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博来霉素损伤肺中转移性肿瘤生长的定量分析。

Quantification of metastatic tumor growth in bleomycin-injured lungs.

作者信息

Orr F W, Adamson I Y, Young L

出版信息

Clin Exp Metastasis. 1986 Apr-Jun;4(2):105-16. doi: 10.1007/BF00119077.

Abstract

The lung is a common target organ in experimental models of tumor metastasis in which quantification usually involves counting labeled tumor cells shortly after injection, or enumeration of grossly visible pleural tumors. In this study, these approaches were used in addition to autoradiographic and morphometric methods to analyse the effect of bleomycin-mediated injury on the development, distribution and quantification of pulmonary metastases. One day after intravenous injection of 2 X 10(5) fibrosarcoma cells, the lungs of C57 bl/6 mice, pretreated with bleomycin (120 mg/kg i.v., 5 days before) contained about nine times as many [131I] iododeoxyuridine-labeled cells as the lungs of control animals given saline injections. At this time, autoradiographic counts of [3H]thymidine-labeled tumor cells in lung sections showed a similar increase in tumor cell localization after bleomycin, with labeled cells distributed equally between parenchymal and pleural areas. However, subsequent tumor growth was demonstrated microscopically to be predominantly in pleural and peribronchial areas, especially at sites of lung injury induced by bleomycin. Counts of grossly visible pleural tumors failed to demonstrate a difference between bleomycin groups and controls at 7 days whereas counts of nodules in lung sections, and quantification of lung area occupied by tumor both showed significantly greater tumor involvement in bleomycin-treated animals. As tumors became confluent, morphometric measurements demonstrated tumor growth in the lung more accurately than did nodule counts. We conclude that bleomycin-induced injury greatly enhances metastatic tumor growth and that morphometric methods are more sensitive than lung colony counts in their ability to quantify pulmonary metastases. Morphometry and autoradiography have also demonstrated that while there is a uniform distribution of arrested tumor cells in the lung initially, there is preferential development of metastatic tumors at sites of pulmonary damage, in particular at the pleura.

摘要

在肿瘤转移的实验模型中,肺是常见的靶器官,其中定量通常涉及在注射后不久对标记的肿瘤细胞进行计数,或对肉眼可见的胸膜肿瘤进行计数。在本研究中,除了放射自显影和形态计量学方法外,还使用了这些方法来分析博来霉素介导的损伤对肺转移瘤的发生、分布和定量的影响。在静脉注射2×10⁵个纤维肉瘤细胞一天后,预先用博来霉素(120mg/kg静脉注射,5天前)处理的C57bl/6小鼠的肺中,[¹³¹I]碘脱氧尿苷标记的细胞数量约为注射生理盐水的对照动物肺中的9倍。此时,肺切片中[³H]胸腺嘧啶核苷标记的肿瘤细胞的放射自显影计数显示,博来霉素处理后肿瘤细胞定位有类似增加,标记细胞在实质和胸膜区域均匀分布。然而,随后显微镜下显示肿瘤生长主要在胸膜和支气管周围区域,特别是在博来霉素诱导的肺损伤部位。在7天时,肉眼可见的胸膜肿瘤计数未显示博来霉素组与对照组之间的差异,而肺切片中的结节计数以及肿瘤占据的肺面积定量均显示博来霉素处理的动物中肿瘤累及明显更多。随着肿瘤融合,形态计量学测量比结节计数更准确地显示了肺中的肿瘤生长。我们得出结论,博来霉素诱导的损伤极大地促进了转移性肿瘤的生长,并且形态计量学方法在量化肺转移方面比肺集落计数更敏感。形态计量学和放射自显影还表明,虽然最初肺中停滞的肿瘤细胞分布均匀,但在肺损伤部位,特别是胸膜处,转移性肿瘤有优先发展。

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