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用促红细胞生成素治疗与慢性肾衰竭相关的贫血:重组人红细胞生成素可能是现有选择中最好的。

Treating anemia associated with chronic renal failure with erythropoiesis stimulators: recombinant human erythropoietin might be the best among the available choices.

机构信息

Department of Pharmacology, Zagreb University School of Medicine, Šalata 11, 10000 Zagreb, Croatia.

出版信息

Med Hypotheses. 2012 Jan;78(1):157-61. doi: 10.1016/j.mehy.2011.10.016. Epub 2011 Nov 10.

Abstract

Chronic renal failure (CRF) is a widespread medical problem commonly accompanied by a hypoproliferative anemia ("renal anemia") due to erythropoietin deficiency. Anemia greatly contributes to reduced quality of life (Hr-QoL) and high morbidity and mortality in CRF patients. Recombinant human erythropoietin (rHu-Epo) was introduced to medical practice some 20years ago. It enables correction of anemia (hemoglobin levels, Hb) with dramatic immediate (Hr-QoL improvement) and long-term effects (reduced morbidity and mortality). Newer experimental data suggest that long-term benefits could be due not only to antianemic effect, but also to a direct organoprotective effect of (rHu)-Epo mediated through a receptor complex different from the "erythropoietic" erythropoietin receptor. During the last decade, two alternative treatments for renal anemia have been approved: darbepoetin and CERA. Both are direct agonists of the "erythropoietic" receptors and both were derived from rHu-Epo. Molecularly, they differ from rHu-Epo in that they are much larger molecules (darbepoetin is genetically modified rHu-Epo with a higher sugar content and CERA is pegylated rHu-Epo) with lower affinity for the erythropoietin receptor but with a longer circulating time. In terms of renal anemia correction, they are non-inferior to rHu-Epo and allow for less frequent dosing. They have never been compared to rHu-Epo regarding the long-term outcomes. It is hypothesized that regarding the long-term outcomes (morbidity, mortality), rHu-Epo might be superior to those larger molecules. The hypothesis is based on two types of observations. First, experimental data emphasize the role of small, erythropoietically less valuable rHu-Epo isoforms in its organoprotective effects. Second, clinical observations suggest that rHu-Epo enables for less variable Hb correction than the larger molecules, and pronounced within-subject Hb variability has been suggested as an independent predictor of poor long-term outcomes of renal anemia management.

摘要

慢性肾衰竭(CRF)是一种广泛存在的医学问题,通常伴有促红细胞生成素缺乏引起的低增生性贫血(“肾性贫血”)。贫血极大地降低了 CRF 患者的生活质量(Hr-QoL)和高发病率和死亡率。重组人促红细胞生成素(rHu-Epo)在大约 20 年前被引入医学实践。它能够纠正贫血(血红蛋白水平,Hb),具有显著的即时(Hr-QoL 改善)和长期效果(降低发病率和死亡率)。新的实验数据表明,长期益处不仅可能由于抗贫血作用,而且还可能由于(rHu)-Epo 通过与“促红细胞生成”促红细胞生成素受体不同的受体复合物介导的直接器官保护作用。在过去十年中,两种替代肾性贫血的治疗方法已获得批准:达贝泊汀和 CERA。两者都是“促红细胞生成”受体的直接激动剂,均源自 rHu-Epo。在分子水平上,它们与 rHu-Epo 不同,因为它们是更大的分子(达贝泊汀是具有更高糖含量的基因修饰 rHu-Epo,而 CERA 是聚乙二醇化 rHu-Epo),对促红细胞生成素受体的亲和力较低,但循环时间更长。在纠正肾性贫血方面,它们与 rHu-Epo 无差异,并且剂量更频繁。关于长期结果,它们从未与 rHu-Epo 进行比较。有人假设,关于长期结果(发病率、死亡率),rHu-Epo 可能优于这些较大的分子。该假设基于两种观察结果。首先,实验数据强调了小的、促红细胞生成素价值较低的 rHu-Epo 同工型在其器官保护作用中的作用。其次,临床观察表明,rHu-Epo 能够实现比较大分子更稳定的 Hb 校正,并且 Hb 内个体变异性较大已被认为是肾性贫血管理不良长期结果的独立预测因子。

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