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共济失调毛细血管扩张症细胞在博来霉素处理后染色体损伤及修复率的异质性。

Heterogeneity in chromosome damage and repair rates after bleomycin in ataxia telangiectasia cells.

作者信息

Hittelman W N, Sen P

机构信息

Department of Medical Oncology, University of Texas M.D. Anderson Hospital and Tumor Institute, Houston.

出版信息

Cancer Res. 1988 Jan 15;48(2):276-9.

PMID:2446745
Abstract

Cells derived from patients with ataxia telangiectasia (AT) are known to be exceptionally sensitive to ionizing radiation and chemotherapeutic agents such as bleomycin (BLM), neocarzinostatin, and etoposide. This increased sensitivity is manifested by high chromosome aberration frequencies after treatment. In order to probe the underlying basis for this phenomenon, the technique of premature chromosome condensation was used to determine whether the increased chromosome damage observed after bleomycin treatment is due to increased initial chromosome damage or to a decreased capability of these cells to repair chromosome damage. Five AT cell lines were brought to quiescence and treated with BLM, and initial chromosome damage and repair rates were determined in the G1 prematurely condensed chromosomes. AT cells exhibited increased aberration frequencies compared to normal human fibroblasts immediately after BLM treatment. The five AT cell lines were heterogeneous in the fast component of chromosome break repair, varying from a nearly normal fast repair component in one cell line to a nearly defunct fast repair component in two other AT cell lines. Thus, while the AT cell lines were heterogeneous in the basis for their chromosome breakage sensitivity, all AT cell lines tested showed increased residual chromosome damage after BLM treatment while still in the quiescent phase.

摘要

已知共济失调毛细血管扩张症(AT)患者来源的细胞对电离辐射以及博来霉素(BLM)、新制癌菌素和依托泊苷等化疗药物异常敏感。这种敏感性增加表现为治疗后染色体畸变频率很高。为了探究这一现象的潜在基础,采用了早熟染色体凝集技术来确定博来霉素处理后观察到的染色体损伤增加是由于初始染色体损伤增加还是由于这些细胞修复染色体损伤的能力下降。使5种AT细胞系进入静止期并用BLM处理,然后在G1期早熟凝集染色体中测定初始染色体损伤和修复率。与正常人类成纤维细胞相比,BLM处理后立即观察到AT细胞的畸变频率增加。这5种AT细胞系在染色体断裂修复的快速成分方面存在异质性,从一个细胞系中接近正常的快速修复成分到另外两个AT细胞系中几乎失效的快速修复成分不等。因此,虽然AT细胞系在其染色体断裂敏感性的基础方面存在异质性,但所有测试的AT细胞系在仍处于静止期时经BLM处理后均显示出残留染色体损伤增加。

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