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胰岛素对阿霉素诱导的大鼠宿主毒性及肿瘤消退的影响。

Impact of insulin on doxorubicin-induced rat host toxicity and tumor regression.

作者信息

Peacock J L, Gorschboth C M, Norton J A

出版信息

Cancer Res. 1987 Aug 15;47(16):4318-22.

PMID:3300963
Abstract

To test whether the anorexia and host depletion following doxorubicin chemotherapy can be improved by concomitant insulin therapy, 70 F344 rats were divided equally between tumor-bearing (TB) and non-tumor-bearing (NTB) groups and studied for food intake, host weight, and tumor size changes. Sarcoma fragments were implanted s.c. in TB rats and 18 days later all rats received an i.v. dose of doxorubicin (8 mg/kg). The following day TB and NTB rats were randomized to receive neutral protaminehagedorn insulin (2 units/100 g/24 h) or normal saline until food intake returned to normal. Following doxorubicin administration food intake and host weight declined in an identical pattern in both NTB and TB rats treated with saline. However, beginning on day 6 insulin-treated TB and NTB rats ate significantly more than saline-treated controls. Insulin-treated animals returned to normal food intake levels in 50% less time than controls. This improved food intake resulted in an improved host mass beginning also on day 6 for both TB and NTB rats. In addition, it appeared that insulin treatment significantly improved the tumor shrinkage initiated by doxorubicin. Following doxorubicin, insulin-treated TB rats had a greater reduction of tumor size (10.6 +/- 1.2 cm3) compared to saline-treated rats (6.6 +/- 0.8 cm3, P less than 0.01). To further characterize the effect of insulin and/or doxorubicin on tumor growth, the experiment was repeated in the same manner except for two additional TB groups: saline- and insulin-treated tumor bearers with treatment beginning 19 days after tumor implant. Rats treated with doxorubicin had a significant reduction in tumor size compared to rats not treated with doxorubicin (P less than 0.001). Insulin alone did not affect tumor growth, but insulin plus doxorubicin significantly decreased tumor size compared to doxorubicin alone (P less than 0.01). In a second experiment using 80 rats insulin treatment had no apparent effect on reduction of peripheral blood counts including white blood cells, neutrophils, lymphocytes, platelets, and hematocrit induced by doxorubicin in either NTB or TB rats. Insulin given 24 h previously had minimal effect on plasma glucose. The marked improvement in food intake and host weight, as well as additional tumor reduction with exogenous insulin following doxorubicin, suggests that insulin may have a role in reversal of doxorubicin host nutritional toxicity and perhaps improvement of antitumor efficacy.

摘要

为了测试多柔比星化疗后出现的厌食和机体消耗是否能通过同时进行胰岛素治疗得到改善,70只F344大鼠被平均分为荷瘤(TB)组和非荷瘤(NTB)组,并对其食物摄入量、机体重量和肿瘤大小变化进行研究。将肉瘤组织块皮下植入TB组大鼠体内,18天后所有大鼠静脉注射一剂多柔比星(8毫克/千克)。第二天,将TB组和NTB组大鼠随机分为接受中性鱼精蛋白锌胰岛素(2单位/100克/24小时)或生理盐水治疗的两组,直至食物摄入量恢复正常。在给予多柔比星后,接受生理盐水治疗的NTB组和TB组大鼠的食物摄入量和机体重量均以相同模式下降。然而,从第6天开始,接受胰岛素治疗的TB组和NTB组大鼠的进食量明显多于接受生理盐水治疗的对照组。接受胰岛素治疗的动物恢复到正常食物摄入量水平所需的时间比对照组少50%。这种食物摄入量的改善也使TB组和NTB组大鼠从第6天开始机体重量有所增加。此外,胰岛素治疗似乎显著增强了多柔比星引发的肿瘤缩小效果。给予多柔比星后,接受胰岛素治疗的TB组大鼠的肿瘤大小缩小幅度(10.6±1.2立方厘米)大于接受生理盐水治疗的大鼠(6.6±0.8立方厘米,P<0.01)。为了进一步明确胰岛素和/或多柔比星对肿瘤生长的影响,除了另外两个TB组外,以相同方式重复该实验:肿瘤植入19天后开始接受生理盐水和胰岛素治疗的荷瘤大鼠。与未接受多柔比星治疗(P<0.001)。单独使用胰岛素对肿瘤生长没有影响,但与单独使用多柔比星相比,胰岛素联合多柔比星能显著减小肿瘤大小(P<0.01)。在第二个实验中,使用80只大鼠,胰岛素治疗对多柔比星诱导的NTB组或TB组大鼠外周血细胞计数(包括白细胞、中性粒细胞、淋巴细胞、血小板和血细胞比容)的降低没有明显影响。提前24小时给予胰岛素对血糖的影响最小。多柔比星治疗后食物摄入量和机体重量的显著改善,以及外源性胰岛素使肿瘤进一步缩小,表明胰岛素可能在逆转多柔比星对机体的营养毒性以及可能提高抗肿瘤疗效方面发挥作用。

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