Tanaka K
Nihon Sanka Fujinka Gakkai Zasshi. 1984 Nov;36(11):2129-37.
Methotrexate (MTX)-resistant sublines were developed by culturing GCH-1 (human gestational choriocarcinoma cell line in vitro) in increasing concentrations of MTX. The parent GCH-1 cells cannot grow at more than 1 X 10(-7)M MTX. The cells which grew at 1 X 10(-7)M MTX and 5 X 10(-7)M MTX are designated GCH-1 : R1 and GCH-1 : RII, respectively. Mechanism of the resistance to MTX has been examined in these lines. The results are as follows: The IC50 of MTX to cells of GCH-1, GCH-1 : RI and GCH-1 : RII was 4.5 X 10(-8)M, 7.5 X 10(-7)M and 9.5 X 10(-7)M, respectively. There was no significant difference between the parent cells and the subline cells in light microscopic findings or secretion of HCG and beta-HCG. A DNA histogram of GCH-1 cells had the main peak at 3n-4n and the second peak at 5n-6n. The second peak diminished after treatment with 5 X 10(-8)M or 1 X 10(-7)M MTX. On the other hand, the DNA histogram of the subline cells had main peak at 3n-4n and second peak at 5n-6n, but the latter was not clear compared with that of the parent cells. The pattern of the DNA histogram of the subline cells didn't change even when they were cultured in MTX free media. Uptake of MTX by the sublines was reduced more than that by the parent line, indicating that affinity of MTX to its carrier component was weakend.(ABSTRACT TRUNCATED AT 250 WORDS)
通过在浓度不断增加的甲氨蝶呤(MTX)中培养GCH - 1(人妊娠滋养层癌细胞系),建立了对MTX耐药的亚系。亲代GCH - 1细胞在MTX浓度超过1×10(-7)M时无法生长。在1×10(-7)M和5×10(-7)M MTX中生长的细胞分别命名为GCH - 1 : R1和GCH - 1 : RII。已对这些细胞系中MTX耐药机制进行了研究。结果如下:MTX对GCH - 1、GCH - 1 : RI和GCH - 1 : RII细胞的IC50分别为4.5×10(-8)M、7.5×10(-7)M和9.5×10(-7)M。亲代细胞和亚系细胞在光学显微镜检查结果或人绒毛膜促性腺激素(HCG)及β - HCG分泌方面无显著差异。GCH - 1细胞的DNA直方图主峰位于3n - 4n,第二个峰位于5n - 6n。用5×10(-8)M或1×10(-7)M MTX处理后第二个峰消失。另一方面,亚系细胞的DNA直方图主峰位于3n - 4n,第二个峰位于5n - 6n,但与亲代细胞相比后者不明显。即使将亚系细胞在无MTX培养基中培养,其DNA直方图模式也未改变。亚系对MTX的摄取比亲代细胞减少得更多,表明MTX与其载体成分的亲和力减弱。(摘要截于250字)
