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P388和L1210白血病的体内生长动力学

In vivo growth kinetics of P388 and L1210 leukemias.

作者信息

Clausen O P, Bolstad K G, Mjelva E

机构信息

Department of Pathology Rikshospitalet, Oslo, Norway.

出版信息

Virchows Arch B Cell Pathol Incl Mol Pathol. 1988;54(5):278-83. doi: 10.1007/BF02899224.

Abstract

The P388 lymphocytic leukemia and the L1210 lymphoid leukemia are used as test systems for putative cytotoxic drugs. These leukemias are also used to investigate the perturbation of cell cycle progression of various chemical compounds in more detail. There is little information on the normal growth kinetics in vivo of these leukemias. In the present report we therefore present the results from growth kinetic studies of P388 and L1210 leukemic cells growing in ascites form in mice. We used 3H-TdR autoradiography, DNA flow cytometry and the stathmokinetic method. During exponential growth both leukemias showed a growth fraction of unity. Whereas no significant cell loss was observed during the early growth phase of P388 cells, cell loss was indicated by a discrepancy between potential and actual doubling times during exponential growth of L1210 cells. During the phase of growth retardation, the proportion of G1 and G2 cells increased at the expence of a reduced S phase fraction in the P388 leukemia, whereas only small changes in cell cycle distributions were seen with time after inoculation of L1210 cells. An increasing discrepancy in the reduction of the S phase fraction and the 3H-TdRLI was seen in the P388 cells with time after inoculation. Thus, a majority of P388 cells with S phase DNA content were unlabelled during the late phase of growth restriction, indicating resting cells in S phase. A good correlation was found between the 3H-TdR LI and S phase fraction throughout the life history of L1210 cells, revealing considerable differences in in vivo growth kinetics between the two leukemias. Such differences should be considered when evaluating test results.

摘要

P388淋巴细胞白血病和L1210淋巴白血病被用作潜在细胞毒性药物的测试系统。这些白血病也被用于更详细地研究各种化合物对细胞周期进程的干扰。关于这些白血病在体内的正常生长动力学的信息很少。因此,在本报告中,我们展示了对在小鼠腹水中生长的P388和L1210白血病细胞进行生长动力学研究的结果。我们使用了3H-TdR放射自显影术、DNA流式细胞术和静止期动力学方法。在指数生长期间,两种白血病的生长分数均为1。在P388细胞的早期生长阶段未观察到明显的细胞丢失,而在L1210细胞指数生长期间,潜在倍增时间与实际倍增时间之间的差异表明存在细胞丢失。在生长迟缓阶段,P388白血病中G1和G2期细胞的比例增加,S期比例降低,而接种L1210细胞后,细胞周期分布随时间仅有微小变化。接种后,P388细胞中S期比例的降低与3H-TdR标记指数之间的差异随时间增加。因此,在生长受限后期,大多数具有S期DNA含量的P388细胞未被标记,表明S期存在静止细胞。在L1210细胞的整个生命历程中,3H-TdR标记指数与S期比例之间发现了良好的相关性,揭示了两种白血病在体内生长动力学方面存在相当大的差异。在评估测试结果时应考虑这些差异。

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