS6编码,是一种膜锚定的丝氨酸蛋白酶。它通过抑制铁调节激素铁调素在铁稳态中发挥关键作用。缺乏功能性MT2会导致铁调素过高和铁难治性缺铁性贫血。Mt2在体外切割铁调素诱导途径的多种成分。它被膜锚定丝氨酸蛋白酶抑制剂Hai-2抑制。早期的体内研究表明,Mt2可以抑制铁调素的表达,而不依赖于其蛋白水解活性。在本研究中,我们的数据表明,肝脏Mt2是抑制铁调素的限制因素。对Tmprss6-/-小鼠的研究表明,将膳食铁含量增加至-0.5%就足以克服高铁调素屏障并纠正缺铁性贫血。有趣的是,Tmprss6-/-小鼠体内铁的增加能够进一步上调铁调素的表达,其幅度与野生型小鼠相似。这些结果表明Mt2的缺乏并不影响铁调素的铁诱导。对野生型Mt2和蛋白水解死亡形式fMt2S762A的额外研究表明,Mt2的功能是以主要依赖于其非促蛋白水解作用的方式降低铁调素表达的基础水平。这一观点得到了肝细胞特异性切除Hai-2的小鼠研究的支持,该研究显示对铁稳态的影响很小,对铁调素的铁调节没有显著影响。总之,这些观察结果表明,Mt2的功能是设定铁调素表达的基础水平,而这一过程主要是通过非蛋白水解机制实现的。
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