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慢性粒细胞白血病和正常骨髓中的姐妹染色单体分化及细胞周期特异性模式。

Sister chromatid differentiation and cell-cycle-specific patterns in chronic myelocytic leukemia and normal bone marrow.

作者信息

Becher R, Schmidt C G

出版信息

Int J Cancer. 1982 Jun 15;29(6):617-20. doi: 10.1002/ijc.2910290603.

Abstract

After in vitro incubation with bromodeoxyuridine (BrdUrd)-containing medium, metaphases of Philadelphia (Ph1)-chromosome positive cells in the blood and/or bone marrow of eight untreated patients with chronic myelocytic leukemia (CML) were analysed by means of sister chromatid differentiation (SCD) and compared to 10 normal bone marrows. The majority of proliferating Ph1-positive cells (range: 46-86%) were unable to complete more than one cell cycle during the culture period of 50 h (MI metaphases). Ph1-positive M2 metaphases which had completed two cell cycles were found in the range of 18-54% and almost no M3 metaphases were detected after passage through three cell cycles (0-1%). The corresponding findings in proliferating normal bone-marrow cells were: MI (13-68%), M2 (30-79%) and M3 (0-18%). These data support the notion that there is a prolonged cell cycle time in CML which can be measured by SCD, demonstrating a proportional shift from M3/M2 to MI metaphases. SCD is suggested for kinetic studies on human malignant cell clones characterized by marker chromosomes.

摘要

在用含溴脱氧尿苷(BrdUrd)的培养基进行体外培养后,采用姐妹染色单体分化(SCD)方法分析了8例未经治疗的慢性粒细胞白血病(CML)患者血液和/或骨髓中费城(Ph1)染色体阳性细胞的中期相,并与10份正常骨髓进行了比较。在50小时的培养期(有丝分裂中期)内,大多数增殖的Ph1阳性细胞(范围:46 - 86%)无法完成超过一个细胞周期。已完成两个细胞周期的Ph1阳性M2中期相占18 - 54%,经过三个细胞周期后几乎未检测到M3中期相(0 - 1%)。增殖的正常骨髓细胞的相应结果为:M1(13 - 68%)、M2(30 - 79%)和M3(0 - 18%)。这些数据支持了CML中存在延长的细胞周期时间这一观点,该时间可通过SCD测量,表明从M3/M2到M1中期相存在比例性变化。建议将SCD用于对以标记染色体为特征的人类恶性细胞克隆的动力学研究。

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