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转移性小鼠肿瘤中的辐射诱导标记染色体。

Irradiation-induced marker chromosomes in a metastasizing murine tumor.

作者信息

McMorrow L E, Wolman S R, Bornstein S, Talmadge J E

机构信息

Department of Pathology, New York University Medical Center, New York 10016.

出版信息

Cancer Res. 1988 Feb 15;48(4):999-1003.

PMID:3338091
Abstract

We have used irradiation to induce marker chromosome formation in a metastasizing murine tumor with a stable karyotype. The induced recombinant chromosomes then served to determine whether metastases were of clonal or multicellular origin. Cumulative data were obtained from four series of experiments on spontaneous metastases originating from tumors grown from irradiated cells; 20 of these metastases expressed unique chromosomal alterations consistent with a clonal origin. The majority of metastasis-derived cell populations remain stable with respect to their marker chromosomes in culture as well as in successive animal transplantation. In several instances, however, chromosomal instability was sufficient to obscure the cellular origins of individual metastases. A few metastases showed mixed chromosomal patterns initially that were consistent with multicellular origin, but repeat examinations have revealed a chromosomal instability which persisted during propagation in culture. The frequency of chromosomal recombinants in metastases from the combined series was sufficient to suggest biological and statistical significance. The morphology of recombinants was not associated with radiation dose but appeared as an apparently random response of the tumor population in different experiments. Analysis of chromosomal markers by banding techniques was performed to determine if specific chromosomes or chromosomal sites were associated with tumor cells from metastatic foci (a host-selected subpopulation with a metastatic phenotype). Our results did not reveal preferential involvement of whole chromosomes or intrachromosomal sites in recombinant formation.

摘要

我们利用辐射在具有稳定核型的转移性小鼠肿瘤中诱导标记染色体形成。然后,诱导产生的重组染色体用于确定转移灶是克隆起源还是多细胞起源。从四组关于源自经辐射细胞生长的肿瘤的自发转移实验中获得了累积数据;其中20个转移灶表现出与克隆起源一致的独特染色体改变。大多数源自转移灶的细胞群体在培养以及连续的动物移植中,其标记染色体保持稳定。然而,在一些情况下,染色体不稳定性足以掩盖个别转移灶的细胞起源。一些转移灶最初显示出与多细胞起源一致的混合染色体模式,但重复检查发现染色体不稳定性在培养传代过程中持续存在。联合系列实验中转移灶的染色体重组频率足以表明其生物学和统计学意义。重组体的形态与辐射剂量无关,而是在不同实验中表现为肿瘤群体的一种明显随机反应。采用显带技术对染色体标记进行分析,以确定特定染色体或染色体位点是否与转移灶(具有转移表型的宿主选择亚群)中的肿瘤细胞相关。我们的结果并未显示在重组形成过程中整条染色体或染色体内位点存在优先参与情况。

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