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利用一种罕见的源自人十二指肠神经内分泌癌的细胞系建立癌症恶病质模型并进行表征。

Development and characterization of a cancer cachexia model employing a rare human duodenal neuroendocrine carcinoma-originating cell line.

作者信息

Yanagihara Kazuyoshi, Kubo Takanori, Iino Yuki, Mihara Keichiro, Morimoto Chie, Seyama Toshio, Kuwata Takeshi, Ochiai Atsushi, Yokozaki Hiroshi

机构信息

Division of Biomarker Discovery, Exploratory Oncology and Clinical Trial Center, National Cancer Center, Chiba, Japan.

Division of Pathology, Department of Pathology, Kobe University Graduate School of Medicine, Kobe, Japan.

出版信息

Oncotarget. 2019 Mar 29;10(25):2435-2450. doi: 10.18632/oncotarget.26764.

Abstract

Cancer cachexia interferes with therapy and worsens patients' quality of life. Therefore, for a better understanding of cachexia, we aimed to establish a reliable cell line to develop a cachexia model. We recently established and characterized the TCC-NECT-2 cell line, derived from a Japanese patient with poorly differentiated neuroendocrine carcinoma of the duodenum (D-NEC). Subcutaneous xenograft of TCC-NECT-2 cells in mice resulted in tumor formation, angiogenesis, and 20% incidence of body weight (BW)-loss. Subsequently, we isolated a potent cachexia-inducing subline using stepwise selection and designated as AkuNEC. Orthotopic and s.c. implantation of AkuNEC cells into mice led to diminished BW, anorexia, skeletal muscle atrophy, adipose tissue loss, and decreased locomotor activity at 100% incidence. Additionally, orthotopic implantation of AkuNEC cells resulted in metastasis and angiogenesis. Serum IL-8 overproduction was observed, and levels were positively correlated with BW-loss and reduced adipose tissue and muscle volumes in tumor-bearing mice. However, shRNA knockdown of the IL-8 gene did not suppress tumor growth and cachexia in the AkuNEC model, indicating that IL-8 is not directly involved in cachexia induction. In conclusion, AkuNEC cells may serve as a useful model to study cachexia and D-NEC.

摘要

癌症恶病质会干扰治疗并恶化患者的生活质量。因此,为了更好地理解恶病质,我们旨在建立一个可靠的细胞系来构建恶病质模型。我们最近建立并鉴定了TCC-NECT-2细胞系,该细胞系源自一名患有十二指肠低分化神经内分泌癌(D-NEC)的日本患者。将TCC-NECT-2细胞皮下异种移植到小鼠体内导致肿瘤形成、血管生成以及20%的体重减轻发生率。随后,我们通过逐步筛选分离出一个强效恶病质诱导亚系,并将其命名为AkuNEC。将AkuNEC细胞原位和皮下植入小鼠体内导致体重下降、厌食、骨骼肌萎缩、脂肪组织丢失以及运动活性降低,发生率达100%。此外,AkuNEC细胞原位植入导致转移和血管生成。观察到血清IL-8过度产生,其水平与荷瘤小鼠的体重减轻以及脂肪组织和肌肉体积减少呈正相关。然而,在AkuNEC模型中,IL-8基因的短发夹RNA敲低并未抑制肿瘤生长和恶病质,这表明IL-8不直接参与恶病质诱导。总之,AkuNEC细胞可能是研究恶病质和D-NEC的有用模型。

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