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正常人淋巴细胞以及HL-60和MOLT-4白血病细胞系中p120核仁抗原的细胞周期相关表达:甲氨蝶呤、喜树碱和替尼泊苷的影响。

Cell cycle-related expression of p120 nucleolar antigen in normal human lymphocytes and in cells of HL-60 and MOLT-4 leukemic lines: effects of methotrexate, camptothecin, and teniposide.

作者信息

Gorczyca W, Bruno S, Melamed M R, Darzynkiewicz Z

机构信息

Cancer Research Institute, New York Medical College, Valhalla 10595.

出版信息

Cancer Res. 1992 Jun 15;52(12):3491-4.

PMID:1596908
Abstract

Expression of the proliferation-associated nucleolar antigen p120 was studied by flow cytometry in human quiescent and phytohemagglutinin-stimulated lymphocytes, as well as in human lymphocytic (MOLT-4) and promyelocytic (HL-60) cell lines. Bivariate analysis of p120 and DNA content made it possible to correlate p120 expression with cell position in the cycle. Proliferating lymphocytes and MOLT-4 and HL-60 cells had a similar pattern of p120 expression. Populations of G1 cells, in all three cell types, were very heterogenous with respect to p120, and a threshold in G1 was observed. The cells with a p120 level below the threshold value did not enter S phase. An increase in p120 was observed during progression through S phase, and the antigen was maximally expressed in G2 cells. The p120/DNA content ratio, however, was highest in late G1 cells (G1B) and was declining during S and G2. The data thus suggest that p120 may be degraded during mitosis and that the postmitotic cells inherit little, if any, of this protein; the antigen then accumulates predominantly during G1, and must reach a threshold level to enable the cells to enter S phase. Antigen p120 could not be detected in noncycling lymphocytes nor in HL-60 cells induced to myeloid differentiation by growth in the presence of dimethyl sulfoxide. Treatment of MOLT-4 cells with pharmacological concentrations of methotrexate, camptothecin, or teniposide induced cell arrest in S or G2; expression of p120 in the arrested cells was unchanged from that of untreated MOLT-4 controls at the same phase of the cycle. The level of p120 was minimal in MOLT-4 or HL-60 cells arrested in M phase by vinblastine, but vinblastine had no effect on p120 fluorescence of interphase cells. Camptothecin or teniposide induced apoptosis selectively in S phase of HL-60 cells; apoptotic cells from camptothecin-treated cultures, however, despite the marked nucleolysis, still expressed p120. The data on the drug-treated cells indicate that the p120 level in tumors of patients may be used as a marker of tumor/malignancy even in clinical samples obtained during treatment.

摘要

通过流式细胞术研究了增殖相关核仁抗原p120在人静止和植物血凝素刺激的淋巴细胞以及人淋巴细胞系(MOLT-4)和早幼粒细胞系(HL-60)中的表达。对p120和DNA含量进行双变量分析,使得将p120表达与细胞周期中的位置相关联成为可能。增殖的淋巴细胞以及MOLT-4和HL-60细胞具有相似的p120表达模式。在所有三种细胞类型中,G1期细胞群体在p120方面非常异质,并且在G1期观察到一个阈值。p120水平低于阈值的细胞不会进入S期。在S期进程中观察到p120增加,并且该抗原在G2期细胞中最大程度表达。然而,p120/DNA含量比值在G1晚期细胞(G1B)中最高,并且在S期和G2期期间下降。因此,数据表明p120可能在有丝分裂期间被降解,并且有丝分裂后细胞几乎不继承这种蛋白质(如果有的话);然后该抗原主要在G1期积累,并且必须达到阈值水平才能使细胞进入S期。在非循环淋巴细胞中以及在存在二甲基亚砜的情况下生长诱导髓系分化的HL-60细胞中均未检测到抗原p120。用药理浓度的甲氨蝶呤、喜树碱或替尼泊苷处理MOLT-4细胞会诱导细胞停滞在S期或G2期;停滞细胞中p120的表达与处于相同细胞周期阶段的未处理MOLT-4对照相比没有变化。长春碱使MOLT-4或HL-60细胞停滞在M期时,p120水平最低,但长春碱对间期细胞的p120荧光没有影响。喜树碱或替尼泊苷在HL-60细胞的S期选择性诱导凋亡;然而,来自喜树碱处理培养物中的凋亡细胞,尽管有明显的核溶解,仍然表达p120。关于药物处理细胞的数据表明,即使在治疗期间获得的临床样本中,患者肿瘤中的p120水平也可作为肿瘤/恶性肿瘤的标志物。

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