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口服1α-羟基维生素D3可抑制小鼠骨肉瘤模型的肿瘤生长和转移。

Oral administration of 1 alpha hydroxyvitamin D3 inhibits tumor growth and metastasis of a murine osteosarcoma model.

作者信息

Hara K, Kusuzaki K, Takeshita H, Kuzuhara A, Tsuji Y, Ashihara T, Hirasawa Y

机构信息

Department of Orthopaedic Surgery, Kyoto Prefectural University of Medicine, Kyoto 602, Japan.

出版信息

Anticancer Res. 2001 Jan-Feb;21(1A):321-4.

PMID:11299756
Abstract

We studied the effect of oral administration of 1 alpha hydroxyvitamin D3 (1-D3) on the growth and metastatic ability of Dunn murine osteosarcoma model. A solution of 1-D3 or vehicle alone was administered daily for 2 weeks to tumor-bearing mice using an esophageal tube and tumor size was serially monitored. In 1-D3-treated mice, the growth of Dunn osteosarcoma was significantly suppressed in a dose-dependent manner. Histologically, tumor cells in the control mice proliferated in marginal regions of the tumor with wide central necrosis, whereas in the 1-D3-treated mice, tumor cells were distributed as scattered islands among extensive necrotic tissue. The mean tumor necrosis area was 55.7% in the control tumors and 94.6% in 1-D3-treated tumors (p < 0.001). There were no substantial differences in the cytofluorometric cell cycle distribution or the histological mitotic index between control and 1-D3-treated tumors. When 1-D3 was administered to mice from 2 days before to 2 weeks after transplantation of the tumor, there were significantly fewer metastatic foci in the lungs in 1-D3-treated mice than in control mice. We also tested the effect of coadministration of 1-D3 and doxorubicin on the growth of Dunn osteosarcoma and found that these two drugs act additively to suppress tumor growth. These results indicated that 1-D3 given orally inhibits tumor growth and metastases in a Dunn osteosarcoma model. Although the mechanism remains unknown, oral administration of 1-D3 might be promising as a new method of treating human osteosarcoma.

摘要

我们研究了口服1α-羟基维生素D3(1-D3)对Dunn小鼠骨肉瘤模型生长和转移能力的影响。使用食管管每天给荷瘤小鼠灌胃1-D3溶液或单独的赋形剂,持续2周,并连续监测肿瘤大小。在1-D3处理的小鼠中,Dunn骨肉瘤的生长以剂量依赖性方式显著受到抑制。组织学上,对照小鼠的肿瘤细胞在肿瘤边缘区域增殖,中央有大片坏死,而在1-D3处理的小鼠中,肿瘤细胞以散在岛屿状分布于广泛的坏死组织中。对照肿瘤的平均肿瘤坏死面积为55.7%,1-D3处理肿瘤的平均肿瘤坏死面积为94.6%(p<0.001)。对照肿瘤和1-D3处理肿瘤之间的细胞荧光计细胞周期分布或组织学有丝分裂指数没有实质性差异。当在肿瘤移植前2天至移植后2周给小鼠施用1-D3时,1-D3处理的小鼠肺中的转移灶明显少于对照小鼠。我们还测试了1-D3与阿霉素联合给药对Dunn骨肉瘤生长的影响,发现这两种药物联合作用可抑制肿瘤生长。这些结果表明,口服1-D3可抑制Dunn骨肉瘤模型中的肿瘤生长和转移。尽管其机制尚不清楚,但口服1-D3可能是一种有前景的治疗人类骨肉瘤的新方法。

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