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Striking the target in iron overload disorders

机译:打击铁过载疾病的靶标

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The liver, a major site of body iron stores, mediates key responses that preserve systemic iron homeostasis. In this issue of the JCI , Guo et al. demonstrate that administration of antisense oligonucleotides that reduce expression of Tmprss6, a hepatic protein that plays an essential role in maintaining iron balance, can attenuate disease severity in mouse models of human iron overload disorders. These data reveal the potential of novel TMPRSS6-targeted therapies for the treatment of clinical conditions such as hereditary hemochromatosis and β-thalassemia.
机译:肝脏是人体铁储存的主要场所,它介导了维持全身铁稳态的关键反应。在JCI的这一期中,Guo等人。证明了减少Tmprss6(一种在维持铁平衡中起重要作用的肝蛋白)表达的反义寡核苷酸的给药可以减轻人类铁过载疾病小鼠模型的疾病严重性。这些数据揭示了靶向TMPRSS6的新型疗法在治疗诸如遗传性血色素沉着症和β地中海贫血等临床疾病中的潜力。

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