Rawson C L, Loo D T, Duimstra J R, Hedstrom O R, Schmidt E E, Barnes D W
Department of Biochemistry and Biophysics, Oregon State University, Corvallis 97331-6503.
J Cell Biol. 1991 May;113(3):671-80. doi: 10.1083/jcb.113.3.671.
Serum-free mouse embryo (SFME) cells, derived in medium in which serum is replaced with growth factors and other supplements, are proastroblasts that are acutely dependent on epidermal growth factor (EGF) for survival. Ultrastructurally, an early change found in SFME cells deprived of EGF was a loss of polysomes which sedimentation analysis confirmed to be a shift from polysomes to monosomes. The ribosomal shift was not accompanied by decreased steady-state level of cytoplasmic actin mRNA examined as an indicator of cellular mRNA level. With time the cells became small and severely degenerate and exhibited nuclear morphology characteristic of apoptosis. Genomic DNA isolated from cultures undergoing EGF deprivation-dependent cell death exhibited a pattern of fragmentation resulting from endonuclease activation characteristic of cells undergoing apoptosis or programmed cell death. Flow cytometric analysis indicated that cultures in the absence of EGF contained almost exclusively G1-phase cells. Some of the phenomena associated with EGF deprivation of SFME cells are similar to those observed upon NGF deprivation of nerve cells in culture, suggesting that these neuroectodermal-derived cell types share common mechanisms of proliferative control involving peptide growth factor-dependent survival.
无血清小鼠胚胎(SFME)细胞是在以生长因子和其他补充剂替代血清的培养基中培养得到的,属于原成纤维细胞,对表皮生长因子(EGF)的存活具有高度依赖性。在超微结构上,在缺乏EGF的SFME细胞中发现的早期变化是多核糖体的丧失,沉降分析证实这是从多核糖体向单核糖体的转变。核糖体的转变并未伴随着作为细胞mRNA水平指标检测的细胞质肌动蛋白mRNA稳态水平的降低。随着时间的推移,细胞变得变小并严重退化,呈现出凋亡特征性的核形态。从经历EGF剥夺依赖性细胞死亡的培养物中分离的基因组DNA呈现出由核酸内切酶激活导致的片段化模式,这是经历凋亡或程序性细胞死亡的细胞的特征。流式细胞术分析表明,在没有EGF的情况下培养的细胞几乎完全是G1期细胞。与SFME细胞EGF剥夺相关的一些现象与培养的神经细胞NGF剥夺时观察到的现象相似,这表明这些神经外胚层来源的细胞类型共享涉及肽生长因子依赖性存活的增殖控制共同机制。
