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内耳感觉上皮再生的大规模基因表达谱。

Large scale gene expression profiles of regenerating inner ear sensory epithelia.

机构信息

Division of Human Genetics, Department of Genetics, Washington University School of Medicine, St. Louis, Missouri, United States of America.

出版信息

PLoS One. 2007 Jun 13;2(6):e525. doi: 10.1371/journal.pone.0000525.

Abstract

Loss of inner ear sensory hair cells (HC) is a leading cause of human hearing loss and balance disorders. Unlike mammals, many lower vertebrates can regenerate these cells. We used cross-species microarrays to examine this process in the avian inner ear. Specifically, changes in expression of over 1700 transcription factor (TF) genes were investigated in hair cells of auditory and vestibular organs following treatment with two different damaging agents and regeneration in vitro. Multiple components of seven distinct known signaling pathways were clearly identifiable: TGFbeta, PAX, NOTCH, WNT, NFKappaB, INSULIN/IGF1 and AP1. Numerous components of apoptotic and cell cycle control pathways were differentially expressed, including p27(KIP) and TFs that regulate its expression. A comparison of expression trends across tissues and treatments revealed identical patterns of expression that occurred at identical times during regenerative proliferation. Network analysis of the patterns of gene expression in this large dataset also revealed the additional presence of many components (and possible network interactions) of estrogen receptor signaling, circadian rhythm genes and parts of the polycomb complex (among others). Equal numbers of differentially expressed genes were identified that have not yet been placed into any known pathway. Specific time points and tissues also exhibited interesting differences: For example, 45 zinc finger genes were specifically up-regulated at later stages of cochlear regeneration. These results are the first of their kind and should provide the starting point for more detailed investigations of the role of these many pathways in HC recovery, and for a description of their possible interactions.

摘要

内耳感觉毛细胞(HC)的丧失是人类听力损失和平衡障碍的主要原因。与哺乳动物不同,许多低等脊椎动物可以再生这些细胞。我们使用跨物种微阵列来研究禽类内耳中的这个过程。具体来说,在使用两种不同的损伤剂进行处理并在体外再生后,研究了听觉和前庭器官中毛细胞中转录因子(TF)基因表达的变化。以下七个不同的已知信号通路的多个组成部分清晰可辨:TGFbeta、PAX、NOTCH、WNT、NFKappaB、INSULIN/IGF1 和 AP1。凋亡和细胞周期控制途径的许多组成部分的表达也不同,包括调节其表达的 p27(KIP)和 TF。跨组织和处理的表达趋势比较显示,在再生增殖过程中相同时间发生了相同的表达模式。对这个大型数据集的基因表达模式的网络分析还揭示了雌激素受体信号、昼夜节律基因和多梳复合物的部分(以及其他)的许多组成部分(和可能的网络相互作用)的存在。鉴定出了数量相等的尚未归入任何已知途径的差异表达基因。特定的时间点和组织也表现出有趣的差异:例如,45 个锌指基因在耳蜗再生的后期阶段特异性地上调。这些结果是首例,应该为更详细地研究这些途径在 HC 恢复中的作用以及描述它们的可能相互作用提供起点。

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