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异黄酮对携带人胃癌的新建立恶病质小鼠模型中肿瘤生长和恶病质的抑制作用。

Inhibitory effects of isoflavones on tumor growth and cachexia in newly established cachectic mouse models carrying human stomach cancers.

机构信息

Division of Genetics, National Cancer Center Research Institute, Tokyo, Japan.

出版信息

Nutr Cancer. 2013;65(4):578-89. doi: 10.1080/01635581.2013.776089.

Abstract

Cachexia, a negative prognostic factor, worsens a patient's quality of life. We established 2 novel cachexia models with the human stomach cancer cell line MKN-45, which was subcloned to produce potent cachexia-inducing cells by repeating the xenografts in immune-deficient mice. After subsequent xenografts, we isolated potent cachexia-inducing cells (MKN45cl85 and 85As2mLuc). Xenografts of MKN45cl85 cells in mice led to substantial weight loss and reduced adipose tissue and musculature volumes, whereas xenografts of 85As2mLuc cells resulted in highly metastatic and cachectic mice. Surgical removal of tumor tissues helped the mice regain body-weight in both mouse models. In vitro studies using these cells showed that isoflavones reduced their proliferation, implying that the isoflavones possess antiproliferative effects of these cancer cell lines. Isoflavone treatment on the models induced tumor cytostasis, attenuation of cachexia, and prolonged survival whereas discontinuation of the treatment resulted in progressive tumor growth and weight loss. The inhibitory effects of tumor growth and weight loss by isoflavones were graded as soy isoflavone aglycone AglyMax > daidzein > genistein. These results demonstrated that the 2 novel cachectic mouse models appear useful for analyzing the mechanism of cancer cachexia and monitoring the efficacy of anticachectic agents.

摘要

恶病质是一种负面的预后因素,会降低患者的生活质量。我们建立了 2 种新型恶病质模型,使用人胃癌细胞系 MKN-45,通过在免疫缺陷小鼠中重复异种移植,使该细胞系亚克隆产生具有强烈恶病质诱导作用的细胞。随后进行异种移植后,我们分离出具有强烈恶病质诱导作用的细胞(MKN45cl85 和 85As2mLuc)。MKN45cl85 细胞的异种移植导致小鼠体重显著下降,脂肪组织和肌肉体积减少,而 85As2mLuc 细胞的异种移植则导致高度转移性和恶病质的小鼠。肿瘤组织的手术切除有助于这两种模型中的小鼠恢复体重。使用这些细胞进行的体外研究表明,异黄酮可降低其增殖能力,这意味着异黄酮对这些癌细胞系具有抗增殖作用。异黄酮治疗可诱导肿瘤细胞静止、恶病质减轻和延长生存时间,而停止治疗则会导致肿瘤生长和体重下降的进行性进展。异黄酮对肿瘤生长和体重减轻的抑制作用呈分级效应,依次为大豆异黄酮苷元 AglyMax > 大豆苷元 > 染料木黄酮。这些结果表明,这 2 种新型恶病质小鼠模型似乎可用于分析癌症恶病质的机制,并监测抗恶病质药物的疗效。

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