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SV40介导的人角质形成细胞的转化与永生化

Transformation and immortalization of human keratinocytes by SV40.

作者信息

Steinberg M L, Defendi V

出版信息

J Invest Dermatol. 1983 Jul;81(1 Suppl):131s-6s. doi: 10.1111/1523-1747.ep12540905.

Abstract

We have studied the appearance of transformed properties following infection of human epidermal keratinocytes by the oncogenic virus SV40. Shortly after infection, only a small fraction of the cells are positive for SV40 T antigen by immunofluorescence; this fraction progressively increases upon serial subcultivation concomitant with an increase in plating/colony-forming efficiency and growth rate. The capacity of the cells to differentiate progressively decreases, as indicated by cytochemical staining and cornified cell-envelope formation induced by suspension in methyl cellulose. The infected cells enter a period of growth crisis characterized by cytopathology and cell death as the level of T antigen synthesis reaches about 90 percent positive cells at about the tenth serial passage. Viable cells emerging from the crisis period are found to exhibit anchorage-independent growth, as indicated by the formation of viable colonies in semisolid media, but there is considerable variability in colony formation among clones isolated from anchorage-independent populations. The emergent population also manifests phenotypic instability in terms of the appearance of variants, which, in contrast to uninfected cells, expresses a well-defined actin cytoskeleton. The infected cells eventually become "immortalized," as evidenced by an indefinite lifespan, i.e., replication capability maintained well beyond the ordinary time of senescence for uninfected cells. We present these findings in the context of a stage-specific model of epithelial transformation in vitro.

摘要

我们研究了致癌病毒SV40感染人表皮角质形成细胞后转化特性的表现。感染后不久,通过免疫荧光检测,只有一小部分细胞的SV40 T抗原呈阳性;随着连续传代培养,这部分细胞逐渐增加,同时接种/集落形成效率和生长速率也增加。细胞的分化能力逐渐下降,这通过细胞化学染色和甲基纤维素悬浮诱导的角质化细胞包膜形成得以体现。当T抗原合成水平在大约第十次连续传代时达到约90%阳性细胞时,感染细胞进入以细胞病理学和细胞死亡为特征的生长危机期。从危机期出现的存活细胞表现出不依赖贴壁生长,这通过在半固体培养基中形成存活集落得以表明,但从非贴壁生长群体中分离的克隆之间集落形成存在相当大的变异性。出现的群体在变体出现方面也表现出表型不稳定性,与未感染细胞相比,其表达明确的肌动蛋白细胞骨架。感染细胞最终变得“永生化”,这通过无限寿命得以证明,即复制能力在未感染细胞的正常衰老时间之后仍能很好地维持。我们在体外上皮细胞转化的阶段特异性模型的背景下呈现这些发现。

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