血色素沉着症相关蛋白对于膳食铁感知至关重要,其突变会导致严重的铁过载。
Hemojuvelin is essential for dietary iron sensing, and its mutation leads to severe iron overload.
作者信息
Niederkofler Vera, Salie Rishard, Arber Silvia
机构信息
Biozentrum, Department of Cell Biology, University of Basel, and Friedrich Miescher Institute, Basel, Switzerland.
出版信息
J Clin Invest. 2005 Aug;115(8):2180-6. doi: 10.1172/JCI25683.
Abstract
Iron homeostasis plays a critical role in many physiological processes, notably synthesis of heme proteins. Dietary iron sensing and inflammation converge in the control of iron absorption and retention by regulating the expression of hepcidin, a regulator of the iron exporter ferroportin. Human mutations in the glycosylphosphatidylinositol-anchored protein hemojuvelin (HJV; also known as RGMc and HFE2) cause juvenile hemochromatosis, a severe iron overload disease, but the way in which HJV intersects with the iron regulatory network has been unclear. Here we show that, within the liver, mouse Hjv is selectively expressed by periportal hepatocytes and also that Hjv-mutant mice exhibit iron overload as well as a dramatic decrease in hepcidin expression. Our findings define a key role for Hjv in dietary iron sensing and also reveal that cytokine-induced inflammation regulates hepcidin expression through an Hjv-independent pathway.
摘要
铁稳态在许多生理过程中起着关键作用,尤其是在血红素蛋白的合成过程中。膳食铁感知和炎症通过调节铁调素(一种铁输出蛋白铁转运蛋白的调节剂)的表达,共同控制铁的吸收和保留。糖基磷脂酰肌醇锚定蛋白血幼素(HJV;也称为RGMc和HFE2)的人类突变会导致青少年血色素沉着症,这是一种严重的铁过载疾病,但HJV与铁调节网络的交集方式尚不清楚。在这里,我们表明,在肝脏中,小鼠Hjv由门静脉周围的肝细胞选择性表达,并且Hjv突变小鼠表现出铁过载以及铁调素表达的显著降低。我们的研究结果确定了Hjv在膳食铁感知中的关键作用,还揭示了细胞因子诱导的炎症通过一条不依赖Hjv的途径调节铁调素的表达。
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