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慢性肾衰竭贫血的特征及其通过人促红细胞生成素制剂(r-HuEPO)纠正的方式。静脉注射促红细胞生成素的药代动力学及其对红细胞生成动力学影响的研究。

Characterization of the anaemia of chronic renal failure and the mode of its correction by a preparation of human erythropoietin (r-HuEPO). An investigation of the pharmacokinetics of intravenous erythropoietin and its effects on erythrokinetics.

作者信息

Cotes P M, Pippard M J, Reid C D, Winearls C G, Oliver D O, Royston J P

机构信息

Section of Haematology, Clinical Research Centre, Harrow, Middlesex.

出版信息

Q J Med. 1989 Feb;70(262):113-37.

PMID:2594953
Abstract

Studies were directed to characterization of the anaemia of renal failure of 11 patients on haemodialysis and determination of the way in which it is corrected by human erythropoietin derived from recombinant DNA expressed in Chinese hamster ovary cells (r-HuEPO) administered intravenously. Erythrokinetics before treatment showed that total red cell mass was below normal and that both erythron transferrin uptake and red cell survival were modestly reduced; treatment increased both total red cell mass and erythron transferrin uptake but did not change red cell survival in previously untransfused patients. When BFU-e and CFU-e from patient bone marrow were cultured in autologous serum we found no evidence for inhibitors of erythroid progenitor maturation in patient serum compared with normal. Erythroid expansion in response to r-HuEPO was not limited by the availability of iron, iron requirements for new red cell formation being met from stores (if adequate) or from oral iron supplements. In pharmacokinetic studies the plasma clearance of r-HuEPO could be expressed by a three-parameter exponential curve with T1/2 range of 2.3 to 7.3 h. T1/2 after the first dose of r-HuEPO was not significantly different from that after 14 to 54 weeks treatment when the erythron had expanded to a new steady state. Erythron transferrin uptake before treatment was related to endogenous production of erythropoietin estimated from the plasma clearance of the first dose of r-HuEPO administered intravenously. This finding suggested that the availability of erythropoietin was the main factor limiting expansion of the erythron. This conclusion was supported by the continuity of the relationship during the response to treatment.

摘要

研究旨在对11例接受血液透析的肾衰竭患者的贫血特征进行描述,并确定静脉注射源自中国仓鼠卵巢细胞表达的重组DNA的人促红细胞生成素(r-HuEPO)对其进行纠正的方式。治疗前的红细胞动力学显示,总红细胞量低于正常水平,红细胞系转铁蛋白摄取和红细胞存活均略有降低;治疗增加了总红细胞量和红细胞系转铁蛋白摄取,但在先前未输血的患者中并未改变红细胞存活。当将患者骨髓中的爆式红系集落形成单位(BFU-e)和红系集落形成单位(CFU-e)在自体血清中培养时,与正常情况相比,我们未发现患者血清中存在抑制红系祖细胞成熟的物质。对r-HuEPO的红系扩增不受铁可用性的限制,新红细胞形成所需的铁可从储存铁(如果充足)或口服铁补充剂中获得。在药代动力学研究中,r-HuEPO的血浆清除率可用三参数指数曲线表示,半衰期范围为2.3至7.3小时。首次注射r-HuEPO后的半衰期与治疗14至54周后红细胞系扩展至新的稳定状态时的半衰期无显著差异。治疗前的红细胞系转铁蛋白摄取与根据静脉注射的首剂r-HuEPO的血浆清除率估算的内源性促红细胞生成素产生相关。这一发现表明促红细胞生成素的可用性是限制红细胞系扩增的主要因素。治疗反应过程中这种关系的连续性支持了这一结论。

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