Alcohol and Breast Cancer

酒精与乳腺癌

• 批准号: 7352613
• 负责人: JIA LUO
• 金额: $ 18.02万
• 依托单位: WEST VIRGINIA UNIVERSITY
• 依托单位国家: 美国
• 财政年份: 2008
• 资助国家: 美国
• 起止时间: 2008-03-05 至 2008-11-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7352613
• 关键词: Adaptor Signaling Protein; Adult; Alcohol abuse; Alcohol consumption; Alcohols; American; Animal Model; Breast Cancer Cell; Cell Communication; Cell-Cell Adhesion; Cells; Cellular Structures; Colon, Rectum; Complex; Development; Disease; Disruption; Dissociation; E-Cadherin; Epidemiologic Studies; Epidermal Growth Factor Receptor; Epithelial Cells; Esophagus; Ethanol; Etiology; Family; Goals; Health; Heavy Drinking; Human; In Vitro; Invasive; Larynx; Liver; Malignant - descriptor; Malignant Neoplasms; Mammary Neoplasms; Mammary Tumorigenesis; Mammary gland; Mediating; Medical; Membrane; Molecular; Mucin-1 Staining Method; Mucins; Neoplasm Metastasis; Nude Mice; Oral cavity; Organ; Outcome; Ovary; Oxidative Stress; Pathogenesis; Patients; Pharyngeal structure; Phosphorylation; Play; Protein Tyrosine Kinase; Proto-Oncogenes; Reactive Oxygen Species; Research Personnel; Risk; Role; Stomach; Testing; Transcriptional Activation; Transgenic Mice; Transgenic Organisms; Tumor Promoters; Tumor Promotion; United States; Up-Regulation; alcohol effect; alcohol related problem; alcoholism/alcohol abuse; cancer cell; cancer risk; carcinogenesis; cell motility; cell transformation; chronic alcohol ingestion; cost; human disease; in vivo; in vivo Model; insight; malignant breast neoplasm; medical complication; member; migration; novel; problem drinker; tumor; tumor progression; tumorigenesis

DESCRIPTION (provided by applicant): Alcoholism, alcohol abuse, and the medical complications of excessive drinking are major world-wide health problems. Alcohol is a tumor promoter. Epidemiological studies indicate that heavy alcohol consumption increases risk of breast cancer and is associated with advanced and invasive breast tumors. However, the etiology of alcohol-induced tumor promotion is elusive. Cellular/molecular mechanisms underlying alcohol-promoted tumor development and progression remain unknown. ErbB2, a member of the epidermal growth factor receptor tyrosine kinase family, is frequently over-expressed in human breast cancers. We have demonstrated that alcohol dramatically promotes migration/invasion of mammary epithelial cells and breast cancer cells over-expressing ErbB2. We also reveal that the human transmembrane mucin (MUC1) is highly sensitive to alcohol. ¿-catenin is a proto-oncogene and plays an important role in tumorigenesis and cancer progression. The E-cadherin/¿-catenin complex, a critical component of cell-cell adherens, maintains the integrity of epithelial cell interactions and regulates cell migration/invasion. We propose a novel role of MUC1 as an adaptor protein that bridges ErbB2 and ¿-catenin and facilitate ErbB2/¿-catenin interaction and the dissociation of E- cadherin/ ¿-catenin complex. Our central hypothesis is that ethanol-induced oxidative stress up- regulates MUC1 as an adaptor protein to promote ErbB2/ ¿-catenin interaction which induces dissociation of the ¿-catenin/E-cadherin complex, leading to cell transformation and cell migration/invasion. Both in vitro and in vivo models will be utilized to test this novel hypothesis. Specific Aim 1 will establish the pivotal role of MUC1 in ethanol-promoted ErbB2/ ¿-catenin interaction. Specific Aim 2 will determine whether ethanol-promoted cell transformation and cancer cell migration/invasion is mediated by MUC1-dependent dissociation of the E-cadherin/2-catenin complex. Specific Aim 3 will investigate in vivo effects of ethanol. We will investigate the effect of ethanol on mammary tumorigenesis/metastasis in MMTV-Neu transgenic mice. We will further investigate the effect of ethanol on the interactions among MUC1, ErbB2, ¿-catenin and E-cadherin as well as the role of ROS and MUC1 in ethanol- mediated tumorigenesis/metastasis in the transgenic and nude mice. As a cohesive unit, the multi-disciplinary approaches using in vitro and in vivo models will systematically explore the mechanisms underlying alcohol-promoted tumorigenesis and malignant progression of breast cancer. The study will elucidate a novel function of ErbB2 and MUC1 in alcohol-induced tumor promotion. The expression/activity of ErbB2 and MUC1 is frequently aberrant in many other human cancers and in a variety of human diseases; their levels are also developmentally regulated. Understanding the interactions among alcohol, ErbB2 and MUC1 will also provide an important insight into the pathogenesis of some human diseases related to alcohol abuse as well as alcohol's teratogenic effect during development.

描述（由申请人提供）：酒精中毒、酒精滥用和过量饮酒的医学并发症是世界范围内的主要健康问题。酒精是一种肿瘤促进剂。流行病学研究表明，大量饮酒会增加患乳腺癌的风险，并与晚期和浸润性乳腺肿瘤有关。然而，酒精诱导的肿瘤促进的病因是难以捉摸的。酒精促进肿瘤发展和进展的细胞/分子机制仍然未知。ErbB 2是表皮生长因子受体酪氨酸激酶家族的成员，在人类乳腺癌中经常过度表达。我们已经证明，酒精显着促进迁移/乳腺上皮细胞和乳腺癌细胞过度表达ErbB 2的入侵。我们还发现，人跨膜粘蛋白（MUC 1）是高度敏感的酒精。连环蛋白是一种原癌基因，在肿瘤发生和癌症进展中起重要作用。E-钙粘蛋白β-连环蛋白复合物是细胞-细胞粘附的关键组分，维持上皮细胞相互作用的完整性并调节细胞迁移/侵袭。我们提出MUC 1作为一种衔接蛋白的新作用，它连接ErbB 2和<$-catenin，促进ErbB 2/<$-catenin相互作用和E-cadherin/<$-catenin复合物的解离。我们的中心假设是乙醇诱导的氧化应激上调MUC 1作为衔接蛋白，以促进ErbB 2/<$-连环蛋白相互作用，其诱导<$-连环蛋白/E-钙粘蛋白复合物的解离，导致细胞转化和细胞迁移/侵袭。将利用体外和体内模型来检验这一新假设。特异性目的1将确立MUC 1在乙醇促进的ErbB 2/β-连环蛋白相互作用中的关键作用。具体目标2将确定乙醇促进的细胞转化和癌细胞迁移/侵袭是否由E-钙粘蛋白/2-连环蛋白复合物的MUC 1依赖性解离介导。具体目标3将研究乙醇的体内效应。我们将研究乙醇对MMTV-Neu转基因小鼠乳腺肿瘤发生/转移的影响。我们将进一步研究乙醇对MUC 1、ErbB 2、<$-catenin和E-cadherin之间相互作用的影响，以及ROS和MUC 1在乙醇介导的转基因和裸鼠肿瘤发生/转移中的作用。作为一个紧密结合的单元，多学科的方法使用体外和体内模型将系统地探讨酒精促进乳腺癌的肿瘤发生和恶性进展的机制。该研究将阐明ErbB 2和MUC 1在酒精诱导的肿瘤促进中的新功能。ErbB 2和MUC 1的表达/活性在许多其他人类癌症和各种人类疾病中经常异常;它们的水平也受到发育调节。了解酒精，ErbB 2和MUC 1之间的相互作用也将提供一个重要的洞察一些人类疾病的发病机制与酒精滥用以及酒精的致畸作用在发展过程中。