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Impact of Octreotide and SOM-230 on liver metastasis and hepatic lipidperoxidation in ductal pancreatic adenocarcinoma in Syrian Hamster

机译:奥曲肽和SOM-230对叙利亚仓鼠导管胰腺腺癌肝转移和肝脂质过氧化的影响

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Octreotide is a somatostatin analogue binding on two receptor subtypes. In previous trials Octreotide showed inhibitory effects on tumour growth and liver metastasis in experimental pancreatic cancer. Thus we evaluated whether the new somatostatin analogue SOM-230 binding on 4 receptor subtypes has superior effects on carcinogenesis in pancreatic carcinoma. About 120 Syrian hamsters were randomised into six groups (n = 20): Gr.1: Aqua/Aqua, Gr.2: BOP/Aqua, Gr.3: Aqua/Octreotide, Gr.4: BOP/Octreotide, Gr.5: Aqua/SOM-230, Gr.6: BOP/SOM-230. Tumour groups 2,4,6 subcutaneously received 10 mg/kg body weight N-nitrosobis-2-oxopropylamin (BOP) weekly for 10 weeks, healthy control Gr.1,3,5 were given aqua. In the 17th week therapy started with Octreotide and SOM-230 for 16 weeks, after 32 weeks animals were sacrificed. Pancreas and liver were histopathologically analysed. Hepatic lipidperoxidation was determined by activities of antioxidative enzymes gluthation-peroxidase (GSH-Px) and superoxiddismutase (SOD) as well as concentration of thiobarbituric-acid reactive substances (TBARS). Incidence of liver metastases was 88.2% in Gr.2 (BOP/Aqua), it was decreased in Gr.4 (BOP/Octreo: 40%) and Gr.6 (BOP/SOM-230: 50%) (P < 0.05). Mean number/animal and mean-2-dimensional size of liver metastases did not differ between tumour groups. Comparing GSH-Px-activity in intrametastatic and extrametastatic hepatic tissue revealed a significant increase extrametastatically in Gr.2 (BOP/Aqua) and Gr.6 (BOP/SOM-230). SOD-activity in liver metastases was decreased in Gr.2 (1,801) (P < 0.05) versus Gr.4 (8,304) and Gr.6 (7,038). Intrametastatic TBARS concentration was increased in Gr.2 compared to Gr.4 (BOP/Octreotid) and Gr.6 (BOP/SOM-230) (P < 0.05). Octreotide and SOM-230 equally reduced liver metastasis in ductal pancreatic adenocarcinoma probably by a reduction of lipidperoxidation.
机译:奥曲肽是一种结合两种受体亚型的生长抑素类似物。在先前的试验中,奥曲肽对实验性胰腺癌显示出对肿瘤生长和肝转移的抑制作用。因此,我们评估了新的生长抑素类似物SOM-230与4种受体亚型的结合是否对胰腺癌的致癌作用具有更好的作用。大约120只叙利亚仓鼠被随机分为六组(n = 20):第1组:Aqua / Aqua,第2组:BOP / Aqua,第3组:Aqua / Octreotide,第4组:BOP / Octreotide,第5组:Aqua / SOM-230,第6组:BOP / SOM-230。皮下肿瘤组2,4,6每周皮下接受10 mg / kg体重的N-亚硝基双-2-氧代丙基胺(BOP),持续10周,健康对照Gr.1,3,5被给予水。在第32周杀死动物后,在第17周以奥曲肽和SOM-230开始治疗16周。胰腺和肝脏进行了组织病理学分析。肝脂质过氧化是通过抗氧化酶谷胱甘肽过氧化物酶(GSH-Px)和超氧化物歧化酶(SOD)的活性以及硫代巴比妥酸反应性物质(TBARS)的浓度来确定的。 Gr.2(BOP / Aqua)的肝转移发生率为88.2%,Gr.4(BOP / Octreo:40%)和Gr.6(BOP / SOM-230:50%)降低了(P <0.05 )。肿瘤组之间肝转移的平均数/动物和二维平均大小无差异。比较转移内和转移外肝组织中的GSH-Px活性,发现Gr.2(BOP / Aqua)和Gr.6(BOP / SOM-230)转移外明显增加。在肝转移中,SOD活性在Gr.2(1,801)(P <0.05)中低于Gr.4(8,304)和Gr.6(7,038)。与Gr.4(BOP / Octreotid)和Gr.6(BOP / SOM-230)相比,Gr.2中的转移内TBARS浓度增加了(P <0.05)。奥曲肽和SOM-230可能通过减少脂质过氧化而同样降低导管型胰腺癌的肝转移。

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