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博来霉素注射后小鼠肺中DNA合成及细胞成分的改变。

Alterations in DNA synthesis and cellular constituents in mouse lung following bleomycin injections.

作者信息

Katsura H, Taguchi T, Kida K

机构信息

Pulmonary Division, Tokyo Metropolitan Geriatric Hospital, Japan.

出版信息

Am J Respir Cell Mol Biol. 1992 Feb;6(2):190-6. doi: 10.1165/ajrcmb/6.2.190.

Abstract

Changes in the DNA synthesis and cellular constituents of mouse lung following repeated bleomycin (BLM) injections were studied. ICR mice were administered BLM subdermally for 10 days. Wet lung weight was increased 1.36 times on day 5 after the final administration compared with control mice receiving an identical volume of saline only for 10 days. The total number of cells in the bronchoalveolar lavage fluid of the BLM group reached a maximum on day 14, and histologic investigation of the lungs revealed marked cellular infiltrations. The labeling index obtained by the antibromodeoxyuridine monoclonal antibody method for cells was increased from days 5 to 14 in the BLM group. By day 28, these inflammatory changes had subsided and fibrotic remodeling had occurred. DNA polymerase activity in the lung tissue reached its maximal level on day 5 and remained unchanged until day 14. This phenomenon occurred in parallel with increases in DNA content and synthesis. During this period, an increase in DNA polymerase-beta activity and new induction of DNA polymerase-alpha activity were observed by phosphocellulose column chromatography. From these observations, it is concluded that: (1) repeated injections of BLM cause DNA injury in lung cells; (2) there is a subsequent increase in the DNA repair function as supported by the finding of an increase in DNA polymerase-beta activity; and (3) these lead further to cell proliferation as supported by the increase in both DNA polymerase-alpha activity and DNA content. Thus, a close relationship between morphologic changes and altered DNA synthesis was observed in the lungs of mice after BLM injections.

摘要

研究了反复注射博来霉素(BLM)后小鼠肺脏DNA合成及细胞成分的变化。对ICR小鼠进行皮下注射BLM,持续10天。末次给药后第5天,与仅接受相同体积生理盐水注射10天的对照小鼠相比,湿肺重量增加了1.36倍。BLM组支气管肺泡灌洗液中的细胞总数在第14天达到最大值,肺组织的组织学检查显示有明显的细胞浸润。通过抗溴脱氧尿苷单克隆抗体法测得的BLM组细胞标记指数在第5天至第14天升高。到第28天,这些炎症变化消退,发生了纤维化重塑。肺组织中的DNA聚合酶活性在第5天达到最高水平,并一直保持到第14天不变。这种现象与DNA含量和合成的增加同时出现。在此期间,通过磷酸纤维素柱色谱法观察到DNA聚合酶-β活性增加以及新诱导出DNA聚合酶-α活性。从这些观察结果可以得出以下结论:(1)反复注射BLM会导致肺细胞DNA损伤;(2)随后DNA修复功能增强,这一发现得到了DNA聚合酶-β活性增加的支持;(3)这些变化进而导致细胞增殖,这一结论得到了DNA聚合酶-α活性和DNA含量增加的支持。因此,在注射BLM后的小鼠肺脏中观察到形态学变化与DNA合成改变之间存在密切关系。

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