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人慢性粒细胞白血病细胞系K-562中c-abl序列的重排与扩增。

Rearrangement and amplification of c-abl sequences in the human chronic myelogenous leukemia cell line K-562.

作者信息

Collins S J, Groudine M T

出版信息

Proc Natl Acad Sci U S A. 1983 Aug;80(15):4813-7. doi: 10.1073/pnas.80.15.4813.

Abstract

Structural rearrangements of specific cellular sequences (c-onc genes) homologous to acute transforming retrovirus oncogenes (v-onc genes) have been recently described in various malignancies. Here we show that human cellular sequences (c-abl) homologous to the transforming sequences of the mouse Abelson leukemia virus (v-abl) are amplified some 4- to 8-fold in K-562, a Philadelphia chromosome-positive cell line derived from a patient with chronic myelogenous leukemia in blast crisis. Restriction analysis of K-562 and other human DNA samples reveals a significant rearrangements of the c-abl sequences in this cell line. In addition, investigation of v-abl-related cytoplasmic RNA reveals relatively high levels of these sequences in K-562 compared to other normal and leukemia cells. We have also observed that lambda light chain constant region immunoglobulin genes are amplified in K-562, whereas kappa light chain sequences exhibit no amplification. These results are discussed within the context of the possibility that these Philadelphia chromosome-positive cells exhibit a reciprocal translocation involving chromosome 9 (containing c-abl) and chromosome 22 (containing the lambda light chain genes).

摘要

近期研究表明,在多种恶性肿瘤中,与急性转化逆转录病毒癌基因(v-onc基因)同源的特定细胞序列(c-onc基因)发生了结构重排。在此,我们发现,与小鼠Abelson白血病病毒(v-abl)转化序列同源的人类细胞序列(c-abl),在K-562细胞系中扩增了约4至8倍。K-562是一种源自慢性粒细胞白血病急变期患者的费城染色体阳性细胞系。对K-562及其他人类DNA样本的限制性分析显示,该细胞系中的c-abl序列发生了显著重排。此外,对与v-abl相关的细胞质RNA的研究表明,与其他正常细胞和白血病细胞相比,K-562细胞中这些序列的水平相对较高。我们还观察到,K-562细胞中λ轻链恒定区免疫球蛋白基因发生了扩增,而κ轻链序列未出现扩增。我们将在费城染色体阳性细胞出现涉及9号染色体(包含c-abl)和22号染色体(包含λ轻链基因)的相互易位这一可能性的背景下,对这些结果进行讨论。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/61bf/384135/b768226517ff/pnas00641-0222-a.jpg

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