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化疗药物或热疗诱导细胞死亡的动力学和物理学研究。

Kinetic and physical studies of cell death induced by chemotherapeutic agents or hyperthermia.

作者信息

Dyson J E, Simmons D M, Daniel J, McLaughlin J M, Quirke P, Bird C C

出版信息

Cell Tissue Kinet. 1986 May;19(3):311-24. doi: 10.1111/j.1365-2184.1986.tb00683.x.

Abstract

The kinetics of three physical parameters: cell density, relative cytoplasmic viscosity and DNA stability to denaturation have been measured during the period preceding cell death induced by hyperthermia, methylprednisolone and a series of cancer chemotherapeutic agents. This series of measurements employed cultured human lymphoblastoid cells as an experimental system to establish the changes that can be observed in the early stages of cell death, prior to applying such measurements to tissue biopsies from solid human tumours. Cell death, induced by hyperthermia up to 43 degrees C, methylprednisolone, vincristine, 5-fluorouracil, BCNU and melphalan, showed essentially identical and reproducible changes corresponding to those which characterize programmed cell death (apoptosis). Such changes could also be observed following hyperthermia above 43 degrees C, but reproducibility was poor and increasing damage to the cell membranes was evident. In cells treated with adriamycin or methotrexate, cell sub-populations showing an increase in cell density were not detected. Measurements of DNA stability were readily performed by flow cytofluorometry thus allowing rapid quantitation of the fraction of cells in the early stages of cell death. Modified flow cytometric instrumentation would further allow measurement of cytoplastic viscosity as an additional parameter to indicate entry into programmed cell death. This suggests that these measurements could readily be applied to cell suspensions derived from tumour tissue biopsies for a more accurate assessment of tumour growth rate, and to allow monitoring of response to therapy in sequential tumour biopsies.

摘要

在由热疗、甲基强的松龙和一系列癌症化疗药物诱导细胞死亡之前的时间段内,已对三个物理参数的动力学进行了测量,这三个参数分别是细胞密度、相对细胞质粘度和DNA对变性的稳定性。这一系列测量采用培养的人淋巴母细胞作为实验系统,以确定在细胞死亡早期阶段可观察到的变化,然后再将此类测量应用于取自人类实体肿瘤的组织活检。由高达43摄氏度的热疗、甲基强的松龙、长春新碱、5-氟尿嘧啶、卡氮芥和苯丁酸氮芥诱导的细胞死亡,显示出与程序性细胞死亡(凋亡)特征基本相同且可重复的变化。在高于43摄氏度的热疗后也可观察到此类变化,但可重复性较差,且细胞膜的损伤明显增加。在用阿霉素或甲氨蝶呤处理的细胞中,未检测到细胞密度增加的细胞亚群。通过流式细胞荧光测定法很容易进行DNA稳定性的测量,从而能够快速定量处于细胞死亡早期阶段的细胞比例。改进后的流式细胞仪还可进一步测量细胞质粘度,作为表明进入程序性细胞死亡的另一个参数。这表明这些测量可很容易地应用于源自肿瘤组织活检的细胞悬液,以便更准确地评估肿瘤生长速率,并在连续的肿瘤活检中监测对治疗的反应。

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