首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Antihepcidin antibody treatment modulates iron metabolism and is effective in a mouse model of inflammation-induced anemia.
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Antihepcidin antibody treatment modulates iron metabolism and is effective in a mouse model of inflammation-induced anemia.

机译:抗铁调素抗体治疗可调节铁代谢,并且在炎症诱发的贫血的小鼠模型中有效。

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摘要

Iron maldistribution has been implicated in multiple diseases, including the anemia of inflammation (AI), atherosclerosis, diabetes, and neurodegenerative disorders. Iron metabolism is controlled by hepcidin, a 25-amino acid peptide. Hepcidin is induced by inflammation, causes iron to be sequestered, and thus, potentially contributes to AI. Human hepcidin (hHepc) overexpression in mice caused an iron-deficient phenotype, including stunted growth, hair loss, and iron-deficient erythropoiesis. It also caused resistance to supraphysiologic levels of erythropoiesis-stimulating agent, supporting the hypothesis that hepcidin may influence response to treatment in AI. To explore the role of hepcidin in inflammatory anemia, a mouse AI model was developed with heat-killed Brucella abortus treatment. Suppression of hepcidin mRNA was a successful anemia treatment in this model. High-affinity antibodies specific for hHepc were generated, and hHepc knock-in mice were produced to enable antibody testing. Antibody treatment neutralized hHepc in vitro and in vivo and facilitated anemia treatment in hHepc knock-in mice with AI. These data indicate that antihepcidin antibodies may be an effective treatment for patients with inflammatory anemia. The ability to manipulate iron metabolism in vivo may also allow investigation of the role of iron in a number of other pathologic conditions.
机译:铁分布不均与多种疾病有关,包括炎症性贫血(AI),动脉粥样硬化,糖尿病和神经退行性疾病。铁代谢受25个氨基酸肽hepcidin的控制。铁调素是由炎症引起的,导致铁被螯合,因此有可能促成AI。小鼠中人类铁调素(hHepc)的过度表达导致铁缺乏表型,包括发育迟缓,脱发和铁缺乏性红细胞生成。它还引起对促红细胞生成素超生理水平的抵抗,支持了铁调素可能影响AI治疗反应的假说。为了探索铁调素在炎性贫血中的作用,采用热灭活布鲁氏菌流产治疗开发了小鼠AI模型。 hepcidin mRNA的抑制是该模型中成功的贫血治疗。产生了对hHepc特异的高亲和力抗体,并产生了hHepc敲入小鼠以进行抗体测试。抗体治疗可在体内和体外中和hHepc,并促进AI感染hHepc敲入小鼠的贫血治疗。这些数据表明抗铁调素抗体可能是炎性贫血患者的有效治疗方法。体内操纵铁代谢的能力也可能允许研究铁在许多其他病理状况中的作用。

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