在小鼠模型中,C9orf10/Ossa调节已建立的肺腺癌细胞亚系H322L-BO4的骨转移。

IF 1.3 4区 生物学 Q4 CELL BIOLOGY
Genes to Cells Pub Date : 2024-02-10 DOI:10.1111/gtc.13103
Takamasa Uekita, Reiko Yagi, Tohru Ichimura, Ryuichi Sakai
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引用次数: 0

摘要

肺癌经常转移到骨骼。迫切需要一种体内模型来确定预防和治疗肺癌骨转移的潜在治疗靶点。我们建立了一个肺腺癌细胞亚系(H322L-BO4),它能特异性地转移到腿骨和肾上腺。这是通过反复从小鼠腿骨中分离转移细胞实现的。这些细胞被注入裸鼠的心内。与原始细胞(H322L)相比,接受 H322L-BO4 细胞的小鼠存活时间更长。与 H322L 细胞相比,H322L-BO4 细胞在与转移潜能相关的体外一般特性(如细胞生长、迁移和侵袭)方面没有表现出明显的变化。然而,在H322L-BO4细胞中,9号染色体开放阅读框10/氧化应激相关Src激活因子(C9orf10/Ossa)的磷酸化增加了。这一结果证实了通过C9orf10/Ossa介导的Src家族酪氨酸激酶活化增加的锚定独立性。通过 shRNA 减少 C9orf10/Ossa 可减少细胞向腿骨的转移,并延长小鼠的存活时间。这些发现表明,H322L-BO4细胞可用于评估候选治疗靶点对骨转移肺癌细胞的作用。此外,C9orf10/Ossa可能是治疗骨转移肺癌的有效靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

C9orf10/Ossa regulates the bone metastasis of established lung adenocarcinoma cell subline H322L-BO4 in a mouse model

C9orf10/Ossa regulates the bone metastasis of established lung adenocarcinoma cell subline H322L-BO4 in a mouse model

C9orf10/Ossa regulates the bone metastasis of established lung adenocarcinoma cell subline H322L-BO4 in a mouse model

Lung cancer frequently metastasizes to the bones. An in vivo model is urgently required to identify potential therapeutic targets for the prevention and treatment of lung cancer with bone metastasis. We established a lung adenocarcinoma cell subline (H322L-BO4) that specifically showed metastasis to the leg bones and adrenal glands. This was achieved by repeated isolation of metastatic cells from the leg bones of mice. The cells were intracardially injected into nude mice. Survival was prolonged for mice that received H322L-BO4 cells versus original cells (H322L). H322L-BO4 cells did not exhibit obvious changes in general in vitro properties associated with the metastatic potential (e.g., cell growth, migration, and invasion) compared with H322L cells. However, the phosphorylation of chromosome 9 open reading frame 10/oxidative stress-associated Src activator (C9orf10/Ossa) was increased in H322L-BO4 cells. This result confirmed the increased anchorage independence through C9orf10/Ossa-mediated activation of Src family tyrosine kinase. Reduction of C9orf10/Ossa by shRNA reduced cells' metastasis to the leg bone and prolonged survival in mice. These findings indicate that H322L-BO4 cells can be used to evaluate the effect of candidate therapeutic targets against bone metastatic lung cancer cells. Moreover, C9orf10/Ossa may be a useful target for treatment of lung cancer with bone metastasis.

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来源期刊
Genes to Cells
Genes to Cells 生物-细胞生物学
CiteScore
3.40
自引率
0.00%
发文量
71
审稿时长
3 months
期刊介绍: Genes to Cells provides an international forum for the publication of papers describing important aspects of molecular and cellular biology. The journal aims to present papers that provide conceptual advance in the relevant field. Particular emphasis will be placed on work aimed at understanding the basic mechanisms underlying biological events.
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