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QTL Mapping of Endocochlear Potential Differences between C57BL/6J and BALB/cJ mice

机译:C57BL / 6J和BALB / cJ小鼠之间的内胚层电位差异的QTL定位

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摘要

We reported earlier that the endocochlear potential (EP) differs between C57BL/6J (B6) and BALB/cJ (BALB) mice, being lower in BALBs by about 10 mV (Ohlemiller et al. Hear Res 220: 10–26, 2006). This difference corresponds to strain differences with respect to the density of marginal cells in cochlear stria vascularis. After about 1 year of age, BALB mice also tend toward EP reduction that correlates with further marginal cell loss. We therefore suggested that early sub-clinical features of the BALB stria vascularis may predispose these mice to a condition modeling Schuknecht’s strial presbycusis. We further reported (Ohlemiller et al. J Assoc Res Otolaryngol 12: 45–58, 2011) that the acute effects of a 2-h 110 dB SPL noise exposure differ between B6 and BALB mice, such that the EP remains unchanged in B6 mice, but is reduced by 40–50 mV in BALBs. In about 25 % of BALBs, the EP does not completely recover, so that permanent EP reduction may contribute to noise-induced permanent threshold shifts in BALBs. To identify genes and alleles that may promote natural EP variation as well as noise-related EP reduction in BALB mice, we have mapped related quantitative trait loci (QTLs) using 12 recombinant inbred (RI) strains formed from B6 and BALB (CxB1–CxB12). EP and strial marginal cell density were measured in B6 mice, BALB mice, their F1 hybrids, and RI mice without noise exposure, and 1–3 h after broadband noise (4–45 kHz, 110 dB SPL, 2 h). For unexposed mice, the strain distribution patterns for EP and marginal cell density were used to generate preliminary QTL maps for both EP and marginal cell density. Six QTL regions were at least statistically suggestive, including a significant QTL for marginal cell density on chromosome 12 that overlapped a weak QTL for EP variation. This region, termed Maced (Marginal cell density QTL) supports the notion of marginal cell density as a genetically influenced contributor to natural EP variation. Candidate genes for Maced notably include Foxg1, Foxa1, Akap6, Nkx2-1, and Pax9. Noise exposure produced significant EP reductions in two RI strains as well as significant EP increases in two RI strains. QTL mapping of the EP in noise-exposed RI mice yielded four suggestive regions. Two of these overlapped with QTL regions we previously identified for noise-related EP reduction in CBA/J mice (Ohlemiller et al. Hear Res 260: 47–53, 2010) on chromosomes 5 and 18 (Nirep). The present map may narrow the Nirep interval to a ~10-Mb region of proximal Chr. 18 that includes Zeb1, Arhgap12, Mpp7, and Gjd4. This study marks the first exploration of natural gene variants that modulate the EP. Their orthologs may underlie some human hearing loss that originates in the lateral wall.Electronic supplementary materialThe online version of this article (doi:10.1007/s10162-016-0558-8) contains supplementary material, which is available to authorized users.
机译:我们之前报道过,C57BL / 6J(B6)和BALB / cJ(BALB)小鼠的耳蜗电位(EP)不同,在BALBs中大约降低10 mV(Ohlemiller et al。Hear Res 220:10–26,2006) 。该差异对应于耳蜗血管纹中边缘细胞密度的应变差异。大约1岁以后,BALB小鼠也趋向于EP降低,这与进一步的边缘细胞丢失有关。因此,我们建议BALB血管纹的早期亚临床特征可能会使这些小鼠处于模拟Schuknecht纹状体老视的状况。我们进一步报道(Ohlemiller等人,J Assoc Res Otolaryngol 12:45-58,2011),B6和BALB小鼠在2 h 110 dB SPL噪声暴露下的急性影响不同,因此B6小鼠的EP保持不变,但在BALB中降低了40–50 mV。在大约25%的BALB中,EP不能完全恢复,因此永久性EP降低可能会导致噪声引起BALB中的永久性阈值漂移。为了鉴定可能促进BALB小鼠自然EP变异以及与噪声相关的EP降低的基因和等位基因,我们使用了由B6和BALB(CxB1–CxB12 )。在没有噪声暴露的B6小鼠,BALB小鼠,它们的F1杂种和RI小鼠中,以及宽带噪声后1-3小时(4-45 kHz,110 dB SPL,2小时),测量EP和部分边缘细胞密度。对于未暴露的小鼠,EP和边缘细胞密度的应变分布模式用于生成EP和边缘细胞密度的初步QTL图。六个QTL区域至少在统计上具有启发性,其中包括12号染色体上边缘细胞密度的显着QTL,与EP变异的弱QTL重叠。这个被称为Maced(边缘细胞密度QTL)的区域支持边缘细胞密度的概念,它是自然EP变异的遗传影响因素。 Maced的候选基因主要包括Foxg1,Foxa1,Akap6,Nkx2-1和Pax9。噪声暴露导致两种RI菌株的EP显着降低,以及两种RI菌株的EP显着增加。暴露于噪音的RI小鼠中EP的QTL定位产生了四个提示区域。其中两个与QTL区域重叠,我们先前在CBA / J小鼠的5号和18号染色体(Nirep)上发现了与噪声相关的EP降低(Ohlemiller等人,Hear Res 260:47-53,2010)。本图可将Nirep区间缩小到近端Chr的〜10 Mb区域。 18,其中包括Zeb1,Arhgap12,Mpp7和Gjd4。这项研究标志着首次探索调节EP的天然基因变异。他们的直系同源物可能是源自侧壁的某些人类听力损失的基础。电子补充材料本文的在线版本(doi:10.1007 / s10162-016-0558-8)包含补充材料,授权用户可以使用。

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