[Alteration of metastatic potential of ovarian cancer in clinical course].

Nihon Sanka Fujinka Gakkai zasshi Pub Date : 1996-08-01
T Kamura
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Abstract

Ovarian cancer is one of the significant and deadly disease. Since 1980 when cisplatin was introduced in the chemotherapy, about 30% of the patients with advanced disease have achieved 5-year survival. However, remaining patients have had progressive disease or recurrence after achieving NED. Forty-seven% of recurrent disease was discovered as distant metastasis, while at initial therapy. In the recurrent disease, distantly metastatic lesions were encountered more frequently than those in primary disease. In the recurrent tumor, expression of immunohistochemical markers of malignancy, such as p53 protein and CD44v6 antigen were increased. These clinical data suggest that recurrent ovarian cancer which are exposed to anticancer agents attain increased metastatic potential. In order to assure that anticancer agent contribute to this increment, an experimental system using two human ovarian cancer cell lines (HRA, KF) and nude mice in which cancer cells were exposed to cisplatin in vivo was introduced. Cancer cells exposed to cisplatin in vivo (treated cells) made spontaneously more metastatic nodules in the mouse lung than those exposed to PBS (untreated cells). This result suggest that cisplatin induce the increase of metastatic potential of cancer cells in vivo. Treated cells showed higher invasiveness compared with untreated cells when inoculated in the footpad. Three major factors which were generally proposed to be necessary for cancer cell to give rise to invasion, such as attachment to extracellular matrix, production of proteolytic enzyme, and cellular mobility. For all of these factors, treated cells were superior to untreated cells. These results obtained suggests that cisplatin could increase the metastatic potential of cancer by enhancing potential of invasion. To investigate the mechanism of this phenomenon from the standpoint of genetic mutation, clonal analysis of experimental cancer in vivo was performed using southern blot method. Cancer cells before inoculation to the mice consisted of multiple clones. In 5 week after inoculation, tumor was wholely occupied by only one clone which showed one band on the lane. At this point cisplatin were administered. In 6 week, new single clone appeared with different band pattern from that of the clone at the administration of cisplatin. Furthermore, the cisplatin-induced new clone metastasized to the lung, while no metastasis was observed in the mouse with PBS-treated tumor during the same period. These data suggest that increased metastatic potential after cisplatin treatment is due not to selection but to creation of highly metastatic clone caused by potential of genetic mutation of cisplatin. In conclusion, chemotherapeutic agent has a potential to create highly malignant cancer cells as well as a potential to kill cancer cells.

【卵巢癌临床病程中转移潜能的改变】。
卵巢癌是严重而致命的疾病之一。自1980年引入顺铂化疗以来,晚期患者的5年生存率约为30%。然而,其余患者在实现NED后病情进展或复发。47%的复发性疾病在最初治疗时被发现为远处转移。在复发性疾病中,远处转移性病变比原发疾病更常见。复发肿瘤中p53蛋白、CD44v6抗原等恶性肿瘤免疫组织化学标志物表达升高。这些临床数据表明,暴露于抗癌药物的复发性卵巢癌有更高的转移潜力。为了确保抗癌药物有助于这种增加,引入了一种实验系统,使用两种人卵巢癌细胞系(HRA, KF)和裸鼠,其中癌细胞在体内暴露于顺铂。在体内暴露于顺铂的癌细胞(处理过的细胞)比暴露于PBS(未处理的细胞)的癌细胞在小鼠肺中自发产生更多的转移性结节。提示顺铂在体内诱导癌细胞转移潜能增加。与未处理细胞相比,处理细胞在足垫中接种时表现出更高的侵袭性。一般认为癌细胞发生侵袭需要三个主要因素,即与细胞外基质的附着、蛋白水解酶的产生和细胞的移动性。对于所有这些因素,处理的细胞优于未处理的细胞。这些结果提示顺铂可能通过增强肿瘤侵袭的潜力而增加肿瘤的转移潜力。为了从基因突变的角度探讨这一现象的发生机制,我们采用southern blot方法对实验肿瘤进行了体内克隆分析。小鼠接种前的癌细胞由多个克隆组成。接种5周后,肿瘤仅被1个无性系完全占据,在细胞壁上显示1条条带。此时给予顺铂。6周后出现新的单克隆,其条带模式与顺铂组不同。此外,顺铂诱导的新克隆转移到肺部,而pbs治疗的小鼠在同一时期未观察到转移。这些数据表明,顺铂治疗后转移潜力的增加不是由于选择,而是由于顺铂基因突变的潜力引起的高转移克隆的产生。综上所述,化疗药物有可能产生高度恶性的癌细胞,也有可能杀死癌细胞。
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