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引用次数: 74

摘要

我们的研究主要集中在花生四烯酸及其产物在化学和紫外光诱导的小鼠皮肤癌模型中的作用,重点是确定前列腺素(pg)的重要性,前列腺素是由环氧化酶(COX)的两种亚型合成的。不同类型的肿瘤启动子可上调角质形成细胞中COX-2的表达,而COX-1的表达变化不大,提示可通过多种信号通路调控COX-2的表达。我们发现两种COX亚型的表达都通过PG处理而增加,并且这种自我调节通过与cAMP信号通路相连的PG受体发生。我们还观察到COX-2在乳头状瘤和癌中的组成性上调,无论是化学启动-促进还是紫外线照射致癌实验。接下来,我们研究了COX-2表达所需的顺式因子和交易因子。COX-2启动子的两个区域,一个E盒和一个核因子- il6 (NF-IL6)位点,通过荧光素酶报告载体含有启动子的各个5'侧区域的瞬时转染,被鉴定为正调控元件。我们发现COX-2在肿瘤中的过表达可能是由于CCAAT/增强子结合蛋白(C/EBP)家族转录因子的表达模式失调引起的。为了证明PG合成在致癌过程中的重要性,在紫外线致癌过程中口服或局部使用了几种非甾体抗炎药(NSAIDs)。饮食中给予吲哚美辛、吡罗西康或选择性COX-2抑制剂塞来昔布可防止紫外线诱发皮肤癌的发生,可达85%。此外,塞来昔布有治疗作用,因为它使原有肿瘤消退。每次紫外线照射后局部使用吲哚美辛也有效,表明暴露后预防皮肤癌的方法可能有效。总的来说,这些研究表明前列腺素在皮肤癌的发展中起着关键作用。
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Is cyclooxygenase-2 important in skin carcinogenesis?
Our studies have focused on the role of arachidonic acid and its products in chemically and UV light-induced murine models of skin carcinogenesis, with an emphasis on determining the importance of prostaglandins (PGs), which are synthesized by the two isoforms of cyclooxygenase (COX). Different types of tumor promoters elevate COX-2 expression in keratinocytes, with little change in COX-1, suggesting that there are multiple signaling pathways by which COX-2 expression can be regulated. We found that the expression of both COX isoforms is increased by treatment with PGs and that this autoregulation occurs via PG receptors linked to a cAMP signaling pathway. We also observed that COX-2 is constitutively upregulated in papillomas and carcinomas from either chemical initiation-promotion or UV-irradiation carcinogenesis experiments. We next investigated cis- and transacting factors required for COX-2 expression. Two regions of the COX-2 promoter, an E box and a nuclear factor-IL6 (NF-IL6) site, were identified as positive regulatory elements through transient transfection with luciferase reporter vectors containing various 5'-flanking regions of the promoter. We found that overexpression of COX-2 in tumors maybe caused by a dysregulation in the expression pattern of the CCAAT/enhancer binding protein (C/EBP) family of transcription factors. To demonstrate the importance of PG synthesis in the carcinogenesis process, several nonsteroidal anti-inflammatory (NSAIDs) drugs were administered either orally or topically during UV carcinogenesis. Dietary administration of indomethacin, piroxicam, or the selective COX-2 inhibitor celecoxib prevented the development of UV-induced skin cancers by up to 85%. In addition, celecoxib had therapeutic efficacy in that it caused regression of preexisting tumors. Topical administration of indomethacin after each UV exposure was also effective, suggesting that a postexposure approach to skin cancer prevention maybe effective. Collectively, these studies suggest that prostaglandins play a critical role in skin cancer development.
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