8;22染色体易位的北美伯基特(NAB-2)淋巴瘤细胞系的癌基因表达和免疫球蛋白合成

Oncogene research Pub Date : 1990-01-01
N C Popescu, J E Dahlberg, D V Ablashi, M Monastier, C A Bona, J A DiPaolo, W C Hooper, D C Swan
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引用次数: 0

摘要

来自北美患者的伯基特淋巴瘤(BL)细胞系(NAB-2)表现出涉及c-myc基因和λ免疫球蛋白基因的8;22 (q22;q11-12)易位。此外,NAB-2细胞还有另外两个一致的易位:1;5 (p22;q23)和3;7 (p25;q22),断点分别接近N-ras、fms和raf-1原癌基因的位置。用myc、N-ras和raf-1放射性标记DNA探针对NAB-2染色体进行原位杂交显示,这些基因都没有因易位而重新定位。然而,通过Northern blot分析,myc mRNA由两个转录本表示,一个约2.4 kb,另一个大得多(74 kb)。NAB-2细胞中也检测到raf-1基因转录物;然而,它的大小和水平与其他两条BL系相似。另一方面,在BL中频繁激活的N-ras、fms和fgr基因转录不活跃。NAB-2细胞也有染色单体缺陷,可见为2号染色体短臂上靠近kappa免疫球蛋白基因位点的消色差区域。这种改变是由eb病毒或病毒产物引起的病毒修饰位点,对免疫球蛋白合成没有影响,因为与8;22易位一致的NAB-2细胞在细胞质和表面λ轻链上呈阳性。尽管NAB-2细胞表现出几种染色体异常,但只有易位8,22与这种恶性肿瘤发展相关的基因改变有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Oncogene expression and immunoglobulin synthesis in a North American Burkitt (NAB-2) lymphoma cell line with a 8;22 chromosome translocation.

A Burkitt's lymphoma (BL) cell line, (NAB-2) deriving from a North American patient, exhibited a 8;22 (q22;q11-12) translocation involving the c-myc gene and lambda immunoglobulin genes. In addition, NAB-2 cells have two other consistent translocations: a 1;5 (p22;q23) and a 3;7 (p25;q22), with breakpoints close to the location of N-ras, fms, and raf-1 protooncogenes, respectively. In situ hybridization with myc, N-ras, and raf-1 radiolabeled DNA probes to NAB-2 chromosomes showed that none of these genes was relocated as a result of translocation. However, by Northern blot analysis, the myc mRNA was represented by two transcripts, one approximately 2.4 kb and the other considerably larger (74 kb). The raf-1 gene transcript was also detected in NAB-2 cells; however, its size and level were similar to those seen in two other BL lines. On the other hand, the N-ras, fms, and fgr genes, which are frequently activated in BL, were not actively transcribed. NAB-2 cells also have a chromatid defect visible as an achromatic region on the short arm of chromosome 2 near the locus of the kappa immunoglobulin gene. This alteration, which is a viral modification site caused by the Epstein-Barr virus or viral products, had no influence on immunoglobulin synthesis, as NAB-2 cells concordant to the 8;22 translocation were positive for cytoplasmic and surface lambda light chains. Although NAB-2 cells exhibit several chromosomal abnormalities, only translocation, 8;22 was associated with gene alterations relevant to the neoplastic development of this malignancy.

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