Sex differences in glutamate AMPA receptor subunits mRNA with fast gating kinetics in the mouse cochlea.

IF 3.1 4区 医学 Q2 NEUROSCIENCES Frontiers in Systems Neuroscience Pub Date : 2023-03-02 eCollection Date: 2023-01-01 DOI:10.3389/fnsys.2023.1100505
Nicholas R Lozier, Steven Muscio, Indra Pal, Hou-Ming Cai, María E Rubio
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Abstract

Evidence shows that females have increased supra-threshold peripheral auditory processing compared to males. This is indicated by larger auditory brainstem responses (ABR) wave I amplitude, which measures afferent spiral ganglion neuron (SGN)-auditory nerve synchrony. However, the underlying molecular mechanisms of this sex difference are mostly unknown. We sought to elucidate sex differences in ABR wave I amplitude by examining molecular markers known to affect synaptic transmission kinetics. Alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptors (AMPARs) mediate fast excitatory transmission in mature SGN afferent synapses. Each AMPAR channel is a tetramer composed of GluA2, 3, and 4 subunits (Gria2, 3, and 4 genes), and those lacking GluA2 subunits have larger currents, are calcium-permeable, and have faster gating kinetics. Moreover, alternatively spliced flip and flop isoforms of each AMPAR subunit affect channel kinetics, having faster kinetics those AMPARs containing Gria3 and Gria4 flop isoforms. We hypothesized that SGNs of females have more fast-gating AMPAR subunit mRNA than males, which could contribute to more temporally precise synaptic transmission and increased SGN synchrony. Our data show that the index of Gria3 relative to Gria2 transcripts on SGN was higher in females than males (females: 48%; males: 43%), suggesting that females have more SGNs with higher Gria3 mRNA relative to Gria2. Analysis of the relative abundance of the flip and flop alternatively spliced isoforms showed that females have a 2-fold increase in fast-gating Gria3 flop mRNA, while males have more slow-gating (2.5-fold) of the flip. We propose that Gria3 may in part mediate greater SGN synchrony in females. Significance Statement: Females of multiple vertebrate species, including fish and mammals, have been reported to have enhanced sound-evoked synchrony of afferents in the auditory nerve. However, the underlying molecular mediators of this physiologic sex difference are unknown. Elucidating potential molecular mechanisms related to sex differences in auditory processing is important for maintaining healthy ears and developing potential treatments for hearing loss in both sexes. This study found that females have a 2-fold increase in Gria3 flop mRNA, a fast-gating AMPA-type glutamate receptor subunit. This difference may contribute to greater neural synchrony in the auditory nerve of female mice compared to males, and this sex difference may be conserved in all vertebrates.

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小鼠耳蜗中具有快速门控动力学的谷氨酸 AMPA 受体亚基 mRNA 的性别差异。
有证据表明,与男性相比,女性的阈上外周听觉处理能力更强。这表现在听性脑干反应(ABR)I 波振幅较大,而听性脑干反应测量的是传入螺旋神经节神经元(SGN)与听觉神经的同步性。然而,这种性别差异的潜在分子机制大多不为人知。我们试图通过研究已知会影响突触传递动力学的分子标记来阐明 ABR 波 I 振幅的性别差异。α-氨基-3-羟基-5-甲基-4-异恶唑丙酸受体(AMPARs)介导成熟 SGN 传入突触的快速兴奋传递。每个 AMPAR 通道都是由 GluA2、3 和 4 亚基(Gria2、3 和 4 基因)组成的四聚体,缺乏 GluA2 亚基的 AMPAR 通道具有更大的电流、钙渗透性和更快的门控动力学。此外,每个 AMPAR 亚基的交替剪接翻转和翻转异构体也会影响通道动力学,那些含有 Gria3 和 Gria4 翻转异构体的 AMPAR 通道动力学更快。我们假设,与雄性相比,雌性 SGN 有更多的快通路 AMPAR 亚基 mRNA,这可能有助于更精确的时间性突触传递和增加 SGN 的同步性。我们的数据显示,相对于 Gria2 转录本,雌性 SGN 上 Gria3 的指数高于雄性(雌性:48%;雄性:43%),这表明相对于 Gria2,雌性有更多的 SGN 具有更高的 Gria3 mRNA。对翻转和翻转交替剪接异构体相对丰度的分析表明,雌性的快速门控 Gria3 翻转 mRNA 增加了 2 倍,而雄性的慢门控翻转 mRNA 增加了 2.5 倍。我们认为,Gria3 可能在一定程度上介导了雌性 SGN 的同步性。意义声明:据报道,包括鱼类和哺乳动物在内的多种脊椎动物的雌性听觉神经传入的声音诱发同步性增强。然而,这种生理性别差异的潜在分子介质尚不清楚。阐明与听觉处理过程中的性别差异有关的潜在分子机制,对于维护健康的耳朵和开发治疗两性听力损失的潜在方法都非常重要。这项研究发现,女性的 Gria3 flop mRNA(一种快速通路 AMPA 型谷氨酸受体亚基)增加了 2 倍。这种差异可能导致雌性小鼠的听觉神经比雄性小鼠具有更强的神经同步性,而且这种性别差异可能在所有脊椎动物中都是一致的。
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来源期刊
Frontiers in Systems Neuroscience
Frontiers in Systems Neuroscience Neuroscience-Developmental Neuroscience
CiteScore
6.00
自引率
3.30%
发文量
144
审稿时长
14 weeks
期刊介绍: Frontiers in Systems Neuroscience publishes rigorously peer-reviewed research that advances our understanding of whole systems of the brain, including those involved in sensation, movement, learning and memory, attention, reward, decision-making, reasoning, executive functions, and emotions.
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