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透析充分性及对促红细胞生成剂的反应:证据基础是什么?

Dialysis adequacy and response to erythropoietic agents: what is the evidence base?

作者信息

Locatelli Francesco, Del Vecchio Lucia

机构信息

Department of Nephrology and Dialysis, Ospedale A. Manzoni, Lecco, Italy.

出版信息

Nephrol Dial Transplant. 2003 Nov;18 Suppl 8:viii29-35. doi: 10.1093/ndt/gfg1089.

Abstract

Anaemia secondary to chronic kidney disease is a complex syndrome. Adequate dialysis can contribute to its correction by removing small, and possibly middle/large molecules, that may inhibit erythropoiesis. A clear relationship between higher haemoglobin or haematocrit levels, lower recombinant human erythropoietin (epoetin) dose and increase in dialysis dose has been reported in a number of prospective and retrospective studies. This is particularly true in patients receiving inadequate dialysis. Increased attention has also been paid to the relationship between dialysis, increased inflammatory stimulus and response to erythropoietic therapy, as dialysate contamination and low-compatible treatments may increase the production of cytokines and consequently inhibit erythropoiesis. As middle-/large-molecular-weight inhibitors can only be adsorbed or removed by more permeable membranes, the biocompatibility of dialysis membranes and flux are also important factors. In highly selected, adequately dialysed patients without iron or vitamin depletion, however, the effect of these treatment modalities on anaemia appears to be smaller than expected. The role of on-line treatments is still controversial; moreover, it is still difficult to discriminate between the effects of on-line haemodiafiltration per se (use of high-flux biocompatible membranes and pyrogen-free dialysate) from that of an increased dialysis dose. Prospective, randomized, adequately sized studies on this topic are still needed. Results, albeit very preliminary, obtained with short or long nocturnal daily haemodialysis on anaemia correction are encouraging. Adequate dialysis is not only a tool for reducing morbidity and mortality of haemodialysis patients, but is also a way of optimizing responsiveness to erythropoietic therapy, allowing easier achievement of anaemia correction in a higher percentage of patients.

摘要

慢性肾脏病继发性贫血是一种复杂的综合征。充分透析可通过清除可能抑制红细胞生成的小分子以及可能的中/大分子来促进贫血的纠正。多项前瞻性和回顾性研究报告了较高的血红蛋白或血细胞比容水平、较低的重组人促红细胞生成素(促红素)剂量与透析剂量增加之间存在明确关系。在接受透析不充分的患者中尤其如此。人们也越来越关注透析、炎症刺激增加与对促红细胞生成治疗的反应之间的关系,因为透析液污染和低生物相容性治疗可能会增加细胞因子的产生,从而抑制红细胞生成。由于中/大分子抑制剂只能被更具通透性的膜吸附或清除,透析膜的生物相容性和通量也是重要因素。然而,在经过高度筛选、透析充分且无铁或维生素缺乏的患者中,这些治疗方式对贫血的影响似乎比预期的要小。在线治疗的作用仍存在争议;此外,仍然难以区分在线血液透析滤过本身(使用高通量生物相容性膜和无热原透析液)与增加透析剂量的效果。仍需要针对该主题进行前瞻性、随机、样本量充足的研究。夜间短程或长程每日血液透析在纠正贫血方面获得的结果虽然非常初步,但令人鼓舞。充分透析不仅是降低血液透析患者发病率和死亡率的一种手段,也是优化对促红细胞生成治疗反应性的一种方式,能使更高比例的患者更轻松地实现贫血纠正。

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