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在低分化而非高分化的视网膜母细胞瘤中,p53和p21waf-1表达与细胞凋亡或细胞存活相关。

p53 and p21waf-1 expression correlates with apoptosis or cell survival in poorly differentiated, but not well-differentiated, retinoblastomas.

作者信息

Divan A, Lawry J, Dunsmore I R, Parsons M A, Royds J A

机构信息

Institute for Cancer Studies, Medical School, University of Sheffield, United Kingdom.

出版信息

Cancer Res. 2001 Apr 1;61(7):3157-63.

Abstract

In human retinoblastomas, rare genetic mutations of the retinoblastoma gene cause massive cell proliferation, altered differentiation, and tumor formation; but paradoxically, this is accompanied by extensive apoptotic cell loss. We quantified the immunohistochemical distribution of p53, its downstream effector p21 (WAF-1), and apoptotic cells in 50 human retinoblastomas, within three concentric zones of sleeves of tumor cells surrounding blood vessels. In poorly differentiated retinoblastomas, both p53 expression and apoptosis increase toward the outer zone of tumor sleeves, whereas p21 expression occurs primarily within the inner zone. This staining pattern of p53 expression is reversed in well-differentiated tumors, whereas p21 staining and apoptotic cell distributions are unchanged. We detected no p53 mutations in four retinoblastomas and two retinoblastoma cell lines. We postulate that oxygen and cell "survival/growth factors" delivered via blood vessels protect retinoblastoma cells from apoptosis. In poorly differentiated tumors, apoptosis is spatially associated with increased p53 expression and may be p53 mediated, but in well-differentiated tumors, apoptosis does not colocalize with p53 and may be p53 independent. In retinoblastomas, p21 is involved not in cell death by apoptosis but in cell survival. Thus, p53 varies its expression (and by implication its function) with altered differentiation in retinoblastomas.

摘要

在人类视网膜母细胞瘤中,视网膜母细胞瘤基因的罕见基因突变会导致大量细胞增殖、分化改变和肿瘤形成;但矛盾的是,这同时伴有广泛的凋亡性细胞丢失。我们对50例人类视网膜母细胞瘤中p53、其下游效应分子p21(WAF-1)以及凋亡细胞的免疫组化分布进行了定量分析,这些样本取自围绕血管的肿瘤细胞袖套的三个同心区域内。在低分化视网膜母细胞瘤中,p53表达和凋亡均朝着肿瘤袖套的外层区域增加,而p21表达主要出现在内层区域。在高分化肿瘤中,p53表达的这种染色模式则相反,而p21染色和凋亡细胞分布不变。我们在4例视网膜母细胞瘤和2个视网膜母细胞瘤细胞系中未检测到p53突变。我们推测,通过血管输送的氧气和细胞“存活/生长因子”可保护视网膜母细胞瘤细胞免于凋亡。在低分化肿瘤中,凋亡在空间上与p53表达增加相关,可能由p53介导,但在高分化肿瘤中,凋亡与p53并不共定位,可能与p53无关。在视网膜母细胞瘤中,p21并非参与凋亡导致的细胞死亡,而是参与细胞存活。因此,在视网膜母细胞瘤中,p53会随着分化改变而改变其表达(进而暗示其功能)。

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