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两个致瘤性卡波西肉瘤细胞系中涉及3号染色体(p14)的缺失和易位。

Deletion and translocation involving chromosome 3 (p14) in two tumorigenic Kaposi's sarcoma cell lines.

作者信息

Popescu N C, Zimonjic D B, Leventon-Kriss S, Bryant J L, Lunardi-Iskandar Y, Gallo R C

机构信息

National Institute of health, Bethesda, MD 20892-4255, USA.

出版信息

J Natl Cancer Inst. 1996 Apr 3;88(7):450-5. doi: 10.1093/jnci/88.7.450.

DOI:10.1093/jnci/88.7.450
PMID:8618237
Abstract

BACKGROUND

Two neoplastic Kaposi's sarcoma (KS) cell lines, KS Y-1 (derived from a patient with KS associated with acquired immunodeficiency syndrome) and KS SLK (derived from an immunosuppressed patient with a renal transplant and KS or iatrogenic KS), have been shown to have abnormal chromosome constitution and to require no exogenous growth factors. They produce malignant tumors in immunodeficient mice. In contrast, all other cell cultures prepared in the past from KS specimens have shown to have normal diploid characteristics are hyperplastic, and depends on cytokines for growth, but they do not produce malignant tumors in immunodeficient mice.

PURPOSE

We investigated whether the chromosomal changes that occurred in these KS cell lines were random contribute to the pathogenesis of KS.

METHODS

We used the conventional G-banding technique and fluorescence in sti hybridization to identify structural and numerical chromosomal changes in the KS cell lines.

RESULTS

We demonstrated that both cell lines are aneuploid and have some additional features in common, i.e., loss of copies of chromosomes 14 and 21 and nonrandom translocations and deletions in the short arm of chromosome 3 at region 3p14. These KS cell lines also exhibits loss of heterozygosity of loci at region 3p14-ter.

CONCLUSION

This is the first time nonrandom chromosomal alterations have been described in KS neoplastic cells. On the basis of information available on other available on other cancers, the chromosome 3 alterations observed here can be expected to contribute to the neoplastic process in KS.

IMPLICATIONS

Future research should focus on the identification cytogenetic markers, thus facilitating generation of specific molecular probes for detecting neoplastic cells early in the disease process.

摘要

背景

两种卡波西肉瘤(KS)肿瘤细胞系,KS Y-1(源自一名患获得性免疫缺陷综合征相关KS的患者)和KS SLK(源自一名接受肾移植且患KS或医源性KS的免疫抑制患者),已被证明具有异常的染色体构成,且无需外源性生长因子。它们在免疫缺陷小鼠中会产生恶性肿瘤。相比之下,过去从KS标本制备的所有其他细胞培养物均显示具有正常的二倍体特征,呈增生性,且生长依赖细胞因子,但它们在免疫缺陷小鼠中不会产生恶性肿瘤。

目的

我们研究了这些KS细胞系中发生的染色体变化是否随机,以及是否对KS的发病机制有影响。

方法

我们使用传统的G显带技术和荧光原位杂交来鉴定KS细胞系中的结构和数量染色体变化。

结果

我们证明这两种细胞系均为非整倍体,且有一些共同的其他特征,即14号和21号染色体拷贝丢失,以及3号染色体短臂3p14区域的非随机易位和缺失。这些KS细胞系在3p14 - ter区域也表现出杂合性缺失。

结论

这是首次在KS肿瘤细胞中描述非随机染色体改变。根据其他癌症的现有信息,此处观察到的3号染色体改变可能会促成KS的肿瘤形成过程。

启示

未来的研究应专注于鉴定细胞遗传学标志物,从而有助于生成用于在疾病早期检测肿瘤细胞的特异性分子探针。

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