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转染的c-myc和c-Ha-ras调节大鼠胚胎细胞中的辐射诱导凋亡。

Transfected c-myc and c-Ha-ras modulate radiation-induced apoptosis in rat embryo cells.

作者信息

Chen C H, Zhang J, Ling C C

机构信息

Laboratory of Radiation Biophysics, Memorial Sloan Kettering Cancer Center, New York, New York 10021.

出版信息

Radiat Res. 1994 Sep;139(3):307-15.

PMID:8073113
Abstract

We studied radiation-induced apoptosis in rat embryo cells (REC) and in REC transfected with a c-myc oncogene [REC:myc(ch1)] or with a c-Ha-ras oncogene [REC:ras(ch1)], or both [REC:myc+ras(ch1)]. Apoptosis, evaluated in terms of altered morphology, dye exclusion and DNA fragmentation, was evident in all the irradiated cells. The development of apoptosis with time was initially rapid and then gradually saturated at > 36 h after irradiation. Radiation-induced apoptosis in REC:ras(ch1) was mildly reduced, but that in REC:myc(ch1) and REC:myc+ras(ch1) was significantly increased, relative to that in REC. The percentage of REC:myc(ch1) and REC:myc+ras(ch1) cells undergoing apoptosis increased rapidly at low doses to about 40% at 5 Gy irradiation and reached a plateau at high doses (of about 60% at > 15 Gy). In contrast, REC and REC:ras(ch1) were much less responsive, with a maximum of about 15 and 7%, respectively.

摘要

我们研究了辐射诱导大鼠胚胎细胞(REC)以及转染了c-myc癌基因[REC:myc(ch1)]、c-Ha-ras癌基因[REC:ras(ch1)]或两者[REC:myc+ras(ch1)]的REC中的细胞凋亡情况。通过形态改变、染料排斥和DNA片段化来评估细胞凋亡,结果显示所有受辐照细胞中均出现明显的细胞凋亡现象。细胞凋亡随时间的发展最初较快,然后在辐照后>36小时逐渐趋于饱和。相对于REC,REC:ras(ch1)中辐射诱导的细胞凋亡略有减少,但REC:myc(ch1)和REC:myc+ras(ch1)中的细胞凋亡显著增加。REC:myc(ch1)和REC:myc+ras(ch1)中发生凋亡的细胞百分比在低剂量时迅速增加,在5 Gy辐照时达到约40%,在高剂量(>15 Gy时约为60%)时达到平台期。相比之下,REC和REC:ras(ch1)的反应性要低得多,最大凋亡率分别约为15%和7%。

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