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Procoagulant Activity of Human Neuroblastoma Cell Lines in Relation to Cell Growth Differentiation and Cytogenetic Abnormalities

机译:人类神经母细胞瘤细胞系的促凝血活性与细胞生长分化和细胞遗传学异常的关系

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摘要

Procoagulant activity (PCA) was investigated in relation to cell growth, differentiation, and cytogenetics in seven human neuroblastoma cell lines. Before 5‐bromodeoxyuridine (BrdUrd) treatment, PCA was notably heterogeneous, with the highest activity in NCG (S‐type in morphology) 40‐to 100‐fold greater than the lowest activity in SK‐N‐D2 (N‐type). PCA was not related to 1p abnormalities. After BrdUrd treatment at 5 μg/ml for 6 days, PCA increased 6.8‐fold in GOTO and 2.7‐fold in SK‐N‐DZ with associated growth inhibition and morphological changes (I‐type morphology converted to S‐type in GOTO and N‐type converted to an advanced N‐type in SK‐N‐DZ). In contrast, only growth suppression was observed in 2 other cell lines, and no changes in PCA, growth or morphology were induced in the remaining 3 cell lines.
机译:研究了人类七种神经母细胞瘤细胞系中与细胞生长,分化和细胞遗传学有关的促凝血活性(PCA)。在进行5-溴脱氧尿苷(BrdUrd)治疗之前,PCA具有明显的异质性,其NCG(形态上为S型)最高活性比SK‐N‐D2(N型)最低活性高40至100倍。 PCA与1p异常无关。在以5μg/ ml的浓度BrdUrd处理6天后,GOTO中PCA升高6.8倍,SK‐N‐DZ中PCA升高2.7倍,并伴有生长抑制和形态变化(GOTO和N中I型形态转化为S型类型转换为SK‐N‐DZ中的高级N类型)。相反,在其他2个细胞系中仅观察到生长抑制,在其余3个细胞系中未诱导PCA,生长或形态的变化。

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