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多阶段致癌过程中细胞信号通路的紊乱:内稳态的作用。

Disorders in cell circuitry during multistage carcinogenesis: the role of homeostasis.

作者信息

Weinstein I B

机构信息

Herbert Irving Comprehensive Cancer Center and Departments of Medicine, Genetics and Development and Public Health, Columbia University College of Physicians and Surgeons, 701 West 168th Street, New York, NY 10032, USA.

出版信息

Carcinogenesis. 2000 May;21(5):857-64. doi: 10.1093/carcin/21.5.857.

Abstract

The multistage process of carcinogenesis involves the progressive acquisition of mutations, and epigenetic abnormalities in the expression, of multiple genes that have highly diverse functions. An important group of these genes are involved in cell cycle control. Thus, cyclin D1 is frequently overexpressed in a varety of human cancers. Cylin D1 plays a critical role in carcinogenesis because (i) overexpression enhances cell transformation and tumorigenesis, and enhances the amplification of other genes, and (ii) an antisense cyclin D1 cDNA reverts the malignant phenotype of carcinoma cells. Therefore, cyclin D1 may be a useful biomarker in molecular epidemiology studies, and inhibitors of its function may be useful in both cancer chemoprevention and therapy. We discovered a paradoxical increase in the cell cycle inhibitors protein p27(Kip1) in a subset of human cancers, and obtained evidence for homeostatic feedback loops between cyclins D1 or E and p27(Kip1). Furthermore, derivatives of HT29 colon cancer cells with increased levels of p27(Kip1) showed increased sensitivity to induction of differentiation. This may explain why decreased p27(Kip1) in a subset of human cancers is associated with a high grade (poorly differentiated) histology and poor prognosis. Agents that increase cellular levels of p27(Kip1) may, therefore, also be useful in cancer therapy. Using an antisense Rb oligonucleotide we obtained evidence that the paradoxical increase in pRb often seen in human colon cancers protects these cells from growth inhibition and apopotosis. On the basis of these, and other findings, we hypothesize that homeostatic feedback mechanisms play a critical role in multistage carcinogenesis. Furthermore, because of their bizarre circuitry, cancer cells suffer from 'gene addiction' and 'gene hypersensitivity' disorders that might be exploited in both cancer prevention and chemotherapy.

摘要

癌症发生的多阶段过程涉及多个功能高度多样的基因逐步获得突变以及表达上的表观遗传异常。这些基因中的一个重要类别参与细胞周期调控。因此,细胞周期蛋白D1在多种人类癌症中经常过度表达。细胞周期蛋白D1在癌症发生中起关键作用,原因如下:(i)过度表达增强细胞转化和肿瘤发生,并增强其他基因的扩增;(ii)反义细胞周期蛋白D1 cDNA可逆转癌细胞的恶性表型。因此,细胞周期蛋白D1可能是分子流行病学研究中的一个有用生物标志物,其功能抑制剂可能在癌症化学预防和治疗中都有用。我们发现,在一部分人类癌症中,细胞周期抑制剂蛋白p27(Kip1)出现了矛盾性增加,并获得了细胞周期蛋白D1或E与p27(Kip1)之间存在稳态反馈环的证据。此外,p27(Kip1)水平升高的HT29结肠癌细胞衍生物对诱导分化表现出更高的敏感性。这可能解释了为什么在一部分人类癌症中p27(Kip1)水平降低与高分级(低分化)组织学和不良预后相关。因此,提高细胞内p27(Kip1)水平的药物可能在癌症治疗中也有用。使用反义Rb寡核苷酸,我们获得了证据,表明在人类结肠癌中经常看到的pRb矛盾性增加可保护这些细胞免受生长抑制和凋亡。基于这些及其他发现,我们假设稳态反馈机制在多阶段癌症发生中起关键作用。此外,由于其怪异的回路,癌细胞患有“基因成瘾”和“基因超敏”疾病,这在癌症预防和化疗中都可能被利用。

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