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Effects of combined octreotide and aspirin on the growth of gastric cancer

机译:奥曲肽联合阿司匹林对胃癌生长的影响

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摘要

Objective To investigate the effects of the combination of octreotide and aspirin on the growth of gastric cancer. Methods Proliferation of gastric cancer cell lines treated with octreotide or aspirin was determined by ~3H-thymidine incorporation. After xenografts of human gastric cancer were implanted orthotropically in the stomach of nude mice, they were administered octreotide plus aspirin for 8 weeks. The mRNA of somatostatin receptor in the tissues of gastric carcinoma was detected by reverse transcription polymerase chain reaction (RT-PCR). Cyclooxygenase-2 in gastric cancer tissues was measured by immuno-histochemistry. Results Both octreotide and aspirin significantly reduced the ~3H-thymidine incorporation of gastric cancer cells. Xenografts in situ were found in all stomachs of nude mice except for two in the combination group. Either size or weight of tumors treated by octreotide, aspirin or in combination was significantly reduced as compared with that of controls. The inhibition rate for tumor was 60.6% (octreotide), 39.3% (aspirin), and 85.6% (in combination) respectively. No severe side effects were observed in any treated groups. Somatostatin receptor-2 and -3 were expressed in the transplanted gastric adenocarcinomas. Aspirin could down-regulate the strong expression of cyclooxygenase-2 in the tissue of gastric adenocarcinomas of nude mice. Conclusion A combination of octreotide and aspirin significantly inhibited proliferation of gastric cancer through mediation of somatosatin receptors and suppression of cyclooxygenase-2.
机译:目的探讨奥曲肽联合阿司匹林对胃癌生长的影响。方法采用〜3H-胸苷掺入法测定奥曲肽或阿司匹林对胃癌细胞的增殖作用。将人胃癌异种移植物正交植入裸鼠的胃中后,给予奥曲肽加阿司匹林8周。通过逆转录聚合酶链反应(RT-PCR)检测胃癌组织中生长抑素受体的mRNA。通过免疫组织化学法测定胃癌组织中的环氧合酶-2。结果奥曲肽和阿司匹林均可显着降低胃癌细胞的〜3H-胸苷掺入。在裸鼠的所有胃中都发现了原位异种移植物,除了联合组中的两只外。与对照组相比,用奥曲肽,阿司匹林或联合治疗的肿瘤的大小或重量均明显降低。肿瘤抑制率分别为60.6%(奥曲肽),39.3%(阿司匹林)和85.6%(联合用药)。在任何治疗组中均未观察到严重的副作用。生长抑素受体2和-3在移植的胃腺癌中表达。阿司匹林可以下调裸鼠胃腺癌组织中环氧合酶2的强表达。结论奥曲肽和阿司匹林联用可通过促生长素受体的介导和环氧合酶-2的抑制显着抑制胃癌的增殖。

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