Ruch R J, Cesen-Cummings K, Malkinson A M
Department of Pathology, Medical College of Ohio, Toledo, USA.
Exp Lung Res. 1998 Jul-Aug;24(4):523-39. doi: 10.3109/01902149809087384.
Reduced gap junctional intercellular communication (GJIC) has been noted in many types of neoplastic cells and may contribute to the neoplastic phenotype. This study assessed GJIC (by fluorescent dye-coupling) and gap junction protein (connexin) expression in mouse and human lung carcinoma cell lines and investigated whether reduced GJIC was involved in their neoplastic phenotype. Dye-coupling and connexin43 (Cx43) expression were much lower in most of the carcinoma lines (16 of 22) compared to nontransformed lung epithelial cells. Other connexins were not detected. A poorly communicating mouse lung carcinoma cell line (E9) was transfected with Cx43 or transduced with Cx32 and several stable clones were isolated that had 2- to 4-fold increased dye coupling. When evaluated for growth in vitro, the population doubling times were increased and the saturation densities were decreased in the clones. When assessed for tumorigenicity, the parental E9 cells formed tumors with a 100% incidence (6/6 mice), whereas the clones varied in tumorigenic response (0-88% incidence). The best communicating clone (E9-2) was not tumorigenic. The highly communicating Cx32 clone, E9/32-9, gave a tumor incidence of 88%. These results suggest that restoration of GJIC by forced connexin expression can reduce the growth and tumorigenicity of lung carcinoma cells in a connexin-specific manner.
在许多类型的肿瘤细胞中都发现细胞间缝隙连接通讯(GJIC)减少,这可能有助于肿瘤表型的形成。本研究评估了小鼠和人肺癌细胞系中的GJIC(通过荧光染料偶联)和缝隙连接蛋白(连接蛋白)表达,并研究了GJIC减少是否参与其肿瘤表型。与未转化的肺上皮细胞相比,大多数癌细胞系(22个中的16个)中的染料偶联和连接蛋白43(Cx43)表达要低得多。未检测到其他连接蛋白。用Cx43转染通讯能力差的小鼠肺癌细胞系(E9)或用Cx32转导,分离出几个稳定克隆,其染料偶联增加了2至4倍。在体外评估生长时,克隆中的群体倍增时间增加,饱和密度降低。在评估致瘤性时,亲本E9细胞形成肿瘤的发生率为100%(6/6只小鼠),而克隆的致瘤反应各不相同(发生率为0-88%)。通讯能力最强的克隆(E9-2)不具有致瘤性。通讯能力高的Cx32克隆E9/32-9的肿瘤发生率为88%。这些结果表明,通过强制表达连接蛋白来恢复GJIC可以以连接蛋白特异性方式降低肺癌细胞的生长和致瘤性。
