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胃癌和肝癌的临床前疗效测试。

Preclinical efficacy testing for stomach and liver cancers.

机构信息

Biomolecular Function Research Branch, National Cancer Center, Goyang, Korea. ; Department of Veterinary Pathology, College of Veterinary Medicine, Seoul National University, Seoul, Korea.

National OncoVenture, Goyang, Korea.

出版信息

Cancer Res Treat. 2014 Apr;46(2):186-93. doi: 10.4143/crt.2014.46.2.186. Epub 2014 Apr 22.

Abstract

PURPOSE

Hollow fiber assays offer an early in vivo method of anticancer drug screening. The assays have been optimized for human cancers originating from the lung, breast, colon, ovary, and brain, but not from the stomach and liver. The current study focused on optimization of hollow fiber assays for gastric and hepatocellular carcinoma cell lines.

MATERIALS AND METHODS

Gastric (SNU-16, SNU-484, SNU-668) and hepatocellular (HepG2, SK-Hep-1, Hep3B) carcinoma cell lines in hollow fibers were transplanted subcutaneously and intraperitoneally into mice, which were subsequently treated with a standard anticancer agent, paclitaxel. The hollow fiber activity of paclitaxel in each cell line was compared with the xenograft activity.

RESULTS

Using optimized inoculation densities and schedules, treatment with paclitaxel was effective in gastric carcinoma cell lines, SNU-16 and SNU-484, but not in SNU-668. In the hollow fiber assays, paclitaxel was effective in hepatocellular carcinoma cell lines, HepG2 and SK-Hep-1, but not in Hep3B. Consistent with the results of the hollow fiber assay, SNU-16 and SNU-484, but not SNU-668, showed tumor regression, and HepG2 and SK-Hep-1, but not Hep3B, showed effective tumor responses following treatment with paclitaxel in xenograft models. When EW7197, a novel compound, and flavopiridol were tested in SNU-16 cells under optimized conditions, the hollow fiber activity showed good correlation with the xenograft activity of each compound.

CONCLUSION

Our protocols may be useful for screening candidate small molecules that may exhibit activity against stomach and liver cancers, both of which are common in Korea.

摘要

目的

中空纤维分析为抗癌药物筛选提供了一种早期的体内方法。该分析已针对源自肺、乳腺、结肠、卵巢和脑的人类癌症进行了优化,但尚未针对胃和肝癌进行优化。本研究专注于优化用于胃和肝细胞癌细胞系的中空纤维分析。

材料和方法

将胃(SNU-16、SNU-484、SNU-668)和肝细胞(HepG2、SK-Hep-1、Hep3B)癌细胞系在中空纤维中皮下和腹腔内移植到小鼠中,随后用标准抗癌药物紫杉醇进行治疗。比较了每个细胞系中紫杉醇的中空纤维活性与异种移植物活性。

结果

使用优化的接种密度和方案,紫杉醇对胃癌细胞系 SNU-16 和 SNU-484 有效,但对 SNU-668 无效。在中空纤维分析中,紫杉醇对肝细胞癌细胞系 HepG2 和 SK-Hep-1 有效,但对 Hep3B 无效。与中空纤维分析的结果一致,紫杉醇治疗后 SNU-16 和 SNU-484 而非 SNU-668 出现肿瘤消退,并且在异种移植模型中,紫杉醇治疗后 HepG2 和 SK-Hep-1 而非 Hep3B 出现有效的肿瘤反应。当在优化条件下在 SNU-16 细胞中测试新型化合物 EW7197 和 flavopiridol 时,中空纤维活性与每个化合物的异种移植物活性具有良好的相关性。

结论

我们的方案可能有助于筛选可能对韩国常见的胃和肝癌有活性的候选小分子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b208/4022828/d8ee941a96fd/crt-46-186-g001.jpg

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