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Nuclear binding of tritiated actinomycin in surface epithelial cells from normal stomach and atrophic gastritis.

机译:normal化放线菌素在正常胃和萎缩性胃炎的表面上皮细胞中的核结合。

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摘要

Triated actinomycin binding to DNA is closely linked to the degree of repression in chromatin. 3H-AM binding to DNA is the most pronounced in nuclei of cells committed into cycle. Inversely, in cells in the last steps of their differentiation or (and) in the resting state (non-dividing cells), 3H-AM binding for DNA is diminished down to a baseline since it is limited by the deoxynucleoproteins. Epithelial cells of stomach mucosa and duodenum demonstrate an increased cell uptake of tritiated actinomycin from the surface to the bottom of the pits. In severe gastritis and in intestinalysed metaplasia this was abolished: with a uniform enhancement of 3H-AM binding. These findings seem to indicate that these cells are derepressed.
机译:与DNA结合的三联放线菌素与染色质的抑制程度密切相关。 3H-AM与DNA的结合在进入循环的细胞核中最为明显。相反,在细胞分化的最后阶段或(和)处于静止状态的细胞(非分裂细胞)中,DNA的3H-AM结合降低至基线,因为它受脱氧核蛋白的限制。胃粘膜和十二指肠的上皮细胞从tri的表面到底部显示the化放线菌素的细胞摄取增加。在严重的胃炎和肠上皮化生中,这种情况已被消除:3H-AM结合的均匀增强。这些发现似乎表明这些细胞被抑制。

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