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首页> 外文期刊>Archives of Toxicology >Nephrotoxicity of a novel antineoplastic platinum complex, nedaplatin: a comparative study with cisplatin in rats.
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Nephrotoxicity of a novel antineoplastic platinum complex, nedaplatin: a comparative study with cisplatin in rats.

机译:新型抗肿瘤铂络合物奈达铂的肾毒性:与顺铂在大鼠中的比较研究。

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摘要

The present study was designed to characterize the nephrotoxicity induced by the antineoplastic platinum complex nedaplatin (NDP) in rats of different ages in comparison with cisplatin (CDDP). A single dose of 15 mg/kg NDP or 7.5 mg/kg CDDP was administered intravenously to 8-, 11-, or 15-week-old male and female SD rats, which were then sacrificed after ten days. Body weight decreases were observed for both drugs, in direct relation to age. CDDP treatment markedly increased urinary excretion of NAG, gamma-GTP, LDH and protein, with peaks on day 4 and complete or partial recovery on day 7; NDP increased NAG, LDH and protein excretion, but to a lesser extent, and these elevations were generally more marked for females. CDDP increased plasma creatinine and BUN in males and females of all age groups at necropsy. No apparent changes were seen following NDP treatment except in the 15-week-old rats. These results also show that NDP is less nephrotoxic than CDDP. CDDP-treated rats showed remarkable proximal tubular lesions in the renal cortex and corticomedullary region, and the papillary lesions were minor. On the other hand, the NDP-induced nephrotoxicity was morphologically characterized by hyaline droplet changes (electron microscopically, hyperplasia of lysosomes), necrosis or hyperplasia of the collecting duct epithelium in the renal papilla and the epithelium covering the papilla. Cortical lesions, indicated by slight tubular dilatation, were found only in the animals with papillary lesions. In summary, NDP is a promising second-generation platinum complex with reduced nephrotoxicity.
机译:本研究旨在表征与顺铂(CDDP)相比,不同年龄的抗肿瘤铂络合物奈达铂(NDP)诱导的肾毒性。向8、11或15周龄的雄性和雌性SD大鼠静脉内施用单剂15 mg / kg NDP或7.5 mg / kg CDDP,然后在十天后将其处死。两种药物均观察到体重下降,与年龄直接相关。 CDDP处理可显着增加NAG,γ-GTP,LDH和蛋白质的尿排泄,在第4天达到峰值,在第7天完全或部分恢复。 NDP增加NAG,LDH和蛋白质排泄,但程度较小,这些升高通常对女性更为明显。剖检时,所有年龄段的男性和女性的CDDP升高血浆肌酐和BUN。除15周大的大鼠外,NDP治疗后未见明显变化。这些结果还表明,NDP比CDDP的肾毒性小。用CDDP处理的大鼠在肾皮质和皮质髓质区域显示出明显的近端肾小管病变,乳头状病变较小。另一方面,NDP诱导的肾毒性的形态学特征是透明液滴的变化(电子显微镜下,溶酶体的增生),肾乳头和覆盖乳头的上皮的收集管上皮坏死或增生。仅在具有乳头状病变的动物中发现了由轻微的管状扩张表示的皮质病变。总之,NDP是具有降低的肾毒性的有希望的第二代铂络合物。

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