具有自发性转移的犬骨肉瘤临床相关的小鼠模型。
A clinically relevant mouse model of canine osteosarcoma with spontaneous metastasis.
机构信息
Department of Veterinary Biosciences, College of Veterinary Medicine, The Ohio State University, 1925 Coffey Rd., Columbus, OH 43210, USA.
出版信息
In Vivo. 2013 Sep-Oct;27(5):599-603.
Abstract
BACKGROUND/AIM: Many patients with osteosarcoma (OS) will succumb to distant metastasis, often involving the lungs. Effective therapies for treating lung metastases depend on the availability of a clinically relevant pre-clinical model.
MATERIALS AND METHODS
Mice were surgically implanted with OS tumor fragments. The time course of primary tumor growth and subsequent spread to the lung were determined.
RESULTS
Following development of a lytic and proliferative primary bone lesion, tumor metastasized to the lung in the majority of mice. There was no evidence of tumor at three weeks, but 10 out of 11 mice ultimately developed secondary OS in the lung within 12 weeks.
CONCLUSION
Implantation of OS tumor fragments leads to the development of primary bone tumors and secondary lung metastases, recapitulating the clinical behavior of OS. This model offers an advantage over cell suspension injection models by precluding initial seeding of the lung with tumor cells.
摘要
背景/目的:许多骨肉瘤(OS)患者将死于远处转移,通常涉及肺部。治疗肺转移的有效疗法取决于是否存在临床相关的临床前模型。
材料和方法
通过手术将 OS 肿瘤碎片植入小鼠体内。确定原发性肿瘤生长和随后向肺部扩散的时间过程。
结果
在形成溶骨性和增殖性原发性骨病变后,肿瘤在大多数小鼠中转移到肺部。在第三周时没有肿瘤的证据,但在 12 周内,11 只小鼠中有 10 只最终在肺部发展为继发性骨肉瘤。
结论
骨肉瘤肿瘤碎片的植入导致原发性骨肿瘤和继发性肺转移的发展,再现了骨肉瘤的临床行为。与细胞悬浮注射模型相比,该模型通过排除肿瘤细胞最初在肺部的播种具有优势。
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