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Non-Anticoagulant Heparins Are Hepcidin Antagonists for the Treatment of Anemia

机译:非抗凝肝素是铁调素拮抗剂,用于治疗贫血

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The peptide hormone hepcidin is a key controller of systemic iron homeostasis, and its expression in the liver is mainly regulated by bone morphogenetic proteins (BMPs), which are heparin binding proteins. In fact, heparins are strong suppressors of hepcidin expression in hepatic cell lines that act by inhibiting the phosphorylation of SMAD1/5/8 proteins elicited by the BMPs. The inhibitory effect of heparins has been demonstrated in cells and in mice, where subcutaneous injections of non-anticoagulant heparins inhibited liver hepcidin expression and increased iron bioavailability. The chemical characteristics for high anti-hepcidin activity in vitro and in vivo include the 2O-and 6O-sulfation and a molecular weight above 7 kDa. The most potent heparins have been found to be the super-sulfated ones, active in hepcidin suppression with a molecular weight as low as 4 kDa. Moreover, the alteration of endogenous heparan sulfates has been found to cause a reduction in hepcidin expression in vitro and in vivo, indicating that heparins act by interfering with the interaction between BMPs and components of the complex involved in the activation of the BMP/SMAD1/5/8 pathway. This review summarizes recent findings on the anti-hepcidin activity of heparins and their possible use for the treatment of anemia caused by hepcidin excess, including the anemia of chronic diseases. View Full-Text
机译:肽激素hepcidin是系统性铁稳态的关键控制器,其在肝脏中的表达主要受骨形态发生蛋白(BMPs)调节,BMP是肝素结合蛋白。实际上,肝素是肝细胞中肝素表达的强抑制剂,其通过抑制BMP引起的SMAD1 / 5/8蛋白的磷酸化发挥作用。肝素的抑制作用已在细胞和小鼠中得到证实,皮下注射非抗凝性肝素可抑制肝铁素的表达并提高铁的生物利用度。体外和体内高抗铁调素活性的化学特征包括2O-和6O-硫酸化以及分子量大于7 kDa的物质。已发现最有效的肝素是超硫酸化的肝素,具有抑制铁调素的活性,分子量低至4 kDa。此外,已发现内源性硫酸乙酰肝素的改变在体外和体内引起铁调素表达的降低,表明肝素通过干扰BMP与参与激活BMP / SMAD1 /的复合物组分之间的相互作用而起作用。 5/8途径。这篇综述总结了有关肝素的抗铁调素活性的最新发现及其在治疗由铁调素过量引起的贫血中的可能用途,包括慢性疾病的贫血。查看全文

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