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CHIP对正常和荷瘤C3H小鼠的生化效应评估。

Evaluation of the biochemical effects of CHIP in normal and tumour-bearing C3H mice.

作者信息

Laverick M, Gordon M, Kind P R, Slavin B M, Nias A H

出版信息

Br J Cancer. 1986 Jun;53(6):761-72. doi: 10.1038/bjc.1986.130.

Abstract

The biochemical effects of CHIP have been studied in C3H mice with and without transplanted mammary tumour. The maximum tolerated dose of CHIP was first determined by lethality and intestinal crypt assays to be 40 mg kg-1 and this dose was used to assay the time course of gastric distension and the pattern of drug distribution. A high level of CHIP uptake was found in liver as well as kidney. For this reason, tests for both kidney and liver damage were undertaken up to 60 days post-treatment using a dose of 10 mg kg-1 Neoplatin for comparison. Despite the high level of platinum drug uptake in liver, there was no biochemical evidence of hepatocellular or cholestatic damage. From the renal point of view, there was the expected rise in serum urea after Neoplatin but not after CHIP and there was also a rise in urinary NAG after Neoplatin in tumour bearing mice. There was, however, evidence of suppression of protein levels including enzymes, following treatment with both drugs. Tumour-bearing mice respond differently from normal mice following treatment with platinum drugs. The study confirms that CHIP is less toxic than Neoplatin.

摘要

已在有或无移植性乳腺肿瘤的C3H小鼠中研究了CHIP的生化效应。首先通过致死率和肠道隐窝试验确定CHIP的最大耐受剂量为40mg/kg,并用该剂量来测定胃扩张的时间进程和药物分布模式。发现肝脏和肾脏中CHIP的摄取水平较高。因此,使用10mg/kg的顺铂作为对照,在治疗后60天内对肾脏和肝脏损伤进行了检测。尽管肝脏中铂类药物的摄取水平较高,但没有肝细胞或胆汁淤积损伤的生化证据。从肾脏方面来看,顺铂治疗后血清尿素升高,但CHIP治疗后未出现这种情况,且荷瘤小鼠在顺铂治疗后尿NAG也升高。然而,两种药物治疗后均有包括酶在内的蛋白质水平受到抑制的证据。荷瘤小鼠在接受铂类药物治疗后的反应与正常小鼠不同。该研究证实CHIP的毒性低于顺铂。

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本文引用的文献

1
Mouse proteinuria.小鼠蛋白尿
Am J Physiol. 1958 Jan;192(1):69-72. doi: 10.1152/ajplegacy.1957.192.1.69.

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