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由HPV16-E6E7病毒癌基因永生化的人卵巢表面上皮细胞中的非随机染色体失衡。

Nonrandom chromosomal imbalances in human ovarian surface epithelial cells immortalized by HPV16-E6E7 viral oncogenes.

作者信息

Tsao S W, Wong N, Wang X, Liu Y, Wan T S, Fung L F, Lancaster W D, Gregoire L, Wong Y C

机构信息

Department of Anatomy, Faculty of Medicine, University of Hong Kong, SAR, Hong Kong, China.

出版信息

Cancer Genet Cytogenet. 2001 Oct 15;130(2):141-9. doi: 10.1016/s0165-4608(01)00473-3.

Abstract

We had previously immortalized human ovarian surface epithelial (HOSE) cells using HPV16E6E7 ORFs. In order to identify crucial genetic events involved during cell immortalization, the genomic profile of immortalization of five HOSE cell lines was analyzed by comparative genomic hybridization. Our results showed that chromosomal imbalance was common in HOSE cells after immortalization. The common chromosomal imbalances identified in immortal HOSE cells are: +19q13.1 (5/5 lines), -13q12 approximately qter (4/5 lines), +5q15 approximately q33 (3/5 lines), +20q11.2 approximately q13.2 (3/5 lines) and -22q11.2 approximately qter (3/5 lines). Other chromosomal imbalances, which were detected in two of the five immortal HOSE cell lines, included gains on chromosome 1 and 11q12 approximately q13, and losses on 2p, 4q, 8p, 10p and 11q14 approximately qter. The chromosomal imbalances observed in HOSE cells before immortalization include -8pter approximately p11.2, -11q23 approximately qter, -13q12 approximately qter and +19 which may represent early genetic events during cell immortalization. The genomic profile was examined in one HOSE cell line (HOSE 6-3) at various stages of immortalization. The genomic profiles of HOSE 6-3 cells after crisis were largely stable. A few additional chromosomal imbalances were detected in the immortalized HOSE cells after an extensive culture period including +11pter approximately q23, -15q23 approximately qter, and +17q12 approximately qter. Identification of nonrandom chromosomal imbalance in immortalized HOSE cells may facilitate the identification of specific chromosomes harboring genes involved in the immortalization of human ovarian surface epithelial cells.

摘要

我们之前使用人乳头瘤病毒16E6E7开放阅读框(HPV16E6E7 ORFs)使人类卵巢表面上皮(HOSE)细胞永生化。为了鉴定细胞永生化过程中涉及的关键基因事件,通过比较基因组杂交分析了五个HOSE细胞系永生化的基因组图谱。我们的结果显示,永生化后HOSE细胞中染色体失衡很常见。在永生化的HOSE细胞中鉴定出的常见染色体失衡包括:+19q13.1(5/5个细胞系)、-13q12至qter(4/5个细胞系)、+5q15至q33(3/5个细胞系)、+20q11.2至q13.2(3/5个细胞系)和-22q11.2至qter(3/5个细胞系)。在五个永生化的HOSE细胞系中的两个中检测到的其他染色体失衡包括1号染色体和11q12至q13的增加,以及2p、4q、8p、10p和11q14至qter的缺失。在永生化前的HOSE细胞中观察到的染色体失衡包括-8pter至p11.2、-11q23至qter、-13q12至qter和+19,这可能代表细胞永生化过程中的早期基因事件。在一个HOSE细胞系(HOSE 6-3)永生化的不同阶段检查了基因组图谱。危机后HOSE 6-3细胞的基因组图谱基本稳定。在长时间培养后,在永生化的HOSE细胞中检测到一些额外的染色体失衡,包括+11pter至q23、-15q23至qter和+17q12至qter。鉴定永生化HOSE细胞中的非随机染色体失衡可能有助于鉴定携带参与人类卵巢表面上皮细胞永生化的基因的特定染色体。

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