ENHANCED TUMORIGENESIS BY SMALL, PROTRACTED DOSES OF DENSELY IONIZING RADIATION
ENHANCED TUMORIGENESIS BY SMALL, PROTRACTED DOSES OF DENSELY IONIZING RADIATION出 版 物:《Chinese Medical Journal》 (中华医学杂志(英文版))
年 卷 期:1994年第6期
页 面:16-21页
核心收录:
学科分类:0831[工学-生物医学工程(可授工学、理学、医学学位)] 100207[医学-影像医学与核医学] 1006[医学-中西医结合] 1002[医学-临床医学] 1001[医学-基础医学(可授医学、理学学位)] 08[工学] 1010[医学-医学技术(可授医学、理学学位)] 100106[医学-放射医学] 10[医学] 100602[医学-中西医结合临床]
主 题:Res rate ENHANCED TUMORIGENESIS BY SMALL PROTRACTED DOSES OF DENSELY IONIZING RADIATION 口口 TPA
摘 要:Starting with observations that were first published in 1982. a series of additional findings led to the discovery of an important property of eel s in late G2/ mitosis. In addition to being the most sensitive to killing, cells in this age-interval were also shown to be the most sensitive to radiation-induced neoplastic transformation. In this work, C3H mouse cells, designated 10T1 / 2, were irradiated with fission-spectrum neutrons and assayed in vitro via the endpoint focus formation on a monolayer of normal cells. From these observations, a biophysical model was developed to explain the anomalous finding that the frequency of transformation by low doses was enhanced when the exposure was protracted. In contrast to transformation by X- and 7-rays where repair and kinetics during exposure play dominant roles, with radiations like reactor neutrons and a-particles repair has a minimal effect; only cell kinetics acts significantly to modify transformation due to protracted doses. In this report, the lack of responsiveness of mitotic cells to promotion by the phorbol ester 12-0-tetradecanoylphorbol-13-acetate is shown further to agree with the findings with fission-neutrons and the model that, at low dose rate, enhanced transformation is due principally to the progression of cells into the window of sensitivity. Implications of this model for lung cancer due to environmental radon are also discussed.
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