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首页> 外文期刊>British Journal of Dermatology >Expression profiling of microdissected cell populations selected from basal cells in normal epidermis and basal cell carcinoma.
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Expression profiling of microdissected cell populations selected from basal cells in normal epidermis and basal cell carcinoma.

机译:从正常表皮和基底细胞癌中的基底细胞中选出的微解剖细胞群的表达谱。

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摘要

Background Basal cell carcinomas (BCCs) are prevalent tumours with uniform histology that develop without any known precursor lesion. Alterations in the sonic hedgehog-patched1 signalling pathway are accepted as necessary events for tumorigenesis, and mutations in the patched1 gene are frequently present in tumours. Objectives To analyse transcript profiles in BCC. Methods We used laser-assisted microdissection to isolate and collect cell populations defined under the microscope. Peripheral cells from nests of BCC were selected to represent tumour cells, and normal keratinocytes from epidermis basal layer were used as control. Extracted RNA was amplified and hybridized on to a cDNA microarray. Results Our results show that BCC cells express a transcript signature that is significantly different from that of normal keratinocytes, and over 350 genes with various functions were identified as differentially expressed. The compiled data suggest an upregulation of the Wnt signalling pathway as a major event in BCC cells. Furthermore, tumour cells appear to have an increased sensitivity to oxygen radicals and dysregulated genes involved in antigen presentation. Results were validated at both the transcriptional level using real-time polymerase chain reaction and at the protein level using immunohistochemistry. Conclusions We show that microdissection in combination with robust strategies for RNA extraction, amplification and cDNA microarray analysis allow for reliable transcript profiling and that antibody-based proteomics provides an advantageous strategy for the analysis of corresponding differentially expressed proteins. We found that expression patterns were significantly altered in BCC cells compared with basal keratinocytes and that the Wnt signalling pathway was upregulated in tumour cells.
机译:背景基底细胞癌(BCC)是具有统一组织学的普遍肿瘤,其发展过程中没有任何已知的前体病变。声波hedgehog-patched1信号通路的改变被认为是发生肿瘤的必要事件,而patched1基因的突变经常出现在肿瘤中。目的分析BCC中的转录本概况。方法我们使用激光辅助显微解剖技术来分离和收集显微镜下确定的细胞群。选择来自BCC巢的外围细胞代表肿瘤细胞,并使用来自表皮基底层的正常角质形成细胞作为对照。提取的RNA被扩增并与cDNA微阵列杂交。结果我们的结果表明,BCC细胞表达的转录标志与正常角质形成细胞显着不同,并且鉴定出350多个具有各种功能的基因被差异表达。汇总的数据表明,Wnt信号通路的上调是BCC细胞中的主要事件。此外,肿瘤细胞似乎对涉及抗原呈递的氧自由基和失调基因具有更高的敏感性。使用实时聚合酶链反应在转录水平和使用免疫组织化学在蛋白质水平均验证了结果。结论我们表明,显微解剖结合用于RNA提取,扩增和cDNA微阵列分析的强大策略可以实现可靠的转录谱分析,而基于抗体的蛋白质组学为分析相应的差异表达蛋白提供了一种有利的策略。我们发现与基底角质形成细胞相比,BCC细胞中的表达模式发生了显着变化,并且肿瘤细胞中的Wnt信号通路被上调。

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