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首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >Inhibition by interleukin 18 of osteolytic bone metastasis by human breast cancer cells.
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Inhibition by interleukin 18 of osteolytic bone metastasis by human breast cancer cells.

机译:白细胞介素18对人乳腺癌细胞的溶骨性骨转移的抑制作用。

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摘要

Effects of interleukin (IL)-18 on experimental bone metastasis of human breast cancer cells, MDA-231 cells, in nude mice were investigated. In addition, effects of IL-18 on subcutaneous growth of MDA-231 cells were examined. Bone metastasis was produced by an intracardiac injection of MDA-231 cells. Twenty eight days after the cell injection, severe osteolytic bone metastasis was examined by X-ray radiography, and both non-osteolytic and osteolytic bone metastases were examined microscopically. IL-18 (1 microgram/mouse) was injected intraperitoneally according to protocols A and B. In protocol A, IL-18 was injected daily from day 7 after an intracardiac or subcutaneous injection of cells, and in protocol B, it was injected daily for 7 days each before and after the cell injection. In protocol A, IL-18 injections significantly suppressed both the incidence of osteolytic bone metastasis detected by X-ray radiography (about 80% vs. about 20% for the control group vs. the treatment group) and the number of its foci/mouse (1.6 vs. 1 for the control group vs. the treatment group). However, they did not cause significant effects on either the incidence of bone metastasis detected microscopically or the number of its foci/mouse. In protocol B, IL-18 injections caused no significant effects on either the incidence of osteolytic bone metastasis detected by X-ray radiography or the number of its foci/mouse. They caused no significant effects on the incidence of bone metastasis detected microscopically, but significantly decreased the number of its foci/mouse (about 2.0 vs. about 1 for the control group vs. the treatment group). In both protocols A and B, IL-18 injections produced no significant effect on the tumor take and subsequent growth of tumors after a subcutaneous injection of the cancer cells. Since in protocol A, IL-18 appears to have exerted its action after establishment of metastasis by cancer cells to the bone marrow, the effects of IL-18 found in Protocol A indicate that IL-18 inhibited osteolytic growth at bone metastatic sites of breast cancers. On the other hand, since in protocol B IL-18 is likely to have functioned around the time when lodging of cancer cells and early development of metastasis occur in the bone marrow, the effects of IL-18 found in Protocol B indicate that the cytokine also suppresses an early stage of bone metastasis of breast cancers, although, this effect was less apparent than the effect on osteolytic growth. Therefore, IL-18 may be useful for suppression of osteolytic bone metastasis which is a serious problem in patients of advanced breast cancers.
机译:研究了白介素(IL)-18对裸鼠人乳腺癌细胞MDA-231细胞实验性骨转移的影响。另外,检查了IL-18对MDA-231细胞的皮下生长的影响。通过心脏内注射MDA-231细胞产生骨转移。细胞注射后第二十八天,通过X射线照相检查了严重的溶骨性骨转移,并且在显微镜下检查了非溶骨性和溶骨性骨转移。按照方案A和B腹膜内注射IL-18(1微克/小鼠)。在方案A中,从心脏内或皮下注射细胞后的第7天起每天注射IL-18,在方案B中,每天注射IL-18细胞注射前后各7天。在方案A中,IL-18注射显着抑制了X射线照相术检测到的溶骨性骨转移的发生率(对照组与治疗组分别为80%和20%)和其病灶/小鼠数目(对照组与治疗组分别为1.6比1)。但是,它们对显微镜下检测到的骨转移的发生率或病灶/小鼠的数量均无明显影响。在方案B中,IL-18注射液对X射线射线照相术检测到的溶骨性骨转移的发生率或其病灶/小鼠数目均无明显影响。它们对显微镜下检测到的骨转移的发生率没有显着影响,但显着减少了其灶/小鼠的数量(对照组与治疗组分别为2.0与1左右)。在方案A和方案B中,在皮下注射癌细胞后,IL-18注射液对肿瘤的摄取和随后的肿瘤生长均无明显影响。由于在方案A中,IL-18似乎在癌细胞转移到骨髓后开始发挥作用,因此在方案A中发现的IL-18的作用表明IL-18抑制了乳腺骨转移部位的溶骨性生长。癌症。另一方面,由于在协议B中IL-18可能在骨髓中发生癌细胞倒伏和转移的早期发展时起作用,因此在协议B中发现的IL-18的作用表明细胞因子尽管这种作用不如对溶骨性生长的作用明显,但它也能抑制乳腺癌的骨转移的早期阶段。因此,IL-18可用于抑制溶骨性骨转移,这在晚期乳腺癌患者中是一个严重的问题。

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