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在皮下 Dunn/LM8 骨肉瘤小鼠模型中,LacZ 转基因的表达可用于识别微转移。

LacZ transgene expression in the subcutaneous Dunn/LM8 osteosarcoma mouse model allows for the identification of micrometastasis.

机构信息

Department of Orthopedics, Balgrist University Hospital, University of Zürich, Zürich, Switzerland.

出版信息

J Orthop Res. 2011 Jun;29(6):938-46. doi: 10.1002/jor.21304. Epub 2011 Jan 31.

Abstract

More effective treatment of patients with metastasizing osteosarcoma (OS) with a mean 5-year survival rate of <20% requires more detailed knowledge on the complex mechanisms of metastasis for the design of new drugs, which selectively target metastasizing cells. Moreover, novel diagnostic imaging technology for early detection of metastases is needed. Mouse models, which reproduce human metastasizing OS and allow visualization of single metastatic cells are instrumental for preclinical testing of new pharmaceuticals and diagnostic instruments. Here, the low metastatic Dunn cell line and its highly metastatic LM8 subline, both equipped with a constitutively expressed lacZ gene, were used to improve the well-established OS models in syngeneic C3H mice to achieve ex vivo visualization of single metastatic cells in affected organs by X-gal staining. These models, combined with a technique for in situ high quality lung tissue-maintaining perfusion revealed, as a novel finding, single metastasizing Dunn cells in lung and liver. Importantly, constitutive lacZ gene expression did not affect in vitro and in vivo tumorigenic and metastatic properties of Dunn and LM8 cells. Thus, these improved Dunn and LM8 OS mouse models will in the future serve as a benchmark for the development of new metastasis-targeting drugs and metastasis-imaging technology.

摘要

为了提高转移性骨肉瘤(OS)患者的治疗效果,患者的 5 年生存率均值需达到<20%,这需要深入了解转移的复杂机制,从而设计出能够选择性靶向转移细胞的新药。此外,还需要新的诊断成像技术来早期发现转移灶。能够重现人类转移性 OS 并可对单个转移细胞进行可视化的小鼠模型,对于新药物和诊断仪器的临床前测试具有重要意义。本研究使用低转移性 Dunn 细胞系及其高转移性 LM8 亚系,均携带组成型表达的 lacZ 基因,对已建立的 C3H 同基因小鼠中 OS 模型进行了改良,通过 X-gal 染色实现了对受累器官中单个转移细胞的体外可视化。这些模型结合原位高质量肺组织维持灌注技术,首次揭示了肺和肝中的单个转移性 Dunn 细胞。重要的是,组成型 lacZ 基因表达并未影响 Dunn 和 LM8 细胞的体外和体内致瘤和转移特性。因此,这些改良的 Dunn 和 LM8 OS 小鼠模型将成为未来开发新的转移性靶向药物和转移性成像技术的基准。

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