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人肉瘤细胞系HT-1080中微细胞的起源

Origin of microcells in the human sarcoma cell line HT-1080.

作者信息

Buiķis I, Harju L, Freivalds T

机构信息

Latvian Institute of Experimental and Clinical Medicine, Riga.

出版信息

Anal Cell Pathol. 1999;18(2):73-85. doi: 10.1155/1999/461805.

Abstract

The aim of this study was to investigate the development of microcells in the human sarcoma cell line HT-1080 after interference with thiophosphamidum. We found that damaged interphase macrocells located at the projection of the nucleolus may form one or several microcells. The micronuclei of the microcells intensively incorporate the thymidine analogue 5-bromo-2'-deoxyuridine and strongly express argyrophilic nucleolar organiser region proteins. At an early phase of the development, the micronuclei contain fragmented DNA, but in subsequent phases, the micronuclei accumulate polymeric DNA, simultaneously with an increase in their size. After desintegration of the damaged macrocell, the microcells appear in the intercellular space. The microcells can enter mitosis and they strongly express the lung resistance protein. Electron microscopic observations suggest that coiled bodies are involved in the development of the microcells. Since the observed path of microcell formation differs from apoptotic cell fragmentation into apoptotic bodies, we propose a new term for this microcell development: sporosis. We suggest that self-renewal of the tumour stem cells is likely based on sporosis.

摘要

本研究旨在探讨硫磷酰胺干扰后人肉瘤细胞系HT-1080中微细胞的发育情况。我们发现,位于核仁突出部位的受损间期巨细胞可形成一个或多个微细胞。微细胞的微核强烈摄取胸腺嘧啶类似物5-溴-2'-脱氧尿苷,并强烈表达嗜银核仁组织区蛋白。在发育早期,微核含有碎片化的DNA,但在随后的阶段,微核积累聚合DNA,同时其大小增加。受损巨细胞解体后,微细胞出现在细胞间隙中。微细胞可进入有丝分裂,且强烈表达肺耐药蛋白。电子显微镜观察表明,卷曲小体参与了微细胞的发育。由于观察到的微细胞形成途径不同于凋亡细胞碎裂形成凋亡小体,我们为此微细胞发育提出一个新术语:芽生。我们认为肿瘤干细胞的自我更新可能基于芽生。

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