乳房外Paget病中错配修复基因功能异常与PI3K/AKT通路在侵袭中的作用

项目名称： 乳房外Paget病中错配修复基因功能异常与PI3K/AKT通路在侵袭中的作用

项目编号： No.81472616

项目类型： 面上项目

立项/批准年度： 2015

项目学科： 医药、卫生

项目作者： 关明

作者单位： 复旦大学

项目金额： 72万元

中文摘要： 乳房外Paget病(extramammary paget's disease，EMPD)是一少见的皮肤恶性肿瘤。由于缺乏分子标志物，患者常被误诊且容易伴发或者继发其他部位的恶性肿瘤，严重影响了患者的预后和生存。我们曾采用二代测序等技术发现30% EMPD患者携有MLH1或MSH2基因的突变；且肿瘤组织中PIK3CA和AKT1的突变率为35%，与肿瘤的侵袭密切相关， 提示DNA错配修复（MMR）基因功能异常以及PIK3CA和AKT1突变引起的PI3K/AKT信号通路异常活化在EMPD发生、发展中起了重要作用。本项目将在EMPD患者中全面筛查MMR系统，首次尝试从MMR基因突变和沉默导致遗传不稳定的角度来阐述EMPD发病的遗传学背景和其易伴发肿瘤的分子机理，揭示EMPD发展过程中PI3K/AKT通路激活后对E-cadherin调控作用和相关的下游效应分子，为该病的诊断和治疗提供新靶点和新策略。

中文关键词： C25_其它肿瘤；乳房外Paget；病；错配修复基因；信号传导；分子诊断

英文摘要： Extramammary Paget's disease (EMPD), a rare skin malignant tumor, is predisoposed to misdiagnosed, since there is lack of biomarker for its early diagnosis. We applied high-throughput pralleled seuqncing strategy to screen the genetic alternations in the malignant tissues of EMPD patients, and found 30% of the patients harbored the mutations in MLH1 and MSH2 gene. The PIK3CA and AKT mutations were detected in 35% of the maligancies, which were validated to be relevent to the tumor migration. Given these data, we are justifed to induce that imperiled DNA mismatch repare (MMR) gene function and mutation caused PIK3CA/AKT pathway hyperactivation may play an important role in the pathogenesis and development of EMPD. In this study, we will make a thorough genetic and epigenetic screen on the MMR system, and explain the molecular background and genetic vulnerability of EMPD with a perspective of MMR mutation and silence. This study will also shed a light on the mechanism of the PI3K/AKT pathway activation mediated E-cadherin modulation and its downstream molecular network, providing the diagnosis and treatment of EMPD with a new target and strategy.

英文关键词： other cancer;extramammary Paget's disease;mismatch repair gene;signal transduction;molecular diagnosis