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脑源性神经营养因子调节听力耳蜗中的听觉功能。

Brain-derived neurotrophic factor modulates auditory function in the hearing cochlea.

机构信息

Department of Otolaryngology, University of Melbourne, 32 Gisborne Street, Melbourne, 3002, Victoria, Australia.

出版信息

J Assoc Res Otolaryngol. 2012 Feb;13(1):1-16. doi: 10.1007/s10162-011-0297-9. Epub 2011 Nov 16.

Abstract

Neurotrophins prevent spiral ganglion neuron (SGN) degeneration in animal models of ototoxin-induced deafness and may be used in the future to improve the hearing of cochlear implant patients. It is increasingly common for patients with residual hearing to undergo cochlear implantation. However, the effect of neurotrophin treatment on acoustic hearing is not known. In this study, brain-derived neurotrophic factor (BDNF) was applied to the round window membrane of adult guinea pigs for 4 weeks using a cannula attached to a mini-osmotic pump. SGN survival was first assessed in ototoxically deafened guinea pigs to establish that the delivery method was effective. Increased survival of SGNs was observed in the basal and middle cochlear turns of deafened guinea pigs treated with BDNF, confirming that delivery to the cochlea was successful. The effects of BDNF treatment in animals with normal hearing were then assessed using distortion product otoacoustic emissions (DPOAEs), pure tone, and click-evoked auditory brainstem responses (ABRs). DPOAE assessment indicated a mild deficit of 5 dB SPL in treated and control groups at 1 and 4 weeks after cannula placement. In contrast, ABR evaluation showed that BDNF lowered thresholds at specific frequencies (8 and 16 kHz) after 1 and 4 weeks posttreatment when compared to the control cohort receiving Ringer's solution. Longer treatment for 4 weeks not only widened the range of frequencies ameliorated from 2 to 32 kHz but also lowered the threshold by at least 28 dB SPL at frequencies ≥16 kHz. BDNF treatment for 4 weeks also increased the amplitude of the ABR response when compared to either the control cohort or prior to treatment. We show that BDNF applied to the round window reduces auditory thresholds and could potentially be used clinically to protect residual hearing following cochlear implantation.

摘要

神经营养因子可预防耳毒性诱导的耳聋动物模型中的螺旋神经节神经元 (SGN) 变性,并且将来可能用于改善人工耳蜗植入患者的听力。越来越多的残余听力患者接受人工耳蜗植入。然而,神经营养因子治疗对听觉的影响尚不清楚。在这项研究中,通过附接到微型渗透泵的套管将脑源性神经营养因子 (BDNF) 应用于成年豚鼠的圆窗膜,持续 4 周。首先在耳毒性耳聋的豚鼠中评估 SGN 的存活情况,以确定该给药方法是否有效。在接受 BDNF 治疗的耳聋豚鼠的基底和中部耳蜗转中观察到 SGN 存活增加,证实了向耳蜗的递送是成功的。然后使用畸变产物耳声发射 (DPOAE)、纯音和 click 诱发的听性脑干反应 (ABR) 评估正常听力动物中 BDNF 治疗的效果。DPOAE 评估表明,在套管放置后 1 周和 4 周时,治疗组和对照组的听力分别有 5dB SPL 的轻度缺陷。相比之下,与接受林格氏液的对照组相比,ABR 评估显示 BDNF 在 1 周和 4 周治疗后降低了特定频率 (8 和 16 kHz) 的阈值。4 周的延长治疗不仅拓宽了从 2 至 32 kHz 改善的频率范围,而且还降低了至少 28 dB SPL 的阈值频率≥16 kHz。与对照组或治疗前相比,BDNF 治疗 4 周还增加了 ABR 反应的幅度。我们表明,圆窗内应用 BDNF 可降低听觉阈值,并且将来可在临床上用于保护耳蜗植入后的残余听力。

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