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将不同数量的转化3T3细胞接种到裸鼠体内后肿瘤生长和细胞适应的动态变化以及肿瘤细胞重新适应培养的情况。

Dynamics of tumor growth and cellular adaptation after inoculation into nude mice of varying numbers of transformed 3T3 cells and of readaptation to culture of the tumor cells.

作者信息

Rubin H, Chu B M, Arnstein P

出版信息

Cancer Res. 1986 Apr;46(4 Pt 2):2027-34.

PMID:3948178
Abstract

Decimal dilutions containing 5 X 10(5) to 5 X 10(1) cells were inoculated s.c. into nude mice and the course of tumor development was recorded. The highest concentration of cells produced rapidly growing poorly differentiated sarcomas within 2-3 weeks of their inoculation. Upon explantation the resultant tumors yielded cells which multiplied on plastic almost as rapidly as did their progenitors used to initiate the tumors, and had as high a colony forming efficiency in agar as long as tryptose phosphate broth was omitted from the agar medium. Tumors initiated by the lower concentrations of cells were disproportionately delayed in their appearance and tended to increase in size at a low rate. At least one tumor regressed and one which apparently regressed appeared again at a later time. These changes are characteristically described under the rubric of tumor regression. Host reactive cells such as neutrophils, eosinophils, macrophages, and fibroblasts were observed in some tumors. One of the tumors was a low grade hemangiosarcoma, another a well-differentiated fibrosarcoma, and the rest poorly differentiated sarcomas. Cells from two tumors initiated by 500 and 5000 cells multiplied slowly in early passages in culture, particularly when seeded at low densities at which they appeared to sustain cumulative damage even when multiplying. In later passages, the "low dose" tumor cells gained the capacity to multiply in culture after seeding at low densities, but it took up to 50 cell generations to reach this capacity. The loss of growth capacity on plastic of cells from the low dose tumors and its subsequent restoration by passaging in culture may provide a quantitative method for analyzing the type of cellular change which underlies tumor progression.

摘要

将含有5×10⁵至5×10¹个细胞的系列稀释液皮下接种到裸鼠体内,并记录肿瘤的发展过程。接种后2 - 3周内,最高细胞浓度产生了快速生长的低分化肉瘤。将产生的肿瘤进行外植培养时,得到的细胞在塑料培养皿上增殖的速度几乎与其用于启动肿瘤的祖细胞一样快,并且只要在琼脂培养基中省略胰蛋白胨磷酸盐肉汤,它们在琼脂中的集落形成效率就很高。较低细胞浓度启动的肿瘤出现时间明显延迟,且生长速度缓慢。至少有一个肿瘤消退,还有一个明显消退的肿瘤在后期再次出现。这些变化通常在肿瘤消退的标题下进行描述。在一些肿瘤中观察到了宿主反应性细胞,如中性粒细胞、嗜酸性粒细胞、巨噬细胞和成纤维细胞。其中一个肿瘤是低级别血管肉瘤,另一个是高分化纤维肉瘤,其余的是低分化肉瘤。由500个和5000个细胞启动的两个肿瘤的细胞在培养早期传代时增殖缓慢,尤其是在低密度接种时,即使增殖时它们似乎也会持续受到累积损伤。在后期传代中,“低剂量”肿瘤细胞在低密度接种后获得了在培养中增殖的能力,但需要多达50个细胞世代才能达到这种能力。低剂量肿瘤细胞在塑料培养皿上生长能力的丧失及其随后通过传代培养恢复的现象,可能为分析肿瘤进展背后的细胞变化类型提供一种定量方法。

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