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维生素D3制剂对小鼠肾细胞癌肿瘤生长和血管生成的抑制作用

Inhibition of tumor growth and angiogenesis by vitamin D3 agents in murine renal cell carcinoma.

作者信息

Fujioka T, Hasegawa M, Ishikura K, Matsushita Y, Sato M, Tanji S

机构信息

Department of Urology, Iwate Medical University School of Medicine, Morioka, Japan.

出版信息

J Urol. 1998 Jul;160(1):247-51.

PMID:9628658
Abstract

PURPOSE

To investigate the effect of active vitamin D3(VD) agents on tumor growth and metastasis.

MATERIALS AND METHODS

BALB/c mice were inoculated with murine renal cancer Renca and graded doses of 1,25-dehydrovitamin D3 or 1- hydrovitamin D3 were given intraperitoneally every other day beginning on day 1, 3, or 7 and ending on day 9, 11, or 15. Direct cytocidal activity and angiogenic activity were evaluated by 48-hour MTT assay and by the colorimetric method, respectively.

RESULTS

Both VD agents inhibited tumor growth and prolonged the life span of Renca-bearing mice in a dose-dependent manner and both suppressed tumor growth in athymic mice and euthymic mice with eliminated NK activity. Marginal body-weight loss without appreciable hypercalcemia was observed in mice given VD agents. When treatment was delayed on day 7, the VD agents failed to inhibit tumor growth. The MTT assay showed no direct cytotoxicity of VD agents on Renca. Tumor angiogenesis was inhibited to 46 to 30% of the control level by VD agents. Furthermore, VD agents reduced pulmonary and hepatic foci in the metastatic models.

CONCLUSIONS

These results suggest that VD agents may be effective as a treatment for renal cell carcinoma, especially when micrometastases are involved.

摘要

目的

研究活性维生素D3(VD)制剂对肿瘤生长和转移的影响。

材料与方法

将小鼠肾癌Renca接种于BALB/c小鼠,从第1、3或7天开始每隔一天腹腔注射分级剂量的1,25 - 二羟维生素D3或1 - 羟维生素D3,至第9、11或15天结束。分别通过48小时MTT法和比色法评估直接杀细胞活性和血管生成活性。

结果

两种VD制剂均以剂量依赖方式抑制肿瘤生长并延长荷Renca小鼠的生存期,且在无胸腺小鼠和NK活性消除的有胸腺小鼠中均抑制肿瘤生长。给予VD制剂的小鼠出现轻微体重减轻但无明显高钙血症。当在第7天延迟治疗时,VD制剂未能抑制肿瘤生长。MTT试验显示VD制剂对Renca无直接细胞毒性。VD制剂将肿瘤血管生成抑制至对照水平的46%至30%。此外,VD制剂减少了转移模型中的肺和肝转移灶。

结论

这些结果表明,VD制剂可能作为肾细胞癌的一种有效治疗方法,尤其是在涉及微转移时。

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