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首页> 外文期刊>Critical care medicine >Pharmacokinetics and pharmacodynamics of six epoetin alfa dosing regimens in anemic critically ill patients without acute blood loss.
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Pharmacokinetics and pharmacodynamics of six epoetin alfa dosing regimens in anemic critically ill patients without acute blood loss.

机译:在无急性失血的贫血重症贫血患者中,六种依泊汀阿法剂量方案的药代动力学和药效学。

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OBJECTIVE: To describe the pharmacokinetic profiles of six different dosing regimens for epoetin alfa, and whether more rapid and robust reticulocytosis can be elicited with more frequent administration of epoetin alfa in anemic critically ill patients. DESIGN: Randomized, open-label, multicenter, 28-day clinical trial. SETTING: Ten centers in the United States. PATIENTS: Adult (age >or=18 years) critically ill patients with hemoglobin or=7 days, with no ongoing acute blood loss. INTERVENTIONS: One of six dosing epoetin alfa regimens for 15 days, as follows: 40,000 IU once weekly, subcutaneously (group A) or intravenously (IV) (group B); 15,000 IU every other day, subcutaneously (group C) or IV (group D); or 40,000 IU day 1 and 3, subcutaneously (group E) or IV (group F), followed by 15,000 IU once every other days 5-15 subcutaneously in both groups. MEASUREMENTS: Serum erythropoietin concentration, absolute reticulocyte count, and adverse events. MAIN RESULTS:Of the 60 patients who were enrolled (60% men, mean age 53 years, mean Acute Physiology and Chronic Health Evaluation II score, 19.5), 30 were evaluable for both pharmacokinetics and pharmacodynamics (50%). Erythropoietin exposure was approximately ten times greater for IV dosing than for subcutaneous dosing. Mean absolute reticulocyte count peaked at day 11 or 15 in each group and appeared to be greater for subcutaneous dosing (mean peak response 149-169 x 10(9)/L) compared with IV dosing (mean peak response 138-147 x 10(9)/L) at most visits. The most frequently reported adverse events were pyrexia (18%), hypokalemia (15%), and hypophosphatemia (15%). CONCLUSIONS: In this study of anemic critically ill patients treated with epoetin alfa, all dosing regimens were well tolerated and appeared to effect reticulocytosis, with a peak at day 11 or 15 in most patients. The pharmacokinetics of epoetin alfa did not predict pharmacodynamic response in anemic critically ill patients.
机译:目的:描述六种不同剂量的依泊汀α的药代动力学,以及在贫血危重患者中更频繁地服用依泊汀α是否可以引起更快,更强的网状细胞增多。设计:随机,开放标签,多中心,28天临床试验。地点:美国的十个中心。患者:成年(≥18岁)血红蛋白≤12 g / dL的重症患者,预期住院时间≥7天,无持续性急性失血。干预措施:六个剂量的依泊汀阿尔法治疗方案之一,为期15天,方法如下:每周一次,皮下注射(A组)或静脉注射(IV组)(B组)40,000 IU;每隔一天15,000 IU,皮下注射(C组)或静脉注射(D组);或皮下注射(第E组)或静脉注射(F组)第1天和第3天40,000 IU,然后每隔5-15天每两天皮下注射15,000 IU。测量:血清促红细胞生成素浓度,网织红细胞绝对计数和不良事件。主要结果:在入组的60例患者中(60%的男性,平均年龄53岁,平均急性生理学和慢性健康评估II评分为19.5),其中30例可同时进行药代动力学和药效学评估(50%)。静脉给药的促红细胞生成素暴露量约为皮下给药的十倍。每组的平均绝对网织红细胞计数在第11天或第15天达到峰值,并且与静脉给药相比,皮下给药的平均绝对网织计数更高(平均峰值响应149-169 x 10(9)/ L)。 9)/ L)。最常见的不良事件是发热(18%),低血钾(15%)和低磷血症(15%)。结论:在这项用依泊汀阿法治疗的贫血危重病患者的研究中,所有给药方案均耐受良好,并且似乎会影响网状细胞增多,大多数患者在第11天或第15天达到峰值。依泊汀α的药代动力学不能预测贫血重症患者的药效学反应。

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