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首页> 外文期刊>British Journal of Cancer >Measurement of cell kinetics in human tumours in vivo using bromodeoxyuridine incorporation and flow cytometry
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Measurement of cell kinetics in human tumours in vivo using bromodeoxyuridine incorporation and flow cytometry

机译:使用溴脱氧尿苷掺入和流式细胞仪测量体内人类肿瘤中的细胞动力学

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摘要

The proliferative potential of human solid tumours, in vivo, was investigated using bromodeoxyuridine (BrdUrd) incorporation and flow cytometry (FCM). Patients with solid tumours from a variety of sites were injected with 500 mg BrdUrd, intravenously, several hours prior to biopsy or surgical excision. The labelling index (LI), duration of S-phase (Ts) and thus the potential doubling time (Tpot) could be measured within 24 h of sampling. The results show that both the LI and Ts vary greatly between tumours (Ts ranges from 5.8 to 30.7 h). However, within this study of 26 evaluable patients, tumours of the same tissue origin tended to have similar Ts values. Melanomas had the shortest Ts (8.8 h), nine patients with head and neck cancer had Ts values ranging from 5.8 to 18.8 h (median 12.5 h). The longest Ts values (24 h) were found in lung and rectum. The estimates of Tpot ranged from only 3.2 days in an oat cell carcinoma to 23.2 days in a lymphoma. The striking feature of the study was that 38% of the tumours had a potential doubling time of 5 days or less. We found no relationship between proliferation and histopathological differentiation or DNA ploidy. It should now be possible to assess the prognostic significance of pretreatment cell kinetic measurements which may, in the future, aid in the selection of treatment schedules for the individual patient.
机译:使用溴脱氧尿苷(BrdUrd)掺入和流式细胞仪(FCM)研究了人体实体瘤在体内的增殖潜力。在活检或手术切除前几个小时,对来自各个部位的实体瘤患者静脉内注射500 mg BrdUrd。标记指数(LI),S相持续时间(Ts)以及潜在的倍增时间(Tpot)可以在采样的24小​​时内进行测量。结果表明,LI和Ts在肿瘤之间差异很大(Ts范围为5.8至30.7 h)。但是,在这项针对26位可评估患者的研究中,相同组织起源的肿瘤往往具有相似的Ts值。黑色素瘤的Ts最短(8.8 h),九名头颈部癌患者的Ts值范围为5.8至18.8 h(中值12.5 h)。在肺和直肠中发现最长的Ts值(24小时)。 Tpot的估计范围从燕麦细胞癌中的仅3.2天到淋巴瘤中的23.2天不等。该研究的显着特征是38%的肿瘤的潜在倍增时间为5天或更短。我们发现增殖与组织病理学分化或DNA倍性之间没有关系。现在应该有可能评估预处理细胞动力学测量的预后意义,将来可能有助于选择个别患者的治疗方案。

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