甲氨蝶呤在角质化上皮中的昼夜周期依赖性。流式细胞术在仓鼠颊袋上皮的体内研究。

U Møller, J K Larsen, N Keiding, I J Christensen
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引用次数: 4

摘要

仓鼠颊袋上皮的部分同步细胞系统显示出典型的细胞增殖昼夜节律。研究发现,致死剂量(10 g/m2)和非致死剂量(2 g/m2)的甲氨蝶呤(Mtx)主要通过损害G1/S转变来抑制细胞周期进展。结果通过流式细胞仪DNA分析获得。Mtx的抑制作用表现为S部分(药物效应期)的相对减少,并且发现其依赖于剂量和给药时间。在1200小时(最小数量的细胞处于S期)或0200小时(最大数量的细胞处于S期)给药。在1200h注射时,S分数的累积下降最大。注射和效果之间的时间(S分数下降)与注射Mtx的时间无关,但似乎与从G1期到S期(暗期开始时)通量增加的自然昼夜周期有关。在接下来的24小时内重复了主要作用(S分数的相对降低),表明Mtx对G1细胞的作用是持久的。受初始高Mtx血浆浓度影响的G1细胞似乎是在第一个和第二个24小时内减少流入S期的原因。在早期的毒理学研究中,仓鼠的存活率与注射时间有关,在注射1200小时后达到最高。因此,对上皮细胞的最大细胞动力学影响是在一天中对动物的致命影响最小的时候发现的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Circadian-stage dependence of methotrexate in a keratinized epithelium. An in-vivo study using flow cytometry on the hamster cheek pouch epithelium.

The partially synchronized cell system of the hamster cheek pouch epithelium shows a characteristic diurnal rhythm of cell proliferation. Bolus injections of methotrexate (Mtx) in both lethal (10 g/m2) and non-lethal (2 g/m2) doses were found to inhibit cell-cycle progression primarily by impairing the G1/S transition. The results were obtained by flow cytometric DNA analysis. The inhibitory effect of Mtx manifested itself as a relative decrease of the S fraction (drug-effector phase), and was found to be dependent both on the dose and on the time of the day it was given. A bolus injection of Mtx was given either at 1200 hr (when a minimal number of cells are in S phase) or at 0200 hr (when a maximum number of cells are in S phase). The greatest cumulative decrease in S fraction was seen when the injection was given at 1200 hr. The time between injection and the effect (seen as a decrease in S fraction) was independent of the time of the Mtx injection, but seemed instead to be related to the natural diurnal period of increasing flux from G1 to S phase (at the onset of the dark period). The main effect (the relative decrease in S fraction) was repeated during the following 24-hr period, pointing to a protracted effect of Mtx on G1 cells. G1 cells affected by the initial high Mtx plasma concentration seem to be responsible for the reduced influx into S phase in both the first and second 24-hr period. In earlier toxicological studies, the survival rate of hamsters was dependent on the time of injection and was highest after injection at 1200 hr. Thus maximum cytokinetic effect on epithelial cells was found at the time of the day when there was a minimum lethal effect on the animal.

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