首页> 外文期刊>Regulatory peptides. >Triple therapy with octreotide, galanin and serotonin induces necrosis and increases apoptosis of a rat colon carcinoma.
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Triple therapy with octreotide, galanin and serotonin induces necrosis and increases apoptosis of a rat colon carcinoma.

机译:奥曲肽,甘丙肽和5-羟色胺的三联疗法可诱导坏死并增加大鼠结肠癌的细胞凋亡。

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A rat colonic adenocarcinoma was implanted subcutaneously (s.c.) in nude mice. After 7 days, the animals were divided into different groups. Two groups received subcutaneous injections twice daily with 3 or 6 micro g/kg body weight octreotide, galanin and serotonin. Three groups were respectively treated with 20, 30, and 40 micro g/kg body weight of the previously mentioned bioactive substances. Control group received only saline solution in the same fashion as treated animals. The treatment lasted for 5 days. The tumour volume and weight, the relative density of blood vessels, of tumour necrotic tissue, of apoptotic nuclei and of proliferating nuclei were measured. Apoptosis was detected by in situ labelling of nuclear DNA fragmentation according to TUNEL method, and proliferation by immunocytochemistry. Morphometry was done with the classical stereological point-counting method. Food consumption, animal weight, faeces weight and its water content were measured for 3 days before and after treatment. Triple therapy with 3 and 6 micro g/kg body weight had no effect on any of the parameters measured, except in reducing the relative volume density of tumour blood vessels. Treatment with 20, 30 and 40 micro g/kg body weight of the previously mentioned bioactive substances reduced the tumour volume, the relative volume density of blood vessels and increased the relative volume density of necrotic tissue and of apoptotic nuclei (in the 20 micro g group). However, there was no difference between treated mice and controls regarding the relative volume density of proliferating nuclei. There was no statistical difference between treated animals regarding food consumption, body weight, faeces weight and its water content before and during treatment. The present study confirms that triple therapy with octreotide, galanin and serotonin causes regression of a rat colon carcinoma. It further showed that optimum treatment dose is 20 micro g/kg body weight of each bioactive substance. Moreover, this therapy regime does not show apparent side effects in the experiments carried out on mice.
机译:将大鼠结肠腺癌皮下(s.c.)植入裸鼠中。 7天后,将动物分成不同的组。两组每天两次皮下注射3或6微克/千克体重的奥曲肽,甘丙肽和5-羟色胺。三组分别用20、30和40微克/千克体重的前述生物活性物质治疗。对照组仅以与治疗动物相同的方式接受盐溶液。治疗持续了5天。测量了肿瘤的体积和重量,血管的相对密度,肿瘤坏死组织,凋亡核和增殖核。通过根据TUNEL方法原位标记核DNA片段来检测凋亡,并通过免疫细胞化学检测增殖。形态计量学是用经典的立体点算方法完成的。在治疗前后3天测量食物消耗,动物体重,粪便重量及其水含量。体重为3和6微克/千克的三重疗法对任何测得的参数均无影响,只是降低了肿瘤血管的相对体积密度。用20、30和40微克/千克体重的上述生物活性物质进行治疗可减少肿瘤体积,血管的相对体积密度并增加坏死组织和凋亡核的相对体积密度(在20微克中组)。但是,在治疗的小鼠和对照组之间,关于增殖核的相对体积密度没有差异。在治疗前和治疗过程中,治疗动物之间的食物消耗,体重,粪便重量及其含水量没有统计学差异。本研究证实,使用奥曲肽,甘丙肽和5-羟色胺的三联疗法可导致大鼠结肠癌消退。进一步表明,最佳治疗剂量为每种生物活性物质20微克/千克体重。而且,这种治疗方案在对小鼠进行的实验中未显示出明显的副作用。

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