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致瘤性播散和停滞癌细胞的定量分析。

Quantitation of tumorigenic disseminating and arrested cancer cells.

作者信息

Mayhew E, Glaves D

出版信息

Br J Cancer. 1984 Aug;50(2):159-66. doi: 10.1038/bjc.1984.158.

Abstract

The numbers of potentially tumorigenic cancer cells released into the circulation and secondarily arrested in the lungs of mice bearing B16F10 melanomas or Lewis lung carcinomas were systematically quantified throughout i.m. tumour growth using a bioassay procedure capable of detecting as few as 10 to 100 tumorigenic cells in the circulation or lungs. Viable disseminating cancer cells were detectable within 4 days of i.m. tumour growth and reached 10(6) per 0.5 ml of blood in carcinoma-bearers and 2 X 10(4) per 0.5 ml in melanoma-bearers; 98% of mice with circulating cancer cells had potentially tumorigenic cells in their lungs, even in the absence of overt metastases. The numbers of cancer cells present in the circulation and lungs were related to the growth rate of the i.m. lesion, more cells being released from faster-growing tumours. The numbers of tumorigenic carcinoma cells were compared with the total numbers of cells released into the circulation as quantitated by direct counting procedures, and it was found that the vast majority of these circulating cells were potentially tumorigenic. These studies provide quantitative information about cancer cell input into the metastatic process. Also, the bioassay procedure provides a useful experimental model for the development of regimens for therapy of metastases since it is a sensitive method of monitoring not only the size of disseminated populations of cancer cells but also their clinically relevant property namely, their tumorigenic potential.

摘要

在携带B16F10黑色素瘤或Lewis肺癌的小鼠体内,通过一种生物测定程序,对在肌肉注射肿瘤生长过程中释放到循环系统并继而滞留在肺部的潜在致瘤癌细胞数量进行了系统定量。该生物测定程序能够检测循环系统或肺部中低至10到100个致瘤细胞。在肌肉注射肿瘤生长4天内即可检测到存活的播散癌细胞,在荷癌小鼠中,每0.5毫升血液中癌细胞数量达到10^6个,在荷黑色素瘤小鼠中为每0.5毫升2×10^4个;即使在没有明显转移的情况下,98%循环系统中有癌细胞的小鼠肺部也有潜在致瘤细胞。循环系统和肺部中的癌细胞数量与肌肉注射病灶的生长速率相关,生长较快的肿瘤释放出的细胞更多。将致瘤癌细胞数量与通过直接计数程序定量的释放到循环系统中的细胞总数进行比较,发现这些循环细胞中的绝大多数都具有潜在致瘤性。这些研究提供了有关癌细胞进入转移过程的定量信息。此外,该生物测定程序为开发转移瘤治疗方案提供了一个有用的实验模型,因为它不仅是监测癌细胞播散群体大小的灵敏方法,而且是监测其临床相关特性即致瘤潜力的灵敏方法。

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