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连接蛋白基因对HeLa细胞的负生长调控:连接蛋白物种特异性。

Negative growth control of HeLa cells by connexin genes: connexin species specificity.

作者信息

Mesnil M, Krutovskikh V, Piccoli C, Elfgang C, Traub O, Willecke K, Yamasaki H

机构信息

International Agency for Research on Cancer, Lyon, France.

出版信息

Cancer Res. 1995 Feb 1;55(3):629-39.

PMID:7834634
Abstract

In order to examine whether different connexin gene species exert different degrees of tumor-suppressing activity, we characterized growth characteristics of a gap junction-deficient human cancer cell line, HeLa cells, before and after transfection with cDNA for three different connexins, connexin (cx) 26, cx 40, and cx 43. All transfected cell lines (3 clones transfected with the cx 26 gene, 2 clones with cx 40, and 1 with cx 43) showed establishment of gap junctional intercellular communication (GJIC). Two of the cx 26-transfected clones showed significantly slower growth compared with the parental HeLa cells. When transfectants were grown in soft agar, the three cx 26-transfected clones grew much less than the other transfectants and parent HeLa cells. When injected into nude mice, the two cx 26 clones which exhibited the highest amount of cx 26 transcript induced almost no tumors, whereas other transfectants, including the cx 26 clone which exhibited the lowest amount of cx 26 transcript, were tumorigenic. Among transfectants of various connexin genes, there was no good inverse correlation between their GJIC and tumorigenicity. GJIC levels were significantly higher in tumors induced in nude mice by clone cx 26 A and E transfectants. These results suggest that all of the connexin genes examined could induce recovery of GJIC of HeLa cells, but only the cx 26 gene exerts strong negative growth control on HeLa cells; thus, this connexin gene may have different functions from other connexin genes.

摘要

为了研究不同的连接蛋白基因是否具有不同程度的肿瘤抑制活性,我们对一种缺乏缝隙连接的人类癌细胞系——HeLa细胞,在转染三种不同连接蛋白(连接蛋白(cx)26、cx40和cx43)的cDNA前后的生长特性进行了表征。所有转染的细胞系(3个克隆转染cx26基因,2个克隆转染cx40,1个克隆转染cx43)均显示建立了缝隙连接细胞间通讯(GJIC)。与亲代HeLa细胞相比,两个转染cx26的克隆生长明显较慢。当转染细胞在软琼脂中生长时,三个转染cx26的克隆生长远低于其他转染细胞和亲代HeLa细胞。当注射到裸鼠体内时,两个cx26转录本含量最高的cx26克隆几乎不诱导肿瘤形成,而其他转染细胞,包括cx26转录本含量最低的cx26克隆,具有致瘤性。在各种连接蛋白基因的转染细胞中,它们的GJIC与致瘤性之间没有良好的负相关关系。克隆cx26 A和E转染细胞在裸鼠中诱导的肿瘤中GJIC水平明显更高。这些结果表明,所检测的所有连接蛋白基因都能诱导HeLa细胞恢复GJIC,但只有cx26基因对HeLa细胞具有强大的负生长控制作用;因此,这种连接蛋白基因可能具有与其他连接蛋白基因不同的功能。

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