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首页> 外文期刊>Therapeutic delivery >Marked antitumor effect of NK012, a SN-38-incorporating micelle formulation, in a newly developed mouse model of liver metastasis resulting from gastric cancer
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Marked antitumor effect of NK012, a SN-38-incorporating micelle formulation, in a newly developed mouse model of liver metastasis resulting from gastric cancer

机译:NK012(一种含SN-38的胶束制剂)在新开发的由胃癌引起的肝转移的小鼠模型中具有明显的抗肿瘤作用

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Background: Gastric cancer with liver metastasis (LM) is associated with poor prognosis due to rapid progression. It is, therefore, important to develop a quantitative and highly reproducible animal model of LM using human gastric cancer cells. Methods: Cells of a human gastric cancer cell line, HSC-57, were injected into the portal vein to produce LMs. Cells from some of these metastatic foci were expanded in vitro and subsequently implanted into the portal veins of mice. This procedure was repeated nine times. The antitumor effects of CPT-11 and NK012 were compared using the LM model. Results: The potent metastatic clone 57L9 was obtained. NK012 exerted a stronger antitumor effect than CPT-11 against 57L9 cells integrated with the luciferase gene (57L9Luc). The survival rates on day 131 in the 57L9Luc mouse model were 100% and 0% for the NK012 and CPT-11 groups, respectively. Conclusion: This 57L9Luc LM model was found to be useful for monitoring the responses to NK012 and CPT-11.
机译:背景:具有肝转移(LM)的胃癌因进展迅速而预后不良。因此,重要的是使用人胃癌细胞建立定量且高度可重复的LM动物模型。方法:将人胃癌细胞系HSC-57的细胞注入门静脉以产生LM。来自其中一些转移灶的细胞在体外扩增,随后植入小鼠的门静脉。将该程序重复九次。使用LM模型比较了CPT-11和NK012的抗肿瘤作用。结果:获得了有效的转移克隆57L9。 NK012对与萤光素酶基因整合的57L9细胞(57L9Luc)的抗肿瘤作用比CPT-11强。 NK012和CPT-11组的57L9Luc小鼠模型在第131天的存活率分别为100%和0%。结论:发现该57L9Luc LM模型可用于监测对NK012和CPT-11的响应。

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