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大鼠噪声性听力损失中的硫醇-二硫化物稳态

Thiol-Disulfide Homeostasis in Noise-Induced Hearing Loss in Rats.

作者信息

Aydın Enes, Mungan Durankaya Serpil, Yilmaz Osman, Kirkim Günay, Aktaş Safiye, Neşelioğlu Salim, Erel Özcan, Olgun Yüksel, Dalgıç Abdullah

机构信息

Clinic of Ear-Nose and Throat, İstanbul Silivri State Hospital, İstanbul, Türkiye.

Department of Ear-Nose and Throat, Audiology Section, Dokuz Eylül University Institute of Health Sciences, İzmir, Türkiye.

出版信息

J Int Adv Otol. 2024 Nov 25;20(6):466-471. doi: 10.5152/iao.2024.241555.

Abstract

BACKGROUND

This study was designed to assess if thiol-disulfide homeostasis could be used as diagnostic biomarker in noise-induced hearing loss (NIHL) in a laboratory animal model.

METHODS

The study was carried out with a total of 28 female albino rats in 4 groups: group 1 (control group) included rats that were not exposed to noise or any study treatment; in group 2, following noise exposure, rats received 2 mg of dexamethasone per kilogram of body weight via the intramuscular route for 5 days; in Group 3, rats were exposed to noise and received a saline solution for 5 days, in a volume (0.15 cc) matched to that of dexamethasone administered in group 2; and in group 4, rats were exposed to noise, and blood samples were collected during the early phase to assess thiol-disulfide homeostasis without administering any treatment. Rats in groups 2, 3, and 4 were exposed to 120 dB noise in the 4 kHz octave band for 4 hours. The auditory brainstem response (ABR) test was performed in all groups on day 1 after noise exposure and was repeated in groups 1, 2, and 3 on day 5. Auditory brainstem response thresholds were recorded at 8, 12, 16, 20, and 32 kHz frequencies. Groups 1, 2, and 3 rats were sacrificed on day 5, and group 4 rats were sacrificed by exsanguination on day 1 after noise exposure. Venous blood samples collected from the caudal vena cava were centrifuged and sent to the corresponding laboratory for thiol-disulfide homeostasis studies. After sacrificing the rats, the right and left temporal bones of each rat were removed and stained with hematoxylin eosin for histological studies to explore any pyknotic changes in spiral ganglion cells.

RESULTS

Intergroup comparisons by frequency on day 5 of noise exposure showed statistically significantly lower responses in ABR measurements at 8 kHz, 12 kHz, and 16 kHz in group 2 compared to group 3 (P = .003, P=.006, and P=.002). Improvements were observed with dexamethasone administered for therapeutic purposes, particularly if the hearing loss was induced by low-frequency noise. In the assessment of the parameters of thiol-disulfide homeostasis, disulfide/native thiol and disulfide/total thiol ratios and ischemia-modified albumin (IMA) levels were higher in group 4 than in other groups, although only the differences between group 1 and group 4 reached statistical significance.

CONCLUSION

According to this study, thiol-disulfide homeostasis and IMA can be shown as diagnostic biomarkers in NIHL, especially in the early period. The results from our study suggest that these markers may be used as adjunctive diagnostic tools in NIHL, in addition to audiological studies. However, this issue can be clarified with further clinical studies.

摘要

背景

本研究旨在评估在实验动物模型中,硫醇 - 二硫键稳态是否可作为噪声性听力损失(NIHL)的诊断生物标志物。

方法

本研究共使用28只雌性白化大鼠,分为4组:第1组(对照组)包括未暴露于噪声或任何研究处理的大鼠;第2组,在噪声暴露后,大鼠通过肌肉注射途径接受每千克体重2毫克地塞米松,持续5天;第3组,大鼠暴露于噪声并接受5天的生理盐水,其体积(0.15立方厘米)与第2组给予的地塞米松体积相同;第4组,大鼠暴露于噪声,在早期阶段采集血样以评估硫醇 - 二硫键稳态,不给予任何处理。第2、3和4组的大鼠在4千赫兹倍频程频段暴露于120分贝噪声4小时。在噪声暴露后第1天对所有组进行听觉脑干反应(ABR)测试,并在第5天对第1、2和3组重复测试。记录8、12、16、20和32千赫兹频率下的听觉脑干反应阈值。第1、2和3组大鼠在第5天处死,第4组大鼠在噪声暴露后第1天放血处死。从尾静脉采集的静脉血样本离心后送至相应实验室进行硫醇 - 二硫键稳态研究。处死大鼠后,取出每只大鼠的左右颞骨,用苏木精伊红染色进行组织学研究,以探索螺旋神经节细胞的任何核固缩变化。

结果

噪声暴露第5天按频率进行的组间比较显示,与第3组相比,第2组在8千赫兹、12千赫兹和16千赫兹的ABR测量反应在统计学上显著更低(P = 0.003、P = 0.006和P = 0.002)。观察到地塞米松用于治疗目的有改善,特别是如果听力损失由低频噪声引起。在硫醇 - 二硫键稳态参数评估中,第4组的二硫键/天然硫醇和二硫键/总硫醇比率以及缺血修饰白蛋白(IMA)水平高于其他组,尽管只有第1组和第4组之间的差异达到统计学意义。

结论

根据本研究,硫醇 - 二硫键稳态和IMA可作为NIHL的诊断生物标志物,尤其是在早期。我们的研究结果表明,除了听力研究外,这些标志物可作为NIHL的辅助诊断工具。然而,这一问题可通过进一步的临床研究加以阐明。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6a5c/11639554/b54ddefc9d0c/jiao-20-6-466_f001.jpg

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