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促红细胞生成素可降低顺铂所致的累积肾毒性,并增强肾小管细胞增殖。

Erythropoietin reduces cumulative nephrotoxicity from cisplatin and enhances renal tubular cell proliferation.

作者信息

Zafirov Dimce, Petrusevska G, Sikole Aleksandar, Trojacanec J, Labacevski N, Kostova E, Jakovski K, Atanasovska E, Petrov S

机构信息

Preclinical and Clinical Pharmacology with Toxicology Department, Medical Faculty, Ss Cyril and Methodius University, Skopje, Republic of Macedonia.

出版信息

Prilozi. 2008 Dec;29(2):167-83.

Abstract

Cisplatin, a heavy metal complex, is one of the most active drugs used in the treatment of several human malignancies. However, high-dose therapy with cisplatin is limited by its cumulative nephrotoxicity. The main objectives of this study were to determine the role of recombinant human erythropoietin (Epoetin alfa) in the prevention of nephrotoxicity induced experimentally in Wistar rats by long-term administration of cisplatin (2 mg/kg/b.w./week) over eight weeks, and an evaluation of its effect on renal tubular cell proliferation. The animals were randomly assigned into three groups, each including 25 rats. Group 1 (CP) received only cisplatin (2 mg/kg/b.w./week), group 2 (CP+EPO) received cisplatin (2 mg/kg/b.w./week) and epoetin alfa (150 IE/kg/b.w./three times a week), and group 3 (control group) received only saline. During the study, the following tests for the assessment of the renal function and renal damages were performed: determination of concentration of serum creatinine and BUN and determination of total protein quantity in 24-hour urine samples. At the end of the study, the abdomen was opened and both kidneys of the rats were removed and sent for histological and morphometric analysis. Ki-67 was used as a tool to determine a proliferative index. The results obtained have shown that epoetin alfa significantly reduced the functional renal failures and renal damages, and increased toleration of high doses of cisplatin. At the same time, our results with regard to tubular proliferative index have confirmed that one of the possible mechanisms by which erythropoietin accomplishes its renoprotective effect is stimulation of tubular cell proliferation and regeneration.

摘要

顺铂是一种重金属络合物,是治疗多种人类恶性肿瘤最有效的药物之一。然而,顺铂的高剂量治疗受到其累积肾毒性的限制。本研究的主要目的是确定重组人促红细胞生成素(阿法依泊汀)在预防Wistar大鼠长期(八周,每周2毫克/千克体重)给予顺铂所致实验性肾毒性中的作用,并评估其对肾小管细胞增殖的影响。将动物随机分为三组,每组25只大鼠。第1组(CP组)仅接受顺铂(每周2毫克/千克体重),第2组(CP + EPO组)接受顺铂(每周2毫克/千克体重)和阿法依泊汀(每周三次,150国际单位/千克体重),第3组(对照组)仅接受生理盐水。在研究过程中,进行了以下评估肾功能和肾损伤的测试:测定血清肌酐和尿素氮浓度以及测定24小时尿液样本中的总蛋白量。研究结束时,打开腹腔,取出大鼠的双肾并送去进行组织学和形态计量学分析。使用Ki-67作为确定增殖指数的工具。获得的结果表明,阿法依泊汀显著降低了功能性肾衰竭和肾损伤,并提高了对高剂量顺铂的耐受性。同时,我们关于肾小管增殖指数的结果证实,促红细胞生成素实现其肾脏保护作用的可能机制之一是刺激肾小管细胞增殖和再生。

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