Beguin Y, Loo M, R'Zik S, Sautois B, Lejeune F, Rorive G, Fillet G
Department of Medicine, University of Liège, Belgium.
Blood. 1993 Oct 1;82(7):2010-6.
Recombinant human erythropoietin (rHuEpo) has been shown to be effective in correcting the anemia of chronic renal failure, but the dose needed may be variable. The reason for this variation is not known, but several factors could be involved, such as iron deficiency, inflammation, aluminum intoxication, hyperparathyroidism, blood losses, or marrow dysfunction. Treatment with rHuEpo was given intravenously thrice weekly after hemodialysis to 64 consecutive unselected patients with the anemia of chronic renal failure. The starting dose was 50 U/kg/dose, which was increased to 75 and 100 U/kg/dose if no response was observed after 1 and 2 months of treatment. After a minimum follow-up of 6 months, response was evaluated as early (hematocrit [Hct] > or = 30% before 3 months) or late (Hct > or = 30% after 3 months) response, or failure (target Hct not attained). We examined the value of various laboratory parameters (baseline values and early changes) as predictors of response to rHuEpo. The best prediction by pretreatment parameters only was obtained with baseline serum transferrin receptor (TfR) (< or > or = 3,500 ng/mL) and fibrinogen (< or > or = 4 g/L): 100% response rate when both parameters were low, versus only 29% when they were both high, and versus 67% when one was low and the other high. When the 2-week TfR increment was greater than 20%, the response rate was 96%. When TfR increment was less than 20%, the response rate was 100% when baseline TfR and fibrinogen were low, 12% when fibrinogen was elevated, and 62% when fibrinogen was low but baseline TfR high. The predictive value of baseline TfR and fibrinogen and of the 2-week increment of TfR was confirmed by life table analysis and stepwise discriminant analysis. Major reasons for failure or late response were identified and included subclinical inflammation, iron deficiency, functional iron deficiency, marrow disorders, hemolysis, bleeding, and low Epo dose. We conclude that response to rHuEpo can be predicted early by pretreatment fibrinogen and TfR, together with early changes of TfR levels. These prognostic factors illustrate the importance of the early erythropoietic response, subclinical inflammation, and functional iron deficiency. Early recognition of a low probability of response in a given patient could help identify and correct specific causes of treatment failure to hasten clinical improvement and avoid prolonged ineffective use of an expensive medication.
重组人促红细胞生成素(rHuEpo)已被证明可有效纠正慢性肾衰竭贫血,但所需剂量可能存在差异。这种差异的原因尚不清楚,但可能涉及多种因素,如缺铁、炎症、铝中毒、甲状旁腺功能亢进、失血或骨髓功能障碍。对64例连续入选的慢性肾衰竭贫血患者,在血液透析后每周静脉注射三次rHuEpo进行治疗。起始剂量为50 U/kg/次,若治疗1个月和2个月后无反应,则剂量增加至75 U/kg/次和100 U/kg/次。在至少随访6个月后,将反应评估为早期(3个月前血细胞比容[Hct]≥30%)或晚期(3个月后Hct≥30%)反应,或无反应(未达到目标Hct)。我们研究了各种实验室参数(基线值和早期变化)作为rHuEpo反应预测指标的价值。仅通过预处理参数进行的最佳预测是基于基线血清转铁蛋白受体(TfR)(<或≥3500 ng/mL)和纤维蛋白原(<或≥4 g/L):当两个参数都低时,反应率为100%;当两个参数都高时,反应率仅为29%;当一个低一个高时,反应率为67%。当2周TfR增量大于20%时,反应率为96%。当TfR增量小于20%时,若基线TfR和纤维蛋白原低,反应率为100%;若纤维蛋白原升高,反应率为12%;若纤维蛋白原低但基线TfR高,反应率为62%。通过生存表分析和逐步判别分析证实了基线TfR和纤维蛋白原以及TfR 2周增量的预测价值。确定了无反应或晚期反应的主要原因,包括亚临床炎症、缺铁、功能性缺铁、骨髓疾病、溶血、出血和促红细胞生成素剂量低。我们得出结论,预处理纤维蛋白原和TfR以及TfR水平的早期变化可早期预测对rHuEpo的反应。这些预后因素说明了早期红细胞生成反应、亚临床炎症和功能性缺铁的重要性。早期识别特定患者反应可能性低,有助于识别和纠正治疗失败的具体原因,以加速临床改善并避免长期无效使用昂贵药物。
