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Gene Expression Architecture of Mouse Dorsal and Tail Skin Reveals Functional Differences in Inflammation and Cancer

机译:小鼠背部和尾部皮肤的基因表达结构揭示了炎症和癌症的功能差异

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摘要

Inherited germline polymorphisms can cause gene expression levels in normal tissues to differ substantially between individuals. We present an analysis of the genetic architecture of normal adult skin from 470 genetically unique mice, demonstrating the effect of germline variants, skin tissue location, and perturbation by exogenous inflammation or tumorigenesis on gene signaling pathways. Gene networks related to specific cell types and signaling pathways, including sonic hedgehog (Shh), Wnt, Lgr family stem cell markers, and keratins, differed at these tissue sites, suggesting mechanisms for the differential susceptibility of dorsal and tail skin to development of skin diseases and tumorigenesis. The Pten tumor suppressor gene network is rewired in premalignant tumors compared to normal tissue, but this response to perturbation is lost during malignant progression. We present a software package for expression quantitative trait loci (eQTL) network analysis and demonstrate how network analysis of whole tissues provides insights into interactions between cell compartments and signaling molecules.
机译:遗传的种系多态性可导致正常组织中的基因表达水平在个体之间显着不同。我们目前对来自470位遗传独特的小鼠的正常成年皮肤的遗传结构进行了分析,证明了种系变体,皮肤组织位置以及基因信号通路上的外源性炎症或肿瘤发生的干扰。在这些组织部位,与特定细胞类型和信号通路相关的基因网络有所不同,包括声波刺猬(Shh),Wnt,Lgr家族干细胞标志物和角蛋白,这表明背侧和尾部皮肤对皮肤发育的敏感性不同疾病和肿瘤发生。与正常组织相比,Pten抑癌基因网络在恶变前肿瘤中进行了重组,但是在恶性进展过程中,这种对摄动的反应消失了。我们提供了用于表达定量性状基因座(eQTL)网络分析的软件包,并演示了整个组织的网络分析如何提供洞​​察到细胞区室和信号分子之间相互作用的信息。

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