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Time-dependent Gene Expression Analysis of the Developing Superior Olivary Complex

机译:发展优质寡糖的时间依赖性基因表达分析

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The superior olivary complex (SOC) is an essential auditory brainstem relay involved in sound localization. To identify the genetic program underlying its maturation, we profiled the rat SOC transcriptome at postnatal days 0, 4, 16, and 25 (P0, P4, P16, and P25, respectively), using genome-wide microarrays (41,012 oligonucleotides (oligos)). Differences in gene expression between two consecutive stages were highest between P4 and P16 (3.6%) and dropped to 0.06% between P16 and P25. To identify SOC-related genetic programs, we also profiled the entire brain at P4 and P25. The number of differentially expressed oligonucleotides between SOC and brain almost doubled from P4 to P25 (4.4% versus 7.6%). These data demonstrate considerable molecular specification around hearing onset, which is rapidly finalized. Prior to hearing onset, several transcription factors associated with the peripheral auditory system were up-regulated, probably coordinating the development of the auditory system. Additionally, crystallin-γ subunits and serotonin-related genes were highly expressed. The molecular repertoire of mature neurons was sculpted by SOC-related up- and down-regulation of voltage-gated channels and G-proteins. Comparison with the brain revealed a significant enrichment of hearing impairment-related oligos in the SOC (26 in the SOC, only 11 in the brain). Furthermore, 29 of 453 SOC-related oligos mapped within 19 genetic intervals associated with hearing impairment. Together, we identified sequential genetic programs in the SOC, thereby pinpointing candidates that may guide its development and ensure proper function. The enrichment of hearing impairment-related genes in the SOC may have implications for restoring hearing because central auditory structures might be more severely affected than previously appreciated.
机译:优质的橄榄球复合体(SOC)是涉及声音本地化的基本听觉脑干继电器。为了识别其成熟的基本遗传计划,我们使用基因组微阵列(41,012寡核苷酸(寡核苷酸)(41,012寡核苷酸(寡核苷酸)(41,012) )。在P4和P16(3.6%)之间,两个连续阶段之间基因表达的差异最高,P16和P25之间的0.06%。为了识别与SoC相关的遗传程序,我们还在P4和P25中分析了整个大脑。 SOC和脑之间的差异表达寡核苷酸的数量几乎加倍P4至P25(4.4%而与7.6%)。这些数据展示了听力发作周围的相当大的分子规范,这是迅速最终确定的。在听力发作之前,有关与外围听觉系统相关的几个转录因子是上调的,可能协调听觉系统的发展。另外,高度表达了晶体素-γ亚基和血清素相关基因。成熟神经元的分子曲目通过SOC相关的和下调电压门控通道和G-蛋白而雕刻。与大脑的比较揭示了在SoC中的听力有损相关的寡核苷酸(SoC中的26位,大脑中只有11个)的显着富集。此外,在与听力障碍相关的19个遗传间隔内映射了29个中的453个相关的寡核苷酸中的29个。我们一起确定了SOC中的连续遗传程序,从而确定了可能引导其开发并确保正常功能的候选人。对SOC中的听力有害相关基因的丰富可能对恢复听力有影有影响,因为中央听觉结构可能比以前欣赏更严重的影响。

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