动力蛋白2介导的核因子-κB与p53之间的相互作用参与了亚砷酸盐诱导的人胚肺成纤维细胞肿瘤发生过程。

mot-2-Mediated cross talk between nuclear factor-B and p53 is involved in arsenite-induced tumorigenesis of human embryo lung fibroblast cells.

作者信息

Li Yuan, Xu Yuan, Ling Min, Yang Ye, Wang Shoulin, Li Zhong, Zhou Jianwei, Wang Xinru, Liu Qizhan

机构信息

Department of Molecular Cell Biology and Toxicology, Nanjing Medical University, Jiangsu, People's Republic of China.

出版信息

Environ Health Perspect. 2010 Jul;118(7):936-42. doi: 10.1289/ehp.0901677. Epub 2010 Mar 3.

DOI:10.1289/ehp.0901677

PMID:20199942

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2920912/

Abstract

BACKGROUND

Inactivation of p53 is involved in arsenite-induced tumorigenesis; however, the molecular mechanisms remain poorly understood.

OBJECTIVE

We investigated the molecular mechanisms underlying the inactivation of p53 and neoplastic transformation induced by arsenite in human embryo lung fibroblast (HELF) cells.

METHODS

Anchorage-independent growth assays were performed, and tumorigenicity in intact animals was assessed to confirm arsenite-induced neoplastic transformation. We determined the levels and functions of p53, nuclear factor-kappa B (NF-B; a key transcriptional regulator), and mot-2 (a p53 inhibitor) and their relationships in arsenite-induced transformed HELF cells by two-dimensional electrophoresis, reverse-transcriptase polymerase chain reaction, Western blot, immunofluorescence, and co-immunoprecipitation assays.

RESULTS

Exposure of HELF cells to low levels of arsenite increased their proliferation rate and anchorage-independent growth and disrupted normal contact inhibition. When introduced into nude mice, transformed cells were tumorigenic. We used proteomic analysis to identify proteins with altered expression between untreated and arsenite-exposed cells. We found decreased expression of NF-B repressing factor (NKRF; an inhibitor of NF-B-mediated gene transcription), increased expression of mot-2, and increased activation of NF-B. Changes in cells exposed to 1.0 microM arsenite were more marked than changes in cells exposed to 0.5 or 2.0 microM arsenite. Inactivation of NF-B prevented malignant transformation induced by 1.0 microM arsenite. Moreover, we also identified a mechanism whereby NF-B regulated p53. Specifically, activation of NF-B up-regulated mot-2 expression, which prevented nuclear translocation of p53 and switched the binding preference of the p53 and NF-B coactivator CBP [cyclic AMP-responsive element binding protein (CREB) binding protein] from p53 to NF-B.

CONCLUSIONS

mot-2-mediated cross talk between NF-B and p53 appears to be involved in arsenite-induced tumorigenesis of HELF cells.

摘要

背景

p53失活参与了亚砷酸盐诱导的肿瘤发生；然而，其分子机制仍知之甚少。

目的

我们研究了亚砷酸盐诱导人胚肺成纤维细胞（HELF）中p53失活及肿瘤转化的分子机制。

方法

进行非贴壁依赖性生长试验，并评估完整动物中的致瘤性以确认亚砷酸盐诱导的肿瘤转化。我们通过二维电泳、逆转录聚合酶链反应、蛋白质免疫印迹、免疫荧光和免疫共沉淀试验，测定了亚砷酸盐诱导的转化HELF细胞中p53、核因子-κB（NF-κB；一种关键的转录调节因子）和mot-2（一种p53抑制剂）的水平和功能及其相互关系。

结果

将HELF细胞暴露于低水平的亚砷酸盐会增加其增殖速率和非贴壁依赖性生长，并破坏正常的接触抑制。当将转化细胞接种到裸鼠体内时，具有致瘤性。我们使用蛋白质组学分析来鉴定未处理细胞和亚砷酸盐处理细胞之间表达改变的蛋白质。我们发现NF-κB抑制因子（NKRF；NF-κB介导的基因转录的抑制剂）表达降低，mot-2表达增加，且NF-κB的激活增加。暴露于1.0μM亚砷酸盐的细胞中的变化比暴露于0.5或2.0μM亚砷酸盐的细胞中的变化更明显。NF-κB失活可阻止1.0μM亚砷酸盐诱导的恶性转化。此外，我们还确定了一种NF-κB调节p53的机制。具体而言，NF-κB的激活上调了mot-2的表达，这阻止了p53的核转位，并将p53与NF-κB共激活因子CBP[环磷酸腺苷反应元件结合蛋白（CREB）结合蛋白]的结合偏好从p53切换到NF-κB。

结论

mot-2介导的NF-κB与p53之间的相互作用似乎参与了亚砷酸盐诱导的HELF细胞肿瘤发生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4eb1/2920912/bd8f3ba95586/ehp-118-936f1.jpg

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动力蛋白2介导的核因子-κB与p53之间的相互作用参与了亚砷酸盐诱导的人胚肺成纤维细胞肿瘤发生过程。

mot-2-Mediated cross talk between nuclear factor-B and p53 is involved in arsenite-induced tumorigenesis of human embryo lung fibroblast cells.

作者信息

Li Yuan, Xu Yuan, Ling Min, Yang Ye, Wang Shoulin, Li Zhong, Zhou Jianwei, Wang Xinru, Liu Qizhan

机构信息

Department of Molecular Cell Biology and Toxicology, Nanjing Medical University, Jiangsu, People's Republic of China.