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首页> 外文期刊>Surgical Endoscopy >Port-site metastasis after CO2 pneumoperitoneum: role of adhesion molecules and prevention with antiadhesion molecules.
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Port-site metastasis after CO2 pneumoperitoneum: role of adhesion molecules and prevention with antiadhesion molecules.

机译:CO2气腹后的端口位转移:粘附分子的作用和抗粘附分子的预防。

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BACKGROUND: Port-site metastasis is a continuing problem in laparoscopic cancer surgery. To clarify the role of adhesion molecules in the development of port-site metastasis, particularly with regard to prevention, we performed experiments in which port-site metastasis was inhibited using antibodies against extracellular matrix proteins or the active Arg-Gly-Asp (RGD) peptide after CO2 pneumoperitoneum in a murine model. METHODS: We examined the development of port-site metastasis under the following conditions: (1) CO2 pneumoperitoneum with or without hyaluronic acid and anti-integrin or anti-CD44 antibody and (2) CO2 pneumoperitoneum and a RGD peptide or pseudo-RGD sequence peptide (FC-336). BALB/c mice ( n = 130) were injected with 5 x 10(5) human gastric cancer cells (MKN45) and either antibody or peptide, treated with CO2 pneumoperitoneum, and injected intraperitoneally with antibody or peptide for 5 days. Three weeks after CO2 pneumoperitoneum, the frequency and weight of port-site metastatic tumors were determined. RESULTS: Anti-integrin antibody significantly decreased the weight of port-site metastatic tumors without hyaluronic acid (control vs anti-integrin: 8.2 +/- 7.1 vs 3.6 +/- 4.5 mg; p < 0.05) but not the frequency of port-site metastases. With hyaluronic acid, the frequency of port-site metastasis and the weight of port-site metastatic tumors were significantly decreased both by anti-integrin and by anti-CD44 antibody (control vs anti-integrin and anti-CD44; 95% and 8.5 +/- 7.2 mg vs 50% and 3.1 +/- 4.3 mg and 55% and 3.3 +/- 5.1 mg, respectively; p < 0.05). RGD peptide and FC-336 also inhibited port-site metastasis in a dose-dependent manner. CONCLUSION: Cell adhesion molecules integrin and CD44 play an important role in the development of port-site metastasis after laparoscopic cancer surgery. Intraperitoneal injection of RGD peptide or pseudo-RGD sequence peptide (FC-336) can prevent port-site metastasis.
机译:背景:腹腔镜转移是腹腔镜癌症手术中的一个持续问题。为了阐明黏附分子在港口部位转移发展中的作用,特别是在预防方面,我们进行了实验,其中使用针对细胞外基质蛋白或活性Arg-Gly-Asp(RGD)的抗体抑制港口部位转移鼠模型中CO2气腹后的多肽。方法:我们在以下情况下检查了端口转移的发展:(1)伴或不伴透明质酸和抗整合素或抗CD44抗体的CO2气腹和(2)CO2气腹和RGD肽或伪RGD序列肽(FC-336)。向BALB / c小鼠(n = 130)注射5 x 10(5)人胃癌细胞(MKN45)和抗体或肽,用CO2气腹膜处理,并腹膜内注射抗体或肽5天。在CO2气腹后三周,确定移植部位转移性肿瘤的频率和重量。结果:抗整合素抗体可显着降低无透明质酸的端口位转移性肿瘤的重量(对照组与抗整合素:8.2 +/- 7.1 vs 3.6 +/- 4.5 mg; p <0.05),但未降低端口-转移频率部位转移。使用透明质酸,抗整合素和抗CD44抗体均可显着降低端口位转移的频率和端口转移肿瘤的重量(对照vs抗整合素和抗CD44; 95%和8.5 +分别为7.2mg对50%和3.1 +/- 4.3mg和55%和3.3 +/- 5.1mg; p <0.05)。 RGD肽和FC-336也以剂量依赖的方式抑制端口位转移。结论:细胞粘附分子整联蛋白和CD44在腹腔镜癌手术后移植部位转移中起重要作用。腹膜内注射RGD肽或伪RGD序列肽(FC-336)可以预防端口位转移。

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