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用于治疗高磷血症的铁、铝和镧基药物

[Iron, aluminum, and lanthanum-based drugs for treatment of hyperphosphatemia].

作者信息

Matsumura Kenji

机构信息

Torii Pharmaceutical Co., Ltd.

出版信息

Yakugaku Zasshi. 2015;135(4):545-9. doi: 10.1248/yakushi.14-00227-1.

DOI:10.1248/yakushi.14-00227-1
PMID:25832833
Abstract

The control of the serum phosphorus (P) level in chronic kidney disease patients is important because elevated serum P levels are associated with progression of vascular calcification and increased mortality in these patients. In 2014, a novel phosphate binder, ferric citrate hydrate (Riona(®)), became available for the treatment of hyperphosphatemia in Japan, the first country to approve this medication. Ferric citrate hydrate, which relies upon the potent phosphate-binding capacity of ferric iron, inhibits P absorption by forming complexes between ferric iron and dietary phosphate in the gut. The active pharmaceutical ingredient in ferric citrate hydrate provides a larger specific surface area and higher water solubility; therefore, it is expected to have greater efficacy in terms of its phosphate-binding capacity. In clinical trials, ferric citrate hydrate significantly reduced the serum phosphate level and effectively maintained serum P concentrations throughout the duration of the trials. Moreover, in one clinical trial, ferric citrate hydrate significantly decreased levels of fibroblast growth factor-23 (FGF-23) in nondialysis patients. FGF-23 is an endocrine hormone that increases urinary phosphate excretion to maintain serum P at the proper level. A portion of the iron from ferric citrate hydrate is absorbed and transported throughout the body as transferrin-bound iron, where it is used for the synthesis of hemoglobin, enzymes, and others. Although safer and more effective phosphate binders are expected in the future, ferric citrate hydrate will become a new approach for the treatment of hyperphosphatemia.

摘要

控制慢性肾病患者的血清磷(P)水平很重要,因为血清P水平升高与这些患者血管钙化的进展和死亡率增加有关。2014年,一种新型的磷结合剂——水合柠檬酸铁(Riona(®)),在日本上市用于治疗高磷血症,日本是首个批准该药物的国家。水合柠檬酸铁依靠三价铁强大的磷结合能力,通过在肠道内使三价铁与膳食磷形成复合物来抑制磷的吸收。水合柠檬酸铁中的活性药物成分具有更大的比表面积和更高的水溶性;因此,预计其在磷结合能力方面具有更大的疗效。在临床试验中,水合柠檬酸铁显著降低了血清磷水平,并在整个试验期间有效维持了血清P浓度。此外,在一项临床试验中,水合柠檬酸铁显著降低了非透析患者的成纤维细胞生长因子23(FGF - 23)水平。FGF - 23是一种内分泌激素,可增加尿磷排泄以将血清P维持在适当水平。水合柠檬酸铁中的一部分铁被吸收,并作为与转铁蛋白结合的铁运输到全身,在那里用于合成血红蛋白、酶等。尽管未来有望出现更安全、更有效的磷结合剂,但水合柠檬酸铁将成为治疗高磷血症的一种新方法。

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